Characterization of the CACNA1C-R518C Missense Mutation in the Pathobiology of Long-QT Syndrome Using Human Induced Pluripotent Stem Cell Cardiomyocytes Shows Action Potential Prolongation and L-Type Calcium Channel Perturbation

被引:16
作者
Estes, Steven, I [1 ,2 ]
Ye, Dan [1 ,2 ]
Zhou, Wei [1 ,2 ]
Dotzler, Steven M. [1 ,2 ]
Tester, David J. [1 ,2 ,3 ]
Bos, J. Martijn [1 ,2 ,3 ]
Kim, C. S. John [1 ,2 ]
Ackerman, Michael J. [1 ,2 ,3 ,4 ]
机构
[1] Mayo Clin, Dept Mol Pharmacol & Expt Therapeut, Rochester, MN 55905 USA
[2] Mayo Clin, Windland Smith Rice Sudden Death Genom Lab, Rochester, MN 55905 USA
[3] Mayo Clin, Dept Cardiovasc Med, Div Heart Rhythm Serv, Rochester, MN 55905 USA
[4] Mayo Clin, Dept Pediat & Adolescent Med, Div Pediat Cardiol, Rochester, MN 55905 USA
来源
CIRCULATION-GENOMIC AND PRECISION MEDICINE | 2019年 / 12卷 / 08期
关键词
calcium; calcium channels; L-type; Fluo-4; humans; male; OF-FUNCTION MUTATIONS; ARRHYTHMIA; INTERVALS;
D O I
10.1161/CIRCGEN.119.002534
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
Background: The CACNA1C-encoded cardiac L-type calcium channel (Cav1.2) is essential for cardiocyte action potential duration (APD). We previously reported the CACNA1C-p.R518C variant associated with prolonged QT intervals, cardiomyopathy, and sudden cardiac death in several pedigrees. Methods: To characterize a patient-derived human induced pluripotent stem cell-derived cardiomyocyte (hiPSC-CM) CACNA1C-p.R518C model, CACNA1C-p.R518C hiPSC-CMs were generated from a 13-year-old man (QTc, >480 ms) with a family history of sudden cardiac death. An isogenic hiPSC-CM gene-corrected control was created using CRISPR/Cas9 (clustered regularly interspaced short palindromic repeats/clustered regularly interspaced short palindromic repeat-associated 9). APD and calcium handling were assessed by live cell imaging with Arclight voltage and Fluo-4 calcium indicators, respectively. The APD and L-type calcium channel biophysical properties were further assessed by whole-cell patch clamp technique. Results: The Bazett formula-corrected, Arclight-measured APD(90) of CACNA1C-p.R518C hiPSC-CMs was significantly longer (62211 ms; n=92) than the isogenic control hiPSC-CMs (453 +/- 5 ms; n=62; P<0.0001). Patch clamp assessment of CACNA1C-p.R518C hiPSC-CMs paced at 1 Hz confirmed a prolonged APD(90) (689 +/- 29 ms; n=10) compared with the patient's isogenic control hiPSC-CMs (434 +/- 30 ms; n=8; P<0.05). Fluo-4-measured calcium transient decay time suggested calcium mishandling in CACNA1C-p.R518C. Patch clamp analysis revealed increased L-type calcium channel window current, slow decay time at various voltages, and increased late calcium current for CACNA1C-p.R518C hiPSC-CMs when compared with isogenic control hiPSC-CMs. Conclusions: Using patient-specific hiPSC-CM mutant and isogenic control lines, we demonstrate that the CACNA1C-p.R518C variant is the self-sufficient, monogenetic substrate for the patient's long-QT syndrome phenotype. These data further bolster the conclusion that CACNA1C is a bona fide, definite evidence long-QT syndrome susceptibility gene.
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页数:8
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