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首页> 外文期刊>Clinical and vaccine immunology: CVI >Human neutralizing Fab molecules against severe acute respiratory syndrome coronavirus generated by phage display.
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Human neutralizing Fab molecules against severe acute respiratory syndrome coronavirus generated by phage display.

机译:人类对噬菌体显示产生的严重急性呼吸综合征冠状病毒的中和Fab分子。

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摘要

Human recombinant Fab fragments specific for the spike protein of severe acute respiratory syndrome coronavirus (SARS-CoV) were screened from a human Fab library, which was generated from RNAs from peripheral lymphocytes of convalescent SARS patients. Among 50 randomly picked clones, 12 Fabs specially reacted with S protein by an enzyme-linked immunosorbent assay. The microneutralizing test showed that one clone, designated M1A, had neutralizing activity on Vero E6 cells against SARS-CoV. DNA sequence analysis indicated that the light- and heavy-chain genes of M1A Fab belong to the kappa2a and 4f families, respectively. A neutralizing test on purified M1A demonstrated that 0.5 mg/ml of M1A completely inhibited SARS-CoV activity, with an absence of cytopathic effect for 7 days. Real-time fluorescence reverse transcription-PCR also proved the neutralizing capacity of M1A. These data showed that the number of virus copies was significantly reduced in the M1A-treated group, suggesting an important role forM1A in passive immunoprophylaxis against the SARS virus.
机译:从人类FAB库中筛选了针对严重急性呼吸综合征冠状病毒(SARS-COV)的尖峰蛋白特异性的人类重组FAB片段,该疾病库是由人类FAB库筛选的,该库是由康复SARS患者的外周淋巴细胞从RNA中产生的。在50个随机采摘的克隆中,有12个FAB通过酶联免疫吸附测定法专门与S蛋白反应。微中和测试表明,一个指定的M1A的克隆对SARS-COV的VERO E6细胞具有中和活性。 DNA序列分析表明,M1A Fab的光和重链基因分别属于Kappa2a和4F家族。对纯化的M1A进行中和测试表明,0.5 mg/ml的M1a完全抑制了SARS-COV活性,而缺乏细胞性效应7天。实时荧光逆转录PCR也证明了M1A的中和能力。这些数据表明,在经M1A处理的组中,病毒副本的数量显着减少,这表明对SARS病毒的被动免疫预保学在被动免疫预防中具有重要作用。

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