Leveraging base-pair mammalian constraint to understand genetic variation and human disease.

Patrick F Sullivan ,Cynthia Steiner ,Michaela K Halsey ,Kevin R Bredemeyer ,Mark Diekhans ,Alyssa J Lawler ,Ross Swofford ,Beth Shapiro ,Wynn K Meyer ,Klaus‐Peter Koepfli ,Laura Huckins ,Jiawen Chen ,Jennifer M Korstian ,Oliver A Ryder ,Aitor Serres ,Carlos J Garcia ,Jenna Grimshaw ,Cornelia Fanter ,Jin P Szatkiewicz ,David A Ray ,James R Xue ,Jessica M Storer ,Jason Turner-Maier ,Chao Wang ,Katherine S Pollard ,William J Murphy ,Eduardo Eizirik ,Glenn Hickey ,Kathleen M Morrill ,Tomàs Marquès-Bonet ,Louise Ryan ,Zhiping Weng ,Federica Di Palma ,Ana M Breit ,Nicole M Foley ,Yun Li ,Irina Ruf ,Mark S Springer ,Gerard Muntané ,Quan Sun ,Karin Forsberg-Nilsson ,Juehan Wang ,Joy-El Talbot ,Graham M Hughes ,Harris A Lewin ,Jian Zeng ,Sergey V Kozyrev ,Joel Armstrong ,Matteo Bianchi ,Diane P Genereux ,Arcadi Navarro ,Amanda Kowalczyk ,Michael X Dong ,Sylvia Ortmann ,Emma C Teeling ,Jill E Moore ,Voichita D Marinescu ,Aryn P Wilder ,Austin Osmanski ,Martin Nweeia ,Daniel E Schäffer ,Elisabeth Sundström ,Kaili Fan ,Matthew J Christmas ,Joana Damas ,Ananya Roy ,Kerstin Lindblad‐Toh ,Victor C Mason ,Alejandro Valenzuela ,Jessica Johnson ,Linda Goodman ,John Gatesy ,Bruce W Birren ,Xue Li ,Jennifer R S Meadows ,Andrew Harris ,Jia Wen ,Arian F A Smit ,Sharadha Sakthikumar ,Jessika Nordin ,Nicole S Paulat ,Colleen Lawless ,Lucas R Moreira ,Jeb Rosen ,Henry E Pratt ,Thomas Lehmann ,Naomi R Wray ,Gregory Andrews ,Ola Wallerman ,Steven Gazal ,Jeremy Johnson ,Andreas R Pfenning ,Danielle L Levesque ,Steven K Reilly ,Franziska Wagner ,Morgan Wirthlin ,Allyson G Hindle ,David Juan ,Ava Mackay-Smith ,Shuyang Yao ,Kathleen C Keough ,Hiram Clawson ,Badoi N Phan ,Zhili Zheng ,Irene M Kaplow ,Chaitanya Srinivasan ,Michael Hiller ,Benedict Paten ,Bogdan Kirilenko ,Kevin A Sullivan ,Robert Hubley ,Diana D Moreno-Santillán ,Megan A Supple ,Pardis C Sabeti ,Abigail Lind ,Elinor K Karlsson ,Xiaomeng Zhang

doi:10.1126/science.abn2937

Abstract

Thousands of genomic regions have been associated with heritable human diseases, but attempts to elucidate biological mechanisms are impeded by an inability to discern which genomic positions are functionally important. Evolutionary constraint is a powerful predictor of function, agnostic to cell type or disease mechanism. Single-base phyloP scores from 240 mammals identified 3.3% of the human genome as significantly constrained and likely functional. We compared phyloP scores to genome annotation, association studies, copy-number variation, clinical genetics findings, and cancer data. Constrained positions are enriched for variants that explain common disease heritability more than other functional annotations. Our results improve variant annotation but also highlight that the regulatory landscape of the human genome still needs to be further explored and linked to disease.

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