Genetic Architecture of Dilated Cardiomyopathy in Individuals of African and European Ancestry

Elizabeth Jordan; Daniel D Kinnamon; Garrie J Haas; Mark Hofmeyer; Evan Kransdorf; Gregory A Ewald; Alanna A Morris; Anjali Owens; Brian Lowes; Douglas Stoller; W H Wilson Tang; Sonia Garg; Barry H Trachtenberg; Palak Shah; Salpy V Pamboukian; Nancy K Sweitzer; Matthew T Wheeler; Jane E Wilcox; Stuart Katz; Stephen Pan; Javier Jimenez; Daniel P Fishbein; Frank Smart; Jessica Wang; Stephen S Gottlieb; Daniel P Judge; Charles K Moore; Jonathan O Mead; Natalie Hurst; Jinwen Cao; Gordon S Huggins; Jason Cowan; Hanyu Ni; Heidi L Rehm; Gail P Jarvik; Matteo Vatta; Wylie Burke; Ray E Hershberger; DCM Precision Medicine Study of the DCM Consortium

doi:10.1001/jama.2023.11970

Genetic Architecture of Dilated Cardiomyopathy in Individuals of African and European Ancestry

JAMA. 2023 Aug 1;330(5):432-441. doi: 10.1001/jama.2023.11970.

Authors

Elizabeth Jordan^{1

2}, Daniel D Kinnamon^{1

2}, Garrie J Haas^{2

3}, Mark Hofmeyer⁴, Evan Kransdorf⁵, Gregory A Ewald⁶, Alanna A Morris⁷, Anjali Owens⁸, Brian Lowes⁹, Douglas Stoller⁹, W H Wilson Tang¹⁰, Sonia Garg¹¹, Barry H Trachtenberg¹², Palak Shah¹³, Salpy V Pamboukian^{14

15}, Nancy K Sweitzer^{16

17}, Matthew T Wheeler¹⁸, Jane E Wilcox¹⁹, Stuart Katz²⁰, Stephen Pan²¹, Javier Jimenez²², Daniel P Fishbein²³, Frank Smart²⁴, Jessica Wang²⁵, Stephen S Gottlieb²⁶, Daniel P Judge²⁷, Charles K Moore²⁸, Jonathan O Mead^{1

2}, Natalie Hurst^{1

2}, Jinwen Cao^{1

2}, Gordon S Huggins²⁹, Jason Cowan^{1

2}, Hanyu Ni^{1

2}, Heidi L Rehm³⁰, Gail P Jarvik^{31

32}, Matteo Vatta³³, Wylie Burke³⁴, Ray E Hershberger^{1

2

3}; DCM Precision Medicine Study of the DCM Consortium

Affiliations

¹ Division of Human Genetics, Department of Internal Medicine, The Ohio State University, Columbus.
² Davis Heart and Lung Research Institute, The Ohio State University, Columbus.
³ Division of Cardiovascular Medicine, Department of Internal Medicine, The Ohio State University, Columbus.
⁴ MedStar Health Research Institute, MedStar Washington Hospital Center, Washington, DC.
⁵ Smidt Heart Institute, Cedars-Sinai Medical Center, Los Angeles, California.
⁶ Washington University, St Louis, Missouri.
⁷ Emory University School of Medicine, Atlanta, Georgia.
⁸ Center for Inherited Cardiovascular Disease, Division of Cardiology, Perelman School of Medicine, University of Pennsylvania, Philadelphia.
⁹ University of Nebraska Medical Center, Omaha.
¹⁰ Cleveland Clinic, Cleveland, Ohio.
¹¹ University of Texas Southwestern Medical Center, Dallas.
¹² Houston Methodist DeBakey Heart and Vascular Center, J. C. Walter Jr Transplant Center, Houston, Texas.
¹³ Inova Heart and Vascular Institute, Falls Church, Virginia.
¹⁴ University of Alabama, Birmingham.
¹⁵ Now with University of Washington, Seattle.
¹⁶ Sarver Heart Center, University of Arizona, Tucson.
¹⁷ Now with Washington University, St Louis, Missouri.
¹⁸ Division of Cardiovascular Medicine, Stanford University School of Medicine, Stanford, California.
¹⁹ Northwestern University Feinberg School of Medicine, Chicago, Illinois.
²⁰ New York University Langone Medical Center, New York, New York.
²¹ Department of Cardiology, Westchester Medical Center and New York Medical College, Valhalla.
²² Miami Cardiac and Vascular Institute, Baptist Health South, Miami, Florida.
²³ University of Washington, Seattle.
²⁴ Louisiana State University Health Sciences Center, New Orleans.
²⁵ University of California Los Angeles Medical Center, Los Angeles.
²⁶ University of Maryland School of Medicine, Baltimore.
²⁷ Medical University of South Carolina, Charleston.
²⁸ University of Mississippi Medical Center, Jackson.
²⁹ Cardiology Division, Tufts Medical Center and Tufts University School of Medicine, Boston, Massachusetts.
³⁰ Center for Genomic Medicine, Massachusetts General Hospital, Boston.
³¹ Division of Medical Genetics, Department of Medicine, University of Washington, Seattle.
³² Department of Genome Sciences, University of Washington, Seattle.
³³ Departments of Medical and Molecular Genetics, Indiana University School of Medicine, Indianapolis.
³⁴ Department of Bioethics and Humanities, University of Washington, Seattle.

Abstract

Importance: Black patients with dilated cardiomyopathy (DCM) have increased familial risk and worse outcomes than White patients, but most DCM genetic data are from White patients.

Objective: To compare the rare variant genetic architecture of DCM by genomic ancestry within a diverse population of patients with DCM.

Design: Cross-sectional study enrolling patients with DCM who self-identified as non-Hispanic Black, Hispanic, or non-Hispanic White from June 7, 2016, to March 15, 2020, at 25 US advanced heart failure programs. Variants in 36 DCM genes were adjudicated as pathogenic, likely pathogenic, or of uncertain significance.

Exposure: Presence of DCM.

Main outcomes and measures: Variants in DCM genes classified as pathogenic/likely pathogenic/uncertain significance and clinically actionable (pathogenic/likely pathogenic).

Results: A total of 505, 667, and 26 patients with DCM of predominantly African, European, or Native American genomic ancestry, respectively, were included. Compared with patients of European ancestry, a lower percentage of patients of African ancestry had clinically actionable variants (8.2% [95% CI, 5.2%-11.1%] vs 25.5% [95% CI, 21.3%-29.6%]), reflecting the lower odds of a clinically actionable variant for those with any pathogenic variant/likely pathogenic variant/variant of uncertain significance (odds ratio, 0.25 [95% CI, 0.17-0.37]). On average, patients of African ancestry had fewer clinically actionable variants in TTN (difference, -0.09 [95% CI, -0.14 to -0.05]) and other genes with predicted loss of function as a disease-causing mechanism (difference, -0.06 [95% CI, -0.11 to -0.02]). However, the number of pathogenic variants/likely pathogenic variants/variants of uncertain significance was more comparable between ancestry groups (difference, -0.07 [95% CI, -0.22 to 0.09]) due to a larger number of non-TTN non-predicted loss of function variants of uncertain significance, mostly missense, in patients of African ancestry (difference, 0.15 [95% CI, 0.00-0.30]). Published clinical case-based evidence supporting pathogenicity was less available for variants found only in patients of African ancestry (P < .001).

Conclusion and relevance: Patients of African ancestry with DCM were less likely to have clinically actionable variants in DCM genes than those of European ancestry due to differences in genetic architecture and a lack of representation of African ancestry in clinical data sets.

Publication types

Research Support, N.I.H., Extramural

MeSH terms

American Indian or Alaska Native* / genetics
Black People* / genetics
Cardiomyopathy, Dilated* / ethnology
Cardiomyopathy, Dilated* / genetics
Cross-Sectional Studies
Genomics
Hispanic or Latino* / genetics
Humans
White People* / genetics

Substances

TTN protein, human

Abstract

Publication types

MeSH terms

Substances

Grants and funding