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骨形态发生蛋白在促卵泡激素合成中的新作用。

A novel role for bone morphogenetic proteins in the synthesis of follicle-stimulating hormone.

作者信息

Huang H J, Wu J C, Su P, Zhirnov O, Miller W L

机构信息

Department of Biochemistry, North Carolina State University, Raleigh 27695-7622, USA.

出版信息

Endocrinology. 2001 Jun;142(6):2275-83. doi: 10.1210/endo.142.6.8159.

Abstract

FSH is produced in pituitary gonadotropes as an alpha/beta heterodimer, and synthesis of the beta-subunit is the rate-limiting step in overall FSH production. Synthesis of FSHbeta can be regulated by activin and inhibin, both of which are members of the transforming growth factor-beta superfamily. Bone morphogenetic proteins (BMPs) also belong to the transforming growth factor-beta family and are multifunctional growth factors involved in many aspects of tissue development and morphogenesis, including regulation of FSH action in the ovary. Here we report a novel function for BMP-7 and BMP-6 in regulating FSH synthesis in the pituitary. Using primary pituitary cell cultures derived from transgenic mice that carry the ovine FSHbeta promoter linked to a luciferase reporter gene (oFSHbetaLuc), BMP-7 or BMP-6 was found to stimulate oFSHbetaLuc expression by 6-fold. Transient expression of the oFSHbetaLuc in a transformed gonadotrope cell line, LbetaT2, was induced 4-fold by BMP-7 or BMP-6 treatment. More importantly, BMP-7 and BMP-6 increased endogenous FSH secretion by 10- and 14-fold, respectively, from LbetaT2 cells, demonstrating for the first time that a functional signaling BMP system is present in gonadotropes. Two bioneutralizing antibodies to BMP-7, which cross-react with BMP-6, but not with activin A, decreased basal oFSHbetaLuc expression and FSH secretion from transgenic mouse pituitary cultures by 83-88% and 47-48%, respectively, suggesting an autocrine or paracrine role for BMP-7 or BMP-6 in FSH synthesis. Neither bioneutralizing antibody to activin A or activin B decreased basal oFSHbetaLuc expression or mouse FSH secretion significantly. Dose-dependent inhibition of FSH synthesis by anti-BMP7 was also observed in rat and sheep pituitary cultures. These results combined with the fact that the messenger RNAs for BMP-7 and BMP-6 were detected in mouse pituitaries and LbetaT2 cells indicate that BMP-7 and/or BMP-6 can function as FSH stimulators and may be significant physiological factors maintaining basal FSH expression in vivo.

摘要

促卵泡激素(FSH)由垂体促性腺细胞产生,为α/β异二聚体,β亚基的合成是FSH整体产生过程中的限速步骤。FSHβ的合成可受激活素和抑制素调节,二者均为转化生长因子-β超家族成员。骨形态发生蛋白(BMPs)也属于转化生长因子-β家族,是多功能生长因子,参与组织发育和形态发生的多个方面,包括对卵巢中FSH作用的调节。在此,我们报告BMP - 7和BMP - 6在调节垂体FSH合成方面的新功能。利用源自携带与荧光素酶报告基因相连的绵羊FSHβ启动子的转基因小鼠的原代垂体细胞培养物,发现BMP - 7或BMP - 6可使绵羊FSHβ荧光素酶(oFSHβLuc)表达增加6倍。在转化的促性腺细胞系LβT2中,BMP - 7或BMP - 6处理可使oFSHβLuc的瞬时表达增加4倍。更重要的是,BMP - 7和BMP - 6分别使LβT2细胞的内源性FSH分泌增加10倍和14倍,首次证明促性腺细胞中存在功能性的BMP信号系统。两种与BMP - 7交叉反应但不与激活素A交叉反应的BMP - 7生物中和抗体,分别使转基因小鼠垂体培养物中的基础oFSHβLuc表达和FSH分泌降低83% - 88%和47% - 48%,提示BMP - 7或BMP - 6在FSH合成中具有自分泌或旁分泌作用。激活素A或激活素B的生物中和抗体均未显著降低基础oFSHβLuc表达或小鼠FSH分泌。在大鼠和绵羊垂体培养物中也观察到抗BMP7对FSH合成的剂量依赖性抑制。这些结果与在小鼠垂体和LβT2细胞中检测到BMP - 7和BMP - 6的信使核糖核酸这一事实相结合,表明BMP - 7和/或BMP - 6可作为FSH刺激因子,可能是体内维持基础FSH表达的重要生理因子。

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