α/β干扰素在委内瑞拉马脑炎病毒致病机制中的作用:5'非翻译区减毒突变的影响
Role of alpha/beta interferon in Venezuelan equine encephalitis virus pathogenesis: effect of an attenuating mutation in the 5' untranslated region.
作者信息
White L J, Wang J G, Davis N L, Johnston R E
机构信息
Department of Microbiology and Immunology, University of North Carolina at Chapel Hill, Chapel Hill, North Carolina 27599-7290, USA.
出版信息
J Virol. 2001 Apr;75(8):3706-18. doi: 10.1128/JVI.75.8.3706-3718.2001.
Venezuelan equine encephalitis virus (VEE) is an important equine and human pathogen of the Americas. In the adult mouse model, cDNA-derived, virulent V3000 inoculated subcutaneously (s.c.) causes high-titer peripheral replication followed by neuroinvasion and lethal encephalitis. A single change (G to A) at nucleotide 3 (nt 3) of the 5' untranslated region (UTR) of the V3000 genome resulted in a virus (V3043) that was avirulent in mice. The mechanism of attenuation by the V3043 mutation was studied in vivo and in vitro. Kinetic studies of virus spread in adult mice following s.c. inoculation showed that V3043 replication was reduced in peripheral organs compared to that of V3000, titers in serum also were lower, and V3043 was cleared more rapidly from the periphery than V3000. Because clearance of V3043 from serum began 1 to 2 days prior to clearance of V3000, we examined the involvement of alpha/beta interferon (IFN-alpha/beta) activity in VEE pathogenesis. In IFN-alpha/betaR(-/-) mice, the course of the wild-type disease was extremely rapid, with all animals dying within 48 h (average survival time of 30 h compared to 7.7 days in the wild-type mice). The mutant V3043 was as virulent as the wild type (100% mortality, average survival time of 30 h). Virus titers in serum, peripheral organs, and the brain were similar in V3000- and V3043-infected IFN-alpha/betaR(-/-) mice at all time points up until the death of the animals. Consistent with the in vivo data, the mutant virus exhibited reduced growth in vitro in several cell types except in cells that lacked a functional IFN-alpha/beta pathway. In cells derived from IFN-alpha/betaR(-/-) mice, the mutant virus showed no growth disadvantage compared to the wild-type virus, suggesting that IFN-alpha/beta plays a major role in the attenuation of V3043 compared to V3000. There were no differences in the induction of IFN-alpha/beta between V3000 and V3043, but the mutant virus was more sensitive than V3000 to the antiviral actions of IFN-alpha/beta in two separate in vitro assays, suggesting that the increased sensitivity to IFN-alpha/beta plays a major role in the in vivo attenuation of V3043.
委内瑞拉马脑炎病毒(VEE)是美洲一种重要的马和人类病原体。在成年小鼠模型中,经皮下接种(s.c.)的cDNA衍生的强毒株V3000会导致外周高滴度复制,随后发生神经侵袭和致死性脑炎。V3000基因组5'非翻译区(UTR)核苷酸3(nt 3)处的单个变化(G变为A)产生了一种在小鼠中无毒的病毒(V3043)。对V3043突变减毒的机制进行了体内和体外研究。对成年小鼠皮下接种后病毒传播的动力学研究表明,与V3000相比,V3043在外周器官中的复制减少,血清中的滴度也较低,并且V3043比V3000更快地从外周清除。由于V3043从血清中的清除比V3000提前1至2天开始,我们研究了α/β干扰素(IFN-α/β)活性在VEE发病机制中的作用。在IFN-α/βR(-/-)小鼠中,野生型疾病的病程极其迅速,所有动物在48小时内死亡(平均存活时间为30小时,而野生型小鼠为7.7天)。突变体V3043与野生型一样具有毒性(100%死亡率,平均存活时间为30小时)。在所有时间点直至动物死亡时,V3000和V3043感染的IFN-α/βR(-/-)小鼠血清、外周器官和大脑中的病毒滴度相似。与体内数据一致,除了缺乏功能性IFN-α/β途径的细胞外,突变病毒在几种细胞类型中的体外生长均减少。在源自IFN-α/βR(-/-)小鼠的细胞中,突变病毒与野生型病毒相比没有生长劣势,这表明与V3000相比,IFN-α/β在V3043的减毒中起主要作用。V3000和V3043之间在IFN-α/β的诱导方面没有差异,但在两项独立的体外试验中,突变病毒比V3000对IFN-α/β的抗病毒作用更敏感,这表明对IFN-α/β敏感性的增加在V3043的体内减毒中起主要作用。
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