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细胞内异型和同型膜融合机制的内部运作。

The inner workings of intracellular heterotypic and homotypic membrane fusion mechanisms.

机构信息

Missouri State University, 901 S. National Ave, Springfield, MO 65897, USA.

出版信息

J Biosci. 2019 Sep;44(4).

Abstract

Intracellular trafficking is a field that has been intensively studied for years and yet there remains much to be learned. Part of the reason that there is so much obscurity remaining in this field is due to all the pathways and the stages that define cellular trafficking. One of the major steps in cellular trafficking is fusion. Fusion is defined as the terminal step that occurs when a cargo-laden vesicle arrives at the proper destination. There are two types of fusion within a cell: homotypic and heterotypic fusion. Homotypic fusion occurs when the two membranes merging together are of the same type such as vacuole to vacuole fusion. Heterotypic fusion occurs when the two membranes at play are of different types such as when an endosomal membrane fuses with a Golgi membrane. In this review, we will focus on all the protein components - Rabs, Golgins, Multisubunit tethers, GTPases, protein phosphatases and SNAREs - that have been known to function in both of these types of fusion. We hope to develop a model of how all of these constituents function together to achieve membrane fusion. Membrane fusion is a biological process absolutely necessary for proper intracellular trafficking. Due to the degree of importance multiple proteins are required for it to be properly carried through. Whether we are talking about heterotypic or homotypic fusion, any defects in the fusion machinery can result in disease states such as Parkinson's and Alzheimer's disease. Although much research has significantly expanded our knowledge of fusion, there is still much more to be learned.

摘要

细胞内运输是一个多年来一直受到深入研究的领域,但仍有许多需要学习的地方。造成该领域如此多的模糊性的部分原因是由于定义细胞运输的所有途径和阶段。细胞内运输的主要步骤之一是融合。融合被定义为当载有货物的囊泡到达适当的目的地时发生的最后一步。细胞内有两种融合类型:同源融合和异源融合。同源融合发生在融合的两个膜是同一类型的情况下,例如液泡到液泡的融合。异源融合发生在两个起作用的膜是不同类型的情况下,例如内体膜与高尔基体膜融合。在这篇综述中,我们将重点介绍所有已知在这两种融合类型中起作用的蛋白质成分——Rab、Golgins、多亚基接头、GTPase、蛋白磷酸酶和 SNARE——。我们希望建立一个模型,说明所有这些成分如何协同作用以实现膜融合。膜融合是细胞内运输所必需的生物学过程。由于其重要性程度,需要多种蛋白质来正确地进行。无论是异源融合还是同源融合,融合机制的任何缺陷都可能导致帕金森病和阿尔茨海默病等疾病状态。尽管大量的研究显著扩展了我们对融合的认识,但仍有许多需要学习。

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