Distribution of maternal age and birth order groups in cases with unclassified multiple congenital abnormalities according to the number of component abnormalities: A national population-based case-control study

Background Multiple congenital abnormalities are caused by chromosomal aberrations, mutant major genes and teratogens. A minor proportion of these patients are identified as syndromes but the major part belonging to the group of unclassified multiple CAs (UMCAs). The main objective of this study was...

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Published in:Birth defects research. A Clinical and molecular teratology 2015-02, Vol.103 (2), p.67-75
Main Authors: Csermely, Gyula, Czeizel, Andrew E., Veszprémi, Béla
Format: Article
Language:English
Subjects:
Abnormalities, Multiple - epidemiology
Abnormalities, Multiple - genetics
Abnormalities, Multiple - pathology
Adult
Age Factors
Birth Order
Case-Control Studies
Down syndrome
Down Syndrome - epidemiology
Down Syndrome - genetics
Down Syndrome - pathology
Epidemiological Monitoring
Female
Humans
Hungary - epidemiology
Infant, Newborn
Male
Maternal Age
Mothers
multiple congenital abnormalities
population-based case-control study
Pregnancy
Registries
Risk
unclassified multiple congenital abnormalities
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Summary:Background Multiple congenital abnormalities are caused by chromosomal aberrations, mutant major genes and teratogens. A minor proportion of these patients are identified as syndromes but the major part belonging to the group of unclassified multiple CAs (UMCAs). The main objective of this study was to evaluate the maternal age and birth order in pregnant women who had offspring affected with UMCA. The strong association between numerical chromosomal aberrations, e.g., Down syndrome and advanced maternal age is well‐known and tested here. Methods The Hungarian Case‐Control Surveillance of Congenital Abnormalities, 1980 to 1996, yielded a large population‐based national data set with 22,843 malformed newborns or fetuses (“informative cases”) included 1349 UMCA cases with their 2407 matched controls. Case‐control comparison of maternal age and birth order was made for cases with UMCA, stratified by component numbers and their controls. In addition, 834 cases with Down syndrome were compared to 1432 matched controls. Results The well‐known advanced maternal age with the higher risk for Down syndrome was confirmed. The findings of the study suggest that the young age of mothers associates with the higher risk of UMCA, in addition birth order 4 or more associates with the higher risk for UMCA with 2 and 3 component CAs. Conclusion This study was the first to analyze the possible maternal and birth order effect for cases with UMCA, and the young age and higher birth order associated with a higher risk for UMCA. Birth Defects Research (Part A) 103:67–75, 2015 © 2014 Wiley Periodicals, Inc.
ISSN:1542-0752
1542-0760
DOI:10.1002/bdra.23304