Published February 27, 2016
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Data from: Genome-wide association studies in dogs and humans identify ADAMTS20 as a risk variant for cleft lip and palate
Authors/Creators
- Wolf, Zena T.1
- Brand, Harrison A.2
- Shaffer, John R.2
- Leslie, Elizabeth J.2
- Arzi, Boaz1
- Willet, Cali E.3
- Cox, Timothy C.4
- McHenry, Toby2
- Narayan, Nicole1
- Feingold, Eleanor2
- Wang, Xioajing2
- Sliskovic, Saundra1
- Karmi, Nili1
- Safra, Noa1
- Sanchez, Carla2
- Deleyiannis, Frederic W. B.
- Murray, Jeffrey C.5
- Wade, Claire M.3
- Marazita, Mary L.2
- Bannasch, Danika L.1
- 1. University of California, Davis
- 2. University of Pittsburgh
- 3. University of Sydney
- 4. Monash University
- 5. University of Iowa
Description
Cleft lip with or without cleft palate (CL/P) is the most commonly occurring craniofacial birth defect. We provide insight into the genetic etiology of this birth defect by performing genome-wide association studies in two species: dogs and humans. In the dog, a genome-wide association study of 7 CL/P cases and 112 controls from the Nova Scotia Duck Tolling Retriever (NSDTR) breed identified a significantly associated region on canine chromosome 27 (unadjusted p=1.1 x 10-13; adjusted p= 2.2 x 10-3). Further analysis in NSDTR families and additional full sibling cases identified a 1.44 Mb homozygous haplotype (chromosome 27: 9.29 – 10.73 Mb) segregating with a more complex phenotype of cleft lip, cleft palate, and syndactyly (CLPS) in 13 cases. Whole-genome sequencing of 3 CLPS cases and 4 controls at 15X coverage led to the discovery of a frameshift mutation within ADAMTS20 (c.1360_1361delAA (p.Lys453Ilefs*3)), which segregated concordant with the phenotype. In a parallel study in humans, a family-based association analysis (DFAM) of 125 CL/P cases, 420 unaffected relatives, and 392 controls from a Guatemalan cohort, identified a suggestive association (rs10785430; p =2.67 x 10-6) with the same gene, ADAMTS20. Sequencing of cases from the Guatemalan cohort was unable to identify a causative mutation within the coding region of ADAMTS20, but four coding variants were found in additional cases of CL/P. In summary, this study provides genetic evidence for a role of ADAMTS20 in CL/P development in dogs and as a candidate gene for CL/P development in humans.
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Additional details
Related works
- Is cited by
- 10.1371/journal.pgen.1005059 (DOI)