溶酶体贮积症中的自噬监测
Monitoring autophagy in lysosomal storage disorders.
作者信息
Raben Nina, Shea Lauren, Hill Victoria, Plotz Paul
机构信息
The Arthritis and Rheumatism Branch, NIAMS, National Institutes of Health, Bethesda, Maryland, USA.
出版信息
Methods Enzymol. 2009;453:417-49. doi: 10.1016/S0076-6879(08)04021-4.
Abstract
Lysosomes are the final destination of the autophagic pathway. It is in the acidic milieu of the lysosomes that autophagic cargo is metabolized and recycled. One would expect that diseases with primary lysosomal defects would be among the first systems in which autophagy would be studied. In reality, this is not the case. Lysosomal storage diseases, a group of more than 60 diverse inherited disorders, have only recently become a focus of autophagic research. Studies of these clinically severe conditions promise not only to clarify pathogenic mechanisms, but also to expand our knowledge of autophagy itself. In this chapter, we will describe the lysosomal storage diseases in which autophagy has been explored, and present the approaches used to evaluate this essential cellular pathway.
摘要
溶酶体是自噬途径的最终目的地。正是在溶酶体的酸性环境中,自噬货物被代谢和循环利用。人们可能会认为,原发性溶酶体缺陷疾病会是最早开展自噬研究的系统之一。但实际上并非如此。溶酶体贮积病是一组超过60种不同的遗传性疾病,直到最近才成为自噬研究的焦点。对这些临床严重疾病的研究不仅有望阐明致病机制,还能扩展我们对自噬本身的认识。在本章中,我们将描述已对自噬进行探索的溶酶体贮积病,并介绍用于评估这一重要细胞途径的方法。
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