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CRISPR-mediated genetic interaction profiling identifies RNA binding proteins controlling metazoan fitness.


ABSTRACT: Genetic interaction screens have aided our understanding of complex genetic traits, diseases, and biological pathways. However, approaches for synthetic genetic analysis with null-alleles in metazoans have not been feasible. Here, we present a CRISPR/Cas9-based Synthetic Genetic Interaction (CRISPR-SGI) approach enabling systematic double-mutant generation. Applying this technique in Caenorhabditis elegans, we comprehensively screened interactions within a set of 14 conserved RNA binding protein genes, generating all possible single and double mutants. Many double mutants displayed fitness defects, revealing synthetic interactions. For one interaction between the MBNL1/2 ortholog mbl-1 and the ELAVL ortholog exc-7, double mutants displayed a severely shortened lifespan. Both genes are required for regulating hundreds of transcripts and isoforms, and both may play a critical role in lifespan extension through insulin signaling. Thus, CRISPR-SGI reveals a rich genetic interaction landscape between RNA binding proteins in maintaining organismal health, and will serve as a paradigm applicable to other biological questions.

SUBMITTER: Norris AD 

PROVIDER: S-EPMC5544425 | biostudies-literature | 2017 Jul

REPOSITORIES: biostudies-literature

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CRISPR-mediated genetic interaction profiling identifies RNA binding proteins controlling metazoan fitness.

Norris Adam D AD   Gracida Xicotencatl X   Calarco John A JA  

eLife 20170718


Genetic interaction screens have aided our understanding of complex genetic traits, diseases, and biological pathways. However, approaches for synthetic genetic analysis with null-alleles in metazoans have not been feasible. Here, we present a CRISPR/Cas9-based Synthetic Genetic Interaction (CRISPR-SGI) approach enabling systematic double-mutant generation. Applying this technique in <i>Caenorhabditis elegans</i>, we comprehensively screened interactions within a set of 14 conserved RNA binding  ...[more]

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