Literature DB >> 27667664

A Genome-wide CRISPR Death Screen Identifies Genes Essential for Oxidative Phosphorylation.

Jason D Arroyo1, Alexis A Jourdain1, Sarah E Calvo1, Carmine A Ballarano1, John G Doench2, David E Root2, Vamsi K Mootha3.   

Abstract

Oxidative phosphorylation (OXPHOS) is the major pathway for ATP production in humans. Deficiencies in OXPHOS can arise from mutations in either mitochondrial or nuclear genomes and comprise the largest collection of inborn errors of metabolism. At present we lack a complete catalog of human genes and pathways essential for OXPHOS. Here we introduce a genome-wide CRISPR "death screen" that actively selects dying cells to reveal human genes required for OXPHOS, inspired by the classic observation that human cells deficient in OXPHOS survive in glucose but die in galactose. We report 191 high-confidence hits essential for OXPHOS, including 72 underlying known OXPHOS diseases. Our screen reveals a functional module consisting of NGRN, WBSCR16, RPUSD3, RPUSD4, TRUB2, and FASTKD2 that regulates the mitochondrial 16S rRNA and intra-mitochondrial translation. Our work yields a rich catalog of genes required for OXPHOS and, more generally, demonstrates the power of death screening for functional genomic analysis.
Copyright © 2016 Elsevier Inc. All rights reserved.

Entities:  

Keywords:  16S RNA; CRISPR; Mitochondria; OXPHOS; death screen; mitochondrial ribosome; neugrin; pseudouridine; pseudouridylation; synthetic lethality

Mesh:

Substances:

Year:  2016        PMID: 27667664      PMCID: PMC5474757          DOI: 10.1016/j.cmet.2016.08.017

Source DB:  PubMed          Journal:  Cell Metab        ISSN: 1550-4131            Impact factor:   27.287


  34 in total

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4.  Insights into RNA biology from an atlas of mammalian mRNA-binding proteins.

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5.  A mitochondrial protein compendium elucidates complex I disease biology.

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6.  Early redistribution of plasma membrane phosphatidylserine is a general feature of apoptosis regardless of the initiating stimulus: inhibition by overexpression of Bcl-2 and Abl.

Authors:  S J Martin; C P Reutelingsperger; A J McGahon; J A Rader; R C van Schie; D M LaFace; D R Green
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7.  MAGeCK enables robust identification of essential genes from genome-scale CRISPR/Cas9 knockout screens.

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8.  GOrilla: a tool for discovery and visualization of enriched GO terms in ranked gene lists.

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9.  Broad metabolic sensitivity profiling of a prototrophic yeast deletion collection.

Authors:  Benjamin VanderSluis; David C Hess; Colin Pesyna; Elias W Krumholz; Tahin Syed; Balázs Szappanos; Corey Nislow; Balázs Papp; Olga G Troyanskaya; Chad L Myers; Amy A Caudy
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10.  MitoCarta2.0: an updated inventory of mammalian mitochondrial proteins.

Authors:  Sarah E Calvo; Karl R Clauser; Vamsi K Mootha
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  94 in total

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Journal:  Am J Hum Genet       Date:  2017-08-03       Impact factor: 11.025

Review 2.  Determinants of nutrient limitation in cancer.

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3.  A pseudouridine synthase module is essential for mitochondrial protein synthesis and cell viability.

Authors:  Hana Antonicka; Karine Choquet; Zhen-Yuan Lin; Anne-Claude Gingras; Claudia L Kleinman; Eric A Shoubridge
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4.  Multiomic Profiling of Tyrosine Kinase Inhibitor-Resistant K562 Cells Suggests Metabolic Reprogramming To Promote Cell Survival.

Authors:  Brett M Noel; Steven B Ouellette; Laura Marholz; Deborah Dickey; Connor Navis; Tzu-Yi Yang; Vinh Nguyen; Sarah J Parker; David Bernlohr; Zohar Sachs; Laurie L Parker
Journal:  J Proteome Res       Date:  2019-02-21       Impact factor: 4.466

5.  Genetic Screen for Cell Fitness in High or Low Oxygen Highlights Mitochondrial and Lipid Metabolism.

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6.  The tRNA pseudouridine synthase TruB1 regulates the maturation of let-7 miRNA.

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7.  Proteome Imbalance of Mitochondrial Electron Transport Chain in Brown Adipocytes Leads to Metabolic Benefits.

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Review 8.  Am I ready for CRISPR? A user's guide to genetic screens.

Authors:  John G Doench
Journal:  Nat Rev Genet       Date:  2017-12-04       Impact factor: 53.242

9.  Somatic evolution and global expansion of an ancient transmissible cancer lineage.

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10.  Mitochondrial Reprogramming Underlies Resistance to BCL-2 Inhibition in Lymphoid Malignancies.

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Journal:  Cancer Cell       Date:  2019-09-19       Impact factor: 31.743

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