首页> 美国卫生研究院文献>Elsevier Public Health Emergency Collection >Mapping of Linear Antigenic Sites on the S Glycoprotein of a Neurotropic Murine Coronavirus with Synthetic Peptides: A Combination of Nine Prediction Algorithms Fails To Identify Relevant Epitopes and Peptide Immunogenicity Is Drastically Influenced by the Nature of the Protein Carrier
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Mapping of Linear Antigenic Sites on the S Glycoprotein of a Neurotropic Murine Coronavirus with Synthetic Peptides: A Combination of Nine Prediction Algorithms Fails To Identify Relevant Epitopes and Peptide Immunogenicity Is Drastically Influenced by the Nature of the Protein Carrier

机译:带有合成肽的神经质鼠冠状病毒S糖蛋白上线性抗原性位点的映射:九种预测算法的组合未能识别相关表位并且肽的免疫原性受蛋白质载体性质的影响很大

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摘要

The elucidation of the antigenic structure of the S glycoprotein of murine coronaviruses will provide further understanding of the Complex pathogenicity of these viruses. In order to identify linear antigenic determinants, the primary structure of the S glycoprotein of murine hepatitis virus strain A59 was analyzed with a combination of nine epitope prediction algorithms. Fifteen potential epitopes were synthesized chemically and injected into BALB/c mice to study their biological relevance. This approach failed to identify novel important epitopes. Furthermore, the algorithms were unable to identify as antigenic the previously mapped immunodominant epitope A [C Daniel, R. Anderson, M. J. Buchmeier, J. O. Fleming, W. J. M. Spaan, H. Wege, and Talbot, P. J. (1993) 67, 1185-1194]. Interestingly, peptide A coupled to KLH induced an immune response that stimulated the immune response induced by the corresponding region of the protein much more accurately than when the same peptide was coupled to BSA. This included drastically enhanced competition with monoclonal antibodies and protection from virus challenge. These findings emphasize the shortcomings of amino acid sequence-based epitope prediction algorithms and demonstrate the critical importance of the carrier when synthetic peptides are considered as potential vaccines.
机译:鼠冠状病毒S糖蛋白的抗原结构的阐明将进一步了解这些病毒的复杂致病性。为了鉴定线性抗原决定簇,结合九种表位预测算法分析了鼠肝炎病毒A59株S糖蛋白的一级结构。化学合成了十五种潜在的表位,并注射到BALB / c小鼠中以研究其生物学相关性。该方法未能鉴定出新颖的重要表位。此外,这些算法无法将先前定位的免疫优势表位A识别为抗原性[C Daniel,R. Anderson,MJ Buchmeier,JO Fleming,WJM Spaan,H.Wege,and Talbot,PJ(1993)67,1185-1194]。 。有趣的是,与相同肽与BSA偶联时相比,与KLH偶联的肽A诱导的免疫应答能更准确地刺激蛋白质相应区域诱导的免疫应答。这包括与单克隆抗体的竞争大大增强,以及免受病毒攻击的保护。这些发现强调了基于氨基酸序列的表位预测算法的缺点,并证明了在将合成肽视为潜在疫苗时载体的至关重要性。

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