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变应原特异性免疫治疗:它终究是针对毒素的疫苗接种吗?

Allergen-specific immunotherapy: is it vaccination against toxins after all?

机构信息

Immunology, RIA, University Hospital Bern, Bern, Switzerland.

The Jenner Institute, University of Oxford, Oxford, UK.

出版信息

Allergy. 2017 Jan;72(1):13-23. doi: 10.1111/all.12890. Epub 2016 Sep 28.

Abstract

IgE-mediated allergies, in particular allergic rhinoconjunctivitis and asthma, have reached epidemic proportions, affecting about one-third of the population in developed countries. The most effective treatment for allergies is specific immunotherapy (SIT), which involves the injection of increasing doses of an allergen extract to allergic individuals. The current form of SIT was first introduced in 1911 and recently celebrated its 100th birthday for the treatment of hay fever. The concept of this therapy at the time was straightforward, as it was believed that pollen contained toxins against which the patient could be vaccinated. However, the understanding became blurred with the discovery that IgE antibodies were the effector molecules of the allergic response. Subsequent research focused on the idea that SIT should induce tolerance keeping the IgE antibodies at bay. In this review, we will discuss the various hypotheses for the mechanism of SIT and we will put forward the concept that allergens may be viewed as 'protoxins' which need to be activated by IgE antibodies. Within this framework, protoxin-neutralizing antibodies are the key effector molecules while a shift to Th1 or Treg cells mainly contributes to the efficacy of SIT by helping B cells to produce neutralizing IgG antibodies.

摘要

IgE 介导的过敏反应,特别是过敏性鼻结膜炎和哮喘,已经达到了流行的程度,影响了大约三分之一的发达国家的人口。过敏反应最有效的治疗方法是特异性免疫治疗(SIT),它涉及给过敏个体注射递增剂量的过敏原提取物。目前形式的 SIT 于 1911 年首次引入,最近为治疗花粉热庆祝了它的 100 岁生日。当时这种治疗的概念很简单,因为人们认为花粉含有可以对患者进行接种的毒素。然而,随着发现 IgE 抗体是过敏反应的效应分子,这种理解变得模糊了。随后的研究集中在 SIT 应该诱导耐受的想法上,使 IgE 抗体保持在海湾。在这篇综述中,我们将讨论 SIT 的各种机制假说,并提出过敏原可以被视为“原毒素”的概念,需要被 IgE 抗体激活。在这个框架内,原毒素中和抗体是关键的效应分子,而向 Th1 或 Treg 细胞的转变主要通过帮助 B 细胞产生中和 IgG 抗体来促进 SIT 的疗效。

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