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Cyclic AMP-elevating Agents Promote Cumulus Cell Survival and Hyaluronan Matrix Stability, Thereby Prolonging the Time of Mouse Oocyte Fertilizability.

机译:环状AMP增强剂可促进积卵细胞存活和透明质酸基质稳定性,从而延长小鼠卵母细胞的受精时间。

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摘要

Cumulus cells sustain the development and fertilization of the mammalian oocyte. These cells are retained around the oocyte by a hyaluronan-rich extracellular matrix synthesized before ovulation, a process called cumulus cell-oocyte complex (COC) expansion. Hyaluronan release and dispersion of the cumulus cells progressively occur after ovulation, paralleling the decline of oocyte fertilization. We show here that, in mice, postovulatory changes of matrix are temporally correlated to cumulus cell death. Cumulus cell apoptosis and matrix disassembly also occurred in ovulated COCs cultured in vitro. COCs expanded in vitro with FSH or EGF underwent the same changes, whereas those expanded with 8-bromo-adenosine-3',5'-cyclic monophosphate (8-Br-cAMP) maintained integrity for a longer time. It is noteworthy that 8-Br-cAMP treatment was also effective on ovulated COCs cultured in vitro, prolonging the vitality of the cumulus cells and the stability of the matrix from a few hours to >2 days. Stimulation of endogenous adenylate cyclase with forskolin or inhibition of phosphodiesterase with rolipram produced similar effects. The treatment with selective cAMP analogues suggests that the effects of cAMP elevation are exerted through an EPAC-independent, PKA type II-dependent signaling pathway, probably acting at the post-transcriptional level. Finally, overnight culture of ovulated COCs with 8-Br-cAMP significantly counteracted the decrease of fertilization rate, doubling the number of fertilized oocytes compared with control conditions. In conclusion, these studies suggest that cAMP-elevating agents prevent cumulus cell senescence and allow them to continue to exert beneficial effects on oocyte and sperm, thereby extending in vitro the time frame of oocyte fertilizability.
机译:累积细胞维持哺乳动物卵母细胞的发育和受精。这些细胞通过在排卵前合成的富含透明质酸的细胞外基质保留在卵母细胞周围,这一过程称为卵丘细胞-卵母细胞复合体(COC)扩展。透明质酸的释放和卵丘细胞的分散在排卵后逐渐发生,与卵母细胞受精的下降平行。我们在这里显示,在小鼠中,排卵后基质的变化在时间上与卵丘细胞死亡相关。体外培养的排卵COCs中也发生积液细胞凋亡和基质分解。用FSH或EGF体外扩增的COC经历了相同的变化,而用8-溴腺苷3',5'-环一磷酸酯(8-Br-cAMP)扩增的COC保持了更长的完整性。值得注意的是,8-Br-cAMP处理对体外培养的排卵COC也有效,将卵丘细胞的活力和基质的稳定性从数小时延长至> 2天。用福司可林刺激内源性腺苷酸环化酶或用咯利普兰抑制磷酸二酯酶产生了相似的效果。选择性cAMP类似物的治疗表明,cAMP升高的影响是通过EPAC独立的,PKA II型依赖的信号传导途径发挥的,可能在转录后水平起作用。最后,与8-Br-cAMP一起排卵的COC过夜培养显着抵消了受精率的下降,与对照条件相比,受精卵的数量增加了一倍。总之,这些研究表明,cAMP增强剂可防止卵丘细胞衰老,并使它们继续对卵母细胞和精子产生有益作用,从而在体外延长卵母细胞受精的时间范围。

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