Introducing an automated high content confocal imaging approach for Organs-on-Chips

共焦 内容(测量理论) 共焦显微镜 纳米技术 计算机科学 工艺工程 化学 材料科学 细胞生物学 工程类 生物 物理 光学 数学分析 数学
作者
S Peel,Adam Corrigan,Beate Ehrhardt,Kyung‐Jin Jang,Pedro Caetano-Pinto,Matthew Boeckeler,Jonathan E. Rubins,Konstantia Kodella,Debora B. Petropolis,Janey Ronxhi,Gauri Kulkarni,Alison J. Foster,Dominic P. Williams,Kyung‐Jin Jang,Lorna Ewart
出处
期刊:Lab on a Chip [The Royal Society of Chemistry]
卷期号:19 (3): 410-421 被引量:85
标识
DOI:10.1039/c8lc00829a
摘要

Organ-Chips are micro-engineered systems that aim to recapitulate the organ microenvironment. Implementation of Organ-Chips within the pharmaceutical industry aims to improve the probability of success of drugs reaching late stage clinical trial by generating models for drug discovery that are of human origin and have disease relevance. We are adopting the use of Organ-Chips for enhancing pre-clinical efficacy and toxicity evaluation and prediction. Whilst capturing cellular phenotype via imaging in response to drug exposure is a useful readout in these models, application has been limited due to difficulties in imaging the chips at scale. Here we created an end-to-end, automated workflow to capture and analyse confocal images of multicellular Organ-Chips to assess detailed cellular phenotype across large batches of chips. By automating this process, we not only reduced acquisition time, but we also minimised process variability and user bias. This enabled us to establish, for the first time, a framework of statistical best practice for Organ-Chip imaging, creating the capability of using Organ-Chips and imaging for routine testing in drug discovery applications that rely on quantitative image data for decision making. We tested our approach using benzbromarone, whose mechanism of toxicity has been linked to mitochondrial damage with subsequent induction of apoptosis and necrosis, and staurosporine, a tool inducer of apoptosis. We also applied this workflow to assess the hepatotoxic effect of an active AstraZeneca drug candidate illustrating its applicability in drug safety assessment beyond testing tool compounds. Finally, we have demonstrated that this approach could be adapted to Organ-Chips of different shapes and sizes through application to a Kidney-Chip.
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