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首页> 外文期刊>PLOS Neglected Tropical Diseases >Impact of CD4+ T Cell Responses on Clinical Outcome following Oral Administration of Wild-Type Enterotoxigenic Escherichia coli in Humans
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Impact of CD4+ T Cell Responses on Clinical Outcome following Oral Administration of Wild-Type Enterotoxigenic Escherichia coli in Humans

机译:口服人类野生型肠毒素大肠杆菌后CD4 + T细胞反应对临床结果的影响

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摘要

Enterotoxigenic Escherichia coli (ETEC) is a non-invasive enteric pathogen of considerable public health importance, being one of the most common attributable causes of diarrheal illness in infants and young children in developing countries and the most common cause of traveler’s diarrhea. To enhance study-to-study consistency of our experimental challenge model of ETEC in volunteers, and to allow concomitant multi-site trials to evaluate anti-ETEC immunoprophylactic products, hundreds of vials, each containing a standardized inoculum of virulent wild-type (wt) ETEC strain H10407 (serotype O78:H11 expressing colonization factor antigen I and heat-labile and heat-stable enterotoxins), were prepared under current Good Manufacturing Practices (cGMP) and frozen. Following thawing, the contents of each vial can be used (diluted as necessary) to prepare consistent challenge inoculum, even at different study sites. A preliminary human experimental challenge study using this cGMP inoculum was conducted on a research isolation ward and the clinical and cell-mediated immune responses evaluated. Of the 6 healthy adult volunteers challenged 83% (5/6) developed diarrhea and 50% developed moderate-to-severe diarrhea (MSD). Moderate and severe diarrhea were defined as passage of ≥ 1 liter or ≥ 3 liters of diarrheal stool respectively. We compared the CD4+ T cell responses of volunteers who developed MSD against those who did not and identified significant differences in ETEC-specific cytokine production and gut homing potential. We furthermore demonstrated that increased expression of the gut-homing molecule integrin α4β7 by peripheral T follicular helper cells (pTfh) correlated with decreased stool volume and increased ETEC-specific IgA B memory cell (BM) development. Collectively, despite small numbers of volunteers, our results indicate a potential role for CD4+ T cells, in particular pTfh, in modulating disease outcome following exposure to wt ETEC in a volunteer experimental challenge model.
机译:肠毒素性大肠杆菌(ETEC)是一种具有重要公共卫生意义的非侵入性肠病原体,是发展中国家婴幼儿腹泻病的最常见归因之一,也是旅行者腹泻的最常见原因。为了增强我们在志愿者中对ETEC的实验性挑战模型的研究与研究的一致性,并允许进行多点试验以评估抗ETEC免疫预防产品,数百个小瓶,每个小瓶都包含有毒力的野生型(wt )按照现行的良好生产规范(cGMP)制备ETEC菌株H10407(表达定殖因子抗原I的血清型O78:H11,对热不稳定和对热稳定的肠毒素),并将其冷冻。解冻后,即使在不同的研究地点,也可以使用每个小瓶的内容物(根据需要稀释)以制备一致的挑战接种物。在隔离病房进行了使用该cGMP接种物的初步人体实验攻击研究,并评估了临床和细胞介导的免疫反应。在接受挑战的6名健康成人志愿者中,有83%(5/6)出现腹泻,而50%出现中度至重度腹泻(MSD)。中度和重度腹泻分别定义为通过≥1升或≥3升的腹泻大便。我们比较了患有MSD的志愿者与未患有MSD的志愿者的CD4 + T细胞反应,并发现了ETEC特异性细胞因子的产生和肠道归巢潜能的显着差异。我们进一步证明,外周T滤泡辅助细胞(pTfh)表达的肠归巢分子整联蛋白α4β7的表达与粪便量减少和ETEC特异性IgA B记忆细胞(BM)的发育增加有关。总体而言,尽管志愿者人数很少,但我们的结果表明,在志愿者实验性攻击模型中,暴露于wt ETEC后,CD4 + T细胞(尤其是pTfh)在调节疾病结局中具有潜在作用。

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