Prevalence and determinants of atrial fibrillation progression in paroxysmal atrial fibrillation

Author:

Nguyen Bao-OanhORCID,Weberndorfer Vanessa,Crijns Harry JGMORCID,Geelhoed Bastiaan,Ten Cate Hugo,Spronk Henri,Kroon Abraham,De With Ruben,Al-Jazairi Meelad,Maass Alexander HORCID,Blaauw YuriORCID,Tieleman Robert G,Hemels Martin E W,Luermans Justin,de Groot Joris,Allaart Cornelis P,Elvan ArifORCID,De Melis Mirko,Scheerder Coert,van Zonneveld Anton Jan,Schotten Ulrich,Linz Dominik,Van Gelder IsabelleORCID,Rienstra MichielORCID

Abstract

ObjectiveAtrial fibrillation (AF) often progresses from paroxysmal AF (PAF) to more permanent forms. To improve personalised medicine, we aim to develop a new AF progression risk prediction model in patients with PAF.MethodsIn this interim-analysis of the Reappraisal of AF: Interaction Between HyperCoagulability, Electrical Remodelling, and Vascular Destabilisation in the Progression of AF study, patients with PAF undergoing extensive phenotyping at baseline and continuous rhythm monitoring during follow-up of ≥1 year were analysed. AF progression was defined as (1) progression to persistent or permanent AF or (2) progression of PAF with >3% burden increase. Multivariable analysis was done to identify predictors of AF progression.ResultsMean age was 65 (58–71) years, 179 (43%) were female. Follow-up was 2.2 (1.6–2.8) years, 51 of 417 patients (5.5%/year) showed AF progression. Multivariable analysis identified, PR interval, impaired left atrial function, mitral valve regurgitation and waist circumference to be associated with AF progression. Adding blood biomarkers improved the model (C-statistic from 0.709 to 0.830) and showed male sex, lower levels of factor XIIa:C1-esterase inhibitor and tissue factor pathway inhibitor, and higher levels of N-terminal pro-brain natriuretic peptide, proprotein convertase subtilisin/kexin type 9 and peptidoglycan recognition protein 1 were associated with AF progression.ConclusionIn patients with PAF, AF progression occurred in 5.5%/year. Predictors for progression included markers for atrial remodelling, sex, mitral valve regurgitation, waist circumference and biomarkers associated with coagulation, inflammation, cardiomyocyte stretch and atherosclerosis. These prediction models may help to determine risk of AF progression and treatment targets, but validation is needed.Trial registration numberNCT02726698.

Funder

Hartstichting

Medtronic Trading

Publisher

BMJ

Subject

Cardiology and Cardiovascular Medicine

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