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心脏超微结构仿生基质诱导分化的人心肌细胞的高级代谢和功能成熟。

Cardiac ultrastructure inspired matrix induces advanced metabolic and functional maturation of differentiated human cardiomyocytes.

机构信息

Department of Medicine, Division of Cardiology, University of California, San Francisco, San Francisco, CA 94158, USA.

Department of Biomedical Engineering, University of Connecticut Health, Farmington, CT 06032, USA.

出版信息

Cell Rep. 2022 Jul 26;40(4):111146. doi: 10.1016/j.celrep.2022.111146.

Abstract

The vast potential of human induced pluripotent stem-cell-derived cardiomyocytes (hiPSC-CMs) in preclinical models of cardiac pathologies, precision medicine, and drug screening remains to be fully realized because hiPSC-CMs are immature without adult-like characteristics. Here, we present a method to accelerate hiPSC-CM maturation on a substrate, cardiac mimetic matrix (CMM), mimicking adult human heart matrix ligand chemistry, rigidity, and submicron ultrastructure, which synergistically mature hiPSC-CMs rapidly within 30 days. hiPSC-CMs matured on CMM exhibit systemic transcriptomic maturation toward an adult heart state, are aligned with high strain energy, metabolically rely on oxidative phosphorylation and fatty acid oxidation, and display enhanced redox handling capability, efficient calcium handling, and electrophysiological features of ventricular myocytes. Endothelin-1-induced pathological hypertrophy is mitigated on CMM, highlighting the role of a native cardiac microenvironment in withstanding hypertrophy progression. CMM is a convenient model for accelerated development of ventricular myocytes manifesting highly specialized cardiac-specific functions.

摘要

人诱导多能干细胞衍生的心肌细胞(hiPSC-CMs)在心脏疾病的临床前模型、精准医学和药物筛选方面具有巨大的潜力,但由于 hiPSC-CMs 不成熟,缺乏成人样特征,其潜力尚未得到充分实现。在这里,我们提出了一种在基质(心脏模拟基质,CMM)上加速 hiPSC-CM 成熟的方法,该基质模拟成人心脏基质配体化学、刚性和亚微米超微结构,协同作用可在 30 天内快速成熟 hiPSC-CM。在 CMM 上成熟的 hiPSC-CMs 表现出向成人心脏状态的系统转录组成熟,与高应变能对齐,代谢上依赖氧化磷酸化和脂肪酸氧化,并表现出增强的氧化还原处理能力、有效的钙处理以及心室肌细胞的电生理特性。CMM 减轻了内皮素-1 诱导的病理性肥大,突出了天然心脏微环境在抵抗肥大进展中的作用。CMM 是一种用于加速表现出高度特化心脏功能的心室肌细胞发育的便捷模型。

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