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白细胞介素12改变小鼠对鸡卵清溶菌酶的同型限制抗体反应。

Interleukin 12 alters the isotype-restricted antibody response of mice to hen eggwhite lysozyme.

作者信息

Buchanan J M, Vogel L A, Van Cleave V H, Metzger D W

机构信息

Department of Microbiology, Medical College of Ohio, Toledo 43699, USA.

出版信息

Int Immunol. 1995 Sep;7(9):1519-28. doi: 10.1093/intimm/7.9.1519.

Abstract

Protein antigens elicit humoral responses in mice that consist predominantly of IgG1 antibodies. We have now investigated the ability of IL-12, a cytokine reported to augment IgG2a anti-hapten responses through activation of Th1 cells, to alter antibody responses to hen eggwhite lysozyme (HEL). The normal response of BALB/c mice to HEL is highly restricted to IgG1 expression and therefore provides an excellent system for determining effects of cytokines on expression of other isotypes. Seven days after immunization, IL-12 treated mice demonstrated greatly elevated HEL-specific IgG2a antibody levels and suppressed IgG1 production, while PBS-treated control mice showed a typical IgG1-restricted response. On day 28, IL-12-treated mice showed heightened serum antibody levels of both isotypes. Delaying cytokine treatment until after the typical IgG1 anti-HEL response had already been established also led to significant elevation of serum IgG2a antibody levels. These effects correlated with increased IFN-gamma production; however, administration of IL-12 plus anti-IFN-gamma had little influence on IgG2a enhancement, although it did relieve the early IgG1 suppression. Furthermore, the differential effects of Il-12 on isotype expression did not correlate with time; in fact, IgG2a enhancement correlated with loss of IgG1 suppression. Our findings indicate that (i) IL-12 reproducibly induces large amounts of IgG2a HEL-specific antibodies in vivo; (ii) it can alter isotype profiles of both primary and secondary responses; and (iii) its effects on humoral immunity are not completely explained by induction of Th1 cell derived IFN-gamma.

摘要

蛋白质抗原在小鼠体内引发体液免疫反应,主要产生IgG1抗体。我们现在研究了白细胞介素-12(IL-12)改变对鸡卵清溶菌酶(HEL)抗体反应的能力,IL-12是一种据报道可通过激活Th1细胞增强IgG2a抗半抗原反应的细胞因子。BALB/c小鼠对HEL的正常反应高度局限于IgG1表达,因此为确定细胞因子对其他同种型表达的影响提供了一个极佳的系统。免疫七天后,接受IL-12治疗的小鼠表现出HEL特异性IgG2a抗体水平大幅升高,IgG1产生受到抑制,而接受PBS治疗的对照小鼠表现出典型的IgG1局限反应。在第28天,接受IL-12治疗的小鼠两种同种型的血清抗体水平均升高。将细胞因子治疗推迟到典型的IgG1抗HEL反应已经建立之后,也导致血清IgG2a抗体水平显著升高。这些效应与干扰素-γ(IFN-γ)产生增加相关;然而,给予IL-12加抗IFN-γ对IgG2a增强影响不大,尽管它确实缓解了早期的IgG1抑制。此外,IL-12对同种型表达的不同影响与时间无关;事实上,IgG2a增强与IgG1抑制的丧失相关。我们的研究结果表明:(i)IL-12在体内可重复性地诱导大量IgG2a HEL特异性抗体;(ii)它可改变初次和二次反应的同种型谱;(iii)其对体液免疫的影响不能完全通过诱导Th1细胞衍生的IFN-γ来解释。

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