首页> 外文OA文献 >Mucosally Delivered Salmonella Live Vector Vaccines Elicit Potent Immune Responses against a Foreign Antigen in Neonatal Mice Born to Naive and Immune Mothers
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Mucosally Delivered Salmonella Live Vector Vaccines Elicit Potent Immune Responses against a Foreign Antigen in Neonatal Mice Born to Naive and Immune Mothers

机译:粘膜递送沙门氏菌活载体疫苗对初生和免疫母亲的新生小鼠的外源抗原产生有效的免疫反应。

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摘要

The development of effective vaccines for neonates and very young infants has been impaired by their weak, short-lived, and Th-2 biased responses and by maternal antibodies that interfere with vaccine take. We investigated the ability of Salmonella enterica serovars Typhi and Typhimurium to mucosally deliver tetanus toxin fragment C (Frag C) as a model antigen in neonatal mice. We hypothesize that Salmonella, by stimulating innate immunity (contributing to adjuvant effects) and inducing Th-1 cytokines, can enhance neonatal dendritic cell maturation and T-cell activation and thereby prime humoral and cell-mediated immunity. We demonstrate for the first time that intranasal immunization of newborn mice with 109 CFU of S. enterica serovar Typhi CVD 908-htrA and S. enterica serovar Typhimurium SL3261 carrying plasmid pTETlpp on days 7 and 22 after birth elicits high titers of Frag C antibodies, previously found to protect against tetanus toxin challenge and similar to those observed in adult mice. Salmonella live vectors colonized and persisted primarily in nasal tissue. Mice vaccinated as neonates induced Frag C-specific mucosal and systemic immunoglobulin A (IgA)- and IgG-secreting cells, T-cell proliferative responses, and gamma interferon secretion. A mixed Th1- and Th2-type response to Frag C was established 1 week after the boost and was maintained thereafter. S. enterica serovar Typhi carrying pTETlpp induced Frag C-specific antibodies and cell-mediated immunity in the presence of high levels of maternal antibodies. This is the first report that demonstrates the effectiveness of Salmonella live vector vaccines in early life.
机译:新生儿和年幼婴儿的有效疫苗的开发因其弱,短暂和Th-2偏倚的应答以及干扰疫苗接种的母体抗体而受到损害。我们调查了鼠伤寒沙门氏菌伤寒和伤寒沙门氏菌的能力,以黏膜递送破伤风毒素片段C(Frag C)作为新生小鼠中的模型抗原。我们假设沙门氏菌通过刺激先天免疫(有助于佐剂作用)和诱导Th-1细胞因子,可以增强新生儿树突状细胞的成熟和T细胞的活化,从而引发体液和细胞介导的免疫。我们首次证明,在出生后的第7天和第22天,携带质粒pTETlpp的肠球菌血清型Typhi CVD 908-htrA和肠球菌血清型SL3261的109 CFU鼻内免疫新生小鼠会产生高滴度的Frag C抗体,以前发现它可以防止破伤风毒素攻击,并且与成年小鼠类似。沙门氏菌活载体定居并主要存在于鼻组织中。新生儿疫苗接种的小鼠诱导Frag C特异性粘膜和全身免疫球蛋白A(IgA)和IgG分泌细胞,T细胞增殖反应和γ干扰素分泌。加强免疫后1周建立了对Frag C的Th1和Th2型混合反应,此后一直保持。在高水平的母源抗体存在下,携带pTETlpp的肠炎链球菌血清型伤寒沙门氏菌诱导的Frag C特异性抗体和细胞介导的免疫力。这是第一份证明沙门氏菌活载体疫苗在生命早期的有效性的报告。

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