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鉴定伯氏疏螺旋体 OspC 蛋白配体结合域 1(LBD1)中对在哺乳动物环境中发挥功能所需的残基。

Identification of residues within ligand-binding domain 1 (LBD1) of the Borrelia burgdorferi OspC protein required for function in the mammalian environment.

机构信息

Department of Microbiology and Immunology, Medical College of Virginia at Virginia Commonwealth University, Richmond, VA, USA.

出版信息

Mol Microbiol. 2010 Apr;76(2):393-408. doi: 10.1111/j.1365-2958.2010.07103.x. Epub 2010 Feb 28.

Abstract

Borrelia burgdorferi outer surface protein C (ospC) is required for the establishment of infection in mammals. However, its precise function remains controversial. The biologically active form of OspC appears to be a homodimer. Alpha helix 1 and 1' of the apposing monomers form a solvent-accessible pocket at the dimeric interface that presents a putative ligand-binding domain (LBD1). Here we employ site-directed and allelic-exchange mutagenesis to test the hypothesis that LBD1 is a determinant of OspC function in the mammalian environment. Substitution of residues K60, E61 and E63 which line LBD1 resulted in the loss of infectivity or influenced dissemination. Analyses of the corresponding recombinant proteins demonstrated that the loss of function was not due to structural perturbation, impaired dimer formation or the loss of plasminogen binding. This study is the first to assess the involvement of individual residues and domains of OspC in its in vivo function. The data support the hypothesis that OspC interacts with a mammalian derived ligand that is critical for survival during early infection. These results shed new light on the structure-functions relationships of OspC and challenge existing hypotheses regarding OspC function in mammals.

摘要

伯氏疏螺旋体外表面蛋白 C(ospC)是在哺乳动物中建立感染所必需的。然而,其确切功能仍存在争议。OspC 的生物活性形式似乎是同源二聚体。相邻单体的α螺旋 1 和 1'在二聚体界面形成一个溶剂可及的口袋,呈现一个假定的配体结合域(LBD1)。在这里,我们采用定点和等位基因交换诱变来检验这样一个假设,即 LBD1 是 ospC 在哺乳动物环境中功能的决定因素。排列在 LBD1 上的残基 K60、E61 和 E63 的取代导致了感染力的丧失或传播的影响。对相应重组蛋白的分析表明,功能丧失不是由于结构扰动、二聚体形成受损或纤溶酶原结合丧失所致。这项研究首次评估了 ospC 中单个残基和结构域在其体内功能中的参与情况。这些数据支持 ospC 与一种哺乳动物衍生配体相互作用的假设,这种配体对于早期感染期间的存活至关重要。这些结果为 ospC 的结构-功能关系提供了新的认识,并挑战了 ospC 在哺乳动物中功能的现有假设。

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