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Innate Immune Responses and Permissiveness to Ranavirus Infection of Peritoneal Leukocytes in the Frog Xenopus laevis▿

机译:蛙爪蟾腹膜白细胞固有免疫反应和对蛙病毒感染的允许性

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摘要

Ranaviruses such as frog virus 3 ([FV3] family Iridoviridae) are increasingly prevalent pathogens that infect reptiles, amphibians, and fish worldwide. Whereas studies in the frog Xenopus laevis have revealed the critical involvement of CD8 T-cell and antibody responses in host resistance to FV3, little is known about the role played by innate immunity to infection with this virus. We have investigated the occurrence, composition, activation status, and permissiveness to infection of peritoneal leukocytes (PLs) in Xenopus adults during FV3 infection by microscopy, flow cytometry, and reverse transcription-PCR. The total number of PLs and the relative fraction of activated mononucleated macrophage-like cells significantly increase as early as 1 day postinfection (dpi), followed by NK cells at 3 dpi, before the peak of the T-cell response at 6 dpi. FV3 infection also induces a rapid upregulation of proinflammatory genes including arginase 1, interleukin-1β, and tumor necrosis factor alpha. Although PLs are susceptible to FV3 infection, as evidenced by apoptotic cells, active FV3 transcription, and the detection of viral particles by electron microscopy, the infection is weaker (fewer infectious particles), more transitory, and involves a smaller fraction (less than 1%) of PLs than the kidney, the main site of infection. However, viral DNA remains detectable in PLs for at least 3 weeks postinfection, past the point of viral clearance observed in the kidneys. This suggests that although PLs are actively involved in anti-FV3 immune responses, some of these cells can be permissive and harbor quiescent, asymptomatic FV3.
机译:蛙病毒,例如青蛙病毒3([FV3]虹膜病毒科),是越来越普遍的病原体,可感染全世界的爬行动物,两栖动物和鱼类。尽管对青蛙非洲爪蟾的研究表明CD8 T细胞和抗体应答在宿主对FV3的抗性中起关键作用,但对这种病毒感染的先天免疫所起的作用知之甚少。我们已经通过显微镜,流式细胞仪和逆转录-PCR研究了非洲爪蟾成虫在FV3感染期间腹膜白细胞(PLs)感染的发生,组成,激活状态和允许性。早在感染后第1天(dpi),PL的总数和活化的单核巨噬细胞样细胞的相对分数就显着增加,然后是3 dpi的NK细胞,然后才是6 dpi的T细胞反应高峰。 FV3感染还诱导促炎基因的快速上调,包括精氨酸酶1,白介素-1β和肿瘤坏死因子α。尽管PL易受FV3感染,如凋亡细胞,活跃的FV3转录以及通过电子显微镜检测病毒颗粒所证明,但感染较弱(感染性颗粒较少),瞬时性更强,并且感染程度较小(小于1) %)PLs超过肾脏,是感染的主要部位。但是,在感染后至少3周内,在肾脏中仍可检测到病毒DNA,超过了在肾脏中观察到的病毒清除点。这表明,尽管PL积极参与抗FV3免疫反应,但其中一些细胞可能是允许的,并具有静止的,无症状的FV3。

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