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Activation of Human VPS4A by ESCRT-III Proteins Reveals Ability of Substrates to Relieve Enzyme Autoinhibition.

J Biol Chem.. 2010-11;  285(46):35428 - 35438
Samuel A. Merrill and Phyllis I. Hanson. Department of Cell Biology and Physiology, Washington University School of Medicine, St Louis, Missouri 63110, USA.
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摘要

VPS4 proteins are AAA(+) ATPases required to form multivesicular bodies, release viral particles, and complete cytokinesis. They act by disassembling ESCRT-III heteropolymers during or after their proposed function in membrane scission. Here we show that purified human VPS4A is essentially inactive but can be stimulated to hydrolyze ATP by ESCRT-III proteins in a reaction that requires both their previously defined MIT interacting motifs and 50 amino acids of the adjacent sequence. Importantly, C-terminal fragments of all ESCRT-III proteins tested, including CHMP2A, CHMP1B, CHMP3, CHMP4A, CHMP6, and CHMP5, activated VPS4A suggesting that it disassembles ESCRT-III heteropolymers by affecting each component prote... More

关键词

ATPases; Endosomes; Enzyme Mechanisms; Membrane Trafficking; Protein-Protein Interactions; AAA+ ATPases; ESCRT Machinery; Multivesicular Body