Engineering a High Throughput Lung-on-a-Chip System with Intravascular Shear Stress to Better Represent In Vivo Lung Physiology and Characterize Acute Respiratory Distress Syndrome

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dc.contributor.advisorGillrie, Mark Robert
dc.contributor.authorVolek, Kelsie Lena
dc.contributor.committeememberYipp, Bryan George
dc.contributor.committeememberKim, Keekyoung
dc.date2024-11
dc.date.accessioned2024-08-20T18:53:27Z
dc.date.available2024-08-20T18:53:27Z
dc.date.issued2024-08-13
dc.description.abstractAcute Respiratory Distress Syndrome (ARDS) is an inflammatory condition often requiring mechanical ventilation due to severe lung injury, frequently leading to fatal outcomes. Traditional models, including animal studies and 2D cell cultures, fail to capture the complexities of human lung physiology, limiting our understanding of ARDS. To address these limitations, we developed a sophisticated lung-on-a-chip (LoC) platform integrating human endothelial cells forming microvessels within a fibrin hydrogel containing fibroblasts alongside an alveolar epithelial cell-lined air-liquid interface. We use this novel LoC to investigate ARDS disease mechanisms and drug responses. First, we demonstrate marked microvascular damage and tissue biomechanical changes induced by double-stranded RNA (PolyI:C), a common inflammatory agonist which mimics viral lung infections. Additionally, we identified a clinically available drug that blocks JAK/STAT inflammatory signaling, ruxolitinib, and prevented this lung damage. With the addition of continuous vascular fluid flow (and hence shear stress), we found enhanced vascularization under standard conditions but retained disruption following polyI:C treatment. A computational fluid dynamics model was also used to provide insight into fluid velocities and shear stresses present in the ‘healthy’ LoC, parameters that are difficult to measure using empiric testing. This modeling along with empiric vascular bulk flow and bead velocity measurements, points towards significant intravascular obstruction during viral lung infection. These results significantly advance our understanding of lung physiology and ARDS disease progression, paving the way for novel therapeutic interventions in respiratory health, particularly targeting the pulmonary vasculature.
dc.identifier.citationVolek, K. L. (2024). Engineering a high throughput lung-on-a-chip system with intravascular shear stress to better represent in vivo lung physiology and characterize acute respiratory distress syndrome (Master's thesis, University of Calgary, Calgary, Canada). Retrieved from https://prism.ucalgary.ca.
dc.identifier.urihttps://hdl.handle.net/1880/119432
dc.language.isoen
dc.publisher.facultyGraduate Studies
dc.publisher.institutionUniversity of Calgary
dc.rightsUniversity of Calgary graduate students retain copyright ownership and moral rights for their thesis. You may use this material in any way that is permitted by the Copyright Act or through licensing that has been assigned to the document. For uses that are not allowable under copyright legislation or licensing, you are required to seek permission.
dc.subjectLung
dc.subjectMicrophysiologic Systems
dc.subjectOrgan on Chip
dc.subject.classificationImmunology
dc.subject.classificationEducation--Health
dc.subject.classificationEngineering--Biomedical
dc.titleEngineering a High Throughput Lung-on-a-Chip System with Intravascular Shear Stress to Better Represent In Vivo Lung Physiology and Characterize Acute Respiratory Distress Syndrome
dc.typemaster thesis
thesis.degree.disciplineEngineering – Biomedical
thesis.degree.grantorUniversity of Calgary
thesis.degree.nameMaster of Science (MSc)
ucalgary.thesis.accesssetbystudentI require a thesis withhold – I need to delay the release of my thesis due to a patent application, and other reasons outlined in the link above. I have/will need to submit a thesis withhold application.
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