Author:
Kettern Nadja,Dreiseidler Michael,Tawo Riga,Höhfeld Jörg
Abstract
AbstractMolecular chaperones are well known as facilitators of protein folding and assembly. However, in recent years multiple chaperone-assisted degradation pathways have also emerged, including CAP (chaperone-assistedproteasomal degradation), CASA (chaperone-assistedselectiveautophagy), and CMA (chaperone-mediatedautophagy). Within these pathways chaperones facilitate the sorting of non-native proteins to the proteasome and the lysosomal compartment for disposal. Impairment of these pathways contributes to the development of cancer, myopathies, and neurodegenerative diseases. Chaperone-assisted degradation thus represents an essential aspect of cellular proteostasis, and its pharmacological modulation holds the promise to ameliorate some of the most devastating diseases of our time. Here, we discuss recent insights into molecular mechanisms underlying chaperone-assisted degradation in mammalian cells and highlight its biomedical relevance.
Subject
Clinical Biochemistry,Molecular Biology,Biochemistry
Cited by
142 articles.
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