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Analysis of GTPase-activating proteins: Rab1 and Rab43 are key Rabs required to maintain a functional Golgi complex in human cells

机译:GTPase激活蛋白分析:Rab1和Rab43是维持人类细胞中功能性高尔基体所需的关键Rab

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Rab GTPases control vesicle movement and tethering membrane events in membrane trafficking. We used the 38 human Rab GTPase activating proteins (GAPs) to identify which of the 60 Rabs encoded in the human genome function at the Golgi complex. Surprisingly, this screen identified only two GAPs, RN-tre and TBC1D20, disrupting both Golgi organization and protein transport. RN-tre is the GAP for Rab43, and controls retrograde transport into the Golgi from the endocytic pathway. TBC1D20 is the ER-localized GAP for Rab1, and is the only GAP blocking the delivery of secretory cargo from the ER to the cell surface. Strikingly, its expression causes the loss of the Golgi complex, highlighting the importance of Rab1 for Golgi biogenesis. These effects can be antagonized by reticulon, a binding partner for TBC1D20 in the ER. Together, these findings indicate that Rab1 and Rab43 are key Rabs required for the biogenesis and maintenance of a functional Golgi structure, and suggest that other Rabs acting at the Golgi complex are likely to be functionally redundant.
机译:Rab GTPases在膜运输中控制囊泡运动和栓系膜事件。我们使用了38种人类Rab GTP酶激活蛋白(GAP)来识别人类基因组中编码的60种Rab中的哪一种在高尔基体中起作用。令人惊讶的是,该筛选仅鉴定出两个GAP,RN-tre和TBC1D20,破坏了高尔基体的组织和蛋白质的运输。 RN-tre是Rab43的GAP,并控制其从内吞途径逆行进入高尔基体。 TBC1D20是Rab1的ER定位GAP,并且是唯一阻止将分泌物从ER传递到细胞表面的GAP。令人惊讶的是,它的表达引起高尔基体的损失,突显了Rab1对高尔基体生物发生的重要性。这些作用可以被网状组织(ER)中TBC1D20的结合伴侣拮抗。在一起,这些发现表明Rab1和Rab43是功能性高尔基体的生物发生和维持所必需的关键Rab,并且表明其他作用于高尔基体的Rab可能在功能上是多余的。

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