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[不同多聚核糖核苷酸干扰素原对小鼠急性和潜伏性病毒感染的影响]

[Effect of different polyribonucleotide interferonogens on acute and latent viral infections in mice].

作者信息

Vil'ner L M, Kogan E M, Timkovskiĭ A L, Tiufanov A V, Finogenova E V

出版信息

Vopr Virusol. 1980 Jan-Feb(1):67-71.

PMID:7415152
Abstract

Poly(G) . poly(C) and poly(I) . poly(C) complexes administered soon after the viral challenge induced a high survival rate in mice with experimental tick-borne encephalitis. The protective effect was still noted when the treatment was given 24 hours after the infection. If the therapy was conducted at the end of the incubation period, at the peak of the virus reproduction in the mouse brain, poly(I) . poly(C) intensified the infection development and increased the animal death rate, while poly(G) . poly(C) had no such effect. Poly(I) . poly(C) injected 12 hours after the peak of the virus-induced interferonogenesis led to death of 80% animals inoculated with non-pathogenous Newcastle disease virus. The action of various samples of poly(I) . poly(C) was diverse. Poly(G) . poly(C) failed to effect the outcome of latent viral infection. The death of infected mice induced by polyribonucleotide complexes was not connected with their anti-viral interferonogenous activity, but correlated with the level of their toxicity for the intact animals. The results of the study have confirmed the risk of using poly(I) . poly(C) for the therapy of viral infections, especially during their clinical manifestation, and proved the safety of application of poly(G) . poly(C) and of some other polyribonucleotide interferonogens.

摘要

在病毒攻击后不久给予的聚(G)·聚(C)和聚(I)·聚(C)复合物可使患有实验性蜱传脑炎的小鼠存活率很高。在感染后24小时进行治疗时,仍可观察到保护作用。如果在潜伏期结束时、小鼠脑中病毒繁殖高峰期进行治疗,聚(I)·聚(C)会加剧感染发展并增加动物死亡率,而聚(G)·聚(C)则没有这种作用。在病毒诱导的干扰素生成高峰期后12小时注射聚(I)·聚(C),导致80%接种非致病性新城疫病毒的动物死亡。聚(I)·聚(C)的不同样本作用各异。聚(G)·聚(C)未能影响潜伏性病毒感染的结果。多聚核苷酸复合物诱导的感染小鼠死亡与其抗病毒干扰素生成活性无关,而是与其对正常动物的毒性水平相关。该研究结果证实了使用聚(I)·聚(C)治疗病毒感染的风险,尤其是在病毒感染临床表现期,并证明了聚(G)·聚(C)和其他一些多聚核苷酸干扰素原应用的安全性。

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