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TRDMT1介导的RNA C-5甲基化作为抗癌治疗的新靶点。

TRDMT1-mediated RNA C-5 methylation as a novel target in anticancer therapy.

作者信息

Lewinska Anna, Adamczyk-Grochala Jagoda, Wnuk Maciej

机构信息

Institute of Biotechnology, College of Natural Sciences, University of Rzeszow, Pigonia 1, 35-310 Rzeszow, Poland.

Institute of Biotechnology, College of Natural Sciences, University of Rzeszow, Pigonia 1, 35-310 Rzeszow, Poland.

出版信息

Biochim Biophys Acta Rev Cancer. 2023 Nov;1878(6):188964. doi: 10.1016/j.bbcan.2023.188964. Epub 2023 Aug 23.

Abstract

Affected landscape of RNA modifications is frequently observed in different cancer cells that can be associated with the development of cancer cell phenotypic traits such as sustained proliferation, migration and invasion, apoptosis resistance and metabolic reprograming. DNMT2/TRDMT1 5-methylcytosine methyltransferase, initially classified as DNA methyltransferase, can methylate both tRNA and mRNA promoting tRNA stability and proper protein synthesis, and orchestrating DNA damage response (DDR) and DNA stability, respectively. TRDMT1 is associated with cancer progression as its levels can be elevated and its mutations can be observed in a number of cancer types. TRDMT1 gene knockout (KO) can sensitize cancer cells of different origin to radiotherapy and chemotherapy. In the present review paper, based on literature data, the physiological and pathophysiological roles of TRDMT1 in different biological systems are described with the emphasis on human normal and cancer cells. Potential TRDMT1 substrates, inhibitors and regulatory mechanisms of catalytic activity and cellular localization are also presented and evaluated. TRDMT1 as a novel promising target in anticancer therapy is proposed and discussed.

摘要

在不同癌细胞中经常观察到RNA修饰的受影响情况,这可能与癌细胞表型特征的发展相关,如持续增殖、迁移和侵袭、抗凋亡以及代谢重编程。DNMT2/TRDMT1 5-甲基胞嘧啶甲基转移酶最初被归类为DNA甲基转移酶,它可以使tRNA和mRNA甲基化,分别促进tRNA稳定性和正确的蛋白质合成,并协调DNA损伤反应(DDR)和DNA稳定性。TRDMT1与癌症进展相关,因为在多种癌症类型中都可以观察到其水平升高和突变。TRDMT1基因敲除(KO)可以使不同来源的癌细胞对放疗和化疗敏感。在本综述中,基于文献数据,描述了TRDMT1在不同生物系统中的生理和病理生理作用,重点是人类正常细胞和癌细胞。还介绍并评估了TRDMT1的潜在底物、抑制剂以及催化活性和细胞定位的调节机制。提出并讨论了TRDMT1作为抗癌治疗中一个有前景的新靶点。

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