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首页> 外文期刊>The Journal of Thoracic and Cardiovascular Surgery >A novel charcoal-induced model of obliterative bronchiolitis-like lesions: implications of chronic nonspecific airway inflammation in the development of posttransplantation obliterative bronchiolitis (see comments)
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A novel charcoal-induced model of obliterative bronchiolitis-like lesions: implications of chronic nonspecific airway inflammation in the development of posttransplantation obliterative bronchiolitis (see comments)

机译:一种新型的木炭诱导的闭塞性细支气管炎样病变模型:慢性非特异性气道炎症在移植后闭塞性细支气管炎发展中的意义(参见评论)

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OBJECTIVES: In this study, we describe the development of a nonallogeneic animal model of obliterative bronchiolitis-like lesions. Furthermore, we examined whether chronic rejection alone can lead to the development of obliterative bronchiolitis or whether additional nonspecific airway inflammation is required. METHODS: Part I: Rats were intratracheally injected with 0.2 ml of activated charcoal or sorbitol solution (carrier for charcoal control). Animals were put to death beginning at 2 weeks up to 20 weeks. Part II: Animals were divided into three groups: group I, underimmunosuppressed Brown Norway to Lewis lung allografts; group II, charcoal-treated underimmunosuppressed allografts; and group III, charcoal-treated rats. Animals were put to death at 3 months after transplantation. RESULTS: Part I: In charcoal-laden bronchioles, subacute nonspecific airway inflammation was detected at 2 weeks. Slow, subclinical fibroproliferation ensued during the following weeks. Obliterative bronchiolitis-like lesions were observed in 80% of charcoal-treated animals at 12 weeks. Part II: Allografts developed extensive vascular lesions consistent with acute and chronic vascular rejection. Obliterative bronchiolitis-like lesions were scarcely detected. Charcoal-treated allografts demonstrated evidence of diffuse and severe obliterative bronchiolitis-like lesions. CONCLUSIONS: Transtracheal injection of activated charcoal into native lungs results in slowly progressive airway injury and inflammation leading to obliterative airway lesions. Inadequate immunosuppression primarily results in chronic vascular rejection but not obliterative bronchiolitis. Underimmunosuppressed allografts subjected to nonspecific airway inflammation develop obliterative airway lesions that are more prominent than in native lungs. This suggests that a cofactor to chronic rejection is likely necessary for the development of lung transplant obliterative bronchiolitis.
机译:目的:在这项研究中,我们描述了闭塞性细支气管炎样病变的非同种动物模型的发展。此外,我们检查了仅慢性排斥反应是否会导致闭塞性细支气管炎的发展,或者是否需要其他非特异性气道炎症。方法:第一部分:向大鼠气管内注射0.2 ml活性炭或山梨糖醇溶液(控制炭的载体)。从2周到20周开始处死动物。第二部分:将动物分为三组:第一组,免疫力低下的布朗挪威对刘易斯肺移植。第二组,用木炭处理的免疫抑制不足的同种异体移植物;第三组,用木炭处理的大鼠。移植后3个月将动物处死。结果:第一部分:在充满木炭的细支气管中,在2周时检测到亚急性非特异性气道炎症。随后几周出现缓慢的亚临床纤维增生。在第12周时,在80%经木炭处理的动物中观察到了闭塞性细支气管炎样病变。第二部分:同种异体移植物形成了广泛的血管病变,与急性和慢性血管排斥反应一致。几乎没有发现闭塞性细支气管炎样病变。木炭处理的同种异体移植物证明弥漫性和严重闭塞性细支气管炎样病变。结论:经气管内将活性炭经气管注入自然肺会导致缓慢的进行性气道损伤和炎症,导致气道闭塞性病变。免疫抑制不足主要导致慢性血管排斥反应,但不会导致闭塞性细支气管炎。受到非特异性气道炎症的免疫抑制不足同种异体移植会产生闭塞性气道病变,这种病变比自然肺更为明显。这表明,慢性排斥反应的辅助因子可能是肺移植闭塞性细支气管炎发展的必要条件。

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