Real-time physiological sensor-based liver-on-chip device for monitoring drug toxicity

Organ-on-chip models, known as microphysiological systems, are created to mimic the anatomy and physiology of a human organ at the micro-level. Besides being pivotal in the reverse engineering of human organs and pathogenesis studies, they serve as an alternative to animal testing and the developmen...

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Veröffentlicht in:Journal of micromechanics and microengineering 2020-11, Vol.30 (11), p.115013
Hauptverfasser: Farooqi, Hafiz Muhammad Umer, Khalid, Muhammad Asad Ullah, Kim, Kyung Hwan, Lee, Sun Ryung, Choi, Kyung Hyun
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container_issue 11
container_start_page 115013
container_title Journal of micromechanics and microengineering
container_volume 30
creator Farooqi, Hafiz Muhammad Umer
Khalid, Muhammad Asad Ullah
Kim, Kyung Hwan
Lee, Sun Ryung
Choi, Kyung Hyun
description Organ-on-chip models, known as microphysiological systems, are created to mimic the anatomy and physiology of a human organ at the micro-level. Besides being pivotal in the reverse engineering of human organs and pathogenesis studies, they serve as an alternative to animal testing and the development of pharmaceutics. Monitoring the extracellular stromal environment is the basis for gaining in-depth knowledge of the pathophysiology of cell culture. Hence, it is extensively employed as an essential tool in the fields of organ-on-chip and in vitro toxicology. In this study, we explore the vitality of a microfluidic system for the automated, online detection of drug-induced physical changes in cellular viability by continual monitoring of a microfluidic 2D monolayer cell culture. Trans-epithelial electrical resistance (TEER) values and pH changes of the immortal HepG2 cell line were measured continuously using microfluidic-based electrical and photoelectric sensors. A chip-embedded transparent, flat, non-toxic sensor and in-house 3D manufactured portable digital microscope supersedes the conventional manual, expensive confocal microscopic assays, and off-line operated isolated sensor systems. The cytotoxicity was induced by various concentrations of doxorubicin, epirubicin and lapatinib, and the acute metabolic and physical response of cells was examined by detecting the variations in TEER, pH and other biological markers. Thus, our liver-on-chip device provides real-time online data on drug-induced liver injury in vitro.
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subjects embedded sensor
HepG2 cells
organ-on-chip
real-time monitoring
trans-epithelial electrical resistance
title Real-time physiological sensor-based liver-on-chip device for monitoring drug toxicity
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