Systematic protein-protein interaction mapping for clinically relevant human GPCRs

dc.contributor.author
Sokolina, Kate
dc.contributor.author
Kittanakom, Sarayana
dc.contributor.author
Snider, Jamie
dc.contributor.author
Kotlyar, Max
dc.contributor.author
Maurice, Pascal
dc.contributor.author
Gandía Sánchez, Jorge
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Benleulmi-Chaachoua, Abla
dc.contributor.author
Tadagaki, Kenjiro
dc.contributor.author
Oishi, Atsuro
dc.contributor.author
Wong, Victoria
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Malty, Ramy H.
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Deineko, Viktor
dc.contributor.author
Aoki, Hiroyuki
dc.contributor.author
Amin, Shahreen
dc.contributor.author
Yao, Zhong
dc.contributor.author
Morató Arús, Xavier
dc.contributor.author
Otasek, David
dc.contributor.author
Kobayashi, Hiroyuki
dc.contributor.author
Menendez, Javier
dc.contributor.author
Auerbach, Daniel
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Angers, Stephan
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Przulj, Natasa
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Bouvier, Michael
dc.contributor.author
Babu, Mohan
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Ciruela Alférez, Francisco
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Jockers, Ralf
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Jurisica, Igor
dc.contributor.author
Stagljar, Igor
dc.date.issued
2018-05-02T13:14:35Z
dc.date.issued
2018-05-02T13:14:35Z
dc.date.issued
2017-03-15
dc.date.issued
2018-05-02T13:14:35Z
dc.identifier
1744-4292
dc.identifier
https://hdl.handle.net/2445/122006
dc.identifier
679440
dc.identifier
28298427
dc.description.abstract
G‐protein‐coupled receptors (GPCRs) are the largest family of integral membrane receptors with key roles in regulating signaling pathways targeted by therapeutics, but are difficult to study using existing proteomics technologies due to their complex biochemical features. To obtain a global view of GPCR‐mediated signaling and to identify novel components of their pathways, we used a modified membrane yeast two‐hybrid (MYTH) approach and identified interacting partners for 48 selected full‐length human ligand‐unoccupied GPCRs in their native membrane environment. The resulting GPCR interactome connects 686 proteins by 987 unique interactions, including 299 membrane proteins involved in a diverse range of cellular functions. To demonstrate the biological relevance of the GPCR interactome, we validated novel interactions of the GPR37, serotonin 5‐HT4d, and adenosine ADORA2A receptors. Our data represent the first large‐scale interactome mapping for human GPCRs and provide a valuable resource for the analysis of signaling pathways involving this druggable family of integral membrane proteins.
dc.format
19 p.
dc.format
application/pdf
dc.format
application/pdf
dc.language
eng
dc.publisher
EMBO Press
dc.relation
Reproducció del document publicat a: https://doi.org/10.15252/msb.20167430
dc.relation
Molecular Systems Biology, 2017, vol. 13, num. 3, p. 918
dc.relation
https://doi.org/10.15252/msb.20167430
dc.relation
info:eu-repo/grantAgreement/EC/FP7/278212/EU//BIONET
dc.rights
cc-by (c) Sokolina, Kate et al., 2017
dc.rights
http://creativecommons.org/licenses/by/3.0/es
dc.rights
info:eu-repo/semantics/openAccess
dc.source
Articles publicats en revistes (Patologia i Terapèutica Experimental)
dc.subject
Proteïnes G
dc.subject
Metabolisme de proteïnes
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Adenosina
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Receptors de serotonina
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Receptors cel·lulars
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Neurotransmissors
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G Proteins
dc.subject
Protein metabolism
dc.subject
Adenosine
dc.subject
Serotonin receptors
dc.subject
Cell receptors
dc.subject
Neurotransmitters
dc.title
Systematic protein-protein interaction mapping for clinically relevant human GPCRs
dc.type
info:eu-repo/semantics/article
dc.type
info:eu-repo/semantics/publishedVersion


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