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Antibodies against a synthetic peptide of the poliovirus replicase protein: reaction with native, virus-encoded proteins and inhibition of virus-specific polymerase activities in vitro

机译:针对脊髓灰质炎病毒复制酶蛋白合成肽的抗体:与天然病毒编码蛋白反应,并在体外抑制病毒特异性聚合酶活性

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摘要

A carboxy-terminal peptide of the poliovirus replicase protein (p63) was chemically synthesized, coupled to bovine serum albumin carrier, and injected into rabbits. The resulting antisera reacted with six virus-specific proteins from HeLa cells infected with poliovirus: NCVP 0b, NCVP 1b, NCVP 2, a protein of about 60,000 daltons, p63, and NCVP 6b. The identity of the 60,000-dalton protein is not known, but the other results were consistent with previous experimental approaches which demonstrated that p63 and the other four polypeptides have common coding sequences. An amino-terminal peptide of p63 failed to elicit an immune response in rabbits. Antibodies raised against the p63 carboxy-terminal peptide inhibited poliovirus replicase and polyuridylic acid polymerase activities in vitro, providing strong support for earlier suggestions that these activities are a property of a single virus-specific polypeptide.
机译:化学合成脊髓灰质炎病毒复制酶蛋白(p63)的羧基末端肽,将其与牛血清白蛋白载体偶联,然后注射到兔中。产生的抗血清与脊髓灰质炎病毒感染的HeLa细胞中的六种病毒特异性蛋白反应:NCVP 0b,NCVP 1b,NCVP 2,约60,000道尔顿的蛋白质,p63和NCVP 6b。 60,000道尔顿蛋白的身份尚不清楚,但其他结果与以前的实验方法一致,后者证明了p63和其他四个多肽具有共同的编码序列。 p63的氨基末端肽未能在兔中引发免疫反应。针对p63羧基末端肽的抗体在体外抑制了脊髓灰质炎病毒复制酶和聚尿苷酸聚合酶的活性,为这些活性是单个病毒特异性多肽的特性的早期建议提供了有力的支持。

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  • 作者单位
  • 年度 1982
  • 总页数
  • 原文格式 PDF
  • 正文语种 {"code":"en","name":"English","id":9}
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