Ban Masarin, Morel Georges, Langonné Isabelle, Huguet Nelly, Pépin Elsa, Binet Stéphane
Institut National de Recherche et de Sécurité, INRS, Avenue de Bourgogne, B.P. 27, 54501 Vandoeuvre Cedex, France.
Toxicology. 2006 Jan 20;218(1):39-47. doi: 10.1016/j.tox.2005.09.013. Epub 2005 Nov 3.
Toluene diisocyanate (TDI), a highly reactive industrial chemical is one of the leading causes of occupation-related asthma in industrialized countries. The pathophysiology of TDI-induced asthma, however, remains poorly understood, in part due to a lack of appropriate animal models. In this study, four models of TDI-sensitised mice were investigated. In model number 1, the mice were sensitised for 4 h/day on four consecutive days to 3 ppm inhaled TDI and challenged twice for 4 h each time with 0.3 ppm inhaled TDI. In model number 2, the sensitising condition was similar to that of model 1, but the challenge conditions involved an initial inhalation of 2 ppmTDI for 4h and then tracheal instillation with 50 microg/mouse albumin-TDI. In model number 3, the mice were sensitised first to 25% TDI (sc) and then three times for 4 h each time to 1 ppm inhaled TDI and challenged twice for 4h each time with 0.1 ppm inhalated TDI. In model number 4, the mice were first sensitised to 1% TDI by skin application and then with 0.2% TDI by tracheal instillation and challenged tree times by tracheal instillation of 0.1% TDI. In model number 4, skin application followed by tracheal instillations of TDI led to local and systemic Th2-dominated immune responses that were characterized: (1) in the lung-associated lymph nodes by a decrease in Th1 cytokine (IFN-gamma) production associated with an increase in Th2 cytokine (IL-4, IL-5, IL-3) production; (2) in the lungs by an allergic inflammation throughout the conducting airways: goblet cell proliferation and eosinophil influx and; (3) in the serums by increased total and specific IgE levels, 17.5- and 3.5-fold higher than that of the controls, respectively. The conditions used for sensitisation in the other models, i.e. inhalation or subcutaneous administration plus inhalation, failed to induce a strong Th2 response like that observed in model number 4. The findings indicate that TDI can induce a Th2-dominated response in mice when administered by topical application plus tracheal instillation for sensitisation and by intra-tracheal instillation for challenge (model number 4). This mouse Th2 model of TDI-induced airway allergy can, in several aspects, mimic occupational TDI asthma in humans and may prove to be useful in determining the mechanistic basis behind this disease.
甲苯二异氰酸酯(TDI)是一种高反应性的工业化学品,是工业化国家职业性哮喘的主要病因之一。然而,TDI诱发哮喘的病理生理学仍知之甚少,部分原因是缺乏合适的动物模型。在本研究中,对四种TDI致敏小鼠模型进行了研究。在模型1中,小鼠连续四天每天4小时吸入3 ppm的TDI进行致敏,然后每次用0.3 ppm吸入TDI激发4小时,共激发两次。在模型2中,致敏条件与模型1相似,但激发条件包括最初吸入2 ppm TDI 4小时,然后每只小鼠气管内注入50微克白蛋白-TDI。在模型3中,小鼠首先皮下注射25%的TDI进行致敏,然后每次4小时吸入1 ppm TDI,共三次,每次用0.1 ppm吸入TDI激发4小时,共激发两次。在模型4中,小鼠首先通过皮肤涂抹1%的TDI进行致敏,然后通过气管内注入0.2%的TDI进行致敏,并用0.1%的TDI气管内注入激发三次。在模型4中,皮肤涂抹后气管内注入TDI导致局部和全身以Th2为主的免疫反应,其特征为:(1)在肺相关淋巴结中,Th1细胞因子(IFN-γ)产生减少,同时Th2细胞因子(IL-4、IL-5、IL-3)产生增加;(2)在肺中,整个传导气道出现过敏性炎症:杯状细胞增殖和嗜酸性粒细胞浸润;(3)在血清中,总IgE和特异性IgE水平升高,分别比对照组高17.5倍和3.5倍。其他模型中用于致敏的条件,即吸入或皮下给药加吸入,未能诱导出如模型4中观察到的强烈Th2反应。研究结果表明,当通过局部涂抹加气管内注入进行致敏,并通过气管内注入进行激发时(模型4),TDI可在小鼠中诱导以Th2为主的反应。这种TDI诱发气道过敏的小鼠Th2模型在几个方面可模拟人类职业性TDI哮喘,可能有助于确定该疾病背后的机制基础。
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