MYT1 role in the microtia‐craniofacial microsomia spectrum

Daniela V. Luquetti; Carrie L. Heike; Ignacio Zarante; Andrew E. Timms; Jonas Gustafson; Harry Pachajoa; Gloria L. Porras‐Hurtado; Paola Ayala‐Ramirez; Milagros M. Duenas‐Roque; Natalia Jimenez; Lina M. Ibanez; Paula Hurtado‐Villa

doi:10.1002/mgg3.1401

Molecular Genetics & Genomic Medicine (Oct 2020)

MYT1 role in the microtia‐craniofacial microsomia spectrum

Daniela V. Luquetti,
Carrie L. Heike,
Ignacio Zarante,
Andrew E. Timms,
Jonas Gustafson,
Harry Pachajoa,
Gloria L. Porras‐Hurtado,
Paola Ayala‐Ramirez,
Milagros M. Duenas‐Roque,
Natalia Jimenez,
Lina M. Ibanez,
Paula Hurtado‐Villa

Affiliations

Daniela V. Luquetti: University of Washington School of Medicine Seattle WA USA
Carrie L. Heike: University of Washington School of Medicine Seattle WA USA
Ignacio Zarante: Human Genomics Institute Pontificia Universidad Javeriana Bogotá Colombia
Andrew E. Timms: Seattle Children's Research Institute Seattle WA USA
Jonas Gustafson: Seattle Children's Research Institute Seattle WA USA
Harry Pachajoa: Universidad Icesi Cali Colombia
Gloria L. Porras‐Hurtado: Clinica Comfamiliar Risaralda Pereira Colombia
Paola Ayala‐Ramirez: Human Genomics Institute Pontificia Universidad Javeriana Bogotá Colombia
Milagros M. Duenas‐Roque: Hospital Edgardo Rebagliati Martins Lima Peru
Natalia Jimenez: Pontificia Universidad Javeriana Cali Colombia
Lina M. Ibanez: Pontificia Universidad Javeriana Cali Colombia
Paula Hurtado‐Villa: Pontificia Universidad Javeriana Cali Colombia

DOI: https://doi.org/10.1002/mgg3.1401
Journal volume & issue: Vol. 8, no. 10
pp. n/a – n/a

Abstract

Read online

Abstract Background Craniofacial microsomia (CFM), also known as the oculo‐auriculo‐vertebral spectrum, comprises a variable phenotype with the most common features including microtia and mandibular hypoplasia on one or both sides, in addition to lateral oral clefts, epibulbar dermoids, cardiac, vertebral, and renal abnormalities. The etiology of CFM is largely unknown. The MYT1 gene has been reported as a candidate based in mutations found in three unrelated individuals. Additional patients with mutations in this gene are required to establish its causality. We present two individuals with CFM that have rare variants in MYT1 contributing to better understand the genotype and phenotype associated with mutations in this gene. Methods/Results We conducted genetic analysis using whole‐exome and ‐genome sequencing in 128 trios with CFM. Two novel MYT1 mutations were identified in two participants. Sanger sequencing was used to confirm these mutations. Conclusion We identified two additional individuals with CFM who carry rare variants in MYT1, further supporting the presumptive role of this gene in the CFM spectrum.

Published in Molecular Genetics & Genomic Medicine

ISSN: 2324-9269 (Online)
Publisher: Wiley
Country of publisher: United States
LCC subjects: Science: Biology (General): Genetics
Website: https://onlinelibrary.wiley.com/journal/23249269

About the journal

Abstract

Keywords