Asthma and Allergic Disease Center, University of Virginia Health Systems, MR4 Bldg, Rm, 5041, Lane Rd, Charlottesville, Virginia, USA 22908.
Allergy Asthma Clin Immunol. 2005 Dec 15;1(4):161-73. doi: 10.1186/1710-1492-1-4-161.
This article summarizes and provides commentary regarding guidelines on the administration of immunotherapy (IT) for allergic airway disease. Recent investigations have provided important insights into the immunologic mechanism of IT and the prominent role of interleukin-10-producing regulatory T lymphocytes. The most important aspect of successful IT is the administration of an appropriate dose of an extract containing a sufficient concentration of the relevant allergen. This is largely possible now only with standardized extracts. When the major allergen content of successful IT extracts was quantified, efficacy was demonstrated across a surprisingly narrow concentration range (approximately 5-24 mug per injection), irrespective of the extract. This presumably reflects the concentration of an antigen that drives an immune response toward tolerance. It may be predicted that as major allergen content is quantified in currently nonstandardized extracts, effective IT will also be achieved by administering a dose in this range, in contrast to current practices involving fairly arbitrary dosing decisions. With the availability of nonsedating antihistamines, intranasal corticosteroids, and the leukotriene modifiers, inadequate pharmacologic response or intolerable side effects are less commonly the major indications for starting IT for allergic rhinitis (AR). However, with the recognition that a relatively short course (3-5 years) of IT can provide long-term immunomodulation and clinical benefit, a desire to avoid long-term pharmacotherapy and the associated high costs may be the primary indication for IT in AR cases. While evidence overwhelmingly supports the beneficial influences of IT in asthma cases, the positioning of IT for this disorder is not established. The observed prevention of asthma in children who have AR is intriguing, but further studies are required to assess the extent to which the prevalence and severity of chronic asthma will be reduced when these children reach adulthood. Similarly, safety issues overwhelmingly suggest that uncontrolled asthma is the greatest risk factor for mortality associated with IT and that IT therefore may be contraindicated for most patients who have inadequate pharmacologic responses or are unable to tolerate useful pharmacologic agents. Paradoxically, these are the patients for whom a response to IT may be most desirable.
这篇文章总结并评论了关于过敏性气道疾病免疫治疗 (IT) 管理的指南。最近的研究为 IT 的免疫机制和白细胞介素-10 产生的调节性 T 淋巴细胞的重要作用提供了重要的见解。成功的 IT 的最重要方面是给予含有足够浓度相关过敏原的提取物的适当剂量。这在很大程度上现在只有通过标准化提取物才有可能。当成功的 IT 提取物的主要过敏原含量被量化时,无论提取物如何,在令人惊讶的狭窄浓度范围内(约 5-24 微克/注射)都证明了疗效。这大概反映了驱动免疫反应向耐受的抗原浓度。可以预测,随着目前非标准化提取物中主要过敏原含量的量化,通过在该范围内给予剂量也将实现有效的 IT,与目前涉及相当任意剂量决策的实践形成对比。随着非镇静抗组胺药、鼻内皮质类固醇和白三烯调节剂的应用,药理反应不足或不可耐受的副作用不再是开始过敏性鼻炎 (AR) IT 的主要指征。然而,随着认识到相对较短的 IT 疗程(3-5 年)可以提供长期免疫调节和临床益处,避免长期药物治疗和相关高成本可能成为 AR 病例中 IT 的主要指征。虽然压倒性的证据支持 IT 在哮喘病例中的有益影响,但 IT 在这种疾病中的定位尚未确定。观察到 AR 患儿哮喘的预防令人着迷,但需要进一步研究来评估当这些儿童成年时,慢性哮喘的患病率和严重程度将在多大程度上降低。同样,安全性问题压倒性地表明,未控制的哮喘是与 IT 相关的死亡率的最大危险因素,因此 IT 可能不适用于大多数药理反应不足或无法耐受有用药物的患者。具有讽刺意味的是,这些是最希望对 IT 有反应的患者。
