免疫治疗在过敏性呼吸道疾病中的作用:对现有知识的重新评价

Rita Arrigo, N. Scichilone
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引用次数: 4

摘要

过敏性鼻-结膜炎和哮喘是由易感个体对一种或多种过敏原致敏引起的。特异性免疫疗法(SIT)用于过敏性疾病,因为它调节免疫反应,诱导外周t细胞耐受和调节性t细胞的激活。在此基础上,SIT被认为是唯一的治疗方法,可以改变过敏性疾病的自然史。工程过敏原的发展有助于降低过敏原的致敏性,从而防止副作用的发生。单体类过敏原具有有利于粘膜吸收的结构构象和分子大小,与给予天然过敏原相比,其副作用风险较低,保持了免疫刺激。经皮(SCIT)或舌下(SLIT)给药的SIT的疗效已在很大程度上证明了鼻结膜炎;此外,临床试验也证明了免疫疗法对过敏性哮喘的疗效。对室内尘螨、顶叶螨或草花粉过敏的哮喘患者有治疗效果。免疫疗法的一个重要而有趣的方面,与标准的药物治疗不同,是停药后的持久效果。在这方面,几项针对成人和儿童的SLIT研究清楚地表明,在停止免疫治疗后,有益效果可维持长达6年。本文综述了该药的主要适应症,并讨论了其在变应性鼻结膜炎和哮喘中的疗效和安全性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
The Effect of Immunotherapy in Allergic Respiratory Diseases: Reappraisal of Current Knowledge
Allergic rhino-conjunctivitis and asthma are induced by sensitization to one or more allergens in susceptible individuals. Specific immunotherapy (SIT) is indicated in allergic diseases, because it modulates the immune response inducing peripheral T-cell tolerance and activation of regulatory T-cells. On this basis, SIT is considered the only therapeutic approach that can modify the natural history of the allergic diseases. The development of engineered-allergen has contributed to reduce the allergenicity thus preventing the risk of side effects. The monomeric allergoids, with structural conformation and molecular size that facilitate the mucosal absorption, carry a lower risk for side effects compared to the administration of native allergens, maintaining the immunological stimulation. The efficacy of SIT, administered percutaneously (SCIT) or sublingual (SLIT), has been largely demonstrated in rhino-conjunctivitis; moreover, clinical trials have also demonstrated the efficacy of immunotherapy in allergic asthma. A therapeutic effect on asthma control has been shown in asthmatic subjects allergic to house dust mites, parietaria or grass pollen. An important and intriguing aspect of immunotherapy, not shared with the standard pharmacological treatments, is the long-lasting effect after discontinuation. In this respect, several SLIT studies in adults and children have clearly shown that the beneficial effects are maintained for up to 6 years after discontinuation of immunotherapy. The current review describes the main indications for SIT, and discusses its efficacy and safety in allergic rhino-conjunctivitis and asthma.
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