Non-oncogene Addiction to SIRT3 Plays a Critical Role in Lymphomagenesis.

Authors :: Li M
Chiang YL
Lyssiotis CA
Teater MR
Hong JY
Shen H
Wang L
Hu J
Jing H
Chen Z
Jain N
Duy C
Mistry SJ
Cerchietti L
Cross JR
Cantley LC
Green MR
Lin H
Melnick AM
Source :: Cancer cell [Cancer Cell] 2019 Jun 10; Vol. 35 (6), pp. 916-931.e9.
Publication Year :: 2019
Abstract: Diffuse large B cell lymphomas (DLBCLs) are genetically heterogeneous and highly proliferative neoplasms derived from germinal center (GC) B cells. Here, we show that DLBCLs are dependent on mitochondrial lysine deacetylase SIRT3 for proliferation, survival, self-renewal, and tumor growth in vivo regardless of disease subtype and genetics. SIRT3 knockout attenuated B cell lymphomagenesis in VavP-Bcl2 mice without affecting normal GC formation. Mechanistically, SIRT3 depletion impaired glutamine flux to the TCA cycle via glutamate dehydrogenase and reduction in acetyl-CoA pools, which in turn induce autophagy and cell death. We developed a mitochondrial-targeted class I sirtuin inhibitor, YC8-02, which phenocopied the effects of SIRT3 depletion and killed DLBCL cells. SIRT3 is thus a metabolic non-oncogene addiction and therapeutic target for DLBCLs.<br /> (Copyright © 2019 Elsevier Inc. All rights reserved.)