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小鼠中干扰素α对免疫球蛋白同种型选择和淋巴因子产生的调节作用。

Regulation by interferon alpha of immunoglobulin isotype selection and lymphokine production in mice.

作者信息

Finkelman F D, Svetic A, Gresser I, Snapper C, Holmes J, Trotta P P, Katona I M, Gause W C

机构信息

Department of Medicine, Uniformed Services University of the Health Sciences, Bethesda, Maryland 20814.

出版信息

J Exp Med. 1991 Nov 1;174(5):1179-88. doi: 10.1084/jem.174.5.1179.

Abstract

Antigens and infectious agents that stimulate interferon alpha(IFN-alpha) production in mice induce antibody responses that are predominantly of the immunoglobulin (Ig)G2a isotype and contain little or no IgE. This suggested the possibility that IFN-alpha might have a role in directing Ig isotype selection. Consistent with this possibility, we have found that injection of mice with recombinant mouse IFN-alpha suppresses IgE secretion, enhances IgG2a secretion, and has no independent effect on IgG1 secretion in mice stimulated with a foreign anti-IgD antibody. Injection of mice with polyinosinic acid.polycytidylic acid (poly I.C), an inducer of macrophage IFN-alpha production, also suppresses the anti-IgD antibody-induced IgE response and stimulates the IgG2a response; these effects are blocked by a sheep antibody that neutralizes mouse IFN-alpha/beta. Both recombinant IFN-alpha and poly I.C have maximum IgE suppressive and IgG2a stimulatory effects when injected early in the anti-IgD antibody-induced immune response. Addition of IFN-alpha to mouse B cells cultured with lipopolysaccharide (LPS) + interleukin 4 (IL-4) suppresses both IgG1 and IgE production, but much less potently than IFN-gamma. IFN-alpha suppresses anti-IgD antibody-induced increases in the level of splenic IL-4 mRNA, but enhances the anti-IgD antibody-induced increase in the splenic level of IFN-gamma mRNA. These results are consistent with the effect of IFN-alpha on Ig isotype expression in mice, as IL-4 stimulates IgE and suppresses IgG2a secretion while IFN-gamma exerts opposite effects. These observations suggest that antigen presenting cells, by secreting IFN-alpha early in the course of an immune response, can influence the nature of that response both through direct effects on B cells and by influencing the differentiation of T cells.

摘要

在小鼠中,能刺激α干扰素(IFN-α)产生的抗原和感染因子会诱导抗体反应,这些反应主要为免疫球蛋白(Ig)G2a同种型,几乎不含或完全不含IgE。这提示了IFN-α可能在指导Ig同种型选择中发挥作用。与这种可能性相符的是,我们发现给小鼠注射重组小鼠IFN-α可抑制IgE分泌,增强IgG2a分泌,并且对用外源性抗IgD抗体刺激的小鼠的IgG1分泌没有独立影响。给小鼠注射聚肌苷酸·聚胞苷酸(poly I.C),一种巨噬细胞IFN-α产生的诱导剂,也能抑制抗IgD抗体诱导的IgE反应并刺激IgG2a反应;这些效应被一种能中和小鼠IFN-α/β的羊抗体所阻断。重组IFN-α和poly I.C在抗IgD抗体诱导的免疫反应早期注射时,对IgE的抑制和对IgG2a的刺激作用最强。将IFN-α添加到用脂多糖(LPS)+白细胞介素4(IL-4)培养的小鼠B细胞中,可同时抑制IgG1和IgE的产生,但效力远低于IFN-γ。IFN-α抑制抗IgD抗体诱导的脾脏IL-4 mRNA水平升高,但增强抗IgD抗体诱导的脾脏IFN-γ mRNA水平升高。这些结果与IFN-α对小鼠Ig同种型表达的影响一致,因为IL-4刺激IgE并抑制IgG2a分泌,而IFN-γ则发挥相反的作用。这些观察结果表明,抗原呈递细胞在免疫反应过程早期通过分泌IFN-α,既能通过对B细胞的直接作用,也能通过影响T细胞的分化来影响该反应的性质。

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