4.6 Article

Peristaltic pumps adapted for laminar flow experiments enhance in vitro modeling of vascular cell behavior

Journal

JOURNAL OF BIOLOGICAL CHEMISTRY
Volume 298, Issue 10, Pages -

Publisher

ELSEVIER
DOI: 10.1016/j.jbc.2022.102404

Keywords

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Funding

  1. National Institutes of Health/National Institute of General Medical Sciences [R35GM133560, R35 GM137976]
  2. Cancer Research Foundation Young Investigator Award

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Endothelial cells are the primary cellular constituent of blood vessels, and studying blood flow in an intact organism is challenging. In vitro modeling of blood flow has become a powerful technique for studying signaling mechanisms in endothelial cells. This study outlines a method to adapt commercially available pumps to simulate laminar flow conditions, allowing for functional studies on shear forces in vascular architecture.
Endothelial cells (ECs) are the primary cellular constituent of blood vessels that are in direct contact with hemodynamic forces over their lifetime. Throughout the body, vessels experience different blood flow patterns and rates that alter vascular architecture and cellular behavior. Because of the complexities of studying blood flow in an intact organism, particularly during development, the field has increasingly relied on in vitro modeling of blood flow as a powerful technique for studying hemodynamic-dependent signaling mechanisms in ECs. While commercial flow systems that recirculate fluids exist, many commercially available pumps are peristaltic and best model pulsatile flow conditions. However, there are many important situations in which ECs experience laminar flow conditions in vivo, such as along long straight stretches of the vasculature. To understand EC function under these contexts, it is important to be able to reproducibly model laminar flow conditions in vitro. Here, we outline a method to reliably adapt commercially available peristaltic pumps to study laminar flow conditions. Our proof-of-concept study focuses on 2D models but could be further adapted to 3D environments to better model in vivo scenarios, such as organ development. Our studies make significant inroads into solving technical challenges associated with flow modeling and allow us to conduct functional studies toward understanding the mechanistic role of shear forces on vascular architecture, cellular behavior, and remodeling in diverse physiological contexts.

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