Conditional Deletion of Bmal1 in Ovarian Theca Cells Disrupts Ovulation in Female Mice.

IF 8.6 1区 物理与天体物理 Q1 ASTRONOMY & ASTROPHYSICS Astrophysical Journal Supplement Series Pub Date : 2016-02-01 Epub Date: 2015-12-15 DOI:10.1210/en.2015-1645
Amanda L Mereness, Zachary C Murphy, Andrew C Forrestel, Susan Butler, CheMyong Ko, JoAnne S Richards, Michael T Sellix
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引用次数: 57

Abstract

Rhythmic events in female reproductive physiology, including ovulation, are tightly controlled by the circadian timing system. The molecular clock, a feedback loop oscillator of clock gene transcription factors, dictates rhythms of gene expression in the hypothalamo-pituitary-ovarian axis. Circadian disruption due to environmental factors (eg, shift work) or genetic manipulation of the clock has negative impacts on fertility. Although the central pacemaker in the suprachiasmatic nucleus classically regulates the timing of ovulation, we have shown that this rhythm also depends on phasic sensitivity to LH. We hypothesized that this rhythm relies on clock function in a specific cellular compartment of the ovarian follicle. To test this hypothesis we generated mice with deletion of the Bmal1 locus in ovarian granulosa cells (GCs) (Granulosa Cell Bmal1 KO; GCKO) or theca cells (TCs) (Theca Cell Bmal1 KO; TCKO). Reproductive cycles, preovulatory LH secretion, ovarian morphology and behavior were not grossly altered in GCKO or TCKO mice. We detected phasic sensitivity to LH in wild-type littermate control (LC) and GCKO mice but not TCKO mice. This decline in sensitivity to LH is coincident with impaired fertility and altered patterns of LH receptor (Lhcgr) mRNA abundance in the ovary of TCKO mice. These data suggest that the TC is a pacemaker that contributes to the timing and amplitude of ovulation by modulating phasic sensitivity to LH. The TC clock may play a critical role in circadian disruption-mediated reproductive pathology and could be a target for chronobiotic management of infertility due to environmental circadian disruption and/or hormone-dependent reprogramming in women.

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卵巢癌细胞中 Bmal1 的条件性缺失会破坏雌性小鼠的排卵。
包括排卵在内的女性生殖生理节律事件受到昼夜节律计时系统的严格控制。分子时钟是时钟基因转录因子的反馈回路振荡器,决定着下丘脑-垂体-卵巢轴的基因表达节律。环境因素(如轮班工作)或基因操纵造成的昼夜节律紊乱会对生育能力产生负面影响。尽管蛛网膜上核的中央起搏器通常调节排卵时间,但我们已经证明这种节律也取决于对 LH 的相位敏感性。我们假设这种节律依赖于卵泡特定细胞区的时钟功能。为了验证这一假设,我们培育了卵巢颗粒细胞(GCs)(Granulosa Cell Bmal1 KO; GCKO)或卵巢细胞(TCs)(Theca Cell Bmal1 KO; TCKO)中Bmal1基因座缺失的小鼠。GCKO 或 TCKO 小鼠的生殖周期、排卵前 LH 分泌、卵巢形态和行为均无明显改变。我们在野生型同窝对照(LC)和 GCKO 小鼠中检测到了对 LH 的阶段性敏感性,但在 TCKO 小鼠中没有检测到。对 LH 敏感性的下降与 TCKO 小鼠生育能力受损和卵巢中 LH 受体 (Lhcgr) mRNA 丰度模式的改变相吻合。这些数据表明,TC是一个起搏器,它通过调节对LH的相位敏感性来影响排卵的时间和幅度。TC时钟可能在昼夜节律紊乱介导的生殖病理学中发挥关键作用,并可能成为慢性生物疗法治疗因环境昼夜节律紊乱和/或激素依赖性重编程导致的女性不孕症的靶点。
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来源期刊
Astrophysical Journal Supplement Series
Astrophysical Journal Supplement Series 地学天文-天文与天体物理
CiteScore
14.50
自引率
5.70%
发文量
264
审稿时长
2 months
期刊介绍: The Astrophysical Journal Supplement (ApJS) serves as an open-access journal that publishes significant articles featuring extensive data or calculations in the field of astrophysics. It also facilitates Special Issues, presenting thematically related papers simultaneously in a single volume.
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