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兔羊膜细胞中催产素受体基因表达的诱导

Induction of oxytocin receptor gene expression in rabbit amnion cells.

作者信息

Jeng Y J, Lolait S J, Soloff M S

机构信息

Department of Obstetrics and Gynecology, University of Texas Medical Branch, Galveston 77555-1062, USA.

出版信息

Endocrinology. 1998 Aug;139(8):3449-55. doi: 10.1210/endo.139.8.6147.

DOI:10.1210/endo.139.8.6147
PMID:9681495
Abstract

Oxytocin (OT)-stimulated PGE2 release by rabbit amnion is enhanced by the up-regulation of oxytocin receptors (OTR), which increase about 200-fold at the end of pregnancy. As recent studies have shown that PGs are essential for parturition, the rise in amnion OTR and associated PGE2 synthesis are probably essential for labor initiation. The present work was directed toward understanding the mechanisms of OTR up-regulation. Levels of agents that stimulate adenylyl cyclase activity and cortisol are increased in amniotic fluid at the end of pregnancy. Addition of either forskolin or cortisol to cultured amnion cells caused an increase in OTR ligand-binding sites and steady state OTR messenger RNA (mRNA) levels. Forskolin treatment elevated OTR mRNA levels rapidly, but transiently, whereas cortisol's effects were slower and sustained. Actinomycin or cycloheximide, added 3 h after forskolin, led to a sustained elevation in OTR mRNA levels, suggesting that forskolin increases the activities of OTR mRNA-destabilizing factors along with increasing OTR mRNA concentration. Cortisol did not appear to affect OTR mRNA stability. Measurement of OTR mRNA transcription rates showed that forskolin's effects were maximal within 1 h of treatment. In contrast, cortisol-induced transcription was not apparent until 8 h. The effects of forskolin and cortisol on OTR gene transcription were synergistic. Thus, the increase in OTR mRNA levels occurring after either forskolin or cortisol treatments is the result of induction of OTR gene expression, but the effects of the two agents appear to occur at separate sites.

摘要

催产素(OT)刺激兔羊膜释放前列腺素E2(PGE2)的作用会因催产素受体(OTR)上调而增强,在妊娠末期OTR数量会增加约200倍。近期研究表明,前列腺素对于分娩至关重要,羊膜OTR的增加及相关PGE2的合成可能对于启动分娩必不可少。本研究旨在了解OTR上调的机制。在妊娠末期,羊水内刺激腺苷酸环化酶活性的物质及皮质醇水平会升高。向培养的羊膜细胞中添加福斯高林或皮质醇会导致OTR配体结合位点及稳态OTR信使核糖核酸(mRNA)水平增加。福斯高林处理能迅速但短暂地提高OTR mRNA水平,而皮质醇的作用则较慢且持续时间长。在福斯高林处理3小时后添加放线菌素或环己酰亚胺会导致OTR mRNA水平持续升高,这表明福斯高林在增加OTR mRNA浓度的同时还增强了OTR mRNA不稳定因子的活性。皮质醇似乎并未影响OTR mRNA的稳定性。对OTR mRNA转录速率的测量显示,福斯高林的作用在处理后1小时内达到最大。相比之下,皮质醇诱导的转录直到8小时后才明显。福斯高林和皮质醇对OTR基因转录的作用具有协同性。因此,福斯高林或皮质醇处理后OTR mRNA水平的增加是OTR基因表达诱导的结果,但这两种物质的作用似乎发生在不同位点。

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