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ERMES-mediated ER-mitochondria contacts: molecular hubs for the regulation of mitochondrial biology.

机译:ERMES介导的ER线粒体接触:调节线粒体生物学的分子中心。

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摘要

Organelles are separate yet interdependent units of eukaryotic cells. They provide an appropriate milieu for the catalysis of many biochemical reactions, and they must establish physical links to communicate and exchange metabolites throughout the cell. Interorganelle communication is an important, yet still poorly understood, aspect of cell biology. We recently identified a protein complex that we refer to as ERMES [endoplasmic reticulum (ER)-mitochondria encounter structure], the main function of which is to provide a tethering force between the ER and the mitochondria. This complex, composed of both ER and mitochondrial transmembrane proteins, is located at the interface of the two organelles and serves to zipper them together. Previous work had implicated several ERMES components in many different physiological processes. The identification of ERMES as an interorganelle tether allows us to re-examine the amply documented phenotypic consequences of the loss of this complex in the light of this new function, thus providing a unique opportunity to assess the physiological relevance of ER-mitochondria junctions. These phenotypes hint at a broad role for ER-mitochondria connections in regulating mitochondrial and cell physiology. In this Hypothesis, we speculate on the potential role of ER-mitochondria connections as hubs in regulating several aspects of mitochondrial biology, including the regulation of mitochondrial membrane biosynthesis, genome replication, Ca(2+) signaling and protein import. Finally, we discuss how cells might use ER-mitochondria communication to fine-tune these processes according to their metabolic needs.
机译:细胞器是真核细胞的独立但相互依存的单元。它们为许多生化反应的催化提供了合适的环境,并且它们必须建立物理联系以在整个细胞内交流和交换代谢产物。细胞间通讯是细胞生物学的重要方面,但仍为人所知。我们最近发现了一种蛋白质复合物,我们称为ERMES [内质网(ER)-线粒体遭遇结构],其主要功能是在ER与线粒体之间提供束缚力。该复合物由ER和线粒体跨膜蛋白组成,位于两个细胞器的界面,可将它们拉链在一起。先前的工作涉及许多不同生理过程中的几种ERMES成分。将ERMES鉴定为细胞器间的系绳,使我们能够根据这一新功能重新检查这种复合物丢失的充分记录的表型后果,从而为评估ER-线粒体连接的生理相关性提供了独特的机会。这些表型暗示ER-线粒体连接在调节线粒体和细胞生理中的广泛作用。在此假设中,我们推测ER-线粒体连接作为调节线粒体生物学若干方面的枢纽的潜在作用,包括调节线粒体膜生物合成,基因组复制,Ca(2+)信号传导和蛋白质导入。最后,我们讨论细胞如何根据其代谢需要使用ER-线粒体通讯来微调这些过程。

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