Affiliation:
1. Hanoi Medical University Hanoi Vietnam
2. National Institute of Ophthalmology Hanoi Vietnam
3. Center for Molecular Medicine, Clinical Genetics Unit Karolinska Institutet, Karolinska University Hospital Stockholm Sweden
4. Hanoi Medical University Hospital, Hanoi Medical University Hanoi Vietnam
Abstract
AbstractBackgroundRetinoblastoma (RB), an intraocular malignancy commonly diagnosed in children, is mostly caused by inactivating mutations of both alleles of the RB1 gene. Early genetic screening for RB1 gene mutations would greatly improve treatment outcomes and patient management.MethodsIn this study, both somatic and germline mutations were detected in blood and tumour samples of 42 RB patients using direct sequencing and multiplex ligation‐dependent probe amplification.ResultsIn total, 34 different mutations were found in 36 patients, including 1 SNP, 4 large deletions, 5 splicing sites, 1 missense, 7 frameshifts and 17 nonsense mutations. There were five novel mutations and one unreported which have not been found in large databases such as Leiden Open Variation Database (LOVD) and ClinVar.ConclusionA higher rate of RB patients carrying heterozygous germline mutation and highly prevalent with pathogenic truncated mutation, hence, early detection of RB is essential for vision salvation and genetic counselling.
Subject
Genetics (clinical),Genetics,Molecular Biology