Arthritis and Clinical Immunology, Oklahoma Medical Research Foundation, Oklahoma City, OK, United States.
Departments of Medicine and Pathology, University of Oklahoma Health Science Center, Oklahoma City, OK, United States.
Front Immunol. 2018 Oct 9;9:2198. doi: 10.3389/fimmu.2018.02198. eCollection 2018.
Epstein Barr virus (EBV) is a gamma herpes virus associated with certain malignancies and autoimmune diseases. EBV maintains latency in B cells with occasional reactivation, in part by overcoming the host immune response with viral homologs of several human proteins. EBV interleukin 10 (vIL-10), a lytic phase protein, is a homolog of human IL-10 (hIL-10). The effect of vIL-10 on human monocytes, which are one of the first immune cells to respond to infection, is not known. To understand the role of vIL-10, monocytes from peripheral blood mononuclear cells were stimulated with hIL-10 or vIL-10. Human IL-10 stimulated STAT3 phosphorylation, which is required for suppression of inflammatory responses. However, vIL-10 induced significantly lower phosphorylation of STAT3 compared to hIL-10, and was less efficient in downregulating inflammatory genes. vIL-10 significantly reduced the expression of scavenger receptor CD163 on monocytes, suggesting inhibition of M2 polarization. Furthermore, uptake of apoptotic cells was reduced in vIL-10-stimulated monocytes compared to hIL-10-stimulated monocytes. A neutralizing antibody to IL-10R1 inhibited STAT3 phosphorylation induced by either hIL-10 or vIL-10, suggesting that vIL-10 signals through IL-10R1. Interestingly, vIL-10 suppressed hIL-10-induced STAT3 phosphorylation and inhibited upregulation of suppressors of inflammatory response by hIL-10. We further show that vIL-10 levels were significantly higher in plasma samples from systemic lupus erythematosus (SLE) patients compared to matched unaffected controls. vIL-10 levels did not correlate with hIL-10 levels, but were associated with levels of IgA antibodies to EBV viral capsid antigen, which is an indirect measure of viral reactivation. We propose that the suppression of hIL-10- induced anti-inflammatory genes by vIL-10, together with an increase in inflammatory gene expression, may overcome the anti-inflammatory effects of hIL-10 and exacerbate autoimmune responses in systemic autoimmune diseases.
EB 病毒(EBV)是一种与某些恶性肿瘤和自身免疫性疾病相关的γ疱疹病毒。EBV 通过病毒与人蛋白的几种同源物克服宿主免疫反应,从而在 B 细胞中维持潜伏状态,偶尔会重新激活。EBV 白细胞介素 10(vIL-10)是一种裂解相蛋白,是人类白细胞介素 10(hIL-10)的同源物。vIL-10 对人单核细胞的影响尚不清楚,单核细胞是对感染最早做出反应的免疫细胞之一。为了了解 vIL-10 的作用,从外周血单核细胞中刺激单核细胞用 hIL-10 或 vIL-10。人 IL-10 刺激 STAT3 磷酸化,这是抑制炎症反应所必需的。然而,与 hIL-10 相比,vIL-10 诱导的 STAT3 磷酸化显著降低,并且下调炎症基因的效率较低。vIL-10 显著降低单核细胞上清道夫受体 CD163 的表达,表明抑制 M2 极化。此外,与 hIL-10 刺激的单核细胞相比,凋亡细胞的摄取在 vIL-10 刺激的单核细胞中减少。抗 IL-10R1 中和抗体抑制 hIL-10 或 vIL-10 诱导的 STAT3 磷酸化,表明 vIL-10 通过 IL-10R1 信号传导。有趣的是,vIL-10 抑制 hIL-10 诱导的 STAT3 磷酸化,并抑制 hIL-10 上调炎症反应抑制剂。我们进一步表明,与匹配的未受影响的对照组相比,系统性红斑狼疮(SLE)患者的血浆样本中的 vIL-10 水平明显更高。vIL-10 水平与 hIL-10 水平不相关,但与 EBV 衣壳抗原的 IgA 抗体水平相关,这是病毒重新激活的间接衡量标准。我们提出,vIL-10 抑制 hIL-10 诱导的抗炎基因,以及炎症基因表达的增加,可能会克服 hIL-10 的抗炎作用,并在系统性自身免疫性疾病中加重自身免疫反应。
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