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Dengue viruses cleave STING in humans but not in nonhuman primates, their presumed natural reservoir

机译:登革热病毒会在人类中切割STING,但在非人类灵长类动物中却不会切割STING,这是它们的天然储备

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摘要

Human dengue viruses emerged from primate reservoirs, yet paradoxically dengue does not reach high titers in primate models. This presents a unique opportunity to examine the genetics of spillover versus reservoir hosts. The dengue virus 2 (DENV2) - encoded protease cleaves human STING, reducing type I interferon production and boosting viral titers in humans. We find that both human and sylvatic (reservoir) dengue viruses universally cleave human STING, but not the STING of primates implicated as reservoir species. The special ability of dengue to cleave STING is thus specific to humans and a few closely related ape species. Conversion of residues 78/79 to the human-encoded ‘RG’ renders all primate (and mouse) STINGs sensitive to viral cleavage. Dengue viruses may have evolved to increase viral titers in the dense and vast human population, while maintaining decreased titers and pathogenicity in the more rare animals that serve as their sustaining reservoir in nature.
机译:人类登革热病毒从灵长类动物库中出现,但自相矛盾的是,登革热在灵长类动物模型中并未达到高滴度。这提供了一个独特的机会来检查溢油与油藏宿主之间的遗传关系。登革热病毒2(DENV2)编码的蛋白酶可裂解人的STING,减少I型干扰素的产生并提高人的病毒效价。我们发现,人类和西尔维克(水库)登革热病毒都普遍切割人类的STING,但不能切割与水库物种有关的灵长类动物的STING。因此,登革热裂解STING的特殊能力是人类和一些紧密相关的猿类物种所特有的。将残基78/79转换为人类编码的“ RG”可使所有灵长类(和小鼠)STINGs对病毒裂解敏感。登革热病毒可能已经进化为增加人口稠密人群的病毒滴度,同时保持了稀有动物的滴度和致病性,而稀有动物在自然界中是它们的维持库。

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