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Discovery of pathogenic variants in EFEMP2 and RAG1 and undetectable fetal phenotype: A challenge of prenatal exome sequencing

外显子组测序 外显子组 产前诊断 遗传学 胎儿 医学 表型 背景(考古学) 生物 怀孕 基因 古生物学
作者
M Favier,Rodolph Dard,G. Gorincour,Aude Tessier,Emmanuelle Motte‐Signoret,C. Duvillier,Caroline Racine,Laurence Faivre,Christel Thauvin‐Robinet,Frédéric Tran Mau‐Them
出处
期刊:Prenatal Diagnosis [Wiley]
卷期号:44 (9): 1115-1118
标识
DOI:10.1002/pd.6629
摘要

Abstract Background Exome sequencing in prenatal context confronts with pathogenic variants associated with phenotypes that are not detectable prenatally. Materials and Methods A consanguineous couple was referred at 24 weeks of gestation for prenatal genetic investigations after ultrasonography findings including decreased fetal movements, hypoplastic male external genitalia, retrognathia, prefrontal edema, anomalies of the great vessels with pulmonary atresia and dilated tortuous aorta. Result Prenatal trio exome sequencing identified two homozygous likely pathogenic variants, i.e. a missense in EFEMP2 involved in cutis laxa and a nonsense in RAG1 involved in several types of severe combined immunodeficiency. Discussion The fetal ultrasonographic phenotype was partially compatible with previously reported prenatal presentations secondary to EFEMP2 biallelic variants, but prenatal presentations have never been reported for RAG1 related disorders because the RAG1 phenotype is undetectable during pregnancy. Conclusion Both EFEMP2 and RAG1 variants were disclosed to the couple because the EFEMP2 variant was considered causative for the fetal ultrasonographic phenotype and the RAG1 variant was considered a finding of strong interest for genetic counselling and monitoring of future pregnancies following the American College of Medical Genetics and Genomics recommendations about the discovery of incidental findings in fetal exome sequencing in prenatal diagnosis.
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