20α-Hydroxysteroid Dehydrogenase Expression in the Human Myometrium at Term and Preterm Birth: Relationships to Fetal Sex and Maternal Body Mass Index

被引:0
|
作者
Marina Paul
Tamas Zakar
Jason Phung
Amy Gregson
Anna Paredes Barreda
Trent A. Butler
Frederick R. Walker
Craig Pennell
Roger Smith
Jonathan W. Paul
机构
[1] University of Newcastle,School of Biomedical Sciences and Pharmacy, College of Health, Medicine and Wellbeing
[2] Hunter Medical Research Institute,Centre for Rehab Innovations
[3] University of Newcastle,School of Medicine and Public Health, College of Health, Medicine and Wellbeing
[4] University of Newcastle,undefined
[5] Mothers and Babies Research Centre,undefined
[6] John Hunter Hospital,undefined
来源
Reproductive Sciences | 2023年 / 30卷
关键词
Myometrium; Progesterone; 20α-HSD; Chorioamnionitis; BMI; Sex;
D O I
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学科分类号
摘要
The mechanism by which human labor is initiated in the presence of elevated circulating progesterone levels remains unknown. Recent evidence indicates that the progesterone-metabolizing enzyme, 20α-hydroxysteroid dehydrogenase (20α-HSD), encoded by the gene AKR1C1, may contribute to functional progesterone withdrawal. We found that AKR1C1 expression significantly increased with labor onset in term myometrium, but not in preterm myometrium. Among preterm laboring deliveries, clinically diagnosed chorioamnionitis was associated with significantly elevated AKR1C1 expression. AKR1C1 expression positively correlated with BMI before labor and negatively correlated with BMI during labor. Analysis by fetal sex showed that AKR1C1 expression was significantly higher in women who delivered male babies compared to women who delivered female babies at term, but not preterm. Further, in pregnancies where the fetus was female, AKR1C1 expression positively correlated with the mother’s age and BMI at the time of delivery. In conclusion, the increase in myometrial AKR1C1 expression with term labor is consistent with 20α-HSD playing a role in local progesterone metabolism to promote birth. Interestingly, this role appears to be specific to term pregnancies where the fetus is male. Upregulated AKR1C1 expression in the myometrium at preterm in-labor with clinical chorioamnionitis suggests that increased 20α-HSD activity is a mechanism through which inflammation drives progesterone withdrawal in preterm labor. The link between AKR1C1 expression and maternal BMI may provide insight into why maternal obesity is often associated with dysfunctional labor. Higher myometrial AKR1C1 expression in male pregnancies may indicate fetal sex-related differences in the mechanisms that precipitate labor onset at term.
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页码:2512 / 2523
页数:11
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