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抗体药物偶联物治疗癌症的药代动力学考虑因素。

Pharmacokinetic Considerations for Antibody-Drug Conjugates against Cancer.

机构信息

School of Pharmacy, University of Waterloo, 10A Victoria St South, Kitchener, Ontario, N2G 1C5, Canada.

DMPK & Translational Modeling, Abbvie Inc., North Chicago, Illinois, 60064, USA.

出版信息

Pharm Res. 2017 Dec;34(12):2579-2595. doi: 10.1007/s11095-017-2259-3. Epub 2017 Sep 18.

Abstract

Antibody-drug conjugates (ADCs) are ushering in the next era of targeted therapy against cancer. An ADC for cancer therapy consists of a potent cytotoxic payload that is attached to a tumour-targeted antibody by a chemical linker, usually with an average drug-to-antibody ratio (DAR) of 3.5-4. The theory is to deliver potent cytotoxic payloads directly to tumour cells while sparing healthy cells. However, practical application has proven to be more difficult. At present there are only two ADCs approved for clinical use. Nevertheless, in the last decade there has been an explosion of options for ADC engineering to optimize target selection, Fc receptor interactions, linker, payload and more. Evaluation of these strategies requires an understanding of the mechanistic underpinnings of ADC pharmacokinetics. Development of ADCs for use in cancer further requires an understanding of tumour properties and kinetics within the tumour environment, and how the presence of cancer as a disease will impact distribution and elimination. Key pharmacokinetic considerations for the successful design and clinical application of ADCs in oncology are explored in this review, with a focus on the mechanistic determinants of distribution and elimination.

摘要

抗体药物偶联物 (ADCs) 正在开启癌症靶向治疗的新时代。用于癌症治疗的 ADC 由一个有效的细胞毒性有效载荷组成,通过化学连接子与肿瘤靶向抗体连接,通常平均药物抗体比 (DAR) 为 3.5-4。理论上是将有效的细胞毒性有效载荷直接递送到肿瘤细胞,同时保护健康细胞。然而,实际应用证明更加困难。目前只有两种 ADC 获准用于临床使用。尽管如此,在过去十年中,ADC 工程在优化目标选择、Fc 受体相互作用、连接子、有效载荷等方面有了爆炸式的选择。评估这些策略需要了解 ADC 药代动力学的机制基础。为了在癌症中使用 ADC 进行开发,还需要了解肿瘤特性和肿瘤微环境中的动力学,以及癌症作为一种疾病的存在将如何影响分布和消除。本文综述了 ADC 在肿瘤学中的成功设计和临床应用的关键药代动力学考虑因素,重点探讨了分布和消除的机制决定因素。

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