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干扰素可增强道迪细胞中爱泼斯坦-巴尔病毒早期抗原的表达。

Interferon enhances the expression of epstein-Barr virus early antigen in Daudi cells.

作者信息

Tovey M G, Dron M, Gresser I

出版信息

J Gen Virol. 1982 May;60(Pt 1):31-8. doi: 10.1099/0022-1317-60-1-31.

Abstract

Treatment of the Burkitt lymphoma-derived cell line Daudi with highly purified human interferon-alpha (IFN-alpha) increased up to 100-fold the number of cells expressing Epstein-Barr virus (EBV)-determined early antigen (EA) without inducing the synthesis of virus capsid antigen (VCA), a late virus function. The increase in the number of EA-positive cells was proportional to interferon concentration up to 10(4) international units (IU)/ml. Treatment of Daudi cells with the same number of units of either partially purified (sp. act. 10(6) IU/mg protein) or electrophoretically pure (sp. act. 2 x 10(8) IU/mg protein) IFN-alpha both gave a similar increase in EA expression, strongly suggesting that the effects observed were indeed due to interferon. Furthermore, treatment of relatively interferon-insensitive Raji cells with IFN-alpha (1 to 10(4) IU/ml) had no significant effect on either spontaneous or 5-iodo-2'-deoxyuridine (IdUrd)-induced expression of EA or VCA. Human IFN-beta also enhanced the expression of EBV EA in Daudi cells. In contrast, when the latent EBV present in Daudi cells was activated to enter into a replicative cycle, either by induction with IdUrd or by superinfection with the non-transforming P3HR1 strain of EBV, then treatment with human IFN-alpha caused a marked inhibition of EA expression. Our results suggest that interferon can exert a differential action on virus replication depending upon the state of the virus genome within the cell.

摘要

用高度纯化的人α干扰素(IFN-α)处理伯基特淋巴瘤衍生的细胞系Daudi,可使表达爱泼斯坦-巴尔病毒(EBV)决定的早期抗原(EA)的细胞数量增加多达100倍,而不诱导病毒衣壳抗原(VCA,一种病毒晚期功能)的合成。EA阳性细胞数量的增加与干扰素浓度成正比,最高可达10⁴国际单位(IU)/毫升。用相同单位数量的部分纯化(比活性为10⁶IU/毫克蛋白)或电泳纯(比活性为2×10⁸IU/毫克蛋白)的IFN-α处理Daudi细胞,EA表达均有类似增加,强烈表明观察到的效应确实是由于干扰素所致。此外,用IFN-α(1至10⁴IU/毫升)处理相对干扰素不敏感的Raji细胞,对EA或VCA的自发表达或5-碘-2'-脱氧尿苷(IdUrd)诱导的表达均无显著影响。人IFN-β也增强了Daudi细胞中EBV EA的表达。相反,当Daudi细胞中潜伏的EBV被激活进入复制周期时,无论是通过IdUrd诱导还是通过用EBV的非转化P3HR1株进行超感染,那么用人IFN-α处理会导致EA表达受到显著抑制。我们的结果表明,干扰素可根据细胞内病毒基因组的状态对病毒复制发挥不同作用。

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