GeneMatcher: A Matching Tool for Connecting Investigators with an Interest in the Same Gene

Sobreira, Nara; Schiettecatte, François; Valle, David; Hamosh, Ada

doi:10.1002/humu.22844

Cited by 1,240 publications

(1,100 citation statements)

References 6 publications

(6 reference statements)

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“…52,53 A homozygous extended splice site mutation, c.322À10G>A, was identified in subjects 2a, 2b, 3a, and 3b of Puerto Rican ethnicity; these subjects were ascertained with assistance from the GeneMatcher tool. 54 This variant is predicted to abolish the acceptor splice site and create a new cryptic splice acceptor site within intron 1, causing abnormal gene splicing. The MRPS34 c.322À10G>A variant is reported in dbSNP (rs563189672), and two heterozygous individuals (both of Latino ethnicity) were reported in the gnomAD Browser (2 of 236,804 alleles examined, no homozygotes observed).…”

Section: Resultsmentioning

confidence: 99%

Biallelic Mutations in MRPS34 Lead to Instability of the Small Mitoribosomal Subunit and Leigh Syndrome

Lake

Webb

Stroud

et al. 2017

The American Journal of Human Genetics

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Section: Resultsmentioning

confidence: 99%

Biallelic Mutations in MRPS34 Lead to Instability of the Small Mitoribosomal Subunit and Leigh Syndrome

Lake

Webb

Stroud

et al. 2017

The American Journal of Human Genetics

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“…GeneMatcher postings, and subsequent communications, enabled independent discoveries to be corroborated. 10 Written informed consent for exome sequencing and approval by ethics review boards were obtained from Erasmus Medical Center (protocol MEC-2012387) for individual 1 and from the University of British Columbia (protocols H-15-00092, H-09-01228, and H-14-01531) for individuals 2 and 4. Individual 3 received sequencing through clinical care, and written informed consent was obtained for publication of medical history.…”

Section: Introductionmentioning

confidence: 99%

Loss-of-Function and Gain-of-Function Mutations in KCNQ5 Cause Intellectual Disability or Epileptic Encephalopathy

Lehman

Thouta

Mancini

et al. 2017

The American Journal of Human Genetics

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“…In an attempt to identify additional carriers of de novo variants in SLC1A2 and YWHAG, we queried biomedical literature on PubMed and three online resources: (1) GeneMatcher, 21 a freely accessible tool that connects clinicians and researchers with interests in the same gene; (2) DECIPHER, which contains exome sequencing data from nearly 4,300 families affected by developmental disorders; 22,23 [REVEL]). None have been reported in public databases (gnomAD Browser), and one mutation (YWHAG c.394C>T) is recurrent in three subjects (B, E, and F).…”

mentioning

confidence: 99%

De Novo Mutations in YWHAG Cause Early-Onset Epilepsy

Guella

McKenzie

Evans

et al. 2017

The American Journal of Human Genetics

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Massively parallel sequencing has revealed many de novo mutations in the etiology of developmental and epileptic encephalopathies (EEs), highlighting their genetic heterogeneity. Additional candidate genes have been prioritized in silico by their co-expression in the brain. Here, we evaluate rare coding variability in 20 candidates nominated with the use of a reference gene set of 51 established EE-associated genes. Variants within the 20 candidate genes were extracted from exome-sequencing data of 42 subjects with EE and no previous genetic diagnosis. We identified 7 rare non-synonymous variants in 7 of 20 genes and performed Sanger sequence validation in affected probands and parental samples. De novo variants were found only in SLC1A2 (aka EAAT2 or GLT1) (c.244G>A [p.Gly82Arg]) and YWHAG (aka 14-3-3g) (c.394C>T [p.Arg132Cys]), highlighting the potential cause of EE in 5% (2/42) of subjects. Seven additional subjects with de novo variants in SLC1A2 (n ¼ 1) and YWHAG (n ¼ 6) were subsequently identified through online tools. We identified a highly significant enrichment of de novo variants in YWHAG, establishing their role in early-onset epilepsy, and we provide additional support for the prior assignment of SLC1A2. Hence, in silico modeling of brain co-expression is an efficient method for nominating EE-associated genes to further elucidate the disorder's etiology and genotype-phenotype correlations.

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GeneMatcher: A Matching Tool for Connecting Investigators with an Interest in the Same Gene

Cited by 1,240 publications

References 6 publications

Biallelic Mutations in MRPS34 Lead to Instability of the Small Mitoribosomal Subunit and Leigh Syndrome

Biallelic Mutations in MRPS34 Lead to Instability of the Small Mitoribosomal Subunit and Leigh Syndrome

Loss-of-Function and Gain-of-Function Mutations in KCNQ5 Cause Intellectual Disability or Epileptic Encephalopathy

De Novo Mutations in YWHAG Cause Early-Onset Epilepsy

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