Prenatal Diagnosis by Array Comparative Genomic Hybridization in Fetuses with Cardiac Abnormalities

Author:

Kowalczyk KatarzynaORCID,Bartnik-Głaska Magdalena,Smyk Marta,Plaskota Izabela,Bernaciak JoannaORCID,Kędzior Marta,Wiśniowiecka-Kowalnik BarbaraORCID,Jakubów-Durska Krystyna,Braun-Walicka Natalia,Barczyk Artur,Geremek MaciejORCID,Castañeda Jennifer,Kutkowska-Kaźmierczak AnnaORCID,Własienko Paweł,Dębska MarzenaORCID,Kucińska-Chahwan Anna,Roszkowski Tomasz,Kozłowski SzymonORCID,Mikulska Boyana,Issat TadeuszORCID,Obersztyn Ewa,Nowakowska Beata Anna

Abstract

Congenital heart defects (CHDs) appear in 8–10 out of 1000 live born newborns and are one of the most common causes of deaths. In fetuses, the congenital heart defects are found even 3–5 times more often. Currently, microarray comparative genomic hybridization (array CGH) is recommended by worldwide scientific organizations as a first-line test in the prenatal diagnosis of fetuses with sonographic abnormalities, especially cardiac defects. We present the results of the application of array CGH in 484 cases with prenatally diagnosed congenital heart diseases by fetal ultrasound scanning (256 isolated CHD and 228 CHD coexisting with other malformations). We identified pathogenic aberrations and likely pathogenic genetic loci for CHD in 165 fetuses and 9 copy number variants (CNVs) of unknown clinical significance. Prenatal array-CGH is a useful method allowing the identification of all unbalanced aberrations (number and structure) with a much higher resolution than the currently applied traditional assessment techniques karyotype. Due to this ability, we identified the etiology of heart defects in 37% of cases.

Publisher

MDPI AG

Subject

Genetics (clinical),Genetics

Reference42 articles.

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