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单克隆抗白细胞介素-4受体抗体对小鼠体内IgG和IgE反应的调节。

Regulation of murine in vivo IgG and IgE responses by a monoclonal anti-IL-4 receptor antibody.

作者信息

Finkelman F D, Urban J F, Beckmann M P, Schooley K A, Holmes J M, Katona I M

机构信息

Department of Medicine, Uniformed Services University of the Health Sciences, Bethesda, MD 20814-4799.

出版信息

Int Immunol. 1991 Jun;3(6):599-607. doi: 10.1093/intimm/3.6.599.

DOI:10.1093/intimm/3.6.599
PMID:1888709
Abstract

Although the cytokine interleukin 4 (IL-4) stimulates LPS-activated mouse B lymphocytes to secrete both IgG1 and IgE, an anti-IL-4 antibody completely inhibits IgE responses but has little or no effect on several in vivo IgG responses. IL-4 might, therefore, have a restricted role in the generation of in vivo humoral immune responses. Alternatively, IgG1 responses might be stimulated by IL-4 secreted by T cells that are interacting directly with B cells, so that anti-IL-4 antibody cannot neutralize IL-4 before it binds to a B cell IL-4 receptor. In contrast, an antibody that blocks the IL-4 receptor (IL-4R) should equally inhibit responses to IL-4 produced proximal to or distant from a B cell. This reasoning led us to determine the ability of an anti-IL-4R mAb to affect antibody production in mice injected with a goat antibody to mouse IgD (GaM delta) or inoculated with the nematode parasite Heligmosomoides polygyrus. Anti-IL-4R mAb, like anti-IL-4 mAb, blocked IgE responses by greater than 95% and enhanced IgG2a responses to a variable extent. Anti-IL-4R mAb, however, had only a modest and variable inhibitory effect on the induction of IgG1 responses, although it caused these responses to terminate more rapidly. A combination of anti-IL-4 and anti-IL-4R mAbs totally blocked goat anti-mouse IgD antibody (GaM delta)-induced IgE production but had no additive inhibitory effect on IgG1 production. These observations are most consistent with the view that IL-4 is required for a primary IgE response, but has relatively little role in the induction of IgG1 responses in the in vivo systems studied.

摘要

尽管细胞因子白细胞介素4(IL-4)可刺激脂多糖激活的小鼠B淋巴细胞分泌IgG1和IgE,但抗IL-4抗体可完全抑制IgE反应,而对多种体内IgG反应几乎没有影响。因此,IL-4在体内体液免疫反应的产生中可能作用有限。或者,IgG1反应可能由与B细胞直接相互作用的T细胞分泌的IL-4刺激,这样抗IL-4抗体在IL-4与B细胞IL-4受体结合之前无法中和IL-4。相比之下,阻断IL-4受体(IL-4R)的抗体应同样抑制对B细胞近端或远端产生的IL-4的反应。这一推理促使我们确定抗IL-4R单克隆抗体对注射山羊抗小鼠IgD抗体(GaMδ)或接种线虫寄生虫多房棘球绦虫的小鼠抗体产生的影响。抗IL-4R单克隆抗体与抗IL-4单克隆抗体一样,可阻断超过95%的IgE反应,并在不同程度上增强IgG2a反应。然而,抗IL-4R单克隆抗体对IgG1反应的诱导仅具有适度且可变的抑制作用,尽管它会使这些反应更快终止。抗IL-4和抗IL-4R单克隆抗体的组合完全阻断了山羊抗小鼠IgD抗体(GaMδ)诱导的IgE产生,但对IgG1产生没有额外的抑制作用。这些观察结果与以下观点最为一致:IL-4是原发性IgE反应所必需的,但在本研究的体内系统中对IgG1反应的诱导作用相对较小。

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Regulation of murine in vivo IgG and IgE responses by a monoclonal anti-IL-4 receptor antibody.单克隆抗白细胞介素-4受体抗体对小鼠体内IgG和IgE反应的调节。
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