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转化生长因子β在颗粒细胞分化过程中调节表皮生长因子的抑制作用。

Transforming growth factor beta regulates the inhibitory actions of epidermal growth factor during granulosa cell differentiation.

作者信息

Feng P, Catt K J, Knecht M

出版信息

J Biol Chem. 1986 Oct 25;261(30):14167-70.

PMID:3095315
Abstract

The effects of transforming growth factor beta (TGF-beta) on epidermal growth factor (EGF) receptor content and EGF action were studied in cultured granulosa cells from immature diethylstilbestrol-implanted rats. During follicle-stimulating hormone (FSH)-induced differentiation in vitro, EGF receptors increased by 20-fold as measured by the binding of 125I-EGF to the intact cells. Addition of TGF-beta during the 48-h culture period amplified the stimulatory effects of FSH on EGF receptors up to 2-fold, with ED50 and maximal concentrations of 2.5 and 8 pM, respectively. Also TGF-beta alone in amounts from 1.6 to 16 pM increased EGF receptor content 4-fold. The stimulatory effects of TGF-beta were due to increased numbers of EGF receptors/cell, since the growth factor had no effect on the Kd (3-5 X 10(-11) M) of the high-affinity EGF binding site. TGF-beta action was observed within 20 h of granulosa cell culture and was maximal by 48 h of a 96-h culture. The stimulatory actions of TGF-beta in gonadotropin-induced cells were exerted through the cAMP effector system of the granulosa cell, since the growth factor also amplified the induction of EGF receptors by cholera toxin, forskolin, and 8-bromo-cAMP. The augmentation of EGF receptors by TGF-beta resulted in a parallel 2-fold increase in the inhibitory effects of EGF on FSH-induced cAMP production and luteinizing hormone receptor expression during granulosa cell development. TGF-beta did not increase granulosa cell numbers during culture although it elevated [3H]thymidine incorporation into DNA by 2-fold over that of FSH-treated cells. These results indicate that TGF-beta regulates the effects of both FSH and EGF during granulosa cell differentiation and provides evidence that ovarian function may be controlled by the combined actions of gonadotropins and multiple growth factors.

摘要

在来自未成熟己烯雌酚植入大鼠的培养颗粒细胞中,研究了转化生长因子β(TGF-β)对表皮生长因子(EGF)受体含量和EGF作用的影响。在体外促卵泡激素(FSH)诱导的分化过程中,通过125I-EGF与完整细胞的结合测定,EGF受体增加了20倍。在48小时培养期内添加TGF-β可将FSH对EGF受体的刺激作用放大至2倍,ED50和最大浓度分别为2.5和8 pM。同样,单独使用1.6至16 pM的TGF-β可使EGF受体含量增加4倍。TGF-β的刺激作用是由于每个细胞的EGF受体数量增加,因为该生长因子对高亲和力EGF结合位点的Kd(3-5×10^(-11) M)没有影响。在颗粒细胞培养20小时内观察到TGF-β的作用,在96小时培养的48小时时达到最大值。TGF-β在促性腺激素诱导的细胞中的刺激作用是通过颗粒细胞的cAMP效应系统发挥的,因为该生长因子还增强了霍乱毒素、福斯可林和8-溴-cAMP对EGF受体的诱导作用。TGF-β对EGF受体的增强导致在颗粒细胞发育过程中,EGF对FSH诱导的cAMP产生和促黄体生成素受体表达的抑制作用平行增加2倍。尽管TGF-β使[3H]胸苷掺入DNA的量比FSH处理的细胞增加了2倍,但在培养过程中它并没有增加颗粒细胞的数量。这些结果表明,TGF-β在颗粒细胞分化过程中调节FSH和EGF的作用,并提供证据表明卵巢功能可能受促性腺激素和多种生长因子的联合作用控制。

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