Beyond G protein and arrestin: GRK2-biased β₂AR signaling

除了G蛋白和阻遏蛋白之外:GRK2偏向的β₂AR信号传导

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Abstract

Biased G-protein-coupled receptor (GPCR) signaling is reshaping drug discovery by enabling pathway-selective drug action. Recent work by Motso et al. identified GPCR kinase 2 (GRK2) as a non-canonical transducer, independent of G proteins or β-arrestins, redefining the biased signaling landscape and highlighting GRK2 as a novel therapeutic target for selective modulation of GPCR-driven metabolic responses.

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