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首页> 外文期刊>Journal of Clinical Microbiology >Identification of Immunodominant Epitopes on the Membrane Protein of the Severe Acute Respiratory Syndrome-Associated Coronavirus
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Identification of Immunodominant Epitopes on the Membrane Protein of the Severe Acute Respiratory Syndrome-Associated Coronavirus

机译:严重急性呼吸综合征相关冠状病毒膜蛋白上的免疫抗原决定簇的鉴定

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Similar to other coronaviruses, the membrane (M) protein of severe acute respiratory syndrome-associated coronavirus (SARS-CoV) is a major transmembrane glycoprotein with multiple biological functions. To date, limited information is available about its antigenic properties. In this study, we identified two major immunodominant epitopes on the M protein located in the extreme N-terminal region (residues 1 to 31) and the interior C-terminal region (residues 132 to 161), respectively, by Pepscan analyses against convalescent-phase sera from SARS patients and antisera from virus-immunized mice and rabbits. Synthetic peptides M1-31 derived from the N-terminal epitope and M132-161 derived from the C-terminal epitope were highly reactive with all of the convalescent-phase sera from 40 SARS patients but not with 30 control serum samples from healthy blood donors, suggesting their potential application for serologic diagnosis of SARS. We showed that both peptides (M1-31 and M132-161) were able to induce high titers of antibody responses in the immunized rabbits, highlighting their antigenicity and immunogenicity. These findings provide important information for developing SARS diagnostics and vaccines.
机译:与其他冠状病毒相似,重症急性呼吸综合征相关冠状病毒(SARS-CoV)的膜蛋白(M)是具有多种生物学功能的主要跨膜糖蛋白。迄今为止,关于其抗原特性的信息有限。在这项研究中,我们通过Pepscan分析针对恢复期的C的Pepscan分析,分别确定了位于极端N末端区域(残基1至31)和内部C末端区域(残基132至161)的M蛋白上的两个主要免疫优势表位。 SARS患者的半数血清和病毒免疫的小鼠和兔子的抗血清。源自N末端抗原决定基的合成肽M1-31和源自C末端抗原决定基的M132-161与来自40名SARS患者的所有恢复期血清具有高反应性,但与来自健康献血者的30份对照血清样品没有反应,提示其在SARS血清学诊断中的潜在应用。我们显示两种肽(M1-31和M132-161)都能够在免疫兔中诱导高滴度的抗体反应,从而突出了它们的抗原性和免疫原性。这些发现为开发SARS诊断和疫苗提供了重要信息。

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