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Monitoring GPCR-beta-arrestin1/2 Interactions in Real Time Living Systems to Accelerate Drug Discovery

Authors
Reyes-Alcaraz, ArfaxadLee, Yoo-NaYun, SeongsikHwang, Jong-IkSeong, Jae Young
Issue Date
Jun-2019
Publisher
JOURNAL OF VISUALIZED EXPERIMENTS
Keywords
Biochemistry; Issue 148; beta-arrestins; G-protein coupled receptors; drug discovery; living systems; real time; structural complementation assay; drug development
Citation
JOVE-JOURNAL OF VISUALIZED EXPERIMENTS, no.148
Indexed
SCIE
SCOPUS
Journal Title
JOVE-JOURNAL OF VISUALIZED EXPERIMENTS
Number
148
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/131417
DOI
10.3791/59994
ISSN
1940-087X
Abstract
Interactions between G-protein coupled receptors (GPCRs) and beta-arrestins are vital processes with physiological implications of great importance. Currently, the characterization of novel drugs towards their interactions with beta-arrestins and other cytosolic proteins is extremely valuable in the field of GPCR drug discovery particularly during the study of GPCR biased agonism. Here, we show the application of a novel structural complementation assay to accurately monitor receptor-beta-arrestin interactions in real time living systems. This method is simple, accurate and can be easily extended to any GPCR of interest and also it has the advantage that it overcomes unspecific interactions due to the presence of a low expression promoter present in each vector system. This structural complementation assay provides key features that allow an accurate and precise monitoring of receptor-beta-arrestin interactions, making it suitable in the study of biased agonism of any GPCR system as well as GPCR c-terminus 'phosphorylation codes' written by different GPCR-kinases (GRKs) and post-translational modifications of arrestins that stabilize or destabilize the receptor-beta-arrestin complex.
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