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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Treatment of SIV-infected sooty mangabeys with a type-I IFN agonist results in decreased virus replication without inducing hyperimmune activation
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Treatment of SIV-infected sooty mangabeys with a type-I IFN agonist results in decreased virus replication without inducing hyperimmune activation

机译:用I型IFN激动剂治疗SIV感染的黑烟病,可导致病毒复制减少而不诱导超免疫激活

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A key feature differentiating nonpathogenic SIV infection of sooty mangabeys (SMs) from pathogenic HIV/SIV infections is the rapid resolution of type I IFN (IFN-I) responses and IFN-stimulated gene expression during the acute-to-chronic phase transition and the establishment of an immune quiescent state that persists throughout the chronic infection. We hypothesized that low levels of IFN-I signaling may help to prevent chronic immune activation and disease progression in SIV-infected SMs. To assess the effects of IFN-I signaling in this setting, in the present study, we administered recombinant rhesus macaque IFNα2-IgFc (rmIFNα2) to 8 naturally SIV-infected SMs weekly for 16 weeks. Gene-expression profiling revealed a strong up-regulation of IFN-stimulated genes in the blood of treated animals, confirming the reagent's bioactivity. Interestingly, we observed an approximately 1-log decrease in viral load that persisted through day 35 of treatment. Flow cytometric analysis of lymphocytes in the blood, lymph nodes, and rectal biopsies did not reveal a significant decline of CD4+ T cells, a robust increase in lymphocyte activation, or change in the level of SIV-specific CD8+ T cells. The results of the present study indicate that administration of type I IFNs in SIV-infected SMs induces a significant antiviral effect that is not associated with a detectable increase in chronic immune activation.
机译:区分黑点菜豆(SMs)的非致病性SIV感染和致病性HIV / SIV感染的一个关键特征是,在急性至慢性相变期间,I型IFN(IFN-I)反应和IFN刺激基因表达的快速解决。建立在整个慢性感染中持续存在的免疫静止状态。我们假设低水平的IFN-I信号传导可能有助于预防SIV感染的SM的慢性免疫激活和疾病进展。为了评估在这种情况下IFN-I信号传导的作用,在本研究中,我们每周将重组恒河猴猕猴IFNα2-IgFc(rmIFNα2)施用到8个自然感染SIV的SM中,持续16周。基因表达谱分析显示,经处理的动物血液中有IFN刺激的基因强烈上调,从而证实了该试剂的生物活性。有趣的是,我们观察到在治疗的第35天,病毒载量下降了约1个对数。血液,淋巴结和直肠活检中淋巴细胞的流式细胞仪分析未发现CD4 + T细胞显着下降,淋巴细胞活化显着增加或SIV特异性CD8 + T细胞水平改变。本研究的结果表明,在SIV感染的SM中施用I型IFN诱导了显着的抗病毒作用,与慢性免疫激活的可检测增加无关。

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