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结核分枝杆菌三酰甘油水解酶LipY的PE结构域的功能作用及免疫原性

Functional role of the PE domain and immunogenicity of the Mycobacterium tuberculosis triacylglycerol hydrolase LipY.

作者信息

Mishra Kanhu C, de Chastellier Chantal, Narayana Yeddula, Bifani Pablo, Brown Alistair K, Besra Gurdyal S, Katoch Vishwa M, Joshi Beenu, Balaji Kithiganahalli N, Kremer Laurent

机构信息

Laboratoire de Dynamique des Interactions Membranaires Normales et Pathologiques, Université de Montpellier II et I, CNRS, UMR 5235, case 107, Place Eugène Bataillon, 34095 Montpellier Cedex 05, France.

出版信息

Infect Immun. 2008 Jan;76(1):127-40. doi: 10.1128/IAI.00410-07. Epub 2007 Oct 15.

Abstract

PE and PPE proteins appear to be important for virulence and immunopathogenicity in mycobacteria, yet the functions of the PE/PPE domains remain an enigma. To decipher the role of these domains, we have characterized the triacylglycerol (TAG) hydrolase LipY from Mycobacterium tuberculosis, which is the only known PE protein expressing an enzymatic activity. The overproduction of LipY in mycobacteria resulted in a significant reduction in the pool of TAGs, consistent with the lipase activity of this enzyme. Unexpectedly, this reduction was more pronounced in mycobacteria overexpressing LipY lacking the PE domain [LipY(deltaPE)], suggesting that the PE domain participates in the modulation of LipY activity. Interestingly, Mycobacterium marinum contains a protein homologous to LipY, termed LipY(mar), in which the PE domain is substituted by a PPE domain. As for LipY, overexpression of LipY(mar) in Mycobacterium smegmatis significantly reduced the TAG pool, and this was further pronounced when the PPE domain of LipY(mar) was removed. Fractionation studies and Western blot analysis demonstrated that both LipY and LipY(deltaPE) were mainly present in the cell wall, indicating that the PE domain was not required for translocation to this site. Furthermore, electron microscopy immunolabeling of LipY(deltaPE) clearly showed a cell surface localization, thereby suggesting that the lipase may interact with the host immune system. Accordingly, a strong humoral response against LipY and LipY(deltaPE) was observed in tuberculosis patients. Together, our results suggest for the first time that both PE and PPE domains can share similar functional roles and that LipY represents a novel immunodominant antigen.

摘要

PE和PPE蛋白似乎对分枝杆菌的毒力和免疫致病性很重要,然而PE/PPE结构域的功能仍是个谜。为了解析这些结构域的作用,我们对结核分枝杆菌的三酰甘油(TAG)水解酶LipY进行了表征,它是唯一已知具有酶活性的PE蛋白。在分枝杆菌中过量表达LipY导致TAG池显著减少,这与该酶的脂肪酶活性一致。出乎意料的是,这种减少在过表达缺乏PE结构域的LipY [LipY(δPE)]的分枝杆菌中更为明显,表明PE结构域参与了LipY活性的调节。有趣的是,海分枝杆菌含有一种与LipY同源的蛋白,称为LipY(mar),其中PE结构域被一个PPE结构域取代。与LipY一样,在耻垢分枝杆菌中过表达LipY(mar)显著减少了TAG池,当去除LipY(mar)的PPE结构域时,这种情况更加明显。分级分离研究和蛋白质印迹分析表明,LipY和LipY(δPE)都主要存在于细胞壁中,这表明PE结构域对于转运到该位点不是必需的。此外,LipY(δPE)的电子显微镜免疫标记清楚地显示了细胞表面定位,从而表明脂肪酶可能与宿主免疫系统相互作用。因此,在结核病患者中观察到了针对LipY和LipY(δPE)的强烈体液反应。总之,我们的结果首次表明PE和PPE结构域可以发挥相似的功能作用,并且LipY代表一种新的免疫显性抗原。

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