Review Article

链球菌胶原蛋白样蛋白1结合伤口纤连蛋白:病原体靶向的意义

卷 26, 期 11, 2019

页: [1933 - 1945] 页: 13

弟呕挨: 10.2174/0929867325666180831165704

价格: $65

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摘要

A组链球菌(GAS)感染是全世界显着的发病率和死亡率的原因。由于全球GAS菌株之间存在显着的抗原变异,因此降低了有效全球疫苗的前景。 GAS治疗中的其他挑战包括发展中国家缺乏常见的抗生素,以及青霉素过敏和治疗失败以及工业化世界中红霉素抗性增加。在进入的入口处,GAS结合新沉积的细胞外基质,其通过表面粘附素,链球菌胶原蛋白样蛋白1(Scl1)富含具有额外结构域A(EDA,也称为EIIIA)的细胞纤连蛋白同种型。衍生自不同GAS菌株的重组Scl1构建体结合位于C和C''β链之间的EDA环区段。尽管Scl1蛋白中的序列多样性,Scl1变体的多序列比对和二级结构预测,以及结晶学和同源性建模研究,指向Scl1-EDA结合的保守机制。我们建议针对这种相互作用可以预防感染的进展。衍生自EDA C-C''环的合成环肽以微摩尔解离常数与重组Scl1结合。该综述强调了目前EDA与Scl1结合的概念,并提供了利用这种结合来治疗GAS感染和伤口定植的激励。

关键词: Scl1,粘附素,A组链球菌定植,EDA纤连蛋白,伤口微环境,病原体。

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