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新发现的哺乳动物 NCX 的冷冻电镜结构为解析其潜在的分子机制和药物发现开辟了新的舞台。

Newly uncovered Cryo-EM structures of mammalian NCXs set a new stage for resolving the underlying molecular mechanisms and drug discovery.

机构信息

Department of Physiology and Pharmacology, Faculty of Medicine, Tel-Aviv University, Tel Aviv 69978, Israel.

出版信息

Cell Calcium. 2024 May;119:102867. doi: 10.1016/j.ceca.2024.102867. Epub 2024 Feb 27.

Abstract

The membrane-abundant NCX proteins mediate an electrogenic ion exchange (3Na:1Ca) in the Ca-exit or Ca-entry mode. The structurally related isoform/splice variants of NCX are expressed in a tissue-specific manner to shape Ca signalling/homeostasis in diverse cell types. The lack of mammalian NCX structure hampered the functional and regulatory resolution of tissue-specific NCX variants and their pharmacological targeting. Recently unveiled Cryo-EM structures of human cardiac NCX1.1[1] and kidney NCX1.3[2] provide new opportunities for resolving structure/functional divergences among NCX variants and their pharmacological targeting.

摘要

膜丰富型 NCX 蛋白以电中性离子交换(3Na:1Ca)的方式介导钙外排或钙内流模式。NCX 的结构相关同工型/剪接变体以组织特异性方式表达,以塑造不同细胞类型的钙信号转导/稳态。哺乳动物 NCX 结构的缺失阻碍了组织特异性 NCX 变体的功能和调节解析及其药理学靶向。最近公布的人类心脏 NCX1.1[1]和肾脏 NCX1.3[2]的冷冻电镜结构为解析 NCX 变体之间的结构/功能差异及其药理学靶向提供了新的机会。

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