Genetic Contribution to End-Stage Cardiomyopathy Requiring Heart Transplantation.

Kim, Yuri; Gunnarsdóttir, Oddný Brattberg; Viveiros, Anissa; Reichart, Daniel; Quiat, Daniel; Willcox, Jon A L; Zhang, Hao; Chen, Huachen; Curran, Justin J; Kim, Daniel H; Urschel, Simon; McDonough, Barbara; Gorham, Joshua; DePalma, Steven R; Seidman, Jonathan G; Seidman, Christine E; Oudit, Gavin Y

Kim, Yuri; Gunnarsdóttir, Oddný Brattberg; Viveiros, Anissa; Reichart, Daniel; Quiat, Daniel; Willcox, Jon A L; Zhang, Hao; Chen, Huachen; Curran, Justin J; Kim, Daniel H; Urschel, Simon; McDonough, Barbara; Gorham, Joshua; DePalma, Steven R; Seidman, Jonathan G; Seidman, Christine E; Oudit, Gavin Y.

Affiliation

Kim Y; Division of Cardiovascular Medicine, Brigham and Women's Hospital (Y.K., B.M., C.E.S.).
Gunnarsdóttir OB; Department of Genetics, Harvard Medical School, Boston, MA (Y.K., O.B.G., D.R., D.Q., J.A.L.W., J.J.C., J.G., S.R.D., J.G.S., C.E.S.).
Viveiros A; Department of Genetics, Harvard Medical School, Boston, MA (Y.K., O.B.G., D.R., D.Q., J.A.L.W., J.J.C., J.G., S.R.D., J.G.S., C.E.S.).
Reichart D; Department of Medicine (A.V., H.Z., H.C., D.H.K., G.Y.O.), University of Alberta.
Quiat D; Mazankowski Alberta Heart Institute, Edmonton, Canada (A.V., H.Z., H.C., D.H.K., G.Y.O.).
Willcox JAL; Department of Genetics, Harvard Medical School, Boston, MA (Y.K., O.B.G., D.R., D.Q., J.A.L.W., J.J.C., J.G., S.R.D., J.G.S., C.E.S.).
Zhang H; Department of Medicine I, University Hospital, Ludwig Maximilian University of Munich, Germany (D.R.).
Chen H; Department of Genetics, Harvard Medical School, Boston, MA (Y.K., O.B.G., D.R., D.Q., J.A.L.W., J.J.C., J.G., S.R.D., J.G.S., C.E.S.).
Curran JJ; Department of Cardiology, Boston Children's Hospital, MA (D.Q.).
Kim DH; Department of Genetics, Harvard Medical School, Boston, MA (Y.K., O.B.G., D.R., D.Q., J.A.L.W., J.J.C., J.G., S.R.D., J.G.S., C.E.S.).
Urschel S; Department of Medicine (A.V., H.Z., H.C., D.H.K., G.Y.O.), University of Alberta.
McDonough B; Mazankowski Alberta Heart Institute, Edmonton, Canada (A.V., H.Z., H.C., D.H.K., G.Y.O.).
Gorham J; Department of Medicine (A.V., H.Z., H.C., D.H.K., G.Y.O.), University of Alberta.
DePalma SR; Mazankowski Alberta Heart Institute, Edmonton, Canada (A.V., H.Z., H.C., D.H.K., G.Y.O.).
Seidman JG; Department of Genetics, Harvard Medical School, Boston, MA (Y.K., O.B.G., D.R., D.Q., J.A.L.W., J.J.C., J.G., S.R.D., J.G.S., C.E.S.).
Seidman CE; Department of Medicine (A.V., H.Z., H.C., D.H.K., G.Y.O.), University of Alberta.
Oudit GY; Mazankowski Alberta Heart Institute, Edmonton, Canada (A.V., H.Z., H.C., D.H.K., G.Y.O.).

Circ Genom Precis Med ; 16(5): 452-461, 2023 10.

Article in En | MEDLINE | ID: mdl-37767697

ABSTRACT

BACKGROUND: Many cardiovascular disorders propel the development of advanced heart failure that necessitates cardiac transplantation. When treatable causes are excluded, studies to define causes are often abandoned, resulting in a diagnosis of end-stage idiopathic cardiomyopathy. We studied whether DNA sequence analyses could identify unrecognized causes of end-stage nonischemic cardiomyopathy requiring heart transplantation and whether the prevalence of genetic causes differed from ambulatory cardiomyopathy cases. METHODS: We performed whole exome and genome sequencing of 122 explanted hearts from 101 adult and 21 pediatric patients with idiopathic cardiomyopathy from a single center. Data were analyzed for pathogenic/likely pathogenic variants in nuclear and mitochondrial genomes and assessed for nonhuman microbial sequences. The frequency of damaging genetic variants was compared among cardiomyopathy cohorts with different clinical severity. RESULTS: Fifty-four samples (44.3%) had pathogenic/likely pathogenic cardiomyopathy gene variants. The frequency of pathogenic variants was similar in pediatric (42.9%) and adult (43.6%) samples, but the distribution of mutated genes differed (P=8.30×10-4). The prevalence of causal genetic variants was significantly higher in end-stage than in previously reported ambulatory adult dilated cardiomyopathy cases (P<0.001). Among remaining samples with unexplained causes, no damaging mitochondrial variants were identified, but 28 samples contained parvovirus genome sequences, including 2 samples with 6- to 9-fold higher levels than the overall mean levels in other samples. CONCLUSIONS: Pathogenic variants and viral myocarditis were identified in 45.9% of patients with unexplained end-stage cardiomyopathy. Damaging gene variants are significantly more frequent among transplant compared with patients with ambulatory cardiomyopathy. Genetic analyses can help define cause of end-stage cardiomyopathy to guide management and risk stratification of patients and family members.

Subject(s)

Cardiomyopathies; Cardiomyopathy, Dilated; Heart Failure; Heart Transplantation; Adult; Humans; Child; Cardiomyopathies/genetics; Cardiomyopathies/pathology; Cardiomyopathy, Dilated/genetics; Cardiomyopathy, Dilated/surgery; Cardiomyopathy, Dilated/diagnosis; Heart Failure/diagnosis

Key words

cardiomyopathies; genetics; heart failure; transplantation; whole exome sequencing; whole genome sequencing

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Full text: 1 Collection: 01-internacional Database: MEDLINE Main subject: Cardiomyopathy, Dilated / Heart Transplantation / Heart Failure / Cardiomyopathies Type of study: Risk_factors_studies Limits: Adult / Child / Humans Language: En Journal: Circ Genom Precis Med Year: 2023 Document type: Article Country of publication: United States

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