Debunking Occam's razor: Diagnosing multiple genetic diseases in families by whole-exome sequencing

T.B. Balci; T. Hartley; Y. Xi; D.A. Dyment; C.L. Beaulieu; F.P. Bernier; L. Dupuis; G.A. Horvath; R. Mendoza-Londono; C. Prasad; J. Richer; X.-R. Yang; C.M. Armour; E. Bareke; B.A. Fernandez; H.J. McMillan; R.E. Lamont; J. Majewski; J.S. Parboosingh; A.N. Prasad; C.A. Rupar; J. Schwartzentruber; A.C. Smith; M. Tétreault; A.M. Innes; K.M. Boycott;  ;

doi:10.1111/cge.12987

A domestic cat whole exome sequencing resource for trait discovery

Scientific Reports ◽

10.1038/s41598-021-86200-7 ◽

2021 ◽

Vol 11 (1) ◽

Author(s):

Alana R. Rodney ◽

Reuben M. Buckley ◽

Robert S. Fulton ◽

Catrina Fronick ◽

Todd Richmond ◽

...

Keyword(s):

Exome Sequencing ◽

Whole Exome Sequencing ◽

Genetic Diseases ◽

Domestic Cat ◽

Whole Genome Sequence ◽

Exome Capture ◽

Single Nucleotide Variants ◽

Whole Exome ◽

Olfactory Receptor Genes ◽

Feline Model

AbstractOver 94 million domestic cats are susceptible to cancers and other common and rare diseases. Whole exome sequencing (WES) is a proven strategy to study these disease-causing variants. Presented is a 35.7 Mb exome capture design based on the annotated Felis_catus_9.0 genome assembly, covering 201,683 regions of the cat genome. Whole exome sequencing was conducted on 41 cats with known and unknown genetic diseases and traits, of which ten cats had matching whole genome sequence (WGS) data available, used to validate WES performance. At 80 × mean exome depth of coverage, 96.4% of on-target base coverage had a sequencing depth > 20-fold, while over 98% of single nucleotide variants (SNVs) identified by WGS were also identified by WES. Platform-specific SNVs were restricted to sex chromosomes and a small number of olfactory receptor genes. Within the 41 cats, we identified 31 previously known causal variants and discovered new gene candidate variants, including novel missense variance for polycystic kidney disease and atrichia in the Peterbald cat. These results show the utility of WES to identify novel gene candidate alleles for diseases and traits for the first time in a feline model.

Download Full-text

Success of Face Analysis Technology in Rare Genetic Diseases Diagnosed by Whole-Exome Sequencing: A Single-Center Experience

Molecular Syndromology ◽

10.1159/000505800 ◽

2020 ◽

Vol 11 (1) ◽

pp. 4-14 ◽

Cited By ~ 2

Author(s):

Muhsin Elmas ◽

Basak Gogus

Keyword(s):

Exome Sequencing ◽

Whole Exome Sequencing ◽

Genetic Diseases ◽

Single Center ◽

Face Analysis ◽

Single Center Experience ◽

Whole Exome ◽

Rare Genetic Diseases

Download Full-text

Pilot study of EVIDENCE: High diagnostic yield and clinical utility of whole exome sequencing using an automated interpretation system for patients with suspected genetic disorders

10.1101/628438 ◽

2019 ◽

Cited By ~ 2

Author(s):

Go Hun Seo ◽

Taeho Kim ◽

Jung-young Park ◽

Jungsul Lee ◽

Sehwan Kim ◽

...

Keyword(s):

Family Member ◽

Exome Sequencing ◽

Whole Exome Sequencing ◽

Diagnostic Yield ◽

Genetic Disorders ◽

Genetic Diseases ◽

Whole Exome ◽

Interpretation System ◽

Automated Interpretation ◽

Age Range

AbstractPurposeEVIDENCE, an automated interpretation system, has been developed to facilitate the entire process of whole exome sequencing (WES) analyses. This study investigated the diagnostic yield of EVIDENCE in patients suspected genetic disorders.MethodsDNA from 330 probands (age range, 0–68 years) with suspected genetic disorders were subjected to WES. Candidate variants were identified by EVIDENCE and confirmed by testing family members and/or clinical reassessments.ResultsThe average number of overlapping organ categories per patient was 4.5 ± 5.0. EVIDENCE reported a total 244 variants in 215 (65.1%) of the 330 probands. After clinical reassessment and/or family member testing, 196 variants were identified in 171 probands (51.8%), including 115 novel variants. These variants were confirmed as being responsible for 146 genetic disorders. One hundred-seven (54.6%) of the 196 variants were categorized as pathogenic or likely pathogenic before, and 146 (74.6%) after, clinical assessment and/or family member testing. Factors associated with a variant being confirmed as causative include rules, such as PVS1, PS1, PM1, PM5, and PP5, and similar symptom scores between that variant and a patient’s phenotype.ConclusionThis new, automated variant interpretation system facilitated the diagnosis of various genetic diseases with a 51% improvement in diagnostic yield.

Download Full-text

Whole exome sequencing uncovered highly penetrant recessive mutations for a spectrum of rare genetic pediatric diseases in Bangladesh

npj Genomic Medicine ◽

10.1038/s41525-021-00173-0 ◽

2021 ◽

Vol 6 (1) ◽

Author(s):

Hosneara Akter ◽

Mohammad Shahnoor Hossain ◽

Nushrat Jahan Dity ◽

Md. Atikur Rahaman ◽

K. M. Furkan Uddin ◽

...

Keyword(s):

Exome Sequencing ◽

Whole Exome Sequencing ◽

Genetic Diseases ◽

Leigh Syndrome ◽

Genetic Profile ◽

Compound Heterozygous ◽

Pathogenic Variants ◽

Whole Exome ◽

Rare Genetic Diseases ◽

Compound Heterozygous Variants

AbstractCollectively, rare genetic diseases affect a significant number of individuals worldwide. In this study, we have conducted whole-exome sequencing (WES) and identified underlying pathogenic or likely pathogenic variants in five children with rare genetic diseases. We present evidence for disease-causing autosomal recessive variants in a range of disease-associated genes such as DHH-associated 46,XY gonadal dysgenesis (GD) or 46,XY sex reversal 7, GNPTAB-associated mucolipidosis II alpha/beta (ML II), BBS1-associated Bardet–Biedl Syndrome (BBS), SURF1-associated Leigh Syndrome (LS) and AP4B1-associated spastic paraplegia-47 (SPG47) in unrelated affected members from Bangladesh. Our analysis pipeline detected three homozygous mutations, including a novel c. 863 G > C (p.Pro288Arg) variant in DHH, and two compound heterozygous variants, including two novel variants: c.2972dupT (p.Met991Ilefs*) in GNPTAB and c.229 G > C (p.Gly77Arg) in SURF1. All mutations were validated by Sanger sequencing. Collectively, this study adds to the genetic heterogeneity of rare genetic diseases and is the first report elucidating the genetic profile of (consanguineous and nonconsanguineous) rare genetic diseases in the Bangladesh population.

Download Full-text

Homozygosity Mapping using Whole-Exome Sequencing: A Valuable Approach for Pathogenic Variant Identification in Genetic Diseases

Proceedings of the 10th International Joint Conference on Biomedical Engineering Systems and Technologies ◽

10.5220/0006248502100216 ◽

2017 ◽

Cited By ~ 2

Author(s):

Jorge Oliveira ◽

Rute Pereira ◽

Rosário Santos ◽

Mário Sousa

Keyword(s):

Exome Sequencing ◽

Whole Exome Sequencing ◽

Genetic Diseases ◽

Homozygosity Mapping ◽

Pathogenic Variant ◽

Whole Exome ◽

Variant Identification

Download Full-text

B.06 Whole exome sequencing in genetic ataxias associated with cerebellar atrophy: the Canadian experience

Canadian Journal of Neurological Sciences / Journal Canadien des Sciences Neurologiques ◽

10.1017/cjn.2019.95 ◽

2019 ◽

Vol 46 (s1) ◽

pp. S11

Author(s):

L Gauquelin ◽

T Hartley ◽

M Tarnopolsky ◽

DA Dyment ◽

B Brais ◽

...

Keyword(s):

Exome Sequencing ◽

Whole Exome Sequencing ◽

Diagnostic Yield ◽

Genetic Diseases ◽

Genetic Diagnosis ◽

Cerebellar Atrophy ◽

Clinical Findings ◽

Disease Genes ◽

Pathogenic Variants ◽

Whole Exome

Background: Cerebellar atrophy is characterized by loss of cerebellar tissue, with evidence on brain imaging of enlarged interfolial spaces compared to the foliae. Genetic ataxias associated with cerebellar atrophy are a heterogeneous group of disorders. We investigated the prevalence in Canada and the diagnostic yield of whole exome sequencing (WES) for this group of conditions. Methods: Between 2011 and 2017, WES was performed in 91 participants with cerebellar atrophy as part of one of two national research programs, Finding of Rare Genetic Disease Genes (FORGE) or Enhanced Care for Rare Genetic Diseases in Canada (Care4Rare). Results: A genetic diagnosis was established in 58% of cases (53/91). Pathogenic variants were found in 24 known genes, providing a diagnosis for 46/53 participants (87%), and in four novel genes, accounting for 7/53 cases (13%). 38/91 cases (42%) remained unsolved. The most common diagnoses were channelopathies in 12/53 patients (23%) and mitochondrial disorders in 9/53 (17%). Inheritance was autosomal recessive in the majority of cases. Additional clinical findings provided useful clues to some of the diagnoses. Conclusions: This is the first report on the prevalence of genetic ataxias associated with cerebellar atrophy in Canada, and the utility of WES for this group of conditions.

Download Full-text

Palmoplantar keratoderma and Charcot-Marie-Tooth disease: combination of two independent genetic diseases? Identification of two point mutations in the MPZ and KRT1 genes by whole-exome sequencing

British Journal of Dermatology ◽

10.1111/bjd.15066 ◽

2017 ◽

Vol 177 (1) ◽

pp. 284-286 ◽

Cited By ~ 2

Author(s):

S. Gagliardi ◽

I. Ricca ◽

A. Ferrarini ◽

M. Valente ◽

G.S. Grieco ◽

...

Keyword(s):

Exome Sequencing ◽

Whole Exome Sequencing ◽

Genetic Diseases ◽

Point Mutations ◽

Palmoplantar Keratoderma ◽

Charcot Marie Tooth ◽

Charcot Marie Tooth Disease ◽

Whole Exome ◽

Tooth Disease

Download Full-text

Whole-exome sequencing in undiagnosed genetic diseases: interpreting 119 trios

Genetics in Medicine ◽

10.1038/gim.2014.191 ◽

2015 ◽

Vol 17 (10) ◽

pp. 774-781 ◽

Cited By ~ 180

Author(s):

Xiaolin Zhu ◽

Slavé Petrovski ◽

Pingxing Xie ◽

Elizabeth K. Ruzzo ◽

Yi-Fan Lu ◽

...

Keyword(s):

Exome Sequencing ◽

Whole Exome Sequencing ◽

Genetic Diseases ◽

Whole Exome

Download Full-text

SUN-721 Implementation of Whole Exome Sequencing for Clinical Diagnostics: A Prospective Busan Kyung-Sang Regional Co-Work Team Experience

Journal of the Endocrine Society ◽

10.1210/jendso/bvaa046.1485 ◽

2020 ◽

Vol 4 (Supplement_1) ◽

Author(s):

Jeong Eun Lee ◽

WooYeong Chung ◽

BoLyun Lee ◽

SooHyun Ku ◽

Ga Won Jeon ◽

...

Keyword(s):

Exome Sequencing ◽

Whole Exome Sequencing ◽

Diagnostic Yield ◽

Genetic Disorder ◽

Genetic Diseases ◽

Clinical Diagnostics ◽

Buccal Swab ◽

Variant Interpretation ◽

Pathogenic Variants ◽

Whole Exome

Abstract Purpose: Next Generation Sequencing (NGS) technology is a highthroughput method for genome sequencing which assists clinicians with diagnosis of patients with suspected genetic disorders. This study was to investigate diagnostic yield and clinical utility of whole exome sequencing prospectively in the rare genetic diseases. Method: WES was performed a total of 178 patients with suspected genetic disorder. Buccal swab samples were collected from the patients to extract genomic DNA. WES and variant interpretation was conducted in 3 Billion Inc (Seoul, Republic of Korea), based on their own software. Patients’ phenotype was interpreted by clinical geneticists. Results: WES reported 117 variants (66.7%). According to the ACMG/AMP guidelines, there were 25 pathogenic variants (14%), 37 likely pathogenic variants (32%), and 55 VUS (31%). Among the 117 patients who detected variants, genotype-phenotype correlation was analyzed and resulted that 44 (38%) were found to be apparently causal mutation of the disease, 37 (32%) were not considered the cause of the disease, and 36 (31%) were withheld judgement. Of the VUS variants, 13% were likely to be the causal variants of the disease considering phenotype of patients. Conclusion: This study showed 38% of diagnostic yield in patients with unidentified genetic condition by using prospective WES based on automating variant interpretation system. In the diagnosis of rare genetic disease, we identified the need for a multi-disciplinary team to select appropriate subjects and interpret the clinical significance of the found genetic variants.

Download Full-text

Ending diagnostic odyssey using clinical whole-exome sequencing (CWES)

Journal of Laboratory Medicine ◽

10.1515/labmed-2021-0127 ◽

2021 ◽

Vol 45 (6) ◽

pp. 259-266

Author(s):

Ching-Wan Lam

Keyword(s):

Hong Kong ◽

Exome Sequencing ◽

Whole Exome Sequencing ◽

Rare Diseases ◽

Genetic Diseases ◽

Definitive Diagnosis ◽

Diagnostic Odyssey ◽

Essential Tool ◽

Whole Exome ◽

Undiagnosed Diseases

Abstract Objectives Most rare diseases are genetic diseases. Due to the diversity of rare diseases and the high likelihood of patients with rare diseases to be undiagnosed or misdiagnosed, it is not unusual that these patients undergo a long diagnostic odyssey before they receive a definitive diagnosis. This situation presents a clear need to set up a dedicated clinical service to end the diagnostic odyssey of patients with rare diseases. Methods Therefore, in 2014, we started an Undiagnosed Diseases Program in Hong Kong with the aim of ending the diagnostic odyssey of patients and families with rare diseases by clinical whole-exome sequencing (CWES), who have not received a definitive diagnosis after extensive investigation. Results In this program, we have shown that genetic diseases diagnosed by CWES were different from that using traditional approaches indicating that CWES is an essential tool to diagnose rare diseases and ending diagnostic odysseys. In addition, we identified several novel genes responsible for monogenic diseases. These include the TOP2B gene for autism spectrum disorder, the DTYMK gene for severe cerebral atrophy, the KIF13A gene for a new mosaic ectodermal syndrome associated with hypomelanosis of Ito, and the CDC25B gene for a new syndrome of cardiomyopathy and endocrinopathy. Conclusions With the incorporation of CWES in an Undiagnosed Diseases Program, we have ended diagnostic odysseys of patients with rare diseases in Hong Kong in the past 7 years. In this program, we have shown that CWES is an essential tool to end diagnostic odysseys. With the declining cost of next-generation sequencers and reagents, CWES set-ups are now affordable for clinical laboratories. Indeed, owing to the increasing availability of CWES and treatment modalities for rare diseases, precedence can be given to both common and rare medical conditions.

Download Full-text