首页> 外文期刊>Nucleic Acids Research >The cyclin-dependent kinase inhibitor p21 is regulated by RNA-binding protein PCBP4 via mRNA stability.
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The cyclin-dependent kinase inhibitor p21 is regulated by RNA-binding protein PCBP4 via mRNA stability.

机译:细胞周期蛋白依赖性激酶抑制剂p21受RNA结合蛋白PCBP4通过mRNA稳定性的调控。

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摘要

RNA-binding proteins (RBPs) play a major role in many post-transcriptional processes, including mRNA stability, alternative splicing and translation. PCBP4, also called MCG10, is an RBP belonging to the poly(C)-binding protein family and a target of p53 tumor suppressor. Ectopic expression of PCBP4 induces cell-cycle arrest in G2 and apoptosis. To identify RNA targets regulated by PCBP4 and further decipher its function, we generated multiple cell lines in which PCBP4 is either inducibly over-expressed or knocked down. We found that PCBP4 expression decreases cyclin-dependent kinase inhibitor p21 induction in response to DNA damage. We also provided evidence that PCBP4 regulates p21 expression independently of p53. In addition, we showed that a deficiency in PCBP4 enhances p21 induction upon DNA damage. To validate PCBP4 regulation of p21, we made PCBP4-deficient mice and showed that p21 expression is markedly increased in PCBP4-deficient primary mouse embryo fibroblasts compared to that in wild-type counterparts. Finally, we uncovered that PCBP4 binds to the 3'-UTR of p21 transcript in vitro and in vivo to regulate p21 mRNA stability. Taken together, we revealed that PCBP4 regulates both basal and stress-induced p21 expression through binding p21 3'-UTR and modulating p21 mRNA stability.
机译:RNA结合蛋白(RBP)在许多转录后过程中起着重要作用,包括mRNA稳定性,选择性剪接和翻译。 PCBP4,也称为MCG10,是一种RBP,属于poly(C)结合蛋白家族,是p53肿瘤抑制子的靶标。 PCBP4的异位表达诱导G2的细胞周期停滞和凋亡。为了鉴定受PCBP4调控的RNA靶标并进一步破译其功能,我们生成了多个细胞系,其中PCBP4被诱导性过表达或被敲除。我们发现,PCBP4表达降低了细胞周期蛋白依赖性激酶抑制剂p21对DNA损伤的诱导作用。我们还提供了PCBP4独立于p53调节p21表达的证据。另外,我们显示了PCBP4的缺乏会增强DNA损伤后的p21诱导。为了验证对p21的PCBP4调控,我们制备了PCBP4缺陷的小鼠,并表明与野生型对应物相比,PCBP4缺陷的原代小鼠胚胎成纤维细胞中p21的表达显着增加。最后,我们发现PCBP4在体内和体外与p21转录物的3'-UTR结合,以调节p21 mRNA的稳定性。综上所述,我们揭示了PCBP4通过结合p21 3'-UTR和调节p21 mRNA稳定性来调节基础和应激诱导的p21表达。

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