爱泼斯坦-巴尔病毒裂解感染促进系统性硬化症单核细胞中Toll样受体8先天免疫反应的激活。
Epstein-Barr virus lytic infection promotes activation of Toll-like receptor 8 innate immune response in systemic sclerosis monocytes.
作者信息
Farina Antonella, Peruzzi Giovanna, Lacconi Valentina, Lenna Stefania, Quarta Silvia, Rosato Edoardo, Vestri Anna Rita, York Michael, Dreyfus David H, Faggioni Alberto, Morrone Stefania, Trojanowska Maria, Farina G Alessandra
机构信息
Rheumatology, Boston University School of Medicine, Arthritis Center, 72 E. Concord Street, E-5, Boston, MA, 02118, USA.
Department of Experimental Medicine, Sapienza University, Rome, Italy.
出版信息
Arthritis Res Ther. 2017 Feb 28;19(1):39. doi: 10.1186/s13075-017-1237-9.
BACKGROUND
Monocytes/macrophages are activated in several autoimmune diseases, including systemic sclerosis (scleroderma; SSc), with increased expression of interferon (IFN)-regulatory genes and inflammatory cytokines, suggesting dysregulation of the innate immune response in autoimmunity. In this study, we investigated whether the lytic form of Epstein-Barr virus (EBV) infection (infectious EBV) is present in scleroderma monocytes and contributes to their activation in SSc.
METHODS
Monocytes were isolated from peripheral blood mononuclear cells (PBMCs) depleted of the CD19+ cell fraction, using CD14/CD16 negative-depletion. Circulating monocytes from SSc and healthy donors (HDs) were infected with EBV. Gene expression of innate immune mediators were evaluated in EBV-infected monocytes from SSc and HDs. Involvement of Toll-like receptor (TLR)8 in viral-mediated TLR8 response was investigated by comparing the TLR8 expression induced by infectious EBV to the expression stimulated by CL075/TLR8/agonist-ligand in the presence of TLR8 inhibitor in THP-1 cells.
RESULTS
Infectious EBV strongly induced TLR8 expression in infected SSc and HD monocytes in vitro. Markers of activated monocytes, such as IFN-regulated genes and chemokines, were upregulated in SSc- and HD-EBV-infected monocytes. Inhibiting TLR8 expression reduced virally induced TLR8 in THP-1 infected cells, demonstrating that innate immune activation by infectious EBV is partially dependent on TLR8. Viral mRNA and proteins were detected in freshly isolated SSc monocytes. Microarray analysis substantiated the evidence of an increased IFN signature and altered level of TLR8 expression in SSc monocytes carrying infectious EBV compared to HD monocytes.
CONCLUSION
This study provides the first evidence of infectious EBV in monocytes from patients with SSc and links EBV to the activation of TLR8 and IFN innate immune response in freshly isolated SSc monocytes. This study provides the first evidence of EBV replication activating the TLR8 molecular pathway in primary monocytes. Immunogenicity of infectious EBV suggests a novel mechanism mediating monocyte inflammation in SSc, by which EBV triggers the innate immune response in infected cells.
背景
单核细胞/巨噬细胞在包括系统性硬化症(硬皮病;SSc)在内的多种自身免疫性疾病中被激活,干扰素(IFN)调节基因和炎性细胞因子的表达增加,提示自身免疫中固有免疫反应失调。在本研究中,我们调查了爱泼斯坦-巴尔病毒(EBV)感染的裂解形式(传染性EBV)是否存在于硬皮病单核细胞中,并导致其在SSc中被激活。
方法
使用CD14/CD16阴性去除法从去除CD19+细胞部分的外周血单核细胞(PBMC)中分离单核细胞。来自SSc患者和健康供体(HD)的循环单核细胞用EBV感染。评估来自SSc和HD的EBV感染单核细胞中固有免疫介质的基因表达。通过比较传染性EBV诱导的TLR8表达与在THP-1细胞中存在TLR8抑制剂时CL075/TLR8/激动剂-配体刺激的表达,研究Toll样受体(TLR)8在病毒介导的TLR8反应中的作用。
结果
传染性EBV在体外强烈诱导感染的SSc和HD单核细胞中TLR8表达。活化单核细胞的标志物,如IFN调节基因和趋化因子,在SSc和HD-EBV感染的单核细胞中上调。抑制TLR8表达可降低THP-1感染细胞中病毒诱导的TLR8,表明传染性EBV引起的固有免疫激活部分依赖于TLR8。在新鲜分离的SSc单核细胞中检测到病毒mRNA和蛋白。微阵列分析证实了与HD单核细胞相比,携带传染性EBV的SSc单核细胞中IFN特征增加和TLR8表达水平改变的证据。
结论
本研究提供了SSc患者单核细胞中存在传染性EBV的首个证据,并将EBV与新鲜分离的SSc单核细胞中TLR8和IFN固有免疫反应的激活联系起来。本研究提供了EBV复制激活原代单核细胞中TLR8分子途径的首个证据。传染性EBV的免疫原性提示了一种介导SSc单核细胞炎症的新机制,即EBV触发感染细胞中的固有免疫反应。
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