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Characterization of a novel protective monoclonal antibody that recognizes an epitope common to Vibrio cholerae Ogawa and Inaba serotypes

机译:新型保护性单克隆抗体的表征该抗体可识别霍乱弧菌小川和稻叶血清型共有的表位

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摘要

A novel protective monoclonal antibody (mAb) that recognizes a lipopolysaccharide (LPS) epitope common between serotypes Ogawa and Inaba of the O1 serogroup of Vibrio cholerae was characterized and the potential to develop peptide mimics of this protective LPS epitope was investigated. mAb 72.1 recognizes both Ogawa and Inaba LPS and it is vibriocidal and protective in passive immunization against infection by strains of both serotypes. The cDNA-derived amino acid sequence of mAb 72.1 is closely related to the previously characterized mAb ZAC-3, which is thought to recognize an epitope in the lipid A core region of O1 LPS. In an attempt to develop a peptide mimic-based vaccine against V. cholerae, phage display libraries were screened with mAb 72.1 and 11 peptide mimics were identified. Remarkably, all of the peptide sequences identified from linear phage display libraries contained two cysteine residues, suggesting that mAb 72.1 preferentially binds to peptides constrained with a disulphide bond. One of the peptide mimics was immunologically characterized. Although immunization of mice with this peptide mimic conjugated to KLH elicited antibodies against the peptide itself, these antibodies did not cross-react with Ogawa or Inaba LPS. Effectiveness of a peptide mimic as a vaccine may depend on how well the peptide can mimic the carbohydrate interactions when binding to the anti-carbohydrate antibody. Thus, investigating how peptides and LPS bind to mAb 72.1 may be useful in improving current peptide mimics or designing more effective peptide mimics. Identification and characterization of novel protective anti-LPS antibodies may be useful in studying protective epitopes of LPS, which may help develop LPS-based therapeutics against V. cholerae.
机译:新颖的保护性单克隆抗体(mAb)识别霍乱弧菌O1血清型的Ogawa和Inaba血清型之间常见的脂多糖(LPS)表位,并研究了开发这种保护性LPS表位的肽模拟物的潜力。 mAb 72.1识别Ogawa和Inaba LPS,并且在被动免疫中具有杀线虫作用和保护作用,可抵抗两种血清型菌株的感染。 mAb 72.1的cDNA氨基酸序列与先前鉴定的mAb ZAC-3密切相关,mAb ZAC-3被认为可识别O1 LPS脂质A核心区域中的表位。为了开发针对霍乱弧菌的基于肽模拟物的疫苗,用mAb 72.1筛选了噬菌体展示文库,并鉴定了11种肽模拟物。值得注意的是,从线性噬菌体展示文库鉴定出的所有肽序列均包含两个半胱氨酸残基,表明mAb 72.1优先结合受二硫键限制的肽。肽模拟物中的一种被免疫学表征。尽管用偶联至KLH的该肽模拟物免疫小鼠可引发针对该肽本身的抗体,但这些抗体并未与Ogawa或Inaba LPS交叉反应。肽模拟物作为疫苗的有效性可能取决于与抗碳水化合物抗体结合时,该肽模拟碳水化合物相互作用的程度。因此,研究肽和LPS如何与mAb 72.1结合可能有助于改善当前的肽模拟物或设计更有效的肽模拟物。新型保护性抗LPS抗体的鉴定和表征可能有助于研究LPS的保护性表位,这可能有助于开发针对霍乱弧菌的基于LPS的疗法。

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