首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Structural features of double-stranded polyribonucleotides required for immunological specificity and interferon induction.
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Structural features of double-stranded polyribonucleotides required for immunological specificity and interferon induction.

机译:免疫特异性和干扰素诱导所需的双链多核糖核苷酸的结构特征。

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摘要

Purified antibody to poly(adenylic acid)-poly(uridylic acid) was used in quantitative microcomplement fixation assays to detect conformational variations among several double-helical polyribonucleotide analogs of poly(adenylic acid)-poly(uridylic acid) or poly(inosinic acid)-poly(cytidylic acid) that had been previously evaluated for their ability to induce interferon. Modification at the furanose 2'-position of one or both strands resulted in a dramatic decrease in serological reactivity. Most modifications of the bases caused smaller serological changes, and no base modification caused complete loss of reactivity. The reaction patterns support the conclusion that the structure of the furanose and the overall conformation of the helix are critical in the formation of antigenic determinants. The backbones of both strands appear to be involved in forming a single antigenic site, and base modifications may alter the steric relationship between the backbones. In addition, the same structural changes that substantially alter recognition by antibody also lead to large changes in the interferon-inducing ability of the nucleic acid.
机译:纯化的聚腺苷酸-聚尿苷酸抗体用于定量微补体固定分析,以检测聚腺苷酸-聚尿苷酸或肌苷酸的几种双螺旋聚核糖核苷酸类似物之间的构象变异-先前已评估了其诱导干扰素能力的聚(胞苷酸)。一条或两条链的呋喃糖2'-位修饰导致血清学反应性急剧下降。碱基的大多数修饰引起较小的血清学变化,并且没有碱基修饰引起反应性完全丧失。反应模式支持以下结论:呋喃糖的结构和螺旋的整体构象对抗原决定簇的形成至关重要。两条链的主链似乎都参与形成单个抗原位点,并且碱基修饰可能会改变主链之间的空间关系。另外,实质上改变抗体识别的相同结构改变也导致核酸的干扰素诱导能力的大改变。

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