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Distinct retrieval and retention mechanisms are required for the quality control of endoplasmic reticulum protein folding

机译:内质网蛋白折叠的质量控制需要不同的检索和保留机制

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Proteins destined for the secretory pathway must first fold and assemble in the lumen of endoplasmic reticulum (ER). The pathway maintains a quality control mechanism to assure that aberrantly processed proteins are not delivered to their sites of function. As part of this mechanism, misfolded proteins are returned to the cytosol via the ER protein translocation pore where they are ubiquitinated and degraded by the 26S proteasome. Previously, little was known regarding the recognition and targeting of proteins before degradation. By tracking the fate of several mutant proteins subject to quality control, we demonstrate the existence of two distinct sorting mechanisms. In the ER, substrates are either sorted for retention in the ER or are transported to the Golgi apparatus via COPII–coated vesicles. Proteins transported to the Golgi are retrieved to the ER via the retrograde transport system. Ultimately, both retained and retrieved proteins converge at a common machinery at the ER for degradation. Furthermore, we report the identification of a gene playing a novel role specific to the retrieval pathway. The gene, BST1, is required for the transport of misfolded proteins to the Golgi, although dispensable for the transport of many normal cargo proteins.
机译:预定用于分泌途径的蛋白质必须首先在内质网(ER)内腔中折叠和组装。该途径维持质量控制机制,以确保异常加工的蛋白质不会传递至其功能位点。作为此机制的一部分,错误折叠的蛋白质会通过ER蛋白质转运孔返回到细胞质中,在那里它们被26S蛋白酶体泛素化并降解。以前,关于降解之前蛋白质的识别和靶向的了解很少。通过跟踪受质量控制的几种突变蛋白的命运,我们证明了两种不同的分类机制的存在。在ER中,将底物分类以保留在ER中,或者通过COPII涂层的囊泡运输到高尔基体中。转运至高尔基体的蛋白质通过逆行转运系统被回收至内质网。最终,保留和回收的蛋白质都在ER的通用机器处汇合降解。此外,我们报告了一个基因的鉴定,该基因在检索途径中起着新颖的作用。 BST1基因是将错误折叠的蛋白质转运到高尔基体所必需的,尽管对于许多正常货物蛋白质的转运是必不可少的。

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