Published May 7, 2025
| Version v1
Journal article
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SIRT2-mediated ACSS2 K271 deacetylation suppresses lipogenesis under nutrient stress
- 1. Cornell University
- 2. University of Chicago
Description
De novo lipogenesis is associated with the development of human diseases such as cancer, diabetes, and obesity. At the core of lipogenesis lies acetyl coenzyme A (CoA), a metabolite that plays a crucial role in fatty acid synthesis. One of the pathways contributing to the production of cytosolic acetyl-CoA is mediated by acetyl-CoA synthetase 2 (ACSS2). Here, we reveal that when cells encounter nutrient stress, particularly a deficiency in amino acids, Sirtuin 2 (SIRT2) catalyzes the deacetylation of ACSS2 at the lysine residue K271. This results in K271 ubiquitination and subsequently proteasomal degradation of ACSS2. Substitution of K271 leads to decreased ubiquitination of ACSS2, increased ACSS2 protein level, and thus increased lipogenesis. Our study uncovers a mechanism that cells employ to efficiently manage lipogenesis during periods of nutrient stress.
Data availability
The study does not generate standard datasets. All data generated during this study are included in the manuscript and supporting files; Source data files have been provided for Figures 1-3 and their figure supplements.Files
elife-97019-v1.pdf
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Additional details
Identifiers
- DOI
- 10.7554/eLife.97019.3
- Other
- oai:uchicago.tind.io:15142
Funding
- Howard Hughes Medical Institute
- National Institutes of Health
- R01AR078555