化脓性链球菌 1 群和 2b 群链激酶的功能差异由其β结构域决定。
Functional differences between Streptococcus pyogenes cluster 1 and cluster 2b streptokinases are determined by their β-domains.
机构信息
W.M. Keck Center for Transgene Research and Department of Chemistry and Biochemistry, University of Notre Dame, Notre Dame, IN 46556, USA.
出版信息
FEBS Lett. 2013 May 2;587(9):1304-9. doi: 10.1016/j.febslet.2013.02.033. Epub 2013 Mar 7.
Abstract
Cluster 1 streptokinases (SK1) from Streptococcus pyogenes (GAS) show substantially higher human plasminogen (hPg) activation activities and tighter hPg binding affinities than cluster 2b streptokinases (SK2b) in solution. The extent to which the different domains of SK are responsible for these differences is unknown. We exchanged each of the three known SK domains (α, β, and γ) between SK1 and SK2b and assessed the function of the resulting variants. Our results show that primary structural differences in the β-domains dictate these functional differences. This first report on the primary structure-functional relationship between naturally occurring SK1 and SK2b sheds new light on the mechanism of hPg activation by SK, a critical virulence determinant in this species of human pathogenic bacteria.
摘要
群 1 链激酶(SK1)来源于酿脓链球菌(GAS),在溶液中比群 2b 链激酶(SK2b)显示出更高的人纤溶酶原(hPg)激活活性和更强的 hPg 结合亲和力。不同 SK 结构域在多大程度上负责这些差异尚不清楚。我们在 SK1 和 SK2b 之间交换了三个已知的 SK 结构域(α、β 和 γ)中的每一个,并评估了产生的变体的功能。我们的结果表明,β-结构域中的主要结构差异决定了这些功能差异。这是关于天然存在的 SK1 和 SK2b 之间的一级结构-功能关系的第一份报告,为 SK 激活 hPg 的机制提供了新的认识,这是该种人类致病细菌的一个关键毒力决定因素。
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