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首页> 外文期刊>American Journal of Physiology >Dose-dependent lung remodeling in transgenic mice expressing transforming growth factor-alpha.
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Dose-dependent lung remodeling in transgenic mice expressing transforming growth factor-alpha.

机译:表达转化生长因子-α的转基因小鼠的剂量依赖性肺重塑。

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Transgenic mice overexpressing human transforming growth factor-alpha (TGF-alpha) develop emphysema and fibrosis during postnatal alveologenesis. To assess dose-related pulmonary alterations, four distinct transgenic lines expressing different amounts of TGF-alpha in the distal lung under control of the surfactant protein C (SP-C) promoter were characterized. Mean lung homogenate TGF-alpha levels ranged from 388 +/- 40 pg/ml in the lowest expressing line to 1,247 +/- 33 pg/ml in the highest expressing line. Histological assessment demonstrated progressive alveolar airspace size changes that were more severe in the higher expressing TGF-alpha lines. Pleural and parenchymal fibrosis were only detected in the highest expressing line (line 28), and increasing terminal airspace area was associated with increasing TGF-alpha expression. Hysteresis on pressure-volume curves was significantly reduced in line 28 mice compared with other lines of mice. There were no differences in bronchoalveolar lavage fluid cell count or differential that would indicate any evidence of lung inflammation among all transgenic lines. Proliferating cells were increased in line 28 without alterations of numbers of type II cells. We conclude that TGF-alpha lung remodeling in transgenic mice is dose dependent and is independent of pulmonary inflammation.
机译:过表达人类转化生长因子-α(TGF-α)的转基因小鼠在产后肺泡形成过程中出现肺气肿和纤维化。为了评估剂量相关的肺部改变,表征了在表面活性剂蛋白C(SP-C)启动子的控制下在远端肺中表达不同量的TGF-α的四个不同的转基因系。平均肺匀浆TGF-α水平范围从最低表达细胞系的388 +/- 40 pg / ml到最高表达细胞系的1,247 +/- 33 pg / ml。组织学评估显示,渐进性肺泡空域大小变化在高表达TGF-α系中更为严重。胸膜和实质纤维化仅在表达最强的细胞系(28系)中检测到,并且末端空域面积的增加与TGF-α表达的增加有关。与其他品系的小鼠相比,品系28的小鼠的压力-容量曲线上的滞后明显降低。在所有转基因株系中,支气管肺泡灌洗液细胞计数或差异均无差异,表明肺炎的任何证据。在第28行中增殖细胞增加,而II型细胞的数目没有改变。我们得出的结论是,转基因小鼠中的TGF-α肺重塑是剂量依赖性的,并且与肺部炎症无关。

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