TY - JOUR
T1 - Congenital cardiovascular malformations associated with chromosome abnormalities
T2 - An epidemiologic study
AU - Ferencz, Charlotte
AU - Neill, Catherine A.
AU - Boughman, Joann A.
AU - Rubin, Judith D.
AU - Brenner, Joel I.
AU - Perry, Lowell W.
N1 - Funding Information:
*The Baltimore-Washington Infant Study coinvestigators who supported this work are Edward B. Clark, MD, Seymour I. Hepner, MD, John W. Downing, MD, Gerard R. Martin, MD, Mohamed K. Mardini, MD, and Robert J. McCarter, ScD. Supported by National Heart, Lung, and Blood Institute grant No. R37-HL25629. Submitted for publication May 9, 1988; accepted Aug. 8, 1988. Reprint requests: Charlotte Ferencz, MD, MPH, University of Maryland School of Medicine, Department of Epidemiology and Preventive Medicine, 655 W. Baltimore St., Baltimore, MD 21201.
Copyright:
Copyright 2014 Elsevier B.V., All rights reserved.
PY - 1989/1
Y1 - 1989/1
N2 - The Baltimore-Washington Infant Study is a population-based case-control study that seeks to identify risk factors for cardiovascular malformations. Between 1981 and 1986, a total of 2102 infants with cardiovascular malformations were ascertained, among whom 271 (12.9%) also had a chromosome abnormality. Among 2328 random control subjects, only two had a chromosome abnormality. Down syndrome with cardiovascular maiformations had a maternal age-adjusted regional prevalence of 4.33/10,000 for the white population and 3.70/10,000 for the nonwhite population. Endocardial cushion defect, the predominant cardiac abnormality in Down syndrome (60.1%), rarely occurred as an isolated cardiac lesion (2.8%). The absence of transpositions and the rarity of heterotaxias and of right- and left-sided obstructive lesions in trisomies indicate that there may be a genetic influence on specific embryologic mechanisms. Allmentary tract lesions were more common in Down syndrome than among euploid patients with heart disease and more severe than in control subjects. Urinary tract lesions also occurred in excess of the rate in control subjects. The coexistence of these major malformations with heart disease raises the possibility of incomplete expression of the VA(C)TER (vertebral, anal, cardiac, fracheal, esophageal renal) association. The selective association of chromosome abnormalities with certain cardiovascular defects is now beginning to be explained by reported embryologic studies on cellular characteristics. An explanation of the negative association with transposition and obstructive lesions requires further multidisciplinary studies on genetic and epigenetic factors.*The Baltimore-Washington Infant Study coinvestigators who supported this work are Edward B. Clark, MD, Seymour I. Hepner, MD, John W. Downing, MD, Gerard R. Martin, MD, Mohamed K. Mardini, MD, and Robert J. McCarter, ScD.
AB - The Baltimore-Washington Infant Study is a population-based case-control study that seeks to identify risk factors for cardiovascular malformations. Between 1981 and 1986, a total of 2102 infants with cardiovascular malformations were ascertained, among whom 271 (12.9%) also had a chromosome abnormality. Among 2328 random control subjects, only two had a chromosome abnormality. Down syndrome with cardiovascular maiformations had a maternal age-adjusted regional prevalence of 4.33/10,000 for the white population and 3.70/10,000 for the nonwhite population. Endocardial cushion defect, the predominant cardiac abnormality in Down syndrome (60.1%), rarely occurred as an isolated cardiac lesion (2.8%). The absence of transpositions and the rarity of heterotaxias and of right- and left-sided obstructive lesions in trisomies indicate that there may be a genetic influence on specific embryologic mechanisms. Allmentary tract lesions were more common in Down syndrome than among euploid patients with heart disease and more severe than in control subjects. Urinary tract lesions also occurred in excess of the rate in control subjects. The coexistence of these major malformations with heart disease raises the possibility of incomplete expression of the VA(C)TER (vertebral, anal, cardiac, fracheal, esophageal renal) association. The selective association of chromosome abnormalities with certain cardiovascular defects is now beginning to be explained by reported embryologic studies on cellular characteristics. An explanation of the negative association with transposition and obstructive lesions requires further multidisciplinary studies on genetic and epigenetic factors.*The Baltimore-Washington Infant Study coinvestigators who supported this work are Edward B. Clark, MD, Seymour I. Hepner, MD, John W. Downing, MD, Gerard R. Martin, MD, Mohamed K. Mardini, MD, and Robert J. McCarter, ScD.
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U2 - 10.1016/S0022-3476(89)80605-5
DO - 10.1016/S0022-3476(89)80605-5
M3 - Article
C2 - 2521249
AN - SCOPUS:0024476864
SN - 0022-3476
VL - 114
SP - 79
EP - 86
JO - The Journal of pediatrics
JF - The Journal of pediatrics
IS - 1
ER -