Rates, distribution and implications of postzygotic mosaic mutations in autism spectrum disorder

Lim, Elaine T.; Uddin, Mohammed; De Rubeis, Silvia; Chan, Yingleong; Kamumbu, Anne S.; Zhang, Xiaochang; D'Gama, Alissa M.; Kim, Sonia N.; Hill, Robert Sean; Goldberg, Arthur P.; Poultney, Christopher; Minshew, Nancy J.; Kushima, Itaru; Aleksic, Branko; Ozaki, Norio; Parellada, Mara; Arango, Celso; Penzol, Maria J.; Carracedo, Angel; Kolevzon, Alexander; Hultman, Christina M.; Weiss, Lauren A.; Fromer, Menachem; Chiocchetti, Andreas G.; Freitag, Christine M.; Church, George M.; Scherer, Stephen W.; Buxbaum, Joseph D.; Walsh, Christopher A; Aleksic B; Anney R; Barbosa M; Barrett J; Betancur C; Bishop S; Brusco A; Buxbaum JD; Carracedo A; Chiocchetti AG; Chung BHY; Cook E; Coon H; Cutler DJ; Daly M; De Rubeis S; Doan R; Fernández-Prieto M; Ferrero GB; Freitag CM; Fromer M; Gargus J; Geschwind D; Gill M; Gómez-Guerrero L; Hansen-Kiss E; He X; Herman G; Hertz-Picciotto I; Hultman C; Iliadou B; Ionita-Laza I; Jugessur A; Knudsen GP; Kolevzon A; Kosmicki J; Kushima I; Lee SL; Lehner T; Lennertz S; Lim E; Maciel P; Magnus P; Manoach D; Minshew N; Morrow E; Mulle J; Neale B; Ozaki N; Palotie A; Parellada M; Passos-Bueno MR; Pericak-Vance M; Persico A; Pessah I; Reichenberg A; Reichert J; Renieri A; Robinson E; Samocha K; Sanders S; Sandin S; Santangelo SL; Satterstrom K; Schafer C; Schellenberg G; Scherer S; Senthil G; Silva M; Singh T; Siper PM; Soares G; Stevens C; Stoltenberg C; Surén P; Sutcliffe JS; Szatmari P; Tassone F; Thurm A; Walsh C; Weiss L; Werling D; Willsey J; Xu X; Yu TW; Yuen R; Zwick ME.

doi:10.1038/nn.4598

We systematically analyzed postzygotic mutations (PZMs) in whole-exome sequences from the largest collection of trios (5,947) with autism spectrum disorder (ASD) available, including 282 unpublished trios, and performed resequencing using multiple independent technologies. We identified 7.5% of de novo mutations as PZMs, 83.3% of which were not described in previous studies. Damaging, nonsynonymous PZMs within critical exons of prenatally expressed genes were more common in ASD probands than controls (P < 1 × 10-6), and genes carrying these PZMs were enriched for expression in the amygdala (P = 5.4 × 10-3). Two genes (KLF16 and MSANTD2) were significantly enriched for PZMs genome-wide, and other PZMs involved genes (SCN2A, HNRNPU and SMARCA4) whose mutation is known to cause ASD or other neurodevelopmental disorders. PZMs constitute a significant proportion of de novo mutations and contribute importantly to ASD risk.