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以大肠杆菌不耐热肠毒素B亚基作为佐剂对小鼠单纯疱疹病毒1型眼部感染的保护性黏膜免疫

Protective mucosal immunity to ocular herpes simplex virus type 1 infection in mice by using Escherichia coli heat-labile enterotoxin B subunit as an adjuvant.

作者信息

Richards C M, Aman A T, Hirst T R, Hill T J, Williams N A

机构信息

Department of Pathology and Microbiology, School of Medical Sciences, University of Bristol, Bristol BS8 1TD, United Kingdom.

出版信息

J Virol. 2001 Feb;75(4):1664-71. doi: 10.1128/JVI.75.4.1664-1671.2001.

Abstract

The potential of nontoxic recombinant B subunits of cholera toxin (rCtxB) and its close relative Escherichia coli heat-labile enterotoxin (rEtxB) to act as mucosal adjuvants for intranasal immunization with herpes simplex virus type 1 (HSV-1) glycoproteins was assessed. Doses of 10 microg of rEtxB or above with 10 microg of HSV-1 glycoproteins elicited high serum and mucosal anti-HSV-1 titers comparable with that obtained using CtxB (10 microg) with a trace (0.5 microg) of whole toxin (Ctx-CtxB). By contrast, doses of rCtxB up to 100 microg elicited only meager anti-HSV-1 responses. As for Ctx-CtxB, rEtxB resulted in a Th2-biased immune response with high immunoglobulin G1 (IgG1)/IgG2a antibody ratios and production of interleukin 4 (IL-4) and IL-10 as well as gamma interferon by proliferating T cells. The protective efficacy of the immune response induced using rEtxB as an adjuvant was assessed following ocular challenge of immunized and mock-immunized mice. Epithelial disease was observed in both groups, but the immunized mice recovered by day 6 whereas mock-immunized mice developed more severe corneal disease leading to stromal keratitis. In addition, a significant reduction in the incidence of lid disease and zosteriform spread was observed in immunized animals and there was no encephalitis compared with 95% encephalitis in mock-immunized mice. The potential of such mucosal adjuvants for use in human vaccines against pathogens such as HSV-1 is discussed.

摘要

评估了霍乱毒素无毒重组B亚基(rCtxB)及其近亲大肠杆菌不耐热肠毒素(rEtxB)作为1型单纯疱疹病毒(HSV-1)糖蛋白鼻内免疫黏膜佐剂的潜力。10微克rEtxB或更高剂量与10微克HSV-1糖蛋白一起引发的高血清和黏膜抗HSV-1滴度,与使用10微克CtxB和微量(0.5微克)全毒素(Ctx-CtxB)所获得的滴度相当。相比之下,高达100微克的rCtxB剂量仅引发微弱的抗HSV-1反应。与Ctx-CtxB一样,rEtxB导致以Th2为主的免疫反应,具有高免疫球蛋白G1(IgG1)/IgG2a抗体比率,增殖T细胞产生白细胞介素4(IL-4)、IL-10以及γ干扰素。在用rEtxB作为佐剂诱导的免疫反应的保护效力在免疫和假免疫小鼠眼部攻击后进行了评估。两组均观察到上皮疾病,但免疫小鼠在第6天恢复,而假免疫小鼠发展为更严重的角膜疾病并导致基质性角膜炎。此外,在免疫动物中观察到眼睑疾病和带状疱疹样扩散的发生率显著降低,并且与假免疫小鼠中95%的脑炎发生率相比,没有脑炎发生。讨论了这种黏膜佐剂用于针对HSV-1等病原体的人类疫苗的潜力。

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