Optical mapping of human embryonic stem cell-derived cardiomyocyte graft electrical activity in injured hearts

Authors

Dominic Filice, University of Washington, Seattle
Wahiba Dhahri, University Health Network University of Toronto
Joell L. Solan, Fred Hutchinson Cancer Research Center
Paul D. Lampe, Fred Hutchinson Cancer Research Center
Erin Steele, University of Washington, Seattle
Nikita Milani, University of Washington, Seattle
Benjamin Van Biber, University of Washington, Seattle
Wei Zhong Zhu, University of Washington, Seattle
Tamilla Sadikov Valdman, University Health Network University of Toronto
Rocco Romagnolo, University Health Network University of Toronto
José David Otero-Cruz, University of Washington, Seattle
Kip D. Hauch, University of Washington, Seattle
Matthew W. Kay, The George Washington University
Narine Sarvazyan, The George Washington University
Michael A. Laflamme, University Health Network University of Toronto

Document Type

Journal Article

Publication Date

9-25-2020

Journal

Stem cell research & therapy

Volume

11

Issue

1

DOI

10.1186/s13287-020-01919-w

Keywords

Cardiac electrophysiology; Cardiomyocyte; Cell transplantation; Human embryonic stem cells; Optical mapping

Abstract

BACKGROUND: Human embryonic stem cell-derived cardiomyocytes (hESC-CMs) show tremendous promise for cardiac regeneration, but the successful development of hESC-CM-based therapies requires improved tools to investigate their electrical behavior in recipient hearts. While optical voltage mapping is a powerful technique for studying myocardial electrical activity ex vivo, we have previously shown that intra-cardiac hESC-CM grafts are not labeled by conventional voltage-sensitive fluorescent dyes. We hypothesized that the water-soluble voltage-sensitive dye di-2-ANEPEQ would label engrafted hESC-CMs and thereby facilitate characterization of graft electrical function and integration. METHODS: We developed and validated a novel optical voltage mapping strategy based on the simultaneous imaging of the calcium-sensitive fluorescent protein GCaMP3, a graft-autonomous reporter of graft activation, and optical action potentials (oAPs) derived from di-2-ANEPEQ, which labels both graft and host myocardium. Cardiomyocytes from three different GCaMP3+ hESC lines (H7, RUES2, or ESI-17) were transplanted into guinea pig models of subacute and chronic infarction, followed by optical mapping at 2 weeks post-transplantation. RESULTS: Use of a water-soluble voltage-sensitive dye revealed pro-arrhythmic properties of GCaMP3+ hESC-CM grafts from all three lines including slow conduction velocity, incomplete host-graft coupling, and spatially heterogeneous patterns of activation that varied beat-to-beat. GCaMP3+ hESC-CMs from the RUES2 and ESI-17 lines both showed prolonged oAP durations both in vitro and in vivo. Although hESC-CMs partially remuscularize the injured hearts, histological evaluation revealed immature graft structure and impaired gap junction expression at this early timepoint. CONCLUSION: Simultaneous imaging of GCaMP3 and di-2-ANEPEQ allowed us to acquire the first unambiguously graft-derived oAPs from hESC-CM-engrafted hearts and yielded critical insights into their arrhythmogenic potential and line-to-line variation.

APA Citation

Filice, D., Dhahri, W., Solan, J., Lampe, P., Steele, E., Milani, N., Van Biber, B., Zhu, W., Valdman, T., Romagnolo, R., Otero-Cruz, J., Hauch, K., Kay, M., Sarvazyan, N., & Laflamme, M. (2020). Optical mapping of human embryonic stem cell-derived cardiomyocyte graft electrical activity in injured hearts. Stem cell research & therapy, 11 (1). http://dx.doi.org/10.1186/s13287-020-01919-w