Lipidomics reveals cell specific changes during pluripotent differentiation to neural and mesodermal lineages.

IF 3 4区 生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY
Molecular omics Pub Date : 2025-03-13 DOI:10.1039/d4mo00261j
Melanie T Odenkirk, Haley C Jostes, Kevin R Francis, Erin S Baker
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引用次数: 0

Abstract

Due to their self-renewal and differentiation capabilities, pluripotent stem cells hold immense potential for advancing our understanding of human disease and developing cell-based or pharmacological interventions. Realizing this potential, however, requires a thorough understanding of the basal cellular mechanisms which occur during differentiation. Lipids are critical molecules that define the morphological, biochemical, and functional role of cells. This, combined with emerging evidence linking lipids to neurodegeneration, cardiovascular health, and other diseases, makes lipids a critical class of analytes to assess normal and abnormal cellular processes. While previous work has examined the lipid composition of stem cells, uncertainties remain about which changes are conserved and which are unique across distinct cell types. In this study, we investigated lipid alterations of induced pluripotent stem cells (iPSCs) at critical stages of differentiation toward neural or mesodermal fates. Lipidomic analyses of distinct differentiation stages were completed using a platform coupling liquid chromatography, ion mobility spectrometry, and mass spectrometry (LC-IMS-MS) separations. Results illustrated a shared triacylglyceride and free fatty acid accumulation in early iPSCs that were utilized at different stages of differentiation. Unique fluctuations through differentiation were also observed for certain phospholipid classes, sphingomyelins, and ceramides. These insights into lipid fluctuations across iPSC differentiation enhance our fundamental understanding of lipid metabolism within pluripotent stem cells and during differentiation, while also paving the way for a more precise and effective application of pluripotent stem cells in human disease interventions.

脂质组学揭示了神经和中胚层谱系多能分化过程中细胞的特异性变化。
由于其自我更新和分化能力,多能干细胞在促进我们对人类疾病的理解和开发基于细胞或药物干预方面具有巨大的潜力。然而,要实现这一潜力,需要对分化过程中发生的基础细胞机制有透彻的了解。脂质是决定细胞形态、生化和功能的关键分子。这一点,再加上将脂质与神经退行性变、心血管健康和其他疾病联系起来的新证据,使脂质成为评估正常和异常细胞过程的关键分析物。虽然以前的工作已经研究了干细胞的脂质组成,但对于哪些变化是保守的,哪些变化在不同的细胞类型中是独特的,仍然存在不确定性。在这项研究中,我们研究了诱导多能干细胞(iPSCs)在向神经或中胚层分化的关键阶段的脂质改变。不同分化阶段的脂质组学分析使用液相色谱、离子迁移率光谱和质谱(LC-IMS-MS)分离的耦合平台完成。结果表明,在分化的不同阶段,早期iPSCs中有共同的甘油三酯和游离脂肪酸积累。通过分化也观察到某些磷脂类、鞘磷脂和神经酰胺的独特波动。这些关于iPSC分化过程中脂质波动的见解增强了我们对多能干细胞内和分化过程中脂质代谢的基本理解,同时也为更精确和有效地应用多能干细胞进行人类疾病干预铺平了道路。
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来源期刊
Molecular omics
Molecular omics Biochemistry, Genetics and Molecular Biology-Biochemistry
CiteScore
5.40
自引率
3.40%
发文量
91
期刊介绍: Molecular Omics publishes high-quality research from across the -omics sciences. Topics include, but are not limited to: -omics studies to gain mechanistic insight into biological processes – for example, determining the mode of action of a drug or the basis of a particular phenotype, such as drought tolerance -omics studies for clinical applications with validation, such as finding biomarkers for diagnostics or potential new drug targets -omics studies looking at the sub-cellular make-up of cells – for example, the subcellular localisation of certain proteins or post-translational modifications or new imaging techniques -studies presenting new methods and tools to support omics studies, including new spectroscopic/chromatographic techniques, chip-based/array technologies and new classification/data analysis techniques. New methods should be proven and demonstrate an advance in the field. Molecular Omics only accepts articles of high importance and interest that provide significant new insight into important chemical or biological problems. This could be fundamental research that significantly increases understanding or research that demonstrates clear functional benefits. Papers reporting new results that could be routinely predicted, do not show a significant improvement over known research, or are of interest only to the specialist in the area are not suitable for publication in Molecular Omics.
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