用重组过敏原或构建过敏原诱导粘膜耐受预防和治疗过敏。

Ursula Wiedermann
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引用次数: 31

摘要

粘膜免疫系统,存在于呼吸道,胃肠道和泌尿生殖系统,必须区分有害的病原体和无害的抗原,如食物,空气中的抗原或共生菌群。因此,粘膜免疫系统获得了两种相反的免疫功能,即诱导免疫和防御粘膜病原体,以及诱导和维持对环境抗原和细菌菌群的耐受性。正如对自身免疫的描述,耐受性诱导的崩溃或失败被认为也会导致过敏和食物肠病。基于防止超敏反应的生理作用,通过粘膜诱导耐受已被提出作为对抗炎症性疾病(如过敏)的治疗策略。我们研究的目的是开发基于诱导粘膜耐受和/或诱导反调节免疫反应的粘膜过敏疫苗,无论是否使用某些粘膜抗原传递系统,如乳酸菌。使用重组过敏原代替具有不同过敏原含量和组成的过敏原提取物可能是改善治疗功效所必需的。在本综述中,我们给出了不同的I型过敏/哮喘动物模型的例子。使用这些模型,我们证明重组过敏原或其低过敏原变体可以成功地用于诱导粘膜耐受预防以及治疗治疗方案。最近的局部(舌下)应用免疫疗法的临床试验支持了粘膜耐受诱导/粘膜疫苗递送的概念在原则上也可能在人类中起作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Prophylaxis and therapy of allergy by mucosal tolerance induction with recombinant allergens or allergen constructs.

The mucosal immune system, present along the respiratory, gastrointestinal and genitourinary tract, has to discriminate between harmful pathogens and innocuous antigens, such as food, airborne antigens or the commensal bacterial flora. Therefore the mucosal immune system has acquired two opposing immunological functions, i.e. the induction of immunity and defence of mucosal pathogens, and the induction and maintenance of tolerance to environmental antigens and bacterial flora. As described for autoimmunity a breakdown or failure of tolerance induction is believed to lead also to allergies and food enteropathies. Based on the physiological role to prevent hypersensitivity reactions, tolerance induction via the mucosa has been proposed as a treatment strategy against inflammatory diseases, such as allergies. The aim of our research is to develop mucosal allergy vaccines based on the induction of mucosal tolerance and/or the induction of counter-regulatory immune responses with or without the use of certain mucosal antigen delivery systems, such as lactic acid bacteria. The use of recombinant allergens instead of allergen extracts with varying allergen content and composition may be essential for improvement of the treatment efficacy. In the present review we give examples of different animal models of type I allergy/asthma. Using these models we demonstrate that recombinant allergens or hypoallergenic variants thereof can be successfully used to induce mucosal tolerance in a prophylactic as well as a therapeutic treatment regime. That the concept of mucosal tolerance induction/mucosal vaccine delivery may in principal also function in humans is supported by recent clinical trials with locally (sublingual) applied immunotherapy.

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