Rare Variant Genetics and Dilated Cardiomyopathy Severity: The DCM Precision Medicine Study.

Hofmeyer, Mark; Haas, Garrie J; Jordan, Elizabeth; Cao, Jinwen; Kransdorf, Evan; Ewald, Gregory A; Morris, Alanna A; Owens, Anjali; Lowes, Brian; Stoller, Douglas; Wilson Tang, W H; Garg, Sonia; Trachtenberg, Barry H; Shah, Palak; Pamboukian, Salpy V; Sweitzer, Nancy K; Wheeler, Matthew T; Wilcox, Jane E; Katz, Stuart; Pan, Stephen; Jimenez, Javier; Smart, Frank; Wang, Jessica; Gottlieb, Stephen S; Judge, Daniel P; Moore, Charles K; Huggins, Gordon S; Kinnamon, Daniel D; Ni, Hanyu; Hershberger, Ray E

Hofmeyer, Mark; Haas, Garrie J; Jordan, Elizabeth; Cao, Jinwen; Kransdorf, Evan; Ewald, Gregory A; Morris, Alanna A; Owens, Anjali; Lowes, Brian; Stoller, Douglas; Wilson Tang, W H; Garg, Sonia; Trachtenberg, Barry H; Shah, Palak; Pamboukian, Salpy V; Sweitzer, Nancy K; Wheeler, Matthew T; Wilcox, Jane E; Katz, Stuart; Pan, Stephen; Jimenez, Javier; Smart, Frank; Wang, Jessica; Gottlieb, Stephen S; Judge, Daniel P; Moore, Charles K; Huggins, Gordon S; Kinnamon, Daniel D; Ni, Hanyu; Hershberger, Ray E.

Afiliação

Hofmeyer M; MedStar Health Research Institute, Medstar Washington Hospital Center, Washington, DC (M.H.).
Haas GJ; The Davis Heart and Lung Research Institute (G.J.H., E.J., J.C., D.D.K., H.N., R.E.H.), Department of Internal Medicine, The Ohio State University, Columbus.
Jordan E; Divisions of Cardiovascular Medicine (G.J.H., R.E.H.), Department of Internal Medicine, The Ohio State University, Columbus.
Cao J; Cardiology Division, Tufts Medical Center and Tufts University School of Medicine, Boston, MA (G.S.H.).
Kransdorf E; The Davis Heart and Lung Research Institute (G.J.H., E.J., J.C., D.D.K., H.N., R.E.H.), Department of Internal Medicine, The Ohio State University, Columbus.
Ewald GA; Human Genetics (E.J., J.C., D.D.K., H.N., R.E.H.), Department of Internal Medicine, The Ohio State University, Columbus.
Morris AA; The Davis Heart and Lung Research Institute (G.J.H., E.J., J.C., D.D.K., H.N., R.E.H.), Department of Internal Medicine, The Ohio State University, Columbus.
Owens A; Human Genetics (E.J., J.C., D.D.K., H.N., R.E.H.), Department of Internal Medicine, The Ohio State University, Columbus.
Lowes B; Smidt Heart Institute, Cedars-Sinai Medical Center, Los Angeles, CA (E.K.).
Stoller D; Washington University, St Louis, MO (G.A.E.).
Wilson Tang WH; Emory University School of Medicine, Atlanta, GA (A.A.M.).
Garg S; Center for Inherited Cardiovascular Disease, Division of Cardiology, Perelman School of Medicine, University of Pennsylvania, Philadelphia (A.O.).
Trachtenberg BH; University of Nebraska Medical Center, Omaha (B.L., D.S.).
Shah P; University of Nebraska Medical Center, Omaha (B.L., D.S.).
Pamboukian SV; Heart Vascular and Thoracic Institute, Cleveland Clinic, OH (W.H.W.T.).
Sweitzer NK; University of Texas Southwestern Medical Center, Dallas (S.G.).
Wheeler MT; Houston Methodist DeBakey Heart and Vascular Center, J.C. Walter Jr Transplant Center, TX (B.H.T.).
Wilcox JE; Inova Heart and Vascular Institute, Falls Church, VA (P.S.).
Katz S; University of Alabama, Birmingham, during study conduct; current affiliation, University of Washington, Seattle (S.V.P.).
Pan S; Sarver Heart Center, University of Arizona, Tucson, during study conduct; current affiliation, Washington University, St Louis, MO (N.K.S.).
Jimenez J; Division of Cardiovascular Medicine, Stanford University School of Medicine, CA (M.T.W.).
Smart F; Northwestern University Feinberg School of Medicine, Chicago, IL (J.E.W.).
Wang J; New York University Langone Medical Center, New York (S.K., S.P.).
Gottlieb SS; New York University Langone Medical Center, New York (S.K., S.P.).
Judge DP; current affiliation, Department of Cardiology, Westchester Medical Center & New York Medical College, Valhalla, NY (S.P.).
Moore CK; Miami Cardiac & Vascular Institute, Baptist Health South, FL (J.J.).
Huggins GS; Louisiana State University Health Sciences Center, New Orleans (F.S.).
Kinnamon DD; University of California Los Angeles Medical Center (J.W.).
Ni H; University of Maryland School of Medicine, Baltimore (S.S.G.).
Hershberger RE; Medical University of South Carolina, Charleston (D.P.J.).

Circulation ; 148(11): 872-881, 2023 09 12.

Article em En | MEDLINE | ID: mdl-37641966

ABSTRACT

ABSTRACT

BACKGROUND:

Dilated cardiomyopathy (DCM) can lead to advanced disease, defined herein as necessitating a durable left ventricular assist device or a heart transplant (LVAD/HT). DCM is known to have a genetic basis, but the association of rare variant genetics with advanced DCM has not been studied.

METHODS:

We analyzed clinical and genetic sequence data from patients enrolled between 2016 and 2021 in the US multisite DCM Precision Medicine Study, which was a geographically diverse, multiracial, multiethnic cohort. Clinical evaluation included standardized patient interview and medical record query forms. DCM severity was classified into 3 groups patients with advanced disease with LVAD/HT; patients with an implantable cardioverter defibrillator (ICD) only; or patients with no ICD or LVAD/HT. Rare variants in 36 DCM genes were classified as pathogenic or likely pathogenic or variants of uncertain significance. Confounding factors we considered included demographic characteristics, lifestyle factors, access to care, DCM duration, and comorbidities. Crude and adjusted associations between DCM severity and rare variant genetic findings were assessed using multinomial models with generalized logit link.

RESULTS:

Patients' mean (SD) age was 51.9 (13.6) years; 42% were of African ancestry, 56% were of European ancestry, and 44% were female. Of 1198 patients, 347 had LVAD/HT, 511 had an ICD, and 340 had no LVAD/HT or ICD. The percentage of patients with pathogenic or likely pathogenic variants was 26.2%, 15.9%, and 15.0% for those with LVAD/HT, ICD only, or neither, respectively. After controlling for sociodemographic characteristics and comorbidities, patients with DCM with LVAD/HT were more likely than those without LVAD/HT or ICD to have DCM-related pathogenic or likely pathogenic rare variants (odds ratio, 2.3 [95% CI, 1.5-3.6]). The association did not differ by ancestry. Rare variant genetic findings were similar between patients with DCM with an ICD and those without LVAD/HT or ICD.

CONCLUSIONS:

Advanced DCM was associated with higher odds of rare variants in DCM genes adjudicated as pathogenic or likely pathogenic, compared with individuals with less severe DCM. This finding may help assess the risk of outcomes in management of patients with DCM and their at-risk family members. REGISTRATION URL https//www. CLINICALTRIALS gov; Unique identifier NCT03037632.

Assuntos

Cardiomiopatia Dilatada; Medicina de Precisão; Feminino; Humanos; Masculino; Pessoa de Meia-Idade; População Negra; Cardiomiopatia Dilatada/epidemiologia; Cardiomiopatia Dilatada/etnologia; Cardiomiopatia Dilatada/genética; Cardiomiopatia Dilatada/terapia; Desfibriladores Implantáveis; Avaliação de Medicamentos; Adulto; Idoso; Brancos; Negro ou Afro-Americano; Estados Unidos/epidemiologia

Palavras-chave

cardiomyopathy, dilated; genetics; risk

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Texto completo: 1 Base de dados: MEDLINE Assunto principal: Cardiomiopatia Dilatada / Medicina de Precisão Tipo de estudo: Clinical_trials / Diagnostic_studies / Prognostic_studies Limite: Adult / Aged / Female / Humans / Male / Middle aged País/Região como assunto: America do norte Idioma: En Revista: Circulation Ano de publicação: 2023 Tipo de documento: Article

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