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Functional and molecular effects of TNF-α on human iPSC-derived cardiomyocytes

Anita Saraf, Antonio Rampoldi, Myra Chao, Dong Li, Lawrence C. Armand, Hyun Sub Hwang, Rui Liu, Rajnesh Jha, Haian Fu, Joshua T. Maxwell, Chunhui Xu

2021Stem Cell Research36 citationsDOIOpen Access PDF

Abstract

Proinflammatory molecule tumor necrosis factor alpha (TNF-α) is predominantly elevated in cytokine storm as well as worsening cardiac function. Here we model the molecular and functional effects of TNF-α in cardiomyocytes (CMs) derived from human induced pluripotent stem cells (hiPSC). We found that treatment of hiPSC-CMs with TNF-α increased reactive oxygen species (ROS) and caspase 3/7 activity and caused cell death and apoptosis. TNF-α treatment also resulted in dysregulation of cardiomyocyte function with respect to the increased abnormal calcium handling, calcium wave propagation between cells and excitation-contraction coupling. We also uncovered significant changes in gene expression and protein localization caused by TNF-α treatment. Notably, TNF-α treatment altered the expression of ion channels, dysregulated cadherins, and affected the localization of gap-junction protein connexin-43. In addition, TNF-α treatment up-regulated IL-32 (a human specific cytokine, not present in rodents and an inducer of TNF-α) and IL-34 and down-regulated glutamate receptors and cardiomyocyte contractile proteins. These findings provide insights into the molecular and functional consequences from the exposure of human cardiomyocytes to TNF-α. Our study provides a model to incorporate inflammatory factors into hiPSC-CM-based studies to evaluate mechanistic aspects of heart disease.

Topics & Concepts

BiologyTumor necrosis factor alphaProinflammatory cytokineCell biologyCytokineConnexinInduced pluripotent stem cellApoptosisInflammationCancer researchGap junctionEndocrinologyImmunologyBiochemistryGeneIntracellularEmbryonic stem cellCardiac electrophysiology and arrhythmiasNeuroscience and Neural EngineeringConnexins and lens biology