PI3K-regulated Glycine N-methyltransferase is required for the development of prostate cancer
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Published:2022-02-23
Issue:1
Volume:11
Page:
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ISSN:2157-9024
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Container-title:Oncogenesis
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language:en
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Short-container-title:Oncogenesis
Author:
Zabala-Letona Amaia, Arruabarrena-Aristorena AmaiaORCID, Fernandez-Ruiz Sonia, Viera Cristina, Carlevaris Onintza, Ercilla Amaia, Mendizabal IsabelORCID, Martin Teresa, Macchia AliceORCID, Camacho Laura, Pujana-Vaquerizo Mikel, Sanchez-Mosquera Pilar, Torrano Verónica, Martin-Martin Natalia, Zuniga-Garcia PatriciaORCID, Castillo-Martin Mireia, Ugalde-Olano Aitziber, Loizaga-Iriarte Ana, Unda MiguelORCID, Mato Jose M.ORCID, Berra Edurne, Martinez-Chantar Maria L.ORCID, Carracedo ArkaitzORCID
Abstract
AbstractGlycine N-Methyltransferase (GNMT) is a metabolic enzyme that integrates metabolism and epigenetic regulation. The product of GNMT, sarcosine, has been proposed as a prostate cancer biomarker. This enzyme is predominantly expressed in the liver, brain, pancreas, and prostate tissue, where it exhibits distinct regulation. Whereas genetic alterations in GNMT have been associated to prostate cancer risk, its causal contribution to the development of this disease is limited to cell line-based studies and correlative human analyses. Here we integrate human studies, genetic mouse modeling, and cellular systems to characterize the regulation and function of GNMT in prostate cancer. We report that this enzyme is repressed upon activation of the oncogenic Phosphoinositide-3-kinase (PI3K) pathway, which adds complexity to its reported dependency on androgen signaling. Importantly, we demonstrate that expression of GNMT is required for the onset of invasive prostate cancer in a genetic mouse model. Altogether, our results provide further support of the heavy oncogenic signal-dependent regulation of GNMT in prostate cancer.
Publisher
Springer Science and Business Media LLC
Subject
Cancer Research,Molecular Biology
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