Abstract
Receptor down-modulation is the key mechanism by which G protein-coupled receptors (GPCRs) prevent excessive receptor signaling in response to agonist stimulation. Recently, the trans- Golgi network (TGN) has been implicated as a key checkpoint for receptor endocytosis and degradation. Here, we investigated the involvement of the TGN in down-modulation of β1-adrenergic receptor in response to persistent isoprotenerol stimulation. Immunofluorescent staining showed that ∼50% of endocytosed β1AR colocalized with TGN-46 at 5 h. Disruption of the TGN by brefeldin A (BFA) led to the robust accumulation of endocytosed β1AR in Rab11 + recycling endosomes, inhibited β1AR entry into LAMP1 + lysosomes, and as a result enhanced β1AR recycling to the plasma membrane. The lysosomotropic agent, chloroquine, arrested the majority of endocytosed β1AR in the TGN by 4 h. Immunoblot analysis showed that either disruption of the TGN or blockage of the lysosome prevented β1AR degradation. Co-expression of GFP-arrestin-3 in β1AR cells increased the endocytosis of β1AR and facilitated its entry to the TGN but inhibited recycling to the plasma membrane. Arrestin-3-induced inhibition of β1AR recycling was reversed by BFA treatment, whereas chloroquine induced the accumulation of arrestin-3 with β1AR in the TGN. These results demonstrate for the first time that the TGN acts as a checkpoint for both the recycling and down-regulation ofβ1AR and that arrestin- 3 not only mediates β1AR endocytosis but also its recycling through the TGN. © 2012 by The American Society for Biochemistry and Molecular Biology, Inc.
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CITATION STYLE
Cheng, S. B., & Filardo, E. J. (2012). Trans-Golgi network (TGN) as a regulatory node for β1-adrenergic receptor (β1AR) down-modulation and recycling. Journal of Biological Chemistry, 287(17), 14178–14191. https://doi.org/10.1074/jbc.M111.323782
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