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ARAP1 regulates the ring size of circular dorsal ruffles through Arf1 and Arf5

机译:ARAP1通过Arf1和Arf5调节圆形背褶的戒指尺寸

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摘要

Small guanosine triphosphatase (GTPase) ADP-ribosylation factors (Arfs) regulate membrane traffic and actin reorganization under the strict control of GTPase-activating proteins (GAPs). ARAP1 (Arf GAP with Rho GAP domain, ankyrin repeat, and PH domain 1) is an Arf GAP molecule with multiple PH domains that recognize phosphatidylinositol 3,4,5-trisphosphate. We found that growth factor stimulation induced localization of ARAP1 to an area of the plasma membrane inside the ring structure of circular dorsal ruffles (CDRs). Moreover, expression of ARAP1 increased the size of the CDR filamentous-actin ring in an Arf GAP activity- dependent manner, whereas smaller CDRs were formed by ARAP1 knockdown. In addition, expression of a dominant-negative mutant of Arf1 and Arf5, the substrates of ARAP1, expanded the size of CDRs, suggesting that the two Arf isoforms regulate ring structure downstream of ARAP1. Therefore our results reveal a novel molecular mechanism of CDR ring size control through the ARAP1-Arf1/5 pathway.
机译:小型鸟苷三磷酸酶(GTPase)ADP-核糖基化因子(Arfs)在GTPase激活蛋白(GAPs)的严格控制下调节膜运输和肌动蛋白重组。 ARAP1(具有Rho GAP结构域,锚蛋白重复序列​​和PH结构域1的Arf GAP)是具有多个PH结构域的Arf GAP分子,可识别磷脂酰肌醇3,4,5-三磷酸。我们发现生长因子刺激诱导ARAP1定位到圆形背褶皱(CDR)的环形结构内质膜的区域。此外,ARAP1的表达以Arf GAP活性依赖性方式增加了CDR丝状肌动蛋白环的大小,而较小的CDRs通过ARAP1敲低形成。另外,ARAP1的底物Arf1和Arf5的显性负突变体的表达扩大了CDR的大小,表明这两个Arf同工型调节了ARAP1下游的环结构。因此,我们的结果揭示了通过ARAP1-Arf1 / 5途径控制CDR环大小的新分子机制。

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