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过敏性哮喘的小鼠模型能模拟临床疾病吗?

Do mouse models of allergic asthma mimic clinical disease?

作者信息

Epstein Michelle M

机构信息

Department of Dermatology, University of Vienna, Vienna, Austria.

出版信息

Int Arch Allergy Immunol. 2004 Jan;133(1):84-100. doi: 10.1159/000076131. Epub 2004 Jan 12.

Abstract

Experimental mouse models of allergic asthma established almost 10 years ago offered new opportunities to study disease pathogenesis and to develop new therapeutics. These models focused on the factors governing the allergic immune response, on modeling clinical behavior of allergic asthma, and led to insights into pulmonary pathophysiology. Although mouse models rarely completely reproduce all the features of human disease, after sensitization and respiratory tract challenges with antigen, wild-type mice develop a clinical syndrome that closely resembles allergic asthma, characterized by eosinophilic lung inflammation, airway hyperresponsiveness (AHR), increased IgE, mucus hypersecretion, and eventually, airway remodeling. There are, however, differences between mouse and human physiology that threaten to limit the value of mouse models. Three examples of such differences relate to both clinical manifestations of disease and underlying pathogenesis. First, in contrast to patients who have increased methacholine-induced AHR even when they are symptom-free, mice exhibit only transient methacholine-induced AHR following allergen exposure. Second, chronic allergen exposure in patients leads to chronic allergic asthma, whereas repeated exposures in sensitized mice causes suppression of disease. Third, IgE and mast cells, in humans, mediate early- and late-phase allergic responses, though both are unnecessary for the generation of allergic asthma in mice. Taken together, these observations suggest that mouse models of allergic asthma are not exact replicas of human disease and thus, question the validity of these models. However, observations from mouse models of allergic asthma support many existing paradigms, although some novel discoveries in mice have yet to be verified in patients. This review presents an overview of the clinical aspects of disease in mouse models of allergic asthma emphasizing (1). the factors influencing the pathophysiological responses during the initiation and perpetuation of disease, (2). the utility of mouse models for studying clinical manifestations of disease, and (3). the applicability of mouse models for testing new treatments for allergic asthma.

摘要

大约10年前建立的过敏性哮喘实验小鼠模型为研究疾病发病机制和开发新疗法提供了新机会。这些模型聚焦于控制过敏性免疫反应的因素、模拟过敏性哮喘的临床行为,并有助于深入了解肺部病理生理学。尽管小鼠模型很少能完全重现人类疾病的所有特征,但在致敏并经抗原进行呼吸道激发后,野生型小鼠会出现一种与过敏性哮喘极为相似的临床综合征,其特征为嗜酸性粒细胞性肺部炎症、气道高反应性(AHR)、IgE增加、黏液分泌过多,最终导致气道重塑。然而,小鼠和人类生理学之间存在差异,这可能会限制小鼠模型的价值。此类差异的三个例子既涉及疾病的临床表现,也涉及潜在的发病机制。首先,与即使无症状时也会出现乙酰甲胆碱诱导的AHR增加的患者不同,小鼠在接触过敏原后仅表现出短暂的乙酰甲胆碱诱导的AHR。其次,患者长期接触过敏原会导致慢性过敏性哮喘,而致敏小鼠反复接触则会导致疾病受到抑制。第三,在人类中,IgE和肥大细胞介导早期和晚期过敏反应,尽管在小鼠中产生过敏性哮喘两者并非必需。综上所述,这些观察结果表明过敏性哮喘的小鼠模型并非人类疾病的精确复制品,因此对这些模型的有效性提出了质疑。然而,过敏性哮喘小鼠模型的观察结果支持了许多现有的范例,尽管小鼠中的一些新发现尚未在患者中得到验证。本综述概述了过敏性哮喘小鼠模型中疾病的临床方面,重点强调了:(1)在疾病起始和持续过程中影响病理生理反应的因素;(2)小鼠模型在研究疾病临床表现方面的实用性;(3)小鼠模型在测试过敏性哮喘新疗法方面的适用性。

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