Department of Pediatric Research Institute, Ministry of Education Key Laboratory of Child Development and Disorders, National Clinical Research Center for Child Health and Disorders (Chongqing), China International Science and Technology Cooperation base of Child development and Critical Disorders, Children's Hospital of Chongqing Medical University, Chongqing, Box 136, No. 3 Zhongshan RD, Yuzhong district, Chongqing, 400014, People's Republic of China.
Chongqing Key Laboratory of Pediatrics, Chongqing, People's Republic of China.
Stem Cell Res Ther. 2021 Mar 24;12(1):208. doi: 10.1186/s13287-021-02264-2.
Human induced pluripotent stem cell-derived cardiomyocytes (hiPSC-CMs) hold great promise for regenerative medicine and in drugs screening. Despite displaying key cardiomyocyte phenotypic characteristics, they more closely resemble fetal/neonatal cardiomyocytes and are still immature; these cells mainly rely on glucose as a substrate for metabolic energy, while mature cardiomyocytes mainly employ oxidative phosphorylation of fatty acids. Studies showed that the alteration of metabolism pattern from glycolysis to oxidative phosphorylation improve the maturity of hiPSC-CMs. As a transcription factor, accumulating evidences showed the important role of NRF2 in the regulation of energy metabolism, which directly regulates the expression of mitochondrial respiratory complexes. Therefore, we hypothesized that NRF2 is involved in the maturation of hiPSC-CMs.
The morphological and functional changes related to mitochondria and cell maturation were analyzed by knock-down and activation of NRF2.
The results showed that the inhibition of NRF2 led to the retardation of cell maturation. The activation of NRF2 leads to a more mature hiPSC-CMs phenotype, as indicated by the increase of cardiac maturation markers, sarcomere length, calcium transient dynamics, the number and fusion events of mitochondria, and mitochondrial respiration. Bioinformatics analysis showed that in addition to metabolism-related genes, NRF2 also activates the expression of myocardial ion channels.
These findings indicated that NRF2 plays an important role in the maturation of hiPSC-CMs. The present work provides greater insights into the molecular regulation of hiPSC-CMs metabolism and theoretical basis in drug screening, disease modeling, and alternative treatment.
人类诱导多能干细胞衍生的心肌细胞(hiPSC-CMs)在再生医学和药物筛选方面具有广阔的应用前景。尽管这些细胞表现出关键的心肌细胞表型特征,但它们更类似于胎儿/新生儿心肌细胞,仍然不成熟;这些细胞主要依赖葡萄糖作为代谢能量的底物,而成熟的心肌细胞主要利用脂肪酸的氧化磷酸化。研究表明,代谢模式从糖酵解向氧化磷酸化的转变可以改善 hiPSC-CMs 的成熟度。作为一种转录因子,越来越多的证据表明 NRF2 在能量代谢的调节中起着重要作用,它直接调节线粒体呼吸复合物的表达。因此,我们假设 NRF2 参与了 hiPSC-CMs 的成熟过程。
通过敲低和激活 NRF2,分析与线粒体和细胞成熟相关的形态和功能变化。
结果表明,NRF2 的抑制导致细胞成熟的延迟。NRF2 的激活导致 hiPSC-CMs 更成熟的表型,表现为心脏成熟标志物的增加、肌节长度、钙瞬变动力学、线粒体数量和融合事件以及线粒体呼吸的增加。生物信息学分析表明,除了与代谢相关的基因外,NRF2 还激活了心肌离子通道的表达。
这些发现表明 NRF2 在 hiPSC-CMs 的成熟过程中起着重要作用。本工作为 hiPSC-CMs 代谢的分子调控提供了更深入的了解,并为药物筛选、疾病建模和替代治疗提供了理论依据。
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