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雷帕霉素在顺铂体内和体外处理过程中保留原始卵泡池。

Rapamycin preserves the primordial follicle pool during cisplatin treatment in vitro and in vivo.

机构信息

Department of Reproductive Medicine Center, Sun Yat-Sen Memorial Hospital, Sun Yat-Sen University, Guangzhou, Gongdong, China.

Department of Obstetrics and Gynecology, Guangdong Provincial People's Hospital, Guangdong Academy of Medical Sciences, Guangzhou, Gongdong, China.

出版信息

Mol Reprod Dev. 2020 Apr;87(4):442-453. doi: 10.1002/mrd.23330. Epub 2020 Feb 28.

DOI:10.1002/mrd.23330
PMID:32112509
Abstract

Rapamycin has been proven to effectively inhibit the activation of primordial follicles while cisplatin-induced the loss of primordial follicles due to the over-activation of the primordial follicle stockpile. Whether rapamycin could inhibit the loss of primordial follicles induced by cisplatin is still unknown. The ovaries of neonatal Sprague Dawley rats were cultured in vitro in different doses of rapamycin (0.08, 0.16, and 0.32 μg/ml) and cisplatin (0.1, 0.4, and 0.8 μg/ml). The immature BALB/c mice were administered cisplatin with or without rapamycin by intraperitoneal injection. Ovaries were collected to analyze the histomorphology, the messenger RNA (mRNA) expression of anti-Mullerian hormone (AMH), growth differentiation factor 9 (GDF9), and bone morphogenetic protein 15 (BMP15) and the expression of key proteins of mammalian target of rapamycin (mTOR) pathway. Growing follicle counts of ovaries cultured in vitro in the R0.16 and R0.32 groups were decreased and the ratio of growing to primordial follicles was also decreased in a dose-dependent manner. In the C0.8 group, growing follicles were decreased compared with the other groups while the ratio was substantially increased in the C0.4 and C0.8 group. Co-treatment attenuated primordial follicle loss and reduced the upregulated ratio induced by cisplatin. Ovarian follicle dynamics in vivo was consistent with the in vitro results. Primordial follicles counts were statistically increased and the ratio was reduced in the rapamycin group compared with the control group. Primordial follicle counts were dramatically reduced in the cisplatin group whereas co-treatment with rapamycin slightly recovered its counts. There was no obvious difference in the number of growing follicles between the cisplatin group and other groups. The ratio was significantly increased in cisplatin-treated mice whereas decreased in the co-treatment group. The apoptosis rate of antral follicles in cisplatin-treated mice was higher than the other groups while the apoptosis rate was decreased in the co-treatment group in vivo. Compared with the control and rapamycin group, the mRNA expression of AMH, GDF9, and BMP15 were downregulated in the cisplatin group. The co-treatment group recovered the mRNA expression of BMP15. In addition, the expression of key protein of mTOR pathway rpS6 and its phosphorylated forms were increased in the cisplatin-treated group while co-treatment decreased their expression. Rapamycin attenuated the loss of primordial follicles induced by cisplatin through the inhibitory effect of rapamycin on the mTOR pathway. These results suggest that rapamycin may be an effective drug for the protection of ovarian function during chemotherapy.

摘要

雷帕霉素已被证明可有效抑制原始卵泡的激活,而顺铂则通过过度激活原始卵泡储备导致原始卵泡丢失。雷帕霉素是否能抑制顺铂诱导的原始卵泡丢失尚不清楚。将新生 Sprague Dawley 大鼠的卵巢在不同剂量的雷帕霉素(0.08、0.16 和 0.32μg/ml)和顺铂(0.1、0.4 和 0.8μg/ml)中进行体外培养。通过腹腔注射向不成熟的 BALB/c 小鼠给予顺铂和/或雷帕霉素。收集卵巢分析组织形态学、抗苗勒管激素(AMH)、生长分化因子 9(GDF9)和骨形态发生蛋白 15(BMP15)的信使 RNA(mRNA)表达以及哺乳动物雷帕霉素靶蛋白(mTOR)通路的关键蛋白的表达。体外培养的 R0.16 和 R0.32 组的生长卵泡计数减少,生长卵泡与原始卵泡的比例也呈剂量依赖性下降。与其他组相比,C0.8 组的生长卵泡减少,而 C0.4 和 C0.8 组的比例显著增加。共同处理可减轻顺铂诱导的原始卵泡丢失并降低上调比例。体内卵巢卵泡动力学与体外结果一致。与对照组相比,雷帕霉素组的原始卵泡计数增加,比例降低。顺铂组的原始卵泡计数显著减少,而雷帕霉素共同处理组的原始卵泡计数略有恢复。与顺铂组相比,其他组的生长卵泡数量无明显差异。顺铂处理组的比例显著增加,而共同处理组的比例降低。顺铂处理组窦前卵泡的凋亡率高于其他组,而共同处理组体内的凋亡率降低。与对照组和雷帕霉素组相比,顺铂组的 AMH、GDF9 和 BMP15 的 mRNA 表达下调。共同处理组恢复了 BMP15 的 mRNA 表达。此外,顺铂处理组 mTOR 通路关键蛋白 rpS6 及其磷酸化形式的表达增加,而共同处理则降低了其表达。雷帕霉素通过抑制 mTOR 通路抑制顺铂诱导的原始卵泡丢失。这些结果表明,雷帕霉素可能是化疗期间保护卵巢功能的有效药物。

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