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Maternal Vaccination with a Fimbrial Tip Adhesin and Passive Protection of Neonatal Mice against Lethal Human Enterotoxigenic Escherichia coli Challenge

机译:孕产妇接种带尾尖黏附素的疫苗以及对小鼠的致死性人类肠毒素性大肠杆菌挑战的被动保护

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摘要

Globally, enterotoxigenic Escherichia coli (ETEC) is a leading cause of childhood and travelers' diarrhea, for which an effective vaccine is needed. Prevalent intestinal colonization factors (CFs) such as CFA/I fimbriae and heat-labile enterotoxin (LT) are important virulence factors and protective antigens. We tested the hypothesis that donor strand-complemented CfaE (dscCfaE), a stabilized form of the CFA/I fimbrial tip adhesin, is a protective antigen, using a lethal neonatal mouse ETEC challenge model and passive dam vaccination. For CFA/I-ETEC strain , which has been extensively studied in volunteers, an inoculum of 2 × 107 bacteria resulted in 50% lethal doses (LD50) in neonatal DBA/2 mice. Vaccination of female DBA/2 mice with CFA/I fimbriae or dscCfaE, each given with a genetically attenuated LT adjuvant (LTK63) by intranasal or orogastric delivery, induced high antigen-specific serum IgG and fecal IgA titers and detectable milk IgA responses. Neonates born to and suckled by dams antenatally vaccinated with each of these four regimens showed 78 to 93% survival after a 20× LD50 challenge with , compared to 100% mortality in pups from dams vaccinated with sham vaccine or LTK63 only. Crossover experiments showed that high pup survival rates after ETEC challenge were associated with suckling but not birthing from vaccinated dams, suggesting that vaccine-specific milk antibodies are protective. In corroboration, preincubation of the ETEC inoculum with antiadhesin and antifimbrial bovine colostral antibodies conferred a dose-dependent increase in pup survival after challenge. These findings indicate that the dscCfaE fimbrial tip adhesin serves as a protective passive vaccine antigen in this small animal model and merits further evaluation.
机译:在全球范围内,产肠毒素的大肠杆菌(ETEC)是导致儿童期和旅行者腹泻的主要原因,因此需要有效的疫苗。常见的肠道定殖因子(CFs),例如CFA / I菌毛和不耐热肠毒素(LT)是重要的毒力因子和保护性抗原。我们使用致命的新生小鼠ETEC攻击模型和被动坝疫苗接种试验验证了供体链互补CfaE(dscCfaE)(CFA / I纤维尖端粘附素的稳定形式)是一种保护性抗原的假设。对于在志愿者中进行了广泛研究的CFA / I-ETEC株,接种2×10 7 细菌的接种物在新生DBA / 2小鼠中产生50%的致死剂量(LD50)。给雌性DBA / 2小鼠接种CFA / I菌毛或dscCfaE,每只小鼠均通过鼻内或口腔灌胃给予遗传减毒的LT佐剂(LTK63),诱导了高抗原特异性血清IgG和粪便IgA滴度和可检测的牛奶IgA反应。用这四种方案中的每一种进行出生前疫苗接种的水坝出生和哺乳的新生儿在经20倍LD50攻击后显示78%至93%的存活率,而仅用假疫苗或LTK63疫苗接种的水坝的幼崽死亡率为100%。交叉实验表明,ETEC攻击后幼崽的高成活率与哺乳但未从疫苗接种的大坝中诞生有关,这表明疫苗特异性乳抗体具有保护性。确证的是,将ETEC接种物与抗粘附素和抗纤维牛初乳抗体进行预培养后,激发后幼仔的存活率呈剂量依赖性增加。这些发现表明,dscCfaE纤维末端粘附素在这种小动物模型中充当保护性被动疫苗抗原,值得进一步评估。

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