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转录因子 SIX3 和 VAX1 是雌性小鼠视交叉上核生物钟输出和生育所必需的。

The transcription factors SIX3 and VAX1 are required for suprachiasmatic nucleus circadian output and fertility in female mice.

机构信息

Department of Obstetrics, Gynecology, and Reproductive Sciences and Center for Reproductive Science and Medicine, University of California, San Diego, La Jolla, CA, USA.

Center for Circadian Biology, University of California, San Diego, La Jolla, CA, USA.

出版信息

J Neurosci Res. 2021 Oct;99(10):2625-2645. doi: 10.1002/jnr.24864. Epub 2021 Jul 2.

Abstract

The homeodomain transcription factors sine oculis homeobox 3 (Six3) and ventral anterior homeobox 1 (Vax1) are required for brain development. Their expression in specific brain areas is maintained in adulthood, where their functions are poorly understood. To identify the roles of Six3 and Vax1 in neurons, we conditionally deleted each gene using Synapsin , a promoter targeting maturing neurons, and generated Six3 and Vax1 mice. Six3 and Vax1 females, but not males, had reduced fertility, due to impairment of the luteinizing hormone (LH) surge driving ovulation. In nocturnal rodents, the LH surge requires a precise timing signal from the brain's circadian pacemaker, the suprachiasmatic nucleus (SCN), near the time of activity onset. Indeed, both Six3 and Vax1 females had impaired rhythmic SCN output, which was associated with weakened Period 2 molecular clock function in both Six3 and Vax1 mice. These impairments were associated with a reduction of the SCN neuropeptide vasoactive intestinal peptide in Vax1 mice and a modest weakening of SCN timekeeping function in both Six3 and Vax1 mice. Changes in SCN function were associated with mistimed peak PER2::LUC expression in the SCN and pituitary in both Six3 and Vax1 females. Interestingly, Six3 ovaries presented reduced sensitivity to LH, causing reduced ovulation during superovulation. In conclusion, we have identified novel roles of the homeodomain transcription factors SIX3 and VAX1 in neurons, where they are required for proper molecular circadian clock function, SCN rhythmic output, and female fertility.

摘要

同源结构域转录因子 sine oculis 同源盒 3(Six3)和腹侧前同源盒 1(Vax1)是脑发育所必需的。它们在特定脑区的表达在成年期得以维持,但它们的功能尚不清楚。为了确定 Six3 和 Vax1 在神经元中的作用,我们使用 Synapsin(一种靶向成熟神经元的启动子)条件性删除了每个基因,并生成了 Six3 和 Vax1 小鼠。Six3 和 Vax1 雌性小鼠而非雄性小鼠的生育能力降低,原因是促黄体激素(LH)激增驱动排卵的能力受损。在夜间活动的啮齿动物中,LH 激增需要来自大脑生物钟起搏器视交叉上核(SCN)的精确时间信号,接近活动开始的时间。事实上,Six3 和 Vax1 雌性小鼠的 SCN 输出节律都受到了损害,这与 Six3 和 Vax1 小鼠中 Period 2 分子时钟功能的减弱有关。这些损伤与 Vax1 小鼠 SCN 神经肽血管活性肠肽的减少以及 Six3 和 Vax1 小鼠 SCN 计时功能的适度减弱有关。SCN 功能的变化与 Six3 和 Vax1 雌性小鼠的 SCN 和垂体中 PER2::LUC 表达的峰值时间错误有关。有趣的是,Six3 卵巢对 LH 的敏感性降低,导致超排卵期间排卵减少。总之,我们已经确定了同源结构域转录因子 SIX3 和 VAX1 在神经元中的新作用,它们是正确的分子生物钟功能、SCN 节律性输出和雌性生育能力所必需的。

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