Litcius/Paper detail

High-content live-cell multiplex screen for chemogenomic compound annotation based on nuclear morphology

Amelie Tjaden, Robert T. Giessmann, Stefan Knapp, Martin Schröder, Susanne Müller

2022STAR Protocols19 citationsDOIOpen Access PDF

Abstract

Well-characterized small molecules enable the study of cell processes and facilitate target validation. Here, we describe a high-content multiplex screen to investigate cell viability over 48 h, which can be combined with investigating phenotypic features, such as tubulin binding and mitochondrial content, as initial cellular quality control of diverse compounds. The protocol is on a live-cell basis and easily adaptable and scalable. It details cell preparation, compound handling, plate layout configuration, image acquisition with the CQ1, and data analysis using the CellPathfinder software. For complete details on the use and execution of this protocol, please refer to Tjaden et al. (2022).

Topics & Concepts

High-content screeningMultiplexComputer scienceScalabilityProtocol (science)AnnotationSoftwareCellComputational biologyBioinformaticsBiologyArtificial intelligenceGeneticsOperating systemAlternative medicinePathologyMedicineCell Image Analysis TechniquesSingle-cell and spatial transcriptomicsCancer Genomics and Diagnostics