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首页> 外文期刊>Endocrine Research >cAMP-induced apoptosis in granulosa cells is associated with up-regulation of P53 and bax and down-regulation of clusterin.
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cAMP-induced apoptosis in granulosa cells is associated with up-regulation of P53 and bax and down-regulation of clusterin.

机译:cAMP诱导的颗粒细胞凋亡与P53和bax的上调以及簇蛋白的下调有关。

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摘要

Evidence indicates that cAMP induces apoptosis in granulosa cells of rat and human ovary. The mechanism by which cAMP induces apoptosis is not known. This study was carried out to evaluate changes in expression of cell death promoters, P53 and bax, and cell death repressor, bcl-2, in cAMP-treated granulosa cells. Treatment of granulosa cells with forskolin (FSK), or 8-bromo-cAMP induced apoptosis as evidenced by internucleosomal DNA fragmentation and chromatin condensation as revealed by gel electrophoresis and fluorescent DAPI staining, respectively. The apoptotic effect of cAMP was accompanied by an increase in the expression of P53 and bax proteins as evaluated by Western blot and immunocytochemistry. No change in bcl-2 protein level was observed in cAMP-treated granulosa cells as compared to control. These data suggest that cAMP may activate apoptosis in granulosa cells by shifting the ratio of the death promoter to death repressor genes via alteration of P53 and bax expression. cAMP was also shown to inhibit gene expression of clusterin, an apoptosis-associated protein, suggesting a role for this protein in cAMP-induced apoptosis in granulosa cells. The data of the present study provide a basis for future studies to elucidate the molecular mechanism of follicular atresia and regulation of apoptotic cell death in ovarian follicles.
机译:有证据表明,cAMP诱导大鼠和人卵巢颗粒细胞的凋亡。 cAMP诱导细胞凋亡的机制尚不清楚。进行这项研究以评估在cAMP处理的颗粒细胞中细胞死亡启动子P53和bax以及细胞死亡阻抑物bcl-2的表达变化。分别用凝胶电泳和荧光DAPI染色显示,用福司可林(FSK)或8-bromo-cAMP处理颗粒细胞可诱导凋亡,这一点可通过核小体间DNA片段化和染色质浓缩来证明。通过蛋白质印迹和免疫细胞化学评估,cAMP的凋亡作用伴随着P53和bax蛋白表达的增加。与对照相比,在经cAMP处理的颗粒细胞中未观察到bcl-2蛋白水平的变化。这些数据表明,cAMP可能通过改变P53和bax表达来改变死亡启动子与死亡抑制基因的比例,从而激活颗粒细胞的凋亡。还显示了cAMP抑制簇蛋白(一种凋亡相关蛋白)的基因表达,表明该蛋白在cAMP诱导的颗粒细胞凋亡中发挥了作用。本研究的数据为进一步研究阐明卵泡闭锁的分子机制和调节卵巢卵泡中凋亡细胞死亡提供了基础。

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