由SP-C启动子驱动的转基因糖皮质激素受体表达降低了GRhypo小鼠新生肺细胞和midkine的表达。

Biology of the neonate Pub Date : 2006-01-01 Epub Date: 2006-03-03 DOI:10.1159/000091844
Stéphane Gagnon, Wayhuni Atmodjo, Daryl Humes, Colin McKerlie, Feige Kaplan, Neil B Sweezey
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引用次数: 9

摘要

背景:已知糖皮质激素受体(GR)的先天性截断会导致新生小鼠致命的肺不成熟,这与肺细胞量(组织与空气的比例)增加有关,正如我们之前所显示的,类视黄酮反应性生长因子midkine的表达延长。目的:我们试图确定在远端气道上皮中转基因表达GR是否会逆转这些变化。方法:以先天性GR截断为背景,在人(h) SP-C启动子的驱动下,用转基因大鼠(r) GR生成小鼠。结果:转基因上皮GR表达将肺细胞数量和midkine表达降低到与野生型幼崽相当的水平。然而,新生的转基因小鼠仍然表现出呼吸衰竭。此外,GR转基因的上皮表达并没有改变肺成熟的一些重要标志物的表达。结论:我们的数据显示,在远端气道上皮中表达转基因GR的新生小鼠的肺组织与空气比率正常化,这与正常间充质细胞损失是由于上皮细胞的GR反应性刺激所致的概念一致。然而,我们没有发现小鼠组间凋亡活性改变的证据。我们推测,纠正GR缺陷小鼠严重的新生儿肺表型将需要在非上皮组织和上皮组织中表达正常GR。
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Transgenic glucocorticoid receptor expression driven by the SP-C promoter reduces neonatal lung cellularity and midkine expression in GRhypo mice.

Background: Congenital truncation of the glucocorticoid receptor (GR) is known to lead to lethal lung immaturity in newborn mice associated with increased lung cellularity (ratio of tissue to airspace) and, as we previously showed, prolonged expression of the retinoid-responsive growth factor midkine.

Objectives: We sought to determine if these changes would be reversed by transgenic expression of GR exclusively in the distal airway epithelium.

Methods: Mice were generated with expression of transgenic rat (r) GR driven by the human (h) SP-C promoter, on a background of congenital GR truncation.

Results: Transgenic epithelial GR expression reduced lung cellularity and midkine expression to levels comparable to wild-type littermates. Nevertheless, the newborn transgenic mice still displayed respiratory failure. Moreover, epithelial expression of the GR transgene did not alter expression of a number of important markers of lung maturation.

Conclusions: Our data demonstrating normalization of the lung tissue to airspace ratio in neonatal mice expressing transgenic GR in the distal airway epithelium is consistent with the concept that normal mesenchymal cell loss is due to GR-responsive stimulation from epithelial cells. However, we could find no evidence of altered apoptotic activity between the groups of mice. We speculate that correction of the severe neonatal lung phenotype of GR-deficient mice will require expression of normal GR in non-epithelial as well as epithelial tissues.

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