TY - JOUR
T1 - Fibromuscular Dysplasia and Abdominal Aortic Aneurysms Are Dimorphic Sex-Specific Diseases with Shared Complex Genetic Architecture
AU - VA Million Veteran Program
AU - Katz, Alexander E.
AU - Yang, Min Lee
AU - Levin, Michael G.
AU - Tcheandjieu, Catherine
AU - Mathis, Michael
AU - Hunker, Kristina
AU - Blackburn, Susan
AU - Eliason, Jonathan L.
AU - Coleman, Dawn M.
AU - Fendrikova-Mahlay, Natalia
AU - Gornik, Heather L.
AU - Karmakar, Monita
AU - Hill, Hannah
AU - Xu, Chang
AU - Zawistowski, Matthew
AU - Brummett, Chad M.
AU - Zoellner, Sebastian
AU - Zhou, Xiang
AU - O'Donnell, Christopher J.
AU - Douglas, Julie A.
AU - Assimes, Themistocles L.
AU - Tsao, Phillip S.
AU - Li, Jun Z.
AU - Damrauer, Scott M.
AU - Stanley, James C.
AU - Ganesh, Santhi K.
AU - Gaziano, J. Michael
AU - Muralidhar, Sumitra
AU - Ramoni, Rachel
AU - Beckham, Jean
AU - Chang, Kyong Mi
AU - Breeling, James
AU - Huang, Grant
AU - Casas, Juan P.
AU - Moser, Jennifer
AU - Whitbourne, Stacey B.
AU - Brewer, Jessica V.
AU - Aslan, Mihaela
AU - Connor, Todd
AU - Argyres, Dean P.
AU - Stephens, Brady
AU - Brophy, Mary T.
AU - Humphries, Donald E.
AU - Selva, Luis E.
AU - Do, Nhan
AU - Shayan, Shahpoor
AU - Cho, Kelly
AU - Churby, Lori
AU - Pyarajan, Saiju
AU - Duvall, Scott L.
AU - Hauser, Elizabeth
AU - Sun, Yan
AU - Zhao, Hongyu
AU - Wilson, Peter
AU - McArdle, Rachel
AU - Dellitalia, Louis
AU - Mattocks, Kristin
AU - Harley, John
AU - Whittle, Jeffrey
AU - Jacono, Frank
AU - Wells, John
AU - Gutierrez, Salvador
AU - Gibson, Gretchen
AU - Hammer, Kimberly
AU - Kaminsky, Laurence
AU - Villareal, Gerardo
AU - Kinlay, Scott
AU - Xu, Junzhe
AU - Hamner, Mark
AU - Mathew, Roy
AU - Bhushan, Sujata
AU - Iruvanti, Pran
AU - Godschalk, Michael
AU - Ballas, Zuhair
AU - Ivins, Douglas
AU - Mastorides, Stephen
AU - Moorman, Jonathan
AU - Gappy, Saib
AU - Klein, Jon
AU - Ratcliffe, Nora
AU - Florez, Hermes
AU - Okusaga, Olaoluwa
AU - Murdoch, Maureen
AU - Sriram, Peruvemba
AU - Yeh, Shing Shing
AU - Tandon, Neeraj
AU - Jhala, Darshana
AU - Aguayo, Samuel
AU - Cohen, David
AU - Sharma, Satish
AU - Liangpunsakul, Suthat
AU - Oursler, Kris Ann
AU - Whooley, Mary
AU - Ahuja, Sunil
AU - Constans, Joseph
AU - Meyer, Paul
AU - Greco, Jennifer
AU - Rauchman, Michael
AU - Servatius, Richard
AU - Gaddy, Melinda
AU - Wallbom, Agnes
AU - Morgan, Timothy
AU - Stapley, Todd
AU - Sherman, Scott
AU - Ross, George
AU - Tsao, Philip
AU - Strollo, Patrick
AU - Boyko, Edward
AU - Meyer, Laurence
AU - Gupta, Samir
AU - Huq, Mostaqul
AU - Fayad, Joseph
AU - Hung, Adriana
AU - Lichy, Jack
AU - Hurley, Robin
AU - Robey, Brooks
AU - Striker, Robert
N1 - Funding Information:
Funding support included grants from the Doris Duke Charitable Foundation (Grant #2013104 to Dr Ganesh), the University of Michigan Frankel Cardiovascular Center and Michigan Biological Research Initiative on Sex Differences in Cardiovascular Disease (M-BRISC) program, and R01HL139672. The Cleveland Clinic FMD Biorepository was supported in part by the National Institutes of Health, National Center for Research Resources, CTSA 1UL1RR024989, Cleveland, Ohio. This work was supported by funding from the Department of Veterans Affairs Office of Research and Development, Million Veteran Program Grants I01BX003362-03A1 and I01BX004821-01A1. Dr Ganesh is supported by R35HL161016, R01HL086694, Department of Defense, and the A. Alfred Taubman Institute. Dr Damrauer is supported by the Department of Veterans Affairs Office of Research and Development (IK2-CX001780). This publication does not represent the views of the Department of Veterans Affairs or the United States Government.
Publisher Copyright:
© 2022 American Heart Association, Inc.
PY - 2022/12/1
Y1 - 2022/12/1
N2 - Background: The risk of arterial diseases may be elevated among family members of individuals having multifocal fibromuscular dysplasia (FMD). We sought to investigate the risk of arterial diseases in families of individuals with FMD. Methods: Family histories for 73 probands with FMD were obtained, which included an analysis of 463 total first-degree relatives focusing on FMD and related arterial disorders. A polygenic risk score for FMD (PRSFMD) was constructed from prior genome-wide association findings of 584 FMD cases and 7139 controls and evaluated for association with an abdominal aortic aneurysm (AAA) in a cohort of 9693 AAA cases and 294 049 controls. A previously published PRSAAA was also assessed among the FMD cases and controls. Results: Of all first degree relatives of probands, 9.3% were diagnosed with FMD, aneurysms, and dissections. Aneurysmal disease occurred in 60.5% of affected relatives and 5.6% of all relatives. Among 227 female first-degree relatives of probands, 4.8% (11) had FMD, representing a relative risk (RR)FMD of 1.5 ([95% CI, 0.75-2.8]; P=0.19) compared with the estimated population prevalence of 3.3%, though not of statistical significance. Of all fathers of FMD probands, 11% had AAAs resulting in a RRAAA of 2.3 ([95% CI, 1.12-4.6]; P=0.014) compared with population estimates. The PRSFMD was found to be associated with an AAA (odds ratio, 1.03 [95% CI, 1.01-1.05]; P=2.6×10-3), and the PRSAAA was found to be associated with FMD (odds ratio, 1.53 [95% CI, 1.2-1.9]; P=9.0×10-5) as well. Conclusions: FMD and AAAs seem to be sex-dimorphic manifestations of a heritable arterial disease with a partially shared complex genetic architecture. Excess risk of having an AAA according to a family history of FMD may justify screening in family members of individuals having FMD.
AB - Background: The risk of arterial diseases may be elevated among family members of individuals having multifocal fibromuscular dysplasia (FMD). We sought to investigate the risk of arterial diseases in families of individuals with FMD. Methods: Family histories for 73 probands with FMD were obtained, which included an analysis of 463 total first-degree relatives focusing on FMD and related arterial disorders. A polygenic risk score for FMD (PRSFMD) was constructed from prior genome-wide association findings of 584 FMD cases and 7139 controls and evaluated for association with an abdominal aortic aneurysm (AAA) in a cohort of 9693 AAA cases and 294 049 controls. A previously published PRSAAA was also assessed among the FMD cases and controls. Results: Of all first degree relatives of probands, 9.3% were diagnosed with FMD, aneurysms, and dissections. Aneurysmal disease occurred in 60.5% of affected relatives and 5.6% of all relatives. Among 227 female first-degree relatives of probands, 4.8% (11) had FMD, representing a relative risk (RR)FMD of 1.5 ([95% CI, 0.75-2.8]; P=0.19) compared with the estimated population prevalence of 3.3%, though not of statistical significance. Of all fathers of FMD probands, 11% had AAAs resulting in a RRAAA of 2.3 ([95% CI, 1.12-4.6]; P=0.014) compared with population estimates. The PRSFMD was found to be associated with an AAA (odds ratio, 1.03 [95% CI, 1.01-1.05]; P=2.6×10-3), and the PRSAAA was found to be associated with FMD (odds ratio, 1.53 [95% CI, 1.2-1.9]; P=9.0×10-5) as well. Conclusions: FMD and AAAs seem to be sex-dimorphic manifestations of a heritable arterial disease with a partially shared complex genetic architecture. Excess risk of having an AAA according to a family history of FMD may justify screening in family members of individuals having FMD.
KW - aneurysm
KW - aortic aneurysm, abdominal
KW - arteries
KW - dissection
KW - fibromuscular dysplasia
KW - genetics
KW - sex dimorphism
UR - http://www.scopus.com/inward/record.url?scp=85144589599&partnerID=8YFLogxK
U2 - 10.1161/CIRCGEN.121.003496
DO - 10.1161/CIRCGEN.121.003496
M3 - Article
C2 - 36374587
AN - SCOPUS:85144589599
SN - 2574-8300
VL - 15
SP - E003496
JO - Circulation: Genomic and Precision Medicine
JF - Circulation: Genomic and Precision Medicine
IS - 6
M1 - e003496
ER -