Post‐mortem rapid aneuploidy testing for holoprosencephaly

Author:

Gergely Lajos1ORCID,Repiská Vanda1,Böhmer Daniel1,Korbeľ Miroslav2,Václavová Zuzana2,McCullough Liam2,Melišová Katarína1,Priščáková Petra1

Affiliation:

1. Institute of Medical Biology, Genetics and Clinical Genetics, Faculty of Medicine Comenius University Bratislava Bratislava Slovakia

2. 1st Department of Gynaecology and Obstetrics, Faculty of Medicine Comenius University Bratislava Bratislava Slovakia

Abstract

AbstractBackgroundAbortion and fetal death are common in fetuses with holoprosencephaly, so genetic examinations often have to be made in a post‐mortem setting. The efficiency of the conventional karyotyping using cultured fibroblasts in these situations is limited due to frequent culture failure. In the current study, archived cases of holoprosencephaly, where post‐mortem genetic evaluation was requested and sufficient frozen material was available, were reevaluated using the quantitative fluorescence polymerase chain reaction (QF‐PCR) technique.MethodsTesting for aneuploidies of chromosomes 13, 15, 16, 18, 21, 22, X, and Y with the QF‐PCR technique was carried out on DNA isolated from archived frozen chorionic villi in seven cases of holoprosencephaly.ResultsQF‐PCR was successful in all seven cases. Two cases of trisomy 13, two cases of triploidy, and one case of trisomy 18 was found meaning a 71% diagnostic yield. The success rate of QF‐PCR (100%, 7/7) was superior compared to conventional karyotyping (43%, 3/7).ConclusionsRapid aneuploidy testing using the QF‐PCR technique is a simple, reliable, time‐ and cost‐effective method sufficient to conclude the etiologic investigation in the majority of holoprosencephaly cases post‐mortem.

Publisher

Wiley

Reference12 articles.

1. American College of Obstetricians and GynecologistsManagement of Stillbirth [online].https://www.acog.org/clinical/clinical-guidance/obstetric-care-consensus/articles/2020/03/management-of-stillbirthAccessed January 16 2024.

2. Holoprosencephaly

3. Holoprosencephaly

4. Holoprosencephaly

5. Stillborn Infants: Associated Malformations

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