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职业性化学接触物和呼吸道变应原在小鼠中引起即刻和迟发性皮肤超敏反应的差异能力。

Differential ability of occupational chemical contact and respiratory allergens to cause immediate and delayed dermal hypersensitivity reactions in mice.

作者信息

Dearman R J, Mitchell J A, Basketter D A, Kimber I

机构信息

ICI Central Toxicology Laboratory, Alderley Park, Macclesfield, Cheshire, UK.

出版信息

Int Arch Allergy Immunol. 1992;97(4):315-21. doi: 10.1159/000236139.

Abstract

Trimellitic anhydride (TMA) is known to cause occupational respiratory allergy associated with the presence of specific IgE antibody. Other chemicals, such as 2,4-dinitrochlorobenzene (DNCB), while exhibiting a clear potential for contact sensitization, apparently lack the ability to induce respiratory allergy in man. It has been shown previously that although both chemicals are immunogenic in mice, each provoking contact sensitization, exposure only to TMA results in an IgE antibody response. In the present study, to examine further the characteristics of human allergens, we have compared the ability of TMA and DNCB to elicit immediate and delayed cutaneous hypersensitivity reactions in mice. Topical exposure to both chemicals resulted in delayed (24 h) hypersensitivity. However, only TMA induced, in addition, an immediate (1 h) dermal reaction following local challenge. Serum from TMA-immune mice, but not from untreated mice or mice sensitized with DNCB, was able to transfer immediate hypersensitivity to naive recipients. The kinetics of passive sensitization with TMA-immune serum, together with the fact that immediate hypersensitivity to DNCB could be induced with monoclonal IgE anti-dinitrophenol (DNP) antibody, suggests that the immediate dermal responses caused by TMA are effected by hapten-specific IgE. These data demonstrate that different classes of occupational chemical allergen exhibit a variable potential to elicit immediate and delayed dermal hypersensitivity reactions in mice, and provide a novel approach to the classification and characterization of human allergens.

摘要

偏苯三酸酐(TMA)已知会引发与特异性IgE抗体存在相关的职业性呼吸道过敏。其他化学物质,如2,4 - 二硝基氯苯(DNCB),虽然具有明显的接触致敏潜力,但显然缺乏在人体中诱发呼吸道过敏的能力。先前已经表明,尽管这两种化学物质在小鼠中都具有免疫原性,均可引发接触致敏,但仅接触TMA会导致IgE抗体反应。在本研究中,为了进一步研究人类过敏原的特性,我们比较了TMA和DNCB在小鼠中引发即刻和延迟皮肤超敏反应的能力。局部接触这两种化学物质均导致延迟(24小时)超敏反应。然而,只有TMA在局部激发后还会诱发即刻(1小时)皮肤反应。来自TMA免疫小鼠的血清能够将即刻超敏反应传递给未致敏的受体,而未处理小鼠或用DNCB致敏的小鼠的血清则不能。用TMA免疫血清进行被动致敏的动力学,以及用单克隆IgE抗二硝基苯酚(DNP)抗体可诱导对DNCB的即刻超敏反应这一事实,表明TMA引起的即刻皮肤反应是由半抗原特异性IgE介导的。这些数据表明,不同类别的职业性化学过敏原在小鼠中引发即刻和延迟皮肤超敏反应的潜力各不相同,并为人类过敏原的分类和表征提供了一种新方法。

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