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Monocytic myeloid-derived suppressor cells regulate T-cell responses against vaccinia virus

机译:单核细胞的myeloid-derived抑制细胞对牛痘病毒调节t细胞反应

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摘要

Vaccinia virus (VV) can potently activate NK- and T-cell responses, leading to efficient viral control and generation of long-lasting protective immunity. However, immune responses against viral infections are often tightly controlled to avoid collateral damage and systemic inflammation. We have previously shown that granulocytic myeloid-derived suppressor cells (g-MDSCs) can suppress the NK-cell response to VV infection. It remains unknown what regulates T-cell responses to VV infection in vivo. In this study, we first showed that monocytic MDSCs (m-MDSCs), but not g-MDSCs, from VV-infected mice could directly suppress CD4(+) and CD8(+) T-cell activation in vitro. We then demonstrated that defective recruitment of m-MDSCs to the site of VV infection in CCR2(-/-) mice enhanced VV-specific CD8(+) T-cell response and that adoptive transfer of m-MDSCs into VV-infected mice suppressed VV-specific CD8(+) T-cell activation, leading to a delay in viral clearance. Mechanistically, we further showed that T-cell suppression by m-MDSCs is mediated by indication of iNOS and production of NO upon VV infection, and that IFN-is required for activation of m-MDSCs. Collectively, our results highlight a critical role for m-MDSCs in regulating T-cell responses against VV infection and may suggest potential strategies using m-MDSCs to modulate T-cell responses during viral infections.
机译:牛痘病毒(VV)可以强有力地激活NK -t细胞反应,导致有效的病毒控制和一代的长效保护免疫力。通常是严格控制,以避免感染间接损害和系统性炎症。曾表明,粒细胞myeloid-derived (g-MDSCs)可以抑制细胞VV感染抑制nk细胞的反应。仍然不知道怎样调节t细胞反应VV体内感染。表明,单核细胞的MDSCs (m-MDSCs),但不是可以直接g-MDSCs,从VV-infected老鼠抑制CD4(+)和CD8 (+) t细胞活化体外。招聘网站m-MDSCs VV感染CCR2(- / -)小鼠增强VV-specificCD8 (+) t细胞反应,过继转移m-MDSCs成VV-infected老鼠的抑制VV-specific CD8 (+) t细胞活化,导致推迟病毒清除。通过m-MDSCs进一步表明t细胞抑制是由伊诺和生产的迹象没有在VV感染,IFN-is必需的m-MDSCs的激活。结果突出m-MDSCs的至关重要的作用调节对VV感染t细胞反应并可能潜在策略使用的建议在病毒m-MDSCs调节t细胞反应感染。

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