Department of Biology, Viral Immunology Center, Georgia State University, Atlanta, Georgia, United States of America.
Department of Ophthalmology, Emory University School of Medicine, Atlanta, Georgia, United States of America.
PLoS Pathog. 2020 Nov 6;16(11):e1009032. doi: 10.1371/journal.ppat.1009032. eCollection 2020 Nov.
Human cytomegalovirus (HCMV) is an opportunistic human herpesvirus that causes a sight-threatening retinitis in immunosuppressed patients, especially those with AIDS. Using an established model of experimental murine cytomegalovirus (MCMV) retinitis in mice with retrovirus-induced immunodeficiency (MAIDS), we have been attempting to define with greater clarity the immunologic mechanisms that contribute to the progression of AIDS-related HCMV retinitis in the unique immunosuppressive setting of HIV infection. Toward this end, we provide herein a comprehensive assessment of immune response gene expression during the onset and development of MAIDS-related MCMV retinitis employing NanoString nCounter. In so doing, we analyzed and compared the intraocular expressions of 561 immune response genes within MCMV-infected eyes of groups of healthy mice, MCMV-infected mice with MAIDS of 4 weeks' (MAIDS-4) duration, and MCMV-infected eyes of mice with MAIDS of 10 weeks' (MAIDS-10) duration. These animal groups show a progression of retinal disease from absolute resistance to retinitis development in healthy mice to the development of classic full-thickness retinal necrosis in MAIDS-10 mice but through an intermediate stage of retinal disease development in MAIDS-4 mice. Our findings showed that increased susceptibility to MCMV retinitis during the progression of MAIDS is associated with robust upregulation or downregulation of a surprisingly large number of immune response genes that operate within several immune response pathways often unique to each animal group. Analysis of 14 additional immune response genes associated with programmed cell death pathways suggested involvement of necroptosis and pyroptosis during MAIDS-related MCMV retinitis pathogenesis. Use of the NanoString nCounter technology provided new and unexpected information on the immunopathogenesis of retinitis within MCMV-infected eyes of mice with retrovirus-induced immunosuppression. Our findings may provide new insights into the immunologic events that operate during the pathogenesis of AIDS-related HCMV retinitis.
人巨细胞病毒(HCMV)是一种机会性人类疱疹病毒,可导致免疫抑制患者(尤其是艾滋病患者)出现视力威胁性视网膜炎。我们使用逆转录病毒诱导免疫缺陷(MAIDS)小鼠中实验性鼠巨细胞病毒(MCMV)视网膜炎的既定模型,试图更清楚地定义有助于 HIV 感染中 AIDS 相关 HCMV 视网膜炎进展的免疫机制。为此,我们在此采用 NanoString nCounter 对 MAIDS 相关 MCMV 视网膜炎发病和发展过程中的免疫反应基因表达进行全面评估。通过这种方式,我们分析并比较了健康小鼠、MAIDS 持续 4 周(MAIDS-4)的 MCMV 感染小鼠以及 MAIDS 持续 10 周(MAIDS-10)的 MCMV 感染小鼠眼内的 561 种免疫反应基因的眼内表达。这些动物组显示出视网膜疾病从健康小鼠对视网膜发育绝对抵抗进展到 MAIDS-10 小鼠出现典型全层视网膜坏死,而 MAIDS-4 小鼠经历了视网膜疾病发展的中间阶段。我们的研究结果表明,在 MAIDS 进展过程中对 MCMV 视网膜炎的易感性增加与大量免疫反应基因的显著上调或下调有关,这些基因在几个免疫反应途径中发挥作用,这些途径通常对每个动物组都是独特的。对与程序性细胞死亡途径相关的 14 个其他免疫反应基因的分析表明,在 MAIDS 相关 MCMV 视网膜炎发病机制中涉及坏死性凋亡和细胞焦亡。使用 NanoString nCounter 技术提供了关于逆转录病毒诱导免疫抑制的 MCMV 感染小鼠眼内视网膜炎发病机制的新的、意外信息。我们的研究结果可能为 AIDS 相关 HCMV 视网膜炎发病机制中涉及的免疫事件提供新的见解。
Zotero 插件
