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B型利钠肽受体的表达与活性在大鼠卵巢细胞中受激素调节。

B-type natriuretic peptide receptor expression and activity are hormonally regulated in rat ovarian cells.

作者信息

Noubani A, Farookhi R, Gutkowska J

机构信息

Department of Medicine, McGill University, Montréal, Québec, Canada.

出版信息

Endocrinology. 2000 Feb;141(2):551-9. doi: 10.1210/endo.141.2.7305.

Abstract

Natriuretic peptides form a family of structurally related peptides known to regulate salt and water homeostasis and to cause vasodilation. Synthesis of atrial (ANP), brain (BNP), and C-type (CNP) natriuretic peptides occurs mainly in the heart and brain and has been identified recently in the female reproductive tract. The expression of ANP and CNP as well as their cognate guanylyl cyclase receptors (NPR-A and NPR-B, respectively) have been detected in the rat ovary. We have shown previously that the expression of the natriuretic peptides and their receptors in the rat ovary appears to be modulated by the estrous cycle. In the present study we have evaluated the expression of the natriuretic peptide system (peptide and receptor) in ovarian cells (granulosa and thecal-interstitial cells) obtained from immature female rats treated with either diethylstilbestrol (DES), an estrogen analog, or equine CG (eCG), a gonadotropin that possesses both LH and FSH activity. Using a whole cell RRA, we found that CNP binding was increased by 2-fold in granulosa cells taken from animals treated with either DES or eCG. Semiquantitative RT-PCR revealed that granulosa cells from DES- or eCG-treated animals have increased levels of NPR-B messenger RNA (mRNA) transcripts, which was in good agreement with the increased binding. The activity of the receptors was assessed by ligand-dependent stimulation of cGMP release. CNP, but not ANP, stimulated the release of cGMP from granulosa cells obtained from DES-treated, but not from eCG-treated, animals. The relative levels of CNP mRNA in granulosa cells were unaltered by either DES or eCG treatment. In contrast, CNP mRNA levels were increased more than 2-fold, but only in theca-interstitial from the eCG-treated animals. Our results indicate that CNP and NPR-B are expressed in the ovary, and their expression is responsive to hormonal treatments. Furthermore, expression of these components of the natriuretic peptide system appears to be compartmentalized, with CNP being derived from the extrafollicular compartment and acting, through NPR-B, on the granulosa cells.

摘要

利钠肽构成了一类结构相关的肽家族,已知其可调节盐和水平衡并引起血管舒张。心房钠尿肽(ANP)、脑钠尿肽(BNP)和C型钠尿肽(CNP)主要在心脏和大脑中合成,最近在女性生殖道中也被发现。在大鼠卵巢中已检测到ANP和CNP及其同源鸟苷酸环化酶受体(分别为NPR - A和NPR - B)的表达。我们之前已经表明,大鼠卵巢中利钠肽及其受体的表达似乎受发情周期调节。在本研究中,我们评估了从用雌激素类似物己烯雌酚(DES)或具有LH和FSH活性的促性腺激素马绒毛膜促性腺激素(eCG)处理的未成熟雌性大鼠获得的卵巢细胞(颗粒细胞和卵泡膜 - 间质细胞)中利钠肽系统(肽和受体)的表达。使用全细胞放射受体分析,我们发现从用DES或eCG处理的动物获取的颗粒细胞中,CNP结合增加了2倍。半定量逆转录 - 聚合酶链反应(RT - PCR)显示,来自DES或eCG处理动物的颗粒细胞中NPR - B信使核糖核酸(mRNA)转录物水平增加,这与结合增加情况良好相符。通过配体依赖性刺激环磷酸鸟苷(cGMP)释放来评估受体的活性。CNP而非ANP刺激了从DES处理但非eCG处理的动物获取的颗粒细胞中cGMP的释放。DES或eCG处理均未改变颗粒细胞中CNP mRNA的相对水平。相反,仅在eCG处理动物的卵泡膜 - 间质细胞中,CNP mRNA水平增加了2倍以上。我们的结果表明,CNP和NPR - B在卵巢中表达,并且它们的表达对激素处理有反应。此外,利钠肽系统这些成分的表达似乎是分隔的,CNP来自卵泡外区域,并通过NPR - B作用于颗粒细胞。

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