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人轮状病毒特异性 IgM 记忆 B 细胞具有不同的克隆效率和转换能力,并在体内抗病毒免疫中发挥作用。

Human rotavirus-specific IgM Memory B cells have differential cloning efficiencies and switch capacities and play a role in antiviral immunity in vivo.

机构信息

Instituto de Genética Humana, Facultad de Medicina, Pontificia Universidad Javeriana, Bogotá, Colombia.

出版信息

J Virol. 2012 Oct;86(19):10829-40. doi: 10.1128/JVI.01466-12. Epub 2012 Aug 1.

DOI:10.1128/JVI.01466-12
PMID:22855480
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3457288/
Abstract

Protective immunity to rotavirus (RV) is primarily mediated by antibodies produced by RV-specific memory B cells (RV-mBc). Of note, most of these cells express IgM, but the function of this subset is poorly understood. Here, using limiting dilution assays of highly sort-purified human IgM(+) mBc, we found that 62% and 21% of total (non-antigen-specific) IgM(+) and RV-IgM(+) mBc, respectively, switched in vitro to IgG production after polyclonal stimulation. Moreover, in these assays, the median cloning efficiencies of total IgM(+) (17%) and RV-IgM(+) (7%) mBc were lower than those of the corresponding switched (IgG(+) IgA(+)) total (34%) and RV-mBc (17%), leading to an underestimate of their actual frequency. In order to evaluate the in vivo role of IgM(+) RV-mBc in antiviral immunity, NOD/Shi-scid interleukin-2 receptor-deficient (IL-2Rγ(null)) immunodeficient mice were adoptively transferred highly purified human IgM(+) mBc and infected with virulent murine rotavirus. These mice developed high titers of serum human RV-IgM and IgG and had significantly lower levels than control mice of both antigenemia and viremia. Finally, we determined that human RV-IgM(+) mBc are phenotypically diverse and significantly enriched in the IgM(hi) IgD(low) subset. Thus, RV-IgM(+) mBc are heterogeneous, occur more frequently than estimated by traditional limiting dilution analysis, have the capacity to switch Ig class in vitro as well as in vivo, and can mediate systemic antiviral immunity.

摘要

轮状病毒(RV)的保护性免疫主要由 RV 特异性记忆 B 细胞(RV-mBc)产生的抗体介导。值得注意的是,这些细胞大多数表达 IgM,但该亚群的功能尚未完全了解。在这里,我们使用高度分选纯化的人 IgM(+) mBc 的有限稀释分析发现,62%和 21%的总(非抗原特异性)IgM(+)和 RV-IgM(+) mBc 分别在体外经多克隆刺激后转换为 IgG 产生。此外,在这些测定中,总 IgM(+)(17%)和 RV-IgM(+)(7%)mBc 的中位克隆效率低于相应的已转换(IgG(+) IgA(+))总(34%)和 RV-mBc(17%),导致对其实际频率的低估。为了评估 IgM(+) RV-mBc 在抗病毒免疫中的体内作用,我们将高度纯化的人 IgM(+) mBc 过继转移到 NOD/Shi-scid 白细胞介素 2 受体缺陷(IL-2Rγ(null))免疫缺陷小鼠中,并感染了强毒鼠轮状病毒。这些小鼠产生了高滴度的血清人 RV-IgM 和 IgG,并且抗原血症和病毒血症水平明显低于对照小鼠。最后,我们确定人 RV-IgM(+) mBc 表型多样化,并且在 IgM(hi) IgD(low)亚群中显著富集。因此,RV-IgM(+) mBc 是异质性的,比传统的有限稀释分析估计的更为常见,具有体外和体内转换 Ig 类别的能力,并能介导系统抗病毒免疫。

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