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A new inhibitor of the β-arrestin/AP2 endocytic complex reveals interplay between GPCR internalization and signalling.

Nat Commun. 2017; 
BeautraitAlexandre,ParadisJustine S,ZimmermanBrandon,GiubilaroJenna,NikolajevLjiljana,ArmandoSylvain,KobayashiHiroyuki,YamaniLama,NamkungYoon,HeydenreichFranziska M,KhouryEtienne,AudetMartin,RouxPhilippe P,VeprintsevDmitry B,LaporteStéphane A,BouvierMi
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Gene Synthesis b-arrestin1 C-terminal peptide (sequence: DDDIVFEDFARQRLKGMKDD) was synthesized by Genscript, while CPM dye was purchased from ThermoFisher Scientific.b2-adaptin deletion in HEK293 cells (CRISPR-b2Ad) were generated using the CRISPR/Cas9 system PspCas9(BB)-2A-Puro (Px459v2) vector (Gift from Feng Zhang: Addgene plasmid #62988)70 and the gRNA target sequences (50-GTA TTTCACAACCAATAAAAA-30 and 50-GGTCTGGCTACCTGCAGTAA-30) against the human AP2B1 gene (GenScript gRNA database). Samples containing 0.5mM Triton X-100 were incubated for 30min without Barbadin (DMSO), with 10mM, 33mM or 100mM Barbadin, or with 20mM b-arrestin1 C-terminal peptide (sequence: DDDIVFEDFARQRLKGMKDD), synthesized by Genscript, USA) before the addition of CPM dye (ThermoFisher Scientific, Switzerland). Get A Quote

摘要

In addition to G protein-coupled receptor (GPCR) desensitization and endocytosis, β-arrestin recruitment to ligand-stimulated GPCRs promotes non-canonical signalling cascades. Distinguishing the respective contributions of β-arrestin recruitment to the receptor and β-arrestin-promoted endocytosis in propagating receptor signalling has been limited by the lack of selective analytical tools. Here, using a combination of virtual screening and cell-based assays, we have identified a small molecule that selectively inhibits the interaction between β-arrestin and the β2-adaptin subunit of the clathrin adaptor protein AP2 without interfering with the formation of receptor/β-arrestin complexes. This selecti... More

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