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纤溶酶原结合A群链球菌M蛋白家族的差异:结合位点的功能保守性及变异体免疫选择的潜在作用

Divergence in the plasminogen-binding group a streptococcal M protein family: functional conservation of binding site and potential role for immune selection of variants.

作者信息

Sanderson-Smith Martina, Batzloff Michael, Sriprakash Kabada S, Dowton Mark, Ranson Marie, Walker Mark J

机构信息

School of Biological Sciences, University of Wollongong, Wollongong, New South Wales 2522, Australia.

出版信息

J Biol Chem. 2006 Feb 10;281(6):3217-26. doi: 10.1074/jbc.M508758200. Epub 2005 Nov 30.

DOI:10.1074/jbc.M508758200
PMID:16319056
Abstract

Group A streptococci (GAS) display receptors for the human zymogen plasminogen on the cell surface, one of which is the plasminogen-binding group A streptococcal M protein (PAM). Characterization of PAM genes from 12 GAS isolates showed significant variation within the plasminogen-binding repeat motifs (a1/a2) of this protein. To determine the impact of sequence variation on protein function, recombinant proteins representing five naturally occurring variants of PAM, together with a recombinant M1 protein, were expressed and purified. Equilibrium dissociation constants for the interaction of PAM variants with biotinylated Glu-plasminogen ranged from 1.58 to 4.99 nm. Effective concentrations of prototype PAM required for 50% inhibition of plasminogen binding to immobilized PAM variants ranged from 0.68 to 22.06 nm. These results suggest that although variation in the a1/a2 region of the PAM protein does affect the comparative affinity of PAM variants, the functional capacity to bind plasminogen is conserved. Additionally, a potential role for the a1 region of PAM in eliciting a protective immune response was investigated by using a mouse model for GAS infection. The a1 region of PAM was found to protect immunized mice challenged with a PAM-positive GAS strain. These data suggest a link between selective immune pressure against the plasminogen-binding repeats and the functional conservation of the binding domain in PAM variants.

摘要

A组链球菌(GAS)在细胞表面表达人酶原纤溶酶原的受体,其中之一是纤溶酶原结合A组链球菌M蛋白(PAM)。对12株GAS分离株的PAM基因进行表征,结果显示该蛋白的纤溶酶原结合重复基序(a1/a2)存在显著变异。为了确定序列变异对蛋白质功能的影响,表达并纯化了代表PAM五种天然变体的重组蛋白以及重组M1蛋白。PAM变体与生物素化的谷氨酸纤溶酶原相互作用的平衡解离常数在1.58至4.99纳米之间。50%抑制纤溶酶原与固定化PAM变体结合所需的原型PAM有效浓度在0.68至22.06纳米之间。这些结果表明,尽管PAM蛋白a1/a2区域的变异确实会影响PAM变体的相对亲和力,但结合纤溶酶原的功能能力是保守的。此外,通过使用GAS感染的小鼠模型,研究了PAM的a1区域在引发保护性免疫反应中的潜在作用。发现PAM的a1区域可保护用PAM阳性GAS菌株攻击的免疫小鼠。这些数据表明,针对纤溶酶原结合重复序列的选择性免疫压力与PAM变体中结合域的功能保守性之间存在联系。

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