Metabolic Maturation Media Improve Physiological Function of Human iPSC-Derived Cardiomyocytes

代谢成熟培养基改善人诱导多能干细胞来源心肌细胞的生理功能

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作者:Dries A M Feyen ,Wesley L McKeithan ,Arne A N Bruyneel ,Sean Spiering ,Larissa Hörmann ,Bärbel Ulmer ,Hui Zhang ,Francesca Briganti ,Michaela Schweizer ,Bence Hegyi ,Zhandi Liao ,Risto-Pekka Pölönen ,Kenneth S Ginsburg ,Chi Keung Lam ,Ricardo Serrano ,Christine Wahlquist ,Alexander Kreymerman ,Michelle Vu ,Prashila L Amatya ,Charlotta S Behrens ,Sara Ranjbarvaziri ,Renee G C Maas ,Matthew Greenhaw ,Daniel Bernstein ,Joseph C Wu ,Donald M Bers ,Thomas Eschenhagen ,Christian M Metallo ,Mark Mercola

Abstract

Induced pluripotent stem cell-derived cardiomyocytes (iPSC-CMs) have enormous potential for the study of human cardiac disorders. However, their physiological immaturity severely limits their utility as a model system and their adoption for drug discovery. Here, we describe maturation media designed to provide oxidative substrates adapted to the metabolic needs of human iPSC (hiPSC)-CMs. Compared with conventionally cultured hiPSC-CMs, metabolically matured hiPSC-CMs contract with greater force and show an increased reliance on cardiac sodium (Na+) channels and sarcoplasmic reticulum calcium (Ca2+) cycling. The media enhance the function, long-term survival, and sarcomere structures in engineered heart tissues. Use of the maturation media made it possible to reliably model two genetic cardiac diseases: long QT syndrome type 3 due to a mutation in the cardiac Na+ channel SCN5A and dilated cardiomyopathy due to a mutation in the RNA splicing factor RBM20. The maturation media should increase the fidelity of hiPSC-CMs as disease models. Keywords: cardiomyocyte; dilated cardiomyopathy; disease modeling; engineered heart tissues; induced pluripotent stem cells; long QT syndrome 3; maturation; physiology.

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