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首页> 外文期刊>Cell Reports >SRSF10 Plays a Role in Myoblast Differentiation and Glucose Production via Regulation of Alternative Splicing
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SRSF10 Plays a Role in Myoblast Differentiation and Glucose Production via Regulation of Alternative Splicing

机译:SRSF10通过调控选择性剪接在成肌细胞分化和葡萄糖产生中发挥作用

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Alternative splicing is a major mechanism of controlling gene expression and protein diversity in higher eukaryotes. We report that the splicing factor SRSF10 functions during striated muscle development, myoblast differentiation, and glucose production both in cells and in mice. A combination of RNA-sequencing and molecular analysis allowed us to identify muscle-specific splicing events controlled by SRSF10 that are critically involved in striated muscle development. Inclusion of alternative exons 16 and 17 of Lrrfip1 is a muscle-specific event that is activated by SRSF10 and essential for myoblast differentiation. On the other hand, in mouse primary hepatocytes, PGC1@a is a key target of SRSF10 that regulates glucose production by fasting. SRSF10 represses inclusion of PGC1@a exon 7a and facilitates the production of functional protein. The results highlight the biological significance of SRSF10 and regulated alternative splicing in vivo.
机译:选择性剪接是控制高级真核生物中基因表达和蛋白质多样性的主要机制。我们报告说,在细胞和小鼠中横纹肌发育,成肌细胞分化和葡萄糖生成过程中,剪接因子SRSF10起作用。 RNA测序和分子分析相结合,使我们能够确定由SRSF10控制的特定于肌肉的剪接事件,这些事件与横纹肌的发育至关重要。包含Lrrfip1的其他外显子16和17是由SRSF10激活的肌肉特定事件,是成肌细胞分化所必需的。另一方面,在小鼠原代肝细胞中,PGC1 @ a是SRSF10的关键靶标,它通过禁食来调节葡萄糖的产生。 SRSF10抑制PGC1 @ a外显子7a的包含并促进功能蛋白的产生。结果突出了SRSF10的生物学意义和体内调控的选择性剪接。

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