Screening for variable drug responses using human iPSC cohorts

bioRxiv (Cold Spring Harbor Laboratory)(2023)

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Abstract
We have used a cohort of human induced pluripotent stem cell (hiPSC) lines to develop a laboratory-based drug screening platform to predict variable drug responses of potential clinical relevance. Our approach is based on the findings that hiPSC lines reflect the genetic identity of the donor and that pluripotent hiPSC lines express a broad repertoire of gene transcripts and proteins. We demonstrate that a cohort of hiPSC lines from different donors can be screened efficiently in their pluripotent state using high-throughput cell painting assays, allowing detection of variable phenotypic responses to a wide range of clinically approved drugs, across multiple disease areas. Furthermore, we provide information on mechanisms of drug-cell interactions underlying the observed variable responses by using quantitative proteomic analysis to compare sets of hiPSC lines that had been stratified objectively using cell painting data. We propose that information derived from comparative drug screening using curated libraries of hiPSC lines can help to increase the success rate of drug development pipelines and improve the delivery of safe new drugs suitable for a broad range of genetic backgrounds and gender diversity within human populations. ### Competing Interest Statement Some of the work reported here is included in pending patent application, WO2022189453A1. MP, AIL, and JRS declare a conflict of interest as founders of Tartan Cell Technologies, Ltd.
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Key words
variable drug responses,ipsc cohorts,screening
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