Quantitative design strategies for fine control of oxygen in microfluidic systems

Hypoxia, or low oxygen (O 2 ) tension, is a central feature of important disease processes including wound healing and cancer. Subtle temporal and spatial variations (≤1% change) in the concentration of O 2 can profoundly impact gene expression and cellular functions. Sodium sulfite reacts rapidly w...

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Bibliographic Details
Published in:Lab on a chip 2020-08, Vol.2 (16), p.336-35
Main Authors: Shirure, Venktesh S, Lam, Sandra F, Shergill, Bhupinder, Chu, Yunli E, Ng, Natalie R, George, Steven C
Format: Article
Language:English
Subjects:
Cancer
Chemical reactions
Fluid dynamics
Fluid flow
Gene expression
Hypoxia
Mass transfer
Material properties
Microfluidics
Phosphorescence
Reaction kinetics
Sodium sulfite
Wound healing
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Summary:Hypoxia, or low oxygen (O 2 ) tension, is a central feature of important disease processes including wound healing and cancer. Subtle temporal and spatial variations (≤1% change) in the concentration of O 2 can profoundly impact gene expression and cellular functions. Sodium sulfite reacts rapidly with O 2 and can be used to lower the O 2 concentrations in PDMS-based tissue culture systems without exposing the cell culture to the chemical reaction. By carefully considering the mass transfer and reaction kinetics of sodium sulfite and O 2 , we developed a flexible theoretical framework to design an experimental microfluidic system that provides fine spatial and temporal control of O 2 tension. The framework packages the dimensions, fluid flow, reaction rates, concentrations, and material properties of the fluidic lines and device into dimensionless groups that facilitate scaling and design. We validated the theoretical results by experimentally measuring O 2 tension throughout the experimental system using phosphorescence lifetime imaging. We then tested the system by examining the impact of hypoxia inducible factor-1α (HIF-1α) on the proliferation and migration of MDA-MB-231 breast cancer cells. Using this system, we demonstrate that mild constant hypoxia (≤4%) induces HIF-1α mediated functional changes in the tumor cells. Furthermore, slow (>12 hours), but not rapid (
ISSN:1473-0197
1473-0189
DOI:10.1039/d0lc00350f