Issue 2, 2021

Mitochondria-targeted inhibitors of the human SIRT3 lysine deacetylase

Abstract

Sirtuin 3 (SIRT3) is the major protein lysine deacetylase in the mitochondria. This hydrolase regulates a wide range of metabolically involved enzymes and has been considered as a potential drug target in certain cancers. Investigation of pharmacological intervention has been challenging due to a lack of potent and selective inhibitors of SIRT3. Here, we developed a strategy for selective inhibition of SIRT3 in cells, over its structurally similar isozymes that localize primarily to the nucleus (SIRT1) and the cytosol (SIRT2). This was achieved by directing the inhibitors to the mitochondria through incorporation of mitochondria-targeting peptide sequences into the inhibitor structures. Our inhibitors exhibited excellent mitochondrial localization in HeLa cells as indicated by fluorophore-conjugated versions, and target engagement was demonstrated by a cellular thermal shift assay of SIRT3 using western blotting. The acetylation state of documented SIRT3 target MnSOD was shown to be increased in cells with little effect on known targets of SIRT1 and SIRT2, showing that our lead compound exhibits selectivity for SIRT3 in cells. We expect that the developed inhibitor will now enable a more detailed investigation of SIRT3 as a potential drug target and help shed further light on the diverse biology regulated by this enzyme.

Graphical abstract: Mitochondria-targeted inhibitors of the human SIRT3 lysine deacetylase

Supplementary files

Article information

Article type
Paper
Submitted
26 พ.ย. 2563
Accepted
24 ม.ค. 2564
First published
01 ก.พ. 2564
This article is Open Access
Creative Commons BY-NC license

RSC Chem. Biol., 2021,2, 627-635

Mitochondria-targeted inhibitors of the human SIRT3 lysine deacetylase

K. S. Troelsen, M. Bæk, A. L. Nielsen, A. S. Madsen, N. Rajabi and C. A. Olsen, RSC Chem. Biol., 2021, 2, 627 DOI: 10.1039/D0CB00216J

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