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Animal models for protein respiratory sensitizers.

机译:蛋白质呼吸致敏剂的动物模型。

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Protein induced respiratory hypersensitivity, particularly atopic disease in general, and allergic asthma in particular, has increased dramatically over the last several decades in the US and other industrialized nations as a result of ill-defined changes in living conditions in modern western society. In addition, work-related asthma has become the most frequently diagnosed occupational respiratory illness. Animal models have demonstrated great utility in developing an understanding of the etiology and mechanisms of many diseases. A few models been developed as predictive models to identify a protein as an allergen or to characterize its potency. Here we describe animal models that have been used to investigate and identify protein respiratory sensitizers. In addition to prototypical experimental design, methods for exposure route, sample collection, and endpoint assessment are described. Some of the most relevant endpoints in assessing the potential for a given protein to induce atopic or allergic asthma respiratory hypersensitivity are the development of cytotropic antibodies (IgE, IgG1), eosinophil influx into the lung, and airway hyperresponsiveness to the sensitizing protein and/or to non-antigenic stimuli (Mch). The utility of technologies such as PCR and multiplexing assay systems is also described. These models and methods have been used to elucidate the potential for protein sources to induce allergy, identify environmental conditions (pollutants) to impact allergy responsiveness, and establish safe exposure limits. As an example, data are presented from an experiment designed to compare the allergenicity of a fungal biopesticide Metarhizium anisopliae (MACA) crude extract with the one of its components, conidia (CON) extract.
机译:在过去的几十年中,由于现代西方社会生活状况的不确定性变化,蛋白质引起的呼吸道超敏反应,特别是一般的特应性疾病,尤其是过敏性哮喘,急剧增加。此外,与工作有关的哮喘已成为诊断最频繁的职业呼吸道疾病。动物模型在发展对许多疾病的病因和机制的理解方面显示出极大的实用性。已经开发了一些模型作为预测模型,以识别蛋白质为过敏原或表征其功效。在这里,我们描述了已经用于研究和鉴定蛋白质呼吸致敏剂的动物模型。除了原型实验设计之外,还介绍了暴露途径,样品收集和终点评估的方法。在评估特定蛋白质诱发特应性或过敏性哮喘呼吸道超敏反应的潜力时,一些最相关的终点是细胞溶性抗体(IgE,IgG1)的发展,嗜酸性粒细胞向肺内的流入以及气道对敏化蛋白质和/或超敏反应非抗原刺激(Mch)。还描述了诸如PCR和多重测定系统之类的技术的实用性。这些模型和方法已用于阐明蛋白质来源诱发过敏的可能性,识别影响过敏反应的环境条件(污染物)以及建立安全暴露极限的方法。举例来说,数据来自一个实验,该实验旨在比较真菌生物杀虫剂金属异硫菌(MACA)粗提物与其分生孢子(CON)提取物之一的致敏性。

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