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Arrhythmogenic right ventricular cardiomyopathy in patients with biallelic JUP-associated skin fragility.

Authors :
Vahidnezhad, Hassan
Youssefian, Leila
Faghankhani, Masoomeh
Mozafari, Nikoo
Saeidian, Amir Hossein
Niaziorimi, Fatemeh
Abdollahimajd, Fahimeh
Sotoudeh, Soheila
Rajabi, Fateme
Mirsafaei, Liaosadat
Sani, Zahra Alizadeh
Liu, Lu
Guy, Alyson
Zeinali, Sirous
Kariminejad, Ariana
Ho, Reginald T
McGrath, John A
Uitto, Jouni
Vahidnezhad, Hassan
Youssefian, Leila
Faghankhani, Masoomeh
Mozafari, Nikoo
Saeidian, Amir Hossein
Niaziorimi, Fatemeh
Abdollahimajd, Fahimeh
Sotoudeh, Soheila
Rajabi, Fateme
Mirsafaei, Liaosadat
Sani, Zahra Alizadeh
Liu, Lu
Guy, Alyson
Zeinali, Sirous
Kariminejad, Ariana
Ho, Reginald T
McGrath, John A
Uitto, Jouni
Source :
Department of Dermatology and Cutaneous Biology Faculty Papers
Publication Year :
2020

Abstract

Arrhythmogenic right ventricular cardiomyopathy (ARVC), with skin manifestations, has been associated with mutations in JUP encoding plakoglobin. Genotype-phenotype correlations regarding the penetrance of cardiac involvement, and age of onset have not been well established. We examined a cohort of 362 families with skin fragility to screen for genetic mutations with next-generation sequencing-based methods. In two unrelated families, a previously unreported biallelic mutation, JUP: c.201delC; p.Ser68Alafs*92, was disclosed. The consequences of this mutation were determined by expression profiling both at tissue and ultrastructural levels, and the patients were evaluated by cardiac and cutaneous work-up. Whole-transcriptome sequencing by RNA-Seq revealed JUP as the most down-regulated gene among 21 skin fragility-associated genes. Immunofluorescence showed the lack of plakoglobin in the epidermis. Two probands, 2.5 and 22-year-old, with the same homozygous mutation, allowed us to study the cross-sectional progression of cardiac involvements in relation to age. The older patient had anterior T wave inversions, prolonged terminal activation duration (TAD), and RV enlargement by echocardiogram, and together with JUP mutation met definite ARVC diagnosis. The younger patient had no evidence of cardiac disease, but met possible ARVC diagnosis with one major criterion (the JUP mutation). In conclusion, we identified the same biallelic homozygous JUP mutation in two unrelated families with skin fragility, but cardiac findings highlighted age-dependent penetrance of ARVC. Thus, young, phenotypically normal patients with biallelic JUP mutations should be monitored for development of ARVC.

Details

Database :
OAIster
Journal :
Department of Dermatology and Cutaneous Biology Faculty Papers
Notes :
application/pdf, English
Publication Type :
Electronic Resource
Accession number :
edsoai.on1237957741
Document Type :
Electronic Resource