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Fatty Acid-Treated Induced Pluripotent Stem Cell-Derived Human Cardiomyocytes Exhibit Adult Cardiomyocyte-Like Energy Metabolism Phenotypes

机译:脂肪酸处理的诱导多能干细胞衍生人心肌细胞表现出成人心肌细胞样能量代谢表型

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Human induced pluripotent stem cell (iPSC)-derived cardiomyocytes (CMs) (iPSC-CMs) are a promising cell source for myocardial regeneration, disease modeling and drug assessment. However, iPSC-CMs exhibit immature fetal CM-like characteristics that are different from adult CMs in several aspects, including cellular structure and metabolism. As an example, glycolysis is a major energy source for immature CMs. As CMs mature, the mitochondrial oxidative capacity increases, with fatty acid β-oxidation becoming a key energy source to meet the heart’s high energy demand. The immaturity of iPSC-CMs thereby limits their applications. The aim of this study was to investigate whether the energy substrate fatty acid-treated iPSC-CMs exhibit adult CM-like metabolic properties. After 20 days of differentiation from human iPSCs, iPSC-CMs were sequentially cultured with CM purification medium (lactate+/glucose-) for 7 days and maturation medium (fatty acids+/glucose-) for 3–7 days by mimicking the adult CM’s preference of utilizing fatty acids as a major metabolic substrate. The purity and maturity of iPSC-CMs were characterized via the analysis of: (1) Expression of CM-specific markers (e.g., troponin T, and sodium and potassium channels) using RT-qPCR, Western blot or immunofluorescence staining and electron microscopy imaging; and (2) cell energy metabolic profiles using the XF96 Extracellular Flux Analyzer. iPSCs-CMs (98% purity) cultured in maturation medium exhibited enhanced elongation, increased mitochondrial numbers with more aligned Z-lines, and increased expression of matured CM-related genes, suggesting that fatty acid-contained medium promotes iPSC-CMs to undergo maturation. In addition, the oxygen consumption rate (OCR) linked to basal respiration, ATP production, and maximal respiration and spare respiratory capacity (representing mitochondrial function) was increased in matured iPSC-CMs. Mature iPSC-CMs also displayed a larger change in basal and maximum respirations due to the utilization of exogenous fatty acids (palmitate) compared with non-matured control iPSC-CMs. Etomoxir (a carnitine palmitoyltransferase 1 inhibitor) but not 2-deoxyglucose (an inhibitor of glycolysis) abolished the palmitate pretreatment-mediated OCR increases in mature iPSC-CMs. Collectively, our data demonstrate for the first time that fatty acid treatment promotes metabolic maturation of iPSC-CMs (as evidenced by enhanced mitochondrial oxidative function and strong capacity of utilizing fatty acids as energy source). These matured iPSC-CMs might be a promising human CM source for broad biomedical application.
机译:人诱导多能干细胞(IPSC)的心肌细胞(CMS)(IPSC-CMS)是对心肌再生,疾病建模和药物评估的有前途的细胞来源。然而,在几个方面,IPSC-CMS表现出与成年CM不同的未成熟胎儿CM样特征,包括细胞结构和代谢。作为一个例子,糖酵解是未成熟CMS的主要能源。作为CMS成熟,线粒体氧化能力增加,脂肪酸β-氧化成为满足心脏高能量需求的关键能源。因此,IPSC-CMS的不舒育将限制其应用。本研究的目的是研究能量底物脂肪酸处理的IPSC-CMS是否表现出成体CM样代谢性质。在从人IPSCS分化20天后,通过模拟成人CM的偏好,用CM纯化培养基(乳酸+ /葡萄糖+ /葡萄糖)依次用CM纯化培养基(乳酸+ /葡萄糖+ /葡萄糖)依次培养IPSC-CMS 3-7天利用脂肪酸作为主要代谢底物。通过分析:(1)使用RT-QPCR,Western印迹或免疫荧光染色和电子显微镜成像,通过分析IPSC-CMS的纯度和成熟度:(1)CM特异性标记(例如,肌钙蛋白T和钠和钾通道)的表达; (2)使用XF96细胞外助焊剂分析仪的细胞能量代谢谱。在成熟培养基中培养的IPSCS-CMS(98%纯度)表现出增强的伸长率,增加的线粒体数量增加,具有更多对齐的Z-线,并增加了成熟的CM相关基因的表达,表明含脂肪酸含量促使IPSC-CM促进了成熟的IPSC-CM 。此外,在成熟的IPSC-CM中增加了与基础呼吸,ATP生产和最大呼吸和备用呼吸能力(代表线粒体功能)连接的氧气消耗率(OCR)。由于与非成熟控制IPSC-CMS相比,成熟的IPSC-CMS也显示出基础和最大呼吸的更大变化和最大呼吸。 Etomoxir(肉毒氨基棕榈酰棕榈酰转移酶1抑制剂)但不是2-脱氧葡萄糖(糖酵解抑制剂)废除了棕榈酸盐预处理介导的OCR成熟IPSC-CMS中的增加。集体,我们的数据首次证明脂肪酸处理促进IPSC-CMS的代谢成熟(如提高的线粒体氧化功能和使用脂肪酸作为能量源的强能力)。这些成熟的IPSC-CM可能是广泛的生物医学应用的有希望的人类CM源。

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