Progression of m6A in the tumor microenvironment: hypoxia, immune and metabolic reprogramming

Author:

Han Xuan,Zhu Yu,Ke Juan,Zhai Yufeng,Huang Min,Zhang Xin,He Hongjie,Zhang Xiaojing,Zhao Xuehong,Guo Kaikai,Li Xianglin,Han Zhongyu,Zhang YanmingORCID

Abstract

AbstractRecently, N6-methyladenosine (m6A) has aroused widespread discussion in the scientific community as a mode of RNA modification. m6A comprises writers, erasers, and readers, which regulates RNA production, nuclear export, and translation and is very important for human health. A large number of studies have found that the regulation of m6A is closely related to the occurrence and invasion of tumors, while the homeostasis and function of the tumor microenvironment (TME) determine the occurrence and development of tumors to some extent. TME is composed of a variety of immune cells (T cells, B cells, etc.) and nonimmune cells (tumor-associated mesenchymal stem cells (TA-MSCs), cancer-associated fibroblasts (CAFs), etc.). Current studies suggest that m6A is involved in regulating the function of various cells in the TME, thereby affecting tumor progression. In this manuscript, we present the composition of m6A and TME, the relationship between m6A methylation and characteristic changes in TME, the role of m6A methylation in TME, and potential therapeutic strategies to provide new perspectives for better treatment of tumors in clinical work.

Publisher

Springer Science and Business Media LLC

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