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首页> 外文期刊>Biochimica et Biophysica Acta. Gene Regulatory Mechanisms >SRSF2 promotes splicing and transcription of exon 11 included isoform in Ron proto-oncogene
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SRSF2 promotes splicing and transcription of exon 11 included isoform in Ron proto-oncogene

机译:SRSF2促进外显子11的剪接和转录包括在RON proto-oncogene中的同种型

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摘要

The product of proto-oncogene Ron is a human receptor for the macrophage-stimulating protein (MSP). Upon activation, Ron is able to induce cell dissociation, migration and matrix invasion. Exon 11 skipping of Ron pre-mRNA produces Ronδ165 protein that is constitutively active even in the absence of its ligand. Here we show that knockdown of SRSF2 promotes the decrease of exon 11 inclusion, whereas overexpression of SRSF2 promotes exon 11 inclusion. We demonstrate that SRSF2 promotes exon 11 inclusion through splicing and transcription procedure. We also present evidence that reduced expression of SRSF2 induces a decrease in the splicing of both introns 10 and 11; by contrast, overexpression of SRSF2 induces an increase in the splicing of introns 10 and 11. Through mutation analysis, we show that SRSF2 functionally targets and physically interacts with CGAG sequence on exon 11. In addition, we reveal that the weak strength of splice sites of exon 11 is not required for the function of SRSF2 on the splicing of Ron exon 11. Our results indicate that SRSF2 promotes exon 11 inclusion of Ron proto-oncogene through targeting exon 11. Our study provides a novel mechanism by which Ron is expressed.
机译:原癌烯RON的产物是巨噬细胞刺激蛋白(MSP)的人受体。激活后,RON能够诱导细胞解离,迁移和基质侵袭。外显子11 RON前mRNA的跳跃产生ronδ165蛋白,即使在没有其配体的情况下也是组成型活性的。在这里,我们表明SRSF2的敲低促进了外显子11的含量减少,而SRSF2的过度表达促进外显子11夹杂物。我们证明SRSF2通过剪接和转录程序促进外显子11夹杂物。我们还提出了证据表明SRSF2的表达减少诱导内含子10和11的拼接减少;相比之下,SRSF2的过度表达诱导内含子10和11的剪接增加。通过突变分析,我们表明SRSF2功能靶向并与外显子11上的CGAG序列物理地相互作用。另外,我们揭示了剪接位点的弱强度SRSF2在RON外显子11拼接的情况下不需要外显子11.我们的结果表明SRSF2通过靶向外显子11促进外显子11含有RON原癌基因11.我们的研究提供了一种新的机制,提供了RON的新机制。

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  • 作者单位

    School of Life Sciences Gwangju Institute of Science and TechnologyGwangju South Korea;

    School of Life Sciences Gwangju Institute of Science and TechnologyGwangju South Korea;

    School of Life Sciences Gwangju Institute of Science and TechnologyGwangju South Korea;

    School of Life Sciences Gwangju Institute of Science and TechnologyGwangju South Korea;

    School of Life Sciences Gwangju Institute of Science and TechnologyGwangju South Korea;

    JiangSu Key Laboratory of Neuroregeneration Nantong UniversityNantong China;

    Department of Bioscience and Biotechnology Sejong UniversitySeoul South Korea;

    Hormel Institute University of MinnesotaAustin MN United States;

    School of Life Sciences Gwangju Institute of Science and TechnologyGwangju South Korea;

    School of Life Sciences Gwangju Institute of Science and TechnologyGwangju South Korea;

    Istituto di Genetica Molecolare Consiglio Nazionale delle Ricerche via Abbiategrasso 207Pavia;

    Istituto di Genetica Molecolare Consiglio Nazionale delle Ricerche via Abbiategrasso 207Pavia;

    Howard Hughes Medical Institute and Programs in Gene Function and Expression and Molecular Medicine;

    School of Life Sciences Gwangju Institute of Science and TechnologyGwangju South Korea;

    School of Life Sciences Gwangju Institute of Science and TechnologyGwangju South Korea;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 分子生物学;
  • 关键词

    Exon 11 inclusion; Pre-mRNA splicing; Proto-oncogene; Ron; SRSF2; Transcription;

    机译:外显子11夹杂物;前mRNA拼接;PROTO- oncogene;RON;SRSF2;转录;

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