Chun S Y, Billig H, Tilly J L, Furuta I, Tsafriri A, Hsueh A J
Department of Gynecology and Obstetrics, Stanford University School of Medicine, California 94305-5317.
Endocrinology. 1994 Nov;135(5):1845-53. doi: 10.1210/endo.135.5.7525255.
Although the majority of ovarian follicles undergo atresia through a mechanism involving apoptotic cell death, in vivo studies concerning the hormonal regulation of atresia have been difficult due to the presence of heterogeneous population of follicles in the ovary. In the present study, the regulation of follicle apoptosis by gonadotropins, insulin-like growth factor I (IGF-I), and IGF-binding protein 3 (IGFBP-3) was examined using a serum-free culture of preovulatory follicles. Immature rats at 26 days of age received a single dose of PMSG. Two days later, the largest preovulatory follicles were collected for in vitro culture with or without hormones. After 24 h of culture, follicular apoptotic DNA fragmentation was analyzed by autoradiography of size-fractionated DNA labeled at 3'-ends by [32P]dideoxy-ATP. A spontaneous increase in apoptotic DNA fragmentation occurred after 24 h of culture in the absence of hormones, whereas treatment with human CG (hCG) or FSH suppressed follicular apoptosis in a dose-dependent manner, with 0.1 microgram/ml causing maximal suppression by 60-62%. Cotreatment with hCG and FSH had no additional effect. Like gonadotropins, treatment with IGF-I and insulin also suppressed the spontaneous onset of apoptosis, with IGF-I being more effective than insulin. Cotreatment with IGFBP-3 and hCG dose-dependently reversed the suppressive effect of hCG on apoptosis by 42%, suggesting a mediatory role of endogenously produced IGF-I. The addition of IGFBP-3 also blocked the suppressive action of IGF-I by 49%, whereas it did not affect the suppressive action of an IGF-I agonist or insulin. Treatment with IGFBP-3 alone had no effect on apoptotic DNA fragmentation. Estrogen and progesterone production by the cultured follicles were also analyzed by RIA. Gonadotropin treatment resulted in a marked stimulation of the production of both steroid productions. In contrast, treatment with IGF-I caused a small increase in estrogen but decreased progesterone production. Although treatment with IGFBP-3 alone decreased both estrogen and progesterone production, cotreatment with IGFBP-3 and hCG resulted in a slight decrease in estrogen production but an increase in progesterone production. Furthermore, IGFBP-3 did not affect IGF-I action on steroid production. To further substantiate the hypothesis that IGFBP-3 blocks the suppressive effect of hCG on apoptosis by neutralizing endogenously produced IGF-I, solution hybridization analysis was performed, and hCG treatment was shown to increase IGF-I messenger RNA levels in cultured follicles by 1.9-fold.(ABSTRACT TRUNCATED AT 400 WORDS)
尽管大多数卵巢卵泡通过涉及凋亡性细胞死亡的机制发生闭锁,但由于卵巢中卵泡群体的异质性,关于闭锁的激素调节的体内研究一直很困难。在本研究中,使用排卵前卵泡的无血清培养来检测促性腺激素、胰岛素样生长因子I(IGF-I)和IGF结合蛋白3(IGFBP-3)对卵泡凋亡的调节。26日龄的未成熟大鼠接受单剂量的孕马血清促性腺激素(PMSG)。两天后,收集最大的排卵前卵泡进行有或无激素的体外培养。培养24小时后,通过对用[32P]双脱氧三磷酸腺苷在3'末端标记的大小分级DNA进行放射自显影分析卵泡凋亡性DNA片段化。在无激素培养24小时后,凋亡性DNA片段化自发增加,而用人绒毛膜促性腺激素(hCG)或促卵泡激素(FSH)处理以剂量依赖性方式抑制卵泡凋亡,0.1微克/毫升时抑制作用最大,可达60 - 62%。hCG和FSH联合处理没有额外作用。与促性腺激素一样,用IGF-I和胰岛素处理也抑制凋亡的自发发生,IGF-I比胰岛素更有效。IGFBP-3与hCG联合处理以剂量依赖性方式使hCG对凋亡的抑制作用逆转42%,表明内源性产生的IGF-I起介导作用。添加IGFBP-3也使IGF-I的抑制作用阻断49%,而它不影响IGF-I激动剂或胰岛素的抑制作用。单独用IGFBP-3处理对凋亡性DNA片段化没有影响。还用放射免疫分析法分析了培养卵泡的雌激素和孕酮生成。促性腺激素处理导致两种类固醇生成均显著增加。相反,用IGF-I处理使雌激素略有增加,但孕酮生成减少。尽管单独用IGFBP-3处理使雌激素和孕酮生成均减少,但IGFBP-3与hCG联合处理导致雌激素生成略有减少,但孕酮生成增加。此外,IGFBP-3不影响IGF-I对类固醇生成的作用。为了进一步证实IGFBP-3通过中和内源性产生的IGF-I来阻断hCG对凋亡的抑制作用这一假说,进行了溶液杂交分析,结果显示hCG处理使培养卵泡中的IGF-I信使核糖核酸水平增加1.9倍。(摘要截断于400字)
