线粒体亢进和活性氧驱动黄热病病毒-17D减毒活疫苗的先天免疫力

Samantha G Muccilli, Bejamin Schwarz, Forrest Jessop, Jeffrey G. Shannon, Eric Bohrnsen, Byron Shue, Seon-Hui Hong, Thomas Hsu, Alison W. Ashbrook, Joseph W. Guarnieri, Justin Lack, Douglas C. Wallace, Catharine M. Bosio, Margaret R. MacDonald, Charles M Rice, Jonathan W Yewdell, Sonja M. Best
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摘要

黄热病病毒 17D(YFV-17D)减毒活疫苗被认为是迄今为止成功的疫苗之一,具有很高的抗病毒免疫力,但人们对驱动受感染细胞产生反应的信号机制尚不清楚。在这里,我们从分子角度了解了新陈代谢压力和先天性免疫反应是如何联系在一起,以驱动 I 型 IFN 表达来应对 YFV-17D 感染的。将 YFV-17D 的复制与其亲本病毒 YFV-Asibi 和相关的登革热病毒进行比较后发现,IFN 的表达需要通过 MAVS 的 RIG-I-like Receptor 信号传导。然而,YFV-17D 能独特地诱导线粒体呼吸和主要的新陈代谢紊乱,包括电子传递亢进,为 ATP 合成酶提供能量。线粒体亢进会产生活性氧(mROS)和过氧亚硝酸盐,阻断活性氧和过氧亚硝酸盐会减弱非免疫细胞中 IFN 的表达,但不会减少 YFV-17D 的复制。清除受 YFV-17D 感染的人树突状细胞中的活性氧可提高细胞活力,但却全面阻止了 IFN 信号通路的表达。因此,YFV-17D 对高生长的适应性独特地赋予了线粒体亢进,产生的 mROS 和过氧化亚硝酸盐是关键的信使,它们能将被削弱的 IFN 反应转化为对疫苗有效性至关重要的先天性免疫的最大激活。
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Mitochondrial Hyperactivity and Reactive Oxygen Species Drive Innate Immunity to the Yellow Fever Virus-17D Live-Attenuated Vaccine
The yellow fever virus 17D (YFV-17D) live attenuated vaccine is considered one of the successful vaccines ever generated associated with high antiviral immunity, yet the signaling mechanisms that drive the response in infected cells are not understood. Here, we provide a molecular understanding of how metabolic stress and innate immune responses are linked to drive type I IFN expression in response to YFV-17D infection. Comparison of YFV-17D replication with its parental virus, YFV-Asibi, and a related dengue virus revealed that IFN expression requires RIG-I-like Receptor signaling through MAVS, as expected. However, YFV-17D uniquely induces mitochondrial respiration and major metabolic perturbations, including hyperactivation of electron transport to fuel ATP synthase. Mitochondrial hyperactivity generates reactive oxygen species (mROS) and peroxynitrite, blocking of which abrogated IFN expression in non-immune cells without reducing YFV-17D replication. Scavenging ROS in YFV-17D-infected human dendritic cells increased cell viability yet globally prevented expression of IFN signaling pathways. Thus, adaptation of YFV-17D for high growth uniquely imparts mitochondrial hyperactivity generating mROS and peroxynitrite as the critical messengers that convert a blunted IFN response into maximal activation of innate immunity essential for vaccine effectiveness.
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