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抗CD70抗体药物偶联物BMS-936561在临床前动物物种中的药代动力学特征及其在人体内药代动力学的预测

Pharmacokinetic characterization of BMS-936561, an anti-CD70 antibody-drug conjugate, in preclinical animal species and prediction of its pharmacokinetics in humans.

作者信息

Wang Haiqing, Rangan Vangipuram S, Sung Mei-Chen, Passmore David, Kempe Thomas, Wang Xiaoli, Thevanayagam Lourdes, Pan Chin, Rao Chetana, Srinivasan Mohan, Zhang Qian, Gangwar Sanjeev, Deshpande Shrikant, Cardarelli Pina, Marathe Punit, Yang Zheng

机构信息

Metabolism and Pharmacokinetics, Bristol-Myers Squibb, Princeton, NJ, United States.

Biologics Discovery California, Bristol-Myers Squibb, Redwood City, CA, United States.

出版信息

Biopharm Drug Dispos. 2016 Mar;37(2):93-106. doi: 10.1002/bdd.1953. Epub 2015 May 15.

Abstract

CD70 is a tumor necrosis factor (TNF)-like type II integral membrane protein that is transiently expressed on activated T- and B-lymphocytes. Aberrant expression of CD70 was identified in both solid tumors and haematologic malignancies. BMS-936561 (αCD70_MED-A) is an antibody-drug conjugate composed of a fully human anti-CD70 monoclonal antibody (αCD70) conjugated with a duocarmycin derivative, MED-A, through a maleimide-containing citrulline-valine dipeptide linker. MED-A is a carbamate prodrug that is activated by carboxylesterase to its active form, MED-B, to exert its DNA alkylation activity. In vitro serum stability studies suggested the efficiencies of hydrolyzing the carbamate-protecting group in αCD70_MED-A followed a rank order of mouse>rat > >monkey>dog~human. Pharmacokinetics of αCD70_MED-A was evaluated in mice, monkeys, and dogs after single intravenous doses. In mice, αCD70_MED-A was cleared rapidly, with no detectable exposures after 15 min following dosing. In contrast, αCD70_MED-A was much more stable in monkeys and dogs. The clearance of αCD70_MED-A in monkeys was 58 mL/d/kg, ~2-fold faster than that in dogs (31 mL/d/kg). The human PK profiles of the total αCD70 and αCD70_MED-A were predicted using allometrically scaled monkeys PK parameters of αCD70 and the carbamate hydrolysis rate constant estimated in dogs. Comparing the predicted and observed human PK from the phase I study, the dose-normalized concentration-time profiles of αCD70_MED-A and the total αCD70 were largely within the 5(th)-95(th) percentile of the predicted profiles.

摘要

CD70是一种肿瘤坏死因子(TNF)样的II型整合膜蛋白,在活化的T淋巴细胞和B淋巴细胞上短暂表达。在实体瘤和血液系统恶性肿瘤中均发现了CD70的异常表达。BMS-936561(αCD70_MED-A)是一种抗体药物偶联物,由完全人源化的抗CD70单克隆抗体(αCD70)与一种多卡霉素衍生物MED-A通过含马来酰亚胺的瓜氨酸-缬氨酸二肽连接子偶联而成。MED-A是一种氨基甲酸酯前药,可被羧酸酯酶激活为其活性形式MED-B,以发挥其DNA烷基化活性。体外血清稳定性研究表明,αCD70_MED-A中氨基甲酸酯保护基团的水解效率排序为小鼠>大鼠>>猴子>狗~人类。单次静脉给药后,在小鼠、猴子和狗中评估了αCD70_MED-A的药代动力学。在小鼠中,αCD70_MED-A清除迅速,给药后15分钟后无可检测到的暴露量。相比之下,αCD70_MED-A在猴子和狗中更稳定。αCD70_MED-A在猴子中的清除率为58 mL/d/kg,比狗(31 mL/d/kg)快约2倍。使用按比例缩放的猴子αCD70药代动力学参数和在狗中估计的氨基甲酸酯水解速率常数预测了总αCD70和αCD70_MED-A的人体药代动力学概况。将I期研究中预测的和观察到的人体药代动力学进行比较,αCD70_MED-A和总αCD70的剂量归一化浓度-时间曲线在预测曲线的第5-95百分位数范围内。

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