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重组钩端螺旋体 LipL32 和 LigA 不能刺激仓鼠模型对钩端螺旋体病产生保护性免疫。

Recombinant LipL32 and LigA from Leptospira are unable to stimulate protective immunity against leptospirosis in the hamster model.

机构信息

Department of Microbiology, Monash University, VIC 3800, Australia.

出版信息

Vaccine. 2011 Apr 18;29(18):3413-8. doi: 10.1016/j.vaccine.2011.02.084. Epub 2011 Mar 9.

Abstract

The major antigenic component of pathogenic Leptospira spp. is lipopolysaccharide (LPS). However, due to the specificity of the immune response generated towards LPS and the diversity in leptospiral LPS carbohydrate structure, current commercial vaccines stimulate protection only against homologous or closely related serovars. Vaccines that confer heterologous protection would enhance protection in vaccinated animals and reduce transmission to humans. Several studies have investigated the potential of various leptospiral outer membrane proteins to stimulate protective immunity against pathogenic Leptospira species. These include the surface-exposed lipoproteins LipL32 and LigA. However, consistent protection from infection has proved difficult to reproduce. In this study we assessed the protective capacity of recombinant LipL32, the six carboxy-terminal unique Ig-like repeat domains of LigA (LigANI) and a LipL32-LigANI fusion protein in hamsters against infection with Leptospira interrogans serovar Manilae. Despite all of the proteins eliciting antibody responses, none of the hamsters was protected against infection.

摘要

致病性钩端螺旋体的主要抗原成分为脂多糖(LPS)。然而,由于针对 LPS 产生的免疫应答具有特异性,并且钩端螺旋体 LPS 碳水化合物结构存在多样性,目前的商业疫苗仅能刺激针对同源或密切相关血清型的保护。具有异源保护作用的疫苗将增强接种动物的保护作用,并减少向人类的传播。已有多项研究探讨了各种钩端螺旋体外膜蛋白刺激针对致病性钩端螺旋体物种的保护性免疫的潜力。其中包括表面暴露的脂蛋白 LipL32 和 LigA。然而,从感染中获得一致的保护作用一直难以复制。在这项研究中,我们评估了重组 LipL32、LigA 的六个羧基末端独特 Ig 样重复结构域(LigANI)和 LipL32-LigANI 融合蛋白在感染导致马尼拉血清型钩端螺旋体的仓鼠中的保护能力。尽管所有这些蛋白都能引起抗体反应,但没有一只仓鼠免受感染。

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