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催产素受体DNA甲基化与分娩和产后出血期间外源性催产素需求有关。

Oxytocin receptor DNA methylation is associated with exogenous oxytocin needs during parturition and postpartum hemorrhage.

作者信息

Erickson Elise N, Myatt Leslie, Danoff Joshua S, Krol Kathleen M, Connelly Jessica J

机构信息

Oregon Health and Science University, Portland, OR, USA.

University of Arizona, Tucson, AZ, USA.

出版信息

Commun Med (Lond). 2023 Jan 27;3(1):11. doi: 10.1038/s43856-023-00244-6.

Abstract

BACKGROUND

The oxytocin receptor gene (OXTR) is regulated, in part, by DNA methylation. This mechanism has implications for uterine contractility during labor and for prevention or treatment of postpartum hemorrhage, an important contributor to global maternal morbidity and mortality.

METHODS

We measured and compared the level of OXTR DNA methylation between matched blood and uterine myometrium to evaluate blood as an indicator of uterine methylation status using targeted pyrosequencing and sites from the Illumina EPIC Array. Next, we tested for OXTR DNA methylation differences in blood between individuals who experienced a postpartum hemorrhage arising from uterine atony and matched controls following vaginal birth. Bivariate statistical tests, generalized linear modeling and Poisson regression were used in the analyses.

RESULTS

Here we show a significant positive correlation between blood and uterine DNA methylation levels at several OXTR loci. Females with higher OXTR DNA methylation in blood had required significantly more exogenous oxytocin during parturition. With higher DNA methylation, those who had oxytocin administered during labor had significantly greater relative risk for postpartum hemorrhage (IRR 2.95, 95% CI 1.53-5.71).

CONCLUSIONS

We provide evidence that epigenetic variability in OXTR is associated with the amount of oxytocin administered during parturition and moderates subsequent postpartum hemorrhage. Methylation can be measured using a peripheral tissue, suggesting potential use in identifying individuals susceptible to postpartum hemorrhage. Future studies are needed to quantify myometrial gene expression in connection with OXTR methylation.

摘要

背景

催产素受体基因(OXTR)部分受DNA甲基化调控。这种机制对分娩时的子宫收缩以及产后出血的预防或治疗具有重要意义,产后出血是全球孕产妇发病和死亡的重要原因。

方法

我们使用靶向焦磷酸测序和Illumina EPIC阵列中的位点,测量并比较了匹配的血液和子宫肌层之间OXTR DNA甲基化水平,以评估血液作为子宫甲基化状态的指标。接下来,我们测试了因子宫收缩乏力导致产后出血的个体与阴道分娩后的匹配对照组之间血液中OXTR DNA甲基化的差异。分析中使用了双变量统计检验、广义线性模型和泊松回归。

结果

我们发现,在几个OXTR基因座上,血液和子宫DNA甲基化水平之间存在显著的正相关。血液中OXTR DNA甲基化水平较高的女性在分娩期间需要显著更多的外源性催产素。DNA甲基化水平越高,分娩期间使用催产素的女性产后出血的相对风险显著更高(发病率比2.95,95%置信区间1.53 - 5.71)。

结论

我们提供的证据表明,OXTR的表观遗传变异性与分娩期间使用的催产素量有关,并影响随后的产后出血。甲基化可以通过外周组织进行测量,这表明其在识别易患产后出血的个体方面具有潜在用途。未来需要开展研究,以量化与OXTR甲基化相关的子宫肌层基因表达。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/135f/9883241/786952368451/43856_2023_244_Fig1_HTML.jpg

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