Abstract

Cardiovascular and pulmonary diseases are two of the most prevalent classes of disease in the US. Environmental pollutants, to include nanoscale allergens and toxins, have deleterious effects on both the healthy and diseased cardiopulmonary system. Furthermore, cardiotoxicity is one of the most prevalent causes of withdrawal of pharmaceuticals from the marketplace. Failure of drugs in the clinic, or in late stage clinical trials, is a contributing factor to the increased cost of health care in the US, as he cost of drug development increases to accommodate such product failures. To date, the model of efficacy and toxicity testing has been largely based on a model of high quantities of low quality data gathered in vitro. Recent advances offer an alternative strategy. Soft lithography has made microscale tissue engineering possible that replicates the cellular microenvironments of healthy and diseased tissues. Microfluidic systems enable long term culture and the ability to mimic the low volume interstitial spaces found in organs and tissues. New techniques for human cell harvest thru biopsies, coupled with human embryonic stem (ES) and induced pluripotency stem (iPS) cells, all of which have some commercial availability, suggest that the animal cell lines typically used for in vitro testing can be replaced with a human surrogate. Recently, we developed a technique called muscular thin films (MTFs), a biohybrid construct composed of a 2D high fidelity, engineered tissue on an elastic polymer thin film that allows a broad spectrum of measurements within engineered muscle tissue to look at contractile and relaxed dysfunction. Combining all of these technologies into a single platform suggests that the current paradigm of high quantity, low quality data with limited applicability to the human patient can be replaced with mid-quantity, high quality data that will eventually be patient specific. Here we propose to combine these technologies to build human organ mimics that recapitulate healthy and diseased cell and tissue architectures, specifically muscular contraction of the heart, vasculature, and airway. As single organ mimics, these systems will be useful in measuring the efficacy of candidate molecules and the safety of drugs directed as therapeutics in other organ systems. When these organ mimics are combined as an ensemble of tissues on a single chip, the side effects of drugs targeted against a specific disease, for example asthma, can be assessed for cardiotoxicity. The goal of the proposed organ on chip technologies is to be used as a stand-alone, or integrated into a bigger, multi-organ system, to mimic human disease and facilitate drug discovery and toxicity screening in a faster, cheaper method than the current industrial paradigm.

Public Health Relevance

We will build microscale replicates of the human muscular tissue in the cardiac ventricle, the vascular system, and the airway on single and consolidated chips. These chips will represent both healthy and diseased human tissues and will be comprised of human cells, amenable to testing for drug efficacy and safety.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Center for Advancing Translational Sciences (NCATS)
Type
Exploratory/Developmental Cooperative Agreement Phase II (UH3)
Project #
5UH3TR000522-05
Application #
9111093
Study Section
Special Emphasis Panel (ZRG1)
Program Officer
Tagle, Danilo A
Project Start
2012-07-24
Project End
2017-06-30
Budget Start
2016-07-01
Budget End
2017-06-30
Support Year
5
Fiscal Year
2016
Total Cost
Indirect Cost

  Institution

Name
Harvard Medical School
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
047006379
City
Boston
State
MA
Country
United States
Zip Code

  Publications

Nawroth, Janna C; Scudder, Lisa L; Halvorson, Ryan T et al. (2018) Automated fabrication of photopatterned gelatin hydrogels for organ-on-chips applications. Biofabrication 10:025004
Pasqualini, Francesco Silvio; Agarwal, Ashutosh; O'Connor, Blakely Bussie et al. (2018) Traction force microscopy of engineered cardiac tissues. PLoS One 13:e0194706
Pasqualini, F S; Emmert, M Y; Parker, K K et al. (2017) Organ Chips: Quality Assurance Systems in Regenerative Medicine. Clin Pharmacol Ther 101:31-34
Lind, Johan U; Busbee, Travis A; Valentine, Alexander D et al. (2017) Instrumented cardiac microphysiological devices via multimaterial three-dimensional printing. Nat Mater 16:303-308
Lind, Johan U; Yadid, Moran; Perkins, Ian et al. (2017) Cardiac microphysiological devices with flexible thin-film sensors for higher-throughput drug screening. Lab Chip 17:3692-3703
Capulli, Andrew K; Emmert, Maximillian Y; Pasqualini, Francesco S et al. (2017) JetValve: Rapid manufacturing of biohybrid scaffolds for biomimetic heart valve replacement. Biomaterials 133:229-241
Horton, Renita E; Yadid, Moran; McCain, Megan L et al. (2016) Angiotensin II Induced Cardiac Dysfunction on a Chip. PLoS One 11:e0146415
Capulli, A K; MacQueen, L A; Sheehy, Sean P et al. (2016) Fibrous scaffolds for building hearts and heart parts. Adv Drug Deliv Rev 96:83-102
Park, Sung-Jin; Gazzola, Mattia; Park, Kyung Soo et al. (2016) Phototactic guidance of a tissue-engineered soft-robotic ray. Science 353:158-62
Aratyn-Schaus, Yvonne; Pasqualini, Francesco S; Yuan, Hongyan et al. (2016) Coupling primary and stem cell-derived cardiomyocytes in an in vitro model of cardiac cell therapy. J Cell Biol 212:389-97

Showing the most recent 10 out of 22 publications