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人生长调节素C/胰岛素样生长因子I对卵巢细胞的营养作用:猪颗粒细胞的体外研究

Trophic actions of human somatomedin C/insulin-like growth factor I on ovarian cells: in vitro studies with swine granulosa cells.

作者信息

Veldhuis J D, Furlanetto R W

出版信息

Endocrinology. 1985 Apr;116(4):1235-42. doi: 10.1210/endo-116-4-1235.

Abstract

We have investigated the responsiveness of swine granulosa cells to somatomedin C/insulin-like growth factor I (IGF I) under serum-free conditions in vitro. Somatomedin C/IGF I (greater than 80% pure) exerted dose-dependent stimulatory effects on the production of progesterone and its reduced metabolite, 20 alpha-hydroxypregn-4-en-3-one. A 50-fold stimulation of progesterone production could be observed after 48-96 h of hormone treatment. These effects were not mimicked by platelet-derived growth factor, epidermal growth factor, fibroblast growth factor, desoctapeptide insulin, or porcine relaxin. The stimulatory action of somatomedin C/IGF I was not attributable to changes in cell protein or DNA content or cell number and reflected enhanced steroidogenesis per se rather than simply release of stored progesterone. In addition, augmented progesterone production was accompanied by increased biosynthesis of its precursor, pregnenolone, measured in the presence of trilostane to block 3 beta-hydroxysteroid dehydrogenase activity. Moreover, somatomedin C/IGF I enhanced progesterone biosynthesis in response to a maximally effective concentration of the soluble sterol substrate for side-chain cleavage, 25-hydroxycholesterol, suggesting that somatomedin C increases the effective activity of the mitochondrial cholesterol side-chain cleavage system. The stimulatory effects of somatomedin C/IGF I were inhibited by cycloheximide and actinomycin D, indicating that protein and RNA synthesis are required for the full expression of somatomedin C's differentiative effects. The physiological importance of such trophic actions was suggested by the capacity of nanomolar concentrations of somatomedin C/IGF I to augment progesterone production further in the presence of maximally stimulating concentrations of 8-bromo-cAMP or estradiol. In addition, equilibrium competition curves and saturation analysis of [125I]somatomedin C/IGF I binding revealed high affinity [dissociation constant (Kd) approximately 0.69 nM], low capacity (0.57 pmol somatomedin C bound/mg DNA) receptor sites on swine granulosa cells. [125I]Somatomedin C/IGF I binding was highly specific in that multiplication stimulating activity, porcine insulin, desoctapeptide insulin, and insulin-receptor antisera competed only sparingly for these binding sites. In summary, human somatomedin C/IGF I exerts potent and specific differentiative effects on swine granulosa cells cultured under serum-free conditions in vitro.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

我们已经在体外无血清条件下研究了猪颗粒细胞对生长调节素C/胰岛素样生长因子I(IGF I)的反应性。生长调节素C/IGF I(纯度大于80%)对孕酮及其还原代谢产物20α-羟基孕-4-烯-3-酮的产生具有剂量依赖性刺激作用。激素处理48 - 96小时后可观察到孕酮产生有50倍的刺激作用。血小板衍生生长因子、表皮生长因子、成纤维细胞生长因子、去八肽胰岛素或猪松弛素均不能模拟这些作用。生长调节素C/IGF I的刺激作用并非归因于细胞蛋白质、DNA含量或细胞数量的变化,而是反映了类固醇生成本身的增强,而非仅仅是储存孕酮的释放。此外,孕酮产生的增加伴随着其前体孕烯醇酮生物合成的增加,这是在存在曲洛司坦以阻断3β-羟基类固醇脱氢酶活性的情况下测定的。而且,生长调节素C/IGF I能增强对侧链裂解的可溶性甾醇底物25-羟基胆固醇最大有效浓度的反应中孕酮的生物合成,这表明生长调节素C增加了线粒体胆固醇侧链裂解系统的有效活性。生长调节素C/IGF I的刺激作用被放线菌酮和放线菌素D抑制,这表明蛋白质和RNA合成是生长调节素C分化作用充分表达所必需的。纳摩尔浓度的生长调节素C/IGF I在存在最大刺激浓度的8-溴-cAMP或雌二醇时能进一步增加孕酮产生,这提示了这种营养作用的生理重要性。此外,[125I]生长调节素C/IGF I结合的平衡竞争曲线和饱和分析显示猪颗粒细胞上存在高亲和力[解离常数(Kd)约为0.69 nM]、低容量(0.57 pmol生长调节素C结合/mg DNA)的受体位点。[125I]生长调节素C/IGF I结合具有高度特异性,因为增殖刺激活性、猪胰岛素、去八肽胰岛素和胰岛素受体抗血清仅少量竞争这些结合位点。总之,人生长调节素C/IGF I对体外无血清条件下培养的猪颗粒细胞具有强大且特异的分化作用。(摘要截断于400字)

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