Matchmaker Exchange

on behalf of the Matchmaker Exchange Consortium

doi:10.1002/cphg.50

Matchmaker Exchange

on behalf of the Matchmaker Exchange Consortium

School of Medicine

Research output: Contribution to journal › Article › peer-review

37 Scopus citations

Abstract

In well over half of the individuals with rare disease who undergo clinical or research next-generation sequencing, the responsible gene cannot be determined. Some reasons for this relatively low yield include unappreciated phenotypic heterogeneity; locus heterogeneity; somatic and germline mosaicism; variants of uncertain functional significance; technically inaccessible areas of the genome; incorrect mode of inheritance investigated; and inadequate communication between clinicians and basic scientists with knowledge of particular genes, proteins, or biological systems. To facilitate such communication and improve the search for patients or model organisms with similar phenotypes and variants in specific candidate genes, we have developed the Matchmaker Exchange (MME). MME was created to establish a federated network connecting databases of genomic and phenotypic data using a common application programming interface (API). To date, seven databases can exchange data using the API (GeneMatcher, PhenomeCentral, DECIPHER, MyGene2, matchbox, Australian Genomics Health Alliance Patient Archive, and Monarch Initiative; the latter included for model organism matching). This article guides usage of the MME for rare disease gene discovery.

Original language	English (US)
Pages (from-to)	9.31.1-9.31.15
Journal	Current protocols in human genetics
Volume	95
Issue number	1
DOIs	https://doi.org/10.1002/cphg.50
State	Published - Oct 2017

Keywords

Australian Genomics Health Alliance Patient Archive
DECIPHER
GeneMatcher
MyGene2
PhenomeCentral
candidate genes
matchbox
matchmaker exchange
monarch initiative

ASJC Scopus subject areas

Genetics
Genetics(clinical)

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10.1002/cphg.50

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title = "Matchmaker Exchange",

abstract = "In well over half of the individuals with rare disease who undergo clinical or research next-generation sequencing, the responsible gene cannot be determined. Some reasons for this relatively low yield include unappreciated phenotypic heterogeneity; locus heterogeneity; somatic and germline mosaicism; variants of uncertain functional significance; technically inaccessible areas of the genome; incorrect mode of inheritance investigated; and inadequate communication between clinicians and basic scientists with knowledge of particular genes, proteins, or biological systems. To facilitate such communication and improve the search for patients or model organisms with similar phenotypes and variants in specific candidate genes, we have developed the Matchmaker Exchange (MME). MME was created to establish a federated network connecting databases of genomic and phenotypic data using a common application programming interface (API). To date, seven databases can exchange data using the API (GeneMatcher, PhenomeCentral, DECIPHER, MyGene2, matchbox, Australian Genomics Health Alliance Patient Archive, and Monarch Initiative; the latter included for model organism matching). This article guides usage of the MME for rare disease gene discovery.",

keywords = "Australian Genomics Health Alliance Patient Archive, DECIPHER, GeneMatcher, MyGene2, PhenomeCentral, candidate genes, matchbox, matchmaker exchange, monarch initiative",

author = "{on behalf of the Matchmaker Exchange Consortium} and Sobreira, {Nara L.M.} and Harindra Arachchi and Buske, {Orion J.} and Chong, {Jessica X.} and Ben Hutton and Julia Foreman and Fran{\c c}ois Schiettecatte and Tudor Groza and Jacobsen, {Julius O.B.} and Haendel, {Melissa A.} and Boycott, {Kym M.} and Ada Hamosh and Rehm, {Heidi L.}",

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year = "2017",

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Matchmaker Exchange

Abstract

Keywords

ASJC Scopus subject areas

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