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首页> 外文期刊>Nucleic Acids Research >Crystal structure of Pseudomonas aeruginosa RsaL bound to promoter DNA reaffirms its role as a global regulator involved in quorum-sensing
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Crystal structure of Pseudomonas aeruginosa RsaL bound to promoter DNA reaffirms its role as a global regulator involved in quorum-sensing

机译:铜绿假单胞菌的晶体结构与启动子DNA结合的铜绿假单胞菌rsal重申其作为涉及批量传感的全球调节器的作用

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摘要

Pseudomonas aeruginosa possesses at least three well-defined quorum-sensing (QS) (las, rhl and pqs) systems that control a variety of important functions including virulence. RsaL is a QS repressor that reduces QS signal production and ensures homeostasis by functioning in opposition to LasR. However, its regulatory role in signal homeostasis remains elusive. Here, we conducted a ChIP-seq assay and revealed that RsaL bound to two new targets, the intergenic regions of PA2228/PA2229 and pqsH/cdpR, which are required for PQS synthesis. Deletion of rsaL reduced transcription of pqsH and cdpR, thus decreasing PQS signal production. The Delta rsaL strain exhibited increased pyocyanin production and reduced biofilm formation, which are dependent on CdpR or PqsH activity. In addition, we solved the structure of the RsaL-DNA complex at a 2.4 angstrom resolution. Although the overall sequence similarity is quite low, RsaL folds into a HTH-like structure, which is conserved among many transcriptional regulators. Complementation results of the rsaL knockout cells with different rsaL mutants further confirmed the critical role of the DNA-binding residues (including Arg20, Gln27, Gln38, Gly35, Ser37 and Ser42) that are essential for DNA binding. Our findings reveal new targets of RsaL and provide insight into the detailed characterization of the RsaL-DNA interaction.
机译:铜绿假单胞菌具有至少三种明确定义的仲裁(QS)(LAS,RHL和PQS)系统,可控制包括毒力的各种重要功能。 RSAL是一个QS压缩机,可减少QS信号产生,并通过反对LASR的运作来确保宿舍。然而,其在信号宿舍中的监管作用仍然难以捉摸。在这里,我们进行了一种芯片SEQ测定,并揭示了与PQS合成所需的PA2228 / PA2229和PQSH / CDPR的rsal结合的rsal。删除RSAL降低PQSH和CDPR的转录,从而降低PQS信号产生。 Delta Rsal菌株表现出富氰蛋白的产量和降低的生物膜形成,这取决于CDPR或PQSH活性。此外,我们解决了2.4埃分辨率的Rsal-DNA复合物的结构。虽然整体序列相似度非常低,Rsal折叠成一个类似的Hth样结构,但是在许多转录调节器之间被保守。具有不同RSAL突变体的RSAL敲除细胞的互补结果进一步证实了DNA结合残基(包括ARG20,GLN27,GLN38,GLY35,SER37和SER42)对DNA结合必需的关键作用。我们的研究结果揭示RSAL的新目标,并提供洞察RSAL-DNA相互作用的详细的表征。

著录项

  • 来源
    《Nucleic Acids Research》 |2017年第2期|共12页
  • 作者单位

    Northwest Univ Coll Life Sci Minist Educ Key Lab Resources Biol &

    Biotechnol Western China Xian 710069 Shaanxi Peoples R China;

    Fudan Univ Sch Life Sci Dept Physiol &

    Biophys Shanghai 200438 Peoples R China;

    Northwest Univ Coll Life Sci Minist Educ Key Lab Resources Biol &

    Biotechnol Western China Xian 710069 Shaanxi Peoples R China;

    Northwest Univ Coll Life Sci Minist Educ Key Lab Resources Biol &

    Biotechnol Western China Xian 710069 Shaanxi Peoples R China;

    Fudan Univ Sch Life Sci Dept Physiol &

    Biophys Shanghai 200438 Peoples R China;

    Northwest Univ Coll Life Sci Minist Educ Key Lab Resources Biol &

    Biotechnol Western China Xian 710069 Shaanxi Peoples R China;

    Northwest Univ Coll Life Sci Minist Educ Key Lab Resources Biol &

    Biotechnol Western China Xian 710069 Shaanxi Peoples R China;

    Northwest Univ Coll Life Sci Minist Educ Key Lab Resources Biol &

    Biotechnol Western China Xian 710069 Shaanxi Peoples R China;

    Northwest Univ Coll Life Sci Minist Educ Key Lab Resources Biol &

    Biotechnol Western China Xian 710069 Shaanxi Peoples R China;

    Northwest Univ Coll Life Sci Minist Educ Key Lab Resources Biol &

    Biotechnol Western China Xian 710069 Shaanxi Peoples R China;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 生物化学;
  • 关键词

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