Doug Vincent scite author profile

Doug Vincent

4Publications

13Citation Statements Received

95Citation Statements Given

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Colgate-Palmolive (United States)

Publications

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Acute Response of Human Aortic Endothelial Cells to Loss of Pulsatility as Seen during Cardiopulmonary Bypass

Nguyen

Donoghue

Giridharan

et al. 2021

Cells Tissues Organs

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Cardiopulmonary bypass (CPB) results in short-term (3–5 h) exposure to flow with diminished pulsatility often referred to as “continuous flow”. It is unclear if short-term exposure to continuous flow influences endothelial function, particularly, changes in levels of pro-inflammatory and pro-angiogenic cytokines. In this study, we used the endothelial cell culture model (ECCM) to evaluate if short-term (≤5 h) reduction in pulsatility alters levels of pro-inflammatory/pro-angiogenic cytokine levels. Human aortic endothelial cells (HAECs) cultured within the ECCM provide a simple model to evaluate endothelial cell function in the absence of confounding factors. HAECs were maintained under normal pulsatile flow for 24 h and then subjected to continuous flow (diminished pulsatile pressure and flow) as observed during CPB for 5 h. The ECCM replicated pulsatility and flow morphologies associated with normal hemodynamic status and CPB as seen with clinically used roller pumps. Levels of angiopoietin-2 (ANG-2), vascular endothelial growth factor-A (VEGF-A), and hepatocyte growth factor were lower in the continuous flow group in comparison to the pulsatile flow group whereas the levels of endothelin-1 (ET-1), granulocyte colony stimulating factor, interleukin-8 (IL-8) and placental growth factor were higher in the continuous flow group in comparison to the pulsatile flow group. Immunolabelling of HAECs subjected to continuous flow showed a decrease in expression of ANG-2 and VEGF-A surface receptors, tyrosine protein kinase-2 and Fms-related receptor tyrosine kinase-1, respectively. Given that the 5 h exposure to continuous flow is insufficient for transcriptional regulation, it is likely that pro-inflammatory/pro-angiogenic signaling observed was due to signaling molecules stored in Weible-Palade bodies (ET-1, IL-8, ANG-2) and via HAEC binding/uptake of soluble factors in media. These results suggest that even short-term exposure to continuous flow can potentially activate pro-inflammatory/pro-angiogenic signaling in cultured HAECs and pulsatile flow may be a successful strategy in reducing the undesirable sequalae following continuous flow CPB.

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In Vitro Examination of the VentriFlo True Pulse Pump for Failing Fontan Support

Trusty

Tree

Vincent³

et al. 2018

Artificial Organs

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The current methodology of Fontan palliation results in a one "pump" circulatory system with passive flow to the lungs. Inherent hemodynamic differences exist between a biventricular circulatory system and this modified physiology, leading to a host of long-term complications. Mechanical circulatory support (MCS) is a potential option to combat these pathophysiological conditions. In this study, we examine the VentriFlo True Pulse Pump as a MCS option to support a failing Fontan patient. An in vitro circulatory loop was used to model a failing Fontan patient, reproducing pathophysiological pressures and flow rates. The VentriFlo True Pulse Pump was positioned as a right sided support, testing multiple cannulation and baffle restriction strategies, as well as various pumping parameters including flow rate, frequency, stroke volume and the ejection to filling time ratio. A 10 mm Hg decrease in IVC pressure and 0.75 L/min increase in cardiac output were achieved using a complete baffle restriction strategy. Additional cannulation and banding strategies were not as successful. Pump flow rate and frequency significantly impacted hemodynamics, while the ejection to filling time ratio did not. Though not ideal, complete baffle restriction was necessary to achieve successful support. The ability to tune individual pumping parameters for a given MCS device will have a substantial impact on the pressures and flow augmentation seen in a Fontan circulation. Both future pump design and off-label VADs for Fontan use should consider the pump configuration and parameter combinations presented here, which offered successful support. Key Words: Congenital heart disease-Fontan-Mechanical circulatory support-Single ventricle-Ventricular assist device.The current methodology of Fontan palliation results in a one "pump" circulatory system with passive, nonpulsatile flow to the lungs. Inherent hemodynamic differences exist between a biventricular circulatory system and this modified physiology, including elevated central venous pressures (CVP) and insufficient cardiac output (CO), as well as a myriad of ventricular function, impedance and congestion issues (1-5). As these patients survive into early adulthood, numerous long-term complications are common, with liver disease, protein losing enteropathy and plastic bronchitis among the most prevalent (3,(6)(7)(8)(9).In order to moderate these long-term problems, a circulatory correction rather than palliation is needed; and with a limited number of immediate heart transplants available, mechanical circulatory support (MCS) has become a potential option as a bridge-to-transplant therapy. However, the use of MCS in Fontan patients poses unique challenges including low preload and afterload, an absent upstream capacitance chamber, and potentially difficult anatomic implementation (10).The two approaches for Fontan MCS include (i) designing a new pump specifically for Fontan use, or (ii) using an existing pump off-label with the hope that it can provide adequate support in an environment othe...

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P25: Assessment of VentriFlo True Pulse Pump in Cardiopulmonary Bypass Circuit In vivo

Kuroda

Vincent

O’Brien

et al. 2023

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P40: Minimal hemolysis and platelet activation with VentriFlo True Pulse Pump, a novel pulsatile extracorporeal blood pump

Vincent

Kuroda

Goodin

et al. 2023

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Doug Vincent

Acute Response of Human Aortic Endothelial Cells to Loss of Pulsatility as Seen during Cardiopulmonary Bypass

In Vitro Examination of the VentriFlo True Pulse Pump for Failing Fontan Support

P25: Assessment of VentriFlo True Pulse Pump in Cardiopulmonary Bypass Circuit In vivo

P40: Minimal hemolysis and platelet activation with VentriFlo True Pulse Pump, a novel pulsatile extracorporeal blood pump

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