mRNA m5C inhibits adipogenesis and promotes myogenesis by respectively facilitating YBX2 and SMO mRNA export in ALYREF-m5C manner

肌发生 脂肪生成 信使核糖核酸 生物 内分泌学 脂肪组织 化学 内科学 分子生物学 生物化学 骨骼肌 基因 医学
作者
Youhua Liu,Ying Yang,Ruifan Wu,Chun‐Chun Gao,Xing Liao,Xiao Han,Botao Zeng,Chaoqun Huang,Yaojun Luo,Yuxi Liu,Yushi Chen,Wei Chen,Jiaqi Liu,Qin Jiang,Yuanling Zhao,Zhen Bi,Guanqun Guo,Yongxi Yao,Yun Xiang,Xiaojun Zhang,Teresa G. Valencak,Yizhen Wang,Xinxia Wang
出处
期刊:Cellular and Molecular Life Sciences [Springer Nature]
卷期号:79 (9) 被引量:13
标识
DOI:10.1007/s00018-022-04474-0
摘要

Although 5-methylcytosine (m5C) has been identified as a novel and abundant mRNA modification and associated with energy metabolism, its regulation function in adipose tissue and skeletal muscle is still limited. This study aimed at investigating the effect of mRNA m5C on adipogenesis and myogenesis using Jinhua pigs (J), Yorkshire pigs (Y) and their hybrids Yorkshire–Jinhua pigs (YJ). We found that Y grow faster than J and YJ, while fatness-related characteristics observed in Y were lower than those of J and YJ. Besides, total mRNA m5C levels and expression rates of NSUN2 were higher both in backfat layer (BL) and longissimus dorsi muscle (LDM) of Y compared to J and YJ, suggesting that higher mRNA m5C levels positively correlate with lower fat and higher muscle mass. RNA bisulfite sequencing profiling of m5C revealed tissue-specific and dynamic features in pigs. Functionally, hyper-methylated m5C-containing genes were enriched in pathways linked to impaired adipogenesis and enhanced myogenesis. In in vitro, m5C inhibited lipid accumulation and promoted myogenic differentiation. Furthermore, YBX2 and SMO were identified as m5C targets. Mechanistically, YBX2 and SMO mRNAs with m5C modification were recognized and exported into the cytoplasm from the nucleus by ALYREF, thus leading to increased YBX2 and SMO protein expression and thereby inhibiting adipogenesis and promoting myogenesis, respectively. Our work uncovered the critical role of mRNA m5C in regulating adipogenesis and myogenesis via ALYREF-m5C-YBX2 and ALYREF-m5C-SMO manners, providing a potential therapeutic target in the prevention and treatment of obesity, skeletal muscle dysfunction and metabolic disorder diseases.
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