首页> 美国卫生研究院文献>Journal of Virology >Wide Variations in Herpes Simplex Virus Type 1 Inoculum Dose and Latency-Associated Transcript Expression Phenotype Do Not Alter the Establishment of Latency in the Rabbit Eye Model
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Wide Variations in Herpes Simplex Virus Type 1 Inoculum Dose and Latency-Associated Transcript Expression Phenotype Do Not Alter the Establishment of Latency in the Rabbit Eye Model

机译:单纯疱疹病毒1型接种剂量和与潜伏期相关的转录表达表型的广泛差异不会改变兔眼模型中潜伏期的建立。

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摘要

The latency-associated transcript (LAT) is required for efficient reactivation of herpes simplex virus type 1 from latent infection in the rabbit eye model, but LAT's mechanism of action is unknown. In addition to reactivation, the LAT region seems to correspond to multiple functions, with some LAT deletion mutants exhibiting increased virulence, increased neuronal death, and restricted establishment of latency. While a LAT promoter deletion mutant (17ΔPst) seems to be primarily restricted in reactivation in the rabbit, subtle effects on virulence or the establishment of latency cannot be precluded at the normal high levels of virus inoculum used in the rabbit model. Since such additional LAT phenotypes may be more evident with lower doses of virus, we evaluated the influence of initial viral inoculum and LAT expression on the progression of acute infection and the establishment of latency. We have assayed both virus recovery rates and viral genome loads in rabbit corneas and trigeminal ganglia. Our results show that (i) in the corneas and trigeminal ganglia, the maximum amount of virus present during acute infection is independent of the LAT genotype and inoculum dose, although greater viral yields are obtained earlier with higher inoculum doses, and (ii) the range in numbers of latent genomes detected in the ganglia is independent of the inoculum dose and the LAT genotype and therefore no difference in establishment of latency is observed.
机译:要从兔眼模型中的潜伏感染中有效地激活1型单纯疱疹病毒,需要与潜伏期相关的转录本(LAT),但是LAT的作用机理尚不清楚。除了重新激活外,LAT区似乎还具有多种功能,其中一些LAT缺失突变体表现出增加的毒力,增加的神经元死亡和有限的潜伏期。虽然LAT启动子缺失突变体(17ΔPst)似乎在兔的再激活中受到主要限制,但在兔模型中使用的正常高水平病毒接种量下,不能排除对毒力的微妙影响或潜伏期的建立。由于这种另外的LAT表型可能在较低剂量的病毒中更加明显,因此我们评估了初始病毒接种物和LAT表达对急性感染进展和潜伏期的影响。我们已经测定了兔子角膜和三叉神经节的病毒回收率和病毒基因组负荷。我们的结果表明(i)在角膜和三叉神经节中,急性感染过程中存在的最大病毒量与LAT基因型和接种量无关,尽管接种量越高,病毒产量越早,并且(ii)在神经节中检测到的潜在基因组数目的范围与接种剂量和LAT基因型无关,因此在潜伏期的建立上没有观察到差异。

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