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Cell-Free DNA in the Investigation of Miscarriage

Authors :: Stephanie Allen
Arri Coomarasamy
Neil V. Morgan
Susan Hamilton
Emily Colley
Paul Smith
Adam J. Devall
Helen Williams
Siobhan Quenby
Source :: Journal of Clinical Medicine, Volume 9, Issue 11, Journal of Clinical Medicine, Vol 9, Iss 3428, p 3428 (2020)
Publication Year :: 2020
Publisher :: Multidisciplinary Digital Publishing Institute, 2020.
Abstract: Approximately one in four pregnancies result in pregnancy loss, and ~50% of these miscarriages are caused by chromosomal abnormalities. Genetic investigations are recommended after three consecutive miscarriages on products of conception (POC) tissue. Cell-free DNA (cfDNA) has been utilised for prenatal screening, but very little work has been carried out in nonviable pregnancies. We investigated the use of cfDNA from maternal blood to identify chromosomal abnormalities in miscarriage. One hundred and two blood samples from women experiencing a first trimester miscarriage were collected and stored. The mean gestational age was 7.1 weeks (range: 5&ndash 11 weeks). In this research, samples without a genetic test result from POC were not analysed. CfDNA was extracted and analysed using a modified commercial genome-wide non-invasive prenatal test. No results were provided to the patient. In 57 samples, cytogenetic results from POC analysis were available. Chromosomal abnormalities were identified in 47% (27/57) of POC analyses, and cfDNA analysis correctly identified 59% (16/27) of these. In total, 75% (43/57) of results were correctly identified. The average cfDNA fetal fraction was 6% (2&ndash 19%). In conclusion, cfDNA can be used to detect chromosomal abnormalities in miscarriages where the &lsquo fetal fraction&rsquo is high enough however, more studies are required to identify variables that can affect the overall results.