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糖皮质激素对人肺表面活性物质蛋白SP-B和SP-C的转录调控

Transcriptional regulation of human pulmonary surfactant proteins SP-B and SP-C by glucocorticoids.

作者信息

Ballard P L, Ertsey R, Gonzales L W, Gonzales J

机构信息

Department of Pediatrics, University of Pennsylvania School of Medicine, Children's Hospital of Philadelphia 19104, USA.

出版信息

Am J Respir Cell Mol Biol. 1996 Jun;14(6):599-607. doi: 10.1165/ajrcmb.14.6.8652188.

DOI:10.1165/ajrcmb.14.6.8652188
PMID:8652188
Abstract

Expression of the pulmonary surfactant-associated proteins SP-B and SP-C is under both developmental and hormonal regulation. We used human fetal lung to investigate developmental changes and the mechanism of glucocorticoid stimulation of SP-B and SP-C gene expression. There were similar approximately 3-fold increases in SP-B cytoplasmic mRNA content and transcription rate comparing lung samples of 24 wk versus 16 wk gestation. During 5 days of lung explant culture without hormones, the transcription rate increased for SP-B and decreased for SP-C, paralleling changes in mRNA content. Treatment with 100 nM dexamethasone maximally increased transcription of the SP-B gene (approximately 3-fold) and SP-C gene (approximately 11-fold) after 2 and 8 h, respectively, similar to changes in mRNA content. In dose-response studies, the maximal increase in transcription rate occurred at approximately 10 nM dexamethasone for SP-B and at > or = 100 nM for SP-C. Induction of SP-B mRNA content and transcription rate were not affected by prior cycloheximide exposure, whereas induction of SP-C mRNA was decreased by as little as 1 h exposure to inhibitor. We conclude that glucocorticoids, acting directly in type II cells, regulate the SP-B and SP-C genes primarily at the level of transcription. Induction of SP-C, but not SP-B, requires ongoing protein synthesis which likely reflects involvement of a labile transcription factor. The difference in glucocorticoid sensitivity may indicate that the two surfactant protein genes contain glucocorticoid response elements with different affinities for receptor.

摘要

肺表面活性物质相关蛋白SP-B和SP-C的表达受发育和激素调节。我们利用人胎儿肺来研究SP-B和SP-C基因表达的发育变化及糖皮质激素刺激机制。比较妊娠16周与24周的肺样本,SP-B细胞质mRNA含量和转录率有相似的约3倍增加。在无激素的肺外植体培养5天期间,SP-B的转录率增加,而SP-C的转录率下降,与mRNA含量变化平行。分别在2小时和8小时后,用100 nM地塞米松处理可使SP-B基因(约3倍)和SP-C基因(约11倍)的转录最大程度增加,与mRNA含量变化相似。在剂量反应研究中,SP-B转录率的最大增加出现在约10 nM地塞米松时,而SP-C则在≥100 nM时出现。预先暴露于环己酰亚胺对SP-B mRNA含量和转录率的诱导无影响,而暴露于抑制剂仅1小时就可降低SP-C mRNA的诱导。我们得出结论,糖皮质激素直接作用于II型细胞,主要在转录水平调节SP-B和SP-C基因。SP-C而非SP-B的诱导需要持续的蛋白质合成,这可能反映了一种不稳定转录因子的参与。糖皮质激素敏感性的差异可能表明这两个表面活性物质蛋白基因含有对受体亲和力不同的糖皮质激素反应元件。

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