| Literature DB >> 32901917 |
Go Hun Seo1, Taeho Kim2, In Hee Choi3, Jung-Young Park1, Jungsul Lee1, Sehwan Kim1, Dhong-Gun Won1, Arum Oh4, Yena Lee4, Jeongmin Choi2, Hajeong Lee5, Hee Gyung Kang6, Hee Yeon Cho7, Min Hyun Cho8, Yoon Jeon Kim9, Young Hee Yoon9, Baik-Lin Eun10, Robert J Desnick11, Changwon Keum1, Beom Hee Lee3,4.
Abstract
EVIDENCE, an automated variant prioritization system, has been developed to facilitate whole exome sequencing analyses. This study investigated the diagnostic yield of EVIDENCE in patients with suspected genetic disorders. DNA from 330 probands (age range, 0-68 years) with suspected genetic disorders were subjected to whole exome sequencing. Candidate variants were identified by EVIDENCE and confirmed by testing family members and/or clinical reassessments. EVIDENCE reported a total 228 variants in 200 (60.6%) of the 330 probands. The average number of organs involved per patient was 4.5 ± 5.0. After clinical reassessment and/or family member testing, 167 variants were identified in 141 probands (42.7%), including 105 novel variants. These variants were confirmed as being responsible for 121 genetic disorders. A total of 103 (61.7%) of the 167 variants in 95 patients were classified as pathogenic or probably to be pathogenic before, and 161 (96.4%) variants in 137 patients (41.5%) after, clinical assessment and/or family member testing. Factor associated with a variant being regarded as causative includes similar symptom scores of a gene variant to the phenotype of the patient. This new, automated variant interpretation system facilitated the diagnosis of various genetic diseases with a 42.7% diagnostic yield.Entities:
Keywords: automated prioritization system; genetic diagnosis; variant; whole exome sequencing
Year: 2020 PMID: 32901917 PMCID: PMC7756481 DOI: 10.1111/cge.13848
Source DB: PubMed Journal: Clin Genet ISSN: 0009-9163 Impact factor: 4.438