Prevalence and Cumulative Risk of Familial Idiopathic Dilated Cardiomyopathy

被引:45
作者
Huggins, Gordon S. [1 ,2 ]
Kinnamon, Daniel D. [3 ,4 ]
Haas, Garrie J. [4 ,5 ]
Jordan, Elizabeth [3 ,4 ]
Hofmeyer, Mark [6 ]
Kransdorf, Evan [7 ]
Ewald, Gregory A. [8 ]
Morris, Alanna A. [9 ]
Owens, Anjali [10 ]
Lowes, Brian [11 ]
Stoller, Douglas [11 ]
Tang, W. H. Wilson [12 ]
Garg, Sonia [13 ]
Trachtenberg, Barry H. [14 ]
Shah, Palak [15 ]
Pamboukian, Salpy, V [16 ]
Sweitzer, Nancy K. [17 ]
Wheeler, Matthew T. [18 ]
Wilcox, Jane E. [19 ]
Katz, Stuart [20 ]
Pan, Stephen [21 ,22 ]
Jimenez, Javier [23 ]
Aaronson, Keith D. [24 ]
Fishbein, Daniel P. [25 ]
Smart, Frank [26 ]
Wang, Jessica [27 ]
Gottlieb, Stephen S. [28 ]
Judge, Daniel P. [29 ]
Moore, Charles K. [30 ]
Mead, Jonathan O. [3 ,4 ]
Ni, Hanyu [3 ,4 ]
Burke, Wylie [31 ]
Hershberger, Ray E. [3 ,4 ,5 ]
机构
[1] Tufts Med Ctr, Cardiol Div, Boston, MA USA
[2] Tufts Univ, Sch Med, Boston, MA 02111 USA
[3] Ohio State Univ, Dept Internal Med, Div Human Genet, Columbus, OH USA
[4] Ohio State Univ, Davis Heart & Lung Res Inst, Columbus, OH USA
[5] Ohio State Univ, Dept Internal Med, Div Cardiovasc Med, Columbus, OH USA
[6] Washington Hosp Ctr, Medstar Res Inst, Washington, DC USA
[7] Cedars Sinai Med Ctr, Smidt Heart Inst, Los Angeles, CA USA
[8] Washington Univ, St Louis, MO 63110 USA
[9] Emory Univ, Sch Med, Atlanta, GA USA
[10] Univ Penn, Ctr Inherited Cardiovasc Dis, Perelman Sch Med, Div Cardiol, Philadelphia, PA USA
[11] Univ Nebraska Med Ctr, Omaha, NE USA
[12] Cleveland Clin, Cleveland, OH 44106 USA
[13] Univ Texas Southwestern Med Ctr Dallas, Dallas, TX 75390 USA
[14] Houston Methodist DeBakey Heart & Vasc Ctr, JC Walter Jr Transplant Ctr, Houston, TX USA
[15] Inova Heart & Vasc Inst, Falls Church, VA USA
[16] Univ Alabama Birmingham, Birmingham, AL USA
[17] Univ Arizona, Sarver Heart Ctr, Tucson, AZ USA
[18] Stanford Univ, Div Cardiovasc Med, Sch Med, Stanford, CA USA
[19] Northwestern Univ, Feinberg Sch Med, Chicago, IL USA
[20] NYU Langone Med Ctr, New York, NY USA
[21] Westchester Med Ctr, Dept Cardiol, Valhalla, NY USA
[22] New York Med Coll, Valhalla, NY 10595 USA
[23] Miami Cardiac & Vasc Inst, Baptist Hlth South, Miami, FL USA
[24] Univ Michigan, Med Ctr, Ann Arbor, MI USA
[25] Univ Washington, Seattle, WA 98195 USA
[26] Louisiana State Univ, Hlth Sci Ctr, New Orleans, LA USA
[27] Univ Calif Los Angeles, Med Ctr, Los Angeles, CA 90024 USA
[28] Univ Maryland, Sch Med, Baltimore, MD 21201 USA
[29] Med Univ South Carolina, Charleston, SC 29425 USA
[30] Univ Mississippi, Med Ctr, Jackson, MS 39216 USA
[31] Univ Washington, Dept Bioeth & Humanities, Seattle, WA USA
来源
JAMA-JOURNAL OF THE AMERICAN MEDICAL ASSOCIATION | 2022年 / 327卷 / 05期
关键词
CONGESTIVE-HEART-FAILURE; SCIENTIFIC STATEMENT; RACIAL-DIFFERENCES; SURVIVAL;
D O I
10.1001/jama.2021.24674
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
IMPORTANCE Idiopathic dilated cardiomyopathy (DCM) aggregates in families, and early detection in at-risk family members can provide opportunity to initiate treatment prior to late-phase disease. Most studies have included only White patients, yet Black patients with DCM have higher risk of heart failure-related hospitalization and death. OBJECTIVE To estimate the prevalence of familial DCM among DCM probands and the age-specific cumulative risk of DCM in first-degree relatives across race and ethnicity groups. DESIGN, SETTING, AND PARTICIPANTS A family-based, cross-sectional study conducted by a multisite consortium of 25 US heart failure programs. Participants included patients with DCM (probands), defined as left ventricular systolic dysfunction and left ventricular enlargement after excluding usual clinical causes, and their first-degree relatives. Enrollment commenced June 7, 2016; proband and family member enrollment concluded March 15, 2020, and April 1, 2021, respectively. EXPOSURES The presence of DCM in a proband. MAIN OUTCOMES AND MEASURES Familial DCM defined by DCM in at least 1 first-degree relative; expanded familial DCM defined by the presence of DCM or either left ventricular enlargement or left ventricular systolic dysfunction without known cause in at least 1 first-degree relative. RESULTS The study enrolled 1220 probands (median age, 52.8 years [IQR, 42.4-61.8]; 43.8% female; 43.1% Black and 8.3% Hispanic) and screened 1693 first-degree relatives for DCM. A median of 28% (IQR, 0%-60%) of living first-degree relatives were screened per family. The crude prevalence of familial DCM among probands was 11.6% overall. The model-based estimate of the prevalence of familial DCM among probands at a typical US advanced heart failure program if all living first-degree relatives were screened was 29.7% (95% CI, 23.5% to 36.0%) overall. The estimated prevalence of familial DCM was higher in Black probands than in White probands (difference, 11.3% [95% CI, 1.9% to 20.8%]) but did not differ significantly between Hispanic probands and non-Hispanic probands (difference. -1.4% [95% Cl. -15.9% to 13.1%]). The estimated prevalence of expanded familial DCM was 56.9% (95% CI, 50.8% to 63.0%) overall. Based on age-specific disease status at enrollment, estimated cumulative risks in first-degree relatives at a typical US advanced heart failure program reached 19% (95% Cl, 13% to 24%) by age 80 years for DCM and 33% (95% CI, 27% to 40%) for expanded DCM inclusive of partial phenotypes. The DCM hazard was higher in first-degree relatives of non-Hispanic Black probands than non-Hispanic White probands (hazard ratio, 1.89 [95% CI, 1.26 to 2.83]). CONCLUSIONS AND RELEVANCE In a US cross-sectional study, there was substantial estimated prevalence of familial DCM among probands and modeled cumulative risk of DCM among their first-degree relatives.
引用
收藏
页码:454 / 463
页数:10
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