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使用表层蛋白对仓鼠进行针对艰难梭菌感染的主动免疫。

Active immunization of hamsters against Clostridium difficile infection using surface-layer protein.

作者信息

Ní Eidhin Déirdre B, O'Brien Julie B, McCabe Matthew S, Athié-Morales Verónica, Kelleher Dermot P

机构信息

Department of Clinical Medicine and Dublin Molecular Medicine Centre, Trinity College Dublin, Trinity Centre for Health Sciences, St James's Hospital, Dublin, Ireland.

出版信息

FEMS Immunol Med Microbiol. 2008 Mar;52(2):207-18. doi: 10.1111/j.1574-695X.2007.00363.x. Epub 2007 Dec 15.

DOI:10.1111/j.1574-695X.2007.00363.x
PMID:18093141
Abstract

Clostridium difficile is the leading cause of infectious antibiotic-associated diarrhoea, particularly among the elderly. Its surface-layer protein (SLP) was tested as a vaccine component in a series of immunization and challenge experiments with Golden Syrian hamsters, combined with different systemic and mucosal adjuvants. Some regimens were also tested in a nonchallenge BALB/c mouse model, enabling closer monitoring of the immune response. None of the regimens conferred complete protection in the hamster model, and antibody stimulation was variable within regimens, and generally modest or poor. Mice displayed stronger antibody responses to SLP compared with hamsters. Two hamsters of five given SLP with Ribi (monophosphoryl lipid A and synthetic trehalose dicorynomycolate) survived the challenge, as did two of three given SLP with Ribi and cholera toxin. This modest trend to protection is interpreted with caution, because the survivors had low anti-SLP serum antibody titres. The hamsters were an outbred line, and subject to more genetic variability than inbred animals; however, BALB/c mice also showed strongly variable antibody responses. There is a clear need for better adjuvants for single-component vaccines, particularly for mucosal delivery. The hamster challenge model may need to be modified to be useful in active immunization experiments with SLP.

摘要

艰难梭菌是抗生素相关性感染性腹泻的主要病因,在老年人中尤为常见。在一系列针对金黄叙利亚仓鼠的免疫和攻毒实验中,将其表层蛋白(SLP)作为疫苗成分进行测试,并与不同的全身和黏膜佐剂联合使用。部分方案也在无攻毒的BALB/c小鼠模型中进行了测试,以便更密切地监测免疫反应。在仓鼠模型中,没有一种方案能提供完全保护,而且方案内的抗体刺激效果各不相同,总体上较弱或很差。与仓鼠相比,小鼠对SLP表现出更强的抗体反应。五只接受含Ribi(单磷酰脂质A和合成海藻糖二硬脂酸酯)的SLP的仓鼠中有两只在攻毒后存活下来,三只接受含Ribi和霍乱毒素的SLP的仓鼠中有两只也存活了下来。鉴于存活者的抗SLP血清抗体滴度较低,对这种适度的保护趋势应谨慎解读。这些仓鼠是远交系,与近交动物相比,其基因变异性更大;然而,BALB/c小鼠也表现出强烈的抗体反应变异性。显然需要更好的佐剂用于单组分疫苗,尤其是用于黏膜给药。仓鼠攻毒模型可能需要改进,以便在SLP的主动免疫实验中发挥作用。

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