OP22.08: Integrating ultrasound findings with chromosomal microarray stretches of homozygosity and principles in founder populations

Abstract

Chromosomal microarray (CMA) analysis is effectively applied prenatally to detect copy number changes. SNP probes included on the microarray platform can detect regions of excessive homozygosity (ROH) and identical-by-descent genomic stretches. The utility of the latter in prenatal diagnosis is not well established. Recessive founder mutations have been identified within distinct ethnic groups. Combining these data with prenatal sonography provides accurate molecular diagnoses quickly. Three gravidae presenting with specific fetal sonographic findings: 1) ventriculomegaly with encephalocele; 2) severe polyhydramnion, and 3) enlarged echogenic kidneys, underwent amniocentesis for CMA, and Genome-Wide Human SNP array was used to analyse DNA from amniocytes. The Genomic Oligoarray and SNP array evaluation tool v3.0 was used to detect recessive loci associated with the reported clinical findings. Candidate regions were further interrogated using the National Genetic Database. Three fetuses from three distinct nuclear families in which the parents shared a similar ethnicity (either Ashkenazi or Bukharan Jews) but no reported consanguinity, were assessed. No copy number changes were observed, however evaluation of regions of homozygosity revealed a relevant candidate gene for the specific phenotype for each fetus. Using the National Genetic Database a specific mutation was examined in both parents (c.1167dupA mutation in the FKTN gene, c.167ins6[TTTCCC] mutation in the BSND gene and c.3761_3762delCCinsG in the PKHD1 gene, respectively). Both parents were found to be carriers and the fetuses homozygotes to the mutation. For the first time, specific sonographic pathology, data from ROH extracted from CMA results, and information regarding common founder mutations in distinct ethnic subgroups were combined to create a comprehensive streamlined approach to provide effective genetic diagnosis and counselling within the time constraints of ongoing pregnancy.