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Clinical Trajectory And Genetic Landscape Of Neonatal-Onset Hypertrophic Cardiomyopathy: Insights From A 30-Year Multicenter Cohort Study

Adorisio, R.; Cantarutti, N.; Di Marzio, S.; Ingrasciotta, G.; Franceschini, A.; Cavarretta, E.; D'Anna, C.; Mencarelli, E.; Martinelli, D.; Silvetti, M. S.; Drago, F.; Campanale, C. M.; Masci, M.; Novelli, A.; Magliozzi, M.; Di Chiara, L.; Galletti, L.; Calzolari, F.; Capolupo, I.; Amodeo, A.; Dotta, A.; Toscano, A.

2026-07-09 cardiovascular medicine
10.64898/2026.07.06.26357420 medRxiv
Show abstract

Background: Neonatal-onset hypertrophic cardiomyopathy (HCM) is a rare condition with limited data regarding clinical presentation, genetic background, and long-term outcomes. We aimed to characterize the phenotype and prognosis of HCM presenting in neonates. Methods: This is a multicenter retrospective study including patients diagnosed with HCM before 1 year of age. Neonatal-onset HCM was defined as presentation {less than or equal to}28 days of life. Clinical, genetic, instrumental data, treatment, and outcomes were collected. Primary outcome included overall and cardiac survival, major arrhythmic events (MAEs), implantable cardioverter-defibrillator (ICD) implantation, and cardiac surgery. Results: Among 321 pediatric HCM, 21% were diagnosed during infancy and 75% were neonates. Median age at diagnosis was 1 day (IQR 0-6), 82% presented within the first week of life. Prenatal suspicion was in 25%. At presentation, 41% were symptomatic. RASopathies represented the most common etiology (41%), followed by gene-elusive (31%), mitochondrial/inborn errors of metabolism (18%), and sarcomeric (8%). Left ventricular outflow tract obstruction was frequent in sarcomeric and RASopathy. Overall survival was 92% and cardiac survival was 96% at 2 years; long-term survival was 88% at 30 years. ICDs were implanted in 8%; 21% required cardiac surgery. Survival free from ICD was 40% at 15 year and 47% from myectomy. All events occurred in patients presenting within the first weeks of life. Conclusions: Neonatal-onset HCM is characterized by etiologic heterogeneity, predominance of syndromic and non-sarcomeric etiologies, and long-term cardiovascular morbidity. Presentation within the first days of life identifies a high-risk subgroup requiring intensive surveillance and specialized multidisciplinary management.

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