Literature DB >> 33243861

In vivo Perturb-Seq reveals neuronal and glial abnormalities associated with autism risk genes.

Aviv Regev1,2,3,4, Feng Zhang1,5,4, Paola Arlotta6,7,8, Xin Jin9,10,7,5, Sean K Simmons7,8,2, Amy Guo7, Ashwin S Shetty10,7,8, Michelle Ko10, Lan Nguyen7,2, Vahbiz Jokhi10, Elise Robinson7,8,11, Paul Oyler10, Nathan Curry10, Giulio Deangeli10, Simona Lodato12, Joshua Z Levin7,8,2.   

Abstract

The number of disease risk genes and loci identified through human genetic studies far outstrips the capacity to systematically study their functions. We applied a scalable genetic screening approach, in vivo Perturb-Seq, to functionally evaluate 35 autism spectrum disorder/neurodevelopmental delay (ASD/ND) de novo loss-of-function risk genes. Using CRISPR-Cas9, we introduced frameshift mutations in these risk genes in pools, within the developing mouse brain in utero, followed by single-cell RNA-sequencing of perturbed cells in the postnatal brain. We identified cell type-specific and evolutionarily conserved gene modules from both neuronal and glial cell classes. Recurrent gene modules and cell types are affected across this cohort of perturbations, representing key cellular effects across sets of ASD/ND risk genes. In vivo Perturb-Seq allows us to investigate how diverse mutations affect cell types and states in the developing organism.
Copyright © 2020, American Association for the Advancement of Science.

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Year:  2020        PMID: 33243861      PMCID: PMC7985844          DOI: 10.1126/science.aaz6063

Source DB:  PubMed          Journal:  Science        ISSN: 0036-8075            Impact factor:   47.728


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