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小分子调节因子,重大影响——内体-内质网界面处的钙离子和胆固醇

Small regulators, major consequences - Ca²⁺ and cholesterol at the endosome-ER interface.

作者信息

van der Kant Rik, Neefjes Jacques

机构信息

Department of Cellular and Molecular Medicine, University of California, San Diego, La Jolla, CA 92093, USA.

出版信息

J Cell Sci. 2014 Mar 1;127(Pt 5):929-38. doi: 10.1242/jcs.137539. Epub 2014 Feb 19.

Abstract

The ER is the largest cellular compartment and a major storage site for lipids and ions. In recent years, much attention has focused on contacts between the ER and other organelles, and one particularly intimate relationship is that between the ER and the endosomal system. ER-endosome contacts intensify when endosomes mature, and the ER participates in endosomal processes, such as the termination of surface receptor signaling, multi-vesicular body formation, and transport and fusion events. Cholesterol and Ca(2+) are transferred between the ER and endosomes, possibly acting as messengers for ER-endosome crosstalk. Here, we summarize different types of ER-endosomal communication and discuss membrane contact sites that might facilitate this crosstalk. We review the protein pairs that interact at the ER-endosome interface and find that many of these have a role in cholesterol exchange. We also summarize Ca(2+) exchange between the ER and endosomes, and hypothesize that ER-endosome contacts integrate several cellular functions to guide endosomal maturation. We post the hypothesis that failure in ER-endosome contacts is an unrecognized but important contributor to diseases, such as Niemann-Pick type C disease, Alzheimer's disease and amyotrophic lateral sclerosis.

摘要

内质网是最大的细胞区室,也是脂质和离子的主要储存位点。近年来,人们将大量注意力集中在内质网与其他细胞器之间的接触上,其中内质网与内体系统之间的关系尤为密切。当内体成熟时,内质网与内体的接触会增强,内质网参与内体过程,如表面受体信号传导的终止、多囊泡体的形成以及运输和融合事件。胆固醇和Ca(2+)在内质网和内体之间转移,可能作为内质网与内体相互作用的信使。在此,我们总结了内质网与内体之间不同类型的通讯,并讨论了可能促进这种相互作用的膜接触位点。我们回顾了在内质网与内体界面相互作用的蛋白对,发现其中许多在胆固醇交换中发挥作用。我们还总结了内质网与内体之间的Ca(2+)交换,并推测内质网与内体的接触整合了多种细胞功能以指导内体成熟。我们提出假说,内质网与内体接触的失败是尼曼-匹克C型病、阿尔茨海默病和肌萎缩侧索硬化症等疾病中一个未被认识但重要的致病因素。

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