Functionally distinct and selectively phosphorylated GPCR subpopulations co-exist in a single cell

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Ao Shen
Madeline Nieves-Cintron
Yawen Deng
Qian Shi
Dhrubajyoti Chowdhury
Jinyi Qi
Johannes W. Hell
Manuel F. Navedo
Yang K. Xiang
机构
[1] University of California Davis,Department of Pharmacology
[2] Sun Yat-sen University,The Second Affiliated Hospital
[3] University of California Davis,Department of Biomedical Engineering
[4] VA Northern California Health Care System,undefined
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G protein-coupled receptors (GPCRs) transduce pleiotropic intracellular signals in a broad range of physiological responses and disease states. Activated GPCRs can undergo agonist-induced phosphorylation by G protein receptor kinases (GRKs) and second messenger-dependent protein kinases such as protein kinase A (PKA). Here, we characterize spatially segregated subpopulations of β2-adrenergic receptor (β2AR) undergoing selective phosphorylation by GRKs or PKA in a single cell. GRKs primarily label monomeric β2ARs that undergo endocytosis, whereas PKA modifies dimeric β2ARs that remain at the cell surface. In hippocampal neurons, PKA-phosphorylated β2ARs are enriched in dendrites, whereas GRK-phosphorylated β2ARs accumulate in soma, being excluded from dendrites in a neuron maturation-dependent manner. Moreover, we show that PKA-phosphorylated β2ARs are necessary to augment the activity of L-type calcium channel. Collectively, these findings provide evidence that functionally distinct subpopulations of this prototypical GPCR exist in a single cell.
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