重症哮喘动物模型构建研究
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上海中医药大学附属龙华医院,呼吸疾病研究所,上海 200032

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Construction of a severe asthma animal model
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Institute of Respiratory Diseases, Longhua Hospital Affliated to Shanghai University of Traditional Chinese Medicine, Shanghai 200032, China

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    目的 构建能够重现重症哮喘临床表型的动物模型。 方法 使用卵清蛋白(ovalbumin,OVA)联合 IL-33 或不同剂量的脂多糖(lipopolysaccharides,LPS)探索构建重症哮喘小鼠模型。 造模后通过肺功能、炎症细胞数量及肺组织病理,评估模型。 通过 GEO 数据库筛选重症哮喘患者的关键基因,对构建的模型进行验证。 结果 OVA 叠加 IL-33 或 LPS(5 μg)相较 OVA 哮喘模型能够显著增加气道阻力,肺泡灌洗液中炎症细胞数量,加重肺组织病理损伤。 在构建的重症哮喘模型中重症哮喘的关键基因表达情况与临床重症哮喘患者一致。 结论 OVA 联合 IL-33 或 LPS(5 μg)可用于构建重症哮喘的实验动物模型。

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    Objective To develop an animal model that replicates the clinical phenotype of severe asthma. Methods Ovalbumin (OVA) combined with IL-33 or varying doses of lipopolysaccharides ( LPS) was used to explore the construction of a severe asthma mouse model. Established model animals were assessed for lung function,number of inflammatory cells, and lung tissue pathology were assessed. Expression of key genes associated with severe asthma identified from the GEO database were validated in the new model. Results Compared with OVA alone,OVA combined with IL-33 or 5 μg LPS significantly increased airway resistance and the number of inflammatory cells in bronchoalveolar lavage fluid, and aggravated the pathological damage to lung tissues. The expression patterns of key genes in the newly constructed severe asthma models were consistent with those observed in clinical patients with severe asthma. Conclusions The modeling method of combining OVA with IL-33 or LPS (5 μg) can be used to construct experimentalanimal models of severe asthma.

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杨迪,鹿振辉,蒋雨薇,李翠,马子风,王钰,陈林锦,陆天逊,崔洁.重症哮喘动物模型构建研究[J].中国实验动物学报,2025,33(4):467~478.

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  • 收稿日期:2024-10-15
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  • 在线发布日期: 2025-06-09
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