Yayınlanmış 1 Ocak 2018
| Sürüm v1
Dergi makalesi
Açık
Identification of likely pathogenic and known variants in TSPEAR, LAMB3, BCOR, and WNT10A in four Turkish families with tooth agenesis
Oluşturanlar
- Du, Renqian1
- Dinckan, Nuriye
- Song, Xiaofei1
- Coban-Akdemir, Zeynep1
- Jhangiani, Shalini N.2
- Guven, Yeliz3
- Aktoren, Oya3
- Kayserili, Hulya4
- Petty, Lauren E.5
- Muzny, Donna M.2
- Below, Jennifer E.5
- Boerwinkle, Eric
- Wu, Nan6
- Gibbs, Richard A.
- Posey, Jennifer E.1
- Lupski, James R.
- Letra, Ariadne
- Uyguner, Z. Oya7
- 1. Baylor Coll Med, Dept Mol & Human Genet, Houston, TX 77030 USA
- 2. Baylor Coll Med, Human Genome Sequencing Ctr, Houston, TX 77030 USA
- 3. Istanbul Univ, Fac Dent, Dept Pedodont, Istanbul, Turkey
- 4. Koc Univ, Sch Med KUSOM, Dept Med Genet, Istanbul, Turkey
- 5. Univ Texas Hlth Sci Ctr Houston, Sch Publ Hlth, Human Genet Ctr, Houston, TX 77030 USA
- 6. Peking Union Med Coll Hosp, Dept Orthoped Surg, Beijing, Peoples R China
- 7. Istanbul Univ, Istanbul Fac Med, Dept Med Genet, TR-34093 Istanbul, Turkey
Açıklama
Tooth agenesis (TA), the failure of development of one or more permanent teeth, is a common craniofacial abnormality observed in different world populations. The genetic etiology of TA is heterogeneous; more than a dozen genes have been associated with isolated or nonsyndromic TA, and more than 80 genes with syndromic forms. In this study, we applied whole exome sequencing (WES) to identify candidate genes contributing to TA in four Turkish families. Likely pathogenic variants with a low allele frequency in the general population were identified in four disease-associated genes, including two distinct variants in TSPEAR, associated with syndromic and isolated TA in one family each; a variant in LAMB3 associated with syndromic TA in one family; and a variant in BCOR plus a disease-associated WNT10A variant in one family with syndromic TA. With the notable exception of WNT10A (Tooth agenesis, selective, 4, MIM #150400), the genotype-phenotype relationships described in the present cohort represent an expansion of the clinical spectrum associated with these genes: TSPEAR (Deafness, autosomal recessive 98, MIM #614861), LAMB3 (Amelogenesis imperfecta, type IA, MIM #104530; Epidermolysis bullosa, junctional, MIMs #226700 and #226650), and BCOR (Microphthalmia, syndromic 2, MIM #300166). We provide evidence supporting the candidacy of these genes with TA, and propose TSPEAR as a novel nonsyndromic TA gene. Our data also suggest potential multilocus genomic variation, or mutational burden, in a single family, involving the BCOR and WNT10A loci, underscoring the complexity of the genotype-phenotype relationship in the common complex trait of TA.
Dosyalar
bib-33152e4c-fc01-4e42-b8ac-562fc4cc9b91.txt
Dosyalar
(395 Bytes)
| Ad | Boyut | Hepisini indir |
|---|---|---|
|
md5:0a48a07e942af7bfe1a0379b44a17a06
|
395 Bytes | Ön İzleme İndir |