Human and mouse essentiality screens as a resource for disease gene discovery

Pilar Cacheiro(Queen Mary University of London), Violeta Muñoz‐Fuentes(European Bioinformatics Institute), Stephen A. Murray(Jackson Laboratory), Mary E. Dickinson(Baylor College of Medicine), Maja Bućan(University of Pennsylvania), Lauryl M. J. Nutter(Hospital for Sick Children), Kevin A. Peterson(Jackson Laboratory), Hamed Haselimashhadi(European Bioinformatics Institute), Ann M. Flenniken(Mount Sinai Hospital), Hugh W. Morgan(Mary Lyon Centre at MRC Harwell), Henrik Westerberg(Mary Lyon Centre at MRC Harwell), Tomasz Konopka(Queen Mary University of London), Chih‐Wei Hsu(Baylor College of Medicine), Audrey E. Christiansen(Baylor College of Medicine), Denise G. Lanza(Baylor College of Medicine), Arthur L. Beaudet(Baylor College of Medicine), Jason D. Heaney(Baylor College of Medicine), Helmut Fuchs(Helmholtz Zentrum München), Valérie Gailus‐Durner(Helmholtz Zentrum München), Tania Sorg(Centre National de la Recherche Scientifique), Jan Procházka(Czech Academy of Sciences, Institute of Molecular Genetics), Vendula Novosadová(Czech Academy of Sciences, Institute of Molecular Genetics), Christopher J. Lelliott(Wellcome Sanger Institute), Hannah Wardle‐Jones(Wellcome Sanger Institute), Sara Wells(Mary Lyon Centre at MRC Harwell), Lydia Teboul(Mary Lyon Centre at MRC Harwell), Heather Cater(Mary Lyon Centre at MRC Harwell), Michelle Stewart(Mary Lyon Centre at MRC Harwell), Tertius Hough(Mary Lyon Centre at MRC Harwell), Wolfgang Wurst(Helmholtz Zentrum München), Radislav Sedláček(Czech Academy of Sciences, Institute of Molecular Genetics), David J. Adams(Wellcome Sanger Institute), John R. Seavitt(Baylor College of Medicine), Glauco P. Tocchini‐Valentini(National Research Council), Fabio Mammano(National Research Council), Robert E. Braun(Jackson Laboratory), Colin McKerlie(Hospital for Sick Children), Yann Hérault(Centre National de la Recherche Scientifique), Martin Hrabě de Angelis(Helmholtz Zentrum München), Ann‐Marie Mallon(Mary Lyon Centre at MRC Harwell), K. C. Kent Lloyd(University of California, Davis), Steve D. M. Brown(Mary Lyon Centre at MRC Harwell), Helen Parkinson(European Bioinformatics Institute), Terrence F. Meehan(European Bioinformatics Institute), Damian Smedley(Queen Mary University of London), J. C. Ambrose(Genomics England), Paramasivam Arumugam(Genomics England), E. L. Baple(Genomics England), Marta Bleda(Genomics England), F. Boardman-Pretty(Queen Mary University of London), J. M. Boissiere(Genomics England), C. R. Boustred(Genomics England), H. Brittain(Genomics England), Mark J. Caulfield(Queen Mary University of London), Gcf Chan(Genomics England), C. E. H. Craig(Genomics England), Louise C. Daugherty(Genomics England), A. de Burca(Genomics England), A. Devereau(Genomics England), Greg Elgar(Queen Mary University of London), Rebecca E. Foulger(Genomics England), Tom Fowler(Genomics England), P. Furió-Tarí(Genomics England), J.M. Hackett(Genomics England), Dina Halai(Genomics England), Angela Hamblin(Genomics England), Seton Henderson(Queen Mary University of London), J. E. Holman(Genomics England), Tim Hubbard(Genomics England), Kristina Ibáñez(Queen Mary University of London), Richard V. Jackson(Genomics England), Lesley Jones(Queen Mary University of London), Dalia Kasperavičiūtė(Queen Mary University of London), M. Kayikci(Genomics England), L. Lahnstein(Genomics England), Kim Lawson(Genomics England), S. E. A. Leigh(Genomics England), Ivone Leong(Genomics England), F. J. Lopez(Genomics England), F. Maleady-Crowe(Genomics England), Joanne Mason(Genomics England), Ellen M. McDonagh(Queen Mary University of London), L. Moutsianas(Queen Mary University of London), Michael Mueller(Queen Mary University of London), Nirupa Murugaesu(Genomics England), A. C. Need(Queen Mary University of London), Christopher A. Odhams(Genomics England), C. Patch(Queen Mary University of London), D. Perez-Gil(Genomics England), Dimitris Polychronopoulos(Genomics England), J. Pullinger(Genomics England), T. Rahim(Genomics England), Álvaro Rendón(Genomics England), Pablo Riesgo-Ferreiro(Genomics England), Tim Rogers(Genomics England), Mina Ryten(Genomics England), K Savage(Genomics England), K. Sawant(Genomics England), Richard H. Scott(Genomics England), A. Siddiq(Genomics England), A. Sieghart(Genomics England), K. R. Smith(Queen Mary University of London), Alona Sosinsky(Queen Mary University of London), W. Spooner(Genomics England), Hallam Stevens(Genomics England), Ashley Stuckey(Genomics England), Rosy Sultana(Genomics England), Elizabeth R. Thomas(Queen Mary University of London), S. R. Thompson(Genomics England), C. Tregidgo(Genomics England), Arianna Tucci(Queen Mary University of London), E. Walsh(Genomics England), Scott Watters(Genomics England), M. J. Welland(Genomics England), Eric O. Williams(Genomics England), Kate Witkowska(Queen Mary University of London), S. M. Wood(Queen Mary University of London), Magdalena Zarowiecki(Genomics England), Susan Marschall(Helmholtz Zentrum München), Christoph Lengger(Helmholtz Zentrum München), Holger Maier(Helmholtz Zentrum München), Claudia Seisenberger(Helmholtz Zentrum München), Antje Bürger(Helmholtz Zentrum München), Ralf Kühn(Helmholtz Zentrum München), Joel Schick(Helmholtz Zentrum München), Andreas Hörlein(Helmholtz Zentrum München), Oskar Oritz(Helmholtz Zentrum München), Florian Giesert(Helmholtz Zentrum München), Joachim Beig(Helmholtz Zentrum München), Janet Kenyon(Mary Lyon Centre at MRC Harwell), Gemma Codner(Mary Lyon Centre at MRC Harwell), Martin Fray(Mary Lyon Centre at MRC Harwell), Sara Johnson(Mary Lyon Centre at MRC Harwell), James Cleak(Mary Lyon Centre at MRC Harwell), Zsombor Szoke-Kovacs(Mary Lyon Centre at MRC Harwell), David Lafont(Wellcome Sanger Institute), Valerie E. Vancollie(Wellcome Sanger Institute), Robbie S. B. McLaren(Wellcome Sanger Institute), Lena Hughes-Hallett(Wellcome Sanger Institute), Christine Rowley(Wellcome Sanger Institute), Emma Sanderson(Wellcome Sanger Institute), Antonella Galli(Wellcome Sanger Institute), Elizabeth Tuck(Wellcome Sanger Institute), Angela Green(Wellcome Sanger Institute), Catherine Tudor(Wellcome Sanger Institute), Emma Siragher(Wellcome Sanger Institute), Monika Dabrowska(Wellcome Sanger Institute), Cecilia Mazzeo(Wellcome Sanger Institute), Mark Griffiths(Wellcome Sanger Institute), David Gannon(Wellcome Sanger Institute), Brendan Doe(Wellcome Sanger Institute), Nicola Cockle(Wellcome Sanger Institute), Andrea Kirton(Wellcome Sanger Institute), Joanna Bottomley(Wellcome Sanger Institute), Catherine Ingle(Wellcome Sanger Institute), Edward J. Ryder(Wellcome Sanger Institute), Diane Gleeson(Wellcome Sanger Institute), Ramiro Ramírez‐Solis(Wellcome Sanger Institute), Marie‐Christine Birling(Centre National de la Recherche Scientifique), Guillaume Pavlovic(Centre National de la Recherche Scientifique), Abdel Ayadi(Centre National de la Recherche Scientifique), Meziane Hamid(Centre National de la Recherche Scientifique), Ghina Bou About(Centre National de la Recherche Scientifique), Marie‐France Champy(Centre National de la Recherche Scientifique), Hugues Jacobs(Centre National de la Recherche Scientifique), Olivia Wendling(Centre National de la Recherche Scientifique), Sophie Leblanc(Centre National de la Recherche Scientifique), Laurent Vasseur(Centre National de la Recherche Scientifique), Elissa J. Chesler(Jackson Laboratory), Vivek Kumar(Jackson Laboratory), Jacqueline K. White(Jackson Laboratory), Karen L. Svenson(Jackson Laboratory), Jean-Paul Wiegand(Jackson Laboratory), Laura L. Anderson(Jackson Laboratory), Troy Wilcox(Jackson Laboratory), James Clark(Jackson Laboratory), Jennifer Ryan(Jackson Laboratory), James M. Denegre(Jackson Laboratory), Timothy M. Stearns(Jackson Laboratory), Vivek M. Philip(Jackson Laboratory), Catherine Witmeyer(Jackson Laboratory), Lindsay Bates(Jackson Laboratory), Zachary Seavey(Jackson Laboratory), Pamela Stanley(Jackson Laboratory), Amelia Willet(Jackson Laboratory), Willson Roper(Jackson Laboratory), Julie Creed(Jackson Laboratory), Michayla Moore(Jackson Laboratory), Alex Dorr(Jackson Laboratory), Pamelia Fraungruber(Jackson Laboratory), Rose E. Presby(Jackson Laboratory), Matthew Mckay(Jackson Laboratory), Dong Nguyen-Bresinsky(Jackson Laboratory), Leslie O. Goodwin(Jackson Laboratory), Rachel Urban(Jackson Laboratory), Coleen Kane(Jackson Laboratory)
Nature Communications
January 31, 2020
10.1038/s41467-020-14284-2
Cited by 125Open Access
Full Text

Abstract

The identification of causal variants in sequencing studies remains a considerable challenge that can be partially addressed by new gene-specific knowledge. Here, we integrate measures of how essential a gene is to supporting life, as inferred from viability and phenotyping screens performed on knockout mice by the International Mouse Phenotyping Consortium and essentiality screens carried out on human cell lines. We propose a cross-species gene classification across the Full Spectrum of Intolerance to Loss-of-function (FUSIL) and demonstrate that genes in five mutually exclusive FUSIL categories have differing biological properties. Most notably, Mendelian disease genes, particularly those associated with developmental disorders, are highly overrepresented among genes non-essential for cell survival but required for organism development. After screening developmental disorder cases from three independent disease sequencing consortia, we identify potentially pathogenic variants in genes not previously associated with rare diseases. We therefore propose FUSIL as an efficient approach for disease gene discovery.

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