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SslE elicits functional antibodies that impair in vitro mucinase activity and in vivo colonization by both intestinal and extraintestinal Escherichia coli strains

机译:SslE引发功能性抗体,这些抗体会削弱肠道粘液酶活性和肠道和肠外大肠杆菌菌株的体内定植

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摘要

SslE, the Secreted and surface-associated lipoprotein from Escherichia coli, has recently been associated to the M60-like extracellular zinc-metalloprotease sub-family which is implicated in glycan recognition and processing. SslE can be divided into two main variants and we recently proposed it as a potential vaccine candidate. By applying a number of in vitro bioassays and comparing wild type, knockout mutant and complemented strains, we have now demonstrated that SslE specifically contributes to degradation of mucin substrates, typically present in the intestine and bladder. Mutation of the zinc metallopeptidase motif of SslE dramatically impaired E. coli mucinase activity, confirming the specificity of the phenotype observed. Moreover, antibodies raised against variant I SslE, cloned from strain IHE3034 (SslEIHE3034), are able to inhibit translocation of E. coli strains expressing different variants through a mucin-based matrix, suggesting that SslE induces cross-reactive functional antibodies that affect the metallopeptidase activity. To test this hypothesis, we used well-established animal models and demonstrated that immunization with SslEIHE3034 significantly reduced gut, kidney and spleen colonization by strains producing variant II SslE and belonging to different pathotypes. Taken together, these data strongly support the importance of SslE in E. coli colonization of mucosal surfaces and reinforce the use of this antigen as a component of a broadly protective vaccine against pathogenic E. coli species.
机译:SslE是一种来自大肠杆菌的分泌的,与表面相关的脂蛋白,最近与M60样细胞外锌金属蛋白酶亚家族相关,该家族与聚糖的识别和加工有关。 SslE可以分为两个主要变体,我们最近提出将其作为潜在的疫苗候选物。通过应用多种体外生物测定并比较野生型,敲除突变体和互补菌株,我们现已证明SslE特异性地促进了通常存在于肠道和膀胱中的粘蛋白底物的降解。 SslE的锌金属肽酶基序的突变显着削弱了大肠杆菌粘蛋白酶的活性,证实了观察到的表型的特异性。此外,从菌株IHE3034(SslEIHE3034)克隆的针对变体I SslE的抗体能够抑制表达不同变体的大肠杆菌菌株通过基于粘蛋白的基质移位,这表明SslE诱导了影响金属肽酶的交叉反应性功能抗体。活动。为了检验该假设,我们使用了建立良好的动物模型,并证明了用SslEIHE3034进行免疫可显着减少产生变体II SslE并属于不同病原体的菌株的肠道,肾脏和脾脏定殖。综上所述,这些数据强烈支持了SslE在大肠杆菌对粘膜表面的定殖中的重要性,并加强了这种抗原作为针对病原性大肠杆菌物种的广泛保护性疫苗成分的用途。

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