TY - JOUR
T1 - Genetic Architecture of Dilated Cardiomyopathy in Individuals of African and European Ancestry
AU - Jordan, Elizabeth
AU - Kinnamon, Daniel D.
AU - Haas, Garrie J.
AU - Hofmeyer, Mark
AU - Kransdorf, Evan
AU - Ewald, Gregory A.
AU - Morris, Alanna A.
AU - Owens, Anjali
AU - Lowes, Brian
AU - Stoller, Douglas
AU - Tang, W. H.Wilson
AU - Garg, Sonia
AU - Trachtenberg, Barry H.
AU - Shah, Palak
AU - Pamboukian, Salpy V.
AU - Sweitzer, Nancy K.
AU - Wheeler, Matthew T.
AU - Wilcox, Jane E.
AU - Katz, Stuart
AU - Pan, Stephen
AU - Jimenez, Javier
AU - Fishbein, Daniel P.
AU - Smart, Frank
AU - Wang, Jessica
AU - Gottlieb, Stephen S.
AU - Judge, Daniel P.
AU - Moore, Charles K.
AU - Mead, Jonathan O.
AU - Hurst, Natalie
AU - Cao, Jinwen
AU - Huggins, Gordon S.
AU - Cowan, Jason
AU - Ni, Hanyu
AU - Rehm, Heidi L.
AU - Jarvik, Gail P.
AU - Vatta, Matteo
AU - Burke, Wylie
AU - Hershberger, Ray E.
N1 - Publisher Copyright:
© 2023 American Medical Association. All rights reserved.
PY - 2023/8/1
Y1 - 2023/8/1
N2 - 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.
AB - 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.
UR - http://www.scopus.com/inward/record.url?scp=85166384994&partnerID=8YFLogxK
U2 - 10.1001/jama.2023.11970
DO - 10.1001/jama.2023.11970
M3 - Article
C2 - 37526719
AN - SCOPUS:85166384994
SN - 0098-7484
VL - 330
SP - 432
EP - 441
JO - JAMA
JF - JAMA
IS - 5
ER -