Platelet Adhesion and Activation in an ECMO Thrombosis‐on‐a‐Chip Model

Author:

Goh Tiffany1234ORCID,Gao Lingzi1234,Singh Jasneil1234ORCID,Totaro Richard56,Carey Ruaidhri6,Yang Kevin6,Cartwright Bruce57,Dennis Mark58,Ju Lining Arnold2349ORCID,Waterhouse Anna134ORCID

Affiliation:

1. School of Medical Sciences, Faculty of Medicine and Health The University of Sydney Sydney NSW 2006 Australia

2. Heart Research Institute Newtown NSW 2042 Australia

3. Charles Perkins Centre The University of Sydney Sydney NSW 2006 Australia

4. The University of Sydney Nano Institute The University of Sydney Sydney NSW 2006 Australia

5. Faculty of Medicine and Health The University of Sydney Sydney NSW 2006 Australia

6. Intensive Care Department Royal Prince Alfred Hospital Missenden Road, Camperdown Sydney NSW 2050 Australia

7. Anaesthetics Department Royal Prince Alfred Hospital Camperdown Sydney NSW 2050 Australia

8. Cardiology Department Royal Prince Alfred Hospital Missenden Road, Camperdown Sydney NSW 2050 Australia

9. School of Biomedical Engineering Faculty of Engineering The University of Sydney Darlington NSW 2008 Australia

Abstract

AbstractUse of extracorporeal membrane oxygenation (ECMO) for cardiorespiratory failure remains complicated by blood clot formation (thrombosis), triggered by biomaterial surfaces and flow conditions. Thrombosis may result in ECMO circuit changes, cause red blood cell hemolysis, and thromboembolic events. Medical device thrombosis is potentiated by the interplay between biomaterial properties, hemodynamic flow conditions and patient pathology, however, the contribution and importance of these factors are poorly understood because many in vitro models lack the capability to customize material and flow conditions to investigate thrombosis under clinically relevant medical device conditions. Therefore, an ECMO thrombosis‐on‐a‐chip model is developed that enables highly customizable biomaterial and flow combinations to evaluate ECMO thrombosis in real‐time with low blood volume. It is observed that low flow rates, decelerating conditions, and flow stasis significantly increased platelet adhesion, correlating with clinical thrombus formation. For the first time, it is found that tubing material, polyvinyl chloride, caused increased platelet P‐selectin activation compared to connector material, polycarbonate. This ECMO thrombosis‐on‐a‐chip model can be used to guide ECMO operation, inform medical device design, investigate embolism, occlusion and platelet activation mechanisms, and develop anti‐thrombotic biomaterials to ultimately reduce medical device thrombosis, anti‐thrombotic drug use and therefore bleeding complications, leading to safer blood‐contacting medical devices.

Funder

National Heart Foundation of Australia

NSW Ministry of Health

Snow Medical

University of Sydney

Ramaciotti Foundations

Publisher

Wiley

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