- Johnston, Jennifer J;
- Sapp, Julie C;
- Turner, Joyce T;
- Amor, David;
- Aftimos, Salim;
- Aleck, Kyrieckos A;
- Bocian, Maureen;
- Bodurtha, Joann N;
- Cox, Gerald F;
- Curry, Cynthia J;
- Day, Ruth;
- Donnai, Dian;
- Field, Michael;
- Fujiwara, Ikuma;
- Gabbett, Michael;
- Gal, Moran;
- Graham, John M;
- Hedera, Peter;
- Hennekam, Raoul CM;
- Hersh, Joseph H;
- Hopkin, Robert J;
- Kayserili, Hülya;
- Kidd, Alexa MJ;
- Kimonis, Virginia;
- Lin, Angela E;
- Lynch, Sally Ann;
- Maisenbacher, Melissa;
- Mansour, Sahar;
- McGaughran, Julie;
- Mehta, Lakshmi;
- Murphy, Helen;
- Raygada, Margarita;
- Robin, Nathaniel H;
- Rope, Alan F;
- Rosenbaum, Kenneth N;
- Schaefer, G Bradley;
- Shealy, Amy;
- Smith, Wendy;
- Soller, Maria;
- Sommer, Annmarie;
- Stalker, Heather J;
- Steiner, Bernhard;
- Stephan, Mark J;
- Tilstra, David;
- Tomkins, Susan;
- Trapane, Pamela;
- Tsai, Anne Chun‐Hui;
- Van Allen, Margot I;
- Vasudevan, Pradeep C;
- Zabel, Bernhard;
- Zunich, Janice;
- Black, Graeme CM;
- Biesecker, Leslie G
A range of phenotypes including Greig cephalopolysyndactyly and Pallister-Hall syndromes (GCPS, PHS) are caused by pathogenic mutation of the GLI3 gene. To characterize the clinical variability of GLI3 mutations, we present a subset of a cohort of 174 probands referred for GLI3 analysis. Eighty-one probands with typical GCPS or PHS were previously reported, and we report the remaining 93 probands here. This includes 19 probands (12 mutations) who fulfilled clinical criteria for GCPS or PHS, 48 probands (16 mutations) with features of GCPS or PHS but who did not meet the clinical criteria (sub-GCPS and sub-PHS), 21 probands (6 mutations) with features of PHS or GCPS and oral-facial-digital syndrome, and 5 probands (1 mutation) with nonsyndromic polydactyly. These data support previously identified genotype-phenotype correlations and demonstrate a more variable degree of severity than previously recognized. The finding of GLI3 mutations in patients with features of oral-facial-digital syndrome supports the observation that GLI3 interacts with cilia. We conclude that the phenotypic spectrum of GLI3 mutations is broader than that encompassed by the clinical diagnostic criteria, but the genotype-phenotype correlation persists. Individuals with features of either GCPS or PHS should be screened for mutations in GLI3 even if they do not fulfill clinical criteria.