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首页> 外文期刊>Molecular biology of the cell >WASP-interacting protein is important for actin filament elongation and prompt pseudopod formation in response to a dynamic chemoattractant gradient
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WASP-interacting protein is important for actin filament elongation and prompt pseudopod formation in response to a dynamic chemoattractant gradient

机译:WASP相互作用蛋白对于肌动蛋白丝伸长和响应动态化学引力梯度而迅速形成假足很重要

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摘要

The role of WASP-interacting protein (WIP) in the process of F-actin assembly during chemotaxis of Dictyostelium was examined. Mutations of the WH1 domain of WASP led to a reduction in binding to WIPa, a newly identified homolog of mammalian WIP, a reduction of F-actin polymerization at the leading edge, and a reduction in chemotactic efficiency. WIPa localizes to sites of new pseudopod protrusion and colocalizes with WASP at the leading edge. WIPa increases F-actin elongation in vivo and in vitro in a WASP-dependent manner. WIPa translocates to the cortical membrane upon uniform cAMP stimulation in a time course that parallels F-actin polymerization. WIPa-overexpressing cells exhibit multiple microspike formation and defects in chemotactic efficiency due to frequent changes of direction. Reduced expression of WIPa by expressing a hairpin WIPa (hp WIPa) construct resulted in more polarized cells that exhibit a delayed response to a new chemoattractant source due to delayed extension of pseudopod toward the new gradient. These results suggest that WIPa is required for new pseudopod protrusion and prompt reorientation of cells toward a new gradient by initiating localized bursts of actin polymerization and/or elongation.
机译:研究了WASP相互作用蛋白(WIP)在Dictyostelium趋化过程中F-肌动蛋白装配过程中的作用。 WASP WH1结构域的突变导致与WIPa的结合减少,新发现的哺乳动物WIP同源物,前沿F-肌动蛋白聚合减少以及趋化效率降低。 WIPa定位到新的伪足突出部位,并与WASP共同定位在前端。 WIPa以WASP依赖性方式在体内和体外增加F-肌动蛋白的延伸。在均匀的cAMP刺激下,WIPA在与F-肌动蛋白聚合反应平行的时间过程中转移到皮质膜上。由于方向的频繁变化,过量表达WIPA的细胞表现出多个微峰形成和趋化效率缺陷。通过表达发夹WIPA(hp WIPa)构建体,WIPA的表达减少,导致更多极化的细胞,由于伪足向新梯度的延迟延伸,对新趋化因子来源的响应有所延迟。这些结果表明,WIPA是新的假足突突所必需的,并通过启动肌动蛋白聚合和/或伸长的局部爆发而迅速向新的梯度定向细胞。

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