COUP-TFII对雌激素受体α(ERα)活性的抑制作用对于成功着床和蜕膜化至关重要。
Suppression of ERalpha activity by COUP-TFII is essential for successful implantation and decidualization.
作者信息
Lee Dong-Kee, Kurihara Isao, Jeong Jae-Wook, Lydon John P, DeMayo Francesco J, Tsai Ming-Jer, Tsai Sophia Y
机构信息
Department of Molecular and Cellular Biology, Baylor College of Medicine, One Baylor Plaza, Houston, Texas 77030, USA.
出版信息
Mol Endocrinol. 2010 May;24(5):930-40. doi: 10.1210/me.2009-0531. Epub 2010 Mar 10.
Synchrony between embryo competency and uterine receptivity is essential for successful implantation. Mice with ablation of chicken ovalbumin upstream promoter-transcription factor II (COUP-TFII) in the uterus (PR(Cre/+);COUP-TFII(flox/flox)) exhibit implantation defects and increased estrogen receptor (ER)alpha activity in the luminal epithelium, suggesting high ERalpha activity may disrupt the window of uterine receptivity. To determine whether increased ERalpha activity in the PR(Cre/+);COUP-TFII(flox/flox) uterus is the cause of defective implantation, we assessed whether inhibition of ERalpha activity could rescue the PR(Cre/+);COUP-TFII(flox/flox) uterine implantation defect. ICI 182,780 (ICI), a pure ERalpha antagonist, was administered to PR(Cre/+);COUP-TFII(flox/flox) mutant and COUP-TFII(flox/flox) control mice during the receptive period, and the number of implantation sites was examined. COUP-TFII(flox/flox) control mice treated with oil or ICI showed the normal number of implantation sites. As expected, no implantation sites were observed in PR(Cre/+);COUP-TFII(flox/flox) mutant mice treated with oil, consistent with previous observations. In contrast, implantation sites were greatly increased in ICI-treated PR(Cre/+);COUP-TFII(flox/flox) mutant mice, albeit at a reduced number in comparison with the control mice. ICI treatment was also able to restore the expression of Wnt4 and bone morphogenetic protein 2, important for endometrial decidualization in the PR(Cre/+);COUP-TFII(flox/flox) mutant mice. To confirm that the rescue of embryo attachment and decidualization is a consequence of a reduced ERalpha activity upon ICI treatment, we showed a reduction of the expression of ERalpha target genes in PR(Cre/+);COUP-TFII(flox/flox) mutant mice. Because COUP-TFII was also shown in our laboratory to be important for placentation during pregnancy, we asked whether ICI treatment could also rescue the placentation defect to allow full-term pregnancy in these mice. We found that whereas mice were born in COUP-TFII(flox/flox) control mice given ICI, no pups were born in the PR(Cre/+);COUP-TFII(flox/flox) mutant mice, suggesting that the increased ERalpha activity is not the reason for placentation defects. These results demonstrate that during the periimplantation period, COUP-TFII regulates embryo attachment and decidualization through controlling ERalpha activity. However, COUP-TFII expression is still required in the postimplantation period to facilitate placentation.
胚胎发育能力与子宫接受性之间的同步对于成功着床至关重要。子宫中鸡卵清蛋白上游启动子转录因子II(COUP-TFII)缺失的小鼠(PR(Cre/+);COUP-TFII(flox/flox))表现出着床缺陷,且腔上皮中雌激素受体(ER)α活性增加,这表明高ERα活性可能会破坏子宫接受期窗口。为了确定PR(Cre/+);COUP-TFII(flox/flox)子宫中ERα活性增加是否是着床缺陷的原因,我们评估了抑制ERα活性是否能挽救PR(Cre/+);COUP-TFII(flox/flox)子宫的着床缺陷。在接受期,将纯ERα拮抗剂ICI 182,780(ICI)给予PR(Cre/+);COUP-TFII(flox/flox)突变小鼠和COUP-TFII(flox/flox)对照小鼠,并检查着床位点的数量。用玉米油或ICI处理的COUP-TFII(flox/flox)对照小鼠的着床位点数量正常。正如预期的那样,用玉米油处理的PR(Cre/+);COUP-TFII(flox/flox)突变小鼠未观察到着床位点,这与之前的观察结果一致。相比之下,用ICI处理的PR(Cre/+);COUP-TFII(flox/flox)突变小鼠的着床位点大大增加,尽管与对照小鼠相比数量有所减少。ICI处理还能够恢复PR(Cre/+);COUP-TFII(flox/flox)突变小鼠中对子宫内膜蜕膜化很重要的Wnt4和骨形态发生蛋白2的表达。为了证实胚胎附着和蜕膜化的挽救是ICI处理后ERα活性降低的结果,我们发现PR(Cre/+);COUP-TFII(flox/flox)突变小鼠中ERα靶基因的表达降低。因为我们实验室还表明COUP-TFII对孕期胎盘形成也很重要,所以我们询问ICI处理是否也能挽救胎盘形成缺陷,以使这些小鼠能够足月妊娠。我们发现,尽管给予ICI的COUP-TFII(flox/flox)对照小鼠产仔,但PR(Cre/+);COUP-TFII(flox/flox)突变小鼠没有产仔,这表明ERα活性增加不是胎盘形成缺陷的原因。这些结果表明,在着床前期,COUP-TFII通过控制ERα活性来调节胚胎附着和蜕膜化。然而,在着床后期仍需要COUP-TFII表达以促进胎盘形成。
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