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A scalable platform for efficient CRISPR-Cas9 chemical-genetic screens of DNA damage-inducing compounds.


ABSTRACT: Current approaches to define chemical-genetic interactions (CGIs) in human cell lines are resource-intensive. We designed a scalable chemical-genetic screening platform by generating a DNA damage response (DDR)-focused custom sgRNA library targeting 1011 genes with 3033 sgRNAs. We performed five proof-of-principle compound screens and found that the compounds' known modes-of-action (MoA) were enriched among the compounds' CGIs. These scalable screens recapitulated expected CGIs at a comparable signal-to-noise ratio (SNR) relative to genome-wide screens. Furthermore, time-resolved CGIs, captured by sequencing screens at various time points, suggested an unexpected, late interstrand-crosslinking (ICL) repair pathway response to camptothecin-induced DNA damage. Our approach can facilitate screening compounds at scale with 20-fold fewer resources than commonly used genome-wide libraries and produce biologically informative CGI profiles.

SUBMITTER: Lin K 

PROVIDER: S-EPMC10828508 | biostudies-literature | 2024 Jan

REPOSITORIES: biostudies-literature

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A scalable platform for efficient CRISPR-Cas9 chemical-genetic screens of DNA damage-inducing compounds.

Lin Kevin K   Chang Ya-Chu YC   Billmann Maximilian M   Ward Henry N HN   Le Khoi K   Hassan Arshia Z AZ   Bhojoo Urvi U   Chan Katherine K   Costanzo Michael M   Moffat Jason J   Boone Charles C   Bielinsky Anja-Katrin AK   Myers Chad L CL  

Scientific reports 20240130 1


Current approaches to define chemical-genetic interactions (CGIs) in human cell lines are resource-intensive. We designed a scalable chemical-genetic screening platform by generating a DNA damage response (DDR)-focused custom sgRNA library targeting 1011 genes with 3033 sgRNAs. We performed five proof-of-principle compound screens and found that the compounds' known modes-of-action (MoA) were enriched among the compounds' CGIs. These scalable screens recapitulated expected CGIs at a comparable s  ...[more]

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