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同源二聚化和特定结构域与目标 DNA 的结合是 HlyU 调节人类病原体创伤弧菌毒力基因 rtxA1 表达所必需的,rtxA1 编码重复入毒素蛋白。

Homodimerization and binding of specific domains to the target DNA are essential requirements for HlyU to regulate expression of the virulence gene rtxA1, encoding the repeat-in-toxin protein in the human pathogen Vibrio vulnificus.

机构信息

Department of Molecular Microbiology and Immunology, Oregon Health and Science University, Portland, OR 97239, USA.

出版信息

J Bacteriol. 2011 Dec;193(24):6895-901. doi: 10.1128/JB.05950-11. Epub 2011 Oct 21.

Abstract

The virulence gene rtxA1, encoding the repeat-in-toxin protein, plays an essential role in the pathogenesis of Vibrio vulnificus infections. Expression of this gene is controlled by the HlyU regulator by direct contact of the DNA upstream of the rtxA1 toxin operon acting as a derepressor of the H-NS protein. The crystal structure suggests that HlyU forms a homodimer in vitro. However, knowledge of the biological implications of these findings in vivo is limited. In this work, we endeavored to dissect, using genetic and biochemical approaches, the domains of this protein that are essential for homodimer formation and the interaction of HlyU with the target DNA. We identified that residues L18, N22, R25, S54, Q55, L57, W59, R61, K70, and Y77 are essential for the HlyU protein binding to the DNA and that amino acids L17 and L91 are important for HlyU dimerization. We also determined that HlyU homodimer formation is an essential requirement for binding to the upstream region of the rtxA1 operon and is the key feature in relieving the H-NS repression of rtxA1 transcription.

摘要

毒力基因 rtxA1 编码重复入毒素蛋白,在创伤弧菌感染的发病机制中发挥重要作用。该基因的表达受 HlyU 调节子控制,通过 rtxA1 毒素操纵子上游的 DNA 直接接触,该 DNA 作为 H-NS 蛋白的去阻遏物发挥作用。晶体结构表明 HlyU 体外形成同源二聚体。然而,这些发现对体内生物学意义的了解有限。在这项工作中,我们试图通过遗传和生化方法来剖析该蛋白的结构域,这些结构域对于同源二聚体形成和 HlyU 与靶 DNA 的相互作用至关重要。我们确定 L18、N22、R25、S54、Q55、L57、W59、R61、K70 和 Y77 残基对于 HlyU 蛋白与 DNA 的结合是必需的,而 L17 和 L91 氨基酸对于 HlyU 二聚化很重要。我们还确定了 HlyU 同源二聚体的形成是结合 rtxA1 操纵子上游区域的必要条件,也是解除 H-NS 对 rtxA1 转录抑制的关键特征。

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