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Proteomics of the lysosome.

机译:溶酶体的蛋白质组学。

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摘要

Defects in lysosomal function have been associated with numerous monogenic human diseases typically classified as lysosomal storage diseases. However, there is increasing evidence that lysosomal proteins are also involved in more widespread human diseases including cancer and Alzheimer disease. Thus, there is a continuing interest in understanding the cellular functions of the lysosome and an emerging approach to this is the identification of its constituent proteins by proteomic analyses. To date, the mammalian lysosome has been shown to contain approximately 60 soluble luminal proteins and approximately 25 transmembrane proteins. However, recent proteomic studies based upon affinity purification of soluble components or subcellular fractionation to obtain both soluble and membrane components suggest that there may be many more of both classes of protein resident within this organelle than previously appreciated. Discovery of such proteins has important implications for understanding the function and the dynamics of the lysosome but can also lead the way towards the discovery of the genetic basis for human diseases of hitherto unknown etiology. Here, we describe current approaches to lysosomal proteomics and data interpretation and review the new lysosomal proteins that have recently emerged from such studies.
机译:溶酶体功能的缺陷与许多单基因人类疾病有关,这些疾病通常被分类为溶酶体贮积病。但是,越来越多的证据表明,溶酶体蛋白也与更广泛的人类疾病有关,包括癌症和阿尔茨海默氏病。因此,人们对理解溶酶体的细胞功能有着持续的兴趣,一种新兴的方法是通过蛋白质组学分析鉴定其组成蛋白。迄今为止,已经显示哺乳动物溶酶体包含约60种可溶性腔蛋白和约25种跨膜蛋白。然而,基于可溶成分的亲和纯化或亚细胞分离以获得可溶成分和膜成分的最新蛋白质组学研究表明,驻留在该细胞器中的两类蛋白质可能比以前认识的更多。此类蛋白质的发现对于理解溶酶体的功能和动力学具有重要意义,但也可以为发现迄今未知病因的人类疾病的遗传基础提供途径。在这里,我们描述了溶酶体蛋白质组学和数据解释的当前方法,并回顾了最近从此类研究中出现的新型溶酶体蛋白。

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