| Literature DB >> 28817111 |
Theodora U J Bruun1,2, Caro-Lyne DesRoches1, Diane Wilson3,4, Vann Chau4, Tadashi Nakagawa5, Masahiro Yamasaki6, Shinya Hasegawa6, Toshiyuki Fukao7, Christian Marshall1,8, Saadet Mercimek-Andrews1,2,9.
Abstract
PurposeNeonatal encephalopathy, which is characterized by a decreased level of consciousness, occurs in 1-7/1,000 live-term births. In more than half of term newborns, there is no identifiable etiological factor. To identify underlying genetic defects, we applied whole-exome sequencing (WES) in term newborns with neonatal encephalopathy as a prospective cohort study.MethodsTerm newborns with neonatal encephalopathy and no history of perinatal asphyxia were included. WES was performed using patient and both parents' DNA.ResultsNineteen patients fulfilling inclusion criteria were enrolled. Five patients were excluded owing to withdrawal of consent, no parental DNA samples, or a genetic diagnosis prior to WES. Fourteen patients underwent WES. We confirmed a genetic diagnosis in five patients (36%): epileptic encephalopathy associated with autosomal dominant de novo variants in SCN2A (p.Met1545Val), KCNQ2 (p.Asp212Tyr), and GNAO1 (p.Gly40Arg); lipoic acid synthetase deficiency due to compound heterozygous variants in LIAS (p.Ala253Pro and p.His236Gln); and encephalopathy associated with an X-linked variant in CUL4B (p.Asn211Ser).ConclusionWES is helpful at arriving genetic diagnoses in neonatal encephalopathy and/or seizures and brain damage. It will increase our understanding and probably enable us to develop targeted neuroprotective treatment strategies.Entities:
Mesh:
Year: 2017 PMID: 28817111 DOI: 10.1038/gim.2017.129
Source DB: PubMed Journal: Genet Med ISSN: 1098-3600 Impact factor: 8.822