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源自经基因工程改造的突变菌株的脑膜炎球菌外膜囊泡疫苗,这些菌株可表达来自抗原变异组1和2的补体因子H结合蛋白。

Meningococcal outer membrane vesicle vaccines derived from mutant strains engineered to express factor H binding proteins from antigenic variant groups 1 and 2.

作者信息

Koeberling Oliver, Giuntini Serena, Seubert Anja, Granoff Dan M

机构信息

Novartis Vaccines, Siena, Italy.

出版信息

Clin Vaccine Immunol. 2009 Feb;16(2):156-62. doi: 10.1128/CVI.00403-08. Epub 2008 Dec 24.

DOI:10.1128/CVI.00403-08
PMID:19109451
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2643535/
Abstract

Meningococcal outer membrane vesicle (OMV) vaccines, which are treated with detergents to decrease endotoxin activity, are safe and effective in humans. However, the vaccines elicit serum bactericidal antibody responses largely directed against PorA, which is antigenically variable. We previously prepared a native (non-detergent-treated) OMV vaccine from a mutant of group B strain H44/76 in which the lpxL1 gene was inactivated, which resulted in penta-acylated lipid A with attenuated endotoxin activity. To enhance protection, we overexpressed factor H binding protein (fHbp) from the antigenic variant 1 group. The vaccine elicited broad serum bactericidal antibody responses in mice against strains with fHbp variant 1 (approximately 70% of group B isolates) but not against strains with variant 2 or 3. In the present study, we constructed a mutant of group B strain NZ98/254 with attenuated endotoxin that expressed both endogenous variant 1 and heterologous fHbp variant 2. A mixture of the two native OMV vaccines from the H44/76 and NZ98/254 mutants stimulated proinflammatory cytokine responses by human peripheral blood mononuclear cells similar to those stimulated by control, detergent-treated OMV vaccines from the wild-type strains. In mice, the mixture of the two native OMV vaccines elicited broad serum bactericidal antibody responses against strains with heterologous PorA and fHbp in the variant 1, 2, or 3 group. By adsorption studies, the principal bactericidal antibody target was determined to be fHbp. Thus, native OMV vaccines from mutants expressing fHbp variants have the potential to be safe for humans and to confer broad protection against meningococcal disease from strains expressing fHbp from each of the antigenic variant groups.

摘要

经去污剂处理以降低内毒素活性的脑膜炎球菌外膜囊泡(OMV)疫苗在人体中是安全有效的。然而,这些疫苗引发的血清杀菌抗体反应主要针对抗原性可变的PorA。我们之前从B群菌株H44/76的一个突变体中制备了一种天然(未用去污剂处理)的OMV疫苗,该突变体中的lpxL1基因失活,导致五酰化脂多糖,其具有减弱的内毒素活性。为了增强保护作用,我们过表达了来自抗原变异体1组的因子H结合蛋白(fHbp)。该疫苗在小鼠中引发了针对具有fHbp变异体1的菌株(约占B群分离株的70%)的广泛血清杀菌抗体反应,但对具有变异体2或变异体3的菌株没有反应。在本研究中,我们构建了一种B群菌株NZ98/254的突变体,其具有减弱的内毒素,并表达内源性变异体1和异源fHbp变异体2。来自H44/76和NZ98/254突变体的两种天然OMV疫苗的混合物刺激人外周血单核细胞产生的促炎细胞因子反应,类似于野生型菌株经去污剂处理的对照OMV疫苗所刺激的反应。在小鼠中,两种天然OMV疫苗的混合物引发了针对变异体1、2或3组中具有异源PorA和fHbp的菌株的广泛血清杀菌抗体反应。通过吸附研究,确定主要的杀菌抗体靶点为fHbp。因此,来自表达fHbp变异体的突变体的天然OMV疫苗有可能对人类安全,并对表达来自每个抗原变异体组的fHbp的菌株引起的脑膜炎球菌疾病提供广泛保护。

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