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Analysis of the Retromer complex-WASH complex interaction illuminates new avenues to explore in Parkinson disease

机译:Retromer复合物与WASH复合物相互作用的分析为帕金森病探索提供了新途径

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The retromer complex mediates endosomal protein sorting by concentrating membrane proteins (cargo) into nascent tubules formed through the action of sorting nexin (SNX) proteins. The WASH complex is recruited to endosomes by binding to the VPS35 subunit of retromer and facilitates cargo protein sorting by promoting formation of endosomally-localized F-actin. The VPS35 protein is mutated in Parkinson disease (PD) and a recent report has revealed that the PD-causing mutation impairs the association of retromer with the WASH complex leading to perturbed endosomal protein sorting. Another important player in endosomal protein sorting is the DNAJC13/RME-8 protein, which associates with SNX1 and has also recently been linked to PD. An additional recent report has now shown that RME-8 also interacts with the WASH complex thus establishing retromer and WASH complex-mediated endosomal protein sorting as a key pathway linked to the pathology of PD and providing new avenues to explore in the search for insights into the disease mechanism.
机译:逆转录复合物通过将膜蛋白(货物)浓缩成新生小管来介导内体蛋白分选,新生小管是通过分选神经毒素(SNX)蛋白而形成的。 WASH复合物通过与逆向异构体的VPS35亚基结合而被募集到内体,并通过促进内体定位的F-肌动蛋白的形成而促进货物蛋白分选。 VPS35蛋白在帕金森氏病(PD)中发生了突变,最近的一份报告显示,导致PD的突变损害了Retromer与WASH复合物的缔合,从而导致内体蛋白分类受到干扰。内体蛋白分选的另一个重要参与者是DNAJC13 / RME-8蛋白,该蛋白与SNX1相关,并且最近还与PD关联。现在,另一份最新报告显示,RME-8还与WASH复合物相互作用,从而建立了逆转录酶和WASH复合物介导的内体蛋白分选,这是与PD病理相关的关键途径,并提供了新的途径来探索洞察力疾病机理。

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