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The serodominant secreted effector protein of Salmonella, SseB, is a strong CD4 antigen containing an immunodominant epitope presented by diverse HLA class II alleles.

机译:沙门氏菌的血清素分泌的效应蛋白SseB是一种强CD4抗原,含有多种HLA II类等位基因呈现的免疫优势表位。

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摘要

Detailed characterization of the protective T-cell response in salmonellosis is a pressing unmet need in light of the global burden of human Salmonella infections and the likely contribution of CD4 T cells to immunity against this intracellular infection. In previous studies screening patient sera against antigen arrays, SseB was noteworthy as a serodominant target of adaptive immunity, inducing significantly raised antibody responses in HIV-seronegative compared with seropositive patients. SseB is a secreted protein, part of the Espa superfamily, localized to the bacterial surface and forming part of the translocon of the type III secretion system (T3SS) encoded by Salmonella pathogenicity island 2. We demonstrate here that SseB is also a target of CD4 T-cell immunity, generating a substantial response after experimental infection in human volunteers, with around 0.1% of the peripheral repertoire responding to it. HLA-DR/peptide binding studies indicate that this protein encompasses a number of peptides with ability to bind to several different HLA-DR alleles. Of these, peptide 11 (p11) was shown in priming of both HLA-DR1 and HLA-DR4 transgenic mice to contain an immunodominant CD4 epitope. Analysis of responses in human donors showed immunity focused on p11 and another epitope in peptide 2. The high frequency of SseB-reactive CD4 T cells and the broad applicability to diverse HLA genotypes coupled with previous observations of serodominance and protective vaccination in mouse challenge experiments, make SseB a plausible candidate for next-generation Salmonella vaccines.
机译:鉴于人沙门氏菌感染的全球负担以及CD4 T细胞对抵抗这种细胞内感染的免疫力的可能贡献,沙门氏菌病中保护性T细胞反应的详细表征是迫切需要解决的问题。在以前的针对患者血清进行抗原阵列筛选的研究中,SseB作为适应性免疫的血清素靶标值得注意,与血清反应阳性的患者相比,HIV血清反应阴性的抗体反应明显升高。 SseB是一种分泌蛋白,是Espa超家族的一部分,位于细菌表面并形成由沙门氏菌致病岛2编码的III型分泌系统(T3SS)的转录子的一部分。我们在此证明SseB也是CD4的靶标T细胞免疫力在人类志愿者的实验性感染后产生实质性反应,约有0.1%的外周血反应性。 HLA-DR /肽结合研究表明,该蛋白包含许多能够与几种不同的HLA-DR等位基因结合的肽。其中,肽11(p11)在HLA-DR1和HLA-DR4转基因小鼠的启动中均显示含有免疫优势CD4表位。对人类供体反应的分析表明,免疫力集中于肽2的p11和另一个表位。SseB反应性CD4 T细胞的高频率以及对各种HLA基因型的广泛适用性,以及先前在小鼠攻击实验中观察到的血清素和保护性疫苗的观察结果,使SseB成为下一代沙门氏菌疫苗的合理候选者。

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