首页> 美国卫生研究院文献>Journal of Visualized Experiments : JoVE >Development of an in vitro model system for studying the interaction of Equuscaballus IgE with its high-affinity receptor FcεRI
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Development of an in vitro model system for studying the interaction of Equuscaballus IgE with its high-affinity receptor FcεRI

机译:开发用于研究马属相互作用的体外模型系统Caballus IgE及其高亲和力受体FcεRI

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摘要

The interaction of IgE with its high-affinity Fc receptor (FcεRI) followed by an antigenic challenge is the principal pathway in IgE mediated allergic reactions. As a consequence of the high affinity binding between IgE and FcεRI, along with the continuous production of IgE by B cells, allergies usually persist throughout life, with currently no permanent cure available. Horses, especially race horses, which are commonly inbred, are a species of mammals that are very prone to the development of hypersensitivity responses, which can seriously affect their performance. Physiological responses to allergic sensitization in horses mirror that observed in humans and dogs. In this paper we describe the development of an in situ assay system for the quantitative assessment of the release of mediators of the allergic response pertaining to the equine system. To this end, the gene encoding equine FcεRIα was transfected into and expressed onto the surface of parental Rat Basophil Leukemia (RBL-2H3.1) cells. The gene product of the transfected equine α-chain formed a functional receptor complex with the endogenous rat β- and γ-chains 1. The resultant assay system facilitated an assessment of the quantity of mediator secreted from equine FcεRIα transfected RBL-2H3.1 cells following sensitization with equine IgE and antigenic challenge using β-hexosaminidase release as a readout 2, 3. Mediator release peaked at 36.68% ± 4.88% at 100 ng ml-1 of antigen. This assay was modified from previous assays used to study human and canine allergic responses 4, 5. We have also shown that this type of assay system has multiple applications for the development of diagnostic tools and the safety assessment of potential therapeutic intervention strategies in allergic disease 6, 2, 3.
机译:IgE与它的高亲和力Fc受体(FcεRI)的相互作用以及随后的抗原攻击是IgE介导的过敏反应的主要途径。由于IgE和FcεRI之间的高亲和力结合以及B细胞连续产生IgE,过敏症通常会持续一生,目前尚无永久性治愈方法。通常自交的马,特别是赛马是很容易产生超敏反应的哺乳动物,会严重影响其性能。对马过敏性变态反应的生理反应与在人和狗中观察到的反应相同。在本文中,我们描述了一种原位分析系统的开发,该系统用于定量评估与马系统有关的过敏反应介体的释放。为此,将编码马FcεRIα的基因转染进亲本大鼠嗜碱性粒细胞白血病(RBL-2H3.1)细胞并在其表面表达。转染的马α链的基因产物与内源性大鼠β链和γ链 1 形成功能性受体复合物。所得的测定系统有助于评估用马IgE致敏并以β-己糖胺酶释放为抗原的抗原攻击后,马FcεRIα转染的RBL-2H3.1细胞分泌的介体数量,其读数为 2,3 。在100 ng ml -1 抗原中,介质释放的峰值为36.68%±4.88%。此方法是对以前用于研究人和犬过敏反应的方法进行了改进, 4,5 。我们还表明,这种化验系统在变应性疾病 6,2,3 的诊断工具开发和潜在治疗干预策略的安全性评估中具有多种应用。

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