Longitudinal assessment of structural phenotype in Brugada syndrome using cardiac magnetic resonance imaging

Longitudinal assessment of structural phenotype in Brugada syndrome using cardiac magnetic resonance imaging.

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Item Type: Article
Status: Published
Official URL: https://doi.org/10.1016/j.hroo.2022.10.004
Journal or Publication Title: Heart Rhythm O2
Volume: 4
Number: 1
Page Range: pp. 34-41
Date: 1 January 2023
Divisions: Molecular Cardiology
Depositing User: General Admin
Identification Number: 10.1016/j.hroo.2022.10.004
ISSN: 26665018
Date Deposited: 15 Mar 2023 03:17
Abstract:

Background
Despite historically being considered a channelopathy, subtle structural changes have been reported in Brugada syndrome (BrS) on histopathology and cardiac magnetic resonance (CMR) imaging. It is not known if these structural changes progress over time.

Objective
The study sought to assess if structural changes in BrS evolve over time with serial CMR assessment and to investigate the utility of parametric mapping techniques to identify diffuse fibrosis in BrS.

Methods
Patients with a diagnosis of BrS based on international guidelines and normal CMR at least 3 years prior to the study period were invited to undergo repeat CMR. CMR images were analyzed de novo and compared at baseline and follow-up.

Results
Eighteen patients with BrS (72% men; mean age at follow-up 47.4 ± 8.9 years) underwent serial CMR with an average of 5.0 ± 1.7 years between scans. No patients had late gadolinium enhancement (LGE) on baseline CMR, but 4 (22%) developed LGE on follow-up, typically localized to the right ventricular (RV) side of the basal septum. RV end-systolic volume increased over time (P = .04) and was associated with a trend toward reduction in RV ejection fraction (P = .07). Four patients showed a reduction in RV ejection fraction >10%. There was no evidence of diffuse myocardial fibrosis observed on parametric mapping.

Conclusions
Structural changes may evolve over time with development of focal fibrosis, evidenced by LGE on CMR in a significant proportion of patients with BrS. These findings have implications for our understanding of the pathological substrate in BrS and the longitudinal evaluation of patients with BrS.

Creators:
Creators
Email
Isbister, Julia C.
UNSPECIFIED
Gray, Belinda
UNSPECIFIED
Offen, Sophie
UNSPECIFIED
Yeates, Laura
UNSPECIFIED
Naoum, Chris
UNSPECIFIED
Medi, Caroline
UNSPECIFIED
Raju, Hariharan
UNSPECIFIED
Semsarian, Christopher
UNSPECIFIED
Puranik, Rajesh
UNSPECIFIED
Sy, Raymond W.
UNSPECIFIED
Last Modified: 15 Mar 2023 03:17
URI: https://eprints.centenary.org.au/id/eprint/1447

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