Regional Variation in RBM20 Causes a Highly Penetrant Arrhythmogenic Cardiomyopathy

Overview

Journal Circ Heart Fail

Specialty Cardiology & Vascular Diseases

Date 2019 Mar 16

PMID 30871351

Citations 65

Authors

Victoria N Parikh

Colleen Caleshu

Chloe Reuter

Laura C Lazzeroni

Jodie Ingles

John Garcia

Kristen McCaleb

Tolulope Adesiyun

Farbod Sedaghat-Hamedani

Saurabh Kumar

Sharon Graw

Marta Gigli

Davide Stolfo

Matteo Dal Ferro

Alexander Y Ing

Robert Nussbaum

Birgit Funke

Matthew T Wheeler

Ray E Hershberger

Stuart Cook

Lars M Steinmetz

Neal K Lakdawala

Matthew R G Taylor

Luisa Mestroni

Marco Merlo

Gianfranco Sinagra

Christopher Semsarian

Benjamin Meder

Daniel P Judge

Euan Ashley

Affiliations

Soon will be listed here.

Abstract

Background Variants in the cardiomyocyte-specific RNA splicing factor RBM20 have been linked to familial cardiomyopathy, but the causative genetic architecture and clinical consequences of this disease are incompletely defined. Methods and Results To define the genetic architecture of RBM20 cardiomyopathy, we first established a database of RBM20 variants associated with cardiomyopathy and compared these to variants observed in the general population with respect to their location in the RBM20 coding transcript. We identified 2 regions significantly enriched for cardiomyopathy-associated variants in exons 9 and 11. We then assembled a registry of 74 patients with RBM20 variants from 8 institutions across the world (44 index cases and 30 from cascade testing). This RBM20 patient registry revealed highly prevalent family history of sudden cardiac death (51%) and cardiomyopathy (72%) among index cases and a high prevalence of composite arrhythmias (including atrial fibrillation, nonsustained ventricular tachycardia, implantable cardiac defibrillator discharge, and sudden cardiac arrest, 43%). Patients harboring variants in cardiomyopathy-enriched regions identified by our variant database analysis were enriched for these findings. Further, these characteristics were more prevalent in the RBM20 registry than in large cohorts of patients with dilated cardiomyopathy and TTNtv cardiomyopathy and not significantly different from a cohort of patients with LMNA-associated cardiomyopathy. Conclusions Our data establish RBM20 cardiomyopathy as a highly penetrant and arrhythmogenic cardiomyopathy. These findings underline the importance of arrhythmia surveillance and family screening in this disease and represent the first step in defining the genetic architecture of RBM20 disease causality on a population level.

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