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含微管抑制剂的抗体药物偶联物所致周围神经病变:从非临床毒理学研究到临床转化中的挑战与前景

Peripheral neuropathy with microtubule inhibitor containing antibody drug conjugates: Challenges and perspectives in translatability from nonclinical toxicology studies to the clinic.

作者信息

Stagg Nicola J, Shen Ben-Quan, Brunstein Flavia, Li Chunze, Kamath Amrita V, Zhong Fiona, Schutten Melissa, Fine Bernard M

机构信息

Safety Assessment, Genentech Inc., 1 DNA Way, South San Francisco, CA 94080, USA.

Department of Preclinical & Translational Pharmacokinetics & Pharmacodynamics, Genentech, Inc., 1 DNA Way, South San Francisco, CA 94080, USA.

出版信息

Regul Toxicol Pharmacol. 2016 Dec;82:1-13. doi: 10.1016/j.yrtph.2016.10.012. Epub 2016 Oct 20.

DOI:10.1016/j.yrtph.2016.10.012
PMID:27773754
Abstract

Antibody drug conjugates (ADC) consist of potent cytotoxic drugs conjugated to antibodies via chemical linkers, which enables specific targeting of tumor cells while reducing systemic exposure to the cytotoxic drug and improving the therapeutic window. The valine citrulline monomethyl auristatin E (vcMMAE, conventional linker-drug) ADC platform has shown promising clinical activity in several cancers, but peripheral neuropathy (PN) is a frequent adverse event leading to treatment discontinuation and dose reduction. This was not predicted based on nonclinical toxicology studies in monkeys or rats treated with vcMMAE ADCs. We evaluated four hypotheses for the lack of translatability of PN with vcMMAE ADCs: 1) species differences in exposure; 2) insensitivity of animal models; 3) species differences in target biology and other vcMMAE ADC properties in peripheral nerves and 4) increased susceptibility of patient population. The result of this hypothesis-based approach identified opportunities to improve the predictivity of PN in our animal models by increasing duration of exposure and adding an expanded neurohistopathology assessment of peripheral nerves. The utility of a predictive animal model would be to provide possible mitigation strategies in the clinic with vcMMAE ADCs and help to screen the next generation microtubule inhibitor (MTI) ADCs for reduced PN.

摘要

抗体药物偶联物(ADC)由通过化学连接子与抗体偶联的强效细胞毒性药物组成,这使得能够特异性靶向肿瘤细胞,同时减少细胞毒性药物的全身暴露并改善治疗窗口。缬氨酸瓜氨酸单甲基澳瑞他汀E(vcMMAE,传统连接子-药物)ADC平台在多种癌症中已显示出有前景的临床活性,但周围神经病变(PN)是导致治疗中断和剂量减少的常见不良事件。在用vcMMAE ADC治疗的猴子或大鼠的非临床毒理学研究中并未预测到这一点。我们评估了关于vcMMAE ADC导致PN缺乏可转化性的四个假设:1)暴露的物种差异;2)动物模型不敏感;3)周围神经中靶生物学和其他vcMMAE ADC特性的物种差异;4)患者群体易感性增加。这种基于假设的方法的结果确定了通过延长暴露时间和增加对周围神经的扩展神经组织病理学评估来提高我们动物模型中PN预测性的机会。预测性动物模型的作用将是在临床上为使用vcMMAE ADC提供可能的缓解策略,并帮助筛选下一代微管抑制剂(MTI)ADC以减少PN。

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