Such data can be generated easily & cheaply, but historically hasn’t been ideal for large-scale functional genomics because imaging experiments could not use pooled genetic perturbation libraries (no way to optically determine which cell received which perturbation). - ThreadSky

jtneal.bsky.social • 30 days ago

Such data can be generated easily & cheaply, but historically hasn’t been ideal for large-scale functional genomics because imaging experiments could not use pooled genetic perturbation libraries (no way to optically determine which cell received which perturbation).

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jtneal.bsky.social•30 days ago

Fortunately, the Blainey Lab and others solved this problem by developing methods to sequence individual perturbation barcodes using in situ sequencing, so we can now assign quantitative cell phenotypes AND barcodes to individual cells, enabling optical pooled screens. https://www.cell.com/cell/fulltext/S0092-8674(19)31067-0

jtneal.bsky.social•30 days ago

So, we teamed up with Anne and Paul’s lab, along with Calvin Jan at Calico, with the aim of building an accessible & unbiased high-content cell profiling platform that could be applied to genome-scale CRISPR screens (Project PERISCOPE).

jtneal.bsky.social•30 days ago

To do this, we first built a variant of the Cell Painting panel that allowed destaining of fluorophores from a subset of markers (via cleavable disulfide or azidomethyl linker) so that we could perform four color in situ sequencing-by-synthesis without fluorescence overlap.

jtneal.bsky.social•30 days ago

We ( @erinweisbart.bsky.social , @bethcimini.bsky.social , Greg Way) also built scalable, distributed open source analysis pipelines for alignment/cropping/background correction/barcode calling/etc. allowing us to turn millions of fluorescence images into sgRNA-assigned single cell profiles

jtneal.bsky.social•30 days ago

We then applied these methods to execute 3 whole genome (80,862 sgRNAs targeting 20,393 genes) CRISPR KO screens in A549, and HeLa (paired screens with different growth media).

jtneal.bsky.social•30 days ago

These screens generated rich phenotypic data, enabling us to use morphological profile similarity to explore relationships between perturbed genes such as clustering protein complex members by morphological similarity, and capturing membership/directionality of signaling pathways.

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