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[缓解期哮喘儿童的免疫学方面]

[Immunological aspects of asthmatic children in remission].

作者信息

Noma T, Yoshizawa I, Kou K, Nakamura Y, Kawano Y, Nakajima T, Itoh M, Maeda K, Ichikawa K, Yamaguchi K

机构信息

Department of Pediatrics, Saitama Medical School.

出版信息

Arerugi. 1993 Mar;42(3 Pt 1):186-91.

PMID:7684586
Abstract

Allergen-activated T cells secrete several kinds of bioactive lymphokines such as IL2, IL3, IL4, IL5 and IFN-gamma. They function as helpers in IgE production involved in immediate type hypersensitivity and/or effector cells in delayed type hypersensitivity in allergic patients. The acquisition of interleukin 2 (IL2) responsiveness by specific antigen-stimulated cells is generally an essential event for the induction of specific immunological phenomena. To investigate the immunological changes in asthmatic children in remission, the induction of IL2-responsiveness and production by Df (Dermatophagoides farinae)-stimulated patient lymphocytes, and Df-induced IFN-gamma production by patient lymphocytes were evaluated. The patients were divided into 3 groups. The remission group (I) consisted of those patients who had had no or only a few asthmatic attacks for more than 2 years without medication. The group of active asthma were divided into 2 groups according to attack frequency and severity (II, partial remission; III, active asthma). IL2 responsiveness and production by Df-stimulated lymphocytes from group II and III were increased. As symptoms improved, the extent of the response subsided to a level comparable to that of normal individuals (group III). IFN-gamma production by Df-stimulated lymphocytes from patients with active asthma was lower than that of normal lymphocytes. In contrast, lymphocytes from patients in complete remission group (I) induced far greater IFN-gamma generation than those from normal and group II and III patients in a Df antigen-dependent manner, which might downregulate Df-induced hyperreactivity for Df-mediated allergic response.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

变应原激活的T细胞分泌多种生物活性淋巴因子,如白细胞介素2(IL2)、白细胞介素3(IL3)、白细胞介素4(IL4)、白细胞介素5和干扰素-γ。它们在速发型超敏反应中作为辅助细胞参与IgE的产生,和/或在过敏性患者的迟发型超敏反应中作为效应细胞。特定抗原刺激的细胞获得白细胞介素2(IL2)反应性通常是诱导特异性免疫现象的一个重要事件。为了研究缓解期哮喘儿童的免疫变化,评估了粉尘螨(Dermatophagoides farinae)刺激的患者淋巴细胞诱导的IL2反应性和产生,以及患者淋巴细胞诱导的粉尘螨刺激的干扰素-γ产生。患者分为3组。缓解组(I)由那些在无药物治疗的情况下超过2年没有或仅有几次哮喘发作的患者组成。活动期哮喘组根据发作频率和严重程度分为2组(II,部分缓解;III,活动期哮喘)。II组和III组粉尘螨刺激的淋巴细胞的IL2反应性和产生增加。随着症状改善,反应程度降至与正常个体相当的水平(III组)。活动期哮喘患者粉尘螨刺激的淋巴细胞产生的干扰素-γ低于正常淋巴细胞。相反,完全缓解组(I)患者的淋巴细胞以粉尘螨抗原依赖的方式诱导产生的干扰素-γ比正常及II组和III组患者的淋巴细胞诱导产生的干扰素-γ多得多,这可能下调粉尘螨介导的过敏反应中粉尘螨诱导的高反应性。(摘要截短于250字)

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