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毒理病理学家的抗体药物偶联物简介

A Brief Introduction to Antibody-Drug Conjugates for Toxicologic Pathologists.

作者信息

Mecklenburg Lars

机构信息

1 Covance Preclinical Services GmbH, Münster, Germany.

出版信息

Toxicol Pathol. 2018 Oct;46(7):746-752. doi: 10.1177/0192623318803059. Epub 2018 Oct 7.

Abstract

Antibody-drug conjugates (ADCs) are an emerging class of anticancer therapeutics, delivering highly cytotoxic molecules directly to cancer cells. ADCs are composed of an antibody, a small molecule drug, and a linker attaching one to another. Antibodies are directed to a large variety of antigens overexpressed on tumor cells, tumor vasculature, or tumor-supporting stroma. After internalization, the ADC is transferred to lysosomes where the cytotoxic component is released, finally killing the target cell. All ADCs are administered via intravenous injection. Once in the circulation, linker stability in plasma is of high importance. In vivo studies in animals address the release of payload over time and typically measure total antibody, conjugated ADC, and free drug. ADC development is driven by ICH (International Council for Harmonisation) guidelines S6(R1) and S9. Dose-limiting toxicities of current ADCs are mainly associated with the payload and correlate well between clinical trials and nonclinical studies in rodents and nonrodents. This mini review is intended to provide general information about ADCs in oncology and shall assist the toxicologic pathologist in correctly interpreting morphological findings acquired in toxicity studies with this entity.

摘要

抗体药物偶联物(ADCs)是一类新兴的抗癌治疗药物,可将高细胞毒性分子直接递送至癌细胞。ADCs由抗体、小分子药物以及连接两者的连接子组成。抗体可靶向肿瘤细胞、肿瘤血管或肿瘤支持基质上过度表达的多种抗原。内化后,ADCs被转运至溶酶体,在那里细胞毒性成分被释放,最终杀死靶细胞。所有ADCs均通过静脉注射给药。一旦进入循环系统,连接子在血浆中的稳定性至关重要。动物体内研究关注随时间推移的有效载荷释放情况,通常会检测总抗体、偶联的ADCs和游离药物。ADCs的研发受国际协调理事会(ICH)指南S6(R1)和S9的推动。当前ADCs的剂量限制性毒性主要与有效载荷相关,并且在啮齿动物和非啮齿动物的临床试验和非临床研究之间具有良好的相关性。本综述旨在提供有关肿瘤学中ADCs的一般信息,并协助毒理病理学家正确解释在此类实体的毒性研究中获得的形态学发现。

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