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孕期母亲肥胖对人体铁状态、胎盘转铁蛋白受体表达及铁调素表达的影响。

The impact of maternal obesity on iron status, placental transferrin receptor expression and hepcidin expression in human pregnancy.

作者信息

Garcia-Valdes L, Campoy C, Hayes H, Florido J, Rusanova I, Miranda M T, McArdle H J

机构信息

1] The Rowett Institute of Nutrition and Health, University of Aberdeen, Bucksburn, Aberdeen, UK [2] Department of Paediatrics, School of Medicine, University of Granada, Granada, Spain.

Department of Paediatrics, School of Medicine, University of Granada, Granada, Spain.

出版信息

Int J Obes (Lond). 2015 Apr;39(4):571-8. doi: 10.1038/ijo.2015.3. Epub 2015 Jan 23.

Abstract

BACKGROUND

Obesity is associated with decreased iron status, possibly due to a rise in hepcidin, an inflammatory protein known to reduce iron absorption. In animals, we have shown that maternal iron deficiency is minimised in the foetus by increased expression of placental transferrin receptor (pTFR1), resulting in increased iron transfer at the expense of maternal iron stores.

OBJECTIVE

This study examines the effect of obesity during pregnancy on maternal and neonatal iron status in human cohorts and whether the placenta can compensate for decreased maternal iron stores by increasing pTFR1 expression.

SUBJECTS/METHODS: A total of 240 women were included in this study. One hundred and fifty-eight placentas (Normal: 90; Overweight: 37; Obese: 31) were collected at delivery. Maternal iron status was measured by determining serum transferrin receptor (sTFR) and ferritin levels at 24 and 34 weeks and at delivery. Hepcidin in maternal and cord blood was measured by ELISA and pTFR1 in placentas by western blotting and real-time RT-PCR.

RESULTS

Low iron stores were more common in obese women. Hepcidin levels (ng ml(-1)) at the end of the pregnancy were higher in obese than normal women (26.03±12.95 vs 18.00±10.77, P<0.05). Maternal hepcidin levels were correlated with maternal iron status (sTFR r=0.2 P=0.025), but not with neonatal values. mRNA and protein levels of pTFR1 were both inversely related to maternal iron status. For mRNA and all women, sTFR r=0.2 P=0.044. Ferritin mRNA levels correlated only in overweight women r=-0.5 P=0.039 with hepcidin (r=0.1 P=0.349), irrespective of maternal body mass index (BMI).

CONCLUSIONS

The data support the hypothesis that obese pregnant women have a greater risk of iron deficiency and that hepcidin may be a regulatory factor. Further, we show that the placenta responds to decreased maternal iron status by increasing pTFR1 expression.

摘要

背景

肥胖与铁状态降低有关,这可能是由于铁调素水平升高所致,铁调素是一种已知会降低铁吸收的炎症蛋白。在动物实验中,我们发现通过增加胎盘转铁蛋白受体(pTFR1)的表达,胎儿期母体铁缺乏可降至最低,这导致铁转运增加,但以母体铁储备为代价。

目的

本研究探讨孕期肥胖对人类队列中母体和新生儿铁状态的影响,以及胎盘是否能通过增加pTFR1表达来补偿母体铁储备的减少。

对象/方法:本研究共纳入240名女性。分娩时收集了158份胎盘(正常:90份;超重:37份;肥胖:31份)。通过测定孕24周、34周及分娩时的血清转铁蛋白受体(sTFR)和铁蛋白水平来评估母体铁状态。采用ELISA法测定母体和脐带血中的铁调素,采用蛋白质印迹法和实时逆转录聚合酶链反应法测定胎盘中的pTFR1。

结果

铁储备低在肥胖女性中更为常见。肥胖女性妊娠末期的铁调素水平(ng/ml)高于正常女性(26.03±12.95 vs 18.00±10.77,P<0.05)。母体铁调素水平与母体铁状态相关(sTFR r=0.2,P=0.025),但与新生儿指标无关。pTFR1的mRNA和蛋白水平均与母体铁状态呈负相关。对于mRNA和所有女性,sTFR r=0.2,P=0.044。铁蛋白mRNA水平仅在超重女性中与铁调素相关(r=-0.5,P=0.039)(r=0.1,P=0.349),与母体体重指数(BMI)无关。

结论

数据支持以下假设,即肥胖孕妇缺铁风险更高,铁调素可能是一个调节因素。此外,我们表明胎盘通过增加pTFR1表达来应对母体铁状态的降低。

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