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登革热2型抗原的免疫和生物物理分离

Immunological and biophysical separation of dengue-2 antigens.

作者信息

Cardiff R D, Brandt W E, McCloud T G, Shapiro D, Russell P K

出版信息

J Virol. 1971 Jan;7(1):15-23. doi: 10.1128/JVI.7.1.15-23.1971.

Abstract

Antigenic compositions of slowly sedimenting dengue-2 hemagglutinin (SHA) and soluble complement-fixing antigen (SCF) were compared with the virion (rapidly sedimenting hemagglutinin, RHA) by radioimmune precipitation (RIP), RIP inhibition, kinetic neutralization, and neutralization blocking tests with the use of hyperimmune mouse ascitic fluids. RHA and SHA were unable to inhibit completely the RIP of each other by anti-RHA, and neutralization by anti-RHA was not blocked by SHA. This indicated that SHA is serologically related, but not identical, to RHA. SHA differed from RHA in that SHA lacked the "core" polypeptide but contained the two envelope polypeptides. In addition, SHA contained a polypeptide with a molecular weight of 16,500 daltons and a suggestion of several other proteins. These data, when considered with other evidence, suggest that SHA is a special form of "incomplete virus." SCF was unable to inhibit the RIP of SHA or RHA or to block neutralizing antibodies. Further, anti-SCF did not neutralize RHA or precipitate significant levels of SHA or RHA. Polyacrylamide gel electrophoresis separated SCF from structural polypeptides by molecular size. This evidence suggests that SCF is a nonstructural antigen.

摘要

通过放射免疫沉淀(RIP)、RIP抑制、动力学中和以及使用超免疫小鼠腹水进行中和阻断试验,将缓慢沉降的登革2型血凝素(SHA)和可溶性补体结合抗原(SCF)的抗原组成与病毒体(快速沉降血凝素,RHA)进行了比较。RHA和SHA无法完全抑制抗RHA对彼此的RIP,并且抗RHA的中和作用也不会被SHA阻断。这表明SHA与RHA在血清学上相关,但并不相同。SHA与RHA的不同之处在于,SHA缺乏“核心”多肽,但含有两种包膜多肽。此外,SHA含有一种分子量为16,500道尔顿的多肽以及其他几种蛋白质的迹象。这些数据与其他证据一起考虑时,表明SHA是“不完全病毒”的一种特殊形式。SCF无法抑制SHA或RHA的RIP,也无法阻断中和抗体。此外,抗SCF不会中和RHA,也不会沉淀显著水平的SHA或RHA。聚丙烯酰胺凝胶电泳按分子大小将SCF与结构多肽分开。这一证据表明SCF是一种非结构抗原。

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