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Assessment of the Genetic Spectrum of Uncombable Hair Syndrome in a Cohort of 107 Individuals

Authors :
F. Buket Basmanav
Nicole Cesarato
Sheetal Kumar
Oleg Borisov
Pavlos Kokordelis
Damian J. Ralser
Maria Wehner
Daisy Axt
Xing Xiong
Holger Thiele
Vadim Dolgin
Yasmina Gossmann
Nadine Fricker
Malin Katharina Dewenter
Karsten Weller
Mohnish Suri
Herbert Reichenbach
Vinzenz Oji
Marie-Claude Addor
Karla Ramirez
Helen Stewart
Natalie Garcia Bartels
Lisa Weibel
Nicola Wagner
Susannah George
Arzu Kilic
Iliana Tantcheva-Poor
Alison Stewart
Nicola Dikow
Bettina Blaumeiser
Márta Medvecz
Ulrike Blume-Peytavi
Paul Farrant
Ramon Grimalt
Sara Bertok
Lisa Bradley
Marina Eskin-Schwartz
Ohad Samuel Birk
Anette Bygum
Michel Simon
Peter Krawitz
Christine Fischer
Henning Hamm
Günter Fritz
Regina C. Betz
Source :
JAMA dermatology
Publication Year :
2023

Abstract

ImportanceUncombable hair syndrome (UHS) is a rare hair shaft anomaly that manifests during infancy and is characterized by dry, frizzy, and wiry hair that cannot be combed flat. Only about 100 known cases have been reported so far.ObjectiveTo elucidate the genetic spectrum of UHS.Design, Setting, and ParticipantsThis cohort study includes 107 unrelated index patients with a suspected diagnosis of UHS and family members who were recruited worldwide from January 2013 to December 2021. Participants of all ages, races, and ethnicities were recruited at referral centers or were enrolled on their own initiative following personal contact with the authors. Genetic analyses were conducted in Germany from January 2014 to December 2021.Main Outcomes and MeasuresClinical photographs, Sanger or whole-exome sequencing and array-based genotyping of DNA extracted from blood or saliva samples, and 3-dimensional protein modeling. Descriptive statistics, such as frequency counts, were used to describe the distribution of identified pathogenic variants and genotypes.ResultsThe genetic characteristics of patients with UHS were established in 80 of 107 (74.8%) index patients (82 [76.6%] female) who carried biallelic pathogenic variants in PADI3, TGM3, or TCHH (ie, genes that encode functionally related hair shaft proteins). Molecular genetic findings from 11 of these 80 individuals were previously published. In 76 (71.0%) individuals, the UHS phenotype were associated with pathogenic variants in PADI3. The 2 most commonly observed PADI3 variants account for 73 (48.0%) and 57 (37.5%) of the 152 variant PADI3 alleles in total, respectively. Two individuals carried pathogenic variants in TGM3, and 2 others carried pathogenic variants in TCHH. Haplotype analyses suggested a founder effect for the 4 most commonly observed pathogenic variants in the PADI3 gene.Conclusions and RelevanceThis cohort study extends and gives an overview of the genetic variant spectrum of UHS based on molecular genetic analyses of the largest worldwide collective of affected individuals, to our knowledge. Formerly, a diagnosis of UHS could only be made by physical examination of the patient and confirmed by microscopical examination of the hair shaft. The discovery of pathogenic variants in PADI3, TCHH, and TGM3 may open a new avenue for clinicians and affected individuals by introducing molecular diagnostics for UHS.

Details

ISSN :
21686084 and 21686068
Volume :
158
Issue :
11
Database :
OpenAIRE
Journal :
JAMA dermatology
Accession number :
edsair.doi.dedup.....64d98f654eadba90de7c6182c524354d