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首页> 外文期刊>The Analyst: The Analytical Journal of the Royal Society of Chemistry: A Monthly International Publication Dealing with All Branches of Analytical Chemistry >Single-cell mass spectrometry with multi-solvent extraction identifies metabolic differences between left and right blastomeres in the 8-cell frog (Xenopus) embryo
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Single-cell mass spectrometry with multi-solvent extraction identifies metabolic differences between left and right blastomeres in the 8-cell frog (Xenopus) embryo

机译:具有多溶剂萃取的单细胞质谱法可识别8细胞青蛙(非洲爪蟾)胚胎中左右卵裂球之间的代谢差异

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Single-cell metabolic mass spectrometry enables the discovery (untargeted) analysis of small molecules in individual cells. Using single-cell capillary electrophoresis high-resolution mass spectrometry (CE-HRMS), we recently uncovered small-molecule differences between embryonic cells located along the animal-vegetal and dorsal-ventral axes of the 16-cell frog (Xenopus laevis) embryo, raising the question whether metabolic cell heterogeneity also exists along the left-right body axis. To address this question, we here advance single-cell CE-HRMS for identifying and quantifying metabolites in higher analytical sensitivity, and then use the methodology to compare metabolite production between left and right cells. Our strategy utilizes multiple solvents with complementary physicochemical properties to extract small molecules from single cells and improve electrophoretic separation, increasing metabolite ion signals for quantification and tandem HRMS. As a result, we were able to identify 55 different small molecules in D1 cells that were isolated from 8-cell embryos. To quantify metabolite production between left and right cells, we analyzed n = 24 different D1 cells in technical duplicate-triplicate measurements. Statistical and multivariate analysis based on 80 of the most repeatedly quantified compounds revealed 10 distinct metabolites that were significantly differentially accumulated in the left or right cells (p < 0.05 and fold change >= 1.5). These metabolites were enriched in the arginine-proline metabolic pathway in the right, but not the left D1 cells. Besides providing analytical benefits for single-cell HRMS, this work provides new metabolic data on the establishment of normal body asymmetry in the early developing embryo.
机译:单细胞代谢质谱法能够发现(非靶向)单个细胞中的小分子。使用单细胞毛细管电泳高分辨率质谱(CE-HRMS),我们最近发现了沿16细胞青蛙(Xenopus laevis)胚胎的动物-植物和背-腹轴分布的胚胎细胞之间的小分子差异,提出了一个问题,即沿左右身体轴是否也存在代谢细胞异质性。为了解决这个问题,我们在此推进单细胞CE-HRMS,以更高的分析灵敏度来鉴定和定量代谢产物,然后使用该方法比较左细胞和右细胞之间的代谢产物。我们的策略是利用具有互补理化特性的多种溶剂从单细胞中提取小分子并改善电泳分离,增加代谢物离子信号进行定量和串联HRMS。结果,我们能够鉴定出从8细胞胚胎分离的D1细胞中的55个不同小分子。为了量化左右细胞之间的代谢产物产生,我们在技术重复测量中分析了n = 24个不同的D1细胞。基于80种最定量重复的化合物的统计和多变量分析显示,左或右细胞中有10种不同的代谢物明显差异累积(p <0.05,倍数变化== 1.5)。这些代谢物在右侧的精氨酸-脯氨酸代谢途径中富集,而在左侧的D1细胞中富集。除了为单细胞HRMS提供分析益处外,这项工作还提供了有关在早期发育的胚胎中建立正常身体不对称性的新代谢数据。

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