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用与白喉类毒素偶联的SfbI或M蛋白衍生肽进行鼻内接种可赋予针对化脓性链球菌致死性攻击的保护性免疫。

Intranasal vaccination with SfbI or M protein-derived peptides conjugated to diphtheria toxoid confers protective immunity against a lethal challenge with Streptococcus pyogenes.

作者信息

Schulze Kai, Olive Colleen, Ebensen Thomas, Guzmán Carlos A

机构信息

Department of Vaccinology, GBF-German Research Centre for Biotechnology, Mascheroder Weg 1, D-38124 Braunschweig, Germany.

出版信息

Vaccine. 2006 Aug 28;24(35-36):6088-95. doi: 10.1016/j.vaccine.2006.05.024. Epub 2006 Jun 2.

Abstract

We investigated whether intranasal immunisation with diphtheria toxoid (DT) conjugated polypeptides encompassing T and B cell epitopes of the SfbI protein (FNBR) or a conformational-constrained B cell epitope of the M1 protein (J8) was able to confer protection against lethal mucosal challenge with a heterologous Streptococcus pyogenes strain. To this end, BALB/c mice were immunised with the conjugates. Strong antigen-specific antibody responses were observed in both serum and mucosal secretions. Vaccinated mice were challenged 10 days after the last boost by the intranasal route. Animals receiving FNBR-DT co-administered with either the cholera toxin B subunit (CTB) or the TLR 2/6 agonist MALP-2 were efficiently protected against the virulent S. pyogenes strain (90% and 70% survival, respectively), whereas those immunised with J8-DT plus either CTB or MALP-2 showed intermediate levels of protection (60% and 40%, respectively). The obtained results indicate that in our experimental animal model peptide-based conjugate vaccines represent a valid alternative to protect against streptococcal infection.

摘要

我们研究了用包含SfbI蛋白(FNBR)的T和B细胞表位的白喉类毒素(DT)缀合多肽或M1蛋白(J8)的构象受限B细胞表位进行鼻内免疫是否能够提供针对异源化脓性链球菌菌株致死性粘膜攻击的保护作用。为此,用这些缀合物对BALB/c小鼠进行免疫。在血清和粘膜分泌物中均观察到强烈的抗原特异性抗体反应。在最后一次加强免疫后10天,通过鼻内途径对接种疫苗的小鼠进行攻击。接受与霍乱毒素B亚基(CTB)或TLR 2/6激动剂MALP-2共同施用的FNBR-DT的动物有效地抵御了强毒化脓性链球菌菌株(分别有90%和70%存活),而用J8-DT加CTB或MALP-2免疫的动物显示出中等水平的保护作用(分别为60%和40%)。所得结果表明,在我们的实验动物模型中,基于肽的缀合疫苗是预防链球菌感染的有效替代方法。

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