| Literature DB >> 29194579 |
M Rasmussen1, L Sunde1,2, M L Nielsen1, M Ramsing3, A Petersen4, T D Hjortshøj5, T E Olsen6, A Tabor7, J M Hertz8, I Johnsen9, L Sperling10, O B Petersen11, U B Jensen1,2, F G Møller12, M B Petersen13,14, D L Lildballe1.
Abstract
Identification of fetal kidney anomalies invites questions about underlying causes and recurrence risk in future pregnancies. We therefore investigated the diagnostic yield of next-generation sequencing in fetuses with bilateral kidney anomalies and the correlation between disrupted genes and fetal phenotypes. Fetuses with bilateral kidney anomalies were screened using an in-house-designed kidney-gene panel. In families where candidate variants were not identified, whole-exome sequencing was performed. Genes uncovered by this analysis were added to our kidney panel. We identified likely deleterious variants in 11 of 56 (20%) families. The kidney-gene analysis revealed likely deleterious variants in known kidney developmental genes in 6 fetuses and TMEM67 variants in 2 unrelated fetuses. Kidney histology was similar in the latter 2 fetuses-presenting a distinct prenatal form of nephronophthisis. Exome sequencing identified ROBO1 variants in one family and a GREB1L variant in another family. GREB1L and ROBO1 were added to our kidney-gene panel and additional variants were identified. Next-generation sequencing substantially contributes to identifying causes of fetal kidney anomalies. Genetic causes may be supported by histological examination of the kidneys. This is the first time that SLIT-ROBO signaling is implicated in human bilateral kidney agenesis.Entities:
Keywords: CAKUT; NGS; kidney agenesis; kidney anomalies; kidney dysplasia; prenatal screening
Mesh:
Substances:
Year: 2018 PMID: 29194579 DOI: 10.1111/cge.13185
Source DB: PubMed Journal: Clin Genet ISSN: 0009-9163 Impact factor: 4.438