基因型 VIId 新城疫病毒感染鸡脾细胞中强烈的固有免疫反应和细胞死亡。
Strong innate immune response and cell death in chicken splenocytes infected with genotype VIId Newcastle disease virus.
机构信息
Animal Infectious Disease Laboratory, School of Veterinary Medicine, Yangzhou University, 12 East Wenhui Road, Yangzhou Jiangsu Province, 225009, China.
出版信息
Virol J. 2012 Sep 18;9:208. doi: 10.1186/1743-422X-9-208.
BACKGROUND
Genotype VIId Newcastle disease virus (NDV) isolates induce more severe damage to lymphoid tissues, especially to the spleen, when compared to virulent viruses of other genotypes. However, the biological basis of the unusual pathological changes remains largely unknown.
METHODS
Virus replication, cytokine gene expression profile and cell death response in chicken splenocytes infected with two genotype VIId NDV strains (JS5/05 and JS3/05), genotype IX NDV strain F48E8 and genotype IV NDV strain Herts/33 were evaluated. Statistical significance of differences between experimental groups was determined using the Independent-Samples T test.
RESULTS
JS5/05 and JS3/05 caused hyperinduction of type I interferons (IFNs) (IFN-α and -β) during detection period compared to F48E8 and Herts/33. JS5/05 increased expression level of IFN-γ gene at 6 h post-inoculation (pi) and JS3/05 initiated sustained activation of IFN-γ within 24 h pi, whereas transcriptional levels of IFN-γ remained unchanged at any of the time points during infection of F48E8 and Herts/33. In addition, compared to F48E8 and Herts/33, JS3/05 and JS5/05 significantly increased the amount of free nucleosomal DNA in splenocytes at 6 and 24 h pi respectively. Annexin-V and Proidium iodid (PI) double staining of infected cells showed that cell death induced by JS3/05 and JS5/05 was characterized by marked necrosis compared to F48E8 and Herts/33 at 24 h pi. These results indicate that genotype VIId NDV strains JS3/05 and JS5/05 elicited stronger innate immune and cell death responses in chicken splenocytes than F48E8 and Herts/33. JS5/05 replicated at a significantly higher efficiency in splenocytes than F48E8 and Herts/33. Early excessive cell death induced by JS3/05 infection partially impaired virus replication.
CONCLUSIONS
Viral dysregulaiton of host response may be relevant to the severe pathological manifestation in the spleen following genotype VIId NDV infection.
背景
与其他基因型的强毒相比,基因型 VIId 新城疫病毒(NDV)分离株感染后更易引起淋巴组织,尤其是脾脏的严重损伤。然而,其异常病理变化的生物学基础仍知之甚少。
方法
本研究评估了两株基因型 VIId NDV 株(JS5/05 和 JS3/05)、一株基因型 IX NDV 株 F48E8 和一株基因型 IV NDV 株 Herts/33 感染鸡脾细胞后的病毒复制、细胞因子基因表达谱和细胞死亡反应。使用独立样本 T 检验确定实验组之间差异的统计学意义。
结果
与 F48E8 和 Herts/33 相比,JS5/05 和 JS3/05 在检测期内引起 I 型干扰素(IFN-α和-β)的过度诱导。JS5/05 在接种后 6 小时(pi)增加 IFN-γ 基因的表达水平,JS3/05 在 24 小时 pi 内持续激活 IFN-γ,而 F48E8 和 Herts/33 感染过程中任何时间点 IFN-γ 的转录水平均无变化。此外,与 F48E8 和 Herts/33 相比,JS3/05 和 JS5/05 分别在 6 和 24 pi 时显著增加了脾细胞中游离核小体 DNA 的量。感染细胞的 Annexin-V 和碘化丙啶(PI)双重染色表明,与 F48E8 和 Herts/33 相比,JS3/05 和 JS5/05 诱导的细胞死亡在 24 pi 时以明显的坏死为特征。这些结果表明,基因型 VIId NDV 株 JS3/05 和 JS5/05 在鸡脾细胞中引发的固有免疫和细胞死亡反应强于 F48E8 和 Herts/33。JS5/05 在脾细胞中的复制效率明显高于 F48E8 和 Herts/33。JS3/05 感染早期过度的细胞死亡部分抑制了病毒复制。
结论
宿主反应的病毒失调可能与基因型 VIId NDV 感染后脾脏的严重病理表现有关。
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