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平衡核苷转运蛋白功能及抑制剂设计的研究进展。

Current Progress on Equilibrative Nucleoside Transporter Function and Inhibitor Design.

机构信息

Institute of Biotechnology, University of Helsinki, Helsinki, Finland.

HiLIFE, University of Helsinki, Helsinki, Finland.

出版信息

SLAS Discov. 2019 Dec;24(10):953-968. doi: 10.1177/2472555219870123. Epub 2019 Sep 10.

DOI:10.1177/2472555219870123
PMID:31503511
Abstract

Physiological nucleosides are used for the synthesis of DNA, RNA, and ATP in the cell and serve as universal mammalian signaling molecules that regulate physiological processes such as vasodilation and platelet aggregation by engaging with cell surface receptors. The same pathways that allow uptake of physiological nucleosides mediate the cellular import of synthetic nucleoside analogs used against cancer, HIV, and other viral diseases. Physiological nucleosides and nucleoside drugs are imported by two families of nucleoside transporters: the SLC28 concentrative nucleoside transporters (CNTs) and SLC29 equilibrative nucleoside transporters (ENTs). The four human ENT paralogs are expressed in distinct tissues, localize to different subcellular sites, and transport a variety of different molecules. Here we provide an overview of the known structure-function relationships of the ENT family with a focus on ligand binding and transport in the context of a new hENT1 homology model. We provide a generic residue numbering system for the different ENTs to facilitate the interpretation of mutational data produced using different ENT homologs. The discovery of paralog-selective small-molecule modulators is highly relevant for the design of new therapies and for uncovering the functions of poorly characterized ENT family members. Here, we discuss recent developments in the discovery of new paralog-selective small-molecule ENT inhibitors, including new natural product-inspired compounds. Recent progress in the ability to heterologously produce functional ENTs will allow us to gain insight into the structure and functions of different ENT family members as well as the rational discovery of highly selective inhibitors.

摘要

生理核苷在细胞内用于 DNA、RNA 和 ATP 的合成,并作为通用的哺乳动物信号分子,通过与细胞表面受体结合,调节血管舒张和血小板聚集等生理过程。允许摄取生理核苷的相同途径介导用于治疗癌症、HIV 和其他病毒疾病的合成核苷类似物的细胞内导入。生理核苷和核苷药物由核苷转运蛋白家族 2(SLC28)的两个家族摄取:浓缩核苷转运蛋白(CNT)和溶质载体家族 29(SLC29)平衡核苷转运蛋白(ENT)。人 ENT 四个基因家族在不同的组织中表达,定位于不同的亚细胞部位,并转运各种不同的分子。本文概述了 ENT 家族的已知结构-功能关系,重点介绍了在新的 hENT1 同源模型背景下的配体结合和转运。我们为不同的 ENT 提供了通用的残基编号系统,以方便使用不同 ENT 同源物产生的突变数据的解释。发现对 paralog 具有选择性的小分子调节剂对于设计新疗法和揭示功能较差的 ENT 家族成员的功能非常重要。本文讨论了发现新的 paralog 选择性小分子 ENT 抑制剂的最新进展,包括受新天然产物启发的化合物。能够异源产生功能性 ENT 的最新进展将使我们能够深入了解不同 ENT 家族成员的结构和功能,以及高度选择性抑制剂的合理发现。

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