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Analysis of the metabolic footprint and tissue metabolome of placental villous explants cultured at different oxygen tensions reveals novel redox biomarkers.

机译:对在不同氧气压力下培养的胎盘绒毛外植体的代谢足迹和组织代谢组进行分析,发现了新颖的氧化还原生物标记。

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摘要

Pre-eclampsia (PE) is a multi-system disorder of pregnancy hypothesised to arise from circulating factors derived from an unhealthy placenta. Some changes in placental phenotype seen in PE can be reproduced by culture in altered oxygen (O(2)) tension. Currently, these circulating factors are unidentified, partly due to the complexity of maternal plasma. Investigation of factors released from placental tissue provides a potential method to identify bioactive compounds. Experimental strategies to study compounds present in a biological system have expanded greatly in recent years. Metabolomics can detect and identify endogenous and secreted metabolites. We aimed to determine whether metabolites could be identified in placental cultures with acceptable experimental variability and to determine whether altered O(2) tension affects the composition of the placental metabolome. In this study we used gas-chromatography-mass spectroscopy to determine the presence of metabolites in conditioned culture medium (CCM) and tissue lysates of placental villous explants cultured in 1, 6 and 20% atmospheric O(2) for 96h. This experimental strategy had an intra-assay variation of 6.1-11.6%. Intra and inter-placental variability were 15.7-35.8% and 44.8-46.2% respectively. Metabolic differences were identified between samples cultured in 1, 6 and 20% O(2) in both CCM and tissue lysate. Differentially expressed metabolites included: 2-deoxyribose, threitol or erythritol and hexadecanoic acid. We conclude that metabolomic strategies offer a novel approach to investigate placental function. When conducted under carefully controlled conditions, with appropriate statistical analysis, metabolic differences can be identified in placental explants in response to altered O(2) tension. Metabolomics could be used to identify changes in conditions associated with placental pathology.
机译:子痫前期(PE)是一种多系统妊娠疾病,据推测是由不健康胎盘产生的循环因子引起的。 PE中可见的胎盘表型的某些变化可以通过改变氧气(O(2))张力的培养来再现。目前,这些循环因素尚不清楚,部分原因是母体血浆的复杂性。从胎盘组织释放的因子的研究提供了一种潜在的方法来鉴定生物活性化合物。近年来,研究生物系统中存在的化合物的实验策略已大大扩展。代谢组学可以检测和鉴定内源性和分泌性代谢物。我们旨在确定是否可以在胎盘培养物中鉴定出具有可接受的实验变异性的代谢物,并确定改变的O(2)张力是否影响胎盘代谢组的组成。在这项研究中,我们使用气相色谱-质谱法确定在条件培养基(CCM)和胎盘绒毛外植体组织裂解物中的代谢产物的存在,分别在1,6%和20%大气O(2)中培养96h。该实验策略的批内分析差异为6.1-11.6%。胎盘内和胎盘间变异分别为15.7-35.8%和44.8-46.2%。在CCM和组织裂解物中,分别在1%,6%和20%O(2)中培养的样品之间鉴定出代谢差异。差异表达的代谢产物包括:2-脱氧核糖,苏糖醇或赤藓糖醇和十六烷酸。我们得出结论,代谢组学策略提供了一种研究胎盘功能的新颖方法。在精心控制的条件下进行适当的统计分析时,可以响应于O(2)张力的变化确定胎盘外植体的代谢差异。代谢组学可用于识别与胎盘病理学相关的状况变化。

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