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母亲接受羟考酮治疗会导致胎盘出现病理生理学改变。

Maternal oxycodone treatment causes pathophysiological changes in the mouse placenta.

机构信息

Christopher S Bond Life Sciences Center, University of Missouri, Columbia, MO, 65211, USA; Biomedical Sciences, University of Missouri, Columbia, MO, 65211, USA.

DNA Core Facility, University of Missouri, Columbia, MO, 65211, USA.

出版信息

Placenta. 2020 Oct;100:96-110. doi: 10.1016/j.placenta.2020.08.006. Epub 2020 Aug 23.

Abstract

INTRODUCTION

Pregnant women are increasingly being prescribed and abusing opioid drugs. As the primary communication organ between mother and conceptus, the placenta may be vulnerable to opioid effects but also holds the key to better understanding how these drugs affect long-term offspring health. We hypothesized that maternal treatment with oxycodone (OXY), the primary opioid at the center of the current crisis, deleteriously affects placental structure and gene expression patterns.

METHODS

Female mice were treated daily with 5 mg OXY/kg or saline solution (Control, CTL) for two weeks prior to breeding and until placenta were collected at embryonic age 12.5. A portion of the placenta was fixed for histology, and the remainder was frozen for RNA isolation followed by RNAseq.

RESULTS

Maternal OXY treatment reduced parietal trophoblast giant cell (pTGC) area and decreased the maternal blood vessel area within the labyrinth region. OXY exposure affected placental gene expression profiles in a sex dependent manner with female placenta showing up-regulation of many placental enriched genes, including Ceacam11, Ceacam14, Ceacam12, Ceacam13, Prl7b1, Prl2b1, Ctsq, and Tpbpa. In contrast, placenta of OXY exposed males had alteration of many ribosomal proteins. Weighted correlation network analysis revealed that in OXY female vs. CTL female comparison, select modules correlated with OXY-induced placental histological changes. Such associations were lacking in the male OXY vs. CTL male comparison.

DISCUSSION

Results suggest OXY exposure alters placental histology. In response to OXY exposure, female placenta responds by upregulating placental enriched transcripts that are either unchanged or downregulated in male placenta. Such changes may shield female offspring from developmental origins of health and disease-based diseases.

摘要

简介

越来越多的孕妇被开处并滥用阿片类药物。作为母体与胎儿之间的主要交流器官,胎盘可能容易受到阿片类药物的影响,但也为更好地理解这些药物如何影响后代的长期健康提供了关键。我们假设,母体每日接受羟考酮(OXY)治疗(目前危机的主要阿片类药物)会对胎盘结构和基因表达模式产生有害影响。

方法

雌性小鼠在配种前和胚胎 12.5 天时接受每日 5mg OXY/kg 或生理盐水(对照,CTL)处理两周。一部分胎盘用于组织学固定,其余胎盘用于 RNA 分离,随后进行 RNAseq。

结果

母体 OXY 处理减少了壁细胞滋养细胞巨细胞(pTGC)的面积,并减少了绒毛板区域内的母体血管面积。OXY 暴露以性别依赖的方式影响胎盘基因表达谱,雌性胎盘表现出许多胎盘富集基因的上调,包括 Ceacam11、Ceacam14、Ceacam12、Ceacam13、Prl7b1、Prl2b1、Ctsq 和 Tpbpa。相比之下,OXY 暴露的雄性胎盘改变了许多核糖体蛋白。加权相关网络分析显示,在 OXY 雌性与 CTL 雌性的比较中,选择模块与 OXY 诱导的胎盘组织学变化相关。在 OXY 雄性与 CTL 雄性的比较中,不存在这种关联。

讨论

结果表明,OXY 暴露改变了胎盘的组织学。对 OXY 暴露的反应,雌性胎盘通过上调在雄性胎盘不变或下调的胎盘富集转录本来作出反应。这些变化可能使雌性后代免受健康和疾病起源的影响。

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