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Protein trafficking and maturation regulate intramembrane proteolysis

机译:蛋白质运输和成熟调节膜内蛋白水解

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摘要

Intramembrane-cleaving proteases (I-CLiPs) are membrane embedded proteolytic enzymes. All substrates identified so far are also membrane proteins, involving a number of critical cellular signaling as well as human diseases. After synthesis and assembly at the endoplasmic reticulum, membrane proteins are exported to the Golgi apparatus and transported to their sites of action. A number of studies have revealed the importance of the intracellular membrane trafficking in i-CLiP-mediated intramembrane proteolysis, not only for limiting the unnecessary encounter between i-CLiPs and their substrate but also for their cleavage site preference. In this review, we will discuss recent advances in our understanding of how each i-CLiP proteolysis is regulated by intracellular vesicle trafficking. This article is part of a Special Issue entitled: Intramembrane Proteases.
机译:膜内切割蛋白酶(I-CLiP)是膜嵌入的蛋白水解酶。迄今为止,所有被鉴定的底物也是膜蛋白,涉及许多关键的细胞信号以及人类疾病。在内质网合成和组装后,膜蛋白被输出到高尔基体,并被转运到它们的作用部位。大量研究揭示了胞内膜运输在i-CLiP介导的膜内蛋白水解中的重要性,不仅是为了限制i-CLiPs与它们的底物之间的不必要接触,而且还因为它们的切割位点偏好。在这篇综述中,我们将讨论在了解每个i-CLiP蛋白水解如何受到细胞内囊泡运输调控方面的最新进展。本文是名为“膜内蛋白酶”的特刊的一部分。

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