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SETDB1 Methylates MCT1 Promoting Tumor Progression by Enhancing the Lactate Shuttle.


ABSTRACT: MCT1 is a critical protein found in monocarboxylate transporters that plays a significant role in regulating the lactate shuttle. However, the post-transcriptional modifications that regulate MCT1 are not clearly identified. In this study, it is reported that SETDB1 interacts with MCT1, leading to its stabilization. These findings reveal a novel post-translational modification of MCT1, in which SETDB1 methylation occurs at K473 in vitro and in vivo. This methylation inhibits the interaction between MCT1 and Tollip, which blocks Tollip-mediated autophagic degradation of MCT1. Furthermore, MCT1 K473 tri-methylation promotes tumor glycolysis and M2-like polarization of tumor-associated macrophages in colorectal cancer (CRC), which enhances the lactate shuttle. In clinical studies, MCT1 K473 tri-methylation is found to be upregulated and positively correlated with tumor progression and overall survival in CRC. This discovery suggests that SETDB1-mediated tri-methylation at K473 is a vital regulatory mechanism for lactate shuttle and tumor progression. Additionally, MCT1 K473 methylation may be a potential prognostic biomarker and promising therapeutic target for CRC.

SUBMITTER: She X 

PROVIDER: S-EPMC10558670 | biostudies-literature | 2023 Oct

REPOSITORIES: biostudies-literature

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SETDB1 Methylates MCT1 Promoting Tumor Progression by Enhancing the Lactate Shuttle.

She Xiaowei X   Wu Qi Q   Rao Zejun Z   Song Da D   Huang Changsheng C   Feng Shengjie S   Liu Anyi A   Liu Lang L   Wan Kairui K   Li Xun X   Yu Chengxin C   Qiu Cheng C   Luo Xuelai X   Hu Junbo J   Wang Guihua G   Xu Feng F   Sun Li L  

Advanced science (Weinheim, Baden-Wurttemberg, Germany) 20230804 28


MCT1 is a critical protein found in monocarboxylate transporters that plays a significant role in regulating the lactate shuttle. However, the post-transcriptional modifications that regulate MCT1 are not clearly identified. In this study, it is reported that SETDB1 interacts with MCT1, leading to its stabilization. These findings reveal a novel post-translational modification of MCT1, in which SETDB1 methylation occurs at K473 in vitro and in vivo. This methylation inhibits the interaction betw  ...[more]

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