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SIRT1 directly activates autophagy in human chondrocytes
Pradeep Kumar Sacitharan, George Bou–Gharios, James Edwards
Cell Death Discovery · 2020 · ▲ 90 citations
Abstract
Osteoarthritis (OA) is the most common form of arthritis worldwide with no effective treatment. Ageing is the primary risk factor for OA. We sought to investigate if there is a distinct and functional convergence of ageing-related mechanisms SIRT1 and autophagy(definition) in chondrocytes. Our results show that, levels of SIRT1 are decreased in human normal aged and OA cartilage compared with young cartilage. Moreover, silencing SIRT1 in chondrocytes lead to decreased expression of chondrogenic markers but did not alter the expression of catabolic proteases. In contrast, activation of SIRT1 increased autophagy in chondrocytes by the deacetylation of lysine residues on crucial autophagy proteins (Beclin1, ATG5, ATG7, LC3). This activation was shown to be mTOR(definition)/ULK1 independent. Our results indicate that maintenance of autophagy in chondrocytes by SIRT1 is essential for preserving cartilage integrity throughout life and therefore is a target for drug intervention to protect against OA.
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- 10.1038/s41420-020-0277-0
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- 2026-06-16 MST
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APA
Sacitharan, P.K., Bou–Gharios, G., & Edwards, J. (2020). SIRT1 directly activates autophagy in human chondrocytes. <em>Cell Death Discovery</em>. https://doi.org/10.1038/s41420-020-0277-0
Vancouver
Sacitharan PK, Bou–Gharios G, Edwards J. SIRT1 directly activates autophagy in human chondrocytes. Cell Death Discovery. 2020. doi:10.1038/s41420-020-0277-0.
BibTeX
@article{pradeep2020SIRTdi,
title = {SIRT1 directly activates autophagy in human chondrocytes},
author = {Pradeep Kumar Sacitharan and George Bou–Gharios and James Edwards},
journal = {Cell Death Discovery},
year = {2020},
doi = {10.1038/s41420-020-0277-0},
}
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