Adhesion Class GPCRs in GtoPdb v.2021.3

Torsten Schöneberg,Diana Le Duc,Uwe Wolfrum,Heike Cappallo-Obermann,Tom I Bonner,Simone Prömel,Lei Xu,Gabriela Aust,Arunkumar Krishnan,Barbara Knapp,Tobias Langenhan,Martin Stacey,Christiane Kirchhoff,Jörg Hamann,Demet Araç-Özkan ,Kathleen Singer ,Caroline J Formstone ,Hsi‐Hsien Lin ,Kelly R Monk ,David C Martinelli ,Xiangshu Piao ,Breanne L Harty ,Helgi B Schiöth ,Henrike O Heyne ,Yuri A Ushkaryov

doi:10.2218/gtopdb/f17/2021.3

Adhesion Class GPCRs in GtoPdb v.2021.3

Torsten Schöneberg, Diana Le Duc + Show 23 more

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https://doi.org/10.2218/gtopdb/f17/2021.3

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Journal: IUPHAR/BPS Guide to Pharmacology CITE	Publication Date: Sep 2, 2021
License type: CC BY-SA 4.0

Affiliation: Leipzig University, Johannes Gutenberg University Mainz, Universität Hamburg, University of Rochester, Uppsala University, University of Leeds, University of Amsterdam, University of Chicago, Boston Children's Hospital, Boston Children's Museum, King's College London, Chang Gung University, University of Washington, Stanford University, University of Kent

#GPCR Proteolytic Site #Adhesion GPCR + Show 8 more

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Abstract

Adhesion GPCRs are structurally identified on the basis of a large extracellular region, similar to the Class B GPCR, but which is linked to the 7TM region by a GPCR autoproteolysis-inducing (GAIN) domain [9] containing a GPCR proteolytic site. The N-terminus often shares structural homology with adhesive domains (e.g. cadherins, immunolobulin, lectins) facilitating inter- and matricellular interactions and leading to the term adhesion GPCR [101, 403]. Several receptors have been suggested to function as mechanosensors [309, 280, 383, 35]. The nomenclature of these receptors was revised in 2015 as recommended by NC-IUPHAR and the Adhesion GPCR Consortium [122].

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