{"id":"paclitaxel","rwe":[{"pmid":"41903690","year":"2026","title":"Envafolimab combined with chemotherapy in advanced thymic carcinoma - first clinical experience with a novel subcutaneous programmed death-ligand 1 inhibitor.","finding":"","journal":"Anti-cancer drugs","studyType":"Clinical Study"},{"pmid":"41903689","year":"2026","title":"Poly(d,l-lactide-co-glycolide) (PLGA) nanoparticles in oncological therapeutics: Mechanisms of targeted delivery and encapsulation strategies for chemotherapeutics, gene modulators, and phytochemicals.","finding":"","journal":"Nanomedicine : nanotechnology, biology, and medicine","studyType":"Clinical Study"},{"pmid":"41903398","year":"2026","title":"Honeysuckle-derived vesicle-like nanoparticle and their hybrid vesicle as novel drug delivery systems for glioma therapy.","finding":"","journal":"Colloids and surfaces. B, Biointerfaces","studyType":"Clinical Study"},{"pmid":"41903397","year":"2026","title":"A semimechanistic PK/PD model-informed Taxus tablets' development: Accelerating early clinical translation of a taxane-based antitumor agent.","finding":"","journal":"Drug metabolism and disposition: the biological fate of chemicals","studyType":"Clinical Study"},{"pmid":"41902997","year":"2026","title":"The logarithmic phase as a therapeutic direction: evaluating pharmacological strategies against cancer progression.","finding":"","journal":"Clinical & translational oncology : official publication of the Federation of Spanish Oncology Societies and of the National Cancer Institute of Mexico","studyType":"Clinical Study"}],"_fda":{"id":"9a4e25af-2c07-46c8-a9f2-28ba744c8117","set_id":"0c12c77c-5fd4-48dc-a318-e96892233992","openfda":{"nui":["N0000175085","N0000175592"],"unii":["P88XT4IS4D"],"route":["INTRAVENOUS"],"rxcui":["312199"],"spl_id":["9a4e25af-2c07-46c8-a9f2-28ba744c8117"],"brand_name":["Paclitaxel"],"spl_set_id":["0c12c77c-5fd4-48dc-a318-e96892233992"],"package_ndc":["62332-620-05","62332-621-17","62332-622-50"],"product_ndc":["62332-620","62332-621","62332-622"],"generic_name":["PACLITAXEL"],"product_type":["HUMAN PRESCRIPTION DRUG"],"pharm_class_pe":["Microtubule Inhibition [PE]"],"substance_name":["PACLITAXEL"],"pharm_class_epc":["Microtubule Inhibitor [EPC]"],"manufacturer_name":["Alembic Pharmaceuticals Inc."],"application_number":["ANDA216874"],"is_original_packager":[true]},"version":"4","warnings":["WARNINGS Anaphylaxis and severe hypersensitivity reactions characterized by dyspnea and hypotension requiring treatment, angioedema, and generalized urticaria have occurred in 2 to 4% of patients receiving paclitaxel in clinical trials. Fatal reactions have occurred in patients despite premedication. All patients should be pretreated with corticosteroids, diphenhydramine, and H 2 antagonists. (see DOSAGE AND ADMINISTRATION ). Patients who experience severe hypersensitivity reactions to paclitaxel should not be rechallenged with the drug. Bone marrow suppression (primarily neutropenia) is dose-dependent and is the dose-limiting toxicity. Neutrophil nadirs occurred at a median of 11 days. Paclitaxel should not be administered to patients with baseline neutrophil counts of less than 1,500 cells/mm 3 (<1,000 cells/mm 3 for patients with KS). Frequent monitoring of blood counts should be instituted during paclitaxel treatment. Patients should not be re-treated with subsequent cycles of paclitaxel until neutrophils recover to a level >1,500 cells/mm 3 (>1,000 cells/mm 3 for patients with KS) and platelets recover to a level >100,000 cells/mm 3 . Severe conduction abnormalities have been documented in <1% of patients during paclitaxel therapy and in some cases requiring pacemaker placement. If patients develop significant conduction abnormalities during paclitaxel infusion, appropriate therapy should be administered and continuous cardiac monitoring should be performed during subsequent therapy with paclitaxel. Pregnancy Paclitaxel can cause fetal harm when administered to a pregnant woman. Administration of paclitaxel during the period of organogenesis to rabbits at doses of 3 mg/kg/day (about 0.2 the daily maximum recommended human dose on a mg/m 2 basis) caused embryo- and fetotoxicity, as indicated by intrauterine mortality, increased resorptions, and increased fetal deaths. Maternal toxicity was also observed at this dose. No teratogenic effects were observed at 1 mg/kg/day (about 1/15 the daily maximum recommended human dose on a mg/m 2 basis); teratogenic potential could not be assessed at higher doses due to extensive fetal mortality. There are no adequate and well-controlled studies in pregnant women. If paclitaxel is used during pregnancy, or if the patient becomes pregnant while receiving this drug, the patient should be apprised of the potential hazard to the fetus. Women of child-bearing potential should be advised to avoid becoming pregnant."],"pregnancy":["Pregnancy (See WARNINGS section)."],"overdosage":["OVERDOSAGE There is no known antidote for paclitaxel overdosage. The primary anticipated complications of overdosage would consist of bone marrow suppression, peripheral neurotoxicity, and mucositis. Overdoses in pediatric patients may be associated with acute ethanol toxicity (see PRECAUTIONS, Pediatric Use )."],"references":["REFERENCES NIOSH Alert: Preventing occupational exposures to antineoplastic and other hazardous drugs in healthcare settings. 2004. U.S. Department of Health and Human Services, Public Health Service, Centers for Disease Control and Prevention, National Institute for Occupational Safety and Health, DHHS (NIOSH) Publication No.2004-165. OSHA Technical Manual, TED 1-0.15A, Section VI: Chapter 2. Controlling occupational exposure to hazardous drugs. OSHA,1999. http://www.osha.gov/dts/osta/otm/otm_vi/otm_vi_2.html. American Society of Health-System Pharmacists. ASHP guidelines on handling hazardous drugs. Am J Health-Syst Pharm . 2006; 63:1172-1193. Polovich M, White JM, Kelleher LO, eds. 2005. Chemotherapy and biotherapy guidelines and recommendations for practice. 2nd ed. Pittsburgh, PA: Oncology Nursing Society. *DaunoXome ® is a registered trademark of Gilead Sciences, Inc. DOXIL ® is a registered trademark of ALZA Corporation. IVEX-2 ® is a registered trademark of the Millipore Corporation. Chemo Dispensing Pin™ is a trademark of B. Braun Medical Incorporated. Manufactured for: Alembic Pharmaceutical, Inc. Bedminster, NJ 07921, USA Made in India. Manufactured by: Alembic Pharmaceuticals Limited Panelav - 389 350, Gujarat, India. Issued: 11/2022 PATIENT INFORMATION Paclitaxel Injection, USP Read this patient information leaflet before you start taking paclitaxel. There may be new information. This information does not take the place of talking to your healthcare provider about your medical condition or your treatment. What is the most important information I should know about paclitaxel? Paclitaxel can cause serious side effects including death. Serious allergic reactions (anaphylaxis) can happen in people who receive paclitaxel injection. Anaphylaxis is a serious medical emergency that can lead to death and must be treated right away. Tell your healthcare provider right away if you have any of these signs of an allergic reaction: trouble breathing sudden swelling of your face, lips, tongue, throat, or trouble swallowing hives (raised bumps) or rash Your healthcare provider will give you medicines to lessen your chance of having an allergic reaction. What is paclitaxel? Paclitaxel is a prescription medicine used to treat some forms of: ovarian cancer breastcancer lung cancer Kaposi’s sarcoma It is not known if paclitaxel is safe or effective in children. Who should not receive paclitaxel? Do not receive paclitaxel if: you are allergic to any of the ingredients in paclitaxel. See the end of this leaflet for a complete list of ingredients in paclitaxel. are allergic to medicines containing polyoxy 35 castor oil. you have low white blood cell counts. What should I tell my healthcare provider before receiving paclitaxel? Before receiving paclitaxel, tell your healthcare provider about all your medical conditions, including if you: have liver problems have heart problemsare pregnant or plan to become pregnant. Paclitaxel can harm your unborn baby. Talk to your healthcare provider if you are pregnant or plan to become pregnant. are breast-feeding or plan to breast-feed. It is not known if paclitaxel passes into your breast milk. You and your healthcare provider should decide if you will receive paclitaxel or breast-feed. Tell your healthcare provider about all the medicines you take, including prescription and non- prescription medicines, vitamins, and herbal supplements. Know the medicines you take. Keep a list of them and show it to your healthcare provider and pharmacist when you get a new medicine. How will I receive paclitaxel? Paclitaxel is injected into a vein (intravenous [IV] infusion) by your healthcare provider. Your healthcare provider will do certain tests while you receive paclitaxel. What are the possible side effects of paclitaxel? Tell your healthcare provider right away if you have: severe stomach pain severe diarrhea The most common side effects of Paclitaxel Injection, USP include: low red blood cell count (anemia) feeling weak or tired hair loss ·numbness, tingling, or burning in your hands or feet (neuropathy) joint and muscle pain ·nausea and vomiting hypersensitivity reaction - trouble breathing; sudden swelling of your face, lips, tongue, throat, or trouble swallowing; hives (raised bumps) or rash diarrhea mouth or lip sores (mucositis) infections - if you have a fever (temperature above 100.4°F) or other sign of infection, tell your healthcare provider right away swelling of your hands, face, or feet bleeding events irritation at the injection site low blood pressure (hypotension) Tell your healthcare provider if you have any side effect that bothers you or that does not go away. These are not all the possible side effects of paclitaxel. For more information, ask your healthcare provider or pharmacist. Call your doctor for medical advice about side effects. You may report side effects to FDA at 1-800- FDA-1088 or Alembic Pharmaceutical, Inc. at 1-866-210-9797 General information about the safe and effective use of paclitaxel. Medicines are sometimes prescribed for purposes other than those listed in a patient information leaflet. Do not use paclitaxel for a condition for which it was not prescribed. Do not give paclitaxel to other people, even if they have the same symptoms that you have. It may harm them. This patient information leaflet summarizes the most important information about paclitaxel. If you would like more information, talk with your healthcare provider. You can ask your pharmacist or healthcare provider for information about paclitaxel that is written for health professionals. For more information go to www.alembicusa.com / or call 1-866-210-9797. What are the ingredients in paclitaxel? Active ingredient: paclitaxel, USP. Inactive ingredients include: Polyoxyl 35 castor oil, NF, Dehydrated alcohol, USP and Citric Acid, USP. What is cancer? Under normal conditions, the cells in your body divide and grow in an orderly, controlled way. Cell division and growth are necessary for the human body to perform its functions and to repair itself, when necessary. Cancer cells are different from normal cells because they are not able to control their own growth. The reasons for this abnormal growth are not yet fully understood. A tumor is a mass of unhealthy cells that are dividing and growing fast and in an uncontrolled way. When a tumor invades surrounding healthy body tissue, it is known as a malignant tumor. A malignant tumor can spread (metastasize) from its original site to other parts of the body if not found and treated early. Manufactured for: Alembic Pharmaceutical, Inc. Bedminster, NJ 07921, USA Made in India. Manufactured by: Alembic Pharmaceuticals Limited Panelav - 389 350, Gujarat, India. Issued: 11/2022 20037361"],"description":["DESCRIPTION Paclitaxel Injection, USP is a clear, colorless to slightly yellow viscous solution. It is supplied as a nonaqueous solution intended for dilution with a suitable parenteral fluid prior to intravenous infusion. Paclitaxel Injection, USP is available in 30 mg (5 mL), 100 mg (16.7 mL), and 300 mg (50 mL) multidose vials. Each mL of sterile nonpyrogenic solution contains 6 mg paclitaxel, USP, 527 mg of polyoxyl 35 castor oil, NF and 49.7% (v/v) dehydrated alcohol, USP and 2 mg citric acid, USP. Paclitaxel is a natural product with antitumor activity. Paclitaxel is obtained via a semi-synthetic process from Taxus baccata . The chemical name for paclitaxel is 5β,20-Epoxy-1,2α,4,7β, 10β,13α-hexahydroxytax-11-en-9-one 4,10-diacetate 2-benzoate 13-ester with (2R,3S)-N-benzoyl-3-phenylisoserine. Paclitaxel has the following structural formula: Paclitaxel, USP is a white to off-white crystalline powder with the empirical formula C 47 H 51 NO 14 and a molecular weight of 853.9. It is highly lipophilic, insoluble in water, and melts at around 216° to 217°C. paclitaxel-str"],"precautions":["PRECAUTIONS Contact of the undiluted concentrate with plasticized polyvinyl chloride (PVC) equipment or devices used to prepare solutions for infusion is not recommended. In order to minimize patient exposure to the plasticizer DEHP [di-(2-ethylhexyl)phthalate], which may be leached from PVC infusion bags or sets, diluted paclitaxel solutions should preferably be stored in bottles (glass, polypropylene) or plastic bags (polypropylene, polyolefin) and administered through polyethylene-lined administration sets. Paclitaxel should be administered through an in-line filter with a microporous membrane not greater than 0.22 microns. Use of filter devices such as IVEX-2® filters which incorporate short inlet and outlet PVC-coated tubing has not resulted in significant leaching of DEHP. Drug Interactions In a Phase 1 trial using escalating doses of paclitaxel (110 to 200 mg/m 2 ) and cisplatin (50 or 75 mg/m 2 ) given as sequential infusions, myelosuppression was more profound when paclitaxel was given after cisplatin than with the alternate sequence (i.e., paclitaxel before cisplatin). Pharmacokinetic data from these patients demonstrated a decrease in paclitaxel clearance of approximately 33% when paclitaxel was administered following cisplatin. The metabolism of paclitaxel is catalyzed by cytochrome P450 isoenzymes CYP2C8 and CYP3A4. Caution should be exercised when administering paclitaxel concomitantly with known substrates or inhibitors of the cytochrome P450 isoenzymes CTP2C8 and CYP3A4. Caution should be exercised when paclitaxel is concomitantly administered with known substrates (e.g., midazolam, buspirone, felodipine, lovastatin, eletriptan, sildenafil, simvastatin, and triazolam), inhibitors (e.g., atazanavir, clarithromycin, indinavir, itraconazole, ketoconazole, nefazodone, nelfinavir, ritonavir, saquinavir, and telithromycin), and inducers (e.g., rifampin and carbamazepine) of CYP3A4. (see CLINICAL PHARMACOLOGY ). Caution should also be exercised when paclitaxel is concomitantly administered with known substrates (e.g., repaglinide and rosiglitazone), inhibitors (e.g., gemfibrozil), and inducers (e.g., rifampin) of CYP2C8. (see CLINICAL PHARMACOLOGY ). Potential interactions between paclitaxel, a substrate of CYP3A4, and protease inhibitors (ritonavir, saquinavir, indinavir, and nelfinavir), which are substrates and/or inhibitors of CYP3A4, have not been evaluated in clinical trials. Reports in the literature suggest that plasma levels of doxorubicin (and its active metabolite doxorubicinol) may be increased when paclitaxel and doxorubicin are used in combination. Hematology Paclitaxel therapy should not be administered to patients with baseline neutrophil counts of less than 1,500 cells/mm 3 . In order to monitor the occurrence of myelotoxicity, it is recommended that frequent peripheral blood cell counts be performed on all patients receiving paclitaxel. Patients should not be re-treated with subsequent cycles of paclitaxel until neutrophils recover to a level >1,500 cells/mm 3 and platelets recover to a level >100,000 cells/mm 3 . In the case of severe neutropenia (<500 cells/mm 3 for 7 days or more) during a course of paclitaxel therapy, a 20% reduction in dose for subsequent courses of therapy is recommended. For patients with advanced HIV disease and poor-risk AIDS-related Kaposi's sarcoma, paclitaxel, at the recommended dose for this disease, can be initiated and repeated if the neutrophil count is at least 1,000 cells/mm 3 . Hypersensitivity Reactions Patients with a history of severe hypersensitivity reactions to products containing Polyoxyl 35 Castor Oil (e.g., cyclosporin for injection concentrate and teniposide for injection concentrate) should not be treated with paclitaxel. In order to avoid the occurrence of severe hypersensitivity reactions, all patients treated with paclitaxel should be premedicated with corticosteroids (such as dexamethasone), diphenhydramine and H 2 antagonists (such as cimetidine or ranitidine). Minor symptoms such as flushing, skin reactions, dyspnea, hypotension, or tachycardia do not require interruption of therapy. However, severe reactions, such as hypotension requiring treatment, dyspnea requiring bronchodilators, angioedema, or generalized urticaria require immediate discontinuation of paclitaxel and aggressive symptomatic therapy. Patients who have developed severe hypersensitivity reactions should not be rechallenged with paclitaxel. Cardiovascular Hypotension, bradycardia, and hypertension have been observed during administration of paclitaxel, but generally do not require treatment. Occasionally paclitaxel infusions must be interrupted or discontinued because of initial or recurrent hypertension. Frequent vital sign monitoring, particularly during the first hour of paclitaxel infusion, is recommended. Continuous cardiac monitoring is not required except for patients with serious conduction abnormalities. (See WARNINGS ). When paclitaxel is used in combination with doxorubicin for treatment of metastatic breast cancer, monitoring of cardiac function is recommended. (See ADVERSE REACTIONS ). Nervous System Although the occurrence of peripheral neuropathy is frequent, the development of severe symptomatology is unusual and requires a dose reduction of 20% for all subsequent courses of paclitaxel. Paclitaxel contains Dehydrated Alcohol USP, 396 mg/mL; consideration should be given to possible CNS and other effects of alcohol. (See PRECAUTIONS, Pediatric Use ). Hepatic There is limited evidence that the myelotoxicity of paclitaxel may be exacerbated in patients with serum total bilirubin >2 times ULN (see CLINICAL PHARMACOLOGY ). Extreme caution should be exercised when administering paclitaxel to such patients, with dose reduction as recommended in DOSAGE AND ADMINISTRATION , TABLE 17. Injection Site Reaction Injection site reactions, including reactions secondary to extravasation, were usually mild and consisted of erythema, tenderness, skin discoloration, or swelling at the injection site. These reactions have been observed more frequently with the 24-hour infusion than with the 3-hour infusion. Recurrence of skin reactions at a site of previous extravasation following administration of paclitaxel at a different site, i.e., “recall”, has been reported. More severe events such as phlebitis, cellulitis, induration, skin exfoliation, necrosis, and fibrosis have been reported. In some cases the onset of the injection site reaction either occurred during a prolonged infusion or was delayed by a week to 10 days. A specific treatment for extravasation reactions is unknown at this time. Given the possibility of extravasation, it is advisable to closely monitor the infusion site for possible infiltration during drug administration. Carcinogenesis, Mutagenesis, Impairment of Fertility The carcinogenic potential of paclitaxel has not been studied. Paclitaxel has been shown to be clastogenic in vitro (chromosome aberrations in human lymphocytes) and in vivo (micronucleus test in mice). Paclitaxel was not mutagenic in the Ames test of the CHO/HGPRT gene mutation assay. Administration of paclitaxel prior to and during mating produced impairment of fertility in male and female rats at doses equal to or greater than 1 mg/kg/day (about 0.04 the daily maximum recommended human dose on a mg/m 2 basis). At this dose, paclitaxel caused reduced fertility and reproductive indices, and increased embryo- and fetotoxicity. (See WARNINGS ). Pregnancy (See WARNINGS section). Nursing Mothers It is not known whether the drug is excreted in human milk. Following intravenous administration of carbon-14 labeled paclitaxel to rats on days 9 to 10 postpartum, concentrations of radioactivity in milk were higher than in plasma and declined in parallel with the plasma concentrations. Because many drugs are excreted in human milk and because of the potential for serious adverse reactions in nursing infants, it is recommended that nursing be discontinued when receiving paclitaxel therapy Pediatric Use The safety and effectiveness of paclitaxel in pediatric patients have not been established. There have been reports of central nervous system (CNS) toxicity (rarely associated with death) in a clinical trial in pediatric patients in which paclitaxel was infused intravenously over 3 hours at doses ranging from 350 mg/m 2 to 420 mg/m 2 . The toxicity is most likely attributable to the high dose of the ethanol component of the paclitaxel vehicle given over a short infusion time. The use of concomitant antihistamines may intensify this effect. Although a direct effect of the paclitaxel itself cannot be discounted, the high doses used in this study (over twice the recommended adult dosage) must be considered in assessing the safety of paclitaxel for use in this population. Geriatric Use Of 2228 patients who received paclitaxel in 8 clinical studies evaluating its safety and effectiveness in the treatment of advanced ovarian cancer, breast carcinoma, or NSCLC, and 1,570 patients who were randomized to receive paclitaxel in the adjuvant breast cancer study, 649 patients (17%) were 65 years or older and 49 patients (1%) were 75 years or older. In most studies, severe myelosuppression was more frequent in elderly patients; in some studies, severe neuropathy was more common in elderly patients. In 2 clinical studies in NSCLC, the elderly patients treated with paclitaxel had a higher incidence of cardiovascular events. Estimates of efficacy appeared similar in elderly patients and in younger patients; however, comparative efficacy cannot be determined with confidence due to the small number of elderly patients studied. In a study of first-line treatment of ovarian cancer, elderly patients had a lower median survival than younger patients, but no other efficacy parameters favored the younger group. TABLE 9 presents the incidences of Grade IV neutropenia and severe neuropathy in clinical studies according to age. TABLE 9. SELECTED ADVERSE EVENTS IN GERIATRIC PATIENTS RECEIVING PACLITAXEL IN CLINICAL STUDIES Patients (n/total [%]) Neutropenia (Grade IV) Peripheral Neuropathy (Grades III/IV) INDICATION Age (y) Age (y) (Study/Regimen) ≥65 <65 ≥65 <65 OVARIAN Cancer (Intergroup First-Line/T175/3 c75 a ) 34/83 (41) 78/252 (31) 24/84(29)* b 46/255 (18) b (GOG-111 First-Line/T135/24 c75 a ) 48/61 (79) 106/129 (82) 3/62 (5) 2/134 (1) (Phase 3 Second-Line/T175/3 c ) 5/19 (26) 21/76 (28) 1/19 (5) 0/76 (0) (Phase 3 Second-Line/T175/24 c ) 21/25 (84) 57/79 (72) 0/25 (0) 2/80 (3) (Phase 3 Second-Line/T135/3 c ) 4/16 (25) 10/81 (12) 0/17 (0) 0/81 (0) (Phase 3 Second-Line/T135/24 c ) 17/22 (77) 53/83 (64) 0/22 (0) 0/83 (0) (Phase 3 Second-Line Pooled) 47/82 (57)* 141/319 (44) 1/83 (1) 2/320 (1) Adjuvant BREAST Cancer (Intergroup/AC followed by T d ) 56/102 (55) 734/1468 (50) 5/102 (5) e 46/1468 (3) e BREAST Cancer after Failure of Initial Therapy (Phase 3/T175/3 c ) 7/24 (29) 56/200 (28) 3/25 (12) 12/204 (6) (Phase 3/T135/3 c ) 7/20 (35) 37/207 (18) 0/20 (0) 6/209 (3) Non-Small Cell LUNG Cancer (ECOG/T135/24 c75 a ) 58/71 (82) 86/124 (69) 9/71 (13) f 16/124 (13) f (Phase 3/T175/3 c80 a ) 37/89 (42)* 56/267 (21) 11/91 (12)* 11/271 (4) * p<0.05 a Paclitaxel dose in mg/m 2 /infusion duration in hours; cisplatin doses in mg/m 2 . b Peripheral neuropathy was included within the neurotoxicity category in the Intergroup First-Line Ovarian Cancer study (see TABLE 11 ). c Paclitaxel dose in mg/m 2 /infusion duration in hours. d Paclitaxel (T) following 4 courses of doxorubicin and cyclophosphamide (AC) at a dose of 175 mg/m 2 /3 hours every 3 weeks for 4 courses. e Peripheral neuropathy reported as neurosensory toxicity in the Intergroup Adjuvant Breast Cancer study (see Table 13 ). f Peripheral neuropathy reported as neurosensory toxicity in the ECOG NSCLC study (see TABLE 15 ). Information for Patients: (See Patient Information Leaflet )."],"how_supplied":["HOW SUPPLIED Paclitaxel Injection, USP (6 mg/mL) is a clear, colorless to slightly yellow viscous solution and supplied as follows: NDC 62332-620-05 30 mg/5 mL Multidose vial individually packaged in a carton. NDC 62332-621-17 100 mg/16.7 mL Multidose vial individually packaged in a carton. NDC 62332-622-50 300 mg/50 mL Multidose vial individually packaged in a carton. Storage Store the vials in original cartons between 20° to 25°C (68° to 77°F). [see USP Controlled Room Temperature]. Retain in the original package to protect from light. Handling and Disposal See DOSAGE AND ADMINISTRATION, Preparation and Administration Precautions."],"boxed_warning":["WARNING Paclitaxel should be administered under the supervision of a physician experienced in the use of cancer chemotherapeutic agents. Appropriate management of complications is possible only when adequate diagnostic and treatment facilities are readily available. Anaphylaxis and severe hypersensitivity reactions characterized by dyspnea and hypotension requiring treatment, angioedema, and generalized urticaria have occurred in 2 to 4% of patients receiving paclitaxel in clinical trials. Fatal reactions have occurred in patients despite premedication. All patients should be pretreated with corticosteroids, diphenhydramine, and H 2 antagonists (see DOSAGE AND ADMINISTRATION ). Patients who experience severe hypersensitivity reactions to paclitaxel should not be rechallenged with the drug. Paclitaxel therapy should not be given to patients with solid tumors who have baseline neutrophil counts of less than 1,500 cells/mm 3 and should not be given to patients with AIDS-related Kaposi's sarcoma if the baseline neutrophil count is less than 1,000 cells/mm 3 . In order to monitor the occurrence of bone marrow suppression, primarily neutropenia, which may be severe and result in infection, it is recommended that frequent peripheral blood cell counts be performed on all patients receiving paclitaxel."],"geriatric_use":["Geriatric Use Of 2228 patients who received paclitaxel in 8 clinical studies evaluating its safety and effectiveness in the treatment of advanced ovarian cancer, breast carcinoma, or NSCLC, and 1,570 patients who were randomized to receive paclitaxel in the adjuvant breast cancer study, 649 patients (17%) were 65 years or older and 49 patients (1%) were 75 years or older. In most studies, severe myelosuppression was more frequent in elderly patients; in some studies, severe neuropathy was more common in elderly patients. In 2 clinical studies in NSCLC, the elderly patients treated with paclitaxel had a higher incidence of cardiovascular events. Estimates of efficacy appeared similar in elderly patients and in younger patients; however, comparative efficacy cannot be determined with confidence due to the small number of elderly patients studied. In a study of first-line treatment of ovarian cancer, elderly patients had a lower median survival than younger patients, but no other efficacy parameters favored the younger group. TABLE 9 presents the incidences of Grade IV neutropenia and severe neuropathy in clinical studies according to age. TABLE 9. SELECTED ADVERSE EVENTS IN GERIATRIC PATIENTS RECEIVING PACLITAXEL IN CLINICAL STUDIES Patients (n/total [%]) Neutropenia (Grade IV) Peripheral Neuropathy (Grades III/IV) INDICATION Age (y) Age (y) (Study/Regimen) ≥65 <65 ≥65 <65 OVARIAN Cancer (Intergroup First-Line/T175/3 c75 a ) 34/83 (41) 78/252 (31) 24/84(29)* b 46/255 (18) b (GOG-111 First-Line/T135/24 c75 a ) 48/61 (79) 106/129 (82) 3/62 (5) 2/134 (1) (Phase 3 Second-Line/T175/3 c ) 5/19 (26) 21/76 (28) 1/19 (5) 0/76 (0) (Phase 3 Second-Line/T175/24 c ) 21/25 (84) 57/79 (72) 0/25 (0) 2/80 (3) (Phase 3 Second-Line/T135/3 c ) 4/16 (25) 10/81 (12) 0/17 (0) 0/81 (0) (Phase 3 Second-Line/T135/24 c ) 17/22 (77) 53/83 (64) 0/22 (0) 0/83 (0) (Phase 3 Second-Line Pooled) 47/82 (57)* 141/319 (44) 1/83 (1) 2/320 (1) Adjuvant BREAST Cancer (Intergroup/AC followed by T d ) 56/102 (55) 734/1468 (50) 5/102 (5) e 46/1468 (3) e BREAST Cancer after Failure of Initial Therapy (Phase 3/T175/3 c ) 7/24 (29) 56/200 (28) 3/25 (12) 12/204 (6) (Phase 3/T135/3 c ) 7/20 (35) 37/207 (18) 0/20 (0) 6/209 (3) Non-Small Cell LUNG Cancer (ECOG/T135/24 c75 a ) 58/71 (82) 86/124 (69) 9/71 (13) f 16/124 (13) f (Phase 3/T175/3 c80 a ) 37/89 (42)* 56/267 (21) 11/91 (12)* 11/271 (4) * p<0.05 a Paclitaxel dose in mg/m 2 /infusion duration in hours; cisplatin doses in mg/m 2 . b Peripheral neuropathy was included within the neurotoxicity category in the Intergroup First-Line Ovarian Cancer study (see TABLE 11 ). c Paclitaxel dose in mg/m 2 /infusion duration in hours. d Paclitaxel (T) following 4 courses of doxorubicin and cyclophosphamide (AC) at a dose of 175 mg/m 2 /3 hours every 3 weeks for 4 courses. e Peripheral neuropathy reported as neurosensory toxicity in the Intergroup Adjuvant Breast Cancer study (see Table 13 ). f Peripheral neuropathy reported as neurosensory toxicity in the ECOG NSCLC study (see TABLE 15 ). Information for Patients: (See Patient Information Leaflet )."],"pediatric_use":["Pediatric Use The safety and effectiveness of paclitaxel in pediatric patients have not been established. There have been reports of central nervous system (CNS) toxicity (rarely associated with death) in a clinical trial in pediatric patients in which paclitaxel was infused intravenously over 3 hours at doses ranging from 350 mg/m 2 to 420 mg/m 2 . The toxicity is most likely attributable to the high dose of the ethanol component of the paclitaxel vehicle given over a short infusion time. The use of concomitant antihistamines may intensify this effect. Although a direct effect of the paclitaxel itself cannot be discounted, the high doses used in this study (over twice the recommended adult dosage) must be considered in assessing the safety of paclitaxel for use in this population."],"effective_time":"20240624","nursing_mothers":["Nursing Mothers It is not known whether the drug is excreted in human milk. Following intravenous administration of carbon-14 labeled paclitaxel to rats on days 9 to 10 postpartum, concentrations of radioactivity in milk were higher than in plasma and declined in parallel with the plasma concentrations. Because many drugs are excreted in human milk and because of the potential for serious adverse reactions in nursing infants, it is recommended that nursing be discontinued when receiving paclitaxel therapy"],"clinical_studies":["CLINICAL STUDIES Ovarian Carcinoma First-Line Data The safety and efficacy of paclitaxel followed by cisplatin in patients with advanced ovarian cancer and no prior chemotherapy were evaluated in 2, Phase 3 multicenter, randomized, controlled trials. In an Intergroup study led by the European Organization for Research and Treatment of Cancer involving the Scandinavian Group NOCOVA, the National Cancer Institute of Canada, and the Scottish Group, 680 patients with Stage II B–C , III, or IV disease (optimally or non-optimally debulked) received either paclitaxel 175 mg/m 2 infused over 3 hours followed by cisplatin 75 mg/m 2 (Tc) or cyclophosphamide 750 mg/m 2 followed by cisplatin 75 mg/m 2 (Cc) for a median of 6 courses. Although the protocol allowed further therapy, only 15% received both drugs for 9 or more courses. In a study conducted by the Gynecological Oncology Group (GOG), 410 patients with Stage III or IV disease (>1 cm residual disease after staging laparotomy or distant metastases) received either paclitaxel 135 mg/m 2 infused over 24 hours followed by cisplatin 75 mg/m 2 or cyclophosphamide 750 mg/m 2 followed by cisplatin 75 mg/m 2 for 6 courses. In both studies, patients treated with paclitaxel in combination with cisplatin had significantly higher response rate, longer time to progression, and longer survival time compared with standard therapy. These differences were also significant for the subset of patients in the Intergroup study with non- optimally debulked disease, although the study was not fully powered for subset analyses ( TABLES 2A and 2B ). Kaplan- Meier survival curves for each study are shown in FIGURES 1 and 2 . TABLE 2A. EFFICACY IN THE PHASE 3 FIRST-LINE OVARIAN CARCINOMA STUDIES Intergroup (non-optimally debulked subset) GOG-111 T175/3 a c75 (n=218) C750 a c75 (n=227) T135/24 a c75 (n=196) C750 a c75 (n=214) Clinical Response b (n=153) (n=153) (n=113) (n=127) - rate (percent) 58 43 62 48 - p-value c 0.016 0.04 Time to Progression - median (months) 13.2 9.9 16.6 13.0 - p-value c 0.0060 0.0008 - hazard ratio (HR) c 0.76 0.70 - 95% CI c 0.62 to 0.92 0.56 to 0.86 Survival - median (months) 29.5 21.9 35.5 24.2 - p-value c 0.0057 0.0002 - hazard ratio (HR) c 0.73 0.64 - 95% CI c 0.58 to 0.91 0.50 to 0.81 a Paclitaxel dose in mg/m 2 /infusion duration in hours; cyclophosphamide and cisplatin doses in mg/m 2 . b Among patients with measurable disease only. c Unstratified for the Intergroup Study, Stratified for Study GOG-111. TABLE 2B. EFFICACY IN THE PHASE 3 FIRST-LINE OVARIAN CARCINOMA INTERGROUP STUDY T175/3 a c75 (n=342) C750 a c75 (n=338) Clinical Response b (n=162) (n=161) - rate (percent) 59 45 - p-value c 0.014 Time to Progression - median (months) 15.3 11.5 - p-value c 0.0005 - hazard ratio (HR) c 0.74 - 95% CI c 0.63 to 0.88 Survival - median (months) 35.6 25.9 - p-value c 0.0016 - hazard ratio (HR) c 0.73 - 95% CI c 0.60 to 0.89 a Paclitaxel dose in mg/m 2 /infusion duration in hours; cyclophosphamide and cisplatin doses in mg/m 2 . b Among patients with measurable disease only. c Unstratified. FIGURE 1. SURVIVAL: Cc VERSUS Tc (INTERGROUP) FIGURE 2. SURVIVAL: Cc VERSUS Tc (GOG-111) The adverse event profile for patients receiving paclitaxel in combination with cisplatin in these studies was qualitatively consistent with that seen for the pooled analysis of data from 812 patients treated with single-agent paclitaxel in 10 clinical studies. These adverse events and adverse events from the Phase 3 first-line ovarian carcinoma studies are described in the ADVERSE REACTIONS section in tabular ( TABLES 10 and 11 ) and narrative form. Second-Line Data Data from five Phase 1 and 2 clinical studies (189 patients), a multicenter randomized Phase 3 study (407 patients), as well as an interim analysis of data from more than 300 patients enrolled in a treatment referral center program were used in support of the use of paclitaxel in patients who have failed initial or subsequent chemotherapy for metastatic carcinoma of the ovary. Two of the Phase 2 studies (92 patients) utilized an initial dose of 135 to 170 mg/m 2 in most patients (>90%) administered over 24 hours by continuous infusion. Response rates in these two studies were 22% (95% CI, 11% to 37%) and 30% (95% CI, 18% to 46%) with a total of 6 complete and 18 partial responses in 92 patients. The median duration of overall response in these two studies measured from the first day of treatment was 7.2 months (range, 3.5 to 15.8 months) and 7.5 months (range, 5.3 to 17.4 months), respectively. The median survival was 8.1 months (range, 0.2 to 36.7 months) and 15.9 months (range, 1.8 to 34.5+ months). The Phase 3 study had a bifactorial design and compared the efficacy and safety of paclitaxel, administered at 2 different doses (135 or 175 mg/m 2 ) and schedules (3- or 24-hour infusion). The overall response rate for the 407 patients was 16.2% (95% CI, 12.8% to 20.2%), with 6 complete and 60 partial responses. Duration of response, measured from the first day of treatment was 8.3 months (range, 3.2 to 21.6 months). Median time to progression was 3.7 months (range, 0.1+ to 25.1+ months). Median survival was 11.5 months (range, 0.2 to 26.3+ months). Response rates, median survival, and median time to progression for the 4 arms are given in the following table. TABLE 3. EFFICACY IN THE PHASE 3 SECOND-LINE OVARIAN CARCINOMA STUDY 175/3 (n=96) 175/24 (n=106) 135/3 (n=99) 135/24 (n=106) Response - rate (percent) 14.6 21.7 15.2 13.2 - 95% Confidence Interval (8.5 to 23.6) (14.5 to 31) (9 to 24.1) (7.7 to 21.5) Time to Progression - median (months) 4.4 4.2 3.4 2.8 - 95% Confidence Interval (3.0 to 5.6) (3.5 to 5.1) (2.8 to 4.2) (1.9 to 4) Survival - median (months) 11.5 11.8 13.1 10.7 - 95% Confidence Interval (8.4 to 14.4) (8.9 to 14.6) (9.1 to 14.6) (8.1 to 13.6) Analyses were performed as planned by the bifactorial study design described in the protocol, by comparing the 2 doses (135 or 175 mg/m 2 ) irrespective of the schedule (3 or 24 hours) and the two schedules irrespective of dose. Patients receiving the 175 mg/m 2 dose had a response rate similar to that for those receiving the 135 mg/m 2 dose: 18% versus 14% (p=0.28). No difference in response rate was detected when comparing the 3-hour with the 24-hour infusion: 15% versus 17% (p=0.50). Patients receiving the 175 mg/m 2 dose of paclitaxel had a longer time to progression than those receiving the 135 mg/m 2 dose: median 4.2 versus 3.1 months (p=0.03). The median time to progression for patients receiving the 3-hour versus the 24-hour infusion was 4.0 months versus 3.7 months, respectively. Median survival was 11.6 months in patients receiving the 175 mg/m 2 dose of paclitaxel and 11.0 months in patients receiving the 135 mg/m 2 dose (p=0.92). Median survival was 11.7 months for patients receiving the 3-hour infusion of paclitaxel and 11.2 months for patients receiving the 24 hour infusion (p=0.91). These statistical analyses should be viewed with caution because of the multiple comparisons made. Paclitaxel remained active in patients who had developed resistance to platinum-containing therapy (defined as tumor progression while on, or tumor relapse within 6 months from completion of, a platinum-containing regimen) with response rates of 14% in the Phase 3 study and 31% in the Phase 1 and 2 clinical studies. The adverse event profile in this Phase 3 study was consistent with that seen for the pooled analysis of data from 812 patients treated in 10 clinical studies. These adverse events and adverse events from the Phase 3 second-line ovarian carcinoma study are described in the ADVERSE REACTIONS section in tabular ( TABLES 10 and 12 ) and narrative form. The results of this randomized study support the use of paclitaxel at doses of 135 to 175 mg/m 2 , administered by a 3-hour intravenous infusion. The same doses administered by 24-hour infusion were more toxic. However, the study had insufficient power to determine whether a particular dose and schedule produced superior efficacy. Breast Carcinoma Adjuvant Therapy A Phase 3 Intergroup study (Cancer and Leukemia Group B [CALGB], Eastern Cooperative Oncology Group [ECOG], North Central Cancer Treatment Group [NCCTG], and Southwest Oncology Group [SWOG]) randomized 3170 patients with node-positive breast carcinoma to adjuvant therapy with paclitaxel or to no further chemotherapy following 4 courses of doxorubicin and cyclophosphamide (AC). This multicenter trial was conducted in women with histologically positive lymph nodes following either a mastectomy or segmental mastectomy and nodal dissections. The 3 x 2 factorial study was designed to assess the efficacy and safety of 3 different dose levels of doxorubicin (A) and to evaluate the effect of the addition of paclitaxel administered following the completion of AC therapy. After stratification for the number of positive lymph nodes (1 to 3, 4 to 9, or 10+), patients were randomized to receive cyclophosphamide at a dose of 600 mg/m 2 and doxorubicin at doses of either 60 mg/m 2 (on day 1), 75 mg/m 2 (in 2 divided doses on days 1 and 2), or 90 mg/m 2 (in 2 divided doses on days 1 and 2 with prophylactic G-CSF support and ciprofloxacin) every 3 weeks for 4 courses and either paclitaxel 175 mg/m 2 as a 3-hour infusion every 3 weeks for 4 additional courses or no additional chemotherapy. Patients whose tumors were positive were to receive subsequent tamoxifen treatment (20 mg daily for 5 years); patients who received segmental mastectomies prior to study were to receive breast irradiation after recovery from treatment-related toxicities. At the time of the current analysis, median follow-up was 30.1 months. Of the 2066 patients who were hormone receptor positive, 93% received tamoxifen. The primary analyses of disease-free survival and overall survival used multivariate Cox models, which included paclitaxel administration, doxorubicin dose, number of positive lymph nodes, tumor size, menopausal status, and estrogen receptor status as factors. Based on the model for disease-free survival, patients receiving AC followed by paclitaxel had a 22% reduction in the risk of disease recurrence compared to patients randomized to AC alone (Hazard Ratio [HR]=0.78, 95% CI, 0.67 to 0.91, p=0.0022). They also had a 26% reduction in the risk of death (HR=0.74, 95% CI, 0.60 to 0.92, p=0.0065). For disease-free survival and overall survival, p-values were not adjusted for interim analyses. Kaplan-Meier curves are shown in FIGURES 3 and 4 . Increasing the dose of doxorubicin higher than 60 mg/m 2 had no effect on either disease-free survival or overall survival. FUGURE 3. DISEASE-FREE SURVIVAL: AC VERSUS AC+T FUGURE 4. SURVIVAL: AC VERSUS AC+T Subset analyses Subsets defined by variables of known prognostic importance in adjuvant breast carcinoma were examined, including number of positive lymph nodes, tumor size, hormone receptor status, and menopausal status. Such analyses must be interpreted with care, as the most secure finding is the overall study result. In general, a reduction in hazard similar to the overall reduction was seen with paclitaxel for both disease-free and overall survival in all of the larger subsets with one exception; patients with receptor-positive tumors had a smaller reduction in hazard (HR=0.92) for disease-free survival with paclitaxel than other groups. Results of subset analyses are shown in TABLE 4 TABLE 4. SUBSET ANALYSES — ADJUVANT BREAST CARCINOMA STUDY Patient Subset Disease-Free Survival Overall Survival No. of Patients No. of Recurrences Hazard Ratio (95% CI) No. of Deaths Hazard Ratio (95% CI) No. Positive Nodes 1 to 3 1,449 221 0.72 (0.55 to 0.94) 107 0.76 (0.52 to 1.12) 4 to 9 1,310 274 0.78 (0.61 to 0.99) 148 0.66 (0.47 to 0.91) 10+ 360 129 0.93 (0.66 to 1.31) 87 0.90 (0.59 to 1.36) Tumor Size (cm) ≤2 1,096 153 0.79 (0.57 to 1.08) 67 0.73 (0.45 to 1.18) >2 and ≤5 1,611 358 0.79 (0.64 to 0.97) 201 0.74 (0.56 to 0.98) >5 397 111 0.75 (0.51 to 1.08) 72 0.73 (0.46 to 1.16) Menopausal Status Pre 1,929 374 0.83 (0.67 to 1.01) 187 0.72 (0.54 to 0.97) Post 1,183 250 0.73 (0.57 to 0.93) 155 0.77 (0.56 to 1.06) Receptor Status Positive a 2,066 293 0.92 (0.73 to 1.16) 126 0.83 (0.59 to 1.18) Negative/Unknown b 1,055 331 0.68 (0.55 to 0.85) 216 0.71 (0.54 to 0.93) a Positive for either estrogen or progesterone receptors. b Negative or missing for both estrogen and progesterone receptors (both missing: n=15). These retrospective subgroup analyses suggest that the beneficial effect of paclitaxel is clearly established in the receptor-negative subgroup, but the benefit in receptor-positive patients is not yet clear. With respect to menopausal status, the benefit of paclitaxel is consistent (see TABLE 4 and FIGURES 5 to 8 ). FIGURE 5. DISEASE-FREE SURVIVAL: RECEPTOR STATUS NEGATIVE / UNKNOWN AC VERSUS AC+T F IGURE 6. DISEASE-FREE SURVIVAL—RECEPTOR STATUS POSITIVE AC VERSUS AC+T F IGURE 7. DISEASE-FREE SURVIVAL—PREMENOPAUSAL AC VERSUS AC+T FIGURE 8. DISEASE-FREE SURVIVAL: POSTMENOPAUSAL AC VERSUS AC+T The adverse event profile for the patients who received paclitaxel subsequent to AC was consistent with that seen in the pooled analysis of data from 812 patients ( TABLE 10 ) treated with single-agent paclitaxel in 10 clinical studies. These adverse events are described in the ADVERSE REACTIONS section in tabular ( TABLES 10 and 13 ) and narrative form. After Failure of Initial Chemotherapy Data from 83 patients accrued in three, Phase 2 open-label studies and from 471 patients enrolled in a Phase 3 randomized study were available to support the use of paclitaxel in patients with metastatic breast carcinoma. Phase 2 Open Label Studies Two studies were conducted in 53 patients previously treated with a maximum of one prior chemotherapeutic regimen. Paclitaxel was administered in these 2 trials as a 24-hour infusion at initial doses of 250 mg/m 2 (with G-CSF support) or 200 mg/m 2 . The response rates were 57% (95% CI: 37% to 75%) and 52% (95% CI: 32% to 72%), respectively. The third Phase 2 study was conducted in extensively pretreated patients who had failed anthracycline therapy and who had received a minimum of 2 chemotherapy regimens for the treatment of metastatic disease. The dose of paclitaxel was 200 mg/m2 as a 24-hour infusion with G-CSF support. Nine of 30 patients achieved a partial response, for a response rate of 30% (95% CI: 15% to 50%). Phase 3 Randomized Study This multicenter trial was conducted in patients previously treated with 1 or 2 regimens of chemotherapy. Patients were randomized to receive paclitaxel at a dose of either 175 mg/m 2 or 135 mg/m 2 given as a 3-hour infusion. In the 471 patients enrolled, 60% had symptomatic disease with impaired performance status at study entry, and 73% had visceral metastases. These patients had failed prior chemotherapy either in the adjuvant setting (30%), the metastatic setting (39%), or both (31%). Sixty-seven percent of the patients had been previously exposed to anthracyclines and 23% of them had disease considered resistant to this class of agents. The overall response rate for the 454 evaluable patients was 26% (95% CI, 22% to 30%), with 17 complete and 99 partial responses. The median duration of response, measured from the first day of treatment, was 8.1 months (range, 3.4 to 18.1+ months). Overall for the 471 patients, the median time to progression was 3.5 months (range, 0.03 to 17.1 months). Median survival was 11.7 months (range, 0 to 18.9 months). Response rates, median survival and median time to progression for the 2 arms are given in the following table. TABLE 5. EFFICACY IN BREAST CANCER AFTER FAILURE OF INITIAL CHEMOTHERAPY OR WITHIN 6 MONTHS OF ADJUVANT CHEMOTHERAPY 175/3 (n=235) 135/3 (n=236) Response - rate (percent) - p-value 28 0.135 22 Time to Progression - median (months) - p-value 4.2 0.027 3 Survival - median (months) - p-value 11.7 0.321 10.5 The adverse event profile of the patients who received single-agent paclitaxel in the Phase 3 study was consistent with that seen for the pooled analysis of data from 812 patients treated in 10 clinical studies. These adverse events and adverse events from the Phase 3 breast carcinoma study are described in the ADVERSE REACTIONS section in tabular ( TABLES 10 and 14 ) and narrative form. Non-Small Cell Lung Carcinoma (NSCLC) In a Phase 3 open-label randomized study conducted by the ECOG, 599 patients were randomized to either paclitaxel (T) 135 mg/m 2 as a 24-hour infusion in combination with cisplatin (c) 75 mg/m 2 , paclitaxel (T) 250 mg/m 2 as a 24-hour infusion in combination with cisplatin (c) 75 mg/m 2 with G-CSF support, or cisplatin (c) 75 mg/m 2 on day 1, followed by etoposide (VP) 100 mg/m 2 on days 1, 2, and 3 (control). Response rates, median time to progression, median survival, and 1-year survival rates are given in the following table. The reported p-values have not been adjusted for multiple comparisons. There were statistically significant differences favoring each of the paclitaxel plus cisplatin arms for response rate and time to tumor progression. There was no statistically significant difference in survival between either paclitaxel plus cisplatin arm and the cisplatin plus etoposide arm. TABLE 6. EFFICACY PARAMETERS IN THE PHASE 3 FIRST-LINE NSCLC STUDY T135/24 c75 (n=198) T250/24 c75 (n=201) VP100 a c75 (n=200) Response - rate (percent) 25 23 12 - p-value b 0.001 <0.001 Time to Progression - median (months) 4.3 4.9 2.7 - p-value b 0.05 0.004 Survival - median (months) 9.3 10 7.4 - p-value b 0.12 0.08 1-Year Survival - percent of patients 36 40 32 a Etoposide (VP) 100 mg/m 2 was administered IV on days 1, 2, and 3. b Compared to cisplatin/etoposide. In the ECOG study, the Functional Assessment of Cancer Therapy-Lung (FACT-L) questionnaire had 7 subscales that measured subjective assessment of treatment. Of the 7, the Lung Cancer Specific Symptoms subscale favored the paclitaxel 135 mg/m 2 /24 hour plus cisplatin arm compared to the cisplatin/etoposide arm. For all other factors, there was no difference in the treatment groups. The adverse event profile for patients who received paclitaxel in combination with cisplatin in this study was generally consistent with that seen for the pooled analysis of data from 812 patients treated with single-agent paclitaxel in 10 clinical studies. These adverse events and adverse events from the Phase 3 first-line NSCLC study are described in the ADVERSE REACTIONS section in tabular ( TABLES 10 and 15 ) and narrative form. AIDS-Related Kaposi’s Sarcoma Data from 2, Phase 2 open-label studies support the use of paclitaxel as second-line therapy in patients with AIDS-related Kaposi’s sarcoma. Fifty-nine of the 85 patients enrolled in these studies had previously received systemic therapy, including interferon alpha (32%), DaunoXome® (31%), DOXIL® (2%), and doxorubicin containing chemotherapy (42%), with 64% having received prior anthracyclines. Eighty-five percent of the pretreated patients had progressed on, or could not tolerate, prior systemic therapy. 1 In Study CA139-174, patients received paclitaxel at 135 mg/m 2 as a 3-hour infusion every 3 weeks (intended dose intensity 45 mg/m 2 /week). If no dose-limiting toxicity was observed, patients were to receive 155 mg/m 2 and 175 mg/m 2 in subsequent courses. Hematopoietic growth factors were not to be used initially. In Study CA139-281, patients received paclitaxel at 100 mg/m 2 as a 3-hour infusion every 2 weeks (intended dose intensity 50 mg/m 2 /week). In this study patients could be receiving hematopoietic growth factors before the start of paclitaxel therapy, or this support was to be initiated as indicated; the dose of paclitaxel was not increased. The dose intensity of paclitaxel used in this patient population was lower than the dose intensity recommended for other solid tumors. All patients had widespread and poor-risk disease. Applying the ACTG staging criteria to patients with prior systemic therapy, 93% were poor risk for extent of disease (T1), 88% had a CD4 count <200 cells/mm 3 (I1), and 97% had poor risk considering their systemic illness (S1). All patients in Study CA139-174 had a Karnofsky performance status of 80 or 90 at baseline; in Study CA139-281, there were 26 (46%) patients with a Karnofsky performance status of 70 or worse at baseline. TABLE 7. EXTENT OF DISEASE AT STUDY ENTRY PERCENT OF PATIENTS Prior Systemic Therapy (n=59) Visceral ± edema ± oral ± cutaneous 42 Edema or lymph nodes ± oral ± cutaneous 41 Oral ± cutaneous 10 Cutaneous only 7 Although the planned dose intensity in the 2 studies was slightly different (45 mg/m 2 /week in Study CA139-174 and 50 mg/m 2 /week in Study CA139-281), delivered dose intensity was 38 to 39 mg/m 2 /week in both studies, with a similar range (20 to 24 to 51 to 61). Efficacy The efficacy of paclitaxel was evaluated by assessing cutaneous tumor response according to the amended ACTG criteria and by seeking evidence of clinical benefit in patients in 6 domains of symptoms and/or conditions that are commonly related to AIDS-related Kaposi’s sarcoma. Cutaneous Tumor Response (Amended ACTG Criteria) The objective response rate was 59% (95% CI, 46 to 72%) (35 of 59 patients) in patients with prior systemic therapy. Cutaneous responses were primarily defined as flattening of more than 50% of previously raised lesions. TABLE 8. OVERALL BEST RESPONSE (AMENDED ACTG CRITERIA) PERCENT OF PATIENTS Prior Systemic Therapy (n=59) Complete response 3 Partial response 56 Stable disease 29 Progression 8 Early death/toxicity 3 The median time to response was 8.1 weeks and the median duration of response measured from the first day of treatment was 10.4 months (95% CI, 7.0 to 11.0 months) for the patients who had previously received systemic therapy. The median time to progression was 6.2 months (95% CI, 4.6 to 8.7 months). Additional Clinical Benefit Most data on patient benefit were assessed retrospectively (plans for such analyses were not included in the study protocols). Nonetheless, clinical descriptions and photographs indicated clear benefit in some patients, including instances of improved pulmonary function in patients with pulmonary involvement, improved ambulation, resolution of ulcers, and decreased analgesic requirements in patients with Kaposi’s sarcoma (KS) involving the feet and resolution of facial lesions and edema in patients with KS involving the face, extremities, and genitalia. Safety The adverse event profile of paclitaxel administered to patients with advanced HIV disease and poor-risk AIDS-related Kaposi’s sarcoma was generally similar to that seen in the pooled analysis of data from 812 patients with solid tumors. These adverse events and adverse events from the Phase 2 second-line Kaposi’s sarcoma studies are described in the ADVERSE REACTIONS section in tabular ( TABLES 10 and 16 ) and narrative form. In this immunosuppressed patient population, however, a lower dose intensity of paclitaxel and supportive therapy including hematopoietic growth factors in patients with severe neutropenia are recommended. Patients with AIDS-related Kaposi’s sarcoma may have more severe hematologic toxicities than patients with solid tumors. paclitaxel-1figure paclitaxel-2figure paclitaxel-3figure paclitaxel-4figure paclitaxel-5figure paclitaxel-6figure paclitaxel-7figure paclitaxel-8figure"],"adverse_reactions":["ADVERSE REACTIONS Pooled Analysis of Adverse Event Experiences from Single-Agent Studies Data in the following table are based on the experience of 812 patients (493 with ovarian carcinoma and 319 with breast carcinoma) enrolled in 10 studies who received single-agent Paclitaxel Injection. Two hundred and seventy-five patients were treated in 8, Phase 2 studies with paclitaxel doses ranging from 135 to 300 mg/m 2 administered over 24 hours (in 4 of these studies, G-CSF was administered as hematopoietic support). Three hundred and one patients were treated in the randomized Phase 3 ovarian carcinoma study which compared 2 doses (135 or 175 mg/m 2 ) and 2 schedules (3 or 24 hours) of paclitaxel. Two hundred and thirty-six patients with breast carcinoma received paclitaxel (135 or 175 mg/m 2 ) administered over 3 hours in a controlled study. TABLE 10. SUMMARY a OF ADVERSE EVENTS IN PATIENTS WITH SOLID TUMORS RECEIVING SINGLE-AGENT PACLITAXEL Percent of Patients (n=812) Bone Marrow - Neutropenia <2,000/mm 3 <500/mm 3 - Leukopenia <4,000/mm 3 <1,000/mm 3 - Thrombocytopenia <100,000/mm 3 <50,000/mm 3 - Anemia <11 g/dL <8 g/dL - Infections - Bleeding - Red Cell Transfusions - Platelet Transfusions 90 52 90 17 20 7 78 16 30 14 25 2 Hypersensitivity Reaction b - All - Severe † 41 2 Cardiovascular - Vital Sign Changes c - Bradycardia (n=537) - Hypotension (n=532) - Significant Cardiovascular Events 3 12 1 Abnormal ECG - All Pts - Pts with normal baseline (n=559) 23 14 Peripheral Neuropathy - Any symptoms - Severe symptoms † 60 3 Myalgia/Arthralgia - Any symptoms - Severe symptoms † 60 8 Gastrointestinal - Nausea and vomiting - Diarrhea - Mucositis 52 38 31 Alopecia 87 Hepatic (Pts with normal baseline and on study data) - Bilirubin elevations (n=765) - Alkaline phosphatase elevations (n=575) - AST (SGOT) elevations (n=591) 7 22 19 Injection Site Reaction 13 a Based on worst course analysis. b All patients received premedication. c During the first 3 hours of infusion † Severe events are defined as at least Grade III toxicity. None of the observed toxicities were clearly influenced by age. Disease-Specific Adverse Event Experiences First-Line Ovary in Combination For the 1,084 patients who were evaluable for safety in the Phase 3 first-line ovary combination therapy studies, TABLE 11 shows the incidence of important adverse events. For both studies, the analysis of safety was based on all courses of therapy (6 courses for the GOG- 111 study and up to 9 courses for the Intergroup study). TABLE 11. FREQUENCY a OF IMPORTANT ADVERSE EVENTS IN THE PHASE 3 FIRST-LINE OVARIAN CARCINOMA STUDIES Percent of Patients Intergroup GOG-111 T175/3 b c75 c (n=339) C750 c c75 c (n=336) T135/24 b c75 c (n=196) C750 c c75 c (n=213) Bone Marrow - Neutropenia <2,000/mm 3 91 d 95 d 96 92 <500/mm 3 33 d 43 d 81 d 58 d - Thrombocytopenia <100,000/mm 3e 21 d 33 d 26 30 <50,000/mm 3 3 d 7 d 10 9 - Anemia <11 g/dL f 96 97 88 86 <8 g/dL 3 d 8 d 13 9 - Infections 25 27 21 15 - Febrile Neutropenia 4 7 15 d 4 d Hypersensitivity Reaction - All 11 d 6 d 8 d,g 1 d,g - Severe † 1 1 3 d,g - d,g Neurotoxicity h - Any symptoms 87 d 52 d 25 20 - Severe symptoms † 21 d 2 d 3 d - d Nausea and Vomiting - Any symptoms 88 93 65 69 - Severe symptoms † 18 24 10 11 Myalgia/Arthralgia - Any symptoms 60 d 27 d 9 d 2 d - Severe symptoms † 6 d 1 d 1 - Diarrhea - Any symptoms 37 d 29 d 16 d 8 d - Severe symptoms † 2 3 4 1 Athenia - Any symptoms NC NC 17 d 10 d - Severe symptoms † NC NC 1 1 Alopecia - Any symptoms 96 d 89 d 55 d 37 d - Severe symptoms † 51 d 21 d 6 8 a Based on worst course analysis. b Paclitaxel (T) dose in mg/m 2 /infusion duration in hours. c Cyclophosphamide (C) or cisplatin (c) dose in mg/m 2 . d p<0.05 by Fisher exact test. e <130,000/mm 3 in the Intergroup study. f <12 g/dL in the Intergroup study. g All patients received premedication. h In the GOG-111 study, neurotoxicity was collected as peripheral neuropathy and in the Intergroup study, neurotoxicity was collected as either neuromotor or neurosensory symptoms. † Severe events are defined as at least Grade III toxicity. NC Not Collected. Second-Line Ovary: For the 403 patients who received single-agent paclitaxel injection in the Phase 3 second-line ovarian carcinoma study, the following table shows the incidence of important adverse events. TABLE 12. FREQUENCY a OF IMPORTANT ADVERSE EVENTS IN THE PHASE 3 SECOND-LINE OVARIAN CARCINOMA STUDY Percent of Patients 175/3 b (n=95) 175/24 b (n=105) 135/3 b (n=98) 135/24 b (n=105) Bone Marrow - Neutropenia <2,000/mm 3 <500/mm 3 - Thrombocytopenia <100,000/mm 3 <50,000/mm 3 - Anemia <11 g/dL <8 g/dL - Infections 78 27 4 1 84 11 26 98 75 18 7 90 12 29 78 14 8 2 68 6 20 98 67 6 1 88 10 18 Hypersensitivity Reaction c - All - Severe † 41 2 45 0 38 2 45 1 Peripheral Neuropathy - Any symptoms - Severe symptoms † 63 1 60 2 55 0 42 0 Mucositis - Any symptoms - Severe symptoms † 17 0 35 3 21 0 25 2 a Based on worst course analysis. b Paclitaxel dose in mg/m 2 /infusion duration in hours. c All patients received premedication. † Severe events are defined as at least Grade III toxicity. Myelosuppression was dose and schedule related, with the schedule effect being more prominent. The development of severe hypersensitivity reactions (HSRs) was rare; 1% of the patients and 0.2% of the courses overall. There was no apparent dose or schedule effect seen for the HSRs. Peripheral neuropathy was clearly dose-related, but schedule did not appear to affect the incidence. Adjuvant Breast For the Phase 3 adjuvant breast carcinoma study, the following table shows the incidence of important severe adverse events for the 3121 patients (total population) who were evaluable for safety as well as for a group of 325 patients (early population) who, per the study protocol, were monitored more intensively than other patients. TABLE 13. FREQUENCY a OF IMPORTANT SEVERE b ADVERSE EVENTS IN THE PHASE 3 ADJUVANT BREAST CARCINOMA STUDY Percent of Patients Early Population Total Population AC c (n=166) AC c followed by T d (n=159) AC c (n=1551) AC c followed by T d (n=1570) Bone Marrow e - Neutropenia <500/mm 3 79 76 48 50 - Thrombocytopenia <50,000/mm 3 27 25 11 11 - Anemia <8 g/dL 17 21 8 8 - Infections 6 14 5 6 - Fever Without Infection – 3 <1 1 Hypersensitivity Reaction f 1 4 1 2 Cardiovascular Events 1 2 1 2 Neuromotor Toxicity 1 1 <1 1 Neurosensory Toxicity – 3 <1 3 Myalgia/Arthralgia – 2 <1 2 Nausea/Vomiting 13 18 8 9 Mucositis 13 4 6 5 a Based on worst course analysis. b Severe events are defined as at least Grade III toxicity. c Patients received 600 mg/m 2 cyclophosphamide and doxorubicin (AC) at doses of either 60 mg/m 2 , 75 mg/m 2 , or 90 mg/m 2 (with prophylactic G-CSF support and ciprofloxacin), every 3 weeks for 4 courses. d Paclitaxel (T) following 4 courses of AC at a dose of 175 mg/m 2 /3 hours every 3 weeks for 4 courses. e The incidence of febrile neutropenia was not reported in this study. f All patients were to receive premedication. The incidence of an adverse event for the total population likely represents an underestimation of the actual incidence given that safety data were collected differently based on enrollment cohort. However, since safety data were collected consistently across regimens, the safety of the sequential addition of paclitaxel following AC therapy may be compared with AC therapy alone. Compared to patients who received AC alone, patients who received AC followed by paclitaxel experienced more Grade III/IV neurosensory toxicity, more Grade III/IV myalgia/arthralgia, more Grade III/IV neurologic pain (5% vs 1%), more Grade III/IV flu-like symptoms (5% vs 3%), and more Grade III/IV hyperglycemia (3% vs 1%). During the additional 4 courses of treatment with paclitaxel, 2 deaths (0.1%) were attributed to treatment. During paclitaxel treatment, Grade IV neutropenia was reported for 15% of patients, Grade II/III neurosensory toxicity for 15%, Grade II/III myalgias for 23%, and alopecia for 46%. The incidences of severe hematologic toxicities, infections, mucositis, and cardiovascular events increased with higher doses of doxorubicin. Breast Cancer After Failure of Initial Chemotherapy For the 458 patients who received single-agent paclitaxel in the Phase 3 breast carcinoma study, the following table shows the incidence of important adverse events by treatment arm (each arm was administered by a 3-hour infusion). TABLE 14. FREQUENCY a OF IMPORTANT ADVERSE EVENTS IN THE PHASE 3 STUDY OF BREAST CANCER AFTER FAILURE OF INITIAL CHEMOTHERAPY OR WITHIN 6 MONTHS OF ADJUVANT CHEMOTHERAPY Percent of Patients 175/3 b (n=229) 135/3 b (n=229) Bone Marrow - Neutropenia <2,000/mm 3 90 81 <500/mm 3 28 19 - Thrombocytopenia <100,000/mm 3 11 7 <50,000/mm 3 3 2 - Anemia <11 g/dL 55 47 <8 g/dL 4 2 - Infections 23 15 - Febrile Neutropenia 2 2 Hypersensitivity Reaction c - All 36 31 - Severe † 0 <1 Peripheral Neuropathy - Any symptoms 70 46 - Severe symptoms † 7 3 Mucositis - Any symptoms 23 17 - Severe symptoms † 3 <1 a Based on worst course analysis. b Paclitaxel dose in mg/m 2 /infusion duration in hours. c All patients received premedication. † Severe events are defined as at least Grade III toxicity. Myelosuppression and peripheral neuropathy were dose related. There was one severe hypersensitivity reaction (HSR) observed at the dose of 135 mg/m 2 . First-Line NSCLC in Combination In the study conducted by the Eastern Cooperative Oncology Group (ECOG), patients were randomized to either paclitaxel (T) 135 mg/m 2 as a 24-hour infusion in combination with cisplatin (c) 75 mg/m 2 , paclitaxel (T) 250 mg/m 2 as a 24-hour infusion in combination with cisplatin (c) 75 mg/m 2 with G-CSF support, or cisplatin (c) 75 mg/m 2 on day 1, followed by etoposide (VP) 100 mg/m 2 on days 1, 2, and 3 (control). The following table shows the incidence of important adverse events. TABLE 15. FREQUENCY a OF IMPORTANT ADVERSE EVENTS IN THE PHASE 3 STUDY FOR FIRST-LINE NSCLC Percent of Patients T135/24 b c75 (n=195) T250/24 c c75 (n=197) VP100 d c75 (n=196) Bone Marrow - Neutropenia <2,000/mm 3 <500/mm 3 - Thrombocytopenia Patients (n/total [%]) Neutropenia (Grade IV) Peripheral Neuropathy (Grades III/IV) INDICATION Age (y) Age (y) (Study/Regimen) ≥65 <65 ≥65 <65 OVARIAN Cancer (Intergroup First-Line/T175/3 c75a) 34/83 (41) 78/252 (31) 24/84(29)*b 46/255 (18)b (GOG-111 First-Line/T135/24 c75a) 48/61 (79) 106/129 (82) 3/62 (5) 2/134 (1) (Phase 3 Second-Line/T175/3c) 5/19 (26) 21/76 (28) 1/19 (5) 0/76 (0) (Phase 3 Second-Line/T175/24c) 21/25 (84) 57/79 (72) 0/25 (0) 2/80 (3) (Phase 3 Second-Line/T135/3c) 4/16 (25) 10/81 (12) 0/17 (0) 0/81 (0) (Phase 3 Second-Line/T135/24c) 17/22 (77) 53/83 (64) 0/22 (0) 0/83 (0) (Phase 3 Second-Line Pooled) 47/82 (57)* 141/319 (44) 1/83 (1) 2/320 (1) Adjuvant BREAST Cancer (Intergroup/AC followed by Td) 56/102 (55) 734/1468 (50) 5/102 (5)e 46/1468 (3)e BREAST Cancer after Failure of Initial Therapy (Phase 3/T175/3c) 7/24 (29) 56/200 (28) 3/25 (12) 12/204 (6) (Phase 3/T135/3c) 7/20 (35) 37/207 (18) 0/20 (0) 6/209 (3) Non-Small Cell LUNG Cancer (ECOG/T135/24 c75a) 58/71 (82) 86/124 (69) 9/71 (13)f 16/124 (13)f (Phase 3/T175/3 c80a) 37/89 (42)* 56/267 (21) 11/91 (12)* 11/271 (4) "],"how_supplied_table":["
NDC 62332-620-05 30 mg/5 mL Multidose vial individually packaged in a carton.
NDC 62332-621-17 100 mg/16.7 mL Multidose vial individually packaged in a carton.
NDC 62332-622-50 300 mg/50 mL Multidose vial individually packaged in a carton.
"],"geriatric_use_table":["
Patients (n/total [%])
Neutropenia (Grade IV) Peripheral Neuropathy (Grades III/IV)
INDICATION Age (y) Age (y)
(Study/Regimen) ≥65 <65 ≥65 <65
OVARIAN Cancer
(Intergroup First-Line/T175/3 c75a) 34/83 (41) 78/252 (31) 24/84(29)*b 46/255 (18)b
(GOG-111 First-Line/T135/24 c75a) 48/61 (79) 106/129 (82) 3/62 (5) 2/134 (1)
(Phase 3 Second-Line/T175/3c) 5/19 (26) 21/76 (28) 1/19 (5) 0/76 (0)
(Phase 3 Second-Line/T175/24c) 21/25 (84) 57/79 (72) 0/25 (0) 2/80 (3)
(Phase 3 Second-Line/T135/3c) 4/16 (25) 10/81 (12) 0/17 (0) 0/81 (0)
(Phase 3 Second-Line/T135/24c) 17/22 (77) 53/83 (64) 0/22 (0) 0/83 (0)
(Phase 3 Second-Line Pooled) 47/82 (57)* 141/319 (44) 1/83 (1) 2/320 (1)
Adjuvant BREAST Cancer
(Intergroup/AC followed by Td) 56/102 (55) 734/1468 (50) 5/102 (5)e 46/1468 (3)e
BREAST Cancer after Failure of Initial Therapy
(Phase 3/T175/3c) 7/24 (29) 56/200 (28) 3/25 (12) 12/204 (6)
(Phase 3/T135/3c) 7/20 (35) 37/207 (18) 0/20 (0) 6/209 (3)
Non-Small Cell LUNG Cancer
(ECOG/T135/24 c75a) 58/71 (82) 86/124 (69) 9/71 (13)f 16/124 (13)f
(Phase 3/T175/3 c80a) 37/89 (42)* 56/267 (21) 11/91 (12)* 11/271 (4)
"],"clinical_pharmacology":["CLINICAL PHARMACOLOGY Paclitaxel is a novel antimicrotubule agent that promotes the assembly of microtubules from tubulin dimers and stabilizes microtubules by preventing depolymerization. This stability results in the inhibition of the normal dynamic reorganization of the microtubule network that is essential for vital interphase and mitotic cellular functions. In addition, paclitaxel induces abnormal arrays or “bundles” of microtubules throughout the cell cycle and multiple asters of microtubules during mitosis. Following intravenous administration of paclitaxel, paclitaxel plasma concentrations declined in a biphasic manner. The initial rapid decline represents distribution to the peripheral compartment and elimination of the drug. The later phase is due, in part, to a relatively slow efflux of paclitaxel from the peripheral compartment. Pharmacokinetic parameters of paclitaxel following 3- and 24-hour infusions of paclitaxel at dose levels of 135 and 175 mg/m 2 were determined in a Phase 3 randomized study in ovarian cancer patients and are summarized in the following table: TABLE 1. SUMMARY OF PHARMACOKINETIC PARAMETERS—MEAN VALUES Dose (mg/m 2 ) Infusion Duration (h) N (patients) C max (ng/mL) AUC (0-∞) (ng•h/mL) T-HALF (h) CL T (L/h/m 2 ) 135 24 2 195 6,300 52.7 21.7 175 24 4 365 7,993 15.7 23.8 135 3 7 2,170 7,952 13.1 17.7 175 3 5 3,650 15,007 20.2 12.2 C max = Maximum plasma concentration AUC (0 ∞) = Area under the plasma concentration-time curve from time 0 to infinity CL T = Total body clearance It appeared that with the 24-hour infusion of paclitaxel, a 30% increase in dose (135 mg/m 2 vs 175 mg/m 2 ) increased the Cmax by 87%, whereas the AUC (0-∞) remained proportional. However, with a 3- hour infusion, for a 30% increase in dose, the Cmax and AUC (0-∞) were increased by 68% and 89%, respectively. The mean apparent volume of distribution at steady state, with the 24-hour infusion of paclitaxel, ranged from 227 to 688 L/m 2 , indicating extensive extravascular distribution and/or tissue binding of paclitaxel. The pharmacokinetics of paclitaxel were also evaluated in adult cancer patients who received single doses of 15 to 135 mg/m 2 given by 1-hour infusions (n=15), 30 to 275 mg/m 2 given by 6-hour infusions (n=36), and 200 to 275 mg/m 2 given by 24-hour infusions (n=54) in Phase 1 and 2 studies. Values for CLT and volume of distribution were consistent with the findings in the Phase 3 study. The pharmacokinetics of paclitaxel in patients with AIDS-related Kaposi's sarcoma have not been studied. In vitro studies of binding to human serum proteins, using paclitaxel concentrations ranging from 0.1 to 50 mcg/mL, indicate that between 89 to 98% of drug is bound; the presence of cimetidine, ranitidine, dexamethasone, or diphenhydramine did not affect protein binding of paclitaxel. After intravenous administration of 15 to 275 mg/m 2 doses of paclitaxel as 1-, 6-, or 24-hour infusions, mean values for cumulative urinary recovery of unchanged drug ranged from 1.3% to 12.6% of the dose, indicating extensive non-renal clearance. In 5 patients administered a 225 or 250 mg/m 2 dose of radiolabeled paclitaxel as a 3-hour infusion, a mean of 71% of the radioactivity was excreted in the feces in 120 hours, and 14% was recovered in the urine. Total recovery of radioactivity ranged from 56% to 101% of the dose. Paclitaxel represented a mean of 5% of the administered radioactivity recovered in the feces, while metabolites, primarily 6α-hydroxypaclitaxel, accounted for the balance. In vitro studies with human liver microsomes and tissue slices showed that paclitaxel was metabolized primarily to 6α-hydroxypaclitaxel by the cytochrome P450 isozyme CYP2C8; and to 2 minor metabolites, 3'- p -hydroxypaclitaxel and 6α, 3'- p -dihydroxypaclitaxel, by CYP3A4. In vitro , the metabolism of paclitaxel to 6α-hydroxypaclitaxel was inhibited by a number of agents (ketoconazole, verapamil, diazepam, quinidine, dexamethasone, cyclosporin, teniposide, etoposide, and vincristine), but the concentrations used exceeded those found in vivo following normal therapeutic doses. Testosterone, 17α-ethinyl estradiol, retinoic acid, and quercetin, a specific inhibitor of CYP2C8, also inhibited the formation of 6α-hydroxypaclitaxel in vitro . The pharmacokinetics of paclitaxel may also be altered in vivo as a result of interactions with compounds that are substrates, inducers, or inhibitors of CYP2C8 and/or CYP3A4 (see PRECAUTIONS, Drug Interactions ). The disposition and toxicity of paclitaxel 3-hour infusion were evaluated in 35 patients with varying degrees of hepatic function. Relative to patients with normal bilirubin, plasma paclitaxel exposure in patients with abnormal serum bilirubin ≤2 times upper limit of normal (ULN) administered 175 mg/m 2 was increased, but with no apparent increase in the frequency or severity of toxicity. In 5 patients with serum total bilirubin >2 times ULN, there was a statistically nonsignificant higher incidence of severe myelosuppression, even at a reduced dose (110 mg/m 2 ), but no observed increase in plasma exposure (see PRECAUTIONS, Hepatic and DOSAGE AND ADMINISTRATION ). The effect of renal or hepatic dysfunction on the disposition of paclitaxel has not been investigated. Possible interactions of paclitaxel with concomitantly administered medications have not been formally investigated."],"indications_and_usage":["INDICATIONS AND USAGE Paclitaxel Injection, USP is indicated as subsequent therapy for the treatment of advanced carcinoma of the ovary. As first-line therapy, Paclitaxel Injection, USP is indicated in combination with cisplatin. Paclitaxel Injection, USP is indicated for the adjuvant treatment of node-positive breast cancer administered sequentially to standard doxorubicin-containing combination chemotherapy. In the clinical trial, there was an overall favorable effect on disease-free and overall survival in the total population of patients with receptor-positive and receptor-negative tumors, but the benefit has been specifically demonstrated by available data (median follow-up 30 months) only in the patients with estrogen and progesterone receptor-negative tumors (see CLINICAL STUDIES, Breast Carcinoma ). Paclitaxel Injection, USP is indicated for the treatment of breast cancer after failure of combination chemotherapy for metastatic disease or relapse within 6 months of adjuvant chemotherapy. Prior therapy should have included an anthracycline unless clinically contraindicated. Paclitaxel Injection, USP, in combination with cisplatin, is indicated for the first-line treatment of non-small cell lung cancer in patients who are not candidates for potentially curative surgery and/or radiation therapy. Paclitaxel Injection, USP is indicated for the second-line treatment of AIDS-related Kaposi's sarcoma."],"clinical_studies_table":["
Intergroup (non-optimally debulked subset) GOG-111
T175/3a c75 (n=218) C750 a c75 (n=227) T135/24a c75 (n=196) C750 a c75 (n=214)
Clinical Responseb(n=153) (n=153) (n=113) (n=127)
- rate (percent) 58 43 62 48
- p-value c 0.016 0.04
Time to Progression
- median (months) 13.2 9.9 16.6 13.0
- p-valuec 0.0060 0.0008
- hazard ratio (HR) c 0.76 0.70
- 95% CIc 0.62 to 0.92 0.56 to 0.86
Survival
- median (months) 29.5 21.9 35.5 24.2
- p-valuec 0.0057 0.0002
- hazard ratio (HR)c 0.73 0.64
- 95% CIc 0.58 to 0.91 0.50 to 0.81
","
T175/3a c75 (n=342) C750 a c75 (n=338)
Clinical Responseb(n=162) (n=161)
- rate (percent) 59 45
- p-valuec 0.014
Time to Progression
- median (months) 15.3 11.5
- p-valuec 0.0005
- hazard ratio (HR) c 0.74
- 95% CIc 0.63 to 0.88
Survival
- median (months) 35.6 25.9
- p-valuec 0.0016
- hazard ratio (HR) c 0.73
- 95% CIc 0.60 to 0.89
","
175/3 (n=96) 175/24 (n=106) 135/3 (n=99) 135/24 (n=106)
Response
- rate (percent) 14.6 21.7 15.2 13.2
- 95% Confidence Interval (8.5 to 23.6) (14.5 to 31) (9 to 24.1) (7.7 to 21.5)
Time to Progression
- median (months) 4.4 4.2 3.4 2.8
- 95% Confidence Interval (3.0 to 5.6) (3.5 to 5.1) (2.8 to 4.2) (1.9 to 4)
Survival
- median (months) 11.5 11.8 13.1 10.7
- 95% Confidence Interval (8.4 to 14.4) (8.9 to 14.6) (9.1 to 14.6) (8.1 to 13.6)
","
Patient Subset Disease-Free Survival Overall Survival
No. of Patients No. of Recurrences Hazard Ratio (95% CI) No. of Deaths Hazard Ratio (95% CI)
No. Positive Nodes
1 to 3 1,449 221 0.72 (0.55 to 0.94) 107 0.76 (0.52 to 1.12)
4 to 9 1,310 274 0.78 (0.61 to 0.99) 148 0.66 (0.47 to 0.91)
10+ 360 129 0.93 (0.66 to 1.31) 87 0.90 (0.59 to 1.36)
Tumor Size (cm)
≤2 1,096 153 0.79 (0.57 to 1.08) 67 0.73 (0.45 to 1.18)
>2 and ≤5 1,611 358 0.79 (0.64 to 0.97) 201 0.74 (0.56 to 0.98)
>5 397 111 0.75 (0.51 to 1.08) 72 0.73 (0.46 to 1.16)
Menopausal Status
Pre 1,929 374 0.83 (0.67 to 1.01) 187 0.72 (0.54 to 0.97)
Post 1,183 250 0.73 (0.57 to 0.93) 155 0.77 (0.56 to 1.06)
Receptor Status
Positivea 2,066 293 0.92 (0.73 to 1.16) 126 0.83 (0.59 to 1.18)
Negative/Unknownb 1,055 331 0.68 (0.55 to 0.85) 216 0.71 (0.54 to 0.93)
","
175/3 (n=235) 135/3 (n=236)
Response - rate (percent) - p-value 28 0.135 22
Time to Progression - median (months) - p-value 4.2 0.027 3
Survival - median (months) - p-value 11.7 0.321 10.5
","
T135/24 c75 (n=198) T250/24 c75 (n=201) VP100a c75 (n=200)
Response
- rate (percent) 25 23 12
- p-valueb 0.001 <0.001
Time to Progression
- median (months) 4.3 4.9 2.7
- p-valueb 0.05 0.004
Survival
- median (months) 9.3 10 7.4
- p-valueb 0.12 0.08
1-Year Survival
- percent of patients 36 40 32
","
Prior Systemic Therapy (n=59)
Visceral ± edema ± oral ± cutaneous 42
Edema or lymph nodes ± oral ± cutaneous 41
Oral ± cutaneous 10
Cutaneous only 7
","
Prior Systemic Therapy (n=59)
Complete response 3
Partial response 56
Stable disease 29
Progression 8
Early death/toxicity 3
"],"adverse_reactions_table":["
Percent of Patients (n=812)
Bone Marrow - Neutropenia <2,000/mm3 <500/mm3 - Leukopenia <4,000/mm3 <1,000/mm3 - Thrombocytopenia <100,000/mm3 <50,000/mm3 - Anemia <11 g/dL <8 g/dL - Infections - Bleeding - Red Cell Transfusions - Platelet Transfusions 90 52 90 17 20 7 78 16 30 14 25 2
Hypersensitivity Reactionb - All - Severe 41 2
Cardiovascular - Vital Sign Changesc - Bradycardia (n=537) - Hypotension (n=532) - Significant Cardiovascular Events 3 12 1
Abnormal ECG - All Pts - Pts with normal baseline (n=559) 23 14
Peripheral Neuropathy - Any symptoms - Severe symptoms 60 3
Myalgia/Arthralgia - Any symptoms - Severe symptoms 60 8
Gastrointestinal - Nausea and vomiting - Diarrhea - Mucositis 52 38 31
Alopecia 87
Hepatic (Pts with normal baseline and on study data) - Bilirubin elevations (n=765) - Alkaline phosphatase elevations (n=575) - AST (SGOT) elevations (n=591) 7 22 19
Injection Site Reaction 13
","
Percent of Patients
Intergroup GOG-111
T175/3b c75c (n=339) C750c c75c (n=336) T135/24b c75c (n=196) C750c c75c (n=213)
Bone Marrow
- Neutropenia <2,000/mm3 91d 95d 96 92
<500/mm3 33d 43d 81d 58d
- Thrombocytopenia <100,000/mm3e 21d 33d 26 30
<50,000/mm3 3d 7d 10 9
- Anemia <11 g/dLf 96 97 88 86
<8 g/dL 3d 8d 13 9
- Infections 25 27 21 15
- Febrile Neutropenia 4 7 15d 4 d
Hypersensitivity Reaction
- All 11d 6d 8d,g 1d,g
- Severe 1 1 3d,g - d,g
Neurotoxicityh
- Any symptoms 87d 52d 25 20
- Severe symptoms 21d 2d 3d - d
Nausea and Vomiting
- Any symptoms 88 93 65 69
- Severe symptoms 18 24 10 11
Myalgia/Arthralgia
- Any symptoms 60d 27d 9d 2d
- Severe symptoms 6d 1d 1 -
Diarrhea
- Any symptoms 37d 29d 16d 8d
- Severe symptoms 2 3 4 1
Athenia
- Any symptoms NC NC 17d 10d
- Severe symptoms NC NC 1 1
Alopecia
- Any symptoms 96d 89d 55d 37d
- Severe symptoms 51d 21d 6 8
","
Percent of Patients
175/3b (n=95) 175/24 b (n=105) 135/3 b (n=98) 135/24 b (n=105)
Bone Marrow - Neutropenia <2,000/mm3 <500/mm3 - Thrombocytopenia <100,000/mm3 <50,000/mm3 - Anemia <11 g/dL <8 g/dL - Infections 78 27 4 1 84 11 26 98 75 18 7 90 12 29 78 14 8 2 68 6 20 98 67 6 1 88 10 18
Hypersensitivity Reactionc - All - Severe 41 2 45 0 38 2 45 1
Peripheral Neuropathy - Any symptoms - Severe symptoms 63 1 60 2 55 0 42 0
Mucositis - Any symptoms - Severe symptoms 17 0 35 3 21 0 25 2
","
Percent of Patients
Early Population Total Population
ACc (n=166) ACc followed by Td (n=159) ACc (n=1551) ACc followed by Td (n=1570)
Bone Marrowe
- Neutropenia <500/mm3 79 76 48 50
- Thrombocytopenia <50,000/mm3 27 25 11 11
- Anemia <8 g/dL 17 21 8 8
- Infections 6 14 5 6
- Fever Without Infection 3 <1 1
Hypersensitivity Reactionf1 4 1 2
Cardiovascular Events1 2 1 2
Neuromotor Toxicity1 1 <1 1
Neurosensory Toxicity3 <1 3
Myalgia/Arthralgia2 <1 2
Nausea/Vomiting13 18 8 9
Mucositis13 4 6 5
","
Percent of Patients
175/3b (n=229) 135/3 b (n=229)
Bone Marrow
- Neutropenia <2,000/mm3 90 81
<500/mm3 28 19
- Thrombocytopenia <100,000/mm3 11 7
<50,000/mm3 3 2
- Anemia <11 g/dL 55 47
<8 g/dL 4 2
- Infections 23 15
- Febrile Neutropenia 2 2
Hypersensitivity Reactionc
- All 36 31
- Severe 0 <1
Peripheral Neuropathy
- Any symptoms 70 46
- Severe symptoms 7 3
Mucositis
- Any symptoms 23 17
- Severe symptoms 3 <1
","
Percent of Patients
T135/24b c75 (n=195) T250/24 c c75 (n=197) VP100 d c75 (n=196)
Bone Marrow- Neutropenia <2,000/mm3 <500/mm3 - Thrombocytopenia <normal <50,000/mm3 - Anemia <normal <8 g/dL - Infections 89 74e 48 6 94 22 38 86 65 68 12 96 19 31 84 55 62 16 95 28 35
Hypersensitivity Reactionf- All - Severe 16 1 27 4e 13 1
Arthralgia/Myalgia- Any symptoms - Severe symptoms 21e 3 42e 11 9 1
Nausea/Vomiting- Any symptoms - Severe symptoms 85 27 87 29 81 22
Mucositis- Any symptoms - Severe symptoms 18 1 28 4 16 2
Neuromotor Toxicity- Any symptoms - Severe symptoms 37 6 47 12 44 7
Neurosensory Toxicity- Any symptoms - Severe symptoms 48 13 61 28e 25 8
Cardiovascular Events- Any symptoms - Severe symptoms 33 13 39 12 24 8
","
Percent of Patients
Study CA139-174 Paclitaxel 135/3b q 3 wk (n=29) Study CA139-281 Paclitaxel 100/3 b q 2 wk (n=56)
Bone Marrow
- Neutropenia <2,000/mm3 100 95
<500/mm3 76 35
- Thrombocytopenia <100,000/mm3 52 27
<50,000/mm3 17 5
- Anemia <11 g/dL 86 73
<8 g/dL 34 25
- Febrile Neutropenia 55 9
Opportunistic Infection
- Any 76 54
- Cytomegalovirus 45 27
- Herpes Simplex 38 11
- Pneumocystis carinii 14 21
- M. avinum intracellulare 24 4
- Candidiasis, esophageal 7 9
- Cryptosporidiosis 7 7
- Cryptococcal meningitis 3 2
- Leukoencephalopathy 2
Hypersensitivity Reactionc
- All 14 9
Cardiovascular
- Hypotension 17 9
- Bradycardia 3 -
Peripheral Neuropathy
- Any 79 46
- Severe 10 2
Myalgia/Arthralgia
- Any 93 48
- Severe 14 16
Gastrointestinal
- Nausea and Vomiting 69 70
- Diarrhea 90 73
- Mucositis 45 20
Renal (creatinine elevation)
- Any 34 18
- Severe 7 5
Discontinuation for drug toxicity 7 16
"],"dosage_and_administration":["DOSAGE & ADMINISTRATION Note: Contact of the undiluted concentrate with plasticized PVC equipment or devices used to prepare solutions for infusion is not recommended. In order to minimize patient exposure to the plasticizer DEHP [di-(2-ethylhexyl)phthalate], which may be leached from PVC infusion bags or sets, diluted paclitaxel solutions should be stored in bottles (glass, polypropylene) or plastic bags (polypropylene, polyolefin) and administered through polyethylene-lined administration sets. All patients should be premedicated prior to paclitaxel administration in order to prevent severe hypersensitivity reactions. Such premedication may consist of dexamethasone 20 mg PO administered approximately 12 and 6 hours before paclitaxel, diphenhydramine (or its equivalent) 50 mg I.V. 30 to 60 minutes prior to paclitaxel, and cimetidine (300 mg) or ranitidine (50 mg) I.V. 30 to 60 minutes before paclitaxel. For patients with carcinoma of the ovary the following regimen is recommended (see CLINICAL STUDIES, Ovarian Carcinoma ): For previously untreated patients with carcinoma of the ovary, one of the following recommended regimens may be given every 3 weeks. In selecting the appropriate regimen, differences in toxicities should be considered (see TABLE 11 in ADVERSE REACTIONS, Disease-Specific Adverse Event Experiences) . Paclitaxel administered intravenously over 3 hours at a dose of 175 mg/m 2 followed by cisplatin at a dose of 75 mg/m 2 ;or Paclitaxel administered intravenously over 24 hours at a dose of 135 mg/m 2 followed by cisplatin at a dose of 75 mg/m 2 . In patients previously treated with chemotherapy for carcinoma of the ovary, paclitaxel has been used at several doses and schedules; however, the optimal regimen is not yet clear (See CLINICAL STUDIES, Ovarian Carcinoma ). The recommended regimen is paclitaxel 135 mg/m 2 or 175 mg/m 2 administered intravenously over 3 hours every 3 weeks. For patients with carcinoma of the breast , the following is recommended (see CLINICAL STUDIES, Breast Carcinoma ): For the adjuvant treatment of node-positive breast cancer, the recommended regimen is paclitaxel, at a dose of 175 mg/m 2 intravenously over 3 hours every 3 weeks for 4 courses administered sequentially to doxorubicin-containing combination chemotherapy. The clinical trial used 4 courses of doxorubicin and cyclophosphamide (see CLINICAL STUDIES, Breast Carcinoma ). After failure of initial chemotherapy for metastatic disease or relapse within 6 months of adjuvant chemotherapy, paclitaxel at a dose of 175 mg/m 2 administered intravenously over 3 hours every 3 weeks has been shown to be effective. For patients with non-small cell lung carcinoma , the recommended regimen, given every 3 weeks, is paclitaxel administered intravenously over 24 hours at a dose of 135 mg/m 2 followed by cisplatin, 75 mg/m 2 . For patients with AIDS-related Kaposi’s sarcoma , paclitaxel administered at a dose of 135 mg/m 2 given intravenously over 3 hours every 3 weeks or at a dose of 100 mg/m 2 given intravenously over 3 hours every 2 weeks is recommended (dose intensity 45 to 50 mg/m 2 /week). In the 2 clinical trials evaluating these schedules (see CLINICAL STUDIES, AIDS-Related Kaposi’s Sarcoma ), the former schedule (135 mg/m 2 every 3 weeks) was more toxic than the latter. In addition, all patients with low performance status were treated with the latter schedule (100 mg/m 2 every 2 weeks). Based upon the immunosuppression in patients with advanced HIV disease, the following modifications are recommended in these patients: Reduce the dose of dexamethasone as 1 of the 3 premedication drugs to 10 mg PO (instead of 20 mg PO); Initiate or repeat treatment with paclitaxel only if the neutrophil count is at least 1,000 cells/mm 3 ; Reduce the dose of subsequent courses of paclitaxel by 20% for patients who experience severe neutropenia (neutrophil <500 cells/mm 3 for a week or longer); and Initiate concomitant hematopoietic growth factor (G-CSF) as clinicallyindicated. For the therapy of patients with solid tumors (ovary, breast and NSCLC), courses of paclitaxel should not be repeated until the neutrophil count is at least 1,500 cells/mm 3 and the platelet count is at least 100,000 cells/mm 3 . Paclitaxel should not be given to patients with AIDS-related Kaposi’s sarcoma if the baseline or subsequent neutrophil count is less than 1,000 cells/mm 3 . Patients who experience severe neutropenia (neutrophil <500 cells/mm 3 for a week or longer) or severe peripheral neuropathy during paclitaxel therapy should have dosage reduced by 20% for subsequent courses of paclitaxel. The incidence of neurotoxicity and the severity of neutropenia increase with dose. Preparation and Administration Precautions Paclitaxel is a cytotoxic anticancer drug and, as with other potentially toxic compounds, caution should be exercised in handling paclitaxel. The use of gloves is recommended. If paclitaxel solution contacts the skin, wash the skin immediately and thoroughly with soap and water. Following topical exposure, events have included tingling, burning and redness. If paclitaxel contacts mucous membranes, the membranes should be flushed thoroughly with water. Upon inhalation, dyspnea, chest pain, burning eyes, sore throat, and nausea have been reported. Hepatic Impairment Patients with hepatic impairment may be at increased risk of toxicity, particularly grade III–IV myelosuppression (see CLINICAL PHARMACOLOGY and PRECAUTIONS, Hepatic ). Recommendations for dosage adjustment for the first course of therapy are shown in TABLE 17 for both 3- and 24-hour infusions. Further dose reduction in subsequent courses should be based on individual tolerance. Patients should be monitored closely for the development of profound myelosuppression. TABLE 17. RECOMMENDATIONS FOR DOSING IN PATIENTS WITH HEPATIC IMPAIRMENT BASED ON CLINICAL TRIAL DATA a Degree of Hepatic Impairment Recommended Paclitaxel Dose c Transaminase Bilirubin Levels b Levels 24-Hour Infusion <2 x ULN and ≤1.5 mg/dL 135 mg/m 2 2 to <10 x ULN and ≤1.5 mg/dL 100 mg/m 2 <10 x ULN and 1.6 to 7.5 mg/dL 50 mg/m 2 ≥10 x ULN or >7.5 mg/dL Not recommended 3-Hour Infusion <10 x ULN and ≤1.25 x ULN 175 mg/m 2 <10 x ULN and 1.26 to 2 x ULN 135 mg/m 2 <10 x ULN and 2.01 to 5 x ULN 90 mg/m 2 ≥10 x ULN or >5.0 x ULN Not recommended a These recommendations are based on dosages for patients without hepatic impairment of 135 mg/m 2 over 24 hours or 175 mg/m 2 over 3 hours; data are not available to make dose adjustment recommendations for other regimens (eg, for AIDS-related Kaposi’s sarcoma). b Differences in criteria for bilirubin levels between the 3- and 24-hour infusion are due to differences in clinical trial design. c Dosage recommendations are for the first course of therapy; further dose reduction in subsequent courses should be based on individual tolerance. Preparation and Administration Precautions Procedures for proper handling and disposal of anticancer drugs should be considered. Several guidelines on this subject have been published. 1-4 To minimize the risk of dermal exposure, always wear impervious gloves when handling vials containing paclitaxel Injection. If paclitaxel solution contacts the skin, wash the skin immediately and thoroughly with soap and water. Following topical exposure, events have included tingling, burning, and redness. If paclitaxel contacts mucous membranes, the membranes should be flushed thoroughly with water. Upon inhalation, dyspnea, chest pain, burning eyes, sore throat, and nausea have been reported. Given the possibility of extravasation, it is advisable to closely monitor the infusion site for possible infiltration during drug administration. (See PRECAUTIONS, Injection Site Reaction ). Preparation for Intravenous Administration Paclitaxel must be diluted prior to infusion. Paclitaxel should be diluted in 0.9% Sodium Chloride Injection, USP; 5% Dextrose Injection, USP; 5% Dextrose and 0.9% Sodium Chloride Injection, USP; or 5% Dextrose in Ringer’s Injection to a final concentration of 0.3 to 1.2 mg/mL. The solutions are physically and chemically stable for up to 27 hours at ambient temperature (approximately 25°C) and room lighting conditions. Parenteral drug products should be inspected visually for particulate matter and discoloration prior to administration whenever solution and container permit. Upon preparation, solutions may show haziness, which is attributed to the formulation vehicle. No significant losses in potency have been noted following simulated delivery of the solution through I.V. tubing containing an in-line (0.22 micron) filter. Data collected for the presence of the extractable plasticizer DEHP [di-(2-ethylhexyl) phthalate] show that levels increase with time and concentration when dilutions are prepared in PVC containers. Consequently, the use of plasticized PVC containers and administration sets is not recommended. Paclitaxel solutions should be prepared and stored in glass, polypropylene, or polyolefin containers. Non-PVC containing administration sets, such as those which are polyethylene-lined, should be used. Paclitaxel should be administered through an in-line filter with a microporous membrane not greater than 0.22 microns. Use of filter devices such as IVEX-2® filters which incorporate short inlet and outlet PVC-coated tubing has not resulted in significant leaching of DEHP. The Chemo Dispensing Pin™ device or similar devices with spikes should not be used with vials of paclitaxel since they can cause the stopper to collapse resulting in loss of sterile integrity of the paclitaxel solution. Stability Unopened vials of paclitaxel are stable until the date indicated on the package when stored between 20° to 25°C (68° to 77°F), in the original package. Neither freezing nor refrigeration adversely affects the stability of the product. Upon refrigeration components in the paclitaxel vial may precipitate, but will redissolve upon reaching room temperature with little or no agitation. There is no impact on product quality under these circumstances. If the solution remains cloudy or if an insoluble precipitate is noted, the vial should be discarded. Solutions for infusion prepared as recommended are stable at ambient temperature (approximately 25°C) and lighting conditions for up to 27 hours."],"spl_product_data_elements":["Paclitaxel Paclitaxel PACLITAXEL PACLITAXEL ANHYDROUS CITRIC ACID POLYOXYL 35 CASTOR OIL ALCOHOL Paclitaxel Paclitaxel PACLITAXEL PACLITAXEL ANHYDROUS CITRIC ACID POLYOXYL 35 CASTOR OIL ALCOHOL Paclitaxel Paclitaxel PACLITAXEL PACLITAXEL ANHYDROUS CITRIC ACID POLYOXYL 35 CASTOR OIL ALCOHOL"],"clinical_pharmacology_table":["
Dose (mg/m2) Infusion Duration (h) N (patients) Cmax (ng/mL) AUC(0-∞) (ng•h/mL) T-HALF (h) CLT (L/h/m2)
135 24 2 195 6,300 52.7 21.7
175 24 4 365 7,993 15.7 23.8
135 3 7 2,170 7,952 13.1 17.7
175 3 5 3,650 15,007 20.2 12.2
"],"dosage_and_administration_table":["
Degree of Hepatic Impairment Recommended Paclitaxel Dosec
Transaminase Bilirubin Levelsb Levels
24-Hour Infusion
<2 x ULN and ≤1.5 mg/dL 135 mg/m2
2 to <10 x ULN and ≤1.5 mg/dL 100 mg/m2
<10 x ULN and 1.6 to 7.5 mg/dL 50 mg/m2
≥10 x ULN or >7.5 mg/dL Not recommended
3-Hour Infusion
<10 x ULN and ≤1.25 x ULN 175 mg/m2
<10 x ULN and 1.26 to 2 x ULN 135 mg/m2
<10 x ULN and 2.01 to 5 x ULN 90 mg/m2
≥10 x ULN or >5.0 x ULN Not recommended
"],"package_label_principal_display_panel":["PACKAGE LABEL.PRINCIPAL DISPLAY PANEL Paclitaxel Injection USP, 30 mg/vial - Vial Label Paclitaxel Injection USP, 30 mg/vial - Carton Label Paclitaxel Injection USP, 100 mg/vial - Vial Label Paclitaxel Injection USP, 100 mg/vial - Carton Label Paclitaxel Injection USP, 300 mg/vial - Vial Label Paclitaxel Injection USP, 300 mg/vial - Carton Label paclitaxel-30mg-vial-label paclitaxel-30mg-carton-label paclitaxel-100mg-vial-label paclitaxel-100mg-carton-label paclitaxel-300mg-vial-label paclitaxel-300mg-carton-label"],"carcinogenesis_and_mutagenesis_and_impairment_of_fertility":["Carcinogenesis, Mutagenesis, Impairment of Fertility The carcinogenic potential of paclitaxel has not been studied. Paclitaxel has been shown to be clastogenic in vitro (chromosome aberrations in human lymphocytes) and in vivo (micronucleus test in mice). Paclitaxel was not mutagenic in the Ames test of the CHO/HGPRT gene mutation assay. Administration of paclitaxel prior to and during mating produced impairment of fertility in male and female rats at doses equal to or greater than 1 mg/kg/day (about 0.04 the daily maximum recommended human dose on a mg/m 2 basis). At this dose, paclitaxel caused reduced fertility and reproductive indices, and increased embryo- and fetotoxicity. (See WARNINGS )."]},"tags":[{"label":"Microtubule Inhibitor","category":"class"},{"label":"Small Molecule","category":"modality"},{"label":"Tubulin beta-3 chain","category":"target"},{"label":"TUBB3","category":"gene"},{"label":"TUBB","category":"gene"},{"label":"TUBB1","category":"gene"},{"label":"L01CD01","category":"atc"},{"label":"Intravenous","category":"route"},{"label":"Injection","category":"form"},{"label":"Off-Patent","category":"patent"},{"label":"Generic Available","category":"availability"},{"label":"Established","category":"status"},{"label":"Carcinoma of breast","category":"indication"},{"label":"Carcinoma of fallopian tube","category":"indication"},{"label":"Hypertensive disorder","category":"indication"},{"label":"Kaposi's sarcoma","category":"indication"},{"label":"Malignant tumor of cervix","category":"indication"},{"label":"Malignant tumor of ovary","category":"indication"},{"label":"Hq Spclt Pharma","category":"company"},{"label":"Approved 1990s","category":"decade"},{"label":"Antimitotic Agents","category":"pharmacology"},{"label":"Antineoplastic Agents","category":"pharmacology"},{"label":"Antineoplastic Agents, Phytogenic","category":"pharmacology"},{"label":"Tubulin Modulators","category":"pharmacology"}],"phase":"marketed","safety":{"boxedWarnings":["WARNING Paclitaxel should be administered under the supervision of a physician experienced in the use of cancer chemotherapeutic agents. Appropriate management of complications is possible only when adequate diagnostic and treatment facilities are readily available. Anaphylaxis and severe hypersensitivity reactions characterized by dyspnea and hypotension requiring treatment, angioedema, and generalized urticaria have occurred in 2 to 4% of patients receiving paclitaxel in clinical trials. Fatal reactions have occurred in patients despite premedication. All patients should be pretreated with corticosteroids, diphenhydramine, and H 2 antagonists (see DOSAGE AND ADMINISTRATION ). Patients who experience severe hypersensitivity reactions to paclitaxel should not be rechallenged with the drug. Paclitaxel therapy should not be given to patients with solid tumors who have baseline neutrophil counts of less than 1,500 cells/mm 3 and should not be given to patients with AIDS-related Kaposi's sarcoma if the baseline neutrophil count is less than 1,000 cells/mm 3 . In order to monitor the occurrence of bone marrow suppression, primarily neutropenia, which may be severe and result in infection, it is recommended that frequent peripheral blood cell counts be performed on all patients receiving paclitaxel."],"safetySignals":[{"date":"","signal":"NAUSEA","source":"FDA FAERS","actionTaken":"5310 reports"},{"date":"","signal":"NEUTROPENIA","source":"FDA FAERS","actionTaken":"5216 reports"},{"date":"","signal":"DIARRHOEA","source":"FDA FAERS","actionTaken":"4969 reports"},{"date":"","signal":"DYSPNOEA","source":"FDA FAERS","actionTaken":"4926 reports"},{"date":"","signal":"OFF LABEL USE","source":"FDA FAERS","actionTaken":"4843 reports"},{"date":"","signal":"ANAEMIA","source":"FDA FAERS","actionTaken":"4615 reports"},{"date":"","signal":"DEATH","source":"FDA FAERS","actionTaken":"4360 reports"},{"date":"","signal":"FATIGUE","source":"FDA FAERS","actionTaken":"4050 reports"},{"date":"","signal":"MALIGNANT NEOPLASM PROGRESSION","source":"FDA FAERS","actionTaken":"3993 reports"},{"date":"","signal":"PYREXIA","source":"FDA FAERS","actionTaken":"3759 reports"}],"commonSideEffects":[{"effect":"Neutropenia","drugRate":"","severity":"serious","_validated":false,"_confidence":0.3},{"effect":"Neuropathy peripheral","drugRate":"","severity":"serious","_validated":false,"_confidence":0.3},{"effect":"Disease progression","drugRate":"","severity":"serious","_validated":false,"_confidence":0.3},{"effect":"Anaemia","drugRate":"","severity":"serious","_validated":false,"_confidence":0.3},{"effect":"Myelosuppression","drugRate":"","severity":"serious","_validated":false,"_confidence":0.3},{"effect":"Metastases to liver","drugRate":"","severity":"serious","_validated":false,"_confidence":0.3},{"effect":"Metastases to bone","drugRate":"","severity":"serious","_validated":false,"_confidence":0.3},{"effect":"Neutrophil count decreased","drugRate":"","severity":"serious","_validated":false,"_confidence":0.3},{"effect":"Flushing","drugRate":"","severity":"serious","_validated":false,"_confidence":0.3},{"effect":"Erythema","drugRate":"","severity":"serious","_validated":false,"_confidence":0.3},{"effect":"Thrombocytopenia","drugRate":"","severity":"serious","_validated":false,"_confidence":0.3},{"effect":"Leukopenia","drugRate":"","severity":"serious","_validated":false,"_confidence":0.3},{"effect":"Peripheral sensory neuropathy","drugRate":"","severity":"serious","_validated":false,"_confidence":0.3}],"contraindications":["Acute cerebrovascular insufficiency","Acute exacerbation of asthma","Acute infectious disease","Acute nephropathy","Anaphylaxis","Anemia","Asthma","Bone marrow depression","Bradycardia","Breastfeeding (mother)","Bronchospasm","Cardiogenic shock","Chronic heart failure","Complete atrioventricular block","Conduction disorder of the heart","Decompensated cardiac failure","Depressive disorder","Diabetes mellitus","Disease of liver","Heart block","Hyperbilirubinemia","Hypoglycemic disorder","Kidney disease","Liver function tests abnormal","Low blood pressure"],"specialPopulations":{"Lactation":"There are no data on the presence of paclitaxel in human milk, or its effect on the breastfed child or on milk production. In animal studies, paclitaxel and/or its metabolites were excreted into the milk of lactating rats. Because of the potential for serious adverse reactions in breastfed child from paclitaxel protein-bound particles for injectable suspension (albumin-bound), advise lactating women not to breastfeed during treatment with paclitaxel protein-bound particles for injectable suspension (albumin-bound).","Pregnancy":"Paclitaxel protein-bound particles for injectable suspension (albumin-bound) can cause fetal harm when administered to pregnant woman. Advise females of reproductive potential of the potential risk to fetus. The background rate of major birth defects and miscarriage is unknown for the indicated population. In the U.S. general population, the estimated background risk of major birth defects and miscarriage in clinically recognized pregnancies is 2% to 4% and 15% to 20%, respectively. Pregnancy Category D.","Geriatric use":"Of 2,228 patients who received paclitaxel in clinical studies evaluating its safety and effectiveness in the treatment of advanced ovarian cancer, breast carcinoma, or NSCLC, and 1,570 patients who were randomized to receive paclitaxel in the adjuvant breast cancer study, 649 patients (17%) were 65 years or older and 49 patients (1%) were 75 years or older. In most studies, severe myelosuppression was more frequent in elderly patients; in some studies, severe neuropathy was more ","Paediatric use":"The safety and effectiveness of paclitaxel in pediatric patients have not been established. There have been reports of central nervous system (CNS) toxicity (rarely associated with death) in clinical trial in pediatric patients in which paclitaxel was infused intravenously over hours at doses ranging from 350 mg/m2 to 420 mg/m2."}},"trials":[],"aliases":[],"company":"Pfizer","patents":[{"type":"Method of Use","number":"8034375","applicant":"BRISTOL-MYERS SQUIBB CO","territory":"US","tradeName":"ABRAXANE","expiryDate":"2026-08-13"},{"type":"Method of Use","number":"9511046","applicant":"BRISTOL-MYERS SQUIBB CO","territory":"US","tradeName":"ABRAXANE","expiryDate":"2034-01-12"},{"type":"Method of Use","number":"9393318","applicant":"BRISTOL-MYERS SQUIBB CO","territory":"US","tradeName":"ABRAXANE","expiryDate":"2032-03-04"},{"type":"Method of Use","number":"9597409","applicant":"BRISTOL-MYERS SQUIBB CO","territory":"US","tradeName":"ABRAXANE","expiryDate":"2032-03-04"},{"type":"Method of Use","number":"8268348","applicant":"BRISTOL-MYERS SQUIBB CO","territory":"US","tradeName":"ABRAXANE","expiryDate":"2026-02-21"},{"type":"Method of Use","number":"9101543","applicant":"BRISTOL-MYERS SQUIBB CO","territory":"US","tradeName":"ABRAXANE","expiryDate":"2026-02-21"},{"type":"Method of Use","number":"7758891","applicant":"BRISTOL-MYERS SQUIBB CO","territory":"US","tradeName":"ABRAXANE","expiryDate":"2026-02-21"},{"type":"Compound","number":"8034375*PED","applicant":"BRISTOL-MYERS SQUIBB CO","territory":"US","tradeName":"ABRAXANE","expiryDate":"2027-02-13"},{"type":"Compound","number":"8268348*PED","applicant":"BRISTOL-MYERS SQUIBB CO","territory":"US","tradeName":"ABRAXANE","expiryDate":"2026-08-21"},{"type":"Compound","number":"7758891*PED","applicant":"BRISTOL-MYERS SQUIBB CO","territory":"US","tradeName":"ABRAXANE","expiryDate":"2026-08-21"},{"type":"Compound","number":"9393318*PED","applicant":"BRISTOL-MYERS SQUIBB CO","territory":"US","tradeName":"ABRAXANE","expiryDate":"2032-09-04"},{"type":"Compound","number":"9101543*PED","applicant":"BRISTOL-MYERS SQUIBB CO","territory":"US","tradeName":"ABRAXANE","expiryDate":"2026-08-21"},{"type":"Compound","number":"9597409*PED","applicant":"BRISTOL-MYERS SQUIBB CO","territory":"US","tradeName":"ABRAXANE","expiryDate":"2032-09-04"},{"type":"Compound","number":"9511046*PED","applicant":"BRISTOL-MYERS SQUIBB CO","territory":"US","tradeName":"ABRAXANE","expiryDate":"2034-07-12"}],"pricing":[],"_sources":{"trials":{"url":"https://clinicaltrials.gov/search?intr=paclitaxel","method":"api_direct","source":"ClinicalTrials.gov","rawText":"","confidence":1,"sourceType":"ctgov","retrievedAt":"2026-04-19T23:52:50.780422+00:00"},"patents":{"url":"","method":"deterministic","source":"FDA Orange Book","rawText":"","confidence":1,"sourceType":"fda_orange_book","retrievedAt":"2026-04-19T23:52:50.780346+00:00"},"timeline":{"url":"https://en.wikipedia.org/wiki/Paclitaxel","method":"deterministic","source":"Wikipedia","rawText":"","confidence":0.8,"sourceType":"wikipedia","retrievedAt":"2026-04-19T23:52:58.026841+00:00"},"regulatory.ca":{"url":"","method":"api_direct","source":"Health Canada DPD","rawText":"","confidence":1,"sourceType":"health_canada_dpd","retrievedAt":"2026-04-19T23:52:56.640802+00:00"},"regulatory.eu":{"url":"","method":"api_direct","source":"European Medicines Agency","rawText":"","confidence":1,"sourceType":"ema_api","retrievedAt":"2026-04-19T23:52:50.853721+00:00"},"regulatory.us":{"url":"","method":"api_direct","source":"FDA Drugs@FDA","rawText":"","confidence":1,"sourceType":"fda_drugsfda","retrievedAt":"2026-04-19T23:52:49.913089+00:00"},"publicationCount":{"url":"https://pubmed.ncbi.nlm.nih.gov/?term=paclitaxel","method":"api_direct","source":"PubMed/NCBI","rawText":"","confidence":1,"sourceType":"pubmed","retrievedAt":"2026-04-19T23:52:56.929380+00:00"},"mechanism.drugClass":{"url":"https://api.fda.gov/drug/label.json","method":"deterministic","source":"FDA Label (EPC)","rawText":"","confidence":1,"sourceType":"fda_label","retrievedAt":"2026-04-19T23:52:47.448078+00:00"},"administration.route":{"url":"","method":"deterministic","source":"FDA Label","rawText":"","confidence":1,"sourceType":"fda_label","retrievedAt":"2026-04-19T23:52:47.448111+00:00"},"safety.boxedWarnings":{"url":"","method":"deterministic","source":"FDA Label (boxed_warning)","rawText":"WARNING Paclitaxel should be administered under the supervision of a physician experienced in the use of cancer chemotherapeutic agents. Appropriate management of complications is possible only when adequate diagnostic and treatment facilities are readily available. Anaphylaxis and severe hypersensitivity reactions characterized by dyspnea and hypotension requiring treatment, angioedema, and generalized urticaria have occurred in 2 to 4% of patients receiving paclitaxel in clinical trials. Fatal","confidence":1,"sourceType":"fda_label","retrievedAt":"2026-04-19T23:52:47.448120+00:00"},"safety.safetySignals":{"url":"https://api.fda.gov/drug/event.json","method":"api_direct","source":"FDA FAERS","rawText":"","confidence":1,"sourceType":"fda_faers","retrievedAt":"2026-04-19T23:52:58.510533+00:00"},"mechanism.target_chembl":{"url":"","method":"api_direct","source":"ChEMBL mechanism: Tubulin inhibitor","rawText":"","confidence":1,"sourceType":"chembl","retrievedAt":"2026-04-19T23:52:58.026787+00:00"},"crossReferences.chemblId":{"url":"https://www.ebi.ac.uk/chembl/compound_report_card/CHEMBL428647/","method":"api_direct","source":"ChEMBL (EMBL-EBI)","rawText":"","confidence":1,"sourceType":"chembl","retrievedAt":"2026-04-19T23:52:57.686241+00:00"},"regulatory.fda_application":{"url":"","method":"deterministic","source":"FDA Label","rawText":"ANDA216874","confidence":1,"sourceType":"fda_label","retrievedAt":"2026-04-19T23:52:47.448130+00:00"}},"allNames":"taxol","offLabel":[],"synonyms":["paclitaxel","(-)-Paclitaxel","abraxane","capxol","cyclopax","ebetaxel","genaxol","mitotax","padexol","plaxicel","taxol","Taxol A","Tocosol Paclitaxel","nabpaclitaxel","ABI-007","nab-paclitaxel"],"timeline":[{"date":"1992-01-01","type":"neutral","source":"FDA Orange Book","milestone":"Rights transferred from HQ SPCLT PHARMA to Hq Spclt Pharma"},{"date":"1992-12-29","type":"positive","source":"DrugCentral","milestone":"FDA approval (Hq Spclt Pharma)"},{"date":"2005-01-07","type":"positive","source":"FDA Orange Book","milestone":"Abraxane approved — 100MG/VIAL"},{"date":"2019-05-10","type":"positive","source":"DrugCentral","milestone":"EMA approval (Teva Bv)"},{"date":"2019-09-20","type":"positive","source":"DrugCentral","milestone":"PMDA approval (Taiho Pharmaceutical Co., Ltd.)"},{"date":"2022-07-27","type":"positive","source":"FDA Orange Book","milestone":"New formulation approved (Am Regent)"},{"date":"2023-05-11","type":"positive","source":"FDA Orange Book","milestone":"New formulation approved (Teva Pharms Inc)"},{"date":"2025-04-10","type":"neutral","source":"FDA Orange Book","milestone":"Generic entry — 16 manufacturers approved"}],"aiSummary":"Taxol (paclitaxel) is a microtubule inhibitor small molecule developed by HQ SPCLT PHARMA and currently owned by Hq Spclt Pharma. It targets the tubulin beta-3 chain and was FDA approved in 1992 for various cancer indications. As an off-patent medication, Taxol is available from multiple generic manufacturers. Key safety considerations include its low bioavailability and moderate half-life of 11 hours. Taxol is used to treat several types of cancer, including breast, ovarian, and cervical cancer.","brandName":"Taxol","ecosystem":[{"indication":"Carcinoma of breast","otherDrugs":[{"name":"cyclophosphamide","slug":"cyclophosphamide","company":"Baxter Hlthcare"},{"name":"docetaxel","slug":"docetaxel","company":"Sanofi Aventis Us"},{"name":"doxorubicin","slug":"doxorubicin","company":""},{"name":"epirubicin","slug":"epirubicin","company":"Pfizer Inc"}],"globalPrevalence":160000000},{"indication":"Carcinoma of fallopian tube","otherDrugs":[],"globalPrevalence":null},{"indication":"Hypertensive disorder","otherDrugs":[{"name":"acebutolol","slug":"acebutolol","company":"Promius Pharma"},{"name":"aliskiren","slug":"aliskiren","company":"Novartis"},{"name":"amiloride","slug":"amiloride","company":"Paddock Llc"},{"name":"amlodipine","slug":"amlodipine","company":"Pfizer"}],"globalPrevalence":null},{"indication":"Kaposi's sarcoma","otherDrugs":[{"name":"daunorubicin","slug":"daunorubicin","company":""},{"name":"doxorubicin","slug":"doxorubicin","company":""},{"name":"vinblastine","slug":"vinblastine","company":""}],"globalPrevalence":null},{"indication":"Malignant tumor of cervix","otherDrugs":[{"name":"bleomycin","slug":"bleomycin","company":"Bristol Myers Squibb"},{"name":"cemiplimab","slug":"cemiplimab","company":"Regeneron Pharmaceuticals "},{"name":"topotecan","slug":"topotecan","company":"Novartis Pharms Corp"}],"globalPrevalence":null},{"indication":"Malignant tumor of ovary","otherDrugs":[{"name":"altretamine","slug":"altretamine","company":"Eisai Inc"},{"name":"carboplatin","slug":"carboplatin","company":""},{"name":"cisplatin","slug":"cisplatin","company":"Hq Spclt Pharma"},{"name":"doxorubicin","slug":"doxorubicin","company":""}],"globalPrevalence":null},{"indication":"Malignant tumor of peritoneum","otherDrugs":[{"name":"bevacizumab","slug":"bevacizumab","company":"Genentech"},{"name":"niraparib","slug":"niraparib","company":"Tesaro Inc"},{"name":"olaparib","slug":"olaparib","company":"Astrazeneca Pharms"}],"globalPrevalence":null},{"indication":"Metastatic Breast Carcinoma","otherDrugs":[{"name":"capecitabine","slug":"capecitabine","company":"Hoffmann La Roche"},{"name":"docetaxel","slug":"docetaxel","company":"Sanofi Aventis Us"},{"name":"doxorubicin","slug":"doxorubicin","company":""},{"name":"eribulin","slug":"eribulin","company":"Eisai Inc"}],"globalPrevalence":null}],"mechanism":{"target":"Tubulin beta-3 chain","novelty":"Follow-on","targets":[{"gene":"TUBB3","source":"DrugCentral","target":"Tubulin beta-3 chain","protein":"Tubulin beta-3 chain"},{"gene":"TUBB","source":"DrugCentral","target":"Tubulin beta","protein":"Tubulin beta chain"},{"gene":"TUBB1","source":"DrugCentral","target":"Tubulin beta","protein":"Tubulin beta-1 chain"},{"gene":"TUBB2A","source":"DrugCentral","target":"Tubulin beta","protein":"Tubulin beta-2A chain"},{"gene":"TUBB2B","source":"DrugCentral","target":"Tubulin beta","protein":"Tubulin beta-2B chain"},{"gene":"TUBB4A","source":"DrugCentral","target":"Tubulin beta","protein":"Tubulin beta-4A chain"},{"gene":"TUBB4B","source":"DrugCentral","target":"Tubulin beta","protein":"Tubulin beta-4B chain"},{"gene":"TUBB6","source":"DrugCentral","target":"Tubulin beta","protein":"Tubulin beta-6 chain"},{"gene":"TUBB8","source":"DrugCentral","target":"Tubulin beta","protein":"Tubulin beta-8 chain"},{"gene":"OPRD1","source":"DrugCentral","target":"Delta-type opioid receptor","protein":"Delta-type opioid receptor"}],"modality":"Small Molecule","drugClass":"Microtubule Inhibitor [EPC]","explanation":"","oneSentence":"","technicalDetail":"Taxol binds to the beta subunit of tubulin, stabilizing microtubule dynamics and preventing the cell cycle progression from G2 to M phase, ultimately leading to cell death."},"_wikipedia":{"url":"https://en.wikipedia.org/wiki/Paclitaxel","title":"Paclitaxel","extract":"Paclitaxel, sold under the brand name Taxol among others, is a chemotherapy medication used to treat ovarian cancer, esophageal cancer, breast cancer, lung cancer, Kaposi's sarcoma, cervical cancer, and pancreatic cancer. It is administered by intravenous injection. There is also an albumin-bound formulation.","wiki_history":"==History==\nThe discovery of paclitaxel began in 1962 as a result of a NCI-funded screening program. These scientists isolated the natural product from the bark of the Pacific yew tree, determined its structure and named it \"taxol\", and arranged for its first biological testing. The compound was then developed commercially by BMS, who had the generic name assigned as \"paclitaxel\".\n\n===Plant screening program===\nIn 1955, the NCI in the United States set up the Cancer Chemotherapy National Service Center (CCNSC) to act as a public screening center for anticancer activity in compounds submitted by external institutions and companies. Although the majority of compounds screened were of synthetic origin, one chemist, Jonathan Hartwell, who was employed there from 1958 onwards, had experience with natural product derived compounds, and began a plant screening operation.\n\nAfter some years of informal arrangements, in July 1960, the NCI commissioned the United States Department of Agriculture (USDA) botanists to collect samples from about 1,000 plant species per year. On 21 August 1962, one of those botanists, Arthur S. Barclay, collected bark from a single Pacific yew tree in a forest north of the town of Packwood, Washington, as part of a four-month trip to collect material from over 200 different species. The material was then processed by a number of specialist CCNSC subcontractors, and one of the tree's samples was found to be cytotoxic in a cellular assay on 22 May 1964.\n\nAccordingly, in late 1964 or early 1965, the fractionation and isolation laboratory run by Monroe E. Wall in Research Triangle Park, North Carolina, began work on fresh Taxus samples, isolating the active ingredient in September 1966 and announcing their findings at an April 1967 American Chemical Society meeting in Miami Beach. They named the pure compound taxol in June 1967. Wall and his colleague Wani published their results, including the chemical structure, in 1971.\n\nThe NCI continued to commiss","wiki_society_and_culture":"== Society and culture ==\n\n=== Legal status ===\nPaclitaxel was approved for medical use in the European Union in 2008. Naveruclif was approved for medical use in the European Union in January 2024. Apexelsin was approved for medical use in the European Union in July 2024."},"commercial":{"launchDate":"1992","revenueYear":2025,"_launchSource":"DrugCentral (FDA 1992-12-29, HQ SPCLT PHARMA)","annualRevenue":368,"revenueSource":"SEC 8-K Bristol-Myers Squibb (2026-02-05)","revenueCurrency":"USD","revenueConfidence":"verified (SEC filing)","revenueExtractedAt":"2026-04-01T11:47:02.206315","revenueExtractedBy":"revenue-sec"},"references":[{"id":1,"url":"https://drugcentral.org/drugcard/2044","fields":["approvals","synonyms","ATC","PK","indications","contraindications","DDIs","targets","patents","FAERS"],"source":"DrugCentral"},{"id":2,"url":"https://clinicaltrials.gov/search?intr=paclitaxel","fields":["trials"],"source":"ClinicalTrials.gov"},{"id":3,"url":"https://pubmed.ncbi.nlm.nih.gov/?term=paclitaxel","fields":["publications"],"source":"PubMed/NCBI"},{"id":4,"url":"https://en.wikipedia.org/wiki/Paclitaxel","fields":["history","overview"],"source":"Wikipedia"},{"id":5,"url":"https://www.fda.gov/drugs/drug-approvals-and-databases/orange-book-data-files","fields":["patents","exclusivity","genericManufacturers"],"source":"FDA Orange Book"}],"_emaChecked":true,"_enrichedAt":"2026-03-30T02:33:52.896024","_validation":{"fieldsValidated":0,"lastValidatedAt":"2026-04-19T23:53:01.312122+00:00","fieldsConflicting":14,"overallConfidence":0.8},"biosimilars":[],"competitors":[{"drugName":"docetaxel","drugSlug":"docetaxel","fdaApproval":"1996-05-14","patentExpiry":"Sep 30, 2033","patentStatus":"Patent protected","relationship":"same-class"},{"drugName":"cabazitaxel","drugSlug":"cabazitaxel","fdaApproval":"2010-06-17","patentExpiry":"Oct 27, 2030","patentStatus":"Patent protected","relationship":"same-class"}],"genericName":"paclitaxel","indications":{"approved":[{"name":"Carcinoma of breast","source":"DrugCentral","snomedId":254838004,"regulator":"FDA","eligibility":{"adjuvant therapy":"node-positive breast cancer, administered sequentially to standard doxorubicin-containing combination chemotherapy","first-line therapy":"node-positive breast cancer, administered sequentially to standard doxorubicin-containing combination chemotherapy","metastatic disease":"prior therapy should have included an anthracycline unless clinically contraindicated"},"usPrevalence":null,"globalPrevalence":160000000,"prevalenceMethod":"curated","prevalenceSource":"Expert Rev Clin Pharmacol, 2019 (PMID:31287333)"},{"name":"Carcinoma of fallopian tube","source":"DrugCentral","snomedId":276870001,"regulator":"FDA","eligibility":{"advanced carcinoma":"no specific eligibility criteria mentioned"}},{"name":"Hypertensive disorder","source":"DrugCentral","snomedId":38341003,"regulator":"FDA","eligibility":{"no indication":"no specific eligibility criteria mentioned"}},{"name":"Kaposi's sarcoma","source":"DrugCentral","snomedId":109385007,"regulator":"FDA","eligibility":{"second-line treatment":"AIDS-related"}},{"name":"Malignant tumor of cervix","source":"DrugCentral","snomedId":363354003,"regulator":"FDA","eligibility":{"no indication":"no specific eligibility criteria mentioned"}},{"name":"Malignant tumor of ovary","source":"DrugCentral","snomedId":363443007,"regulator":"FDA","eligibility":{"advanced carcinoma":"no specific eligibility criteria mentioned"}},{"name":"Malignant tumor of peritoneum","source":"DrugCentral","snomedId":363492001,"regulator":"FDA","eligibility":{"no indication":"no specific eligibility criteria mentioned"}},{"name":"Metastatic Breast Carcinoma","source":"DrugCentral","snomedId":"","regulator":"FDA","eligibility":{"prior therapy":"prior therapy should have included an anthracycline unless clinically contraindicated"}},{"name":"Non-small cell lung cancer","source":"DrugCentral","snomedId":254637007,"regulator":"FDA","eligibility":{"first-line treatment":"not candidates for potentially curative surgery and/or radiation therapy"},"usPrevalence":236000,"globalPrevalence":2200000,"prevalenceMethod":"curated","prevalenceSource":"IARC GLOBOCAN, 2022"},{"name":"Ocular hypertension","source":"DrugCentral","snomedId":4210003,"regulator":"FDA","eligibility":{"no indication":"no specific eligibility criteria mentioned"},"usPrevalence":119900000,"globalPrevalence":1280000000,"prevalenceMethod":"curated","prevalenceSource":"WHO, 2023"},{"name":"Open-angle glaucoma","source":"DrugCentral","snomedId":84494001,"regulator":"FDA"},{"name":"Secondary malignant neoplasm of pancreas","source":"DrugCentral","snomedId":94459006,"regulator":"FDA"}],"offLabel":[{"name":"Aphakic glaucoma","source":"DrugCentral","drugName":"paclitaxel","evidenceCount":0,"evidenceLevel":"emerging"},{"name":"Endometrial carcinoma","source":"DrugCentral","drugName":"paclitaxel","evidenceCount":912,"evidenceLevel":"strong"},{"name":"Malignant glaucoma","source":"DrugCentral","drugName":"paclitaxel","evidenceCount":4,"evidenceLevel":"emerging"},{"name":"Malignant tumor of head and/or neck","source":"DrugCentral","drugName":"paclitaxel","evidenceCount":511072,"evidenceLevel":"strong"},{"name":"Malignant tumor of testis","source":"DrugCentral","drugName":"paclitaxel","evidenceCount":192,"evidenceLevel":"strong"},{"name":"Malignant tumor of urinary bladder","source":"DrugCentral","drugName":"paclitaxel","evidenceCount":410,"evidenceLevel":"strong"},{"name":"Neoplasm of esophagus","source":"DrugCentral","drugName":"paclitaxel","evidenceCount":967,"evidenceLevel":"strong"},{"name":"Secondary glaucoma","source":"DrugCentral","drugName":"paclitaxel","evidenceCount":2,"evidenceLevel":"emerging"},{"name":"Small cell carcinoma of lung","source":"DrugCentral","drugName":"paclitaxel"}],"pipeline":[]},"currentOwner":"Hq Spclt Pharma","drugCategory":"established","labelChanges":[],"patentStatus":"Off-patent — no active Orange Book patents","relatedDrugs":[{"drugId":"docetaxel","brandName":"docetaxel","genericName":"docetaxel","approvalYear":"1996","relationship":"same-class"},{"drugId":"cabazitaxel","brandName":"cabazitaxel","genericName":"cabazitaxel","approvalYear":"2010","relationship":"same-class"}],"trialDetails":[{"nctId":"NCT03907475","phase":"PHASE2","title":"Durvalumab in Combination With Chemotherapy in Treating Patients With Advanced Solid Tumors, DURVA+ Trial","status":"RECRUITING","sponsor":"National Cancer Institute (NCI)","startDate":"2019-07-16","conditions":["Locally Advanced Malignant Solid Neoplasm","Metastatic Malignant Solid Neoplasm"],"enrollment":115,"completionDate":"2026-06-01"},{"nctId":"NCT01167712","phase":"PHASE3","title":"Paclitaxel and Carboplatin With or Without Bevacizumab in Treating Patients With Stage II, Stage III, or Stage IV Ovarian Epithelial Cancer, Primary Peritoneal Cancer, or Fallopian Tube Cancer","status":"ACTIVE_NOT_RECRUITING","sponsor":"National Cancer Institute (NCI)","startDate":"2010-09-27","conditions":["Fallopian Tube Endometrioid Adenocarcinoma","Fallopian Tube Mucinous Adenocarcinoma","Fallopian Tube Transitional Cell Carcinoma","Ovarian Brenner Tumor","Ovarian Clear Cell Adenocarcinofibroma","Ovarian Endometrioid Adenocarcinoma","Ovarian Mucinous Adenocarcinoma","Ovarian Seromucinous Carcinoma","Ovarian Serous Adenocarcinoma","Ovarian Transitional Cell Carcinoma","Ovarian Undifferentiated Carcinoma","Primary Peritoneal Serous Adenocarcinoma","Stage IIA Fallopian Tube Cancer AJCC v6 and v7","Stage IIA Ovarian Cancer AJCC V6 and v7","Stage IIB Fallopian Tube Cancer AJCC v6 and v7","Stage IIB Ovarian Cancer AJCC v6 and v7","Stage IIC Fallopian Tube Cancer AJCC v6 and v7","Stage IIC Ovarian Cancer AJCC v6 and v7","Stage IIIA Fallopian Tube Cancer AJCC v7","Stage IIIA Ovarian Cancer AJCC v6 and v7","Stage IIIA Primary Peritoneal Cancer AJCC v7","Stage IIIB Fallopian Tube Cancer AJCC v7","Stage IIIB Ovarian Cancer AJCC v6 and v7","Stage IIIB Primary Peritoneal Cancer AJCC v7","Stage IIIC Fallopian Tube Cancer AJCC v7","Stage IIIC Ovarian Cancer AJCC v6 and v7","Stage IIIC Primary Peritoneal Cancer AJCC v7","Stage IV Fallopian Tube Cancer AJCC v6 and v7","Stage IV Ovarian Cancer AJCC v6 and v7","Stage IV Primary Peritoneal Cancer AJCC v7"],"enrollment":692,"completionDate":"2026-07-02"},{"nctId":"NCT05768932","phase":"PHASE1","title":"BAL0891 in Patients With Advanced Solid Tumors or Relapsed or Refractory Acute Myeloid Leukemia","status":"RECRUITING","sponsor":"SillaJen, Inc.","startDate":"2022-12-14","conditions":["Advanced Solid Tumor","TNBC - Triple-Negative Breast Cancer","Gastric Cancer","Leukemia Acute Myeloid Leukemia (AML)"],"enrollment":260,"completionDate":"2026-12-24"},{"nctId":"NCT07020065","phase":"PHASE2","title":"Reduced-dose Carboplatin-doublet-chemotherapy + Cemiplimab vs Cemiplimab Monotherapy in Treatment Naive Older and Frail Patients With Metastatic NSCLC With PD-L1 <50%","status":"NOT_YET_RECRUITING","sponsor":"Swiss Cancer Institute","startDate":"2026-05","conditions":["Metastatic NSCLC - Non-Small Cell Lung Cancer"],"enrollment":156,"completionDate":"2030-03"},{"nctId":"NCT06841354","phase":"PHASE3","title":"A Study of Sacituzumab Tirumotecan (Sac-TMT, MK-2870) as Monotherapy and in Combination With Pembrolizumab (MK-3475) in Participants With Triple-Negative Breast Cancer (MK-2870-011/TroFuse-011)","status":"RECRUITING","sponsor":"Merck Sharp & Dohme LLC","startDate":"2025-03-16","conditions":["Triple Negative Breast Neoplasms"],"enrollment":1000,"completionDate":"2030-05-18"},{"nctId":"NCT06203600","phase":"PHASE2,PHASE3","title":"Adding Nivolumab to Usual Treatment for People With Advanced Stomach or Esophageal Cancer, PARAMUNE Trial","status":"RECRUITING","sponsor":"National Cancer Institute (NCI)","startDate":"2024-06-24","conditions":["Advanced Esophageal Adenocarcinoma","Advanced Gastric Adenocarcinoma","Advanced Gastroesophageal Junction Adenocarcinoma","Clinical Stage II Esophageal Adenocarcinoma AJCC v8","Clinical Stage III Esophageal Adenocarcinoma AJCC v8","Clinical Stage III Gastric Cancer AJCC v8","Clinical Stage III Gastroesophageal Junction Adenocarcinoma AJCC v8","Clinical Stage IV Esophageal Adenocarcinoma AJCC v8","Clinical Stage IV Gastric Cancer AJCC v8","Clinical Stage IV Gastroesophageal Junction Adenocarcinoma AJCC v8","Metastatic Esophageal Adenocarcinoma","Metastatic Gastric Adenocarcinoma","Metastatic Gastroesophageal Junction Adenocarcinoma","Unresectable Esophageal Adenocarcinoma","Unresectable Gastric Adenocarcinoma","Unresectable Gastroesophageal Junction Adenocarcinoma"],"enrollment":224,"completionDate":"2027-10-31"},{"nctId":"NCT03568422","phase":"PHASE1,PHASE2","title":"CFI-402257 in Combination With Paclitaxel in Patients With Advanced/Metastatic HER2-Negative Breast Cancer","status":"ACTIVE_NOT_RECRUITING","sponsor":"Canadian Cancer Trials Group","startDate":"2019-02-05","conditions":["Breast Cancer"],"enrollment":37,"completionDate":"2026-12-31"},{"nctId":"NCT06966700","phase":"PHASE3","title":"A Clinical Study of Sacituzumab Tirumotecan (Sac-TMT, MK-2870) in People With Breast Cancer (MK-2870-032)","status":"RECRUITING","sponsor":"Merck Sharp & Dohme LLC","startDate":"2025-06-30","conditions":["Breast Neoplasms","Triple Negative Breast Neoplasms","HR Low-Positive/HER2-Negative Breast Neoplasms"],"enrollment":2400,"completionDate":"2034-12-29"},{"nctId":"NCT07493993","phase":"PHASE2","title":"Clinical Study on the Efficacy and Safety of Iparomlimab and Tuvonralimab Injection Combined With Nab-Paclitaxel in Neoadjuvant Therapy for Locally Advanced Resectable Esophageal Squamous Cell Carcinoma","status":"NOT_YET_RECRUITING","sponsor":"Tianjin Medical University Cancer Institute and Hospital","startDate":"2026-06-01","conditions":["ESCC"],"enrollment":26,"completionDate":"2030-12-31"},{"nctId":"NCT04090398","phase":"PHASE2","title":"Testing the Addition of Radium Therapy (Radium-223 Dichloride) to the Usual Chemotherapy Treatment (Paclitaxel) for Advanced Breast Cancer That Has Spread to the Bones","status":"ACTIVE_NOT_RECRUITING","sponsor":"National Cancer Institute (NCI)","startDate":"2020-08-04","conditions":["Anatomic Stage IV Breast Cancer AJCC v8","Metastatic HER2-Negative Breast Carcinoma","Metastatic Malignant Neoplasm in the Bone"],"enrollment":70,"completionDate":"2026-06-30"},{"nctId":"NCT02610439","phase":"","title":"Whole Exome Sequencing in Finding Causative Variants in Germline DNA Samples From Patients With Peripheral Neuropathy Receiving Paclitaxel for Breast Cancer","status":"RECRUITING","sponsor":"National Cancer Institute (NCI)","startDate":"2014-03-25","conditions":["Breast Carcinoma","Neuropathy"],"enrollment":575,"completionDate":"2100-01-01"},{"nctId":"NCT05564377","phase":"PHASE2","title":"Targeted Therapy Directed by Genetic Testing in Treating Patients With Locally Advanced or Advanced Solid Tumors, The ComboMATCH Screening Trial","status":"RECRUITING","sponsor":"National Cancer Institute (NCI)","startDate":"2023-04-07","conditions":["Advanced Malignant Solid Neoplasm","Anatomic Stage III Breast Cancer AJCC v8","Anatomic Stage IV Breast Cancer AJCC v8","Locally Advanced Malignant Solid Neoplasm","Malignant Female Reproductive System Neoplasm","Metastatic HER2-Negative Breast Carcinoma","Metastatic Malignant Solid Neoplasm","Recurrent Endometrial Carcinoma","Recurrent Fallopian Tube Carcinoma","Recurrent Malignant Female Reproductive System Neoplasm","Recurrent Malignant Solid Neoplasm","Recurrent Ovarian Carcinoma","Recurrent Primary Peritoneal Carcinoma","Unresectable HER2-Negative Breast Carcinoma","Unresectable Malignant Solid Neoplasm"],"enrollment":2900,"completionDate":"2030-07-01"},{"nctId":"NCT03606967","phase":"PHASE2","title":"Testing the Addition of an Individualized Vaccine to Durvalumab and Tremelimumab and Chemotherapy in Patients With Metastatic Triple Negative Breast Cancer","status":"RECRUITING","sponsor":"National Cancer Institute (NCI)","startDate":"2021-04-13","conditions":["Anatomic Stage IV Breast Cancer AJCC v8","Invasive Breast Carcinoma","Metastatic Triple-Negative Breast Carcinoma"],"enrollment":70,"completionDate":"2026-12-30"},{"nctId":"NCT06998940","phase":"PHASE3","title":"Studying Chemotherapy With or Without Panitumumab for Unresectable, Locally Advanced, or Metastatic Pancreatic Cancer Without KRAS Mutations","status":"RECRUITING","sponsor":"SWOG Cancer Research Network","startDate":"2026-04-01","conditions":["Locally Advanced Pancreatic Adenocarcinoma","Metastatic Pancreatic Adenocarcinoma","Stage III Pancreatic Cancer AJCC v8","Stage IV Pancreatic Cancer AJCC v8","Unresectable Pancreatic Adenocarcinoma"],"enrollment":94,"completionDate":"2030-12"},{"nctId":"NCT07198074","phase":"PHASE3","title":"Testing the Addition of an Antiangiogenic Drug (Bevacizumab) to Chemotherapy (Carboplatin and Paclitaxel) Combined With Immunotherapy (Pembrolizumab) for pMMR, TP53 Mutated Endometrial Cancer","status":"RECRUITING","sponsor":"National Cancer Institute (NCI)","startDate":"2026-01-27","conditions":["Advanced Endometrial Carcinoma","Recurrent Endometrial Carcinoma"],"enrollment":255,"completionDate":"2028-07-01"},{"nctId":"NCT04579224","phase":"PHASE3","title":"Comparing the New Anti-cancer Drug Eribulin With Chemotherapy Against the Usual Chemotherapy Alone in Metastatic Urothelial Cancer","status":"ACTIVE_NOT_RECRUITING","sponsor":"National Cancer Institute (NCI)","startDate":"2021-06-28","conditions":["Metastatic Bladder Urothelial Carcinoma","Metastatic Urothelial Carcinoma","Refractory Bladder Urothelial Carcinoma","Refractory Urothelial Carcinoma","Stage IV Bladder Cancer AJCC v8"],"enrollment":184,"completionDate":"2030-08-15"},{"nctId":"NCT06422143","phase":"PHASE3","title":"Pembrolizumab With or Without Maintenance Sacituzumab Tirumotecan (Sac-TMT; MK-2870) in Metastatic Squamous Non-small Cell Lung Cancer (NSCLC) [MK-2870-023]","status":"RECRUITING","sponsor":"Merck Sharp & Dohme LLC","startDate":"2024-06-10","conditions":["Non-small Cell Lung Cancer","NSCLC"],"enrollment":851,"completionDate":"2031-02-12"},{"nctId":"NCT04444921","phase":"PHASE3","title":"EA2176: Phase 3 Clinical Trial of Carboplatin and Paclitaxel +/- Nivolumab in Metastatic Anal Cancer Patients","status":"ACTIVE_NOT_RECRUITING","sponsor":"National Cancer Institute (NCI)","startDate":"2020-11-17","conditions":["Anal Basaloid Carcinoma","Anal Canal Cloacogenic Carcinoma","Metastatic Anal Squamous Cell Carcinoma","Recurrent Anal Squamous Cell Carcinoma","Stage III Anal Cancer AJCC v8","Stage IV Anal Cancer AJCC v8","Unresectable Anal Squamous Cell Carcinoma"],"enrollment":205,"completionDate":"2027-03-31"},{"nctId":"NCT01366144","phase":"PHASE1","title":"Veliparib, Paclitaxel, and Carboplatin in Treating Patients With Solid Tumors That Are Metastatic or Cannot Be Removed by Surgery and Liver or Kidney Dysfunction","status":"ACTIVE_NOT_RECRUITING","sponsor":"National Cancer Institute (NCI)","startDate":"2011-06-20","conditions":["Breast Carcinoma","Carcinoma of Unknown Primary","Endometrial Carcinoma","Esophageal Carcinoma","Liver Failure","Lung Carcinoma","Malignant Head and Neck Neoplasm","Malignant Testicular Neoplasm","Melanoma","Metastatic Malignant Solid Neoplasm","Ovarian Carcinoma","Renal Failure","Unresectable Malignant Neoplasm","Urothelial Carcinoma"],"enrollment":94,"completionDate":"2027-03-03"},{"nctId":"NCT05554341","phase":"PHASE2","title":"Testing the Use of Nilotinib and Paclitaxel as a Treatment for Patients With Prior Taxane Treatment, A ComboMATCH Treatment Trial","status":"ACTIVE_NOT_RECRUITING","sponsor":"National Cancer Institute (NCI)","startDate":"2023-07-14","conditions":["Metastatic Malignant Solid Neoplasm","Refractory Malignant Solid Neoplasm"],"enrollment":40,"completionDate":"2026-06-30"},{"nctId":"NCT05017012","phase":"PHASE1","title":"A Study to Evaluate the Bioavailability of Pembrolizumab (MK-3475) Via Subcutaneous (SC) Injection of Pembrolizumab Formulated With Berahyaluronidase Alfa (MK-5180) [MK-3475A] In Advanced Solid Tumors (MK-3475A-C18)","status":"ACTIVE_NOT_RECRUITING","sponsor":"Merck Sharp & Dohme LLC","startDate":"2021-09-21","conditions":["Advanced or Metastatic Solid Tumors"],"enrollment":72,"completionDate":"2026-05-19"},{"nctId":"NCT05554380","phase":"PHASE2","title":"Study of Chemotherapy Plus Ipatasertib for People With Solid Tumors With PTEN/AKT Mutations, A ComboMATCH Treatment Trial","status":"SUSPENDED","sponsor":"National Cancer Institute (NCI)","startDate":"2023-09-22","conditions":["Locally Advanced Malignant Solid Neoplasm","Metastatic Malignant Solid Neoplasm","Unresectable Malignant Solid Neoplasm"],"enrollment":33,"completionDate":"2026-08-31"},{"nctId":"NCT07259317","phase":"PHASE2","title":"Relacorilant With Nab-Paclitaxel and Gemcitabine in Patients With Metastatic Pancreatic Adenocarcinoma","status":"RECRUITING","sponsor":"Corcept Therapeutics","startDate":"2026-01-27","conditions":["Adenocarcinoma","Carcinoma, Pancreatic Ductal"],"enrollment":60,"completionDate":"2027-07"},{"nctId":"NCT06953323","phase":"PHASE1,PHASE2","title":"A Phase I/II Study of WJB001 Combination Therapy on Safety and Efficacy for Advanced Solid Tumors","status":"RECRUITING","sponsor":"Wigen Biomedicine Technology (Shanghai) Co., Ltd.","startDate":"2025-07-10","conditions":["Advanced Solid Tumor"],"enrollment":86,"completionDate":"2029-12-30"},{"nctId":"NCT06312176","phase":"PHASE3","title":"A Study of Sacituzumab Tirumotecan (MK-2870) as a Single Agent and in Combination With Pembrolizumab (MK-3475) Versus Treatment of Physician's Choice in Participants With HR+/HER2- Unresectable Locally Advanced or Metastatic Breast Cancer (MK-2870-010)","status":"RECRUITING","sponsor":"Merck Sharp & Dohme LLC","startDate":"2024-04-14","conditions":["Breast Neoplasms"],"enrollment":1200,"completionDate":"2031-04-12"},{"nctId":"NCT04449549","phase":"PHASE2","title":"Rapid Analysis and Response Evaluation of Combination Anti-Neoplastic Agents in Rare Tumors (RARE CANCER) Trial: RARE 1 Nilotinib and Paclitaxel","status":"RECRUITING","sponsor":"National Cancer Institute (NCI)","startDate":"2020-08-24","conditions":["Neoplasms"],"enrollment":82,"completionDate":"2026-04-08"},{"nctId":"NCT07195734","phase":"PHASE2","title":"Testing the Addition of Chemotherapy or Chemo-Immunotherapy to the Usual Surgery for Advanced Head and Neck Cancer","status":"RECRUITING","sponsor":"National Cancer Institute (NCI)","startDate":"2026-10-09","conditions":["Clinical Stage II HPV-Mediated (p16-Positive) Oropharyngeal Carcinoma AJCC v8","Clinical Stage III HPV-Mediated (p16-Positive) Oropharyngeal Carcinoma AJCC v8","Locally Recurrent Head and Neck Squamous Cell Carcinoma","Locally Recurrent Hypopharyngeal Squamous Cell Carcinoma","Locally Recurrent Laryngeal Squamous Cell Carcinoma","Locally Recurrent Oral Cavity Squamous Cell Carcinoma","Locally Recurrent Oropharyngeal Squamous Cell Carcinoma","Stage II Laryngeal Cancer AJCC v8","Stage II Lip and Oral Cavity Cancer AJCC v8","Stage II Oropharyngeal (p16-Negative) Carcinoma AJCC v8","Stage III Laryngeal Cancer AJCC v8","Stage III Lip and Oral Cavity Cancer AJCC v8","Stage III Oropharyngeal (p16-Negative) Carcinoma AJCC v8","Stage IVA Laryngeal Cancer AJCC v8","Stage IVA Lip and Oral Cavity Cancer AJCC v8","Stage IVA Oropharyngeal (p16-Negative) Carcinoma AJCC v8","Stage IVB Laryngeal Cancer AJCC v8","Stage IVB Oropharyngeal (p16-Negative) Carcinoma AJCC v8"],"enrollment":180,"completionDate":"2033-02-01"},{"nctId":"NCT01386385","phase":"PHASE1,PHASE2","title":"Veliparib With or Without Radiation Therapy, Carboplatin, and Paclitaxel in Patients With Stage III Non-small Cell Lung Cancer That Cannot Be Removed by Surgery","status":"ACTIVE_NOT_RECRUITING","sponsor":"National Cancer Institute (NCI)","startDate":"2011-06-20","conditions":["Lung Adenocarcinoma","Lung Adenocarcinoma, Mixed Subtype","Lung Large Cell Carcinoma","Lung Squamous Cell Carcinoma","Minimally Invasive Lung Adenocarcinoma","Stage III Lung Non-Small Cell Cancer AJCC v7","Stage IIIA Lung Non-Small Cell Cancer AJCC v7","Stage IIIB Lung Non-Small Cell Cancer AJCC v7"],"enrollment":53,"completionDate":"2026-12-31"},{"nctId":"NCT05685602","phase":"PHASE1","title":"CA-4948 Added to Standard Chemotherapy to Treat Metastatic or Unresectable Pancreatic Cancer","status":"RECRUITING","sponsor":"National Cancer Institute (NCI)","startDate":"2023-06-12","conditions":["Metastatic Pancreatic Ductal Adenocarcinoma","Stage III Pancreatic Cancer AJCC v8","Stage IV Pancreatic Cancer AJCC v8","Unresectable Pancreatic Ductal Adenocarcinoma"],"enrollment":43,"completionDate":"2026-04-30"},{"nctId":"NCT03914612","phase":"PHASE3","title":"Testing the Addition of the Immunotherapy Drug Pembrolizumab to the Usual Chemotherapy Treatment (Paclitaxel and Carboplatin) in Stage III-IV or Recurrent Endometrial Cancer","status":"ACTIVE_NOT_RECRUITING","sponsor":"National Cancer Institute (NCI)","startDate":"2019-08-22","conditions":["Endometrial Clear Cell Adenocarcinoma","Endometrial Dedifferentiated Carcinoma","Endometrial Endometrioid Adenocarcinoma","Endometrial Mixed Cell Adenocarcinoma","Endometrial Serous Adenocarcinoma","Endometrial Undifferentiated Carcinoma","Recurrent Endometrial Adenocarcinoma","Recurrent Endometrial Carcinoma","Recurrent Endometrial Clear Cell Adenocarcinoma","Recurrent Endometrial Dedifferentiated Carcinoma","Recurrent Endometrial Endometrioid Adenocarcinoma","Recurrent Endometrial Mixed Cell Adenocarcinoma","Recurrent Endometrial Serous Adenocarcinoma","Recurrent Endometrial Undifferentiated Carcinoma","Stage III Uterine Corpus Carcinoma or Carcinosarcoma AJCC v8","Stage IV Uterine Corpus Carcinoma or Carcinosarcoma AJCC v8"],"enrollment":813,"completionDate":"2026-09-26"},{"nctId":"NCT03604991","phase":"PHASE2,PHASE3","title":"Nivolumab and Ipilimumab in Treating Patients With Esophageal and Gastroesophageal Junction Adenocarcinoma Undergoing Surgery","status":"SUSPENDED","sponsor":"National Cancer Institute (NCI)","startDate":"2019-05-03","conditions":["Clinical Stage II Esophageal Adenocarcinoma AJCC v8","Clinical Stage II Gastroesophageal Junction Adenocarcinoma AJCC v8","Clinical Stage III Esophageal Adenocarcinoma AJCC v8","Clinical Stage III Gastroesophageal Junction Adenocarcinoma AJCC v8","Clinical Stage IVA Esophageal Adenocarcinoma AJCC v8","Clinical Stage IVA Gastroesophageal Junction Adenocarcinoma AJCC v8","Esophageal Adenocarcinoma","Gastroesophageal Junction Adenocarcinoma"],"enrollment":278,"completionDate":"2026-12-31"},{"nctId":"NCT06561685","phase":"PHASE1","title":"A Study of LY4050784 in Participants With Advanced or Metastatic Solid Tumors","status":"RECRUITING","sponsor":"Eli Lilly and Company","startDate":"2024-09-19","conditions":["Metastatic Solid Tumor","Advanced Solid Tumor","Non-small Cell Lung Cancer","SMARCA4-Deficient Tumor"],"enrollment":340,"completionDate":"2027-10"},{"nctId":"NCT06843447","phase":"PHASE1,PHASE2","title":"A Clinical Study of Raludotatug Deruxtecan in People With Ovarian Cancer (MK-5909-003)","status":"RECRUITING","sponsor":"Merck Sharp & Dohme LLC","startDate":"2025-04-15","conditions":["Ovarian Cancer Recurrent"],"enrollment":280,"completionDate":"2029-03-27"},{"nctId":"NCT05256225","phase":"PHASE3","title":"Testing the Addition of Herceptin Hylecta or Phesgo to the Usual Chemotherapy for HER2 Positive Endometrial Serous Carcinoma or Carcinosarcoma","status":"RECRUITING","sponsor":"National Cancer Institute (NCI)","startDate":"2022-11-16","conditions":["Endometrial Carcinoma","Endometrial Clear Cell Adenocarcinoma","Endometrial Dedifferentiated Carcinoma","Endometrial Endometrioid Adenocarcinoma","Endometrial Mixed Cell Adenocarcinoma","Endometrial Serous Adenocarcinoma","Endometrial Undifferentiated Carcinoma","Uterine Corpus Malignant Mixed Mesodermal (Mullerian) Tumor"],"enrollment":360,"completionDate":"2027-10-31"},{"nctId":"NCT04251533","phase":"PHASE3","title":"Study Assessing the Efficacy and Safety of Alpelisib + Nab-paclitaxel in Subjects With Advanced TNBC Who Carry Either a PIK3CA Mutation or Have PTEN Loss","status":"TERMINATED","sponsor":"Novartis Pharmaceuticals","startDate":"2020-06-08","conditions":["Triple Negative Breast Neoplasms"],"enrollment":137,"completionDate":"2026-02-05"},{"nctId":"NCT07061977","phase":"PHASE3","title":"Induction Pembrolizumab and Chemotherapy Followed by Pembrolizumab Before Chemoradiation and Pembrolizumab Maintenance Compared to Standard Chemoradiation With Pembrolizumab Followed by Pembrolizumab Maintenance in High-Risk Cervical Cancer","status":"RECRUITING","sponsor":"National Cancer Institute (NCI)","startDate":"2025-11-05","conditions":["Locally Advanced Cervical Adenocarcinoma","Locally Advanced Cervical Adenosquamous Carcinoma","Locally Advanced Cervical Squamous Cell Carcinoma","Stage IIIA Cervical Cancer FIGO 2018","Stage IIIB Cervical Cancer FIGO 2018","Stage IIIC1 Cervical Cancer FIGO 2018","Stage IIIC2 Cervical Cancer FIGO 2018","Stage IVA Cervical Cancer FIGO 2018"],"enrollment":336,"completionDate":"2030-12-31"},{"nctId":"NCT04092283","phase":"PHASE3","title":"Testing the Addition of an Antibody to Standard Chemoradiation Followed by the Antibody for One Year to Standard Chemoradiation Followed by One Year of the Antibody in Patients With Unresectable Stage III Non-Small Cell Lung Cancer","status":"ACTIVE_NOT_RECRUITING","sponsor":"National Cancer Institute (NCI)","startDate":"2020-04-29","conditions":["Recurrent Lung Non-Small Cell Carcinoma","Stage III Lung Cancer AJCC v8","Stage IIIA Lung Cancer AJCC v8","Stage IIIB Lung Cancer AJCC v8","Stage IIIC Lung Cancer AJCC v8","Unresectable Lung Non-Small Cell Carcinoma"],"enrollment":660,"completionDate":"2028-12-31"},{"nctId":"NCT05307705","phase":"PHASE1","title":"A Study of LOXO-783 in Patients With Breast Cancer/Other Solid Tumors","status":"ACTIVE_NOT_RECRUITING","sponsor":"Eli Lilly and Company","startDate":"2022-05-11","conditions":["Breast Cancer"],"enrollment":193,"completionDate":"2026-12"},{"nctId":"NCT05982522","phase":"PHASE1,PHASE2","title":"IN10018 Combination Therapy in Previously-treated Solid Tumors","status":"WITHDRAWN","sponsor":"InxMed (Shanghai) Co., Ltd.","startDate":"2025-08-13","conditions":["Solid Tumor"],"enrollment":0,"completionDate":"2026-12-31"},{"nctId":"NCT06058377","phase":"PHASE3","title":"Adding an Immunotherapy Drug, MEDI4736 (Durvalumab), to the Usual Chemotherapy Treatment (Paclitaxel, Cyclophosphamide, and Doxorubicin) for Stage II-III Breast Cancer","status":"RECRUITING","sponsor":"National Cancer Institute (NCI)","startDate":"2023-11-27","conditions":["Anatomic Stage II Breast Cancer AJCC v8","Anatomic Stage III Breast Cancer AJCC v8","HER2-Negative Breast Carcinoma","Hormone Receptor-Positive Breast Carcinoma"],"enrollment":3680,"completionDate":"2026-05-31"},{"nctId":"NCT05019716","phase":"PHASE1,PHASE2","title":"Testing the Safety and Efficacy of the Addition of a New Anti-cancer Drug, ZEN003694, to Chemotherapy Treatment (Cisplatin and Etoposide or Carboplatin and Paclitaxel) for Adult and Pediatric Patients (12-17 Years) With NUT Carcinoma","status":"RECRUITING","sponsor":"National Cancer Institute (NCI)","startDate":"2022-07-13","conditions":["Advanced NUT Carcinoma","Metastatic NUT Carcinoma","Unresectable NUT Carcinoma"],"enrollment":36,"completionDate":"2026-06-30"},{"nctId":"NCT06312137","phase":"PHASE3","title":"A Study to Assess Efficacy and Safety of Pembrolizumab With or Without Sacituzumab Tirumotecan (MK- 2870) in Adult Participants With Resectable Non Small Cell Lung Cancer (NSCLC) Not Achieving Pathological Complete Response (pCR) (MK-2870-019)","status":"RECRUITING","sponsor":"Merck Sharp & Dohme LLC","startDate":"2024-04-03","conditions":["Non Small Cell Lung Cancer"],"enrollment":780,"completionDate":"2034-10-23"},{"nctId":"NCT07281417","phase":"PHASE2","title":"Testing the Addition of Cemiplimab (REGN2810) to Chemotherapy Treatment Given Prior to Surgery in Patients With Sinonasal Squamous Cell Carcinoma","status":"RECRUITING","sponsor":"National Cancer Institute (NCI)","startDate":"2026-11-24","conditions":["Sinonasal Squamous Cell Carcinoma","Stage III Sinonasal Cancer AJCC v8","Stage IVA Sinonasal Cancer AJCC v8","Stage IVB Sinonasal Cancer AJCC v8"],"enrollment":108,"completionDate":"2030-12-16"},{"nctId":"NCT07060807","phase":"PHASE3","title":"A Clinical Study of Patritumab Deruxtecan to Treat Breast Cancer (MK-1022-016)","status":"RECRUITING","sponsor":"Merck Sharp & Dohme LLC","startDate":"2025-07-21","conditions":["Breast Neoplasms"],"enrollment":1000,"completionDate":"2033-07-14"},{"nctId":"NCT04310007","phase":"PHASE2","title":"Testing the Addition of the Pill Chemotherapy, Cabozantinib, to the Standard Immune Therapy Nivolumab Compared to Standard Chemotherapy for Non-small Cell Lung Cancer","status":"ACTIVE_NOT_RECRUITING","sponsor":"National Cancer Institute (NCI)","startDate":"2020-07-13","conditions":["Metastatic Lung Non-Squamous Non-Small Cell Carcinoma","Recurrent Lung Non-Squamous Non-Small Cell Carcinoma","Stage IV Lung Cancer AJCC v8"],"enrollment":117,"completionDate":"2026-12-31"},{"nctId":"NCT05673200","phase":"PHASE1","title":"Testing the Addition of an Anti-cancer Drug, ASTX727 (Cedazuridine, Decitabine), to Chemotherapy (Paclitaxel) and Immunotherapy (Pembrolizumab) for Metastatic Triple-Negative Breast Cancer","status":"RECRUITING","sponsor":"National Cancer Institute (NCI)","startDate":"2023-09-25","conditions":["Anatomic Stage III Breast Cancer AJCC v8","Anatomic Stage IV Breast Cancer AJCC v8","Metastatic Triple-Negative Breast Carcinoma","Unresectable Triple-Negative Breast Carcinoma"],"enrollment":32,"completionDate":"2027-02-23"},{"nctId":"NCT06096844","phase":"PHASE3","title":"Chemotherapy Combined With Immunotherapy Versus Immunotherapy Alone for Older Adults With Stage IIIB-IV Lung Cancer, The ACHIEVE Trial","status":"RECRUITING","sponsor":"National Cancer Institute (NCI)","startDate":"2024-07-19","conditions":["Advanced Lung Non-Small Cell Carcinoma","Stage IIIB Lung Cancer AJCC v8","Stage IIIC Lung Cancer AJCC v8","Stage IV Lung Cancer AJCC v8"],"enrollment":304,"completionDate":"2026-06-01"},{"nctId":"NCT04267848","phase":"PHASE3","title":"Testing the Addition of a Type of Drug Called Immunotherapy to the Usual Chemotherapy Treatment for Non-small Cell Lung Cancer, an ALCHEMIST Treatment Trial (Chemo-IO [ACCIO])","status":"RECRUITING","sponsor":"National Cancer Institute (NCI)","startDate":"2020-06-16","conditions":["Lung Non-Small Cell Carcinoma","Lung Non-Small Cell Squamous Carcinoma","Lung Non-Squamous Non-Small Cell Carcinoma","Stage II Lung Cancer AJCC v8","Stage IIIA Lung Cancer AJCC v8","Stage IIIB Lung Cancer AJCC v8"],"enrollment":1210,"completionDate":"2027-01-31"},{"nctId":"NCT02194738","phase":"NA","title":"Genetic Testing in Screening Patients With Stage IB-IIIA Non-small Cell Lung Cancer That Has Been or Will Be Removed by Surgery (The ALCHEMIST Screening Trial)","status":"ACTIVE_NOT_RECRUITING","sponsor":"National Cancer Institute (NCI)","startDate":"2014-09-26","conditions":["Stage IB Lung Non-Small Cell Carcinoma AJCC v7","Stage II Lung Non-Small Cell Cancer AJCC v7","Stage IIA Lung Cancer AJCC v8","Stage IIB Lung Cancer AJCC v8","Stage IIIA Lung Cancer AJCC v8","Stage IIIA Lung Non-Small Cell Cancer AJCC v7","Stage IIIB Lung Cancer AJCC v8"],"enrollment":8300,"completionDate":"2026-09-28"},{"nctId":"NCT06694454","phase":"PHASE1,PHASE2","title":"Neoadjuvant Inhaled Azacytidine With Platinum-Based Chemotherapy and Durvalumab (MEDI4736) - a Combined Epigenetic-Immunotherapy (AZA-AEGEAN) Regimen for Operable Early-Stage Non-Small Cell Lung Cancer (NSCLC)","status":"NOT_YET_RECRUITING","sponsor":"National Cancer Institute (NCI)","startDate":"2026-04-01","conditions":["Non-small Cell Lung Cancer (NSCLC)","Carcinoma, Non-Small Cell Lung","Non-Small Cell Lung Carcinoma","Non Small Cell Lung Cancer","Non Small Cell Lung Carcinoma"],"enrollment":60,"completionDate":"2034-12-31"},{"nctId":"NCT06524544","phase":"PHASE3","title":"A Study Comparing the Combination of Pembrolizumab and Sacituzumab Govitecan Versus Standard of Care in the Treatment of Advanced Urothelial Cancer","status":"RECRUITING","sponsor":"National Cancer Institute (NCI)","startDate":"2025-12-02","conditions":["Locally Advanced Urothelial Carcinoma","Metastatic Urothelial Carcinoma","Unresectable Urothelial Carcinoma"],"enrollment":320,"completionDate":"2028-12-31"},{"nctId":"NCT05771480","phase":"PHASE3","title":"Durvalumab With Chemotherapy as First Line Treatment in Patients With Advanced Biliary Tract Cancers (aBTCs)","status":"ACTIVE_NOT_RECRUITING","sponsor":"AstraZeneca","startDate":"2023-08-16","conditions":["Biliary Tract Cancer"],"enrollment":142,"completionDate":"2026-09-17"},{"nctId":"NCT02905591","phase":"PHASE2","title":"A Phase 2 Study Adding Ascorbate to Chemotherapy and Radiation Therapy for NSCLC","status":"ACTIVE_NOT_RECRUITING","sponsor":"Joseph J. Cullen, MD, FACS","startDate":"2018-11-16","conditions":["Carcinoma, Non-Small-Cell Lung","Non-Small Cell Lung Cancer","Nonsmall Cell Lung Cancer","Non-Small-Cell Lung Carcinoma","NSCLC"],"enrollment":43,"completionDate":"2027-12-31"},{"nctId":"NCT07138755","phase":"PHASE2","title":"The Efficacy and Safety of the Combination of PD-1 With Chemotherapy and Adaptive Radiotherapy Strategy in the Treatment of Stage III Non-small Cell Lung Cancer Patients","status":"RECRUITING","sponsor":"The Third Xiangya Hospital of Central South University","startDate":"2025-08-29","conditions":["NSCLC","Sintilimab","Adaptive Radiotherapy"],"enrollment":35,"completionDate":"2030-09"},{"nctId":"NCT07492680","phase":"PHASE2","title":"A Study of BMS-986504 Monotherapy and in Combination With Other Agents in Participants With Advanced and/or Metastatic Solid Tumors With Homozygous MTAP Deletion (MountainTAP-5)","status":"NOT_YET_RECRUITING","sponsor":"Bristol-Myers Squibb","startDate":"2026-07-17","conditions":["Solid Tumors"],"enrollment":260,"completionDate":"2032-05-20"},{"nctId":"NCT05825066","phase":"PHASE2","title":"Neoadjuvant Chemotherapy for Borderline Resectable and Locally Advanced Pancreatic Adenocarcinoma","status":"RECRUITING","sponsor":"Wake Forest University Health Sciences","startDate":"2023-08-01","conditions":["Pancreas Adenocarcinoma","Borderline Resectable Pancreatic Adenocarcinoma","Locally Advanced Pancreatic Adenocarcinoma"],"enrollment":64,"completionDate":"2028-07"},{"nctId":"NCT05108870","phase":"PHASE1,PHASE2","title":"TheraT® Vectors (Vaccines) Combined With Chemotherapy to Treat HPV16 Head and Neck Cancers","status":"NOT_YET_RECRUITING","sponsor":"University of Chicago","startDate":"2026-07-17","conditions":["Human Papilloma Virus","HPV","HPV Positive Oropharyngeal Squamous Cell Carcinoma","Head and Neck Cancer"],"enrollment":98,"completionDate":"2027-01-01"},{"nctId":"NCT05806060","phase":"PHASE3","title":"Precise Treatment for BLIS Subtype of TNBC in the First-line Treatment of Locally Advanced or Metastatic Breast Cancer","status":"RECRUITING","sponsor":"Fudan University","startDate":"2023-04-25","conditions":["Triple-Negative Breast Cancer"],"enrollment":134,"completionDate":"2026-11-01"},{"nctId":"NCT07493421","phase":"NA","title":"To Evaluate the Feasibility and Safety of Combining Surgery (Pancreatectomy and Cytoreduction) With HIPEC for Treating Pancreatic Cancer With Peritoneal Involvement.","status":"RECRUITING","sponsor":"Unidade Local de Saúde São João","startDate":"2026-03-01","conditions":["Pancreatic Adenocarcinoma","Peritoneal (Metastatic) Cancer"],"enrollment":20,"completionDate":"2028-10-01"},{"nctId":"NCT05620095","phase":"","title":"Durg Coated Balloon Angioplasty in Infrapopliteal Lesions","status":"RECRUITING","sponsor":"Liyuan Hospital of Tongji Medical College, Huazhong University of Science and Technology","startDate":"2020-12-01","conditions":["Arteriosclerosis","Peripheral Artery Disease","Chronic Limb Threatening Ischemia"],"enrollment":1000,"completionDate":"2026-11-01"},{"nctId":"NCT06333951","phase":"PHASE1","title":"AMG 193 Alone or in Combination With Other Therapies in Subjects With Advanced Thoracic Tumors With Homozygous MTAP-deletion (Master Protocol) (MTAPESTRY 104).","status":"RECRUITING","sponsor":"Amgen","startDate":"2024-09-17","conditions":["Thoracic Tumors","Non-small Cell Lung Cancer"],"enrollment":500,"completionDate":"2031-10-27"},{"nctId":"NCT07173751","phase":"PHASE3","title":"ROSETTA Breast-01: The Effects and Safety of Pumitamig in Patients With Triple-Negative Breast Cancer","status":"RECRUITING","sponsor":"BioNTech SE","startDate":"2025-10-30","conditions":["Breast Neoplasms"],"enrollment":558,"completionDate":"2030-09"},{"nctId":"NCT07492342","phase":"PHASE2","title":"Fulzerasib Sequential Sintilimab Plus Platinum-Doublet Neoadjuvant Therapy for Resectable KRAS G12C-Mutant NSCLC","status":"RECRUITING","sponsor":"Jianxing He","startDate":"2026-01-29","conditions":["Resectable NSCLC","KRAS G12C Mutation","Stage IB-IIIA NSCLC","Neoadjuvant Therapy"],"enrollment":30,"completionDate":"2027-12-31"},{"nctId":"NCT07221474","phase":"PHASE2","title":"A Study of V940/Placebo + Pembrolizumab and Chemotherapy in Metastatic Squamous Non-Small Cell Lung Cancer (V940-013)","status":"RECRUITING","sponsor":"Merck Sharp & Dohme LLC","startDate":"2025-12-12","conditions":["Squamous Non-small Cell Lung Cancer"],"enrollment":180,"completionDate":"2031-05-06"},{"nctId":"NCT06946797","phase":"PHASE2","title":"A Study to Evaluate Two Dosing Regimens of Subcutaneous Nivolumab in Combination With Intravenous Ipilimumab and Chemotherapy in Participants With Previously Untreated Metastatic or Recurrent Non-Small Cell Lung Cancer (NSCLC)","status":"RECRUITING","sponsor":"Bristol-Myers Squibb","startDate":"2025-09-19","conditions":["Non-Small Cell Lung Cancer"],"enrollment":76,"completionDate":"2028-10-25"},{"nctId":"NCT06926868","phase":"PHASE2,PHASE3","title":"A Study of Izalontamab Brengitecan Versus Chemotherapy in Participants With Previously Untreated, Locally Advanced, Recurrent Inoperable, or Metastatic Triple-negative Breast Cancer Ineligible for Anti-PD(L)1 Drugs (IZABRIGHT-Breast01)","status":"RECRUITING","sponsor":"Bristol-Myers Squibb","startDate":"2025-09-11","conditions":["Breast Neoplasms"],"enrollment":500,"completionDate":"2030-05-15"},{"nctId":"NCT04095364","phase":"PHASE3","title":"Letrozole With or Without Paclitaxel and Carboplatin in Treating Patients With Stage II-IV Ovarian, Fallopian Tube, or Primary Peritoneal Cancer","status":"ACTIVE_NOT_RECRUITING","sponsor":"NRG Oncology","startDate":"2019-09-20","conditions":["Low Grade Fallopian Tube Serous Adenocarcinoma","Ovarian Low Grade Serous Adenocarcinoma","Primary Peritoneal Low Grade Serous Adenocarcinoma","Stage II Fallopian Tube Cancer AJCC v8","Stage II Ovarian Cancer AJCC v8","Stage II Primary Peritoneal Cancer AJCC v8","Stage III Fallopian Tube Cancer AJCC v8","Stage III Ovarian Cancer AJCC v8","Stage III Primary Peritoneal Cancer AJCC v8","Stage IV Fallopian Tube Cancer AJCC v8","Stage IV Ovarian Cancer AJCC v8","Stage IV Primary Peritoneal Cancer AJCC v8"],"enrollment":450,"completionDate":"2028-02-01"},{"nctId":"NCT06535607","phase":"PHASE2","title":"Study of Volrustomig as Monotherapy or in Combination With Anti- Cancer Agents in Participants With Advanced/Metastatic Solid Tumors","status":"RECRUITING","sponsor":"AstraZeneca","startDate":"2024-08-22","conditions":["Sub-study 1 Cervical Cancer (Volrustomig Monotherapy)","Sub-study 2 Head and Neck Squamous Cell Carcinoma (Volrustomig Monotherapy)","Sub-study 3 Head and Neck Squamous Cell Carcinoma (Volrustomig in Combination With Chemotherapy)","Sub-study 4 Esophageal Squamous Cell Carcinoma (Volrustomig in Combination With Chemotherapy)","Sub-study 5 Unresectable Pleural Mesothelioma (Volrustomig Monotherapy)"],"enrollment":257,"completionDate":"2028-11-30"},{"nctId":"NCT07076121","phase":"PHASE2,PHASE3","title":"A Study Comparing BMS-986504 in Combination With Nab-paclitaxel and Gemcitabine Versus Placebo in Combination With Nab-paclitaxel and Gemcitabine in Participants With Untreated Metastatic Pancreatic Ductal Adenocarcinoma With Homozygous MTAP Deletion (MountainTAP-30)","status":"RECRUITING","sponsor":"Bristol-Myers Squibb","startDate":"2025-10-23","conditions":["Pancreatic Ductal Adenocarcinoma"],"enrollment":470,"completionDate":"2029-05-03"},{"nctId":"NCT06323460","phase":"PHASE2","title":"Adaptive De-intensified Radiotherapy Using Circulating Tumor DNA in HPV- Associated Oropharyngeal Cancer","status":"RECRUITING","sponsor":"Ohio State University Comprehensive Cancer Center","startDate":"2024-03-21","conditions":["Clinical Stage I HPV-Mediated (p16-Positive) Oropharyngeal Carcinoma AJCC v8","Clinical Stage II HPV-Mediated (p16-Positive) Oropharyngeal Carcinoma AJCC v8","Oropharyngeal Squamous Cell Carcinoma"],"enrollment":45,"completionDate":"2026-12-31"},{"nctId":"NCT07491445","phase":"PHASE3","title":"Study of Daraxonrasib and Daraxonrasib + GnP as First-line Treatment in Patients With Metastatic Pancreatic Adenocarcinoma","status":"RECRUITING","sponsor":"Revolution Medicines, Inc.","startDate":"2026-03-09","conditions":["Pancreatic Cancer","Pancreatic Cancer Metastatic","PDAC","PDAC - Pancreatic Ductal Adenocarcinoma","Pancreatic Ductal Adenocarcinoma (PDAC)","Pancreatic Adenocarcinoma Metastatic","Pancreatic Adenocarcinoma","Pancreatic Adenosquamous Carcinoma"],"enrollment":900,"completionDate":"2029-03"},{"nctId":"NCT04858269","phase":"PHASE2","title":"First Line Weekly Chemo/Immunotherapy for Metastatic Head/Neck Squamous Cell Carcinoma Patients","status":"RECRUITING","sponsor":"Wake Forest University Health Sciences","startDate":"2021-05-27","conditions":["Head Neck Cancer","Metastatic Squamous Cell Carcinoma","Oral Cavity Squamous Cell Carcinoma","Oropharynx Squamous Cell Carcinoma","Hypopharynx Squamous Cell Carcinoma","Larynx Squamous Cell Carcinoma"],"enrollment":32,"completionDate":"2028-08"},{"nctId":"NCT07490002","phase":"PHASE2","title":"Neoadjuvant Therapy With Iparomlimab and Tuvonralimab, Lenvatinib and Chemotherapy in Resectable ESCC","status":"NOT_YET_RECRUITING","sponsor":"Changhai Hospital","startDate":"2026-04-06","conditions":["Esophageal Squamous Carcinoma"],"enrollment":33,"completionDate":"2030-11-30"},{"nctId":"NCT06623422","phase":"PHASE3","title":"A Study of Pembrolizumab (MK-3475) With or Without Intismeran Autogene (V940) in Participants With Non-small Cell Lung Cancer (V940-009/INTerpath-009)","status":"RECRUITING","sponsor":"Merck Sharp & Dohme LLC","startDate":"2024-10-21","conditions":["Carcinoma, Non-Small-Cell Lung"],"enrollment":680,"completionDate":"2038-01-26"},{"nctId":"NCT07191860","phase":"NA","title":"Paclitaxel-Coated Pulmonary Balloon for the Treatment of Benign Central Airway Stenosis","status":"NOT_YET_RECRUITING","sponsor":"Airiver Medical, Inc.","startDate":"2026-03-01","conditions":["Adult Subjects With Symptomatic Benign Airway Obstruction","Adult Benign Central Airway Stenosis","Adult Tracheobronchial Stenosis","Tracheal Stenosis","Central Airway Stenosis","Central Airway Obstruction"],"enrollment":200,"completionDate":"2030-11-01"},{"nctId":"NCT07491822","phase":"NA","title":"A Single-Arm, Single-Center, Phase II Clinical Study of Camrelizumab Combined With Radiochemotherapy as Neoadjuvant Therapy for Early-Stage Triple-Negative Breast Cancer","status":"NOT_YET_RECRUITING","sponsor":"Tianjin Medical University Cancer Institute and Hospital","startDate":"2026-03-25","conditions":["TNBC"],"enrollment":43,"completionDate":"2031-03-15"},{"nctId":"NCT04008797","phase":"PHASE1,PHASE2","title":"A Study of E7386 in Combination With Other Anticancer Drug(s) in Participants With Solid Tumor","status":"ACTIVE_NOT_RECRUITING","sponsor":"Eisai Inc.","startDate":"2019-07-11","conditions":["Endometrial Neoplasms","Neoplasms","Carcinoma, Hepatocellular","Liver Neoplasms","Colorectal Neoplasms"],"enrollment":301,"completionDate":"2027-03-31"},{"nctId":"NCT06792786","phase":"NA","title":"A Multicenter Prospective Study Evaluating Concurrent Chemoradiotherapy Following Induction Immunochemotherapy for Esophageal Cancer Based on Dynamic ctDNA Monitoring","status":"RECRUITING","sponsor":"The Central Hospital of Lishui City","startDate":"2024-12-10","conditions":["Esophageal Cancer","ctDNA"],"enrollment":30,"completionDate":"2027-12-30"},{"nctId":"NCT06917079","phase":"PHASE1","title":"BBO-11818 in Adult Subjects With KRAS Mutant Cancer","status":"RECRUITING","sponsor":"TheRas, Inc., d/b/a BBOT (BridgeBio Oncology Therapeutics)","startDate":"2025-03-31","conditions":["Non-Small Cell Lung Cancer","NSCLC","PDAC - Pancreatic Ductal Adenocarcinoma","CRC (Colorectal Cancer)","Metastatic Non-Small Lung Cell Cancer","Metastatic Colorectal Cancer (CRC)","KRAS G12A","KRAS G12C","KRAS G12D","KRAS G12S","KRAS G12V","Metastatic Pancreatic Ductal Adenocarcinoma","Advanced Lung Carcinoma","Solid Tumor, Adult"],"enrollment":387,"completionDate":"2029-09"},{"nctId":"NCT04677816","phase":"PHASE2","title":"Impact of Vitamin D Supplementation on the Rate of Pathologic Complete Response in Vitamin D Deficient Patients","status":"RECRUITING","sponsor":"Wake Forest University Health Sciences","startDate":"2021-10-22","conditions":["Triple Negative Breast Cancer","Vitamin D Deficiency","Invasive Breast Cancer"],"enrollment":50,"completionDate":"2026-08"},{"nctId":"NCT04266249","phase":"PHASE2","title":"CompassHER2-pCR: Decreasing Chemotherapy for Breast Cancer Patients After Pre-surgery Chemo and Targeted Therapy","status":"ACTIVE_NOT_RECRUITING","sponsor":"ECOG-ACRIN Cancer Research Group","startDate":"2020-03-13","conditions":["Anatomic Stage II Breast Cancer AJCC v8","Anatomic Stage IIA Breast Cancer AJCC v8","Anatomic Stage IIB Breast Cancer AJCC v8","Anatomic Stage IIIA Breast Cancer AJCC v8","Invasive Breast Carcinoma","Prognostic Stage II Breast Cancer AJCC v8","Prognostic Stage IIA Breast Cancer AJCC v8","Prognostic Stage IIB Breast Cancer AJCC v8","Prognostic Stage IIIA Breast Cancer AJCC v8"],"enrollment":2175,"completionDate":"2038-12-31"},{"nctId":"NCT04647253","phase":"PHASE3","title":"A Clinical Trial to Assess the Agent Paclitaxel Coated PTCA Balloon Catheter for the Treatment of Subjects With In-Stent Restenosis (ISR)","status":"ACTIVE_NOT_RECRUITING","sponsor":"Boston Scientific Corporation","startDate":"2021-05-11","conditions":["In-Stent Restenosis"],"enrollment":600,"completionDate":"2027-09"},{"nctId":"NCT07487896","phase":"PHASE3","title":"A Phase III Study Evaluating YL201 Versus ICC in 2L ESCC","status":"NOT_YET_RECRUITING","sponsor":"MediLink Therapeutics (Suzhou) Co., Ltd.","startDate":"2026-04-30","conditions":["Advanced Esophageal Squamous Cell Carcinoma"],"enrollment":440,"completionDate":"2028-12-31"},{"nctId":"NCT07214779","phase":"PHASE3","title":"Study to Evaluate INCB123667 Versus Investigator's Choice of Chemotherapy in Participants With Platinum-Resistant Ovarian Cancer With Cyclin E1 Overexpression","status":"RECRUITING","sponsor":"Incyte Corporation","startDate":"2025-12-09","conditions":["Ovarian Cancer"],"enrollment":466,"completionDate":"2029-05-14"},{"nctId":"NCT02654119","phase":"PHASE2","title":"Cyclophosphamide, Paclitaxel, and Trastuzumab in Treating Stage I-II HER2/Neu Positive Breast Cancer After Surgery","status":"COMPLETED","sponsor":"University of Nebraska","startDate":"2015-12-11","conditions":["HER2 Positive Breast Carcinoma","Stage I Breast Cancer AJCC v7","Stage IA Breast Cancer AJCC v7","Stage IB Breast Cancer AJCC v7","Stage II Breast Cancer AJCC v6 and v7","Stage IIA Breast Cancer AJCC v6 and v7","Stage IIB Breast Cancer AJCC v6 and v7"],"enrollment":20,"completionDate":"2025-12-08"},{"nctId":"NCT06915025","phase":"PHASE3","title":"Phase 3 Trial Evaluating the Safety & Efficacy of IMNN-001 Administered in Combination w/ Standard NACT & Adjuvant Chemotherapy in Newly Diagnosed Patients w/ Advanced EOC, Fallopian Tube or Primary Peritoneal Cancer","status":"RECRUITING","sponsor":"Imunon","startDate":"2025-07-09","conditions":["Epithelial Ovarian Cancer","Ovarian Cancer","Fallopian Tube Cancer","Primary Peritoneal Carcinoma"],"enrollment":500,"completionDate":"2032-10-31"},{"nctId":"NCT07001748","phase":"PHASE2,PHASE3","title":"Testing the Addition of Paclitaxel Administered Into the Abdominal Cavity Combined With Chemotherapy for Patients With Gastric Cancer Spread to the Abdominal Cavity","status":"RECRUITING","sponsor":"ECOG-ACRIN Cancer Research Group","startDate":"2025-08-19","conditions":["Gastric Adenocarcinoma","Gastroesophageal Junction Adenocarcinoma","Peritoneal Carcinomatosis"],"enrollment":148,"completionDate":"2030-05-30"},{"nctId":"NCT03044613","phase":"PHASE1","title":"Nivolumab +/- Relatlimab Prior to Chemoradiation With II/III Gastro/Esophageal Cancer","status":"ACTIVE_NOT_RECRUITING","sponsor":"Sidney Kimmel Comprehensive Cancer Center at Johns Hopkins","startDate":"2017-07-11","conditions":["Gastric Cancer","Esophageal Cancer","GastroEsophageal Cancer"],"enrollment":32,"completionDate":"2027-08"},{"nctId":"NCT04233866","phase":"PHASE2","title":"Comparing Two Treatment Combinations, Gemcitabine and Nab-Paclitaxel With 5-Fluorouracil, Leucovorin, and Liposomal Irinotecan for Older Patients With Pancreatic Cancer That Has Spread","status":"ACTIVE_NOT_RECRUITING","sponsor":"ECOG-ACRIN Cancer Research Group","startDate":"2020-08-26","conditions":["Metastatic Pancreatic Adenocarcinoma","Stage IV Pancreatic Cancer AJCC v8"],"enrollment":176,"completionDate":"2026-12-31"},{"nctId":"NCT07488884","phase":"PHASE1","title":"Open-Label, Phase 1 Clinical Trial of Neoadjuvant Nogapendekin Alfa Inbakicept, Sotevtamab, and Zabadinostat in Combination With Gemcitabine and Nab-Paclitaxel for Participants With Borderline Resectable or Locally Advanced Pancreatic Cancer","status":"NOT_YET_RECRUITING","sponsor":"ImmunityBio, Inc.","startDate":"2026-03-01","conditions":["Pancreatic Cancer Resectable","Pancreatic Cancer"],"enrollment":30,"completionDate":"2029-06-01"},{"nctId":"NCT06492174","phase":"PHASE3","title":"A Clinical Trial to Assess the Agent Paclitaxel Coated PTCA Balloon Catheter for the Treatment of Subjects With In-Stent Restenosis (ISR) - Long Lesion Cohort","status":"ACTIVE_NOT_RECRUITING","sponsor":"Boston Scientific Corporation","startDate":"2024-10-07","conditions":["In-Stent Restenosis"],"enrollment":20,"completionDate":"2027-12"},{"nctId":"NCT06493019","phase":"PHASE2","title":"Study of Pembrolizumab, Carboplatin, Paclitaxel, and Radiation for the Treatment of Early-Stage Anal Cancer","status":"RECRUITING","sponsor":"Dustin Deming","startDate":"2024-09-30","conditions":["Anal Cancer"],"enrollment":23,"completionDate":"2029-04-14"},{"nctId":"NCT05980169","phase":"NA","title":"The Effect of Low Frequency Soundwave Stimulation on Chemotherapy Induced Peripheral Neuropathy","status":"ACTIVE_NOT_RECRUITING","sponsor":"Augusta University","startDate":"2023-11-29","conditions":["Gynecologic Cancer","Neuropathy;Peripheral"],"enrollment":80,"completionDate":"2029-12-01"},{"nctId":"NCT05319730","phase":"PHASE1,PHASE2","title":"A Study to Evaluate Investigational Agents With or Without Pembrolizumab (MK-3475) in Participants With Advanced Esophageal Cancer Previously Exposed to Programmed Cell Death 1 Protein (PD-1)/ Programmed Cell Death Ligand 1 (PD-L1) Treatment (MK-3475-06B)","status":"RECRUITING","sponsor":"Merck Sharp & Dohme LLC","startDate":"2023-05-16","conditions":["Esophageal Squamous Cell Carcinoma"],"enrollment":230,"completionDate":"2029-04-10"},{"nctId":"NCT05700461","phase":"PHASE1","title":"Drug Screening Using Novel IMD in Renal Cell Carcinoma","status":"ENROLLING_BY_INVITATION","sponsor":"Oliver Jonas","startDate":"2024-12-01","conditions":["Renal Cell Carcinoma","Metastatic Renal Cell Carcinoma","Kidney Cancer"],"enrollment":20,"completionDate":"2029-08-31"},{"nctId":"NCT06831955","phase":"PHASE2","title":"LifEStyle Intervention to Enhance Efficacy of Neoadjuvant Therapy in Patients With Triple Negative Breast Cancer","status":"RECRUITING","sponsor":"Universitaire Ziekenhuizen KU Leuven","startDate":"2026-02-01","conditions":["Triple Negative Breast Cancer (TNBC), Early Setting"],"enrollment":356,"completionDate":"2031-09-01"},{"nctId":"NCT07481058","phase":"PHASE2","title":"KC1036 in Combination With PD-1 Antibody and Platinum-based Chemotherapy for First-line Advanced Esophageal Cancer","status":"RECRUITING","sponsor":"Beijing Konruns Pharmaceutical Co., Ltd.","startDate":"2025-12-12","conditions":["Esophageal Squamous Cell Carcinoma (ESCC)"],"enrollment":60,"completionDate":"2028-12"},{"nctId":"NCT07216703","phase":"PHASE3","title":"A Clinical Study of Sacituzumab Tirumotecan (MK-2870) in Combination With Pembrolizumab (MK-3475) as First-line Maintenance Treatment of Cervical Cancer (MK-2870-036/TroFuse-036/GOG-3123/ENGOT-cx22)","status":"RECRUITING","sponsor":"Merck Sharp & Dohme LLC","startDate":"2026-01-19","conditions":["Cervical Cancer"],"enrollment":1023,"completionDate":"2031-10-29"},{"nctId":"NCT05143970","phase":"PHASE1","title":"A Phase 1 First-In-Human Study of the Anti-CD73 IPH5301 Alone or in Combination With Chemotherapy and Trastuzumab in Patients With Advanced Solid Tumors","status":"RECRUITING","sponsor":"Institut Paoli-Calmettes","startDate":"2022-01-21","conditions":["Metastatic Cancer","Metastatic Breast Cancer","Metastatic Pancreatic Cancer","Metastatic Gastric Cancer","Metastatic Lung Cancer","Metastatic Ovary Cancer","Oesophageal Cancer","Endometrial Cancer","Advanced Solid Tumor"],"enrollment":27,"completionDate":"2027-03"},{"nctId":"NCT05039801","phase":"PHASE1","title":"IACS-6274 With or Without Bevacizumab and Paclitaxel for the Treatment of Advanced Solid Tumors","status":"RECRUITING","sponsor":"M.D. Anderson Cancer Center","startDate":"2021-09-09","conditions":["Advanced Endometrial Carcinoma","Advanced Head and Neck Squamous Cell Carcinoma","Advanced Malignant Solid Neoplasm","Advanced Melanoma","Advanced Ovarian Clear Cell Adenocarcinoma","Chondrosarcoma","Clinical Stage III Cutaneous Melanoma AJCC v8","Clinical Stage IV Cutaneous Melanoma AJCC v8","Pathologic Stage III Cutaneous Melanoma AJCC v8","Pathologic Stage IIIA Cutaneous Melanoma AJCC v8","Pathologic Stage IIIB Cutaneous Melanoma AJCC v8","Pathologic Stage IIIC Cutaneous Melanoma AJCC v8","Pathologic Stage IIID Cutaneous Melanoma AJCC v8","Pathologic Stage IV Cutaneous Melanoma AJCC v8","Recurrent Ovarian High Grade Serous Adenocarcinoma","Refractory Endometrial Carcinoma","Refractory Head and Neck Squamous Cell Carcinoma","Refractory Melanoma","Refractory Ovarian Clear Cell Adenocarcinoma","Refractory Ovarian High Grade Serous Adenocarcinoma","Stage III Ovarian Cancer AJCC v8","Stage III Uterine Corpus Cancer AJCC v8","Stage IIIA Ovarian Cancer AJCC v8","Stage IIIA Uterine Corpus Cancer AJCC v8","Stage IIIA1 Ovarian Cancer AJCC v8","Stage IIIA2 Ovarian Cancer AJCC v8","Stage IIIB Ovarian Cancer AJCC v8","Stage IIIB Uterine Corpus Cancer AJCC v8","Stage IIIC Ovarian Cancer AJCC v8","Stage IIIC Uterine Corpus Cancer AJCC v8","Stage IIIC1 Uterine Corpus Cancer AJCC v8","Stage IIIC2 Uterine Corpus Cancer AJCC v8","Stage IV Ovarian Cancer AJCC v8","Stage IV Uterine Corpus Cancer AJCC v8","Stage IVA Ovarian Cancer AJCC v8","Stage IVA Uterine Corpus Cancer AJCC v8","Stage IVB Ovarian Cancer AJCC v8","Stage IVB Uterine Corpus Cancer AJCC v8"],"enrollment":54,"completionDate":"2026-05-29"}],"_emaApprovals":[{"date":"2019-05-10","status":"Authorised","company":"TEVA BV"}],"genericFilers":[],"latestUpdates":[],"manufacturing":[],"administration":{"route":"Intravenous","formulation":"Injection","formulations":[{"form":"INJECTION","route":"INTRAVENOUS","productName":"Paclitaxel"},{"form":"INJECTION","route":"INTRAVENOUS","productName":"Paclitaxel"},{"form":"INJECTION, POWDER, LYOPHILIZED, FOR SUSPENSION","route":"INTRAVENOUS","productName":"ABRAXANE"},{"form":"INJECTION, POWDER, LYOPHILIZED, FOR SUSPENSION","route":"INTRAVENOUS","productName":"Paclitaxel"},{"form":"INJECTION, POWDER, LYOPHILIZED, FOR SUSPENSION","route":"INTRAVENOUS","productName":"Paclitaxel Protein-Bound Particles for Injectable Suspension (Albumin-Bound)"},{"form":"INJECTION, POWDER, LYOPHILIZED, FOR SUSPENSION","route":"INTRAVENOUS","productName":"Paclitaxel protein-bound particles for injectable suspension (albumin-bound)"},{"form":"INJECTION, SOLUTION","route":"INTRAVENOUS","productName":"PACLITAXELPACLITAXEL"},{"form":"INJECTION, SOLUTION","route":"INTRAVENOUS","productName":"Paclitaxel"},{"form":"INJECTION, SOLUTION, CONCENTRATE","route":"INTRAVENOUS","productName":"Paclitaxel"}]},"_patentsChecked":true,"crossReferences":{"NUI":"N0000148314","MMSL":"2296","NDDF":"004116","UNII":"P88XT4IS4D","VUID":"4020736","CHEBI":"CHEBI:45863","VANDF":"4020736","INN_ID":"7052","RXNORM":"196466","UMLSCUI":"C0144576","chemblId":"CHEMBL428647","ChEMBL_ID":"CHEMBL428647","KEGG_DRUG":"D00491","DRUGBANK_ID":"DB01229","PDB_CHEM_ID":" TA1","PUBCHEM_CID":"36314","SNOMEDCT_US":"387374002","IUPHAR_LIGAND_ID":"2770","MESH_DESCRIPTOR_UI":"D017239"},"formularyStatus":[],"_enricherVersion":"v2","_offLabelChecked":true,"developmentCodes":[],"ownershipHistory":[{"period":"1992-","companyName":"Hq Spclt Pharma","relationship":"Original Developer"},{"period":"2019","companyName":"Teva Bv","relationship":"EMA Licensee"},{"period":"2019","companyName":"Taiho Pharmaceutical Co., Ltd.","relationship":"PMDA Licensee"}],"pharmacokinetics":{"source":"DrugCentral","halfLife":"11.0 hours","clearance":"6.4 mL/min/kg","bioavailability":"6%","fractionUnbound":"0.12%","volumeOfDistribution":"3.0 L/kg"},"publicationCount":42607,"therapeuticAreas":["Oncology"],"_revenueScrapedAt":"2026-04-01 10:47:02.229477+00","atcClassification":{"source":"DrugCentral","atcCode":"L01CD01","allCodes":["L01CD01","L01CD51"]},"biosimilarFilings":[],"originalDeveloper":"Hq Spclt Pharma","recentPublications":[{"date":"2026 Mar 2","pmid":"41903690","title":"Envafolimab combined with chemotherapy in advanced thymic carcinoma - first clinical experience with a novel subcutaneous programmed death-ligand 1 inhibitor.","journal":"Anti-cancer drugs"},{"date":"2026 Mar 26","pmid":"41903689","title":"Poly(d,l-lactide-co-glycolide) (PLGA) nanoparticles in oncological therapeutics: Mechanisms of targeted delivery and encapsulation strategies for chemotherapeutics, gene modulators, and phytochemicals.","journal":"Nanomedicine : nanotechnology, biology, and medicine"},{"date":"2026 Mar 22","pmid":"41903398","title":"Honeysuckle-derived vesicle-like nanoparticle and their hybrid vesicle as novel drug delivery systems for glioma therapy.","journal":"Colloids and surfaces. B, Biointerfaces"},{"date":"2026 Mar 2","pmid":"41903397","title":"A semimechanistic PK/PD model-informed Taxus tablets' development: Accelerating early clinical translation of a taxane-based antitumor agent.","journal":"Drug metabolism and disposition: the biological fate of chemicals"},{"date":"2026 Mar 28","pmid":"41902997","title":"The logarithmic phase as a therapeutic direction: evaluating pharmacological strategies against cancer progression.","journal":"Clinical & translational oncology : official publication of the Federation of Spanish Oncology Societies and of the National Cancer Institute of Mexico"}],"companionDiagnostics":[],"genericManufacturers":18,"_genericFilersChecked":true,"genericManufacturerList":["Accord Hlthcare","Actavis Totowa","Alembic","Cipla","Dash Pharms","Fresenius Kabi Usa","Gland","Hengrui Pharma","Hikma","Hospira","Msn","Mylan","Pharmobedient","Pliva Lachema","Sandoz","Shuangcheng","Teva Pharms","Teva Pharms Usa"],"status":"approved","companyName":"Hq Spclt Pharma","companyId":"pfizer","modality":"Small Molecule","firstApprovalDate":"1992","enrichmentLevel":4,"visitCount":3,"regulatoryByCountry":[{"country_code":"US","regulator":"FDA","status":"approved","approval_date":"2015-07-21T00:00:00.000Z","mah":"BRISTOL-MYERS","brand_name_local":null,"application_number":"NDA021660"},{"country_code":"US","regulator":"FDA","status":"approved","approval_date":"2016-08-23T00:00:00.000Z","mah":"GLAND","brand_name_local":null,"application_number":"ANDA207326"},{"country_code":"US","regulator":"FDA","status":"approved","approval_date":"2022-07-27T00:00:00.000Z","mah":"AM REGENT","brand_name_local":null,"application_number":"NDA211875"},{"country_code":"US","regulator":"FDA","status":"approved","approval_date":"2023-05-11T00:00:00.000Z","mah":"TEVA PHARMS INC","brand_name_local":null,"application_number":"NDA216338"},{"country_code":"US","regulator":"FDA","status":"approved","approval_date":"2025-05-15T00:00:00.000Z","mah":"SHUANGCHENG","brand_name_local":null,"application_number":"ANDA216355"},{"country_code":"IL","regulator":"MOH","status":"likely_approved","approval_date":null,"mah":null,"brand_name_local":null,"application_number":null},{"country_code":"IL","regulator":"MOH","status":"likely_approved","approval_date":null,"mah":null,"brand_name_local":null,"application_number":null},{"country_code":"IL","regulator":"MOH","status":"likely_approved","approval_date":null,"mah":null,"brand_name_local":null,"application_number":null},{"country_code":"SG","regulator":"HSA","status":"likely_approved","approval_date":null,"mah":null,"brand_name_local":null,"application_number":null},{"country_code":"SG","regulator":"HSA","status":"likely_approved","approval_date":null,"mah":null,"brand_name_local":null,"application_number":null},{"country_code":"SG","regulator":"HSA","status":"likely_approved","approval_date":null,"mah":null,"brand_name_local":null,"application_number":null},{"country_code":"SG","regulator":"HSA","status":"likely_approved","approval_date":null,"mah":null,"brand_name_local":null,"application_number":null},{"country_code":"SG","regulator":"HSA","status":"likely_approved","approval_date":null,"mah":null,"brand_name_local":null,"application_number":null},{"country_code":"AE","regulator":"MOH","status":"likely_approved","approval_date":null,"mah":null,"brand_name_local":null,"application_number":null},{"country_code":"AE","regulator":"MOH","status":"likely_approved","approval_date":null,"mah":null,"brand_name_local":null,"application_number":null},{"country_code":"AE","regulator":"MOH","status":"likely_approved","approval_date":null,"mah":null,"brand_name_local":null,"application_number":null},{"country_code":"AE","regulator":"MOH","status":"likely_approved","approval_date":null,"mah":null,"brand_name_local":null,"application_number":null},{"country_code":"AE","regulator":"MOH","status":"likely_approved","approval_date":null,"mah":null,"brand_name_local":null,"application_number":null},{"country_code":"KR","regulator":"MFDS","status":"likely_approved","approval_date":null,"mah":null,"brand_name_local":null,"application_number":null},{"country_code":"KR","regulator":"MFDS","status":"likely_approved","approval_date":null,"mah":null,"brand_name_local":null,"application_number":null},{"country_code":"KR","regulator":"MFDS","status":"likely_approved","approval_date":null,"mah":null,"brand_name_local":null,"application_number":null},{"country_code":"KR","regulator":"MFDS","status":"likely_approved","approval_date":null,"mah":null,"brand_name_local":null,"application_number":null},{"country_code":"KR","regulator":"MFDS","status":"likely_approved","approval_date":null,"mah":null,"brand_name_local":null,"application_number":null},{"country_code":"AU","regulator":"TGA","status":"likely_approved","approval_date":null,"mah":null,"brand_name_local":null,"application_number":null},{"country_code":"AU","regulator":"TGA","status":"likely_approved","approval_date":null,"mah":null,"brand_name_local":null,"application_number":null},{"country_code":"AU","regulator":"TGA","status":"likely_approved","approval_date":null,"mah":null,"brand_name_local":null,"application_number":null},{"country_code":"AU","regulator":"TGA","status":"likely_approved","approval_date":null,"mah":null,"brand_name_local":null,"application_number":null},{"country_code":"AU","regulator":"TGA","status":"likely_approved","approval_date":null,"mah":null,"brand_name_local":null,"application_number":null},{"country_code":"GB","regulator":"MHRA","status":"likely_approved","approval_date":null,"mah":null,"brand_name_local":null,"application_number":null},{"country_code":"GB","regulator":"MHRA","status":"likely_approved","approval_date":null,"mah":null,"brand_name_local":null,"application_number":null},{"country_code":"GB","regulator":"MHRA","status":"likely_approved","approval_date":null,"mah":null,"brand_name_local":null,"application_number":null},{"country_code":"GB","regulator":"MHRA","status":"likely_approved","approval_date":null,"mah":null,"brand_name_local":null,"application_number":null},{"country_code":"GB","regulator":"MHRA","status":"likely_approved","approval_date":null,"mah":null,"brand_name_local":null,"application_number":null},{"country_code":"CA","regulator":"Health Canada","status":"approved","approval_date":null,"mah":"","brand_name_local":"","application_number":""},{"country_code":"EU","regulator":"EMA","status":"pending","approval_date":null,"mah":"","brand_name_local":"","application_number":""},{"country_code":"IL","regulator":"MOH","status":"likely_approved","approval_date":null,"mah":null,"brand_name_local":null,"application_number":null},{"country_code":"IL","regulator":"MOH","status":"likely_approved","approval_date":null,"mah":null,"brand_name_local":null,"application_number":null}],"patentsNormalised":[{"patent_number":"8268348","territory":"US","patent_type":"Method of Use","expiry_date":"2026-02-21T00:00:00.000Z","status":"active","paragraph_iv_filed":false},{"patent_number":"9101543","territory":"US","patent_type":"Method of Use","expiry_date":"2026-02-21T00:00:00.000Z","status":"active","paragraph_iv_filed":false},{"patent_number":"7758891","territory":"US","patent_type":"Method of Use","expiry_date":"2026-02-21T00:00:00.000Z","status":"active","paragraph_iv_filed":false},{"patent_number":"8034375","territory":"US","patent_type":"Method of Use","expiry_date":"2026-08-13T00:00:00.000Z","status":"active","paragraph_iv_filed":false},{"patent_number":"8268348*PED","territory":"US","patent_type":"Compound","expiry_date":"2026-08-21T00:00:00.000Z","status":"active","paragraph_iv_filed":false},{"patent_number":"9101543*PED","territory":"US","patent_type":"Compound","expiry_date":"2026-08-21T00:00:00.000Z","status":"active","paragraph_iv_filed":false},{"patent_number":"7758891*PED","territory":"US","patent_type":"Compound","expiry_date":"2026-08-21T00:00:00.000Z","status":"active","paragraph_iv_filed":false},{"patent_number":"8034375*PED","territory":"US","patent_type":"Compound","expiry_date":"2027-02-13T00:00:00.000Z","status":"active","paragraph_iv_filed":false},{"patent_number":"9597409","territory":"US","patent_type":"Method of Use","expiry_date":"2032-03-04T00:00:00.000Z","status":"active","paragraph_iv_filed":false},{"patent_number":"9393318","territory":"US","patent_type":"Method of Use","expiry_date":"2032-03-04T00:00:00.000Z","status":"active","paragraph_iv_filed":false},{"patent_number":"9393318*PED","territory":"US","patent_type":"Compound","expiry_date":"2032-09-04T00:00:00.000Z","status":"active","paragraph_iv_filed":false},{"patent_number":"9597409*PED","territory":"US","patent_type":"Compound","expiry_date":"2032-09-04T00:00:00.000Z","status":"active","paragraph_iv_filed":false},{"patent_number":"9511046","territory":"US","patent_type":"Method of Use","expiry_date":"2034-01-12T00:00:00.000Z","status":"active","paragraph_iv_filed":false},{"patent_number":"9511046*PED","territory":"US","patent_type":"Compound","expiry_date":"2034-07-12T00:00:00.000Z","status":"active","paragraph_iv_filed":false}],"trialStats":{"total":95,"withResults":49},"validation":{"fieldsValidated":0,"lastValidatedAt":"2026-04-19T23:53:01.312122+00:00","fieldsConflicting":14,"overallConfidence":0.8},"verificationStatus":"verified","dataCompleteness":{"mechanism":false,"indications":true,"safety":true,"trials":true,"score":3}}