| Literature DB >> 34183356 |
Nora Pällmann1, Ke Deng2, Marte Livgård1,2, Martina Tesikova3, Yixin Jin1, Nicolai Sebastian Frengen1, Nermin Kahraman4, Hamada M Mokhlis4,5, Bulent Ozpolat4, Wanja Kildal2, Havard Emil Danielsen2,6,7,8, Ladan Fazli9, Paul S Rennie9, Partha P Banerjee10, Aykut Üren11, Yang Jin1, Omer F Kuzu12, Fahri Saatcioglu12,2.
Abstract
One-carbon (1C) metabolism has a key role in metabolic programming with both mitochondrial (m1C) and cytoplasmic (c1C) components. Here we show that activating transcription factor 4 (ATF4) exclusively activates gene expression involved in m1C, but not the c1C cycle in prostate cancer cells. This includes activation of methylenetetrahydrofolate dehydrogenase 2 (MTHFD2) expression, the central player in the m1C cycle. Consistent with the key role of m1C cycle in prostate cancer, MTHFD2 knockdown inhibited prostate cancer cell growth, prostatosphere formation, and growth of patient-derived xenograft organoids. In addition, therapeutic silencing of MTHFD2 by systemically administered nanoliposomal siRNA profoundly inhibited tumor growth in preclinical prostate cancer mouse models. Consistently, MTHFD2 expression is significantly increased in human prostate cancer, and a gene expression signature based on the m1C cycle has significant prognostic value. Furthermore, MTHFD2 expression is coordinately regulated by ATF4 and the oncoprotein c-MYC, which has been implicated in prostate cancer. These data suggest that the m1C cycle is essential for prostate cancer progression and may serve as a novel biomarker and therapeutic target. SIGNIFICANCE: These findings demonstrate that the mitochondrial, but not cytoplasmic, one-carbon cycle has a key role in prostate cancer cell growth and survival and may serve as a biomarker and/or therapeutic target. ©2021 American Association for Cancer Research.Entities:
Mesh:
Year: 2021 PMID: 34183356 DOI: 10.1158/0008-5472.CAN-20-3956
Source DB: PubMed Journal: Cancer Res ISSN: 0008-5472 Impact factor: 12.701