Integrating Computational and Biological Hemodynamic Approaches to Improve Modeling of Atherosclerotic Arteries

Author:

Vuong Thao Nhu Anne Marie1,Bartolf‐Kopp Michael2ORCID,Andelovic Kristina2ORCID,Jungst Tomasz23ORCID,Farbehi Nona145ORCID,Wise Steven G.6ORCID,Hayward Christopher7,Stevens Michael Charles1ORCID,Rnjak‐Kovacina Jelena148ORCID

Affiliation:

1. Graduate School of Biomedical Engineering University of New South Wales Sydney 2052 Australia

2. Department of Functional Materials in Medicine and Dentistry Institute of Functional Materials and Biofabrication (IFB) KeyLab Polymers for Medicine of the Bavarian Polymer Institute (BPI) University of Würzburg Pleicherwall 2 97070 Würzburg Germany

3. Department of Orthopedics, Regenerative Medicine Center Utrecht University Medical Center Utrecht Utrecht 3584 Netherlands

4. Tyree Institute of Health Engineering University of New South Wales Sydney NSW 2052 Australia

5. Garvan Weizmann Center for Cellular Genomics Garvan Institute of Medical Research Sydney NSW 2010 Australia

6. School of Medical Sciences University of Sydney Sydney NSW 2006 Australia

7. St Vincent's Hospital Sydney Victor Chang Cardiac Research Institute Sydney 2010 Australia

8. Australian Centre for NanoMedicine (ACN) University of New South Wales Sydney NSW 2052 Australia

Abstract

AbstractAtherosclerosis is the primary cause of cardiovascular disease, resulting in mortality, elevated healthcare costs, diminished productivity, and reduced quality of life for individuals and their communities. This is exacerbated by the limited understanding of its underlying causes and limitations in current therapeutic interventions, highlighting the need for sophisticated models of atherosclerosis. This review critically evaluates the computational and biological models of atherosclerosis, focusing on the study of hemodynamics in atherosclerotic coronary arteries. Computational models account for the geometrical complexities and hemodynamics of the blood vessels and stenoses, but they fail to capture the complex biological processes involved in atherosclerosis. Different in vitro and in vivo biological models can capture aspects of the biological complexity of healthy and stenosed vessels, but rarely mimic the human anatomy and physiological hemodynamics, and require significantly more time, cost, and resources. Therefore, emerging strategies are examined that integrate computational and biological models, and the potential of advances in imaging, biofabrication, and machine learning is explored in developing more effective models of atherosclerosis.

Funder

Australian Research Council

University of New South Wales

Publisher

Wiley

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