Kaushik Susmita, Cuervo Ana Maria
Department of Developmental and Molecular Biology, Marion Bessin Liver Research Center, Institute for Aging Research, Albert Einstein College of Medicine, Bronx, New York, USA.
Methods Enzymol. 2009;452:297-324. doi: 10.1016/S0076-6879(08)03619-7.
Chaperone-mediated autophagy (CMA) is a selective type of autophagy responsible for the lysosomal degradation of soluble cytosolic proteins. In contrast to other forms of autophagy where cargo is sequestered and delivered to lysosomes through membrane fusion/excision, CMA substrates reach the lysosomal lumen after direct translocation across the lysosomal membrane. CMA is part of the cellular quality control systems and as such, essential for the cellular response to stress. CMA activity decreases with age, likely contributing to the accumulation of altered proteins characteristic in tissues from old organisms. Furthermore, impairment of CMA underlies the pathogenesis of certain human pathologies such as neurodegenerative disorders. These findings have drawn renewed attention to CMA and a growing interest in the measurement of changes in CMA activity under different physiological and pathological conditions. In this chapter we review the different experimental approaches used to assess CMA activity both in cells in culture and in different organs from animals.
伴侣介导的自噬(CMA)是一种选择性自噬类型,负责可溶性胞质蛋白的溶酶体降解。与其他形式的自噬不同,在其他自噬形式中,货物通过膜融合/切割被隔离并输送到溶酶体,而CMA底物在直接穿过溶酶体膜后到达溶酶体腔。CMA是细胞质量控制系统的一部分,因此对于细胞对压力的反应至关重要。CMA活性随年龄增长而降低,这可能导致老年生物体组织中特征性改变蛋白的积累。此外,CMA功能障碍是某些人类疾病(如神经退行性疾病)发病机制的基础。这些发现重新引起了人们对CMA的关注,并越来越关注在不同生理和病理条件下测量CMA活性的变化。在本章中,我们回顾了用于评估培养细胞和动物不同器官中CMA活性的不同实验方法。
