2024 : 11 : 21
omid Jazayeri

omid Jazayeri

Academic rank: Assistant Professor
ORCID: 0000-0002-4054-1704
Education: PhD.
ScopusId:
HIndex: 0/00
Faculty: Science
Address: Department of Molecular and Cell Biology, Faculty of Science, University of Mazandaran, Babolsar, Iran
Phone: 011-35302450

Research

Title
Whole-exome sequencing is a powerful approach for establishing the etiological diagnosis in patients with intellectual disability and microcephaly
Type
JournalPaper
Keywords
Autosomal recessive inheritance, ASPM, BRCA2, CASK, DYRK1A, ERCC8, KIF11, Microcephaly, RAB3GAP1 RNASEH2B, RTTN, Whole-exome sequencing
Year
2016
Journal BMC Medical Genomics
DOI
Researchers Patrick Rump ، omid Jazayeri ، Krista K. Van Dijk-Bos ، Lennart F. Johansson ، Anthonie J. van Essen ، Johanna B. G. M. Verheij ، Hermine E. Veenstra-Knol ، Egbert J. W. Redeker ، Marcel M. A. M. Mannens ، Morris A. Swertz ، Behrooz Z. Alizadeh ، Conny M.A. van Ravenswaaij-Arts ، Richard J. Sinke ، Birgit Sikkema-Raddatz

Abstract

Background: Clinical and genetic heterogeneity in monogenetic disorders represents a major diagnostic challenge. Although the presence of particular clinical features may aid in identifying a specific cause in some cases, the majority of patients remain undiagnosed. Here, we investigated the utility of whole-exome sequencing as a diagnostic approach for establishing a molecular diagnosis in a highly heterogeneous group of patients with varied intellectual disability and microcephaly. Methods: Whole-exome sequencing was performed in 38 patients, including three sib-pairs, in addition to or in parallel with genetic analyses that were performed during the diagnostic work-up of the study participants. Results: In ten out of these 35 families (29 %), we found mutations in genes already known to be related to a disorder in which microcephaly is a main feature. Two unrelated patients had mutations in the ASPM gene. In seven other patients we found mutations in RAB3GAP1, RNASEH2B, KIF11, ERCC8, CASK, DYRK1A and BRCA2. In one of the sib-pairs, mutations were found in the RTTN gene. Mutations were present in seven out of our ten families with an established etiological diagnosis with recessive inheritance. Conclusions: We demonstrate that whole-exome sequencing is a powerful tool for the diagnostic evaluation of patients with highly heterogeneous neurodevelopmental disorders such as intellectual disability with microcephaly. Our results confirm that autosomal recessive disorders are highly prevalent among patients with microcephaly.