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A network of cytosolic factors targets SRP-independent proteins to the endoplasmic reticulum

机译:胞质因子网络将不依赖SRP的蛋白靶向内质网

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摘要

Translocation into the endoplasmic reticulum (ER) is an initial and crucial biogenesis step for all secreted and endomembrane proteins in eukaryotes. ER insertion can take place through the well-characterized signal recognition particle (SRP)-dependent pathway or the less-studied route of SRP-independent translocation. To better understand the prevalence of the SRP-independent pathway, we systematically defined the translocational dependence of the yeast secretome. By combining hydropathy-based analysis and microscopy, we uncovered that a previously unappreciated fraction of the yeast secretome translocates without the aid of the SRP. Furthermore, we validated a family of SRP-independent substrates - the glycosylphosphatidylinositol (GPI)-anchored proteins. Studying this family, we identified a determinant for ER targeting and uncovered a network of cytosolic proteins that facilitate SRP-independent targeting and translocation. These findings highlight the underappreciated complexity of SRP-independent translocation, which enables this pathway to efficiently cope with its extensive substrate flux.
机译:对于真核生物中所有分泌的和内膜蛋白而言,易位进入内质网(ER)是重要的初始生源步骤。 ER插入可通过特征明确的信号识别颗粒(SRP)依赖性途径或研究较少的SRP依赖性易位途径进行。为了更好地了解SRP非依赖性途径的普遍性,我们系统地定义了酵母分泌组的易位依赖性。通过结合基于水肿的分析和显微镜检查,我们发现酵母分泌基因组以前未被认识的部分在没有SRP的帮助下易位。此外,我们验证了不依赖SRP的底物家族-糖基磷脂酰肌醇(GPI)锚定的蛋白质。通过研究这个家族,我们确定了ER靶向的决定因素,并发现了促进SRP非依赖性靶向和易位的细胞溶质蛋白网络。这些发现突显了与SRP无关的易位的低估的复杂性,这使得该途径能够有效应对其广泛的底物通量。

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