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HuR/YB1 复合物的形成对于稳定靶 mRNA 以促进成肌作用是必需的。

The formation of HuR/YB1 complex is required for the stabilization of target mRNA to promote myogenesis.

机构信息

KAUST Smart-Health Initiative King Abdullah University of Science and Technology (KAUST), Jeddah, Saudi Arabia.

KAUST Biological Environmental Science and Engineering (BESE) Division, King Abdullah University of Science and Technology (KAUST), Jeddah, Saudi Arabia.

出版信息

Nucleic Acids Res. 2023 Feb 22;51(3):1375-1392. doi: 10.1093/nar/gkac1245.

Abstract

mRNA stability is the mechanism by which cells protect transcripts allowing their expression to execute various functions that affect cell metabolism and fate. It is well-established that RNA binding proteins (RBPs) such as HuR use their ability to stabilize mRNA targets to modulate vital processes such as muscle fiber formation (myogenesis). However, the machinery and the mechanisms regulating mRNA stabilization are still elusive. Here, we identified Y-Box binding protein 1 (YB1) as an indispensable HuR binding partner for mRNA stabilization and promotion of myogenesis. Both HuR and YB1 bind to 409 common mRNA targets, 147 of which contain a U-rich consensus motif in their 3' untranslated region (3'UTR) that can also be found in mRNA targets in other cell systems. YB1 and HuR form a heterodimer that associates with the U-rich consensus motif to stabilize key promyogenic mRNAs. The formation of this complex involves a small domain in HuR (227-234) that if mutated prevents HuR from reestablishing myogenesis in siHuR-treated muscle cells. Together our data uncover that YB1 is a key player in HuR-mediated stabilization of pro-myogenic mRNAs and provide the first indication that the mRNA stability mechanism is as complex as other key cellular processes such as mRNA decay and translation.

摘要

mRNA 的稳定性是细胞保护转录本的机制,使它们的表达能够执行各种影响细胞代谢和命运的功能。众所周知,RNA 结合蛋白(RBPs)如 HuR 利用其稳定 mRNA 靶标来调节重要过程的能力,如肌肉纤维形成(成肌作用)。然而,调节 mRNA 稳定性的机制和机制仍然难以捉摸。在这里,我们确定 Y 盒结合蛋白 1 (YB1) 是 HuR 稳定 mRNA 和促进成肌作用所必需的结合伙伴。HuR 和 YB1 都结合到 409 个共同的 mRNA 靶标上,其中 147 个靶标在其 3'非翻译区(3'UTR)中含有富含 U 的保守基序,该基序也可以在其他细胞系统中的 mRNA 靶标中找到。YB1 和 HuR 形成异二聚体,与富含 U 的保守基序结合,稳定关键的成肌 mRNA。该复合物的形成涉及 HuR 中的一个小结构域(227-234),如果该结构域发生突变,会阻止 HuR 在 siHuR 处理的肌肉细胞中重新建立成肌作用。我们的数据揭示了 YB1 是 HuR 介导的促肌生成 mRNA 稳定性的关键因子,并首次表明 mRNA 稳定性机制与其他关键细胞过程(如 mRNA 衰变和翻译)一样复杂。

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