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split-intein Gal4 provides intersectional genetic labeling that is repressible by Gal80

Ben Ewen‐Campen, Haojiang Luan, Jun Xu, Rohit Singh, Neha Joshi, Tanuj Thakkar, Bonnie Berger, Benjamin H. White, Norbert Perrimon

2023Proceedings of the National Academy of Sciences36 citationsDOIOpen Access PDF

Abstract

. However, the existing split-Gal4 system, unlike the standard Gal4 system, cannot be repressed by Gal80, and therefore cannot be controlled temporally. This lack of temporal control precludes split-Gal4 experiments in which a genetic manipulation must be restricted to specific timepoints. Here, we describe a split-Gal4 system based on a self-excising split-intein, which drives transgene expression as strongly as the current split-Gal4 system and Gal4 reagents, yet which is repressible by Gal80. We demonstrate the potent inducibility of "split-intein Gal4" in vivo using both fluorescent reporters and via reversible tumor induction in the gut. Further, we show that our split-intein Gal4 can be extended to the drug-inducible GeneSwitch system, providing an independent method for intersectional labeling with inducible control. We also show that the split-intein Gal4 system can be used to generate highly cell type-specific genetic drivers based on in silico predictions generated by single-cell RNAseq (scRNAseq) datasets, and we describe an algorithm ("Two Against Background" or TAB) to predict cluster-specific gene pairs across multiple tissue-specific scRNA datasets. We provide a plasmid toolkit to efficiently create split-intein Gal4 drivers based on either CRISPR knock-ins to target genes or using enhancer fragments. Altogether, the split-intein Gal4 system allows for the creation of highly specific intersectional genetic drivers that are inducible/repressible.

Topics & Concepts

InteinBiologyEnhancerTransgeneGeneCRISPRComputational biologyGeneticsCell biologyGene expressionRNARNA splicingCRISPR and Genetic EngineeringNeurobiology and Insect Physiology ResearchRNA Research and Splicing
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