TY - JOUR
T1 - Mutant ANP induces mitochondrial and ion channel remodeling in a human iPSC-derived atrial fibrillation model
AU - Ly, Olivia T.
AU - Chen, Hanna
AU - Brown, Grace E.
AU - Hong, Liang
AU - Wang, Xinge
AU - Han, Yong Duk
AU - Pavel, Mahmud Arif
AU - Sridhar, Arvind
AU - Maienschein-Cline, Mark
AU - Chalazan, Brandon
AU - Ong, Sang Ging
AU - Abdelhady, Khaled
AU - Massad, Malek
AU - Rizkallah, Lona Ernst
AU - Rehman, Jalees
AU - Khetani, Salman R.
AU - Darbar, Dawood
N1 - Publisher Copyright:
© 2022, Ly et al.
PY - 2022/4/8
Y1 - 2022/4/8
N2 - Human induced pluripotent stem cell-derived cardiomyocytes (iPSC-CMs) can model heritable arrhythmias to personalize therapies for individual patients. Although atrial fibrillation (AF) is a leading cause of cardiovascular morbidity and mortality, current platforms to generate iPSC-atrial (a) CMs are inadequate for modeling AF. We applied a combinatorial engineering approach, which integrated multiple physiological cues, including metabolic conditioning and electrical stimulation, to generate mature iPSC-aCMs. Using the patient's own atrial tissue as a gold standard benchmark, we assessed the electrophysiological, structural, metabolic, and molecular maturation of iPSC-aCMs. Unbiased transcriptomic analysis and inference from gene regulatory networks identified key gene expression pathways and transcription factors mediating atrial development and maturation. Only mature iPSC-aCMs generated from patients with heritable AF carrying the non-ion channel gene (NPPA) mutation showed enhanced expression and function of a cardiac potassium channel and revealed mitochondrial electron transport chain dysfunction. Collectively, we propose that ion channel remodeling in conjunction with metabolic defects created an electrophysiological substrate for AF. Overall, our electro-metabolic approach generated mature human iPSC-aCMs that unmasked the underlying mechanism of the first non-ion channel gene, NPPA, that causes AF. Our maturation approach will allow for the investigation of the molecular underpinnings of heritable AF and the development of personalized therapies.
AB - Human induced pluripotent stem cell-derived cardiomyocytes (iPSC-CMs) can model heritable arrhythmias to personalize therapies for individual patients. Although atrial fibrillation (AF) is a leading cause of cardiovascular morbidity and mortality, current platforms to generate iPSC-atrial (a) CMs are inadequate for modeling AF. We applied a combinatorial engineering approach, which integrated multiple physiological cues, including metabolic conditioning and electrical stimulation, to generate mature iPSC-aCMs. Using the patient's own atrial tissue as a gold standard benchmark, we assessed the electrophysiological, structural, metabolic, and molecular maturation of iPSC-aCMs. Unbiased transcriptomic analysis and inference from gene regulatory networks identified key gene expression pathways and transcription factors mediating atrial development and maturation. Only mature iPSC-aCMs generated from patients with heritable AF carrying the non-ion channel gene (NPPA) mutation showed enhanced expression and function of a cardiac potassium channel and revealed mitochondrial electron transport chain dysfunction. Collectively, we propose that ion channel remodeling in conjunction with metabolic defects created an electrophysiological substrate for AF. Overall, our electro-metabolic approach generated mature human iPSC-aCMs that unmasked the underlying mechanism of the first non-ion channel gene, NPPA, that causes AF. Our maturation approach will allow for the investigation of the molecular underpinnings of heritable AF and the development of personalized therapies.
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U2 - 10.1172/jci.insight.155640
DO - 10.1172/jci.insight.155640
M3 - Article
C2 - 35393944
AN - SCOPUS:85128154716
SN - 2379-3708
VL - 7
JO - JCI Insight
JF - JCI Insight
IS - 7
M1 - e155640
ER -