A novel standalone microfluidic device for local control of oxygen tension for intestinal‐bacteria interactions

氧气 氧气张力 微流控 极限氧浓度 无氧运动 细菌 化学 缺氧(环境) 厌氧菌 生物物理学 细胞生物学 生物 纳米技术 材料科学 有机化学 遗传学 生理学
作者
Chengyao Wang,Thao Dang,Jasmine Baste,Advait Anil Joshi,Abhinav Bhushan
出处
期刊:The FASEB Journal [Wiley]
卷期号:35 (2): e21291-e21291 被引量:23
标识
DOI:10.1096/fj.202001600rr
摘要

Abstract The intestinal environment is unique because it supports the intestinal epithelial cells under a normal oxygen environment and the microbiota under an anoxic environment. Due to importance of understanding the interactions between the epithelium and the microbiota, there is a strong need for developing representative and simple experimental models. Current approaches do not capture the partitioned oxygen environment, require external anaerobic chambers, or are complex. Another major limitation is that with the solutions that can mimic this oxygen environment, the oxygenation level of the epithelial cells is not known, raising the question whether the cells are hypoxic or not. We report standalone microfluidic devices that form a partitioned oxygen environment without the use of an external anaerobic chamber or oxygen scavengers to coculture intestinal epithelial and bacterial cells. By changing the thickness of the device cover, the oxygen tension in the chamber was modulated. We verified the oxygen levels using several tests: microscale oxygen sensitive sensors which were integrated within the devices, immunostaining of Caco‐2 cells to determine hypoxia levels, and genetically encoded bacteria to visualize the growth. Collectively, these methods monitored oxygen concentrations in the devices more comprehensively than previous reports and allowed for control of oxygen tension to match the requirements of both intestinal cells and anaerobic bacteria. Our experimental model is supported by the mathematical model that considered diffusion of oxygen into the top chamber. This allowed us to experimentally determine the oxygen consumption rate of the intestinal epithelial cells under perfusion.
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