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Pathogenic Role for Virus-Specific CD4 T Cells in Mice with Coronavirus-Induced Acute Encephalitis

机译:病毒特异性CD4 T细胞在冠状病毒诱发的急性脑炎小鼠中的致病作用

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摘要

Acute viral encephalitis is believed to result from direct virus destruction of infected cells and from virus-induced host immune response, but the relative contribution of each remains largely unknown. For example, C57BL/6 (B6) mice infected with mouse hepatitis virus (JHM strain, JHMV) develop severe encephalitis, with death occurring within 7 days. Here, we show that the host response to a single JHMV-specific immunodominant CD4 T-cell epitope is critical for severe disease. We engineered a recombinant JHMV with mutations in the immunodominant CD4 T-cell epitope (rJ.MY135Q). Infection of naïve B6 mice with this virus resulted in mild disease with no mortality. However, introduction of a CD4 T-cell epitope from Listeria monocytogenes into rJ.MY135Q generated a highly virulent virus. The decrease in disease severity was not due to a switch from Th1 to Th2 predominance in rJ.MY135Q-infected mice, an effect on CD8 T-cell function, or differential expression of tumor necrosis factor-α by JHMV-specific CD4 T cells. These results show that the response to a single virus-specific CD4 T-cell epitope may contribute to a pathogenic host response in the setting of acute viral disease and that abrogation of this response ameliorates clinical disease without diminishing virus clearance.
机译:急性病毒性脑炎被认为是由感染细胞的直接病毒破坏和病毒诱导的宿主免疫反应引起的,但是每种病毒的相对贡献仍然未知。例如,感染了小鼠肝炎病毒(JHM株,JHMV)的C57BL / 6(B6)小鼠会发展为严重的脑炎,并在7天内死亡。在这里,我们显示宿主对单个JHMV特异性免疫优势CD4 T细胞表位的反应对于严重疾病至关重要。我们设计了一种重组JHMV,在免疫优势CD4 T细胞表位(rJ.MY135Q)中具有突变。幼稚的B6小鼠感染这种病毒可导致轻度疾病,且无死亡。但是,将单核细胞增生性李斯特菌CD4 T细胞表位引入rJ.MY135Q会产生高毒力病毒。疾病严重程度的降低不是由于在感染rJ.MY135Q的小鼠中Th1占主导地位向Th2转变,对CD8 T细胞功能的影响或JHMV特异性CD4 T细胞对肿瘤坏死因子-α的差异表达。这些结果表明,在急性病毒性疾病中,对单个病毒特异性CD4 T细胞表位的应答可能有助于病原体宿主应答,并且该应答的消除在不降低病毒清除率的情况下改善了临床疾病。

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