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内质网系留与COP-I囊泡脱衣之间的联系。

A link between ER tethering and COP-I vesicle uncoating.

作者信息

Zink Sabrina, Wenzel Dirk, Wurm Christian A, Schmitt Hans Dieter

机构信息

Department Neurobiology, Max Planck Institute for Biophysical Chemistry, Göttingen, D37077, Germany.

出版信息

Dev Cell. 2009 Sep;17(3):403-16. doi: 10.1016/j.devcel.2009.07.012.

Abstract

The yeast Dsl1p vesicle tethering complex, comprising the three subunits Dsl1p, Dsl3p, and Tip20p, is stably associated with three endoplasmic reticulum-localized Q-SNAREs and is believed to play a central role in the tethering and fusion of Golgi-derived COP-I transport vesicles. Dsl1p also interacts directly with COP-I subunits. We now show that binding of Dsl1p to COP-I subunits involves binding sites identical to those involved in interactions between COP-I subunits that stabilize the COP-I coat. Cells with defects in Dsl/SNARE complex function show massive accumulation of COP-I-coated vesicles in a cluster to which COP-II coat proteins are also recruited. Our results suggest that binding of Dsl/SNARE complex to the COP-I coat complex serves two functions: to mediate vesicle tethering and to assist the uncoating process by blocking domains in COP-I that drive repolymerization and the formation of large COP-I aggregates.

摘要

酵母Dsl1p囊泡拴系复合体由三个亚基Dsl1p、Dsl3p和Tip20p组成,与三种内质网定位的Q-SNARE稳定结合,被认为在高尔基体衍生的COP-I运输囊泡的拴系和融合中起核心作用。Dsl1p还直接与COP-I亚基相互作用。我们现在表明,Dsl1p与COP-I亚基的结合涉及与稳定COP-I衣被的COP-I亚基之间相互作用相同的结合位点。Dsl/SNARE复合体功能有缺陷的细胞中,COP-I包被囊泡大量聚集形成簇,COP-II衣被蛋白也被募集到该簇中。我们的结果表明,Dsl/SNARE复合体与COP-I衣被复合体的结合具有两个功能:介导囊泡拴系,并通过阻断COP-I中驱动再聚合和形成大的COP-I聚集体的结构域来协助去衣被过程。

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