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脂磷壁酸和M蛋白:A组链球菌的双重黏附素

Lipoteichoic acid and M protein: dual adhesins of group A streptococci.

作者信息

Courtney H S, von Hunolstein C, Dale J B, Bronze M S, Beachey E H, Hasty D L

机构信息

Veterans Affairs Medical Center Research Service, Memphis, TN 38104.

出版信息

Microb Pathog. 1992 Mar;12(3):199-208. doi: 10.1016/0882-4010(92)90054-r.

Abstract

The roles of lipoteichoic acid (LTA) and M protein in the adherence of group A streptococci to human cells were investigated. Both M+ and M- streptococci bound to pharyngeal and buccal epithelial cells in similar numbers. Streptococcal attachment was inhibited by LTA, but not by the pepsin-extracted, amino-terminal half of M protein (pep M), suggesting that M protein does not mediate attachment to these cells. However, a purified, recombinant, intact M protein did block attachment of streptococci to buccal cells. Using synthetic peptides, the inhibitory domain was localized to a region of intact M protein that is within or near the bacterial cell wall. Evidence is presented to suggest that on the surface of streptococci this region of the M protein is probably not accessible for interactions with host cell receptors and that M protein does not mediate attachment to buccal or pharyngeal cells. In contrast, approximately 10-times more M+ streptococci bound to Hep-2 cells than did M- streptococci and pep M protein blocked binding of streptococci to Hep-2 cells. The data suggest that at least two streptococcal adhesins, LTA and M protein, are involved in the adherence of streptococci to certain cells and that the relative contributions of these adhesins to the attachment process depends on the type of host cells used to study adherence.

摘要

研究了脂磷壁酸(LTA)和M蛋白在A组链球菌与人细胞黏附中的作用。M⁺和M⁻链球菌与咽部和颊部上皮细胞的结合数量相似。链球菌的黏附受到LTA的抑制,但不受胃蛋白酶提取的M蛋白氨基末端一半(pep M)的抑制,这表明M蛋白不介导与这些细胞的黏附。然而,纯化的重组完整M蛋白确实能阻止链球菌与颊细胞的黏附。使用合成肽,抑制结构域定位于完整M蛋白位于细菌细胞壁内或附近的区域。有证据表明,在链球菌表面,M蛋白的这个区域可能无法与宿主细胞受体相互作用,并且M蛋白不介导与颊部或咽部细胞的黏附。相比之下,与M⁻链球菌相比,M⁺链球菌与Hep-2细胞的结合量大约多10倍,并且pep M蛋白可阻止链球菌与Hep-2细胞的结合。数据表明,至少两种链球菌黏附素,即LTA和M蛋白,参与了链球菌与某些细胞的黏附,并且这些黏附素对黏附过程的相对贡献取决于用于研究黏附的宿主细胞类型。

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