- Girirajan, Santhosh;
- Rosenfeld, Jill A;
- Cooper, Gregory M;
- Antonacci, Francesca;
- Siswara, Priscillia;
- Itsara, Andy;
- Vives, Laura;
- Walsh, Tom;
- McCarthy, Shane E;
- Baker, Carl;
- Mefford, Heather C;
- Kidd, Jeffrey M;
- Browning, Sharon R;
- Browning, Brian L;
- Dickel, Diane E;
- Levy, Deborah L;
- Ballif, Blake C;
- Platky, Kathryn;
- Farber, Darren M;
- Gowans, Gordon C;
- Wetherbee, Jessica J;
- Asamoah, Alexander;
- Weaver, David D;
- Mark, Paul R;
- Dickerson, Jennifer;
- Garg, Bhuwan P;
- Ellingwood, Sara A;
- Smith, Rosemarie;
- Banks, Valerie C;
- Smith, Wendy;
- McDonald, Marie T;
- Hoo, Joe J;
- French, Beatrice N;
- Hudson, Cindy;
- Johnson, John P;
- Ozmore, Jillian R;
- Moeschler, John B;
- Surti, Urvashi;
- Escobar, Luis F;
- El-Khechen, Dima;
- Gorski, Jerome L;
- Kussmann, Jennifer;
- Salbert, Bonnie;
- Lacassie, Yves;
- Biser, Alisha;
- McDonald-McGinn, Donna M;
- Zackai, Elaine H;
- Deardorff, Matthew A;
- Shaikh, Tamim H;
- Haan, Eric;
- Friend, Kathryn L;
- Fichera, Marco;
- Romano, Corrado;
- Gécz, Jozef;
- DeLisi, Lynn E;
- Sebat, Jonathan;
- King, Mary-Claire;
- Shaffer, Lisa G;
- Eichler, Evan E
We report the identification of a recurrent, 520-kb 16p12.1 microdeletion associated with childhood developmental delay. The microdeletion was detected in 20 of 11,873 cases compared with 2 of 8,540 controls (P = 0.0009, OR = 7.2) and replicated in a second series of 22 of 9,254 cases compared with 6 of 6,299 controls (P = 0.028, OR = 2.5). Most deletions were inherited, with carrier parents likely to manifest neuropsychiatric phenotypes compared to non-carrier parents (P = 0.037, OR = 6). Probands were more likely to carry an additional large copy-number variant when compared to matched controls (10 of 42 cases, P = 5.7 x 10(-5), OR = 6.6). The clinical features of individuals with two mutations were distinct from and/or more severe than those of individuals carrying only the co-occurring mutation. Our data support a two-hit model in which the 16p12.1 microdeletion both predisposes to neuropsychiatric phenotypes as a single event and exacerbates neurodevelopmental phenotypes in association with other large deletions or duplications. Analysis of other microdeletions with variable expressivity indicates that this two-hit model might be more generally applicable to neuropsychiatric disease.