Investigation of the Fate of Type I Angiotensin Receptor after Biased Activation

Szakadáti, Gyöngyi; Tóth, András; Oláh, Ilona; Erdélyi, László Sándor; Balla, Tamás; Várnai, Péter; Hunyady, László; Balla, András

doi:10.1124/mol.114.097030

Cited by 28 publications

(37 citation statements)

References 52 publications

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“…Biased AT 1 R agonists accelerated receptor internalization compared with ANG II stimulation. This is due to the differences in plasma membrane phosphatidylinositol 4,5-bisphosphate depletion (1019).…”

Section: G Protein-independent Signal Via ␤-Arrestinmentioning

confidence: 99%

Angiotensin II Signal Transduction: An Update on Mechanisms of Physiology and Pathophysiology

Forrester

Booz

Sigmund

et al. 2018

Physiological Reviews

778

780

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The renin-angiotensin-aldosterone system plays crucial roles in cardiovascular physiology and pathophysiology. However, many of the signaling mechanisms have been unclear. The angiotensin II (ANG II) type 1 receptor (ATR) is believed to mediate most functions of ANG II in the system. ATR utilizes various signal transduction cascades causing hypertension, cardiovascular remodeling, and end organ damage. Moreover, functional cross-talk between ATR signaling pathways and other signaling pathways have been recognized. Accumulating evidence reveals the complexity of ANG II signal transduction in pathophysiology of the vasculature, heart, kidney, and brain, as well as several pathophysiological features, including inflammation, metabolic dysfunction, and aging. In this review, we provide a comprehensive update of the ANG II receptor signaling events and their functional significances for potential translation into therapeutic strategies. ATR remains central to the system in mediating physiological and pathophysiological functions of ANG II, and participation of specific signaling pathways becomes much clearer. There are still certain limitations and many controversies, and several noteworthy new concepts require further support. However, it is expected that rigorous translational research of the ANG II signaling pathways including those in large animals and humans will contribute to establishing effective new therapies against various diseases.

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Section: G Protein-independent Signal Via ␤-Arrestinmentioning

confidence: 99%

Angiotensin II Signal Transduction: An Update on Mechanisms of Physiology and Pathophysiology

Forrester

Booz

Sigmund

et al. 2018

Physiological Reviews

778

780

View full text Add to dashboard Cite

show abstract

“…It has been shown previously that receptor-β-arrestin interaction may regulate the receptor's intracellular processing (47), so we hypothesized that PKC-induced β-arrestin drives intracellular receptor trafficking differently compared to the fully engaged form. To test this idea we used bystander BRET measurements between AT1R-Rluc8 and one of the intracellular vesicle markers, Venus-Rab4, Venus-Rab5, Venus-Rab7 or VenusRab11, as described previously (48,49). Rab5 is located in the early endosomes, Rab4 and Rab11 in the fast and slow recycling vesicles, respectively, whereas Rab7 is found in late endosomes, which fuse with lysosomes (46).…”

Section: Pkc-activated β-Arrestin2 Dictates Distinct Fate Of Internalmentioning

confidence: 99%

“…Cerulean-tagged versions of these mutants and wild type V2R were generated by replacing Sluc to Cerulean using AgeI/NotI restriction enzymes. Venus-Rab4, Venus-Rab7 and Venus-Rab11 were created by replacing EYFP to monomeric Venus in YFP-Rab4, YFP-Rab7 and YFP-Rab11 constructs (48). To generate Rluc8-β-arrestin2, the coding sequence of rat β-arrestin2 was subcloned from YFP-β-arrestin2 (72) after Rluc8 with a short linker sequence (RSRAQACTR) into pRluc8-C1.…”

Section: O N F I D E N T I a L Heterologous Regulation Of Inactive mentioning

confidence: 99%

Heterologous phosphorylation–induced formation of a stability lock permits regulation of inactive receptors by β-arrestins

Tóth

Prokop

Gyombolai

et al. 2018

Journal of Biological Chemistry

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β-arrestins are key regulators and signal transducers of G protein-coupled receptors (GPCRs). The interaction between receptorsand β-arrestins is generally believed to require both receptor activity and phosphorylation by GPCR kinases. In this study, we investigated whether β-arrestins are able to bind second messenger kinase-phosphorylated, but inactive receptors as well. Since heterologous phosphorylation is a common phenomenon among GPCRs, this mode of β-arrestin activation may represent a novel mechanism of signal transduction and receptor cross-talk.Here we demonstrate that activation of protein kinase C (PKC) by phorbol myristate acetate, G q/11-coupled GPCR or epidermal growth factor receptor stimulation promotes β-arrestin2 recruitment to unliganded AT1 angiotensin receptor (AT1R). We found that this interaction depends on the stability lock, a structure responsible for the sustained binding between GPCRs and β-arrestins, formed by phosphorylated serine-threonine clusters in the receptor's C-terminus and two conserved phosphate-binding lysines in the β-arrestin2 Ndomain. Using improved FlAsH-based β-arrestin2 conformational biosensors, we also show that the stability lock not only stabilizes the receptor-β-arrestin interaction, but also governs the structural rearrangements within β-arrestins. Furthermore, we found that β-arrestin2 binds to PKC-phosphorylated AT1R in a distinct active conformation, which triggers MAPK recruitment and receptor internalization. Our results provide new insights into the activation of β-arrestins and reveal their novel role in receptor cross-talk.The family of G protein-coupled receptors (GPCRs) consists of ~800 members in humans and about 30% of modern drugs target these molecules (1). GPCRs respond to a wide variety of endogenous ligands, including hormones, neurotransmitters, and lipids. Despite their huge diversity, the signal transduction mechanisms of GPCRs share several common features: agonist binding is followed by the activation of a relatively small number of heterotrimeric G proteins, which initiate complex intracellular signaling cascades. Receptor responsiveness to further stimulation is attenuated by a multistep process, called desensitization (2). In case of homologous desensitization, active GPCRs are phosphorylated by GPCR kinases (GRKs) followed by the recruitment of β-arrestin proteins (β-arrestin1 and JBC C o n f i d e n t i a lHeterologous regulation of inactive receptors via β-arrestin 2 β-arrestin2, also known as arrestin-2 and arrestin-3, respectively). β-arrestins uncouple the receptors from G proteins and initiate receptor internalization (3), thereby serving as the key regulators of GPCRs' function. In contrast, heterologous desensitization is mediated by second-messenger activated kinases, such as protein kinase C (PKC), which can phosphorylate active and inactive receptors. Heterologous desensitization was originally thought to be independent of β-arrestins, however, some data have challenged this concept (4-6). In addition to their rol...

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“…This method was successfully used to follow the intracellular trafficking route of GPCRs from the PM to different intracellular compartments (18,19). To investigate the dynamic changes of the membrane localization of peripheral membrane proteins that bind the PM, and follow their intracellular fates, we utilized the same approach with some modifications.…”

Section: Resultsmentioning

confidence: 99%

Plasma membrane phosphatidylinositol 4-phosphate and 4,5-bisphosphate determine the distribution and function of K-Ras4B but not H-Ras proteins

Gulyás

Radvánszki

Matuska

et al. 2017

Journal of Biological Chemistry

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Investigation of the Fate of Type I Angiotensin Receptor after Biased Activation

Cited by 28 publications

References 52 publications

Angiotensin II Signal Transduction: An Update on Mechanisms of Physiology and Pathophysiology

Angiotensin II Signal Transduction: An Update on Mechanisms of Physiology and Pathophysiology

Heterologous phosphorylation–induced formation of a stability lock permits regulation of inactive receptors by β-arrestins

Plasma membrane phosphatidylinositol 4-phosphate and 4,5-bisphosphate determine the distribution and function of K-Ras4B but not H-Ras proteins

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