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配体对胎鼠肺细胞中糖皮质激素受体表达的差异调节

Differential regulation of glucocorticoid receptor expression by ligand in fetal rat lung cells.

作者信息

Sweezey N, Mawdsley C, Ghibu F, Song L, Buch S, Moore A, Antakly T, Post M

机构信息

Hospital for Sick Children Research Institute, University of Toronto, Ontario, Canada.

出版信息

Pediatr Res. 1995 Oct;38(4):506-12. doi: 10.1203/00006450-199510000-00006.

Abstract

The glucocorticoid receptor (GR) mediates glucocorticoid stimulation of surfactant production by fetal mammalian lung. In many other tissues, glucorticoids decrease expression of GR, thereby reducing responsiveness to these hormones. We therefore determined whether there is a similar effect of exogenous glucocorticoids on GR in fetal rat whole lung, and in the principal cell types involved in the stimulation of surfactant, the fibroblasts and the epithelial cells. The ontogeny of GR in late gestation lung differed between the two cell types, with maximal levels occurring in fibroblasts on gestational d 19, and on d 20 in epithelial cells. Administration of dexamethasone (1 mg/kg) to the mother on gestational d 18 or 19 (term = 22 d) increased specific GR binding activity in whole lung 24 h later. Furthermore, in vitro, incubation of cultured fibroblasts of gestational d 20 with 10(-7) M cortisol increased GR immunoreactive protein and binding activity in a dose- and time-dependent manner, without affecting cellular levels of GR mRNA. However, identical treatment of d 20 distal airway epithelial cells was followed by decreased GR protein without significant change in cellular GR mRNA. Surfactant protein-A protein levels, taken as assessments of lung maturation, were increased in response to the same treatment. Our findings suggest that hormonal regulation of GR in fetal lung cells occurs at a posttranscriptional level, and is cell-specific. In the context of substantial increases in circulating glucocorticoid concentrations during late gestation, these findings may be of physiologic importance to the biochemical maturation of the antenatal lung.

摘要

糖皮质激素受体(GR)介导糖皮质激素对胎生哺乳动物肺表面活性物质产生的刺激作用。在许多其他组织中,糖皮质激素会降低GR的表达,从而降低对这些激素的反应性。因此,我们确定外源性糖皮质激素对胎鼠全肺以及参与刺激表面活性物质产生的主要细胞类型(成纤维细胞和上皮细胞)中的GR是否有类似作用。妊娠后期肺中GR的个体发生在两种细胞类型之间有所不同,成纤维细胞在妊娠第19天达到最高水平,上皮细胞在第20天达到最高水平。在妊娠第18天或19天(足月为22天)给母鼠注射地塞米松(1毫克/千克),24小时后全肺中GR的特异性结合活性增加。此外,在体外,将妊娠第20天的培养成纤维细胞与10^(-7) M皮质醇一起孵育,GR免疫反应蛋白和结合活性呈剂量和时间依赖性增加,而不影响细胞中GR mRNA的水平。然而,对第20天的远端气道上皮细胞进行相同处理后,GR蛋白减少,而细胞GR mRNA没有明显变化。作为肺成熟评估指标的表面活性蛋白-A蛋白水平,对相同处理有增加反应。我们的研究结果表明,胎儿肺细胞中GR的激素调节发生在转录后水平,并且具有细胞特异性。在妊娠后期循环糖皮质激素浓度大幅增加的情况下,这些发现可能对产前肺的生化成熟具有生理重要性。

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