CRISPR/Cas13 effectors have differing extents of off-target effects that limit their utility in eukaryotic cells

Ai, Yuxi; Liang, Dongming; Wilusz, Jeremy E.

doi:10.1101/2021.11.04.467323

Cited by 5 publications

References 61 publications

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Deep learning and CRISPR-Cas13d ortholog discovery for optimized RNA targeting

Wei

Lotfy

Faizi

et al. 2021

Preprint

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Transcriptome engineering requires flexible RNA-targeting technologies that can perturb mammalian transcripts in a robust and scalable manner. CRISPR systems that natively target RNA molecules, such as Cas13 enzymes, are enabling rapid progress in the investigation of RNA biology and advancement of RNA therapeutics. Here, we sought to develop a Cas13 platform for high-throughput phenotypic screening and elucidate the design principles underpinning its RNA targeting efficiency. We employed the RfxCas13d (CasRx) system in a positive selection screen by tiling 55 known essential genes with single nucleotide resolution. Leveraging this dataset of over 127,000 guide RNAs, we systematically compared a series of linear regression and machine learning algorithms to train a convolutional neural network (CNN) model that is able to robustly predict guide RNA performance based on guide sequence alone. We further incorporated secondary features including secondary structure, free energy, target site position, and target isoform percent. To evaluate model performance, we conducted orthogonal screens via cell surface protein knockdown. The final CNN model is able to predict highly effective guide RNAs (gRNAs) within each transcript with >90% accuracy in this independent test set. To provide user interpretability, we evaluate feature contributions using both integrated gradients and SHapley Additive exPlanations (SHAP). We identify a specific sequence motif at guide position 15-24 along with selected secondary features to be predictive of highly efficient guides. Taken together, we derive Cas13d guide design rules from large-scale screen data, release a guide design tool (http://rnatargeting.org) to advance the RNA targeting toolbox, and describe a path for systematic development of deep learning models to predict CRISPR activity.

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Deep learning and CRISPR-Cas13d ortholog discovery for optimized RNA targeting

Wei

Lotfy

Faizi

et al. 2021

Preprint

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Spatio-temporal, optogenetic control of gene expression in organoids

Legnini

Emmenegger

Wurmus

et al. 2021

Preprint

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Quantifying gene expression in space, for example by spatial transcriptomics, is essential for describing the biology of cells and their interactions in complex tissues. Perturbation experiments, at single-cell resolution and conditional on both space and time, are necessary for dissecting the molecular mechanisms of these interactions. To this aim, we combined optogenetics and CRISPR technologies to activate or knock-down RNA of target genes, at single-cell resolution and in programmable spatial patterns. As a proof of principle, we optogenetically induced Sonic Hedgehog (SHH) signaling at a distinct spatial location within human neural organoids. This robustly induced known SHH spatial domains of gene expression, cell-autonomously and across the entire organoid. In principle, our approach can be used to induce or knock down RNAs from any gene of interest in specific spatial locations or patterns of complex biological systems.

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RNA-guided cell targeting with CRISPR/RfxCas13d collateral activity in human cells

Shi

Murphy

Aparicio

et al. 2021

Preprint

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While single-cell sequencing has allowed rapid identification of novel cell types or states and associated RNA markers, functional studies remain challenging due to the lack of tools that are able to target specific cells based on these markers. Here we show that targeting a single marker RNA with CRISPR/RfxCas13d led to collateral transcriptome destruction in human cells, which can be harnessed to inhibit cell proliferation or to suppress cell state transition.

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CRISPR/Cas13 effectors have differing extents of off-target effects that limit their utility in eukaryotic cells

Cited by 5 publications

References 61 publications

Deep learning and CRISPR-Cas13d ortholog discovery for optimized RNA targeting

Deep learning and CRISPR-Cas13d ortholog discovery for optimized RNA targeting

Spatio-temporal, optogenetic control of gene expression in organoids

RNA-guided cell targeting with CRISPR/RfxCas13d collateral activity in human cells

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