首页> 外文期刊>Frontiers in Cellular and Infection Microbiology >Leptospira Immunoglobulin-Like Protein B Interacts with the 20th Exon of Human Tropoelastin Contributing to Leptospiral Adhesion to Human Lung Cells
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Leptospira Immunoglobulin-Like Protein B Interacts with the 20th Exon of Human Tropoelastin Contributing to Leptospiral Adhesion to Human Lung Cells

机译:钩端螺旋体免疫球蛋白样蛋白B与人类促弹性蛋白的第20外显子相互作用,促成钩端螺旋体对人肺细胞的粘附

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Leptospira immunoglobulin-like protein B (LigB), a surface adhesin, is capable of mediating the attachment of pathogenic leptospira to the host through interaction with various components of the extracellular matrix (ECM). Human tropoelastin (HTE), the building block of elastin, confers resilience and elasticity to lung and other tissues. Previously identified Ig-like domains of LigB, including LigB4 and LigB12, bind to HTE, which is likely to promote Leptospira adhesion to lung tissue. However, the molecular mechanism that mediates the LigB-HTE interaction is unclear. In this study, the LigB-binding site on HTE was further pinpointed to a N-terminal region of the 20th exon of HTE (HTE20N). Alanine mutants of basic and aromatic residues on HTE20N significantly reduced binding to the LigB. Additionally, HTE-binding site was narrowed down to the first β-sheet of LigB12. On this binding surface, residues F1054, D1061, A1065 and D1066 were critical for the association with HTE. Most importantly, the recombinant HTE truncates could diminish the binding of LigB to human lung fibroblasts (WI-38) by 68%, and could block the association of LigA-expressing L. biflexa to lung cells by 61%. These findings should expand our understanding of leptospiral pathogenesis, particularly in pulmonary manifestations of leptospirosis.
机译:钩端螺旋体免疫球蛋白样蛋白B(LigB)是一种表面粘附素,能够通过与细胞外基质(ECM)的各种成分相互作用介导病原性钩端螺旋体与宿主的附着。人类弹性蛋白(HTE)是弹性蛋白的组成部分,赋予肺和其他组织弹性和弹性。先前鉴定的LigB的Ig样结构域(包括LigB4和LigB12)与HTE结合,这可能会促进钩端螺旋体粘附到肺组织。但是,尚不清楚介导LigB-HTE相互作用的分子机制。在这项研究中,HTE上的LigB结合位点被进一步精确定位到HTE第20外显子(HTE20N)的N端区域。 HTE20N上碱性和芳香族残基的丙氨酸突变体显着降低了与LigB的结合。另外,将HTE结合位点缩小至LigB12的第一β-折叠。在该结合表面上,残基F1054,D1061,A1065和D1066对于与HTE缔合至关重要。最重要的是,重组HTE截短体可以使LigB与人肺成纤维细胞(WI-38)的结合减少68%,并可以使表达LigA biflexa与肺细胞的结合减少61%。这些发现应扩大我们对钩端螺旋体发病机理的理解,尤其是在钩端螺旋体病的肺部表现方面。

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