Flutamide induces uterus and ovary damage in the mouse via apoptosis and excessive autophagy of cells following triggering of the unfolded protein response

氟他胺 卵巢 内分泌学 子宫 后代 内科学 子宫内 自噬 未折叠蛋白反应 内质网 生物 细胞凋亡 男科 发情周期 医学 怀孕 细胞生物学 胎儿 癌症 雄激素受体 生物化学 遗传学 前列腺癌
作者
Haiming Yu,Xiaoqing Zhou,Yujing Zhang,Kexin Wen,Zhengli Yan,Hu Fu,Yongfei Zhu
出处
期刊:Reproduction, Fertility and Development [CSIRO Publishing]
卷期号:33 (7): 466-475 被引量:2
标识
DOI:10.1071/rd20287
摘要

Intrauterine exposure to flutamide not only causes abnormal development of the reproductive organs in male offspring, but also damages ovaries and uteri. The unfolded protein response (UPR) is believed to play an important role in embryo development and teratogenic processes. In the present study, pregnant mice were administered either flutamide (300mg kg-1 day-1, p.o.) on an equivalent volume of soybean oil (control) on Days 12-18 of gestation. Eight weeks after birth, female offspring in the flutamide-treated group had a lower bodyweight and lower ovarian and uterine weights, but there was no significant difference in uterine and ovarian weights normalised by bodyweight between the flutamide-treated and control groups. Furthermore, histopathological changes were observed in all uteri and ovaries in the flutamide-treated group, with fewer and less-developed follicles in the ovaries. In both the uteri and ovaries, flutamide increased the expression of UPR members, although the expression of cell cycle-related genes remained unchanged compared with the control group. Flutamide increased the expression of all autophagy- and apoptosis-related genes evaluated in the uterus, as well as some in the ovary. The results suggest that the in utero exposure of mice to flutamide may contribute to uterine and ovarian damage in the offspring, with endoplasmic reticulum stress possibly triggered by the UPR leading to the induction of excessive autophagy and apoptosis.
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