首页> 美国卫生研究院文献>Endocrinology >Activin Decoy Receptor ActRIIB:Fc Lowers FSH and Therapeutically Restores Oocyte Yield Prevents Oocyte Chromosome Misalignments and Spindle Aberrations and Increases Fertility in Midlife Female SAMP8 Mice
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Activin Decoy Receptor ActRIIB:Fc Lowers FSH and Therapeutically Restores Oocyte Yield Prevents Oocyte Chromosome Misalignments and Spindle Aberrations and Increases Fertility in Midlife Female SAMP8 Mice

机译:激活素诱饵受体ActRIIB:Fc降低FSH并治疗性恢复卵母细胞产量防止卵母细胞染色体错位和纺锤畸变并增加中年雌性SAMP8小鼠的生育力

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摘要

Women of advanced maternal age (AMA) (age ≥ 35) have increased rates of infertility, miscarriages, and trisomic pregnancies. Collectively these conditions are called “egg infertility.” A root cause of egg infertility is increased rates of oocyte aneuploidy with age. AMA women often have elevated endogenous FSH. Female senescence-accelerated mouse-prone-8 (SAMP8) has increased rates of oocyte spindle aberrations, diminished fertility, and rising endogenous FSH with age. We hypothesize that elevated FSH during the oocyte's FSH-responsive growth period is a cause of abnormalities in the meiotic spindle. We report that eggs from SAMP8 mice treated with equine chorionic gonadotropin (eCG) for the period of oocyte growth have increased chromosome and spindle misalignments. Activin is a molecule that raises FSH, and ActRIIB:Fc is an activin decoy receptor that binds and sequesters activin. We report that ActRIIB:Fc treatment of midlife SAMP8 mice for the duration of oocyte growth lowers FSH, prevents egg chromosome and spindle misalignments, and increases litter sizes. AMA patients can also have poor responsiveness to FSH stimulation. We report that although eCG lowers yields of viable oocytes, ActRIIB:Fc increases yields of viable oocytes. ActRIIB:Fc and eCG cotreatment markedly reduces yields of viable oocytes. These data are consistent with the hypothesis that elevated FSH contributes to egg aneuploidy, declining fertility, and poor ovarian response and that ActRIIB:Fc can prevent egg aneuploidy, increase fertility, and improve ovarian response. Future studies will continue to examine whether ActRIIB:Fc works via FSH and/or other pathways and whether ActRIIB:Fc can prevent aneuploidy, increase fertility, and improve stimulation responsiveness in AMA women.
机译:孕晚期(AMA)(≥35岁)的妇女不孕,流产和三体妊娠的发生率增加。这些情况统称为“卵子不育”。卵子不育症的根本原因是随着年龄的增长,卵母细胞非整倍性率增加。 AMA妇女通常内源性FSH升高。随着年龄的增长,雌性衰老加速的小鼠倾向性8(SAMP8)的卵母细胞纺锤畸变率增加,生育力降低和内源性FSH升高。我们假设卵母细胞FSH反应生长期间FSH升高是减数分裂纺锤体异常的原因。我们报告说,卵母细胞生长期间,用马绒毛膜促性腺激素(eCG)处理过的SAMP8小鼠的卵具有增加的染色体和纺锤体错位。激活素是产生FSH的分子,而ActRIIB:Fc是结合并隔离激活素的激活素诱饵受体。我们报告ActRIIB:Fc治疗中年SAMP8小鼠卵母细胞生长的持续时间降低FSH,防止卵染色体和纺锤体未对准,并增加产仔大小。 AMA患者对FSH刺激的反应也较差。我们报告,尽管eCG降低了活卵母细胞的产量,但ActRIIB:Fc增加了活卵母细胞的产量。 ActRIIB:Fc和eCG共同处理显着降低了活卵母细胞的产量。这些数据与以下假说相符:FSH升高可导致卵异倍性,生育力下降和卵巢反应差,ActRIIB:Fc可预防卵异倍性,增加生育力并改善卵巢反应。未来的研究将继续检查ActRIIB:Fc是否通过FSH和/或其他途径起作用,以及ActRIIB:Fc是否可以预防非整倍性,增加生育力并改善AMA妇女的刺激反应。

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