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健康妊娠、子痫前期及胎儿生长受限中人类胎盘过氧化物酶体增殖物激活受体δ和γ的表达

Human placental peroxisome proliferator-activated receptor delta and gamma expression in healthy pregnancy and in preeclampsia and intrauterine growth restriction.

作者信息

Rodie Vanessa A, Young Anne, Jordan Fiona, Sattar Naveed, Greer Ian A, Freeman D J

机构信息

Division of Developmental Medicine, University of Glasgow, Glasgow Royal Infirmary, Glasgow, United Kingdom.

出版信息

J Soc Gynecol Investig. 2005 Jul;12(5):320-9. doi: 10.1016/j.jsgi.2005.03.004.

DOI:10.1016/j.jsgi.2005.03.004
PMID:15979543
Abstract

OBJECTIVES

Human and animal studies have demonstrated that peroxisome proliferator-activated receptors (PPARs) are important in placental development and play key roles in metabolism and inflammation. We studied placental PPARdelta, PPARgamma, and retinoid X receptor alpha (RXRalpha) expression in healthy pregnancy and in preeclampsia (PET) and intrauterine growth restriction (IUGR).

METHODS AND RESULTS

Using immunocytochemistry, PPARdelta, PPARgamma, and RXRalpha were localized to the cyto- and syncytiotrophoblast and invading trophoblast columns in first and second trimester placentas. Third trimester placentas from healthy pregnancy, and in PET and IUGR, demonstrated PPARdelta, PPARgamma, and RXRalpha staining within the syncytium, and localization within isolated cells in the stroma. In uncomplicated pregnancies, PPARdelta mRNA expression (PPARdelta:18s ratio, third trimester median 0.43 [interquartile (IQ) range 0.26-0.52] vs first trimester 0.20 [0.00-0.26], P = .03) and PPARdelta protein expression (third trimester 3.94 [2.45-4.68] vs first trimester 1.29 [0.78-2.29] optical densitometry [OD] mm(2), P = .04) were higher in the third trimester than in the first trimester. There were no consistent differences in PPARdelta, PPARgamma, or RXRalpha mRNA and protein expression among PET or IUGR placentas and controls.

CONCLUSION

PPARdelta expression is up-regulated between the first and third trimester, indicating a role for this nuclear receptor in placental function. We found no evidence that placental PPARdelta, PPARgamma, and RXRalpha expression is changed in PET or IUGR. This suggests that changes in total placental PPAR expression are not involved in the pathophysiology of these conditions.

摘要

目的

人和动物研究已表明,过氧化物酶体增殖物激活受体(PPARs)在胎盘发育中很重要,且在代谢和炎症中起关键作用。我们研究了健康妊娠、子痫前期(PET)和胎儿生长受限(IUGR)时胎盘PPARδ、PPARγ和视黄酸X受体α(RXRα)的表达。

方法与结果

采用免疫细胞化学方法,在孕早期和孕中期胎盘的细胞滋养层、合体滋养层及侵入性滋养层柱中定位到PPARδ、PPARγ和RXRα。来自健康妊娠、PET和IUGR的孕晚期胎盘,在合体细胞内显示PPARδ、PPARγ和RXRα染色,并在间质中的单个细胞内定位。在无并发症的妊娠中,PPARδ mRNA表达(PPARδ:18s比值,孕晚期中位数为0.43 [四分位间距(IQ)范围0.26 - 0.52] 对比孕早期0.20 [0.00 - 0.26],P = 0.03)和PPARδ蛋白表达(孕晚期光密度测定 [OD] mm²为3.94 [2.45 - 4.68] 对比孕早期1.29 [0.78 - 2.29],P = 0.04)在孕晚期高于孕早期。PET或IUGR胎盘与对照之间,PPARδ、PPARγ或RXRα mRNA和蛋白表达没有一致的差异。

结论

PPARδ表达在孕早期和孕晚期之间上调,表明该核受体在胎盘功能中起作用。我们没有发现证据表明PET或IUGR时胎盘PPARδ、PPARγ和RXRα表达发生改变。这表明胎盘PPAR总表达的变化不参与这些情况的病理生理过程。

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