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巨细胞病毒感染后,角膜内皮细胞会激活抗病毒反应的先天性和获得性免疫分支。

Corneal endothelial cells activate innate and acquired arm of anti-viral responses after cytomegalovirus infection.

作者信息

Miyazaki Dai, Uotani Ryu, Inoue Michiko, Haruki Tomoko, Shimizu Yumiko, Yakura Keiko, Yamagami Satoru, Suzutani Tatsuo, Hosogai Mayumi, Isomura Hiroki, Inoue Yoshitsugu

机构信息

Division of Ophthalmology and Visual Science, Faculty of Medicine, Tottori University, Tottori, Japan.

Division of Ophthalmology and Visual Science, Faculty of Medicine, Tottori University, Tottori, Japan.

出版信息

Exp Eye Res. 2017 Aug;161:143-152. doi: 10.1016/j.exer.2017.06.017. Epub 2017 Jun 23.

Abstract

Infection of the corneal endothelial cells by human cytomegalovirus (CMV) is an important cause of corneal endotheliitis. CMV endotheliitis is difficult to completely cure and relapses are frequent. This can cause blinding corneal bullous keratopathy. However, the pathogenesis of CMV endotheliitis remains undetermined. To understand the immunopathology of endotheliitis, we examined how corneal endothelial cells prime the anti-viral immunity after CMV infection based on global transcriptional responses. To accomplish this, human corneal endothelial (HCEn) cells were infected with CMV, and the global transcriptional responses were determined by microarray analyses for primary anti-viral responses using network analysis. Real-time reverse transcriptase-polymerase chain reaction (RT-PCR) and protein array analyses were used to examine whether anti-viral cytokines were induced, i.e., to determine whether innate immune responses were activated. To examine whether priming of acquired immune response was activated, CMV-infected HCEn cells were co-cultured with allogeneic CD8 T cells from CMV seropositive donors and tested for priming activity for the CD8 effector T cells by measuring interferon-γ secretion. The CMV-induced responses of HCEn cells were characterized by type I interferon and pattern recognition receptor pathways which represent innate immune priming. The global transcriptional activation was specifically associated with antigen presentation with the antimicrobial response functions. Protein array analyses indicated a significant increase in the secretion of anti-viral inflammatory cytokines including CXCL10 as innate immune responses. When HCEn cells were examined to determine whether CMV infection activated anti-viral acquired immunity, CMV-infected HCEn cells directly stimulated the proliferation of CD8 T cells from CMV-seropositive donors, and pp65 viral epitope induced interferon-γ secretion from the CD8 T cells. We conclude that CMV-infected HCEn cells induce innate immune priming along with provisions of acquired immune priming of CD8 effector T cells. This information should help in the development of useful diagnostic procedures and efficacious therapeutic strategy to treat refractory corneal endotheliitis.

摘要

人巨细胞病毒(CMV)感染角膜内皮细胞是角膜内皮炎的重要病因。CMV内皮炎难以彻底治愈且复发频繁,可导致致盲性角膜大疱性病变。然而,CMV内皮炎的发病机制仍未明确。为了解内皮炎的免疫病理学,我们基于全局转录反应研究了CMV感染后角膜内皮细胞如何启动抗病毒免疫。为此,用CMV感染人角膜内皮(HCEn)细胞,并通过微阵列分析利用网络分析确定原发性抗病毒反应的全局转录反应。采用实时逆转录聚合酶链反应(RT-PCR)和蛋白质阵列分析来检测是否诱导了抗病毒细胞因子,即确定先天免疫反应是否被激活。为检测获得性免疫反应的启动是否被激活,将CMV感染的HCEn细胞与来自CMV血清阳性供体的同种异体CD8 T细胞共培养,并通过测量干扰素-γ分泌来检测对CD8效应T细胞的启动活性。HCEn细胞的CMV诱导反应以代表先天免疫启动的I型干扰素和模式识别受体途径为特征。全局转录激活与具有抗菌反应功能的抗原呈递特异性相关。蛋白质阵列分析表明,作为先天免疫反应,包括CXCL10在内的抗病毒炎性细胞因子的分泌显著增加。当检测HCEn细胞以确定CMV感染是否激活抗病毒获得性免疫时,CMV感染的HCEn细胞直接刺激来自CMV血清阳性供体的CD8 T细胞增殖,并且pp65病毒表位诱导CD8 T细胞分泌干扰素-γ。我们得出结论,CMV感染的HCEn细胞诱导先天免疫启动以及CD8效应T细胞获得性免疫启动。这些信息应有助于开发有用的诊断程序和有效的治疗策略来治疗难治性角膜内皮炎。

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