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Backbone resonance assignments of innate immune evasion protein EapH2 from the S. aureus

机译:来自S.金黄色葡萄球菌的先天免疫逃避蛋白EAPH2的骨干共振分配

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Staphylococcus aureus is a ubiquitous and persistent pathogen of humans and livestock. The bacterium disrupts the host's innate immune system's ability to recognize and clear bacteria with optimal efficiency by expressing a wide variety of virulence proteins. Two single domain protein homologs (EapH1, EapH2) of the extracellular adherence protein (Eap) have been reported. Eap is a multidomain protein that participates in various protein-protein interactions that inhibit the innate immune response, including both the complement and Neutrophil Serine Proteases (NSPs). EapH1 and EapH2 are also inhibitors of NSPs (Stapels et al., Proc Natl Acad Sci 111:13187-13192, 2014), but lack the ability to inhibit the classical, and lectin pathways of the complement activation system (Woehl et al., J Immunol 193:6161-6171, 2014). We continue the characterization of Eap domains, here with the experiments on EapH2, we acquired a series of 2D and 3D NMR spectra of EapH2 in solution. We completed 99% of expected non-proline backbone H-1, N-15, and C-13 resonance assignments of EapH2 and predicted secondary structure via the TALOS-N server. The assignment data have been deposited in the BMRB data bank under Accession Number 27540.
机译:金黄色葡萄球菌是人类和牲畜的普遍存在和持续的病原体。细菌通过表达各种毒力蛋白来破坏宿主的先天免疫系统识别和清除细菌的能力。已经报道了两个单一结构域蛋白质(EAPH1,EAPH2)的细胞外粘附蛋白(EAP)。 EAP是一种多畴蛋白质,其参与各种蛋白质 - 蛋白质相互作用,抑制先天免疫应答,包括补体和中性粒细胞丝氨酸蛋白酶(NSP)。 EAPH1和EAPH2也是NSP的抑制剂(Stapels等,Proc Natl Acad SCI 111:13187-13192,2014),但缺乏能够抑制补体激活系统的经典和凝集素途径(WOEHL等, J免疫素193:6161-6171,2014)。我们继续表征EAP域,这里有EAPH2的实验,我们在解决方案中获得了一系列EAPH2的2D和3D NMR光谱。我们通过Talos-N服务器完成了EAPH2和预测的二级结构的99%的预期非脯氨酸骨干H-1,N-15和C-13共振分配。在加入号码27540下,已在BMRB数据库中存放分配数据。

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