Abstract

Optogenetics refers to the use of light in conjunction with light-sensitive proteins to stimulate excitable cells and tissues. This project aims at extending the utility of optogenetics to cardiac applications. We exploit the heart's efficient cell to cell coupling, to develop the first cell delivery system for expression of light-sensitive ion channels, LSICs, i.e. non-viral cardiac optogenetics. We term our strategy a tandem cell unit (TCU) approach, where a light-responsive unit is formed by a host cardiomyocyte and a non-excitable donor cell carrying exogenous LSICs. Biophysically, for this unit to function (to fire an action potential upon light excitation), low-resistance coupling is required. Although in its infancy, cardiac optogenetics can be demonstrated effective for cardiac pacing, with a therapeutic application in the clinic, and as a research tool ideal for dissection of cardiac arrhythmias in vitro and perhaps in vivo owing to the robustness, remote nature and spatiotemporal precision of optical control. The driving hypothesis of this proposal is that optogenetics can provide a useful research and clinical approach to study cardiac excitability. Our experimental aims to test this hypothesis will employ single cardiac myocytes, tandem cell units and cardiac syncytia in vitro, along with in silico simulations and ultimately combined in vivo/in vitro proof of principle experiments for whole heart applications.
The Specific Aims are as follows: 1) Conduct comprehensive biophysical characterization of LSICs and develop in silico tools for cardiac optogenetics and integrate those in a dynamic clamp; 2) Quantify energy requirements of LSIC-based control of cardiac excitation and demonstrate optimization strategies for cardiac optogenetics based on the TCU concept; 3) Demonstrate utility of cardiac optogenetics in pacing and cardioversion in vitro; 4) Devise proof of principle experiments for in vivo optical pacing based on optimization results: If successful, we will determine the optimal donor cell parameters to minimize energy consumption and maximize spatial control of light-induced cardiac excitability and refractoriness in vitro, in silico and ex vivo at the single cell, tandem cell unit, cardiac syncytium and whole heart level. These experiments serve as a necessary prelude to therapeutic applications of optogenetics to the heart.

Public Health Relevance

This project offers several important innovations: 1) pioneering work in extending the use of optogenetics to control of cardiac muscle; 2) validation of a new approach to optogenetics - a non-viral cell delivery with translational potential for cardiac pacing; 3) quantitative biophysical analysis of light-sensitive ion channels and development of mathematical and experimental tools to facilitate optogenetic investigation and optimize optical stimulation beyond the cardiac field.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
7R01HL111649-05
Application #
8990497
Study Section
Electrical Signaling, Ion Transport, and Arrhythmias Study Section (ESTA)
Program Officer
Danthi, Narasimhan
Project Start
2012-01-15
Project End
2017-05-31
Budget Start
2016-06-10
Budget End
2017-05-31
Support Year
5
Fiscal Year
2016
Total Cost
Indirect Cost

  Institution

Name
George Washington University
Department
Engineering (All Types)
Type
Biomed Engr/Col Engr/Engr Sta
DUNS #
043990498
City
Washington
State
DC
Country
United States
Zip Code
20052

  Publications

Klimas, Aleksandra; Ambrosi, Christina M; Yu, Jinzhu et al. (2016) OptoDyCE as an automated system for high-throughput all-optical dynamic cardiac electrophysiology. Nat Commun 7:11542
Yu, Jinzhu; Entcheva, Emilia (2016) Inscribing Optical Excitability to Non-Excitable Cardiac Cells: Viral Delivery of Optogenetic Tools in Primary Cardiac Fibroblasts. Methods Mol Biol 1408:303-17
Entcheva, Emilia; Bub, Gil (2016) All-optical control of cardiac excitation: combined high-resolution optogenetic actuation and optical mapping. J Physiol 594:2503-10
Yu, Jinzhu; Chen, Kay; Lucero, Rachel V et al. (2015) Cardiac Optogenetics: Enhancement by All-trans-Retinal. Sci Rep 5:16542
Burton, Rebecca A B; Klimas, Aleksandra; Ambrosi, Christina M et al. (2015) Optical control of excitation waves in cardiac tissue. Nat Photonics 9:813-816
Boyle, Patrick M; Karathanos, Thomas V; Entcheva, Emilia et al. (2015) Computational modeling of cardiac optogenetics: Methodology overview & review of findings from simulations. Comput Biol Med 65:200-8
Ambrosi, Christina M; Boyle, Patrick M; Chen, Kay et al. (2015) Optogenetics-enabled assessment of viral gene and cell therapy for restoration of cardiac excitability. Sci Rep 5:17350
Williams, John C; Entcheva, Emilia (2015) Optogenetic versus Electrical Stimulation of Human Cardiomyocytes: Modeling Insights. Biophys J 108:1934-45
Ambrosi, Christina M; Entcheva, Emilia (2014) Optogenetic control of cardiomyocytes via viral delivery. Methods Mol Biol 1181:215-28
Entcheva, Emilia; Williams, John C (2014) Channelrhodopsin2 current during the action potential: ""optical AP clamp"" and approximation. Sci Rep 4:5838

Showing the most recent 10 out of 21 publications