2013.03.05�����,我院孫斐教授研究組在Mol Cell Endocrinol上發(fā)表題為“Transcriptional cooperation between p53 and NF-κB p65 regulates microRNA-224 transcription in mouse ovarian granulosa cells”文章, online
作者:梁猛��、姚桂東�����、陰棉棉�、呂明榮、田卉�、劉琳、連杰���、黃行許��、孫斐
DOI: 10.1016/j.mce.2013.02.014
MicroRNAs (miRNAs) have been indicated to play key roles in ovarian follicular development. However, little is known about how the miRNA gene expression itself is regulated in the mammalian ovary. We previously reported that miR-224 is involved in TGF-β1-mediated follicular granulosa cell (GC) growth and estradiol (E2) production by targeting Smad4. Here, the transcriptional regulation of miR-224 expression in GCs was further investigated. Our results showed that both the tumor suppressor gene p53 and NF-κB p65 subunit suppressed the TGF-β1-induced increase in pri-miR-224 expression in GCs. ChIP assays demonstrated that TGF-β1 enhanced the binding of p53 and p65 to the proximal promoter region of GABAA receptor ε subunit (miR-224 host gene). p53 and p65 transcriptionally cooperated to inactivate the GABAA receptor ε subunit promoter. In addition, p53/p65 could up-regulate Smad4 expression by inhibiting its target miR-224 in GCs which contributed, at least partially, to the effects of miR-224 and Smad4 on GC proliferation and E2 release. Our results provide new data about the interplay between transcription factors involved in GC proliferation and function by cooperatively regulating miRNA expression.
版權(quán)與免責(zé)聲明:本網(wǎng)頁的內(nèi)容由收集互聯(lián)網(wǎng)上公開發(fā)布的信息整理獲得����。目的在于傳遞信息及分享���,并不意味著贊同其觀點或證實其真實性����,也不構(gòu)成其他建議。僅提供交流平臺����,不為其版權(quán)負責(zé)。如涉及侵權(quán)�,請聯(lián)系我們及時修改或刪除。郵箱:sales@allpeptide.com