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- W2134920278 endingPage "559" @default.
- W2134920278 startingPage "535" @default.
- W2134920278 abstract "Despite the fact that G protein-coupled receptors (GPCRs) are the most successful drug targets in history, this supergene family of cell surface receptors has yet to be fully exploited as targets in the treatment of human disease. Here, we present optimism that this may change in the future by reviewing the substantial progress made in the understanding of GPCR molecular pharmacology that has generated an extensive toolbox of ligand types that include orthosteric, allosteric, and bitopic ligands, many of which show signaling bias. We discuss how combining these advances with recently described transgenic, chemical genetic, and optogenetic animal models will provide the framework to allow for the rational design of next-generation GPCR drugs that possess increased therapeutic efficacy and decreased adverse/toxic responses." @default.
- W2134920278 created "2016-06-24" @default.
- W2134920278 creator A5035925879 @default.
- W2134920278 creator A5084866615 @default.
- W2134920278 date "2016-01-06" @default.
- W2134920278 modified "2023-10-18" @default.
- W2134920278 title "Design of Next-Generation G Protein–Coupled Receptor Drugs: Linking Novel Pharmacology and In Vivo Animal Models" @default.
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