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Article T-bet+ Memory B Cells Link to Local Cross-Reactive IgG upon Human Rhinovirus Infection

机译:第T-Bet + Memory B细胞链接到人鼻病毒感染后局部交叉反应性IgG

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Human rhinoviruses cause the common cold and exacerbate chronic respiratory diseases. Although infection elicits neutralizing antibodies, these do not persist or cross-protect across multiple rhinovirus strains. To analyze rhinovirus-specific B cell responses in humans, we developed techniques using intact RV-A16 and RV-A39 for high-throughput high-dimensional single-cell analysis, with parallel assessment of antibody isotypes in an experimental infection model. Our approach identified T-bet+ B cells binding both viruses that account for ~5% of CXCR5? memory B cells. These B cells infiltrate nasal tissue and expand in the blood after infection. Their rapid secretion of heterotypic immunoglobulin G (IgG) in?vitro , but not IgA, matches the nasal antibody profile post-infection. By contrast, CXCR5+ memory B cells binding a single virus are clonally distinct, absent in nasal tissue, and secrete homotypic IgG and IgA, mirroring the systemic response. Temporal and spatial functions of dichotomous memory B cells might explain the ability to resolve infection while rendering the host susceptible to re-infection.
机译:人鼻病毒导致常见的感冒和加剧慢性呼吸系统疾病。虽然感染引发中和抗体,但这些不会持续或穿过多个鼻病毒菌株的交叉保护。为了分析人类中的鼻病毒特异性B细胞应答,我们使用完整的RV-A16和RV-A39开发了用于高通量高维单细胞分析的技术,并在实验性感染模型中并行评估抗体同种型。我们的方法鉴定了T-Bet + B细胞结合占CXCR5的〜5%的病毒?记忆B细胞。这些B细胞渗透鼻组织并在感染后在血液中膨胀。它们在β体外但不是IgA的异型免疫球蛋白G(IgG)的快速分泌与感染后的鼻抗体谱。相比之下,结合单个病毒的CXCR5 +内存B细胞是克隆性不同的,在鼻组组织中不存在,并且分泌均质IgG和IgA,镜像系统响应。二分记忆B细胞的时间和空间功能可以解释解决感染的能力,同时使宿主容易受到重新感染。

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