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抗原特异性与总免疫球蛋白合成:总IgE和IgG1水平而非IgG2a水平可预测小鼠的抗原特异性反应。

Antigen-specific versus total immunoglobulin synthesis: total IgE and IgG1, but not IgG2a levels predict murine antigen-specific responses.

作者信息

Lewkowich Ian P, Rempel Julia D, HayGlass Kent T

机构信息

Department of Immunology, CIHR National Training Program in Allergy and Asthma Research, Winnipeg, Canada.

出版信息

Int Arch Allergy Immunol. 2004 Feb;133(2):145-53. doi: 10.1159/000076440. Epub 2004 Jan 26.

Abstract

BACKGROUND

Induction of an effective antibody (Ab) response requires delivery of multiple signals to B cells. Cross-linking of the B cell antigen receptor (BCR), signaling through CD40 and CD80/86 and cytokine signals combine to induce class switching and expression of specific isotypes. These signals are principally derived from activated, antigen (Ag)-specific T cells. In contrast, IFNgamma, the only cytokine known to induce class switch to IgG2a, can be produced systemically by activated NK or NKT cells, suggesting that Ag-nonspecific signals may also regulate IgG2a production.

METHODS

Given the potential differences in regulation between IgE/IgG1 versus IgG2a, we immunized mice on day 0 with ovalbumin (OVA) in the presence of strong type-1- or type-2-immunity-inducing adjuvants and boosted mice 4 weeks later. Mice were bled during the primary immune response and after boost to assess primary and recall Ab responses.

RESULTS

Regardless of strain of mice used, phenotype (type 1 versus type 2 dominated) or nature of the immune response induced (primary versus recall), strong correlations between OVA-specific and total IgE and IgG1 were demonstrated. In contrast, a consistent lack of correlation between OVA-specific and total IgG2a levels was observed in all but BALB/c mice.

CONCLUSION

These data indicate that the increase in total levels of IgE/IgG1 isotypes is primarily a result of increased levels of OVA-specific Ab. In contrast, the lack of correlation between total and OVA-specific IgG2a suggests broader activation of IgG2a-producing B cells routinely occurs following exogenous Ag immunization.

摘要

背景

诱导有效的抗体(Ab)反应需要向B细胞传递多种信号。B细胞抗原受体(BCR)的交联、通过CD40和CD80/86的信号传导以及细胞因子信号共同作用,诱导类别转换和特定同种型的表达。这些信号主要来自活化的、抗原(Ag)特异性T细胞。相比之下,已知唯一能诱导向IgG2a类别转换的细胞因子IFNγ可由活化的NK或NKT细胞全身性产生,这表明Ag非特异性信号也可能调节IgG2a的产生。

方法

鉴于IgE/IgG1与IgG2a在调节方面可能存在差异,我们在第0天用卵清蛋白(OVA)在强1型或2型免疫诱导佐剂存在的情况下免疫小鼠,并在4周后对小鼠进行加强免疫。在初次免疫反应期间和加强免疫后采集小鼠血液,以评估初次和回忆性Ab反应。

结果

无论使用的小鼠品系、表型(1型与2型主导)或诱导的免疫反应性质(初次与回忆)如何,OVA特异性IgE和IgG1与总IgE和IgG1之间均显示出强相关性。相比之下,除BALB/c小鼠外,在所有小鼠中均观察到OVA特异性IgG2a水平与总IgG2a水平之间始终缺乏相关性。

结论

这些数据表明,IgE/IgG1同种型总水平的增加主要是OVA特异性Ab水平增加的结果。相比之下,总IgG2a与OVA特异性IgG2a之间缺乏相关性表明,在外源性Ag免疫后,产生IgG2a的B细胞通常会发生更广泛的活化。

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