Laboratoire Physico Chimie Curie, Institut Curie, PSL Research University, CNRS UMR168, Paris, France.
Sorbonne Université, Paris, France.
Nat Commun. 2021 Jun 8;12(1):3459. doi: 10.1038/s41467-021-23799-1.
Membrane contact sites (MCS) are subcellular regions where two organelles appose their membranes to exchange small molecules, including lipids. Structural information on how proteins form MCS is scarce. We designed an in vitro MCS with two membranes and a pair of tethering proteins suitable for cryo-tomography analysis. It includes VAP-A, an ER transmembrane protein interacting with a myriad of cytosolic proteins, and oxysterol-binding protein (OSBP), a lipid transfer protein that transports cholesterol from the ER to the trans Golgi network. We show that VAP-A is a highly flexible protein, allowing formation of MCS of variable intermembrane distance. The tethering part of OSBP contains a central, dimeric, and helical T-shape region. We propose that the molecular flexibility of VAP-A enables the recruitment of partners of different sizes within MCS of adjustable thickness, whereas the T geometry of the OSBP dimer facilitates the movement of the two lipid-transfer domains between membranes.
膜接触位点(MCS)是两个细胞器将它们的膜贴在一起以交换小分子,包括脂质的亚细胞区域。关于蛋白质如何形成 MCS 的结构信息很少。我们设计了一种具有两个膜和一对系绳蛋白的体外 MCS,适合冷冻断层分析。它包括 VAP-A,一种与无数细胞质蛋白相互作用的内质网跨膜蛋白,和 oxysterol 结合蛋白(OSBP),一种将胆固醇从内质网转运到反高尔基网络的脂质转运蛋白。我们表明,VAP-A 是一种高度灵活的蛋白质,允许形成可变的膜间距离的 MCS。OSBP 的系绳部分包含一个中央的、二聚体的和螺旋的 T 形区域。我们提出,VAP-A 的分子灵活性使得能够在可调厚度的 MCS 中招募不同大小的伙伴,而 OSBP 二聚体的 T 形几何形状则有利于两个脂质转移结构域在膜之间的移动。
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