Mutations in COL27A1 cause Steel syndrome and suggest a founder mutation effect in the Puerto Rican population.

Journal: European Journal Of Human Genetics : EJHG
Published:
Abstract

Osteochondrodysplasias represent a large group of developmental structural disorders that can be caused by mutations in a variety of genes responsible for chondrocyte development, differentiation, mineralization and early ossification. The application of whole-exome sequencing to disorders apparently segregating as Mendelian traits has proven to be an effective approach to disease gene identification for conditions with unknown molecular etiology. We identified a homozygous missense variant p.(Gly697Arg) in COL27A1, in a family with Steel syndrome and no consanguinity. Interestingly, the identified variant seems to have arisen as a founder mutation in the Puerto Rican population.

Authors
Claudia Gonzaga Jauregui, Candace Gamble, Bo Yuan, Samantha Penney, Shalini Jhangiani, Donna Muzny, Richard Gibbs, James Lupski, Jacqueline Hecht

Similar Publications

Evaluating variants classified as pathogenic in ClinVar in the DDD Study.
Evaluating variants classified as pathogenic in ClinVar in the DDD Study.
Journal: Genetics in medicine : official journal of the American College of Medical Genetics
Published: July 30, 2020
DHX37 and NR5A1 Variants Identified in Patients with 46,XY Partial Gonadal Dysgenesis.
DHX37 and NR5A1 Variants Identified in Patients with 46,XY Partial Gonadal Dysgenesis.
Journal: Life (Basel, Switzerland)
Published: February 28, 2023
Identification of a novel de novo variant in OTX2 in a patient with congenital microphthalmia using targeted next-generation sequencing followed by prenatal diagnosis.
Identification of a novel de novo variant in OTX2 in a patient with congenital microphthalmia using targeted next-generation sequencing followed by prenatal diagnosis.
Journal: Ophthalmic genetics
Published: November 18, 2021