PEER-REVIEWED PUBLICATION

2019

Biowire Model of Interstitial and Focal Cardiac Fibrosis

Wang EY, Rafatian N, et al.

ACS Central Science

University of Toronto, Toronto General Research Institute, University of Oxford, McGill University, York University

RESEARCH SUMMARY
This paper presents a human cardiac fibrosis disease model built on the Biowire II heart-on-a-chip platform, where engineered cardiac tissues are suspended between elastic POMaC wires that enable noninvasive, repeated functional readouts based on wire deflection. By tuning cardiomyocyte–fibroblast composition to generate normal vs fibrotic tissues, the authors recapitulate hallmark fibrosis phenotypes including increased collagen deposition, myofibroblast activation, elevated passive tension, reduced active force, and electrophysiological dysfunction/arrhythmogenic behavior. The study also constructs an integrated scar–myocardium (heteropolar) model combining healthy and fibrotic tissue compartments to mimic regional heterogeneity (scar, border zone, adjacent myocardium). Finally, the platform is used for proof-of-concept antifibrotic compound evaluation (furin inhibition), using functional biomechanics (especially passive tension) plus collagen readouts to assess treatment timing effects.

CELLSCALE INSTRUMENT USED

Custom

A customized CellScale MicroSquisher was used to directly measure the elastic modulus (Young’s modulus) of engineered Biowire tissues via longitudinal stretching tests in culture media. In this protocol, one end of the tissue was anchored and the MicroSquisher’s tungsten probe displaced the opposite end at a controlled rate while recording force and displacement, enabling construction of stress–strain curves and extraction of modulus from the initial linear region (reported up to ~15% strain). These CellScale-derived tissue stiffness measurements were used to quantitatively demonstrate fibrosis-associated tissue stiffening and to link compositional remodeling (collagen accumulation and myofibroblast enrichment) to biomechanical changes in the engineered myocardium—supporting the study’s core claims that the model reproduces contractile, biomechanical, and electromechanical hallmarks of fibrotic heart disease.
AUTHORS

Erika Yan Wang; Naimeh Rafatian; Yimu Zhao; Angela Lee; Benjamin Fook Lun Lai; Rick Xingze Lu; Danica Jekic; Locke Davenport Huyer; Ericka J. Knee-Walden; Shoumo Bhattacharya; Peter H. Backx; Milica Radisic.

PUBLICATION DETAILS
JOURNAL

ACS Central Science

YEAR

2019

INSTITUTIONS

University of Toronto, Toronto General Research Institute, University of Oxford, McGill University, York University

COUNTRIES

Canada, United Kingdom

INSTRUMENT USED

Custom

TESTING METHODS

Micro-Mechanical TestingTensile Testing

RESEARCH APPLICATIONS

Cardiac Tissue Engineering & MechanicsDrug Screening & Drug Delivery MechanicsFibrosis & Tissue RemodelingMechanotransductionOrgan-On-A-Chip SystemsStem Cell Mechanobiology

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