来曲唑、丙酸睾酮和高脂饮食诱导的多囊卵巢综合征大鼠模型的特征
Characteristics of polycystic ovary syndrome rat models induced by letrozole, testosterone propionate and high-fat diets.
作者信息
Hu Runan, Huang Yanjing, Liu Zhuo, Dong Haoxu, Ma Wenwen, Song Kunkun, Xu Xiaohu, Wu Xiao, Geng Yuli, Li Fan, Zhang Mingmin, Song Yufan
机构信息
Institute of Integrated Traditional Chinese and Western Medicine, Tongji Hospital, Tongji Medical College, Huazhong University of Science and Technology, Wuhan, China.
Department of Integrated Traditional Chinese and Western Medicine, Tongji Hospital, Tongji Medical College, Huazhong University of Science and Technology, Wuhan, China.
出版信息
Reprod Biomed Online. 2025 Jan;50(1):104296. doi: 10.1016/j.rbmo.2024.104296. Epub 2024 May 30.
RESEARCH QUESTION
What are the long-term effects of different models of polycystic ovary syndrome (PCOS), and which model could be used in future research?
DESIGN
PCOS models induced by letrozole, letrozole plus high-fat diet (LE+HFD), testosterone propionate (TP) or testosterone propionate plus HFD (TP+HFD) were established in rats. Body weight, energy intake, blood glucose, sex hormone concentrations, lipid profiles and the oestrus cycle were observed. Histology of ovaries, large intestine and fat was displayed. Protein and mRNA levels relating to hormone synthesis, oocyte maturation, the gut barrier, lipid metabolism and inflammation were evaluated using western blotting, immunohistochemistry and PCR. The composition of the microbial community was measured using 16S RNA sequencing.
RESULTS
Letrozole treatment induced hyperandrogenaemia, polycystic ovarian morphology, a disrupted oestrus cycle and impaired ovarian function, which could be restored within 42 days. Concurrently, letrozole disturbed glucose, fat, and energy metabolism, affected the inflammatory state and compromised intestinal homeostasis. HFD could amplify the disturbances in the metabolism and intestinal microenvironment, and the pituitary-ovarian axis was more efficiently and consistently affected by testosterone propionate. Testosterone propionate and TP+HFD treatment also disturbed the intestinal microenvironment. Although the metabolic effects of testosterone propionate were not as profound as those of letrozole, they were enhanced by HFD.
CONCLUSIONS
Letrozole is useful for studies on metabolic disturbances in PCOS, and LE+HFD treatment is suitable for investigations on PCOS metabolic abnormalities and the gut-PCOS link. Testosterone propionate injection is appropriate for studying reproductive abnormalities in PCOS, while TP+HFD treatment is the most comprehensive for studying PCOS reproductive abnormalities, metabolic disturbances and the gut-PCOS link.
研究问题
不同多囊卵巢综合征(PCOS)模型的长期影响是什么,哪种模型可用于未来的研究?
设计
在大鼠中建立了由来曲唑、来曲唑加高脂饮食(LE+HFD)、丙酸睾酮(TP)或丙酸睾酮加HFD(TP+HFD)诱导的PCOS模型。观察体重、能量摄入、血糖、性激素浓度、血脂谱和发情周期。展示卵巢、大肠和脂肪的组织学。使用蛋白质印迹法、免疫组织化学和PCR评估与激素合成、卵母细胞成熟、肠道屏障、脂质代谢和炎症相关的蛋白质和mRNA水平。使用16S RNA测序测量微生物群落的组成。
结果
来曲唑治疗导致高雄激素血症、多囊卵巢形态、发情周期紊乱和卵巢功能受损,这些在42天内可恢复。同时,来曲唑扰乱了葡萄糖、脂肪和能量代谢,影响炎症状态并损害肠道稳态。HFD可放大代谢和肠道微环境的紊乱,垂体-卵巢轴受丙酸睾酮的影响更有效且更一致。丙酸睾酮和TP+HFD治疗也扰乱了肠道微环境。尽管丙酸睾酮的代谢作用不如来曲唑那样显著,但HFD可增强其作用。
结论
来曲唑可用于PCOS代谢紊乱的研究,LE+HFD治疗适用于PCOS代谢异常和肠道-PCOS联系的研究。注射丙酸睾酮适用于研究PCOS的生殖异常,而TP+HFD治疗对于研究PCOS生殖异常、代谢紊乱和肠道-PCOS联系最为全面。
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