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大鼠自身抗IgE反应的诱导。IV. 对肥大细胞脱颗粒的影响。

Induction of an auto-anti-IgE response in rats. IV. Effects on mast cell degranulation.

作者信息

Jaffery G, Bell E B, Coleman J W

机构信息

Department of Cell and Structural Biology, University of Manchester Medical School, U.K.

出版信息

Immunology. 1993 Apr;78(4):635-42.

Abstract

Induction of an auto-anti-IgE (auto-aIgE) response in the rat inhibits both total and specific IgE production and alters the distribution of mast cell (MC) subpopulations identified by differential Alcian blue/safranin staining. We have extended these observations by characterizing the auto-aIgE antibodies and determining their effects on MC degranulation in vitro and in vivo. An auto-aIgE response was induced in bacillus Calmette-Guérin (BCG)-primed rats by injecting a conjugate of highly purified rat IgE myeloma (IR2) coupled to tuberculin-derived purified protein derivative (PPD). Anti-IgE autoantibodies were almost exclusively IgG2a. The intradermal injection of auto-aIgE into untreated rats induced local MC degranulation as shown by a strong immediate skin response. Histologically there was evidence of significant degranulation of safranin staining connective tissue MC (SMC) in the skin but not of the Alcian blue staining MC (ABMC) in the sub-epidermal region. The induced degranulation was epsilon-chain specific; immunopurified anti-idiotypic antibodies raised to the IgE IR2 myeloma had no MC degranulating activity. When administered locally, auto-aIgE inhibited a subsequent passive cutaneous anaphylaxis (PCA) response elicited by anti-ovalbumin IgE. In addition, the PCA response was significantly decreased in animals with an ongoing auto-aIgE response. Immunopurified auto-aIgE also induced histamine release in vitro from rat peritoneal MC. These results are discussed in the context of naturally occurring autoantibodies to IgE present in patients with allergic disease.

摘要

在大鼠中诱导自身抗IgE(自身aIgE)反应可抑制总IgE和特异性IgE的产生,并改变通过阿尔辛蓝/番红差异染色鉴定的肥大细胞(MC)亚群的分布。我们通过表征自身aIgE抗体并确定它们在体外和体内对MC脱颗粒的影响来扩展了这些观察结果。通过注射与结核菌素衍生的纯化蛋白衍生物(PPD)偶联的高度纯化的大鼠IgE骨髓瘤(IR2)共轭物,在卡介苗(BCG)致敏的大鼠中诱导自身aIgE反应。抗IgE自身抗体几乎完全是IgG2a。将自身aIgE皮内注射到未处理的大鼠中会诱导局部MC脱颗粒,如强烈的即时皮肤反应所示。组织学上,有证据表明皮肤中番红染色的结缔组织MC(SMC)有明显脱颗粒,但表皮下区域的阿尔辛蓝染色MC(ABMC)没有脱颗粒。诱导的脱颗粒是ε链特异性的;针对IgE IR2骨髓瘤产生的免疫纯化抗独特型抗体没有MC脱颗粒活性。当局部给药时,自身aIgE抑制了随后由抗卵清蛋白IgE引发的被动皮肤过敏反应(PCA)。此外,在具有持续自身aIgE反应的动物中,PCA反应显著降低。免疫纯化的自身aIgE在体外也能诱导大鼠腹膜MC释放组胺。本文在过敏性疾病患者中存在的针对IgE的天然自身抗体的背景下讨论了这些结果。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ad51/1421891/63c414b98c30/immunology00099-0128-a.jpg

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