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CD83 expression regulates antibody production in response to influenza A virus infection

机译:CD83表达调节抗体产生响应流感病毒感染

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摘要

CD83 is known to regulate lymphocyte maturation, activation, homeostasis, and antibody response to immunization and infection. While CD83 has a major part in B cell function, its role in influenza A virus infection has not yet been investigated. We investigated the role of CD83 using C57BL/6J wild type mice and CD83 knockout (KO) mice after intraperitoneal administration of the influenza A/WSN/1933 virus. We analyzed cells of the peritoneal cavity, splenocytes, and cells of the bone marrow with FACS to investigate CD83 expression and cell population change in response to the virus infection. ELISA was performed with sera and peritoneal cavity fluids to detect A/WSN/1933 virus-specific IgG and the subclasses of IgG. FACS analysis data showed a transient but distinct induction of CD83 expression in the peritoneal B cells of wild type mice. CD83 KO mice exhibited a delayed recovery of B cells in the bone marrow after influenza virus infection and overall, a smaller T cell population compared to wild type mice. The peritoneal cavity and serum of the wild type mice contained a high titer of IgG within 14?days after infection, whereas the CD83 KO mice had a very low titer of IgG. These results show the importance of CD83 in lymphocytes homeostasis and antibody production during influenza A virus infection.
机译:已知CD83调节淋巴细胞成熟,激活,稳态和抗体反应对免疫和感染。虽然CD83具有B细胞功能的主要部分,但尚未调查其在流感病毒感染中的作用。我们在腹腔施用流感A / WSN / 1933病毒后使用C57BL / 6J野生型小鼠和CD83敲除(KO)小鼠的CD83的作用。我们分析了骨髓腔,脾细胞和骨髓细胞的细胞与FACS进行研究,以研究CD83表达和细胞群的变化,以应对病毒感染。用血清和腹膜腔液进行ELISA检测A / WSN / 1933病毒特异性IgG和IgG的亚类。 FACS分析数据显示野生型小鼠腹膜B细胞中CD83表达的瞬态但明显诱导。 CD83 KO小鼠在流感病毒感染后骨髓中的B细胞延迟回收,与野生型小鼠相比,较小的T细胞群。野生型小鼠的腹膜腔和血清含有高滴度的IgG,在感染后14天内,而CD83 KO小鼠具有非常低的IgG滴度。这些结果表明CD83在流感病毒感染过程中CD83在淋巴细胞稳态和抗体产生的重要性。

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