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用于治疗IgE介导的过敏性疾病的抗IgE抗体。

Anti-IgE antibodies for the treatment of IgE-mediated allergic diseases.

作者信息

Chang Tse Wen, Wu Pheidias C, Hsu C Long, Hung Alfur F

机构信息

Genomics Research Center, Academia Sinica, Nankang, Taipei 115, Taiwan.

出版信息

Adv Immunol. 2007;93:63-119. doi: 10.1016/S0065-2776(06)93002-8.

Abstract

The pharmacological purposes of the anti-IgE therapy are to neutralize IgE and to inhibit its production to attenuate type I hypersensitivity reactions. The therapy is based on humanized IgG1 antibodies that bind to free IgE and to membrane-bound IgE on B cells, but not to IgE bound by the high-affinity IgE.Fc receptors on basophils and mast cells or by the low-affinity IgE.Fc receptors on B cells. After nearly 20 years since inception, therapeutic anti-IgE antibodies (anti-IgE) have been studied in about 30 Phase II and III clinical trials in many allergy indications, and a lead antibody, omalizumab, has been approved for treating patients (12 years and older) with moderate-to-severe allergic asthma. Anti-IgE has confirmed the roles of IgE in the pathogenesis of asthma and helped define the concept "allergic asthma" in clinical practice. It has been shown to be safe and efficacious in treating pediatric allergic asthma and treating allergic rhinitis and is being investigated for treating peanut allergy, atopic dermatitis, latex allergy, and others. It has potential for use to combine with specific and rush immunotherapy for increased safety and efficacy. Anti-IgE thus appears to provide a prophylactic and therapeutic option for moderate to severe cases of many allergic diseases and conditions in which IgE plays a significant role. This chapter reviews the evolution of the anti-IgE concept and the clinical studies of anti-IgE on various disease indications, and presents a comprehensive analysis on the multiple intricate immunoregulatory pharmacological effects of anti-IgE. Finally, it reviews other approaches that target IgE or IgE-expressing B cells.

摘要

抗IgE疗法的药理学目的是中和IgE并抑制其产生,以减轻I型超敏反应。该疗法基于人源化IgG1抗体,其可与游离IgE以及B细胞上的膜结合IgE结合,但不与嗜碱性粒细胞和肥大细胞上的高亲和力IgE.Fc受体或B细胞上的低亲和力IgE.Fc受体结合的IgE结合。自问世近20年来,治疗性抗IgE抗体(抗IgE)已在多种过敏适应症的约30项II期和III期临床试验中进行了研究,一种先导抗体奥马珠单抗已被批准用于治疗中度至重度过敏性哮喘患者(12岁及以上)。抗IgE已证实IgE在哮喘发病机制中的作用,并有助于在临床实践中定义“过敏性哮喘”的概念。已证明其在治疗儿童过敏性哮喘和过敏性鼻炎方面安全有效,并且正在研究用于治疗花生过敏、特应性皮炎、乳胶过敏等。它有可能与特异性和快速免疫疗法联合使用,以提高安全性和疗效。因此,抗IgE似乎为许多IgE起重要作用的中度至重度过敏性疾病和病症提供了一种预防和治疗选择。本章回顾了抗IgE概念的演变以及抗IgE在各种疾病适应症上的临床研究,并对抗IgE复杂的多种免疫调节药理作用进行了综合分析。最后,回顾了其他靶向IgE或表达IgE的B细胞的方法。

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