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发动蛋白的自组装刺激其GTP酶活性。

Dynamin self-assembly stimulates its GTPase activity.

作者信息

Warnock D E, Hinshaw J E, Schmid S L

机构信息

Department of Cell Biology, The Scripps Research Institute, La Jolla, California 92037, USA.

出版信息

J Biol Chem. 1996 Sep 13;271(37):22310-4. doi: 10.1074/jbc.271.37.22310.

Abstract

GTP hydrolysis by dynamin is required to drive coated vesicle budding at the plasma membrane. A diverse set of molecules including microtubules, grb2, and acidic phospholipids stimulate dynamin GTPase activity in vitro, although the physiological relevance of these effectors remains to be determined. Dynamin has been shown to assemble around microtubules, the most potent stimulatory molecule, into structures indistinguishable by electron microscopy from collars captured in vivo at the necks of endocytic coated pits. Under low ionic strength conditions purified dynamin self-assembles into rings and helical stacks of rings. Here we show that dynamin self-assembly stimulates its GTPase activity as much as 10-fold. Thus, we identify dynamin, itself, as the first effector of dynamin GTPase activity known to be physiologically relevant. Assembled dynamin's stimulated GTPase activity is not dependent on the direct interaction of high affinity GTP binding sites since a mutant defective in GTP binding and hydrolysis can coassemble with and stimulate GTP hydrolysis by wild-type dynamin. Finally, we find that GTP destabilizes assembled dynamin structures, suggesting that the activated rates of GTP hydrolysis reflect a continuing cycle of assembly, GTP hydrolysis, and disassembly.

摘要

发动蛋白水解GTP是驱动质膜上被膜小泡出芽所必需的。包括微管、生长因子受体结合蛋白2(Grb2)和酸性磷脂在内的多种分子在体外可刺激发动蛋白的GTP酶活性,不过这些效应分子的生理相关性仍有待确定。已证实发动蛋白可围绕微管(最有效的刺激分子)组装成结构,通过电子显微镜观察,这些结构与在体内内吞被膜小窝颈部捕获的环难以区分。在低离子强度条件下,纯化的发动蛋白可自组装成环以及环的螺旋堆叠。在此我们表明,发动蛋白自组装可将其GTP酶活性刺激多达10倍。因此,我们确定发动蛋白自身是已知具有生理相关性的发动蛋白GTP酶活性的首个效应分子。组装后的发动蛋白受刺激的GTP酶活性并不依赖于高亲和力GTP结合位点的直接相互作用,因为在GTP结合和水解方面存在缺陷的突变体可与野生型发动蛋白共同组装并刺激其GTP水解。最后,我们发现GTP会使组装后的发动蛋白结构不稳定,这表明GTP水解的活化速率反映了组装、GTP水解和解聚的持续循环。

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