Lipid packing sensed by ArfGAP1 couples COPI coat disassembly to membrane bilayer curvature

被引:0
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作者
Joëlle Bigay
Pierre Gounon
Sylviane Robineau
Bruno Antonny
机构
[1] Institut de Pharmacologie Moléculaire et Cellulaire,Centre Commun de Microscopie Appliquée
[2] CNRS,undefined
[3] Université de Nice,undefined
来源
Nature | 2003年 / 426卷
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摘要
Protein coats deform flat lipid membranes into buds and capture membrane proteins to form transport vesicles1,2,3. The assembly/disassembly cycle of the COPI coat on Golgi membranes is coupled to the GTP/GDP cycle of the small G protein Arf1. At the heart of this coupling is the specific interaction of membrane-bound Arf1–GTP with coatomer, a complex of seven proteins that forms the building unit of the COPI coat4,5,6,7. Although COPI coat disassembly requires the catalysis of GTP hydrolysis in Arf1 by a specific GTPase-activating protein (ArfGAP1)8,9,10, the precise timing of this reaction during COPI vesicle formation is not known. Using time-resolved assays for COPI dynamics on liposomes of controlled size, we show that the rate of ArfGAP1-catalysed GTP hydrolysis in Arf1 and the rate of COPI disassembly increase over two orders of magnitude as the curvature of the lipid bilayer increases and approaches that of a typical transport vesicle. This leads to a model for COPI dynamics in which GTP hydrolysis in Arf1 is organized temporally and spatially according to the changes in lipid packing induced by the coat.
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页码:563 / 566
页数:3
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