Literature DB >> 33363131

Mechanical Stimulation: A Crucial Element of Organ-on-Chip Models.

Clare L Thompson1, Su Fu1, Martin M Knight1, Stephen D Thorpe2.   

Abstract

Organ-on-chip (OOC) systems recapitulate key biological processes and responses in vitro exhibited by cells, tissues, and organs in vivo. Accordingly, these models of both health and disease hold great promise for improving fundamental research, drug development, personalized medicine, and testing of pharmaceuticals, food substances, pollutants etc. Cells within the body are exposed to biomechanical stimuli, the nature of which is tissue specific and may change with disease or injury. These biomechanical stimuli regulate cell behavior and can amplify, annul, or even reverse the response to a given biochemical cue or drug candidate. As such, the application of an appropriate physiological or pathological biomechanical environment is essential for the successful recapitulation of in vivo behavior in OOC models. Here we review the current range of commercially available OOC platforms which incorporate active biomechanical stimulation. We highlight recent findings demonstrating the importance of including mechanical stimuli in models used for drug development and outline emerging factors which regulate the cellular response to the biomechanical environment. We explore the incorporation of mechanical stimuli in different organ models and identify areas where further research and development is required. Challenges associated with the integration of mechanics alongside other OOC requirements including scaling to increase throughput and diagnostic imaging are discussed. In summary, compelling evidence demonstrates that the incorporation of biomechanical stimuli in these OOC or microphysiological systems is key to fully replicating in vivo physiology in health and disease.
Copyright © 2020 Thompson, Fu, Knight and Thorpe.

Entities:  

Keywords:  biomechanical stimulation; biomechanics; fluid shear; mechanobiology; microphysiological systems; organ-on-chip; pre-clinical model; tensile strain

Year:  2020        PMID: 33363131      PMCID: PMC7758201          DOI: 10.3389/fbioe.2020.602646

Source DB:  PubMed          Journal:  Front Bioeng Biotechnol        ISSN: 2296-4185


  170 in total

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