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首页> 外文期刊>eLife journal >Multiple selection filters ensure accurate tail-anchored membrane protein targeting
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Multiple selection filters ensure accurate tail-anchored membrane protein targeting

机译:多种选择的过滤器可确保准确定位尾部锚定的膜蛋白

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Accurate protein localization is crucial to generate and maintain organization in all cells. Achieving accuracy is challenging, as the molecular signals that dictate a protein’s cellular destination are often promiscuous. A salient example is the targeting of an essential class of tail-anchored (TA) proteins, whose sole defining feature is a transmembrane domain near their C-terminus. Here we show that the Guided Entry of Tail-anchored protein (GET) pathway selects TA proteins destined to the endoplasmic reticulum (ER) utilizing distinct molecular steps, including differential binding by the co-chaperone Sgt2 and kinetic proofreading after ATP hydrolysis by the targeting factor Get3. Further, the different steps select for distinct physicochemical features of the TA substrate. The use of multiple selection filters may be general to protein biogenesis pathways that must distinguish correct and incorrect substrates based on minor differences.
机译:准确的蛋白质定位对于在所有细胞中生成和维持组织至关重要。实现准确性具有挑战性,因为指示蛋白质细胞目的地的分子信号通常是混杂的。一个突出的例子是针对必需的尾锚(TA)蛋白类别,其唯一的特征是在其C端附近的跨膜结构域。在这里,我们显示尾巴锚定蛋白(GET)路径的引导进入通过不同的分子步骤选择了发往内质网(ER)的TA蛋白,包括通过伴侣伴侣Sgt2进行的差异结合以及通过靶向水解后的ATP的动力学校对因子Get3。此外,针对TA底物的不同理化特征选择不同的步骤。多种选择过滤器的使用可能是蛋白质生物发生途径的常规方法,必须根据微小差异区分正确和错误的底物。

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