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与蛋白质载体结合的霍乱弧菌O1稻叶型O-特异性多糖的合成片段在小鼠中具有免疫原性,但不会诱导产生保护性抗体。

Synthetic fragments of Vibrio cholerae O1 Inaba O-specific polysaccharide bound to a protein carrier are immunogenic in mice but do not induce protective antibodies.

作者信息

Meeks Michael D, Saksena Rina, Ma Xingquan, Wade Terri K, Taylor Ronald K, Kovác Pavol, Wade William F

机构信息

Department of Microbiology and Immunology, Dartmouth Medical School, 630 W. Borwell Bldg., Lebanon, NH 03756, USA.

出版信息

Infect Immun. 2004 Jul;72(7):4090-101. doi: 10.1128/IAI.72.7.4090-4101.2004.

DOI:10.1128/IAI.72.7.4090-4101.2004
PMID:15213154
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC427411/
Abstract

Development of Vibrio cholerae lipopolysaccharide (LPS) as a cholera vaccine immunogen is justified by the correlation of vibriocidal anti-LPS response with immunity. Two V. cholerae O1 LPS serotypes, Inaba and Ogawa, are associated with endemic and pandemic cholera. Both serotypes induce protective antibody following infection or vaccination. Structurally, the LPSs that define the serotypes are identical except for the terminal perosamine moiety, which has a methoxyl group at position 2 in Ogawa but a hydroxyl group in Inaba. The terminal sugar of the Ogawa LPS is a protective B-cell epitope. We chemically synthesized the terminal hexasaccharides of V. cholerae serotype Ogawa, which comprises in part the O-specific polysaccharide component of the native LPS, and coupled the oligosaccharide at different molar ratios to bovine serum albumin (BSA). Our initial studies with Ogawa immunogens showed that the conjugates induced protective antibody. We hypothesized that antibodies specific for the terminal sugar of Inaba LPS would also be protective. Neoglycoconjugates were prepared from synthetic Inaba oligosaccharides (disaccharide, tetrasaccharide, and hexasaccharide) and BSA at different levels of substitution. BALB/c mice responded to the Inaba carbohydrate (CHO)-BSA conjugates with levels of serum antibodies of comparable magnitude to those of mice immunized with Ogawa CHO-BSA conjugates, but the Inaba-specific antibodies (immunoglobulin M [IgM] and IgG1) were neither vibriocidal nor protective in the infant mouse cholera model. We hypothesize that the anti-Inaba antibodies induced by the Inaba CHO-BSA conjugates have enough affinity to be screened via enzyme-linked immunosorbent assay but not enough to be protective in vivo.

摘要

霍乱弧菌脂多糖(LPS)作为霍乱疫苗免疫原的开发是合理的,因为杀弧菌抗LPS反应与免疫力之间存在相关性。两种霍乱弧菌O1 LPS血清型,稻叶型和小川型,与地方性和大流行性霍乱有关。两种血清型在感染或接种疫苗后均诱导产生保护性抗体。从结构上看,定义血清型的LPS除了末端的鼠李糖胺部分外是相同的,在小川型中,该部分在2位有一个甲氧基,而在稻叶型中有一个羟基。小川型LPS的末端糖是一个保护性B细胞表位。我们化学合成了霍乱弧菌小川型血清型的末端六糖,其部分包含天然LPS的O特异性多糖成分,并将该寡糖以不同的摩尔比与牛血清白蛋白(BSA)偶联。我们对小川型免疫原的初步研究表明,这些偶联物诱导产生了保护性抗体。我们推测,对稻叶型LPS末端糖具有特异性的抗体也将具有保护作用。从合成的稻叶型寡糖(二糖、四糖和六糖)和BSA制备了不同取代水平的新糖偶联物。BALB/c小鼠对稻叶型碳水化合物(CHO)-BSA偶联物的反应产生的血清抗体水平与用小川型CHO-BSA偶联物免疫的小鼠相当,但在婴儿小鼠霍乱模型中,稻叶型特异性抗体(免疫球蛋白M [IgM]和IgG1)既没有杀弧菌活性也没有保护作用。我们推测,由稻叶型CHO-BSA偶联物诱导的抗稻叶型抗体具有足够的亲和力,可通过酶联免疫吸附测定进行筛选,但在体内不足以起到保护作用。

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