cyp3a介导的药物-药物相互作用潜力和brentuximab vedotin(一种抗体-药物偶联物)在cd30阳性血液恶性肿瘤患者中的排泄

IF 2.9 4区 医学 Journal of Clinical Pharmacology Pub Date : 2013-08-01 Epub Date: 2013-06-10 DOI:10.1002/jcph.116
Tae H Han, Ajay K Gopal, Radhakrishnan Ramchandren, Andre Goy, Robert Chen, Jeffrey V Matous, Maureen Cooper, Laurie E Grove, Stephen C Alley, Carmel M Lynch, Owen A O'Connor
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引用次数: 59

摘要

Brentuximab vedotin是一种抗体-药物偶联物(ADC),可选择性地将单甲基auristatin E (MMAE)递送到表达cd30的细胞中。本研究评估了布伦妥昔单抗维多汀的cyp3a介导的药物相互作用潜力和MMAE的排泄。56例cd30阳性血液恶性肿瘤患者接受brentuximab vedotin(1.2或1.8 mg/kg静脉注射)两个21天周期的治疗。每位患者还接受了敏感的CYP3A底物(咪达唑仑),有效的诱导剂(利福平)或强抑制剂(酮康唑)。Brentuximab vedotin对咪达唑仑暴露没有影响。同时使用利福平或酮康唑对ADC暴露无影响;然而,MMAE暴露在利福平组较低,酮康唑组较高。本研究中brentuximab vedotin的短期安全性与历史临床观察基本一致。最常见的不良反应是恶心、疲劳、腹泻、头痛、发热和中性粒细胞减少。在1周的时间内,给予brentuximab vedotin后,约23.5%的完整MMAE被恢复;其他种均低于定量限。主要的排泄途径是通过粪便(中位数为回收MMAE的72%)。这些结果表明brentuximab vedotin (1.8 mg/kg)和MMAE既不是CYP3A的抑制剂也不是诱诱剂;然而,MMAE是CYP3A的底物。
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CYP3A-mediated drug-drug interaction potential and excretion of brentuximab vedotin, an antibody-drug conjugate, in patients with CD30-positive hematologic malignancies.

Brentuximab vedotin is an antibody-drug conjugate (ADC) that selectively delivers monomethyl auristatin E (MMAE) into CD30-expressing cells. This study evaluated the CYP3A-mediated drug-drug interaction potential of brentuximab vedotin and the excretion of MMAE. Two 21-day cycles of brentuximab vedotin (1.2 or 1.8 mg/kg intravenously) were administered to 56 patients with CD30-positive hematologic malignancies. Each patient also received either a sensitive CYP3A substrate (midazolam), an effective inducer (rifampin), or a strong inhibitor (ketoconazole). Brentuximab vedotin did not affect midazolam exposures. ADC exposures were unaffected by concomitant rifampin or ketoconazole; however, MMAE exposures were lower with rifampin and higher with ketoconazole. The short-term safety profile of brentuximab vedotin in this study was generally consistent with historic clinical observations. The most common adverse events were nausea, fatigue, diarrhea, headache, pyrexia, and neutropenia. Over a 1-week period, ∼23.5% of intact MMAE was recovered after administration of brentuximab vedotin; all other species were below the limit of quantitation. The primary excretion route is via feces (median 72% of the recovered MMAE). These results suggest that brentuximab vedotin (1.8 mg/kg) and MMAE are neither inhibitors nor inducers of CYP3A; however, MMAE is a substrate of CYP3A.

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来源期刊
Journal of Clinical Pharmacology
Journal of Clinical Pharmacology PHARMACOLOGY & PHARMACY-
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期刊介绍: The Journal of Clinical Pharmacology (JCP) is a Human Pharmacology journal designed to provide physicians, pharmacists, research scientists, regulatory scientists, drug developers and academic colleagues a forum to present research in all aspects of Clinical Pharmacology. This includes original research in pharmacokinetics, pharmacogenetics/pharmacogenomics, pharmacometrics, physiologic based pharmacokinetic modeling, drug interactions, therapeutic drug monitoring, regulatory sciences (including unique methods of data analysis), special population studies, drug development, pharmacovigilance, womens’ health, pediatric pharmacology, and pharmacodynamics. Additionally, JCP publishes review articles, commentaries and educational manuscripts. The Journal also serves as an instrument to disseminate Public Policy statements from the American College of Clinical Pharmacology.
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