Pregnancy involving intricate tissue transformations governed by the progesterone hormone (P4). P4 signaling via P4 receptors (PRs) is vital for endometrial receptivity, decidualization, myometrial quiescence, and labor initiation. This study explored the role of TCF23 as a downstream target of PR during pregnancy. TCF23 was found to be expressed in female reproductive organs, predominantly in uterine stromal and smooth muscle cells. Tcf23 expression was high during midgestation and was specifically regulated by P4, but not estrogen. The Tcf23 knockout (KO) mouse was generated and analyzed. Female KO mice aged 4-6âmonths exhibited subfertility, reduced litter size, and defective parturition. Uterine histology revealed disrupted myometrial structure, altered collagen organization, and disarrayed smooth muscle sheets at the conceptus sites of KO mice. RNA-Seq analysis of KO myometrium revealed dysregulation of genes associated with cell adhesion and extracellular matrix organization. TCF23 potentially modulates TCF12 activity to mediate cell-cell adhesion and matrix modulation in smooth muscle cells. Overall, TCF23 deficiency leads to impaired myometrial remodeling, causing parturition delay and fetal demise. This study sheds light on the critical role of TCF23 as a dowstream mediator of PR in uterine remodeling, reflecting the importance of cell-cell communication and matrix dynamics in myometrial activation and parturition.
Transcription Factor 23 is an Essential Determinant of Murine Term Parturition.
转录因子 23 是小鼠足月分娩的重要决定因素
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作者:Minisy Fatma M, Shawki Hossam H, Fujita Tsubasa, Moustafa Ahmed M, Sener Rumeysa, Nishio Youske, Shimada Issei S, Saitoh Shinji, Sugiura-Ogasawara Mayumi, Oishi Hisashi
| 期刊: | Molecular and Cellular Biology | 影响因子: | 2.700 |
| 时间: | 2024 | 起止号: | 2024;44(8):316-333 |
| doi: | 10.1080/10985549.2024.2376146 | 研究方向: | 其它 |
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