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首页> 外文期刊>Microbiology >Down-regulation of PE11, a cell wall associated esterase, enhances the biofilm growth of Mycobacterium tuberculosis and reduces cell wall virulence lipid levels
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Down-regulation of PE11, a cell wall associated esterase, enhances the biofilm growth of Mycobacterium tuberculosis and reduces cell wall virulence lipid levels

机译:PE11(一种与细胞壁相关的酯酶)的下调可增强结核分枝杆菌的生物膜生长并降低细胞壁的毒性脂质水平

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PE11 (Rv1169c or LipX) is a cell wall associated esterase/lipase of Mycobacterium tuberculosis (Mtb). Evidences suggest that PE11 is expressed by Mtb both in vitro and in vivo. Previous studies have shown that PE11 leads to modification in cell wall lipid content and enhanced virulence when expressed in the non-pathogenic surrogate Mycobacterium smegmatis. Since cell wall lipids often play different roles in pathogenic and non-pathogenic mycobacteria, we investigated the role of PE11 in its host, Mtb. Mtb with lowered expression of PE11 (PE11 knock-down) displayed significant changes in colony morphology and cell wall lipid profile, confirming the role of PE11 in cell wall architecture. In addition, the levels of phthiocerol dimycocerosates, a cell wall virulence factor, were decreased. Levels of trehalose esters and free mycolic acids were increased. In contrast to M. smegmatis expressing Mtb PE11, a role reversal was observed in Mtb with respect to pellicle/biofilm formation. The PE11 knock-down Mtb strain showed significantly enhanced aggregation and early biofilm growth in detergent-free medium, compared to the wild-type. Knock-down strain also showed nearly 27-fold up-regulation of a fibronectin attachment protein (Rv1759c), linking biofilm growth with over-expression of bacterial proteins that help in aggregation and/or binding to host extracellular matrix. The knock-down also resulted in poor virulence of Mtb in PMA (phorbol 12-myristate 13-acetate) treated and PMA+IFN-γ treated THP-1 macrophages. Therefore, the study not only links PE11 to cell wall virulence lipids but also reveals the involvement of this cell wall associated esterase in down-regulation of biofilm in Mtb.
机译:PE11(Rv1169c或LipX)是结核分枝杆菌(Mtb)的细胞壁相关酯酶/脂肪酶。有证据表明PE11在体外和体内均由Mtb表达。先前的研究表明,当在非病原性替代性耻垢分枝杆菌中表达时,PE11会导致细胞壁脂质含量的修饰和增强的毒力。由于细胞壁脂质在致病性和非致病性分枝杆菌中通常发挥不同的作用,因此我们研究了PE11在其宿主Mtb中的作用。降低PE11表达的Mtb(敲低PE11)显示出集落形态和细胞壁脂质分布的显着变化,证实了PE11在细胞壁结构中的作用。另外,降低了细胞壁毒力因子-苯二酚二椰油酸酯的水平。海藻糖酯和游离霉菌酸的水平增加。与表达Mtb PE11的耻垢分枝杆菌相反,在Mtb中观察到了膜/生物膜形成的作用反转。与野生型相比,在不含洗涤剂的培养基中,PE11敲低的Mtb菌株显示出显着增强的聚集和早期生物膜生长。敲除菌株还显示了纤连蛋白附着蛋白(Rv1759c)的近27倍上调,将生物膜的生长与细菌蛋白的过表达联系在一起,从而有助于聚集和/或结合宿主细胞外基质。敲低还导致在PMA(佛波醇12-肉豆蔻酸酯13-乙酸酯)处理和PMA +IFN-γ处理的THP-1巨噬细胞中Mtb的毒力较差。因此,该研究不仅将PE11与细胞壁毒性脂质相关联,而且还揭示了该细胞壁相关酯酶参与下调Mtb生物膜的作用。

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