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干扰素诱导抗病毒反应需要胸苷激酶。

Induction of an antiviral response by interferon requires thymidine kinase.

作者信息

Lewis J A, Mengheri E, Esteban M

出版信息

Proc Natl Acad Sci U S A. 1983 Jan;80(1):26-30. doi: 10.1073/pnas.80.1.26.

Abstract

Mouse fibroblastoid cells (Ltk-) that lack thymidine kinase (tk) activity are unable to respond to murine beta-interferon by establishing antiviral activity or inducing the double-stranded RNA-dependent enzymes, oligo[(2'-5')A] polymerase and Mr 68,000 protein kinase. In contrast, the parental L-929 cell line or clonal derivatives of Ltk- cells into which the herpes virus tk gene was introduced by DNA-mediated gene transfer respond normally to interferon in developing resistance to viral infection and in inducing double-stranded RNA-dependent enzymes. Further evidence for a role of tk in the response to interferon was obtained by isolating revertants of tk+ clones that lost the herpes virus tk gene during growth in BrdUrd-containing medium. In such revertant sublines both tk enzyme activity and viral tk genes were undetectable and treatment with interferon failed to produce an antiviral effect or induce synthesis of the double-stranded RNA-dependent enzymes. Our results indicate that the ability of mouse L cells to respond to beta-interferon is dependent upon the presence of a functional tk gene. We propose that the induction of antiviral responses by interferon stringently requires a metabolite, the level of which is determined by tk activity. The system described may provide a means for elucidating the mechanisms by which responses to interferon are induced.

摘要

缺乏胸苷激酶(tk)活性的小鼠成纤维样细胞(Ltk-)无法通过建立抗病毒活性或诱导双链RNA依赖性酶、寡聚[(2'-5')A]聚合酶和68,000分子量蛋白激酶来对小鼠β干扰素产生反应。相比之下,通过DNA介导的基因转移将疱疹病毒tk基因导入的亲本L-929细胞系或Ltk-细胞的克隆衍生物,在产生对病毒感染的抗性和诱导双链RNA依赖性酶方面对干扰素的反应正常。通过分离在含BrdUrd培养基中生长期间失去疱疹病毒tk基因的tk+克隆的回复突变体,获得了tk在对干扰素反应中起作用的进一步证据。在这种回复突变亚系中,既检测不到tk酶活性,也检测不到病毒tk基因,用干扰素处理未能产生抗病毒作用或诱导双链RNA依赖性酶的合成。我们的结果表明,小鼠L细胞对β干扰素产生反应的能力取决于功能性tk基因的存在。我们提出,干扰素诱导抗病毒反应严格需要一种代谢物,其水平由tk活性决定。所描述的系统可能为阐明诱导对干扰素反应的机制提供一种手段。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4339/393302/4e2334ff348c/pnas00627-0042-a.jpg

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