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速发型风团及潮红皮肤反应的晚期阶段。其对IgE抗体的依赖性。

The late phase of the immediate wheal and flare skin reaction. Its dependence upon IgE antibodies.

作者信息

Solley G O, Gleich G J, Jordon R E, Schroeter A L

出版信息

J Clin Invest. 1976 Aug;58(2):408-20. doi: 10.1172/JCI108485.

Abstract

IgE antibodies are usually thought to induce only immediate skin reactions. We have shown that the intradermal injection of a number of different allergens can produce a prolonged inflammatory reaction after the immediate wheal and flare in most sensitive subjects. This late inflammatory response occurs 6-12 h after challenge and is characterized by diffuse edema, erythema, pruritus, and heat. Both immediate and late responses can also be seen after passive sensitization of skin sites in nonatopic subjects. That IgE is involved in inducing the reaction was shown by the abolition of both immediate and late responses by passive transfer tests in the following experiments: (a) heating atopic serum at 56degreesC for 4 h, (b) removing IgE from the atopic serum by a solid phase anti-IgE immunoabsorbent, and (c) competitively inhibiting the binding of IgE antibodies to cells by an IgE myeloma protein. In addition, both responses were induced by affinity chromatography-purified IgE antibody, followed by antigenic challenge. Very similar lesions could also be induced by intradermal injection of Compound 48/80, thus suggesting a central role in the reaction for the mast cell or basophil. Histologically, the late phase is characterized by edema and a mixed cellular infiltration, predominantly lymphocytic but also containing eosinophils, neutrophils and basophils. Direct immunofluorescent staining did not show deposition of immunoglobulins or complement components, except IgM in 2 of 15 and C3 in 1 of 15 patients. This finding indicates that the late phase does not depend on the deposition of immune complexes. The results of the study suggest that IgE-allergen interaction on the surfaces of mast cells or on infiltrating basophils causes both immediate and late cutaneous responses.

摘要

IgE抗体通常被认为仅能引发即刻皮肤反应。我们已经表明,在大多数敏感个体中,皮内注射多种不同变应原后,在即刻风团和潮红之后可产生持续的炎症反应。这种迟发性炎症反应在激发后6 - 12小时出现,其特征为弥漫性水肿、红斑、瘙痒和发热。在非特应性个体的皮肤部位进行被动致敏后,也可观察到即刻和迟发反应。在以下实验中,通过被动转移试验消除即刻和迟发反应,表明IgE参与了反应的诱导:(a) 将特应性血清在56℃加热4小时;(b) 用固相抗IgE免疫吸附剂从特应性血清中去除IgE;(c) 用IgE骨髓瘤蛋白竞争性抑制IgE抗体与细胞的结合。此外,通过亲和层析纯化的IgE抗体进行抗原激发后,也可诱导出这两种反应。皮内注射化合物48/80也可诱导出非常相似的病变,因此提示肥大细胞或嗜碱性粒细胞在该反应中起核心作用。组织学上,迟发期的特征为水肿和混合性细胞浸润,主要为淋巴细胞,但也含有嗜酸性粒细胞、中性粒细胞和嗜碱性粒细胞。直接免疫荧光染色未显示免疫球蛋白或补体成分的沉积,15例患者中仅有2例显示IgM沉积,1例显示C3沉积。这一发现表明迟发期并不依赖于免疫复合物的沉积。该研究结果提示,肥大细胞表面或浸润的嗜碱性粒细胞上的IgE - 变应原相互作用可导致即刻和迟发性皮肤反应。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b573/333196/e8c997d52586/jcinvest00644-0159-a.jpg

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