Fine-grained facial phenotype–genotype analysis in Wolf–Hirschhorn syndrome

被引:0
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作者
Peter Hammond
Femke Hannes
Michael Suttie
Koen Devriendt
Joris Robert Vermeesch
Francesca Faravelli
Francesca Forzano
Susan Parekh
Steve Williams
Dominic McMullan
Sarah T South
John C Carey
Oliver Quarrell
机构
[1] Molecular Medicine Unit,Department of Clinical Genetics
[2] UCL Institute of Child Health,Department of Cytogenetics
[3] Centre for Human-Genetics,Department of Pediatrics, Division of Medical Genetics
[4] University of Leuven,undefined
[5] SC Genetica Umana,undefined
[6] EO Ospedali Galliera,undefined
[7] UCL Eastman Dental Institute,undefined
[8] Sheffield Children's Hospital,undefined
[9] Birmingham Women's Hospital,undefined
[10] University of Utah,undefined
来源
关键词
Wolf–Hirschhorn syndrome; facial dysmorphism; 3D shape analysis;
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摘要
Wolf–Hirschhorn syndrome is caused by anomalies of the short arm of chromosome 4. About 55% of cases are due to de novo terminal deletions, 40% from unbalanced translocations and 5% from other abnormalities. The facial phenotype is characterized by hypertelorism, protruding eyes, prominent glabella, broad nasal bridge and short philtrum. We used dense surface modelling and pattern recognition techniques to delineate the milder facial phenotype of individuals with a small terminal deletion (breakpoint within 4p16.3) compared to those with a large deletion (breakpoint more proximal than 4p16.3). Further, fine-grained facial analysis of several individuals with an atypical genotype and/or phenotype suggests that multiple genes contiguously contribute to the characteristic Wolf–Hirschhorn syndrome facial phenotype.
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页码:33 / 40
页数:7
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