De Novo Coding Variants Are Strongly Associated with Tourette Disorder

A. Jeremy Willsey,Thomas V. Fernandez,Dongmei Yu,Robert A. King,Andrea Dietrich,Jinchuan Xing,Stephan J. Sanders,Jeffrey D. Mandell,Alden Y. Huang,Petra Richer,Louw Smith,Shan Dong,Kaitlin E. Samocha,Mohamed Abdulkadir,Julia Bohnenpoll,Yana Bromberg,Lawrence W. Brown,Keun-Ah Cheon,Barbara J. Coffey,Li Deng,Lonneke Elzerman,Odette Fründt,Blanca Garcia-Delgar,Erika Gedvilaite,Donald L. Gilbert,Dorothy E. Grice,Julie Hagstrøm,Tammy Hedderly,Gary A. Heiman,Isobel Heyman,Pieter J. Hoekstra,Hyun Ju Hong,Chaim Huyser,Laura Ibanez-Gomez,Young Key Kim,Young Shin Kim,Yun-Joo Koh,Sodahm Kook,Samuel Kuperman,Andreas Lamerz,Bennett L. Leventhal,Andrea G. Ludolph,Claudia Lühr da Silva,Marcos Madruga-Garrido,Athanasios Maras,Pablo Mir,Astrid Morer,Alexander Münchau,Tara Murphy,Cara Nasello,Thaïra J.C. Openneer,Kerstin J. Plessen,Veit Roessner,Stephan J. Sanders,Eun-Young Shin,Deborah A. Sival,Dong-Ho Song,Jungeun Song,Matthew W. State,Anne Marie Stolte,Nawei Sun,Jay A. Tischfield,Jennifer Tübing,Frank Visscher,Michael F. Walker,Sina Wanderer,Shuoguo Wang,Martin Woods,Yeting Zhang,Anbo Zhou,Samuel H. Zinner,Cathy L. Barr,James R. Batterson,Cheston M. Berlin,Ruth D. Bruun,Cathy L. Budman,Danielle C. Cath,Sylvain Chouinard,Giovanni Coppola,Nancy J. Cox,Sabrina M. Darrow,Lea K. Davis,Yves Dion,Nelson B. Freimer,Marco A. Grados,Matthew E. Hirschtritt,Cornelia Illmann,Roger Kurlan,James F. Leckman,Gholson J. Lyon,Irene A. Malaty,Carol A. Mathews,William M. MaMahon,Benjamin M. Neale,Michael S. Okun,Lisa Osiecki,David L. Pauls,Danielle Posthuma,Vasily Ramensky,Mary M. Robertson,Guy A. Rouleau,Paul Sandor,Jeremiah M. Scharf,Harvey S. Singer,Jan Smit,Jae Hoon Sul

De Novo Coding Variants Are Strongly Associated with Tourette Disorder

2017

Whole-exome sequencing (WES) and de novo variant detection have proven a powerful approach to gene discovery in complex neurodevelopmental disorders. We have completed WES of 325 Tourette disorder trios from the Tourette International Collaborative Genetics cohort and a replication sample of 186 trios from the Tourette Syndrome Association International Consortium on Genetics (511 total). We observe strong and consistent evidence for the contribution of de novo likely gene-disrupting (LGD) variants (rate ratio [RR] 2.32, p = 0.002). Additionally, de novo damaging variants (LGD and probably damaging missense) are overrepresented in probands (RR 1.37, p = 0.003). We identify four likely risk genes with multiple de novo damaging variants in unrelated probands: WWC1 (WW and C2 domain containing 1), CELSR3 (Cadherin EGF LAG seven-pass G-type receptor 3), NIPBL (Nipped-B-like), and FN1 (fibronectin 1). Overall, we estimate that de novo damaging variants in approximately 400 genes contribute risk in 12% of clinical cases. VIDEO ABSTRACT.

Keywords:

Correction
Source
Cite
Save
Machine Reading By IdeaReader

References

Citations