Ligand-induced genetic degradation as a tool for target validation

Q1 Pharmacology, Toxicology and Pharmaceutics

Drug Discovery Today: Technologies Pub Date : 2019-04-01 DOI:10.1016/j.ddtec.2018.11.001

Aisha Yesbolatova , Yusuke Tominari , Masato T. Kanemaki

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引用次数: 23

Abstract

Targeted protein degraders, known as proteolysis targeting chimeras (PROTACs), are drawing more attention as next-generation drugs to target currently undruggable proteins. As drug discovery of functional degraders involves time- and cost-consuming laborious processes, we propose employing a ligand-induced genetic degradation system to validate candidate proteins before degrader development. Genetic degradation mimics degrader treatment by depleting a degron-fused protein in the presence of a defined ligand. All genetic systems use a combination of a degron and defined ligand that enables a protein of interest fused with the degron to be recruited to an E3 ubiquitin ligase for ubiquitylation and subsequent degradation by the proteasome. However, these events are based on different principles and have different features. We review the dTAG, HaloTag-based, auxin-inducible degron (AID), and destabilizing domain (DD) systems and discuss a strategy for degrader discovery against novel target proteins.

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配体诱导的遗传降解作为靶标验证的工具

靶向蛋白质降解剂，即蛋白质水解靶向嵌合体(proteolysis targeting chimeras, PROTACs)，作为靶向目前无法治疗的蛋白质的下一代药物，正受到越来越多的关注。由于功能降解物的药物发现涉及时间和成本的费力过程，我们建议在降解物开发之前采用配体诱导的遗传降解系统来验证候选蛋白质。遗传降解通过在确定配体存在的情况下耗尽降解融合蛋白来模拟降解处理。所有的遗传系统都使用degron和定义配体的组合，使与degron融合的感兴趣的蛋白质被招募到E3泛素连接酶上进行泛素化，随后被蛋白酶体降解。然而，这些事件基于不同的原则，具有不同的特点。我们回顾了dTAG、基于halotag、生长素诱导降解(AID)和不稳定结构域(DD)系统，并讨论了针对新靶蛋白的降解物发现策略。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Drug Discovery Today: Technologies Pharmacology, Toxicology and Pharmaceutics-Drug Discovery

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期刊介绍： Discovery Today: Technologies compares different technological tools and techniques used from the discovery of new drug targets through to the launch of new medicines.