Incidence and Outcomes of Atrial Fibrillation and Systolic Dysfunction in Patients Receiving Mavacamten for Obstructive Hypertrophic Cardiomyopathy: A Multicenter Study.

Publication Title

medRxiv

Authors

Olives Nguyen
Jack Wiedrick
Daniele Massera
Elizabeth Adlestein
Sumar Frejat
Matteo Castrichini
Said Alsidawi
John R Giudicessi
Jeffrey B Geske
Richard T Carrick
Jose Madrazo
Nicole Dellise
Mark A Zenker
Thomas A Boyle
Nosheen Reza
Anjali Tiku Owens
David S Frankel
Prabhjot Hundal
Jamil Tajik
Patrycja Galazka
Myra Lewontin
Michael Ayers
Timothy Wong
Michael Flanagan
Sumeet Singh Mitter
Arjun Kanwal
Ozlem Bilen
Sarah Baghdadi
Hirak Shah
Jared Kvapil
Paola Roldan
Loren Berenbom
Jill Jesurum
Denise Tootill
Alice Siqueira-Benzow
Mariko Harper
Danish Saleh
Lubna Choudhury
Isabela Valenta
Melissa Lang
Dermot M Phelan
Dmitry Prizand
Neal Lakdawala
Carolyn Y Ho
Lusha W Liang
Shepard D Weiner
Sririam Ravi, Providence Heart Institute, Portland, OR USAFollow
Ahmed Sami Abuzaid
Mohammed Makkiya
Jeremy S Markowitz
Mark Sherrid
Ahmad Masri

Document Type

Article

Publication Date

9-19-2025

Keywords

oregon; portland

Abstract

IMPORTANCE: Mavacamten is highly effective in treating symptomatic obstructive hypertrophic cardiomyopathy (oHCM) and was approved for commercial use with a risk mitigation program (REMS) to monitor the impact on left ventricular systolic function (LVSD). The impact of mavacamten on atrial fibrillation (AF) occurrence is not well characterized.

OBJECTIVE: Determine the real-world incidence of new-onset and recurrent AF among patients with HCM treated with commercial mavacamten. Secondary objectives included assessing the incidences of LVSD, heart failure (HF), and cardiogenic shock.

DESIGN: A multicenter cohort study. Center-level data were aggregated for patients who received mavacamten from May 2022 through December 2024.

SETTING: Twenty-one outpatient HCM centers in the United States.

PARTICIPANTS: Consecutive patients ≥18 years of age with oHCM were included; those with permanent AF were excluded.

EXPOSURES: At least one dose of commercial mavacamten.

MAIN OUTCOMES AND MEASURES: Incidence of new-onset and recurrent AF, LVSD, HF, and cardiogenic shock.

RESULTS: Among 1,538 patients (median age, 66 years [95% CI, 65.9-66.1]; 57% female [95% CI, 54-59%]), 25% [95% CI, 22-27%] had prior AF. Median mavacamten exposure was 13.4 months [95% CI, 11.8-15.0]. Overall AF incidence was 13% [95% CI, 10-17%], including 5% [95% CI, 4-7%] new-onset and 39% [95% CI, 27-51%] recurrent AF in those with history of AF prior to mavacamten initiation. LVEF < 50% occurred in 8% [95% CI, 6-9%], of whom 70% had AF. Symptomatic HF occurred in 1.5% [95% CI, 0.8-2.2%], cardiogenic shock in 0.6% [95% CI, 0.1-1.0%], and an overall permanent discontinuation of mavacamten in 7% [95% CI, 4-10%].

CONCLUSIONS AND RELEVANCE: In this multicenter cohort receiving commercial mavacamten, we identified an annual incidence of 5% new-onset AF and 39% recurrent AF, while 70% of patients who developed LVEF< 50% had concurrent AF. Given this association and the morbidity that can be associated with AF, protocols for LVEF assessment and aggressive rhythm management following AF detection may be warranted to improve patient care. Further studies are needed to improve understanding of the impact of mavacamten on AF and patient outcomes.

Area of Special Interest

Cardiovascular (Heart)

Specialty/Research Institute

Cardiology

Specialty/Research Institute

Pharmacy

DOI

10.1101/2025.09.15.25335783