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The tomosyn homologue Sro7 is a direct effector of the Rab GTPase Sec4 in post-Golgi vesicle tethering

机译:tomosyn同源物Sro7在高尔基体后囊泡系留中是Rab GTPase Sec4的直接效应子

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摘要

The tomosyn/Sro7 family is thought to play an important role in cell surface trafficking both as an effector of Rab family GTPases and as a regulator of plasma-membrane SNARE function. Recent work has determined the binding site of GTP-bound Sec4 on Sro7. Here we examine the effect of mutations in Sro7 that block Sec4 binding in determining the role of this interaction in Sro7 function. Using an in vitro vesicle:vesicle tethering assay, we find that most of Sro7’s ability to tether vesicles is blocked by mutations that disrupt binding to Sec4-GTP. Similarly, genetic analysis demonstrates that the interaction with Sec4 is important for most of Sro7’s functions in vivo. The interaction of Sro7 with Sec4 appears to be particularly important when exocyst function is compromised. This provides strong evidence that Sro7 and the exocyst act as dual effector pathways downstream of Sec4. We also demonstrate that Sro7 tethering requires the presence of Sec4 on both opposing membranes and that homo-oligomerization of Sro7 occurs during vesicle tethering. This suggests a simple model for Sro7 function as a Rab effector in tethering post-Golgi vesicles to the plasma membrane in a pathway parallel to that of the exocyst complex.
机译:人们认为tomosyn / Sro7家族作为Rab家族GTPases的效应子和血浆膜SNARE功能的调节剂,在细胞表面运输中起着重要作用。最近的工作已经确定了Gro结合的Sec4在Sro7上的结合位点。在这里,我们检查了Sro7中突变的作用,该突变可阻止Sec4结合,从而决定这种相互作用在Sro7功能中的作用。使用体外的囊泡:囊泡束缚测定法,我们发现Sro7束缚囊泡的能力大部分被破坏与Sec4-GTP结合的突变所阻断。同样,遗传分析表明,与Sec4的相互作用对于Sro7在体内的大多数功能都很重要。当囊外功能受损时,Sro7与Sec4的相互作用显得尤为重要。这提供了有力的证据,证明Sro7和囊泡是Sec4下游的双重效应途径。我们还证明了Sro7系留需要两个相对膜上都存在Sec4,并且Sro7的均聚在囊泡系留期间发生。这表明Sro7可以作为简单的模型,充当高尔基体后囊泡以平行于囊外复合物的途径束缚于质膜的Rab效应子。

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