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首页> 外文期刊>Journal of cell biology >The BEACH-containing protein WDR81 coordinates p62 and LC3C to promote aggrephagy
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The BEACH-containing protein WDR81 coordinates p62 and LC3C to promote aggrephagy

机译:含沙滩的蛋白质WDR81坐标P62和LC3C促进聚心电图

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Autophagy-dependent clearance of ubiquitinated and aggregated proteins is critical to protein quality control, but the underlying mechanisms are not well understood. Here, we report the essential role of the BEACH (beige and Chediak–Higashi) and WD40 repeat-containing protein WDR81 in eliminating ubiquitinated proteins through autophagy. WDR81 associates with ubiquitin (Ub)-positive protein foci, and its loss causes accumulation of Ub proteins and the autophagy cargo receptor p62. WDR81 interacts with p62, facilitating recognition of Ub proteins by p62. Furthermore, WDR81 interacts with LC3C through canonical LC3-interacting regions in the BEACH domain, promoting LC3C recruitment to ubiquitinated proteins. Inactivation of LC3C or defective autophagy results in accumulation of Ub protein aggregates enriched for WDR81. In mice, WDR81 inactivation causes accumulation of p62 bodies in cortical and striatal neurons in the brain. These data suggest that WDR81 coordinates p62 and LC3C to facilitate autophagic removal of Ub proteins, and provide important insights into CAMRQ2 syndrome, a WDR81-related developmental disorder.
机译:泛噬依赖性和占蛋白质的自噬依赖性对蛋白质质量控​​制至关重要,但潜在的机制并不熟知。在这里,我们报告了海滩(米色和Chediak-higashi)和Wd40含有蛋白质WDR81通过自噬消除普发蛋白质的基本作用。 WDR81与泛素(UB) - 阳性蛋白质病灶相关联,其损失引起UB蛋白的积累和自噬碳受体P62。 WDR81与P62相互作用,促进P62识别UB蛋白。此外,WDR81通过在海滩域中的Canonical LC3相互作用区域与LC3C相互作用,促进LC3C募集到普遍植物蛋白。 LC3C的灭活或缺陷的自噬导致富含WDR81的UB蛋白质聚集体的积累。在小鼠中,WDR81失活导致脑中皮质和纹状体神经元中的P62体积累。这些数据表明,WDR81坐标P62和LC3C促进UB蛋白的自噬去除,并为CAMRQ2综合征,WDR81相关发育障碍提供重要见解。

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