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BtaE 是一种黏附素,属于三聚体自转运家族,对于 Brucella suis 的完全毒力是必需的,并定义了一个特定的黏附极。

BtaE, an adhesin that belongs to the trimeric autotransporter family, is required for full virulence and defines a specific adhesive pole of Brucella suis.

机构信息

Fundación Instituto Leloir, IIBBA CONICET, Buenos Aires, Argentina.

出版信息

Infect Immun. 2013 Mar;81(3):996-1007. doi: 10.1128/IAI.01241-12. Epub 2013 Jan 14.

Abstract

Brucella is responsible for brucellosis, one of the most common zoonoses worldwide that causes important economic losses in several countries. Increasing evidence indicates that adhesion of Brucella spp. to host cells is an important step to establish infection. We have previously shown that the BmaC unipolar monomeric autotransporter mediates the binding of Brucella suis to host cells through cell-associated fibronectin. Our genome analysis shows that the B. suis genome encodes several additional potential adhesins. In this work, we characterized a predicted trimeric autotransporter that we named BtaE. By expressing btaE in a nonadherent Escherichia coli strain and by phenotypic characterization of a B. suis ΔbtaE mutant, we showed that BtaE is involved in the binding of B. suis to hyaluronic acid. The B. suis ΔbtaE mutant exhibited a reduction in the adhesion to HeLa and A549 epithelial cells compared with the wild-type strain, and it was outcompeted by the wild-type strain in the binding to HeLa cells. The knockout btaE mutant showed an attenuated phenotype in the mouse model, indicating that BtaE is required for full virulence. BtaE was immunodetected on the bacterial surface at one cell pole. Using old and new pole markers, we observed that both the BmaC and BtaE adhesins are consistently associated with the new cell pole, suggesting that, in Brucella, the new pole is functionally differentiated for adhesion. This is consistent with the inherent polarization of this bacterium, and its role in the invasion process.

摘要

布鲁氏菌可引起布鲁氏菌病,这是一种全球最常见的动物源性传染病之一,在多个国家造成了重大经济损失。越来越多的证据表明,布鲁氏菌属黏附宿主细胞是建立感染的重要步骤。我们之前已经表明,BmaC 单极单体型自转运蛋白通过细胞相关纤维连接蛋白介导猪布鲁氏菌与宿主细胞的结合。我们的基因组分析表明,猪布鲁氏菌基因组编码了几个额外的潜在黏附素。在这项工作中,我们鉴定了一种预测的三聚体自转运蛋白,我们将其命名为 BtaE。通过在非黏附性大肠杆菌菌株中表达 btaE 并对 B. suis ΔbtaE 突变体进行表型特征分析,我们表明 BtaE 参与了 B. suis 与透明质酸的结合。与野生型菌株相比,B. suis ΔbtaE 突变体在黏附 HeLa 和 A549 上皮细胞方面表现出减少,并且在与 HeLa 细胞的结合中被野生型菌株竞争淘汰。敲除 btaE 突变体在小鼠模型中表现出减毒表型,表明 BtaE 是完全毒力所必需的。BtaE 在细菌表面的一个细胞极被免疫检测到。使用新旧极标记物,我们观察到 BmaC 和 BtaE 黏附素都与新的细胞极一致相关,这表明在布鲁氏菌中,新的细胞极在黏附功能上是有差异的。这与该细菌的固有极化及其在入侵过程中的作用一致。

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