| Literature DB >> 32906196 |
Lauren S Akesson1,2,3, Adam Bournazos4,5, Andrew Fennell3,6, Emma I Krzesinski3,6, Kenneth Tan6,7, Amanda Springer3,6, Katherine Rose3,6, Ilias Goranitis8,9, David Francis1, Crystle Lee1, Fathimath Faiz10, Mark R Davis10, John Christodoulou1,2,9,11, Sebastian Lunke1,9,12, Zornitza Stark1,2,9, Matthew F Hunter3,6, Sandra T Cooper4,5,13.
Abstract
Rapid genomic diagnosis programs are transforming rare disease diagnosis in acute pediatrics. A ventilated newborn with cerebellar hypoplasia underwent rapid exome sequencing (75 h), identifying a novel homozygous ASNS splice-site variant (NM_133436.3:c.1476+1G>A) of uncertain significance. Rapid ASNS splicing studies using blood-derived messenger RNA from the family trio confirmed a consistent pattern of abnormal splicing induced by the variant (cryptic 5' splice-site or exon 12 skipping) with absence of normal ASNS splicing in the proband. Splicing studies reported within 10 days led to reclassification of c.1476+1G>A as pathogenic at age 27 days. Intensive care was redirected toward palliation. Cost analyses for the neonate and his undiagnosed, similarly affected deceased sibling, demonstrate that early diagnosis reduced hospitalization costs by AU$100,828. We highlight the diagnostic benefits of adjunct RNA testing to confirm the pathogenicity of splicing variants identified via rapid genomic testing pipelines for precision and preventative medicine.Entities:
Keywords: ASNS; asparagine synthetase deficiency; exome sequencing; mRNA splicing analysis; rapid genomic diagnosis program
Year: 2020 PMID: 32906196 DOI: 10.1002/humu.24101
Source DB: PubMed Journal: Hum Mutat ISSN: 1059-7794 Impact factor: 4.878