Reduced Penetrance, Variable Expressivity, and Genetic Heterogeneity of Familial Atrial Septal Defects

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Circulation. 1998;97:2043-2048

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(Circulation. 1998;97:2043-2048.)
© 1998 American Heart Association, Inc.

Clinical Investigation and Reports

Reduced Penetrance, Variable Expressivity, and Genetic Heterogeneity of Familial Atrial Septal Defects

D. Woodrow Benson, MD, PhD; Angela Sharkey, MD; Diane Fatkin, MD, BSc(Med); Peter Lang, MD; Craig T. Basson, MD, PhD; Barbara McDonough, BSN; Arnold W. Strauss, MD; J. G. Seidman, PhD; ; Christine E. Seidman, MD

From the Cardiovascular Division and Howard Hughes Medical Institute, Brigham and Women's Hospital (D.W.B., D.F., C.T.B., B.M., C.E.S.), the Department of Genetics, Howard Hughes Medical Institute (J.G.S.), and the Department of Cardiology, Children's Hospital (P.L.), Boston, Mass; and the Division of Pediatric Cardiology, Washington University, St Louis, Mo (A.S., A.W.S.).

Correspondence to D. Woodrow Benson, MD, PhD, Director, Cardiovascular Genetics, Pediatric Cardiology, Medical University of South Carolina, 171 Ashley Ave, Charleston, SC 29425-0680.

Background—Secundum atrial septal defect (ASD) is a commoncongenital heart malformation that occurs as an isolated anomalyin 10% of individuals with congenital heart disease. Althoughsome embryological pathways have been elucidated, the molecularetiologies of ASD are not fully understood. Most cases of ASD areisolated, but some individuals with ASD have a family historyof this defect or other congenital heart malformations.

Methods and Results—Clinical evaluation of three families identifiedindividuals with ASD in multiple generations. ASD was transmittedas an autosomal dominant trait in each family. ASD was the mostcommon anomaly, but other heart defects occurred alone or in associationwith ASD in individuals from each kindred. Genome-wide linkagestudies in one kindred localized a familial ASD disease geneto chromosome 5p (multipoint LOD score=3.6, ${theta}$ =0.0). Assessmentof 20 family members with the disease haplotype revealed that9 had ASD, 8 were clinically unaffected, and 3 had other cardiacdefects (aortic stenosis, atrial septal aneurysm, and persistentleft superior vena cava). Familial ASD did not map to chromosome5p in two other families.

Conclusions—Familial ASD is a genetically heterogeneousdisorder; one disease gene maps to chromosome 5p. Recognitionof the heritable basis of familial ASD is complicated by lowdisease penetrance and variable expressivity. Identification ofASD or other congenital heart defects in more than one familymember should prompt clinical evaluation of all relatives.

Key Words: echocardiography • genetics • heart septal defects

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