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Valve Endothelial Cell Exposure to High Levels of Flow Oscillations Exacerbates Valve Interstitial Cell Calcification. | LitMetric

AI Article Synopsis

  • The aortic valve ensures one-way blood flow from the left ventricle to the aorta, relying on its leaflets and a structure made up of valve endothelial cells (VECs) and valve interstitial cells (VICs).
  • Abnormal communication between VECs and VICs can lead to calcification of the aortic valve, particularly due to flow irregularities that affect VEC function and subsequently alter VIC behavior.
  • The study measured flow oscillations VECs experienced and found that under maximum oscillations, VICs showed increased calcification, linking this effect to specific regions of the aortic valve known for severe calcified deposits, paving the way for future research into treatment options.

Article Abstract

The aortic valve facilitates unidirectional blood flow to the systemic circulation between the left cardiac ventricle and the aorta. The valve's biomechanical function relies on thin leaflets to adequately open and close over the cardiac cycle. A monolayer of valve endothelial cells (VECs) resides on the outer surface of the aortic valve leaflet. Deeper within the leaflet are sublayers of valve interstitial cells (VICs). Valve tissue remodeling involves paracrine signaling between VECs and VICs. Aortic valve calcification can result from abnormal paracrine communication between these two cell types. VECs are known to respond to hemodynamic stimuli, and, specifically, flow abnormalities can induce VEC dysfunction. This dysfunction can subsequently change the phenotype of VICs, leading to aortic valve calcification. However, the relation between VEC-exposed flow oscillations under pulsatile flow to the progression of aortic valve calcification by VICs remains unknown. In this study, we quantified the level of flow oscillations that VECs were exposed to under dynamic culture and then immersed VICs in VEC-conditioned media. We found that VIC-induced calcification was augmented under maximum flow oscillations, wherein the flow was fully forward for half the cardiac cycle period and fully reversed for the other half. We were able to computationally correlate this finding to specific regions of the aortic valve that experience relatively high flow oscillations and that have been shown to be associated with severe calcified deposits. These findings establish a basis for future investigations on engineering calcified human valve tissues and its potential for therapeutic discovery of aortic valve calcification.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9405348PMC
http://dx.doi.org/10.3390/bioengineering9080393DOI Listing

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