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Adaptive Immune Responses To Zika Virus Are Important For Controlling Virus Infection And Preventing Infection In Brain And Testes

机译:对寨卡病毒的适应性免疫反应对于控制病毒感染和预防脑部和睾丸感染非常重要

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摘要

The recent association between Zika Virus (ZIKV) and neurological complications including Guillain-Barré Syndrome (GBS) in adults and CNS abnormalities in fetuses highlights the urgency to understand the immunological mechanisms controlling this emerging infection. Studies have indicated that ZIKV evades the human type I IFN response suggesting a role for the adaptive immune response in resolving infection. However, the inability of ZIKV to antagonize the mouse IFN response renders the virus highly susceptible to circulating IFN in murine models. Thus, as we show here, although wild type C57BL/6 mice mount both cell-mediated and humoral adaptive immune responses to ZIKV, these responses were not required to prevent disease. However, when the type I IFN response of mice was suppressed, then the adaptive immune responses became critical. For example, when type I IFN signaling was blocked by antibodies in Rag1−/− immunodeficient mice, the mice showed dramatic weight loss and ZIKV infection in the brain and testes. This phenotype was not observed in Rag1−/− mice or mice treated with anti-IFNAR alone. Furthermore, we found that the CD8+ T cell responses of pregnant mice to ZIKV infection were diminished compared to non-pregnant mice. It is possible that diminished cell-mediated immunity during pregnancy could increase virus spread to the fetus. These results demonstrate an important role for the adaptive immune response in control of ZIKV infection, and imply that vaccination may prevent ZIKV-related disease, particularly when the type I IFN response is suppressed as it is in humans.
机译:寨卡病毒(ZIKV)和神经系统并发症,包括成人格林-巴利综合征(GBS)和胎儿中枢神经系统异常之间的最新关联,凸显了迫切需要了解控制这种新发感染的免疫机制。研究表明,ZIKV逃避了人类的I型IFN反应,提示了适应性免疫反应在解决感染中的作用。但是,ZIKV不能拮抗小鼠IFN反应,使得该病毒高度易受鼠模型中循环IFN的影响。因此,正如我们在此处显示的,尽管野生型C57BL / 6小鼠对ZIKV发出了细胞介导的和体液适应性免疫应答,但这些应答对于预防疾病并不是必需的。但是,当抑制小鼠的I型IFN反应时,适应性免疫反应就变得至关重要。例如,当免疫缺陷小鼠Rag1 -/-中的抗体阻断I型IFN信号传导时,小鼠的大脑和睾丸显示出明显的体重减轻和ZIKV感染。在Rag1 -/-小鼠或仅接受抗IFNAR治疗的小鼠中未观察到此表型。此外,我们发现与未怀孕的小鼠相比,怀孕小鼠对ZIKV感染的CD8 + T细胞反应减弱。怀孕期间细胞介导的免疫力降低可能会增加病毒向胎儿的传播。这些结果证明了适应性免疫应答在控制ZIKV感染中起着重要作用,并暗示疫苗接种可以预防ZIKV相关疾病,特别是当I型IFN应答像在人类中一样被抑制时。

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