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关于霍乱弧菌O:1型小川血清型和稻叶血清型脂多糖的抗原决定簇

On the antigenic determinants of the lipopolysaccharides of Vibrio cholerae O:1, serotypes Ogawa and Inaba.

作者信息

Wang J, Villeneuve S, Zhang J, Lei P, Miller C E, Lafaye P, Nato F, Szu S C, Karpas A, Bystricky S, Robbins J B, Kovác P, Fournier J M, Glaudemans C P

机构信息

Laboratory of Medicinal Chemistry, NIDDK, National Institutes of Health, Bethesda, Maryland 20892, USA.

出版信息

J Biol Chem. 1998 Jan 30;273(5):2777-83. doi: 10.1074/jbc.273.5.2777.

Abstract

Monoclonal, murine IgG1s S-20-4, A-20-6, and IgA 2D6, directed against Vibrio cholerae O:1 Ogawa-lipopolysaccharide exhibited the same fine specificities and similar affinities for the synthetic methyl alpha-glycosides of the (oligo)saccharide fragments mimicking the Ogawa O-polysaccharide (O-PS). They did not react with the corresponding synthetic fragments of Inaba O-PS. IgG1s S-20-4 and A-20-6 have absolute affinity constants for synthetic Ogawa mono- to hexasaccharides of from approximately 10(5) to approximately 10(6) M-1. For IgG1s S-20-4, A-20-6, and IgA 2D6, the nonreducing terminal residue of Ogawa O-PS is the dominant determinant, accounting for approximately 90% of the maximal binding energy shown by these antibodies. Binding studies of derivatives of the Ogawa monosaccharide and IgGs S-20-4 and A-20-6 revealed that the C-2 O-methyl group fits into a somewhat flexible antibody cavity and that hydrogen bonds involving the oxygen and, respectively, the OH at the 2- and 3-position of the sugar moiety as well as the 2'-position in the amide side chain are required. Monoclonal IgA ZAC-3 and IgG3 I-24-2 are specific for V. cholerae O:1 serotypes Ogawa/Inaba-LPS.1 The former did not show binding with members of either series of the synthetic ligands related to the O-antigens of the Ogawa or Inaba serotypes, in agreement with its reported specificity for the lipid/core region (1). Inhibition studies revealed that the binding of purified IgG3 I-24-2 to Ogawa-LPS might be mediated by a region in the junction of the OPS to the lipid-core region of the LPS. cDNA cloning and analysis of the anti-Ogawa antibodies S-20-4, A-20-6, and 2D6 revealed a very high degree of homology among the heavy chains. Among the light chains, no such homology between S-20-4 and A-20-6 on the one hand, and 2D6 on the other hand, exists. For the anti-Inaba/Ogawa antibodies I-24-2 and ZAC-3, their heavy chains are completely different, with some homology among the light chains.

摘要

针对霍乱弧菌O:1小川型脂多糖的单克隆鼠源IgG1 S-20-4、A-20-6和IgA 2D6,对模拟小川型O-多糖(O-PS)的(寡)糖片段的合成α-甲基糖苷表现出相同的精细特异性和相似亲和力。它们不与稻叶型O-PS的相应合成片段发生反应。IgG1 S-20-4和A-20-6对合成的小川型单糖至六糖的绝对亲和常数约为10⁵至约10⁶ M⁻¹。对于IgG1 S-20-4、A-20-6和IgA 2D6,小川型O-PS的非还原末端残基是主要决定因素,约占这些抗体所显示的最大结合能的90%。小川型单糖衍生物与IgG S-20-4和A-20-6的结合研究表明,C-2 O-甲基适合进入一个有点灵活的抗体腔,并且需要涉及糖部分2位和3位的氧以及酰胺侧链2'位的OH形成氢键。单克隆IgA ZAC-3和IgG3 I-24-2对霍乱弧菌O:1血清型小川/稻叶型-LPS具有特异性。前者与小川型或稻叶型血清型O抗原相关的任何一系列合成配体均未显示结合,这与其报道的对脂质/核心区域的特异性一致(1)。抑制研究表明,纯化的IgG3 I-24-2与小川型-LPS的结合可能由OPS与LPS脂质核心区域连接处中的一个区域介导。抗小川型抗体S-20-4、A-20-6和2D6的cDNA克隆和分析显示重链之间具有非常高的同源性。在轻链中,一方面S-20-4和A-20-6之间,另一方面与2D6之间不存在这种同源性。对于抗稻叶型/小川型抗体I-24-2和ZAC-3,它们的重链完全不同,轻链之间有一些同源性。

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