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耻垢分枝杆菌产生一种与上皮细胞黏附无关的HBHA同源物。

Mycobacterium smegmatis produces an HBHA homologue which is not involved in epithelial adherence.

作者信息

Biet Franck, Angela de Melo Marques Maria, Grayon Maggy, Xavier da Silveira Erika Kopp, Brennan Patrick J, Drobecq Hervé, Raze Dominique, Vidal Pessolani Maria Cristina, Locht Camille, Menozzi Franco Dante

机构信息

UR1282, Infectiologie Animale, Santé Publique (IASP-311), INRA Centre de Tours, F-37380 Nouzilly France.

出版信息

Microbes Infect. 2007 Feb;9(2):175-82. doi: 10.1016/j.micinf.2006.11.007. Epub 2006 Dec 12.

DOI:10.1016/j.micinf.2006.11.007
PMID:17208488
Abstract

Mycobacterium tuberculosis produces heparin-binding hemagglutinin (TB-HBHA), an adhesin involved in binding to non-professional phagocytes and in extrapulmonary dissemination. TB-HBHA binds sulphated glycoconjugates through its C-terminal lysine-rich domain and can be purified by heparin-Sepharose chromatography. Homologues of HBHA are found in other pathogenic mycobacteria, but previous investigations failed to demonstrate them in non-pathogenic Mycobacterium smegmatis. We identified a gene encoding a HBHA-like protein, named MS-HBHA, from the complete M. smegmatis genome. The deduced MS-HBHA amino acid sequence revealed 68% identity with that of TB-HBHA and contains lysine-rich repeats in its C-terminal domain. However, in contrast to TB-HBHA, the lysine-rich domain of MS-HBHA is preceded by a stretch of acidic residues. This difference likely explains the low affinity for heparin displayed by MS-HBHA compared to TB-HBHA. Isolation by heparin-Sepharose chromatography procedure and mass spectrometry analysis indicated that MS-HBHA, similar to TB-HBHA contains several methylated lysine residues in its C-terminal domain. Although MS-HBHA is associated with M. smegmatis cell wall fractions, it does not seem to play a role in epithelial adherence and its function remains unknown. We therefore conclude that TB-HBHA may have evolved as an adhesin in pathogenic mycobacteria from a homolog that serves a different function in a saprophytic mycobacterium.

摘要

结核分枝杆菌产生肝素结合血凝素(TB-HBHA),这是一种黏附素,参与与非专职吞噬细胞的结合以及肺外播散。TB-HBHA通过其富含赖氨酸的C末端结构域与硫酸化糖缀合物结合,并且可以通过肝素-琼脂糖层析进行纯化。在其他致病性分枝杆菌中发现了HBHA的同源物,但先前的研究未能在非致病性耻垢分枝杆菌中证实它们的存在。我们从耻垢分枝杆菌的完整基因组中鉴定出一个编码HBHA样蛋白的基因,命名为MS-HBHA。推导的MS-HBHA氨基酸序列与TB-HBHA的序列有68%的同一性,并且在其C末端结构域中含有富含赖氨酸的重复序列。然而,与TB-HBHA不同的是,MS-HBHA富含赖氨酸的结构域之前有一段酸性残基。这种差异可能解释了与TB-HBHA相比,MS-HBHA对肝素的亲和力较低的原因。通过肝素-琼脂糖层析程序分离和质谱分析表明,与TB-HBHA类似,MS-HBHA在其C末端结构域中含有几个甲基化的赖氨酸残基。尽管MS-HBHA与耻垢分枝杆菌细胞壁组分相关,但它似乎在上皮细胞黏附中不起作用,其功能仍然未知。因此,我们得出结论,TB-HBHA可能是从在腐生分枝杆菌中发挥不同功能的同源物进化而来的致病性分枝杆菌中的一种黏附素。

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