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在持续将蛋白质循环利用至内质网的情况下维持高尔基体结构:收支平衡。

Maintenance of Golgi apparatus structure in the face of continuous protein recycling to the endoplasmic reticulum: making ends meet.

作者信息

Storrie Brian

机构信息

Department of Physiology and Biophysics, University of Arkansas for Medical Sciences, Little Rock, Arkansas 72205, USA.

出版信息

Int Rev Cytol. 2005;244:69-94. doi: 10.1016/S0074-7696(05)44002-4.

Abstract

I focus here on the Golgi apparatus and the dynamic relationship between the Golgi apparatus, the central organelle of the secretory pathway, and the endoplasmic reticulum (ER). The proteins and lipids of the Golgi apparatus originate in the ER, and cargo proteins and lipids that also originate in the ER are processed and sorted within the Golgi apparatus. The Golgi apparatus is indeed the central organelle of the secretory pathway. Surprisingly, many, if not all, of the proteins and accompanying lipids of the Golgi apparatus cycle continuously between the Golgi and the ER. Neither the Cisternal Maturation nor the Vesicular Transport/Stable Compartment model of Golgi apparatus function predicts continuous cycling of Golgi resident proteins through the ER. Evidence for this cycling comes from multiple experimental approaches, including ER-exit block-revealed accumulation of recycled Golgi resident proteins in the ER, evidence for exchange of green fluorescent protein (GFP)-tagged Golgi proteins or their analogues between Golgi and ER pools, and cisternal rab overexpression-induced redistribution of Golgi resident proteins to the ER. The implications of Golgi protein cycling for the maintenance of Golgi structure in the interphase mammalian cell are discussed. The challenge for the future is to put Golgi resident protein cycling pathway(s) to protein machinery and to characterize the cumulative, weak, dynamic interactions that hold the Golgi apparatus together. In doing so, new paradigms of organelle biogenesis will emerge.

摘要

我在此聚焦于高尔基体以及高尔基体(分泌途径的核心细胞器)与内质网(ER)之间的动态关系。高尔基体的蛋白质和脂质起源于内质网,同样起源于内质网的货物蛋白和脂质在高尔基体中进行加工和分选。高尔基体确实是分泌途径的核心细胞器。令人惊讶的是,高尔基体的许多(如果不是全部的话)蛋白质和伴随的脂质在高尔基体和内质网之间持续循环。高尔基体功能的潴泡成熟模型和囊泡运输/稳定区室模型都没有预测到高尔基体驻留蛋白会通过内质网进行持续循环。这种循环的证据来自多种实验方法,包括内质网出口阻断揭示的回收的高尔基体驻留蛋白在内质网中的积累、绿色荧光蛋白(GFP)标记的高尔基体蛋白或其类似物在高尔基体和内质网池之间交换的证据,以及潴泡rab过表达诱导的高尔基体驻留蛋白向内质网的重新分布。本文讨论了高尔基体蛋白循环对间期哺乳动物细胞中高尔基体结构维持的影响。未来的挑战是将高尔基体驻留蛋白循环途径与蛋白质机制联系起来,并表征将高尔基体维系在一起的累积的、微弱的、动态的相互作用。这样做将会出现细胞器生物发生的新范式。

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