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细菌衍生的人α干扰素对小鼠脑心肌炎病毒感染的抗病毒活性。

Antiviral activity of bacteria-derived human alpha interferons against encephalomyocarditis virus infection of mice.

作者信息

Weck P K, Rinderknecht E, Estell D A, Stebbing N

出版信息

Infect Immun. 1982 Feb;35(2):660-5. doi: 10.1128/iai.35.2.660-665.1982.

Abstract

Bacteria-derived human leukocyte interferon (IFN) subtypes, IFN-alpha A, -alpha B, and -alpha D, and two hybrid IFNs, IFN-alpha AD and -alpha DA, were examined for both in vitro and in vivo antiviral activity. Two of these materials in highly purified form (IFN-alpha D and -alpha D) protect mice against lethal doses of encephalomyocarditis virus infection. A single dose of 1 microgram of protein of IFN-alpha D 3 h before infection conferred protection in both BDF1 and CD-1 mice against encephalomyocarditis virus infection, and multiple treatments with IFN-alpha D or IFN-alpha AD extend the mean survival time of infected mice. On a weight basis, IFN-alpha AD was approximately 100-fold more effective than IFN-alpha D. There is a direct correlation between the antiviral activity of the various human IFN species in L-929 cells and in mice for both single and multiple treatments before infection, but none of the cloned human IFN subtypes were effective when administered 24 h after infection. Mixtures of the two parental materials, IFN-alpha A and -alpha D, were not as protective as the hybrid molecule IFN-alpha AD, suggesting that IFNs with unique and altered species specificity can be produced by recombinant DNA methods.

摘要

对细菌衍生的人白细胞干扰素(IFN)亚型,即IFN-αA、-αB和-αD,以及两种杂合干扰素,IFN-αAD和-αDA,进行了体外和体内抗病毒活性检测。其中两种高度纯化的物质(IFN-αD和-αD)可保护小鼠免受致死剂量脑心肌炎病毒感染。在感染前3小时,单剂量1微克的IFN-αD蛋白质可使BDF1和CD-1小鼠均免受脑心肌炎病毒感染,用IFN-αD或IFN-αAD多次治疗可延长感染小鼠的平均存活时间。以重量计,IFN-αAD的效力约为IFN-αD的100倍。在感染前进行单次和多次治疗时,各种人IFN在L-929细胞和小鼠中的抗病毒活性之间存在直接相关性,但在感染后24小时给予时,没有一种克隆的人IFN亚型有效。两种亲本物质IFN-αA和-αD的混合物不如杂合分子IFN-αAD具有保护作用,这表明可以通过重组DNA方法产生具有独特和改变的种属特异性的IFN。

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