PRDM16 Deletion Is Associated With Sex-dependent Cardiomyopathy and Cardiac Mortality: A Translational, Multi-Institutional Cohort Study.

医学 心肌病 回顾性队列研究 内科学 队列 心脏病学 病理 心力衰竭
作者
Ryan J Kramer,Amir Nima Fatahian,Alice Chan,Jeffery Mortenson,Jennifer Osher,Bo Sun,Lauren E Parker,Michael B. Rosamilia,Kyra B Potter,Kaila Moore,Sage L Atkins,Jill A. Rosenfeld,Alona Birjiniuk,Edward Jones,Taylor S Howard,Jeffrey J. Kim,Daryl A. Scott,Seema Lalani,Omid M T Rouzbehani,Samantha Kaplan,Marissa A Hathaway,Jennifer L Cohen,S Yukiko Asaki,Hugo R. Martinez,Sihem Boudina,Andrew P. Landstrom
出处
期刊:PubMed 卷期号:: e003912-e003912
标识
DOI:10.1161/circgen.122.003912
摘要

1p36 deletion syndrome can predispose to pediatric-onset cardiomyopathy. Deletion breakpoints are variable and may delete the transcription factor PRDM16. Early studies suggest that deletion of PRDM16 may underlie cardiomyopathy in patients with 1p36 deletion; however, the prognostic impact of PRDM16 loss is unknown.This retrospective cohort included subjects with 1p36 deletion syndrome from 4 hospitals. Prevalence of cardiomyopathy and freedom from death, cardiac transplantation, or ventricular assist device were analyzed. A systematic review cohort was derived for further analysis. A cardiac-specific Prdm16 knockout mouse (Prdm16 conditional knockout) was generated. Echocardiography was performed at 4 and 6 to 7 months. Histology staining and qPCR were performed at 7 months to assess fibrosis.The retrospective cohort included 71 patients. Among individuals with PRDM16 deleted, 34.5% developed cardiomyopathy versus 7.7% of individuals with PRDM16 not deleted (P=0.1). In the combined retrospective and systematic review cohort (n=134), PRDM16 deletion-associated cardiomyopathy risk was recapitulated and significant (29.1% versus 10.8%, P=0.03). PRDM16 deletion was associated with increased risk of death, cardiac transplant, or ventricular assist device (P=0.04). Among those PRDM16 deleted, 34.5% of females developed cardiomyopathy versus 16.7% of their male counterparts (P=0.2). We find sex-specific differences in the incidence and the severity of contractile dysfunction and fibrosis in female Prdm16 conditional knockout mice. Further, female Prdm16 conditional knockout mice demonstrate significantly elevated risk of mortality (P=0.0003).PRDM16 deletion is associated with a significantly increased risk of cardiomyopathy and cardiac mortality. Prdm16 conditional knockout mice develop cardiomyopathy in a sex-biased way. Patients with PRDM16 deletion should be assessed for cardiac disease.

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