Your search keyword '"Gpr3"' showing total 140 results

1. Potential role of inducible GPR3 expression under stimulated T cell conditions

Author

Hiroko Shiraki, Shigeru Tanaka, Yun Guo, Kana Harada, Izumi Hide, Tomoharu Yasuda, and Norio Sakai

Subjects

GPR3, T cell, NR4A2, cAMP, Gαs protein, Therapeutics. Pharmacology, RM1-950

Abstract

G protein-coupled receptor 3 (GPR3) constitutively activates Gαs proteins without any ligands and is predominantly expressed in neurons. Since the expression and physiological role of GPR3 in immune cells is still unknown, we examined the possible role of GPR3 in T lymphocytes. The expression of GPR3 was upregulated 2 h after phorbol 12-myristate 13-acetate (PMA)/ionomycin stimulation and was sustained in Jurkat cells, a human T lymphocyte cell line. In addition, the expression of nuclear receptor 4 group A member 2 (NR4A2) was highly modulated by GPR3 expression. Additionally, GPR3 expression was linked with the transcriptional promoter activity of NR4A in Jurkat cells. In mouse CD4+ T cells, transient GPR3 expression was induced immediately after the antigen receptor stimulation. However, the expression of NR4A2 was not modulated in CD4+ T cells from GPR3-knockout mice after stimulation, and the population of Treg cells in thymocytes and splenocytes was not affected by GPR3 knockout. By contrast, spontaneous effector activation in both CD4+ T cells and CD8+ T cells was observed in GPR3-knockout mice. In summary, GPR3 is immediately induced by T cell stimulation and play an important role in the suppression of effector T cell activation.

Published

2022

2. The role of PDZ interactions in regulating surface expression of GPR3 in fat tissue

Author

Madsen, Kenneth Lindegaard, Nielsen, Tommas Theiss Ehler, Nierich, Rebecca Mai, Madsen, Kenneth Lindegaard, Nielsen, Tommas Theiss Ehler, and Nierich, Rebecca Mai

Abstract

The capacity of the G-protein coupled receptor GPR3 to activate non-shivering thermogenesis in BAT is a compelling alternative target for weight management. As GPR3 exhibit constitutive activity and internalisation in the absence of a ligand, cytosolic interaction was investigated to further understand surface expression regulation of GPR3. In the C-terminus of GPR3 a putative PDZ- binding motif is located, and removal of this motif have shown decreased internalisation of the receptor. Thus, it was hypothesised that a PDZ-interaction was involved in the regulation of GPR3 internalisation. The phenotypic distribution along the endocytic pathway of GPR3 wildtype (WT) and mutant was altered determined by co-localisation assays. This study highlighted the importance of the motif for internalisation behaviour of the receptor. A possible GPR3 interaction partner, MAGUK p55 scaffold protein 7 (MPP7), was identified by mass-spectrometry, but an interaction could not be confirmed by either fluorescence polarisation or knock down (KD) studies of MPP7. Closely related GPR6 and GPR12 was further investigated, and the PDZ dependent internalisation seemed unique for GPR3, indicating that other regions within the receptor could play an important role for internalisation as well. This study explores the role of GPR3 PDZ interactions with the aim to further understand how to regulate surface expression of GPR3.

Published

2024

3. GPR3 expression in retinal ganglion cells contributes to neuron survival and accelerates axonal regeneration after optic nerve crush in mice

Author

Shun Masuda, Shigeru Tanaka, Hiroko Shiraki, Yusuke Sotomaru, Kana Harada, Izumi Hide, Yoshiaki Kiuchi, and Norio Sakai

Subjects

GPR3, cAMP, Axonal regeneration, Retinal granular cells, Neuronal survival, Optic nerve injury, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Glaucoma is an optic neuropathy and is currently one of the most common diseases that leads to irreversible blindness. The axonal degeneration that occurs before retinal ganglion neuronal loss is suggested to be involved in the pathogenesis of glaucoma. G protein-coupled receptor 3 (GPR3) belongs to the class A rhodopsin-type GPCR family and is highly expressed in various neurons. GPR3 is unique in its ability to constitutively activate the Gαs protein without a ligand, which elevates the basal intracellular cAMP level. Our earlier reports suggested that GPR3 enhances both neurite outgrowth and neuronal survival. However, the potential role of GPR3 in axonal regeneration after neuronal injury has not been elucidated. Herein, we investigated retinal GPR3 expression and its possible involvement in axonal regeneration after retinal injury in mice. GPR3 was relatively highly expressed in retinal ganglion cells (RGCs). Surprisingly, RGCs in GPR3 knockout mice were vulnerable to neural death during aging without affecting high intraocular pressure (IOP) and under ischemic conditions. Primary cultured neurons from the retina showed that GPR3 expression was correlated with neurite outgrowth and neuronal survival. Evaluation of the effect of GPR3 on axonal regeneration using GPR3 knockout mice revealed that GPR3 in RGCs participates in axonal regeneration after optic nerve crush (ONC) under zymosan stimulation. In addition, regenerating axons were further stimulated when GPR3 was upregulated in RGCs, and the effect was further augmented when combined with zymosan treatment. These results suggest that GPR3 expression in RGCs helps maintain neuronal survival and accelerates axonal regeneration after ONC in mice.

Published

2022

4. Molecular cloning, expression patterns and functional characterization of Gpr3 in the orange-spotted grouper (Epinephelus coioides)

Author

Fengying Yan, Xinxun Xiao, Lin Tang, Yikun Song, Chong Han, Chongwei Wang, Jin Zhang, Haoran Lin, Chunren Huang, Jiarui He, Yong Zhang, and Shuisheng Li

Subjects

Gpr3, Cloning, Expression patterns, Functional characterization, Orange-spotted grouper, Aquaculture. Fisheries. Angling, SH1-691

Abstract

G Protein-coupled receptor 3 (Gpr3) plays a critical role in maintaining oocyte meiotic arrest in mammals. To ascertain the function of Gpr3 in oocyte maturation in fish, the Gpr3 cDNA was cloned from orange-spotted grouper (Epinephelus coioides). The open reading frame of cloned sequence was 993 bp in length, encoding 330 amino acids. Gpr3 was primarily expressed in brain regions and ovary. During oocyte maturation induced by human chorionic gonadotropin (hCG), Gpr3 expression levels were dramatically elevated in follicular cell layers. Functional analysis showed that Gpr3 could constitutively active the cAMP/PKA signaling pathway, and hCG treatment activated Gpr3 promoter activities in cultured eukaryotic cells expressing luteinizing hormone receptors (LHRs). Finally, the role of Gpr3 in oocyte maturation was studied. Sphingosine 1-phosphate (S1P), an agonist of Gpr3, had no effect on oocyte maturation in vivo, suggesting that Gpr3 may be not involved in oocyte maturation in orange-spotted grouper.

Published

2022

5. The development of diphenyleneiodonium analogs as GPR3 agonists.

Author

Gay, Elaine A., Harris, Danni L., Wilson, Joseph W., and Blough, Bruce E.

Subjects

*PHARMACEUTICAL chemistry, *PSILOCYBIN, *BINDING sites, *SEQUENCE alignment, *DRUG abuse, *NEURALGIA

Abstract

[Display omitted] G protein-coupled receptor 3 (GPR3) is an orphan receptor potentially involved in many important physiological processes such as drug abuse, neuropathic pain, and anxiety and depression related disorders. Pharmacological studies of GPR3 have been limited due to the restricted number of known agonists and inverse agonists for this constitutively active receptor. In this medicinal chemistry study, we report the discovery of GPR3 agonists based off the diphenyleneiodonium (DPI) scaffold. The most potent full agonist was the 3-trifluoromethoxy analog (32) with an EC 50 of 260 nM and 90% efficacy compared to DPI. Investigation of a homology model of GPR3 from multiple sequence alignment resulted in the finding of a binding site rich in potential π-π and π-cation interactions stabilizing DPI-scaffold agonists. MMGBSA free energy analysis showed a good correlation with trends in observed EC 50 s. DPI analogs retained the same high receptor selectivity for GPR3 over GPR6 and GPR12 as observed with DPI. Collectively, the DPI analog series shows that order of magnitude improvements in potency with the scaffold were attainable; however, attempts to replace the iodonium ion to make the scaffold more druggable failed. [ABSTRACT FROM AUTHOR]

Published

2023

6. Towards a better understanding of the cannabinoid-related orphan receptors GPR3, GPR6, and GPR12.

Author

Morales, Paula, Isawi, Israa, and Reggio, Patricia H.

Subjects

*CANNABINOID receptors, *G protein coupled receptors, *ADENYLATE cyclase, *GENE expression, *PARKINSON'S disease

Abstract

GPR3, GPR6, and GPR12 are three orphan receptors that belong to the Class A family of G-protein-coupled receptors (GPCRs). These GPCRs share over 60% of sequence similarity among them. Because of their close phylogenetic relationship, GPR3, GPR6, and GPR12 share a high percentage of homology with other lipid receptors such as the lysophospholipid and the cannabinoid receptors. On the basis of sequence similarities at key structural motifs, these orphan receptors have been related to the cannabinoid family. However, further experimental data are required to confirm this association. GPR3, GPR6, and GPR12 are predominantly expressed in mammalian brain. Their high constitutive activation of adenylyl cyclase triggers increases in cAMP levels similar in amplitude to fully activated GPCRs. This feature defines their physiological role under certain pathological conditions. In this review, we aim to summarize the knowledge attained so far on the understanding of these receptors. Expression patterns, pharmacology, physiopathological relevance, and molecules targeting GPR3, GPR6, and GPR12 will be analyzed herein. Interestingly, certain cannabinoid ligands have been reported to modulate these orphan receptors. The current debate about sphingolipids as putative endogenous ligands will also be addressed. A special focus will be on their potential role in the brain, particularly under neurological conditions such as Parkinson or Alzheimer’s disease. Reported physiological roles outside the central nervous system will also be covered. This critical overview may contribute to a further comprehension of the physiopathological role of these orphan GPCRs, hopefully attracting more research towards a future therapeutic exploitation of these promising targets. [ABSTRACT FROM AUTHOR]

Published

2018

7. The switch from cAMP-independent to cAMP-dependent arrest of meiotic prophase is associated with coordinated GPR3 and CDK1 expression in mouse oocytes.

Author

Firmani, Laura D., Uliasz, Tracy F., and Mehlmann, Lisa M.

Subjects

*CYCLIC adenylic acid, *MEIOSIS, *CYCLIN-dependent kinases, *PROTEIN expression, *G protein coupled receptors, *OVULATION

Abstract

Mammalian oocytes are arrested in meiotic prophase from around the time of birth until just before ovulation. Following an extended period of growth, they are stimulated to mature to the metaphase II stage by a preovulatory luteinizing hormone (LH) surge that occurs with each reproductive cycle. Small, growing oocytes are not competent to mature into fertilizable eggs because they do not possess adequate amounts of cell cycle regulatory proteins, particularly cyclin-dependent kinase 1 (CDK1). As oocytes grow, they synthesize CDK1 and acquire the ability to mature. After oocytes achieve meiotic competence, meiotic arrest at the prophase stage is dependent on high levels of cAMP that are generated in the oocyte under the control of the constitutively active G s -coupled receptor, GPR3. In this study, we examined the switch between GPR3-independent and GPR3-dependent meiotic arrest. We found that the ability of oocytes to mature, as well as oocyte CDK1 levels, were dependent on follicle size, but CDK1 expression in oocytes from preantral follicles was not acutely altered by the activity of follicle stimulating hormone (FSH). Gpr3 was expressed and active in incompetent oocytes within early stage follicles, well before cAMP is required to maintain meiotic arrest. Oocytes from Gpr3 -/- mice were less competent to mature than oocytes from Gpr3 +/+ mice, as assessed by the time course of germinal vesicle breakdown. Correspondingly, Gpr3 -/- oocytes contained significantly lower CDK1 levels than their Gpr3 +/+ counterparts that were at the same stage of follicle development. These results demonstrate that GPR3 potentiates meiotic competence, most likely by raising cAMP. [ABSTRACT FROM AUTHOR]

Published

2018

8. Developmental expression of GPR3 in rodent cerebellar granule neurons is associated with cell survival and protects neurons from various apoptotic stimuli

Author

Shigeru Tanaka, Tatsuhiro Miyagi, Eisuke Dohi, Takahiro Seki, Izumi Hide, Yusuke Sotomaru, Yoshinaga Saeki, E. Antonio Chiocca, Masayasu Matsumoto, and Norio Sakai

Subjects

GPR3, Brain ischemia, Cerebellar granular neurons, Neuronal protection, cAMP, Apoptosis, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

G-protein coupled receptor 3 (GPR3), GPR6, and GPR12 belong to a family of constitutively active Gs-coupled receptors that activate 3′-5′-cyclic adenosine monophosphate (cAMP) and are highly expressed in the brain. Among these receptors, the endogenous expression of GPR3 in cerebellar granule neurons (CGNs) is increased following development. GPR3 is important for neurite outgrowth and neural maturation; however, the physiological functions of GPR3 remain to be fully elucidated. Here, we investigated the survival and antiapoptotic functions of GPR3 under normal and apoptosis-inducing culture conditions. Under normal culture conditions, CGNs from GPR3-knockout mice demonstrated lower survival than did CGNs from wild-type or GPR3-heterozygous mice. Cerebellar sections from GPR3−/− mice at P7, P14, and P21 revealed more caspase-3-positive neurons in the internal granular layer than in cerebellar sections from wild-type mice. Conversely, in a potassium-deprivation model of apoptosis, increased expression of these three receptors promoted neuronal survival. The antiapoptotic effect of GPR3 was also observed under hypoxic (1% O2/5% CO2) and reactive oxygen species (ROS)-induced apoptotic conditions. We further investigated the signaling pathways involved in the GPR3-mediated antiapoptotic effect. The addition of the PKA inhibitor KT5720, the MAP kinase inhibitor U0126, and the PI3 kinase inhibitor LY294002 abrogated the GPR3-mediated antiapoptotic effect in a potassium-deprivation model of apoptosis, whereas the PKC inhibitor Gö6976 did not affect the antiapoptotic function of GPR3. Furthermore, downregulation of endogenous GPR3 expression in CGNs resulted in a marked reduction in the basal levels of ERK and Akt phosphorylation under normal culture conditions. Finally, we used a transient middle cerebral artery occlusion (tMCAO) model in wild-type and GPR3-knockout mice to determine whether GPR3 expression modulates neuronal survival after brain ischemia. After tMCAO, GPR3-knockout mice exhibited a significantly larger infarct area than did wild-type mice. Collectively, these in vitro and in vivo results suggest that the developmental expression of constitutively active Gs-coupled GPR3 activates the ERK and Akt signaling pathways at the basal level, thereby protecting neurons from apoptosis that is induced by various stimuli.

Published

2014

9. Amino acids differ in their capacity to stimulate GLP-1 release from the perfused rat small intestine and stimulate secretion by different sensing mechanisms

Author

Mette M. Rosenkilde, Stella Feng Sheng Xu, Sara L. Jepsen, Cathrine Ørskov, Rune E. Kuhre, Thue W. Schwartz, Ida M. Modvig, Maja S. Engelstoft, Jens J. Holst, and Kristoffer L. Egerod

Subjects

Male, 0301 basic medicine, medicine.medical_specialty, Physiology, Endocrinology, Diabetes and Metabolism, Mice, Transgenic, 030209 endocrinology & metabolism, GPR3, Rat Small Intestine, Receptors, G-Protein-Coupled, Mice, 03 medical and health sciences, 0302 clinical medicine, Glucagon-Like Peptide 1, Physiology (medical), Internal medicine, Intestine, Small, medicine, Animals, Secretion, Amino Acids, Rats, Wistar, Receptors, Lysophosphatidic Acid, chemistry.chemical_classification, Secretory Pathway, Chemistry, Glucagon-like peptide-1, Small intestine, Rats, Amino acid, Mice, Inbred C57BL, Perfusion, 030104 developmental biology, Endocrinology, medicine.anatomical_structure, Signal Transduction

Abstract

The aim of this study was to explore individual amino acid-stimulated GLP-1 responses and the underlying stimulatory mechanisms, as well as to identify the amino acid-sensing-receptors involved in amino acid-stimulated GLP-1 release. Experiments were primarily based on isolated perfused rat small intestines, which have intact epithelial polarization allowing discrimination between luminal and basolateral mechanisms as well as quantitative studies of intestinal absorption and hormone secretion. Expression analysis of amino acid sensors on isolated murine GLP-1 secreting L-cells was assessed by qPCR. We found that L-valine powerfully stimulated GLP-1 secretion but only from the luminal side (2.9-fold increase). When administered from the vascular side, L-arginine and the aromatic amino acids stimulated GLP-1 secretion equally (2.6-2.9 fold increases). Expression analysis revealed that Casr expression was enriched in murine GLP-1 secreting L-cells, whereas Gpr35, Gprc6a, Gpr142, Gpr93 (Lpar5) and the umami taste receptor subunits Tas1r3 and Tas1r1 were not. Consistently, activation of GPR35, GPR93, GPR142 and the umami taste receptor with specific agonists or allosteric modulators did not increase GLP-1 secretion (P>0.05 for all experiments), whereas vascular inhibition of CaSR reduced GLP-1 secretion in response to luminal infusion of mixed amino acids. In conclusion, amino acids differ in their capacity to stimulate GLP-1 secretion. Some amino acids stimulated secretion only from the intestinal lumen, while other amino acids exclusively stimulated secretion from the vascular side, indicating that amino acid-stimulated GLP-1 secretion involves both apical and basolateral (post-absorptive) sensing mechanisms. Sensing of absorbed amino acids involves CaSR activation as vascular inhibition of CaSR markedly diminished amino acid stimulated GLP-1 release.

Published

2021

10. GPR3 and GPR6, novel molecular targets for cannabidiol.

Author

Laun, Alyssa S. and Song, Zhao-Hui

Subjects

*G protein coupled receptors, *MOLECULAR biology, *ALZHEIMER'S disease, *CANNABINOID receptors, *ARRESTINS

Abstract

GPR3 and GPR6 are members of a family of constitutively active, Gs protein-coupled receptors. Previously, it has been reported that GPR3 is involved in Alzheimer's disease whereas GPR6 plays potential roles in Parkinson's disease. GPR3 and GPR6 are considered orphan receptors because there are no confirmed endogenous agonists for them. However, GPR3 and GPR6 are phylogenetically related to the cannabinoid receptors. In this study, the activities of endocannabinoids and phytocannabinoids were tested on GPR3 and GPR6 using a β-arrestin2 recruitment assay. Among the variety of cannabinoids tested, cannabidiol (CBD), the major non-psychoactive component of marijuana, significantly reduced β-arrestin2 recruitment to both GPR3 and GPR6. In addition, the inhibitory effects of CBD on β-arrestin2 recruitment were concentration-dependent for both GPR3 and GPR6, with a higher potency for GPR6. These data show that CBD acts as an inverse agonist at both GPR3 and GPR6 receptors. These results demonstrate for the first time that both GPR3 and GPR6 are novel molecular targets for CBD. Our discovery that CBD acts as a novel inverse agonist on both GPR3 and GPR6 indicates that some of the potential therapeutic effects of CBD (e.g. treatment of Alzheimer's disease and Parkinson's disease) may be mediated through these important receptors. [ABSTRACT FROM AUTHOR]

Published

2017

11. GPR3 sets brown fat on fire

Author

Miroslav Balaz and Christian Wolfrum

Subjects

Norepinephrine, Physiology, Brown Adipocytes, Chemistry, medicine, Lipolysis, GPR3, Cell Biology, Receptor, Molecular Biology, Thermogenesis, Cell biology, medicine.drug

Abstract

Activation of thermogenic adipocytes, a process canonically driven by norepinephrine through β-adrenergic receptors, presents an appealing therapeutic approach to combat obesity. Recent work by Sveidahl Johansen et al., 2021 published in Cell has identified a noncanonical mechanism of brown adipocyte activation, in which lipolysis transcriptionally drives the constitutive activation of the Gs protein-coupled receptor, GPR3, to induce thermogenesis.

Published

2021

12. Development of a High-Throughput Screening-Compatible Assay for Discovery of GPR3 Inverse Agonists Using a cAMP Biosensor

Author

Tomomi Kinoshita, Hiroyuki Ogasawara, Chie Suzuki, Gentaroh Suzuki, Kumiko Ayukawa, and Masahiro Furuno

Subjects

endocrine system, Drug Inverse Agonism, Repressor, GPR3, Endogeny, Biosensing Techniques, Computational biology, Ligands, 01 natural sciences, Biochemistry, Receptors, G-Protein-Coupled, Analytical Chemistry, 03 medical and health sciences, Alzheimer Disease, Cyclic AMP, Humans, Inverse agonist, Receptor, 030304 developmental biology, G protein-coupled receptor, 0303 health sciences, Chemistry, HEK 293 cells, High-Throughput Screening Assays, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Cell culture, Molecular Medicine, Protein Binding, Biotechnology

Abstract

While G-protein-coupled receptors (GPCRs) represent the largest class of cell surface proteins, there are ≥100 orphan GPCRs whose endogenous ligands are unknown. Accordingly, these could prove to be potential therapeutic targets for the pharmaceutical intervention of various diseases. Constitutively active orphan GPCRs are activated without ligands; thus, inverse agonists may be very useful pharmacological tools for inhibiting constitutive activity. However, in general, inverse agonist screening is considered more difficult to perform with high quality than antagonist screening, particularly due to the narrow assay window. We developed a high-throughput screening (HTS)-compatible assay to identify inverse agonists of GPR3. GPR3 is expressed in the central nervous system (CNS) and is known to be related to Alzheimer's disease and other CNS diseases. The GPR3 inducible cell line was established using T-REx 293 cells that stably expressed the tetracycline repressor protein, and the cAMP biosensor, GloSensor, was stably co-expressed. After optimization of the induction level of GPR3 and assay conditions, the GloSensor assay showed an approximately 20-fold signal-to-background ratio and high sensitivity. Using the HTS method, we successfully screened a library of hundreds of thousands of compounds for the inhibition of constitutive activity with good quality and excellent reproducibility. Finally, 35 compounds were identified as GPR3 selective inverse agonists. This inverse agonist screening approach using GloSensor in combination with the inducible expression of orphan GPCR indicates universal applicability to the search for inverse agonists of constitutively active orphan GPCRs.

Published

2020

13. GPR3, GPR6, and GPR12 as novel molecular targets: their biological functions and interaction with cannabidiol

Author

Laun, Alyssa S., Shrader, Sarah H., Brown, Kevin J., and Song, Zhao-Hui

Published

2019

14. Silencing the G-protein coupled receptor 3-salt inducible kinase 2 pathway promotes human β cell proliferation

Author

Robert A. Screaton, Tatsuya Kin, Jillian L Rourke, Jun-Ichi Sakamaki, Emily Moon, Caterina Iorio, Queenie Hu, and Lisa Wells

Subjects

0301 basic medicine, endocrine system, QH301-705.5, Medicine (miscellaneous), GPR3, Protein Serine-Threonine Kinases, Article, General Biochemistry, Genetics and Molecular Biology, Receptors, G-Protein-Coupled, Cell-cycle exit, Mice, 03 medical and health sciences, 0302 clinical medicine, Cell quiescence, RNA interference, Insulin-Secreting Cells, Animals, Humans, Gene silencing, Biology (General), Receptor, Cell Proliferation, Cell growth, Chemistry, Cell cycle, Cell biology, Type 1 diabetes, 030104 developmental biology, Stem cell, General Agricultural and Biological Sciences, 030217 neurology & neurosurgery, Signal Transduction

Abstract

Loss of pancreatic β cells is the hallmark of type 1 diabetes, for which provision of insulin is the standard of care. While regenerative and stem cell therapies hold the promise of generating single-source or host-matched tissue to obviate immune-mediated complications, these will still require surgical intervention and immunosuppression. Here we report the development of a high-throughput RNAi screening approach to identify upstream pathways that regulate adult human β cell quiescence and demonstrate in a screen of the GPCRome that silencing G-protein coupled receptor 3 (GPR3) leads to human pancreatic β cell proliferation. Loss of GPR3 leads to activation of Salt Inducible Kinase 2 (SIK2), which is necessary and sufficient to drive cell cycle entry, increase β cell mass, and enhance insulin secretion in mice. Taken together, our data show that targeting the GPR3-SIK2 pathway is a potential strategy to stimulate the regeneration of β cells., Caterina Iorio et al. use a high-throughput RNAi screen to identify the GPR3-SIK2-CDKN1B axis as key players involved in regulating pancreatic beta cell proliferation. These results suggest that GPR3 and SIK2 are both potential targets to stimulate regeneration of beta cells in diseases like type 1 diabetes.

Published

2021

15. GPR3 expression in retinal ganglion cells contributes to neuron survival and accelerates axonal regeneration after optic nerve crush in mice.

Author

Masuda, Shun, Tanaka, Shigeru, Shiraki, Hiroko, Sotomaru, Yusuke, Harada, Kana, Hide, Izumi, Kiuchi, Yoshiaki, and Sakai, Norio

Subjects

*NERVOUS system regeneration, *RETINAL ganglion cells, *OPTIC nerve injuries, *RETINAL injuries, *OPTIC nerve, *GLAUCOMA, *G protein coupled receptors

Abstract

Glaucoma is an optic neuropathy and is currently one of the most common diseases that leads to irreversible blindness. The axonal degeneration that occurs before retinal ganglion neuronal loss is suggested to be involved in the pathogenesis of glaucoma. G protein-coupled receptor 3 (GPR3) belongs to the class A rhodopsin-type GPCR family and is highly expressed in various neurons. GPR3 is unique in its ability to constitutively activate the Gαs protein without a ligand, which elevates the basal intracellular cAMP level. Our earlier reports suggested that GPR3 enhances both neurite outgrowth and neuronal survival. However, the potential role of GPR3 in axonal regeneration after neuronal injury has not been elucidated. Herein, we investigated retinal GPR3 expression and its possible involvement in axonal regeneration after retinal injury in mice. GPR3 was relatively highly expressed in retinal ganglion cells (RGCs). Surprisingly, RGCs in GPR3 knockout mice were vulnerable to neural death during aging without affecting high intraocular pressure (IOP) and under ischemic conditions. Primary cultured neurons from the retina showed that GPR3 expression was correlated with neurite outgrowth and neuronal survival. Evaluation of the effect of GPR3 on axonal regeneration using GPR3 knockout mice revealed that GPR3 in RGCs participates in axonal regeneration after optic nerve crush (ONC) under zymosan stimulation. In addition, regenerating axons were further stimulated when GPR3 was upregulated in RGCs, and the effect was further augmented when combined with zymosan treatment. These results suggest that GPR3 expression in RGCs helps maintain neuronal survival and accelerates axonal regeneration after ONC in mice. • GPR3 was relatively highly expressed in RGCs. • GPR3 expression in RGCs had a neuroprotective effect against aging and retinal ischemia. • GPR3 expression in primary cultured RGCs have potential for neurite outgrowth and neuronal survival. • GPR3 expression in RGCs augmented axonal regeneration after optic nerve crush under zymosan stimulation. [ABSTRACT FROM AUTHOR]

Published

2022

16. Lipolysis drives expression of the constitutively active receptor GPR3 to induce adipose thermogenesis

Author

Seth McGonigle, Susanne Mandrup, Olivia Sveidahl Johansen, Laia Reverte-Salisa, Rudolf Zechner, Lasse K. Markussen, Thomas Nielsen, Eline N. Kuipers, Andreas Kjaer, Maria Razzoli, Alexander Pfeifer, Jakob Bondo Hansen, Cheryl Cero, Alessandro Bartolomucci, James G. Granneman, Brice Emanuelli, Raymond E. Soccio, Morten Lundh, Thue Walter Schwartz, Søren Nielsen, Wenfei Sun, Dan Ploug Christensen, Hua Dong, Christa Broholm, Thorsten Gnad, Nienke Willemsen, Camilla Scheele, William Orchard, Oksana Dmytriyeva, Iuliia Karavaeva, Patrick C.N. Rensen, Marie S. Isidor, Sander Kooijman, Niels Grarup, Mikkel Frost, Cecilie Mørch Hallgren, Davide Calebiro, Tao Ma, Naja Z. Jespersen, M. Madan Babu, Mikael Rydén, Shannon L. O'Brien, Carsten H. Nielsen, Renate Schreiber, Zachary Gerhart-Hines, Jacob B. Hansen, Jonas T. Treebak, Yachen Shen, Torben Hansen, Oluf Pedersen, and Elahu G. Sustarsic

Subjects

endocrine system, Sympathetic Nervous System, Transcription, Genetic, Adrenergic receptor, Lipolysis, Adipose tissue, GPR3, Biology, Article, General Biochemistry, Genetics and Molecular Biology, Receptors, G-Protein-Coupled, 03 medical and health sciences, 0302 clinical medicine, GPCR, Adipose Tissue, Brown, constitutively active, Chlorocebus aethiops, Brown adipose tissue, energy expenditure, Adipocytes, medicine, Animals, Humans, G protein-coupled receptor, Receptor, Cells, Cultured, Constitutive Androstane Receptor, 030304 developmental biology, adrenergic receptor, 0303 health sciences, Thermogenesis, brown adipose tissue, thermogenesis, Dietary Fats, Cell biology, Cold Temperature, Mice, Inbred C57BL, Phenotype, medicine.anatomical_structure, COS Cells, lipolysis, transcription, 030217 neurology & neurosurgery, Signal Transduction

Abstract

Thermogenic adipocytes possess a therapeutically appealing, energy-expending capacity, which is canonically cold-induced by ligand-dependent activation of β-adrenergic G protein-coupled receptors (GPCRs). Here, we uncover an alternate paradigm of GPCR-mediated adipose thermogenesis through the constitutively active receptor, GPR3. We show that the N terminus of GPR3 confers intrinsic signaling activity, resulting in continuous Gs-coupling and cAMP production without an exogenous ligand. Thus, transcriptional induction of Gpr3 represents the regulatory parallel to ligand-binding of conventional GPCRs. Consequently, increasing Gpr3 expression in thermogenic adipocytes is alone sufficient to drive energy expenditure and counteract metabolic disease in mice. Gpr3 transcription is cold-stimulated by a lipolytic signal, and dietary fat potentiates GPR3-dependent thermogenesis to amplify the response to caloric excess. Moreover, we find GPR3 to be an essential, adrenergic-independent regulator of human brown adipocytes. Taken together, our findings reveal a noncanonical mechanism of GPCR control and thermogenic activation through the lipolysis-induced expression of constitutively active GPR3., Cell, 184 (13), ISSN:0092-8674, ISSN:1097-4172

Published

2021

17. Author response for 'Cellular distribution of cannabinoid‐related receptors TRPV1, PPAR‐gamma, GPR55 and GPR3 in the equine cervical dorsal root ganglia'

Author

Fiorella Giancola, Giorgia Galiazzo, Angelo Peli, Margherita De Silva, Roberto Chiocchetti, and Riccardo Rinnovati

Subjects

chemistry.chemical_classification, Dorsum, medicine.medical_treatment, TRPV1, Peroxisome proliferator-activated receptor, GPR3, Biology, Cell biology, chemistry, GPR55, Cellular distribution, medicine, Cannabinoid, Receptor

Published

2021

18. Effects of aging on gene expression and mitochondrial DNA in the equine oocyte and follicle cells.

Author

Campos-Chillon, Fernando, Farmerie, Todd A., Bouma, Gerrit J., Clay, Colin M., and Carnevale, Elaine M.

Subjects

*MARES, *MESSENGER RNA, *GRANULOSA cells, *PHOSPHODIESTERASES, *G protein coupled receptors, *GENE expression in mammals, *OVUM, *MITOCHONDRIAL DNA, *REPRODUCTION, *MAMMALS

Abstract

We hypothesised that advanced mare age is associated with follicle and oocyte gene alterations. The aims of the study were to examine quantitative and temporal differences in mRNA for LH receptor (LHR), amphiregulin (AREG) and epiregulin (EREG) in granulosa cells, phosphodiesterase (PDE) 4D in cumulus cells and PDE3A, G-protein-coupled receptor 3 (GPR3), growth differentiation factor 9 (GDF9), bone morphogenetic protein 15 (BMP15) and mitochondrial (mt) DNA in oocytes. Samples were collected from dominant follicles of Young (3-12 years) and Old (≥20 years) mares at 0, 6, 9 and 12 h after administration of equine recombinant LH. LHR mRNA declined after 0 h in Young mares, with no time effect in Old mares. For both ages, gene expression of AREG was elevated at 6 and 9 h and EREG was expression was elevated at 9 h, with higher expression in Old than Young mares. Cumulus cell PDE4D expression increased by 6 h (Old) and 12 h (Young). Oocyte GPR3 expression peaked at 9 and 12 h in Young and Old mares, respectively. Expression of PDE3A increased at 6 h, with the increase greater in oocytes from Old than Young mares at 6 and 9 h. Mean GDF9 and BMP15 transcripts were higher in Young than Old, with a peak at 6 h. Copy numbers of mtDNA did not vary over time in oocytes from Young mares, but a temporal decrease was observed in oocytes from Old mares. The results support an age-associated asynchrony in the expression of genes that are essential for follicular and oocyte maturation before ovulation. Maternal aging is related to reduced fertility in various species, including the mare. We compared gene expression in follicle cells and oocytes from Young and Old mares after an ovulation-induction signal. Differences were observed in the timing and amount of expression for key regulatory genes between Young and Old mares, suggesting age-associated changes in follicles and oocytes that could impact fertility. [ABSTRACT FROM AUTHOR]

Published

2015

19. Characterization of Four Orphan Receptors (GPR3, GPR6, GPR12 and GPR12L) in Chickens and Ducks and Regulation of GPR12 Expression in Ovarian Granulosa Cells by Progesterone

Author

Juan Li, Yan Huang, Zheng Zhang, Zejiao Li, Yajun Wang, Jiannan Zhang, Baolong Cao, and Biying Jiang

Subjects

0301 basic medicine, endocrine system, lcsh:QH426-470, GPR3, Ovary, Stimulation, progesterone, Article, Receptors, G-Protein-Coupled, Avian Proteins, 03 medical and health sciences, 0302 clinical medicine, Downregulation and upregulation, Species Specificity, Genetics, medicine, ducks, Animals, Tissue Distribution, Cloning, Molecular, Receptor, Zebrafish, Genetics (clinical), Reporter gene, Granulosa Cells, biology, Sequence Analysis, RNA, Gene Expression Profiling, GPR6, GPR12L, biology.organism_classification, Cell biology, lcsh:Genetics, 030104 developmental biology, medicine.anatomical_structure, Gene Expression Regulation, chickens, Female, ovary, GPR12, 030217 neurology & neurosurgery

Abstract

The three structurally related orphan G protein-coupled receptors, GRP3, GPR6, and GPR12, are reported to be constitutively active and likely involved in the regulation of many physiological/pathological processes, such as neuronal outgrowth and oocyte meiotic arrest in mammals. However, the information regarding these orphan receptors in nonmammalian vertebrates is extremely limited. Here, we reported the structure, constitutive activity, and tissue expression of these receptors in two representative avian models: chickens and ducks. The cloned duck GPR3 and duck/chicken GPR6 and GPR12 are intron-less and encode receptors that show high amino acid (a.a.) sequence identities (66–88%) with their respective mammalian orthologs. Interestingly, a novel GPR12-like receptor (named GPR12L) sharing 66% a.a. identity to that in vertebrates was reported in the present study. Using dual-luciferase reporter assay and Western blot, we demonstrated that GPR3, GPR6, GPR12, and GPR12L are constitutively active and capable of stimulating the cAMP/PKA signaling pathway without ligand stimulation in birds (and zebrafish), indicating their conserved signaling property across vertebrates. RNA-seq data/qRT-PCR assays revealed that GPR6 and GPR12L expression is mainly restricted to the chicken brain, while GPR12 is highly expressed in chicken ovarian granulosa cells (GCs) and oocytes of 6 mm growing follicles and its expression in cultured GCs is upregulated by progesterone. Taken together, our data reveal the structure, function, and expression of GPR3, GPR6, GPR12, and GPR12L in birds, thus providing the first piece of evidence that GPR12 expression is upregulated by gonadal steroid (i.e., progesterone) in vertebrates.

Published

2021

20. Review for 'Cellular distribution of cannabinoid‐related receptors TRPV1, PPAR‐gamma, GPR55 and GPR3 in the equine cervical dorsal root ganglia'

Author

V. L. H. Roberts

Subjects

chemistry.chemical_classification, Dorsum, medicine.medical_treatment, TRPV1, Peroxisome proliferator-activated receptor, GPR3, Biology, Cell biology, chemistry, GPR55, Cellular distribution, medicine, Cannabinoid, Receptor

Published

2021

21. Refolding and characterization of two G protein-coupled receptors purified from E. coli inclusion bodies

Author

Marcus D. Hartmann, Hans Kiefer, René Handrick, and Bastian Heim

Subjects

0301 basic medicine, Surfactants, Cell Membranes, medicine.disease_cause, Biochemistry, Inclusion bodies, Protein Refolding, Receptors, G-Protein-Coupled, 0302 clinical medicine, Chemical Precipitation, Receptor, Materials, Thermostability, Orphan receptor, Inclusion Bodies, Multidisciplinary, Crystallography, Chemistry, Physics, Escherichia coli Proteins, Monomers, Chemical Reactions, Condensed Matter Physics, Lipids, Physical Sciences, Medicine, Cellular Structures and Organelles, Crystallization, Diffraction, Research Article, Signal Transduction, Transmembrane Receptors, Science, Materials Science, Detergents, GPR3, Crystals, 03 medical and health sciences, medicine, Escherichia coli, Solid State Physics, Sphingosine-1-Phosphate Receptors, G protein-coupled receptor, Biology and Life Sciences, Proteins, Membrane Proteins, Cell Biology, Polymer Chemistry, 030104 developmental biology, Membrane protein, Waves, G Protein Coupled Receptors, 030217 neurology & neurosurgery

Abstract

Aiming at streamlining GPCR production from E. coli inclusion bodies for structural analysis, we present a generic approach to assess and optimize refolding yield through thermostability analysis. Since commonly used hydrophobic dyes cannot be applied as probes for membrane protein unfolding, we adapted a technique based on reacting cysteins exposed upon thermal denaturation with fluorescent 7-Diethylamino-3-(4-maleimidophenyl)-4-methylcoumarin (CPM). Successful expression, purification and refolding is shown for two G protein-coupled receptors (GPCR), the sphingosine-1-phosphate receptor S1P1, and the orphan receptor GPR3. Refolded receptors were subjected to lipidic cubic phase crystallization screening.

Published

2021

22. Studies of involvement of G-protein coupled receptor-3 in cannabidiol effects on inflammatory responses of mouse primary astrocytes and microglia

Author

Hui Shao, Nu Chen, Zhao-Hui Song, Yongqing Liu, Henry J. Kaplan, Grzegorz Godlewski, Sarah H. Shrader, and Jun Wu

Subjects

Lipopolysaccharides, Central Nervous System, Macroglial Cells, Physiology, Anti-Inflammatory Agents, Biochemistry, Nervous System, Immune Receptors, Receptors, G-Protein-Coupled, Mice, Cell Signaling, Animal Cells, Immune Physiology, Medicine and Health Sciences, Cannabidiol, Post-Translational Modification, Phosphorylation, Toll-like Receptors, Cells, Cultured, Innate Immune System, Multidisciplinary, Immune System Proteins, Microglia, Chemistry, Animal Models, Cell biology, medicine.anatomical_structure, surgical procedures, operative, Experimental Organism Systems, Cytokines, Medicine, Signal transduction, Inflammation Mediators, Cellular Types, Anatomy, medicine.drug, Signal Transduction, Research Article, Signal Inhibition, Science, Central nervous system, Primary Cell Culture, Immunology, GPR3, Glial Cells, Mouse Models, Research and Analysis Methods, Neuroprotection, digestive system, Model Organisms, medicine, Animals, Humans, Microglial Cells, Neuroinflammation, Inflammation, Biology and Life Sciences, Proteins, Cell Biology, Molecular Development, digestive system diseases, Disease Models, Animal, Astrocytes, Immune System, TLR4, Animal Studies, Developmental Biology

Abstract

Cannabidiol (CBD) exhibits anti-inflammatory and neuroprotective properties and is suggested to be effective in the pre-clinical and clinical treatment of illnesses of the central nervous system (CNS). Two major types of CNS glial cells, astrocytes and microglia, play critical roles in the development and pathogenesis of CNS diseases. However, the mechanisms by which CBD plays an anti-inflammatory and neuroprotective role for these glial cells have not been fully elucidated. In this study, we examined the effects of CBD on the inflammatory response of mouse primary astrocytes and microglia. We also investigated whether the effect of CBD on cytokine release is mediated by the G protein coupled receptor 3 (GPR3), which was recently identified as a novel receptor for CBD. Our results showed that CBD inhibited inflammatory responses of astrocytes and microglia stimulated with lipopolysaccharide (LPS), a Toll-like receptor 4 (TLR4) ligand in vitro and in vivo. In addition, CBD reduced the phosphorylation of STAT3 and NF-κB signaling pathways in LPS-stimulated astrocytes. However, the inhibitory effect of CBD on pro-inflammatory cytokine production was independent of GPR3 expression in both types of glial cells. Thus, although CBD is effective in ameliorating the activation of astrocytes and microglia, its mechanism of action still requires further study. Our data support the concept that CBD may have therapeutic potential for neurological disorders that involve neuroinflammation.

Published

2021

23. Detouring adrenergic stimulation to induce adipose thermogenesis

Author

Christopher Auger and Shingo Kajimura

Subjects

endocrine system, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, Adipose tissue, Article, Adrenergic Agents, GPCR, Endocrinology, Adipose Tissue, Brown, Adrenergic stimulation, constitutively active, Internal medicine, energy expenditure, medicine, Humans, G protein-coupled receptor, Receptor, adrenergic receptor, GPR3, business.industry, Thermogenesis, brown adipose tissue, Receptor signaling, lipolysis, transcription, business

Abstract

Summary Thermogenic adipocytes possess a therapeutically appealing, energy-expending capacity, which is canonically cold-induced by ligand-dependent activation of β-adrenergic G protein-coupled receptors (GPCRs). Here, we uncover an alternate paradigm of GPCR-mediated adipose thermogenesis through the constitutively active receptor, GPR3. We show that the N terminus of GPR3 confers intrinsic signaling activity, resulting in continuous Gs-coupling and cAMP production without an exogenous ligand. Thus, transcriptional induction of Gpr3 represents the regulatory parallel to ligand-binding of conventional GPCRs. Consequently, increasing Gpr3 expression in thermogenic adipocytes is alone sufficient to drive energy expenditure and counteract metabolic disease in mice. Gpr3 transcription is cold-stimulated by a lipolytic signal, and dietary fat potentiates GPR3-dependent thermogenesis to amplify the response to caloric excess. Moreover, we find GPR3 to be an essential, adrenergic-independent regulator of human brown adipocytes. Taken together, our findings reveal a noncanonical mechanism of GPCR control and thermogenic activation through the lipolysis-induced expression of constitutively active GPR3., Graphical abstract, Highlights • Gpr3 is a cold-induced Gs-coupled receptor in brown and beige adipose tissue • A noncanonical lipolytic signal triggers Gpr3 transcription during cold exposure • GPR3 is a nonadrenergic activator of mouse and human thermogenic adipocytes • GPR3 drives thermogenesis without a ligand via its intrinsic Gs-coupling activity, Cold-induced lipolysis drives the expression of a constitutively active GPCR that regulates thermogenesis in mouse and human adipocytes independent of sympathetic or adrenergic inputs.

Published

2021

24. The identification of GPR3 inverse agonist AF64394; The first small molecule inhibitor of GPR3 receptor function.

Author

Jensen, Thomas, Elster, Lisbeth, Nielsen, Søren Møller, Poda, Suresh Babu, Loechel, Frosty, Volbracht, Christiane, Klewe, Ib Vestergaard, David, Laurent, and Watson, Stephen P.

Subjects

*G protein coupled receptors, *STRUCTURE-activity relationship in pharmacology, *SMALL molecules, *CHEMICAL synthesis, *PHARMACEUTICAL chemistry, *BIOORGANIC chemistry

Abstract

The identification of the novel and selective GPR3 inverse agonist AF64394 , the first small molecule inhibitor of GPR3 receptor function, is described. Structure activity relationships and syntheses based around AF64394 are reported. [ABSTRACT FROM AUTHOR]

Published

2014

25. Developmental expression of GPR3 in rodent cerebellar granule neurons is associated with cell survival and protects neurons from various apoptotic stimuli.

Author

Tanaka, Shigeru, Miyagi, Tatsuhiro, Dohi, Eisuke, Seki, Takahiro, Hide, Izumi, Sotomaru, Yusuke, Saeki, Yoshinaga, Antonio Chiocca, E., Matsumoto, Masayasu, and Sakai, Norio

Subjects

*NEURONS, *GENE expression, *G protein coupled receptors, *CEREBELLAR cortex, *APOPTOSIS, *NEURAL stimulation

Abstract

Abstract: G-protein coupled receptor 3 (GPR3), GPR6, and GPR12 belong to a family of constitutively active Gs-coupled receptors that activate 3′-5′-cyclic adenosine monophosphate (cAMP) and are highly expressed in the brain. Among these receptors, the endogenous expression of GPR3 in cerebellar granule neurons (CGNs) is increased following development. GPR3 is important for neurite outgrowth and neural maturation; however, the physiological functions of GPR3 remain to be fully elucidated. Here, we investigated the survival and antiapoptotic functions of GPR3 under normal and apoptosis-inducing culture conditions. Under normal culture conditions, CGNs from GPR3-knockout mice demonstrated lower survival than did CGNs from wild-type or GPR3-heterozygous mice. Cerebellar sections from GPR3−/− mice at P7, P14, and P21 revealed more caspase-3-positive neurons in the internal granular layer than in cerebellar sections from wild-type mice. Conversely, in a potassium-deprivation model of apoptosis, increased expression of these three receptors promoted neuronal survival. The antiapoptotic effect of GPR3 was also observed under hypoxic (1% O2/5% CO2) and reactive oxygen species (ROS)-induced apoptotic conditions. We further investigated the signaling pathways involved in the GPR3-mediated antiapoptotic effect. The addition of the PKA inhibitor KT5720, the MAP kinase inhibitor U0126, and the PI3 kinase inhibitor LY294002 abrogated the GPR3-mediated antiapoptotic effect in a potassium-deprivation model of apoptosis, whereas the PKC inhibitor Gö6976 did not affect the antiapoptotic function of GPR3. Furthermore, downregulation of endogenous GPR3 expression in CGNs resulted in a marked reduction in the basal levels of ERK and Akt phosphorylation under normal culture conditions. Finally, we used a transient middle cerebral artery occlusion (tMCAO) model in wild-type and GPR3-knockout mice to determine whether GPR3 expression modulates neuronal survival after brain ischemia. After tMCAO, GPR3-knockout mice exhibited a significantly larger infarct area than did wild-type mice. Collectively, these in vitro and in vivo results suggest that the developmental expression of constitutively active Gs-coupled GPR3 activates the ERK and Akt signaling pathways at the basal level, thereby protecting neurons from apoptosis that is induced by various stimuli. [Copyright &y& Elsevier]

Published

2014

26. Expression, purification, refolding and structure analysis of stabilized G protein-coupled receptors expressed in E. coli inclusion bodies

Author

Heim, Bastian, Weil, Tanja, and Kiefer, Hans

Subjects

GPR3, Detergent, E. coli, Lipid, G-Protein gekoppelter Rezeptor, Synchrotron, X-ray, S1P1, GPCR, DDC 570 / Life sciences, LCP, ddc:570, Escherichia coli, Crystallization

Abstract

G protein–coupled receptors are membrane proteins involved in signal transduction across the biological lipid bilayer. This receptor class represent both the largest membrane protein and drug target family, accounting for ~800 members encoded in the human genome. GPCRs are distributed across nearly all of the body’s organs and tissues, which makes them a key regulatory element in a broad range of normal and pathological processes. The structure determination of G protein-coupled receptors with high-resolution crystals is a key focus in membrane protein biology to understand the basic mechanism of their activation and signaling for structure-based drug design. High-resolution crystal structures in combination with multiple complex structures for a specific target are a prerequisite for a successful structure-based drug discovery. Currently, obtaining X-ray structures of membrane proteins is still far from becoming routine due to their notorious instability in detergent micelles, the inherent conformational flexibility, bottlenecks in overexpressing large quantities of the recombinant receptor and the hydrophobic protein surface, which often impairs crystallization. In the present project, we overexpressed two G protein-coupled receptors in Escherichia coli inclusion bodies. One of these two receptors is the sphingosine-1-phosphate receptor 1 with known structure, which was used for validation purposes. The second receptor was the orphan G protein-coupled receptor 3 with unknown structure. Both receptors were refolded in vitro by detergent exchange into detergent micelles. The monomeric form of the refolded receptors was isolated by size exclusion chromatography and quality checked using a thermal stability assay. Receptor stability was optimized for higher thermal stability through improving refolding conditions into mixed lipid detergent micelles. Ligand binding was shown for both receptors, which were crystallized in the lipidic cubic phase. Beside crystal formation for both receptors in different crystallization conditions, the reproduction of sphingosine-1-phosphate receptor 1 crystallization conditions resulted in crystal formation. Harvested crystals were analyzed at a synchrotron beamline, which resulted in non-diffracting potential protein crystals for both receptors.

Published

2020

27. Orphan G protein-coupled receptors: The role in CNS disorders

Author

Hassan Azhdari-Zarmehri, Mohaddeseh Sadat Alavi, Ali Roohbakhsh, and Ali Shamsizadeh

Subjects

0301 basic medicine, Pharmacology, Mental Disorders, GPR3, General Medicine, Disease, Biology, Receptors, G-Protein-Coupled, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, GPR55, Central Nervous System Diseases, GPR50, GPR6, Animals, Humans, Psychopharmacology, Receptor, Neuroscience, 030217 neurology & neurosurgery, Central Nervous System Agents, Signal Transduction, G protein-coupled receptor

Abstract

There are various types of receptors in the central nervous system (CNS). G protein-coupled receptors (GPCRs) have the highest expression with a wide range of physiological functions. A newer sub group of these receptors namely orphan GPCRs have been discovered. GPR3, GPR6, GPR17, GPR26, GPR37, GPR39, GPR40, GPR50, GPR52, GPR54, GPR55, GPR85, GPR88, GPR103, and GPR139 are the selected orphan GPCRs for this article. Their roles in the central nervous system have not been understood well so far. However, recent studies show that they may have very important functions in the CNS. Hence, in the present study, we reviewed most recent findings regarding the physiological roles of the selected orphan GPCRs in the CNS. After a brief presentation of each receptor, considering the results from genetic and pharmacological manipulation of the receptors, their roles in the pathophysiology of different diseases and disorders including anxiety, depression, schizophrenia, epilepsy, Alzheimer's disease, Parkinson's disease, and substance abuse will be discussed. At present, our knowledge regarding the role of GPCRs in the brain is very limited. However, previous limited studies show that orphan GPCRs have an important place in psychopharmacology and these receptors are potential new targets for the treatment of major CNS diseases.

Published

2018

28. Towards a better understanding of the cannabinoid-related orphan receptors GPR3, GPR6, and GPR12

Author

Paula Morales, Israa H. Isawi, and Patricia H. Reggio

Subjects

0301 basic medicine, endocrine system, Cannabinoid receptor, medicine.medical_treatment, GPR3, Biology, Article, Receptors, G-Protein-Coupled, Adenylyl cyclase, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, chemistry, GPR6, medicine, Animals, Humans, lipids (amino acids, peptides, and proteins), Pharmacology (medical), Cannabinoid, General Pharmacology, Toxicology and Pharmaceutics, Receptor, Structural motif, Neuroscience, G protein-coupled receptor

Abstract

GPR3, GPR6, and GPR12 are three orphan receptors that belong to the Class A family of G-protein-coupled receptors (GPCRs). These GPCRs share over 60% of sequence similarity among them. Because of their close phylogenetic relationship, GPR3, GPR6, and GPR12 share a high percentage of homology with other lipid receptors such as the lysophospholipid and the cannabinoid receptors. On the basis of sequence similarities at key structural motifs, these orphan receptors have been related to the cannabinoid family. However, further experimental data are required to confirm this association. GPR3, GPR6, and GPR12 are predominantly expressed in mammalian brain. Their high constitutive activation of adenylyl cyclase triggers increases in cAMP levels similar in amplitude to fully activated GPCRs. This feature defines their physiological role under certain pathological conditions. In this review, we aim to summarize the knowledge attained so far on the understanding of these receptors. Expression patterns, pharmacology, physiopathological relevance, and molecules targeting GPR3, GPR6, and GPR12 will be analyzed herein. Interestingly, certain cannabinoid ligands have been reported to modulate these orphan receptors. The current debate about sphingolipids as putative endogenous ligands will also be addressed. A special focus will be on their potential role in the brain, particularly under neurological conditions such as Parkinson or Alzheimer's disease. Reported physiological roles outside the central nervous system will also be covered. This critical overview may contribute to a further comprehension of the physiopathological role of these orphan GPCRs, hopefully attracting more research towards a future therapeutic exploitation of these promising targets.

Published

2018

29. Signaling and functions of G-protein-coupled receptor 3 in cerebellar granular neurons

Author

Shigeru Tanaka

Subjects

Neurons, Pharmacology, endocrine system, Cerebellum, Gs alpha subunit, Neurite, Chemistry, GPR3, Receptors, G-Protein-Coupled, Cell biology, medicine.anatomical_structure, Downregulation and upregulation, Cyclic AMP, Neurites, medicine, Signal transduction, Receptor, Signal Transduction, G protein-coupled receptor

Abstract

G-protein-coupled receptor 3 (GPR3) is a member of the class A rhodopsin-type GPCR family and is highly expressed in various neurons. A unique feature of GPR3 is its ability to constitutively activate the Gαs protein without the addition of ligands, which results in the elevation of the basal level of intracellular cAMP. During the development of the cerebellum, GPR3 expression is upregulated in cerebellar granular neurons (CGNs) and maintained thereafter. In our previous studies, we showed that the intrinsic expression of GPR3 in CGNs is highly associated with neurite outgrowth, neurite differentiation, and neuronal survival. Recently, we have focused on the possible signaling pathways associated with GPR3-mediated neurite outgrowth in CGNs. Interestingly, GPR3-mediated neurite outgrowth is mediated by not only PKA-dependent signaling pathways but also PI3K-mediated signaling pathways. Moreover, the Gβγ-mediated signaling pathway is involved in GPR3-mediated neurite outgrowth. These results suggested that neural expression of GPR3 stimulates multiple downstream signaling pathways, contributing to the maintenance of homeostasis in neurons. Further precise analyses of constitutively active GPCRs may help in unveiling novel neuronal functions.

Published

2018

30. Keeping warm one cell at a time

Author

Stella M. Hurtley

Subjects

endocrine system, Multidisciplinary, Chemistry, Receptor expression, Cell, Adipose tissue, Stimulation, GPR3, Dietary excess, Cell biology, medicine.anatomical_structure, medicine, Receptor, Thermogenesis

Abstract

Cell Biology Adipose thermogenesis is a conserved response to environmental cold or dietary excess and is classically triggered by ligand-dependent receptor activation. Johansen et al. report that cold regulation of Gs-coupled receptor expression represents a parallel point of control. Gpr3 turns out to be the most cold-induced Gs-coupled receptor in both brown and beige thermogenic adipose tissues. GPR3 has high basal Gs-coupled activity in the absence of an exogenous ligand. Mimicking the cold induction of Gpr3 triggered cAMP production, activated the thermogenic response, and counteracted metabolic disease in mice. A disease-associated genetic variant in GPR3 in patient-derived adipocytes revealed that GPR3 also acts as a regulator of human thermogenic adipose tissue. Targeting GPR3 could thus enable therapeutic stimulation of thermogenic adipose tissue in metabolic disease. Cell 184 , 3502 (2021).

Published

2021

31. GPR3 accelerates neurite outgrowth and neuronal polarity formation via PI3 kinase-mediating signaling pathway in cultured primary neurons.

Author

Tanaka, Shigeru, Shimada, Naoto, Shiraki, Hiroko, Miyagi, Tatsuhiro, Harada, Kana, Hide, Izumi, and Sakai, Norio

Subjects

*EXTRACELLULAR signal-regulated kinases, *NEUROTROPHIN receptors, *PROTEIN kinase B, *CELLULAR signal transduction, *G protein coupled receptors, *NEURONS, *DENDRITES, *THREONINE, *PROTEIN kinases

Abstract

During neuronal development, immature neurons extend neurites and subsequently polarize to form an axon and dendrites. We have previously reported that G protein-coupled receptor 3 (GPR3) levels increase during neuronal development, and that GPR3 has functions in neurite outgrowth and neuronal differentiation in cerebellar granular neurons. Moreover, GPR3 is transported and concentrated at the tips of neurite, thereby contributing to the local activation of protein kinase A (PKA). However, the signaling pathways for GPR3-mediated neurite outgrowth and its subsequent effects on neuronal polarization have not yet been elucidated. We therefore analyzed the signaling pathways related to GPR3-mediated neurite outgrowth, and also focused on the possible roles of GPR3 in axon polarization. We demonstrated that, in cerebellar granular neurons, GPR3-mediated neurite outgrowth was mediated by multiple signaling pathways, including those of PKA, extracellular signal-regulated kinases (ERKs), and most strongly phosphatidylinositol 3-kinase (PI3K). In addition, the GPR3-mediated activation of neurite outgrowth was associated with G protein-coupled receptor kinase 2 (GRK2)-mediated signaling and phosphorylation of the C-terminus serine/threonine residues of GPR3, which affected downstream protein kinase B (Akt) signaling. We further demonstrated that GPR3 was transiently increased early in the development of rodent hippocampal neurons. It was subsequently concentrated at the tip of the longest neurite, and was thus associated with accelerated polarity formation in a PI3K-dependent manner in rat hippocampal neurons. In addition, GPR3 knockout in mouse hippocampal neurons led to delayed neuronal polarity formation, thereby affecting the dephosphorylation of collapsing response mediator protein 2 (CRMP2), which is downstream of the PI3K signaling pathway. Taken together, these findings suggest that the intrinsic expression of GPR3 in differentiated neurons constitutively activates PI3K-mediated signaling pathway predominantly, thus accelerating neurite outgrowth and further augmenting polarity formation in primary cultured neurons. • GPR3 accelerates neurite outgrowth via PI3 kinase-mediating signaling pathway in cerebellar granular neurons. • GPR3-mediated activation of neurite outgrowth is associated with GRK2-mediated signaling and Akt phosphorylation. • GPR3 is enriched in the longest tips of neurites during differentiation of rat hippocampal neurons. • GPR3 accelerates neuronal polarization in a PI3K-dependent manner in rodent hippocampal neurons. [ABSTRACT FROM AUTHOR]

Published

2022

32. Molecular modeling and molecular dynamics simulation-based structural analysis of GPR3

Author

Kaushik, Aman Chandra and Sahi, Shakti

Published

2017

33. A role for GPRx, a novel GPR3/6/12-related G-protein coupled receptor, in the maintenance of meiotic arrest in Xenopus laevis oocytes

Author

Ríos-Cardona, Diana, Ricardo-González, Roberto R., Chawla, Ajay, and Ferrell, James E.

Subjects

*XENOPUS laevis, *PROGESTERONE, *GENETIC transcription, *MESSENGER RNA

Abstract

Abstract: Progesterone-induced Xenopus laevis oocyte maturation is mediated via a plasma membrane-bound receptor and does not require gene transcription. Evidence from several species suggests that the relevant progesterone receptor is a G-protein coupled receptor (GPCR) and that a second receptor–GPR3 and/or GPR12 in mammals–tonically opposes the progesterone receptor. We have cloned a novel X. laevis GPCR, GPRx, which may play a similar role to GPR3/GPR12 in amphibians and fishes. GPRx is related to but distinct from GPR3, GPR6, and GPR12; GPRx orthologs are present in Xenopus tropicalis and Danio rerio, but apparently not in birds or mammals. X. laevis GPRx is mainly expressed in brain, ovary, and testis. The GPRx mRNA increases during oogenesis, persists during oocyte maturation and early embryogenesis, and then falls after the midblastula transition. Microinjection of GPRx mRNA increases the concentration of cAMP in oocytes and causes the oocytes to fail to respond to progesterone, and this block is reversed by co-injecting GPRx with morpholino oligonucleotides. Morpholino injections did not cause spontaneous maturation of oocytes, but did accelerate progesterone-induced maturation. Thus, GPRx contributes to the maintenance of G2-arrest in immature X. laevis oocytes. [Copyright &y& Elsevier]

Published

2008

34. Oocyte-specific expression of Gpr3 is required for the maintenance of meiotic arrest in mouse oocytes

Author

Mehlmann, Lisa M.

Subjects

*KARYOKINESIS, *MEIOSIS, *INTERFERON inducers, *RNA, *NUCLEIC acids

Abstract

Abstract: The maintenance of meiotic prophase arrest in mouse oocytes within fully grown follicles, prior to the surge of luteinizing hormone (LH) that triggers meiotic resumption, depends on a high level of cAMP within the oocyte. cAMP is produced within the oocyte, at least in large part, by the Gs-linked G-protein-coupled receptor, GPR3. Gpr3 is localized in the mouse oocyte but is also present throughout the follicle. To investigate whether Gpr3 in the follicle cells contributes to the maintenance of meiotic arrest, RNA interference (RNAi) was used to reduce the amount of Gpr3 RNA within follicle-enclosed oocytes. Follicle-enclosed oocytes injected with small interfering double-stranded RNA (siRNA) targeting Gpr3, but not control siRNAs, stimulated the resumption of meiosis in the majority of oocytes following a 3-day culture period. Reduction of RNA was specific for Gpr3 because an unrelated gene was not reduced by microinjection of siRNA. Meiotic resumption was stimulated in isolated oocytes injected with the same siRNA and cultured for 1 to 2 days, but at a much lower rate than in follicle-enclosed oocytes that could be cultured for longer. These results demonstrate that GPR3 specifically in the oocyte, rather than in the follicle cells, is responsible for maintenance of meiotic arrest in mouse oocytes. Furthermore, the method developed here for specifically reducing RNA in follicle-enclosed oocytes, which can be cultured for a sufficient time to reduce the level of endogenous protein, should be generally useful for targeting a wide range of other proteins that may be involved in meiotic arrest, the resumption of meiosis, fertilization, or early embryonic development. [Copyright &y& Elsevier]

Published

2005

35. Simula??o computacional das intera??es moleculares entre GPR3 e agonistas inversos

Author

Russo, Silvana da Cunha and Palmini, Andr? Luiz Fernandes

Subjects

GPR3, Neuroinflama??o, Canabidiol, Neuroinflammation, Doen?a de Alzheimer, MEDICINA [CIENCIAS DA SAUDE], Neurodegenera??o, Alzheimer?s Disease, Cannabidiol, Receptores Ligados a Prote?na G, Neurodegeneration, G Protein Coupled Receptors

Abstract

As doen?as neurodegenerativas s?o causas importantes de morbidade e mortalidade, principalmente entre a popula??o idosa. Elas representam um grupo grande de doen?as neurol?gicas, com padr?es cl?nicos variados (ZUCCHELLA et al., 2018). Os tratamentos existentes apenas oferecem melhora sintom?tica, mas n?o curam a doen?a (GAUTHIER et al., 2018). V?rios alvos terap?uticos s?o propostos na investiga??o e tratamento das doen?as neurodegenerativas. Entre o grande n?mero de alvos moleculares, os Receptores Ligados a Prote?na G (GPCR) comp?e um grupo de mol?culas muito estudado pela ind?stria farmac?utica e, atualmente, respons?vel pelo maior n?mero de f?rmacos aprovados dispon?veis no mercado (HUANG et al., 2017). Recentemente, o receptor ?rf?o GPR3, que ? um membro da fam?lia GPCR, por?m, do qual ainda n?o se descobriu o ligante end?geno, tem recebido aten??o nas pesquisas em Doen?a de Alzheimer (LAUN et al., 2018). Hoje se sabe que est? expresso em grande quantidade no Sistema Nervoso Central (SNC), e a sua rela??o com doen?as neurodegenerativas come?ou a ser evidenciada em pesquisas usando modelos de Doen?a de Alzheimer (THATHIAH et al., 2009). Estudos recentes desvendaram f?rmacos ligantes de GPR3 (JENSEN et al., 2014, LAUN; SONG, 2017). A investiga??o das intera??es moleculares de GPR3 com seus ligantes rec?m-descobertos poderia ajudar no desenvolvimento de novos f?rmacos para o tratamento das doen?as neurodegenerativas. A dificuldade na pesquisa dessas intera??es se relaciona a falta de uma estrutura tridimensional obtida por cristalografia de raios x de GPR3, fato que pretenderemos contornar usando simula??es computacionais. Os m?todos computacionais s?o consagrados na pesquisa e desenvolvimento de f?rmacos porque trazem agilidade ? pesquisa aliada a baixo custo. Neurodegenerative diseases are considered a burden to the ageing population. They represent a number of different pathologies which have different symptoms. (ZUCCHELLA et al., 2018). Until now, there was no viable treatment, just ways to alleviate the symptoms. (GAUTHIER et al., 2018). In the research of neurodegenerative diseases, several molecular targets are proposed. Among them, the G Protein Coupled Receptors (GPCR) group has been widely studied by the pharmaceutical industry, with a significant number of drugs approved to treat human diseases (HUANG et al., 2017). Recently, the orphan receptor GPR3, from the GPCR family, for which no endogenous ligand has yet been found, has been researched in Alzheimer?s Disease (LAUN et al., 2018). It is expressed broadly in the Central Nervous System, and its relation to neurodegenerative disease has been brought to light in Alzheimer?s Disease model research (THATHIAH et al., 2009). Some studies had now discovered a few ligands to GPR3 (JENSEN et al., 2014, LAUN; SONG, 2017). The investigation of GPR3 molecular interactions with its newly found ligands could help in the development of new drugs to treat neurodegenerative diseases. The main challenge in this investigation is the lack of available 3D structure for GPR3, which we intend to address using computational simulations. Computational methods bring agility and affordability to drug development.

Published

2019

36. Potential role of inducible GPR3 expression under stimulated T cell conditions.

Author

Shiraki H, Tanaka S, Guo Y, Harada K, Hide I, Yasuda T, and Sakai N

Subjects

Animals, Cell Line, Chromogranins metabolism, Cyclic AMP metabolism, GTP-Binding Protein alpha Subunits, Gs metabolism, Gene Expression, Mice, Knockout, Nuclear Receptor Subfamily 4, Group A, Member 2 genetics, Nuclear Receptor Subfamily 4, Group A, Member 2 metabolism, Receptors, G-Protein-Coupled genetics, Receptors, G-Protein-Coupled metabolism, T-Lymphocytes metabolism, Mice, Lymphocyte Activation genetics, Receptors, G-Protein-Coupled physiology, T-Lymphocytes immunology

Abstract

G protein-coupled receptor 3 (GPR3) constitutively activates Gαs proteins without any ligands and is predominantly expressed in neurons. Since the expression and physiological role of GPR3 in immune cells is still unknown, we examined the possible role of GPR3 in T lymphocytes. The expression of GPR3 was upregulated 2 h after phorbol 12-myristate 13-acetate (PMA)/ionomycin stimulation and was sustained in Jurkat cells, a human T lymphocyte cell line. In addition, the expression of nuclear receptor 4 group A member 2 (NR4A2) was highly modulated by GPR3 expression. Additionally, GPR3 expression was linked with the transcriptional promoter activity of NR4A in Jurkat cells. In mouse CD4 + T cells, transient GPR3 expression was induced immediately after the antigen receptor stimulation. However, the expression of NR4A2 was not modulated in CD4 + T cells from GPR3-knockout mice after stimulation, and the population of Treg cells in thymocytes and splenocytes was not affected by GPR3 knockout. By contrast, spontaneous effector activation in both CD4 + T cells and CD8 + T cells was observed in GPR3-knockout mice. In summary, GPR3 is immediately induced by T cell stimulation and play an important role in the suppression of effector T cell activation., Competing Interests: Declaration of competing interest The authors declare no conflicts of interest., (Copyright © 2022 The Authors. Production and hosting by Elsevier B.V. All rights reserved.)

Published

2022

37. Structural basis for the binding of a selective inverse agonist AF64394 with the human G-protein coupled receptor 3 (GPR3).

Author

Bharathi and Roy KK

Subjects

Humans, Ligands, Molecular Dynamics Simulation, Nitrogen, Triazoles, Drug Inverse Agonism, Receptors, G-Protein-Coupled agonists, Receptors, G-Protein-Coupled chemistry

Abstract

The orphan class A G-protein coupled receptor 3 (GPR3) is highly expressed in brain and linked with various neuronal functions, and therefore, expected to play a vital role in the progression of Alzheimer's disease. In view of the lack of its experimental structure, we describe herein the three-dimensional structure and conformational dynamics of GPR3 complexed with the inverse agonist AF64394. The GPR3 model was predicted using the Iterative Threading ASSEmbly Refinement (I-TASSER) method. The Induced Fit Docking predicted two unique poses, Pose 1 and Pose 2, for AF64394, and then, molecular dynamics (MD) simulations followed by binding free-energy calculation revealed the Pose 1 as a very stable pose with the least fluctuation during the MD simulation while the Pose 2 underwent a significant fluctuation. The [1,2,4]triazolo[1,5-a]pyrimidine core was engaged in multiple hydrogen bonds (H-bonds), such as a water-mediated H-bond between the triazole nitrogen and T31, two direct H-bonds between the protonated triazole-ring nitrogen and V186 and T279, a direct H-bond between the secondary amine and V187. The phenyl substituent of AF64394 exhibited aromatic π-π stacking interactions with F97, F101, W43 and Y280. AF64394 showed a direct interaction with E28 and polar interactions with H96, T31 and T279. Throughout the MD simulation, the toggle switch residues, F120 and W260, remained in close contact, indicating that the GPR3 conformation represented an inactive state. The 4-(3-chloro-5-isopropoxyphenethyl) group resided near to the toggle switch residues. The insights gained here are expected to be useful in the structure-based design of new ligands targeting GPR3 modulation. Communicated by Ramaswamy H. Sarma.

Published

2022

38. Orphan G Protein Coupled Receptors in Affective Disorders

Author

Lyndsay R. Watkins and Cesare Orlandi

Subjects

Central Nervous System, 0301 basic medicine, orphan GPCR (oGPCR), lcsh:QH426-470, G protein, GPR3, Review, Anxiety, Biology, Ligands, Receptors, G-Protein-Coupled, 03 medical and health sciences, 0302 clinical medicine, anxiety disorders, Genetics, GPR62, medicine, Humans, Genetic Predisposition to Disease, G protein coupled receptor (GPCR), Genetics (clinical), G protein-coupled receptor, antidepressant, bipolar disorder (BPD), major depressive disorder (MDD), medicine.disease, mood disorders, animal models, Antidepressive Agents, lcsh:Genetics, 030104 developmental biology, GPR56, Mood disorders, GPR50, Autopsy, Signal transduction, Transcriptome, Neuroscience, 030217 neurology & neurosurgery, Genome-Wide Association Study, Signal Transduction, G proteins

Abstract

G protein coupled receptors (GPCRs) are the main mediators of signal transduction in the central nervous system. Therefore, it is not surprising that many GPCRs have long been investigated for their role in the development of anxiety and mood disorders, as well as in the mechanism of action of antidepressant therapies. Importantly, the endogenous ligands for a large group of GPCRs have not yet been identified and are therefore known as orphan GPCRs (oGPCRs). Nonetheless, growing evidence from animal studies, together with genome wide association studies (GWAS) and post-mortem transcriptomic analysis in patients, pointed at many oGPCRs as potential pharmacological targets. Among these discoveries, we summarize in this review how emotional behaviors are modulated by the following oGPCRs: ADGRB2 (BAI2), ADGRG1 (GPR56), GPR3, GPR26, GPR37, GPR50, GPR52, GPR61, GPR62, GPR88, GPR135, GPR158, and GPRC5B.

Published

2020

39. A study of GPR3, GPR6, of GPR12 as novel molecular targets for cannabidiol

Author

Alyssa S. Laun

Subjects

endocrine system, Cannabinoid receptor, G protein, medicine.medical_treatment, GPR3, Biology, GPR6, medicine, Inverse agonist, Cannabinoid, Receptor, Neuroscience, Cannabidiol, medicine.drug

Abstract

The G protein-coupled receptors 3, 6, and 12 (GPR3, GPR6, and GPR12) comprise a family of closely related orphan receptors with no confirmed endogenous ligands. These receptors are constitutively active, capable of signaling through G protein and non-G protein mediated mechanisms. These orphan receptors have previously been reported to play important roles in many normal physiological functions and to be involved in a variety of pathological conditions. Although they are orphans, GPR3, GPR6, and GPR12 are phylogenetically most closely related to the cannabinoid receptors. Using β-arrestin2 recruitment and cAMP accumulation assays, we have recently found that the non-psychoactive phytocannabinoid cannabidiol (CBD) is an inverse agonist for GPR3, GPR6, and GPR12. This discovery highlights these orphan receptors as potential new molecular targets for CBD, provides novel mechanisms of action, and suggests new therapeutic uses of CBD for illnesses such as Alzheimer’s disease, Parkinson’s disease, cancer, and infertility. Furthermore, identification of CBD as a new inverse agonist for GPR3, GPR6, and GPR12 provides the initial chemical scaffolds upon which potent and efficacious agents acting on these receptors can be developed, with the goal of developing chemical tools for studying these orphan receptors and ultimately new therapeutic agents.

Published

2018

40. GPR3, GPR6, and GPR12 as novel molecular targets: their biological functions and interaction with cannabidiol

Author

Alyssa S. Laun, Sarah H. Shrader, Kevin J. Brown, and Zhao-Hui Song

Subjects

0301 basic medicine, endocrine system, Cannabinoid receptor, Drug Inverse Agonism, Endogeny, GPR3, Review Article, Biology, Ligands, Receptors, G-Protein-Coupled, 03 medical and health sciences, 0302 clinical medicine, medicine, Inverse agonist, Animals, Cannabidiol, Humans, Pharmacology (medical), Receptor, Pharmacology, Neurons, General Medicine, 030104 developmental biology, GPR6, 030220 oncology & carcinogenesis, Neuroscience, medicine.drug, Signal Transduction

Abstract

The G protein-coupled receptors 3, 6, and 12 (GPR3, GPR6, and GPR12) comprise a family of closely related orphan receptors with no confirmed endogenous ligands. These receptors are constitutively active and capable of signaling through G protein-mediated and non-G protein-mediated mechanisms. These orphan receptors have previously been reported to play important roles in many normal physiological functions and to be involved in a variety of pathological conditions. Although they are orphans, GPR3, GPR6, and GPR12 are phylogenetically most closely related to the cannabinoid receptors. Using β-arrestin2 recruitment and cAMP accumulation assays, we recently found that the nonpsychoactive phytocannabinoid cannabidiol (CBD) is an inverse agonist for GPR3, GPR6, and GPR12. This discovery highlights these orphan receptors as potential new molecular targets for CBD, provides novel mechanisms of action, and suggests new therapeutic uses of CBD for illnesses such as Alzheimer’s disease, Parkinson’s disease, cancer, and infertility. Furthermore, identification of CBD as a new inverse agonist for GPR3, GPR6, and GPR12 provides the initial chemical scaffolds upon which potent and efficacious agents acting on these receptors can be developed, with the goal of developing chemical tools for studying these orphan receptors and ultimately new therapeutic agents.

Published

2018

41. Lipolysis drives expression of the constitutively active receptor GPR3 to induce adipose thermogenesis.

Author

Sveidahl Johansen, Olivia, Ma, Tao, Hansen, Jakob Bondo, Markussen, Lasse Kruse, Schreiber, Renate, Reverte-Salisa, Laia, Dong, Hua, Christensen, Dan Ploug, Sun, Wenfei, Gnad, Thorsten, Karavaeva, Iuliia, Nielsen, Thomas Svava, Kooijman, Sander, Cero, Cheryl, Dmytriyeva, Oksana, Shen, Yachen, Razzoli, Maria, O'Brien, Shannon L., Kuipers, Eline N., and Nielsen, Carsten Haagen

Subjects

*LIPOLYSIS, *BROWN adipose tissue, *BODY temperature regulation, *FAT cells, *ADRENERGIC receptors

Abstract

Thermogenic adipocytes possess a therapeutically appealing, energy-expending capacity, which is canonically cold-induced by ligand-dependent activation of β-adrenergic G protein-coupled receptors (GPCRs). Here, we uncover an alternate paradigm of GPCR-mediated adipose thermogenesis through the constitutively active receptor, GPR3. We show that the N terminus of GPR3 confers intrinsic signaling activity, resulting in continuous Gs-coupling and cAMP production without an exogenous ligand. Thus, transcriptional induction of Gpr3 represents the regulatory parallel to ligand-binding of conventional GPCRs. Consequently, increasing Gpr3 expression in thermogenic adipocytes is alone sufficient to drive energy expenditure and counteract metabolic disease in mice. Gpr3 transcription is cold-stimulated by a lipolytic signal, and dietary fat potentiates GPR3-dependent thermogenesis to amplify the response to caloric excess. Moreover, we find GPR3 to be an essential, adrenergic-independent regulator of human brown adipocytes. Taken together, our findings reveal a noncanonical mechanism of GPCR control and thermogenic activation through the lipolysis-induced expression of constitutively active GPR3. [Display omitted] • Gpr3 is a cold-induced Gs-coupled receptor in brown and beige adipose tissue • A noncanonical lipolytic signal triggers Gpr3 transcription during cold exposure • GPR3 is a nonadrenergic activator of mouse and human thermogenic adipocytes • GPR3 drives thermogenesis without a ligand via its intrinsic Gs-coupling activity Cold-induced lipolysis drives the expression of a constitutively active GPCR that regulates thermogenesis in mouse and human adipocytes independent of sympathetic or adrenergic inputs. [ABSTRACT FROM AUTHOR]

Published

2021

42. Characterization of Four Orphan Receptors (GPR3, GPR6, GPR12 and GPR12L) in Chickens and Ducks and Regulation of GPR12 Expression in Ovarian Granulosa Cells by Progesterone.

Author

Li, Zejiao, Jiang, Biying, Cao, Baolong, Zhang, Zheng, Zhang, Jiannan, Li, Juan, Huang, Yan, and Wang, Yajun

Subjects

*GRANULOSA cells, *ORPHANS, *PROGESTERONE, *PROGESTERONE receptors, *G protein coupled receptors, *DUCKS, *CHICKENS

Abstract

The three structurally related orphan G protein-coupled receptors, GRP3, GPR6, and GPR12, are reported to be constitutively active and likely involved in the regulation of many physiological/pathological processes, such as neuronal outgrowth and oocyte meiotic arrest in mammals. However, the information regarding these orphan receptors in nonmammalian vertebrates is extremely limited. Here, we reported the structure, constitutive activity, and tissue expression of these receptors in two representative avian models: chickens and ducks. The cloned duck GPR3 and duck/chicken GPR6 and GPR12 are intron-less and encode receptors that show high amino acid (a.a.) sequence identities (66–88%) with their respective mammalian orthologs. Interestingly, a novel GPR12-like receptor (named GPR12L) sharing 66% a.a. identity to that in vertebrates was reported in the present study. Using dual-luciferase reporter assay and Western blot, we demonstrated that GPR3, GPR6, GPR12, and GPR12L are constitutively active and capable of stimulating the cAMP/PKA signaling pathway without ligand stimulation in birds (and zebrafish), indicating their conserved signaling property across vertebrates. RNA-seq data/qRT-PCR assays revealed that GPR6 and GPR12L expression is mainly restricted to the chicken brain, while GPR12 is highly expressed in chicken ovarian granulosa cells (GCs) and oocytes of 6 mm growing follicles and its expression in cultured GCs is upregulated by progesterone. Taken together, our data reveal the structure, function, and expression of GPR3, GPR6, GPR12, and GPR12L in birds, thus providing the first piece of evidence that GPR12 expression is upregulated by gonadal steroid (i.e., progesterone) in vertebrates. [ABSTRACT FROM AUTHOR]

Published

2021

43. Detailed neuronal distribution of GPR3 and its co-expression with EF-hand calcium-binding proteins in the mouse central nervous system.

Author

Ikawa, Fumiaki, Tanaka, Shigeru, Harada, Kana, Hide, Izumi, Maruyama, Hirofumi, and Sakai, Norio

Subjects

*CENTRAL nervous system, *CALCIUM-binding proteins, *GABAERGIC neurons, *G protein coupled receptors, *CEREBRAL cortex

Abstract

• Fluorescence-based detection of GPR3 promoter activity allows GPR3 expression to be identified in detail in the mouse CNS. • GPR3 was expressed in both glutamatergic excitatory neurons and GABAergic inhibitory neurons. • GPR3 was expressed in areas related to olfactory, auditory, emotional, and motor functions. • GPR3-positive neurons often also expressed NECAB2 in various regions of the mouse CNS. The G-protein coupled receptor 3 (GPR3), a member of the class A rhodopsin-type GPR family, constitutively activates Gαs proteins without any ligands. Although there have been several reports concerning the functions of GPR3 in neurons, the physiological roles of GPR3 have not been fully elucidated. To address this issue, we analyzed GPR3 distribution in detail using fluorescence-based X-gal staining in heterozygous GPR3 knockout/ LacZ knock-in mice, and further investigated the types of GPR3-expressing neurons using fluorescent double labeling with various EF-hand Ca2+-binding proteins. In addition to the previously reported GPR3-expressing areas, we identified GPR3 expression in the basal ganglia and in many nuclei of the cranial nerves, in regions related to olfactory, auditory, emotional, and motor functions. In addition, GPR3 was not only observed in excitatory neurons in layer V of the cerebral cortex, the CA2 region of the hippocampus, and the lateral nucleus of the thalamus, but also in γ-aminobutyric acid (GABA)-ergic interneurons in the cortex, hippocampus, thalamus, striatum, and cerebellum. GPR3 was frequently co-expressed with neuronal Ca2+-binding protein 2 (NECAB2) in neurons in various regions of the central nervous system, especially in the hippocampal CA2, medial habenular nucleus, lateral thalamic nucleus, dorsolateral striatum, brainstem, and spinal cord anterior horn. Furthermore, GPR3 also co-localized with NECAB2 at the tips of neurites in differentiated PC12 cells. These results suggest that GPR3 and NECAB2 are highly co-expressed in specific neurons, and that GPR3 may modulate Ca2+ signaling by interacting with NECAB2 in specific areas of the central nervous system. [ABSTRACT FROM AUTHOR]

Published

2021

44. The switch from cAMP-independent to cAMP-dependent arrest of meiotic prophase is associated with coordinated GPR3 and CDK1 expression in mouse oocytes

Author

Tracy F. Uliasz, Lisa M. Mehlmann, and Laura D. Firmani

Subjects

0301 basic medicine, endocrine system, media_common.quotation_subject, GPR3, Biology, Second Messenger Systems, Receptors, G-Protein-Coupled, 03 medical and health sciences, Follicle, Mice, 0302 clinical medicine, Prophase, Meiosis, CDC2 Protein Kinase, medicine, Cyclic AMP, Animals, Meiotic Prophase I, Molecular Biology, Ovulation, media_common, Mice, Knockout, Cyclin-dependent kinase 1, 030219 obstetrics & reproductive medicine, Germinal vesicle, Cell Biology, Cell Cycle Checkpoints, Oocyte, Cell biology, 030104 developmental biology, medicine.anatomical_structure, Gene Expression Regulation, Oocytes, Female, Developmental Biology

Abstract

Mammalian oocytes are arrested in meiotic prophase from around the time of birth until just before ovulation. Following an extended period of growth, they are stimulated to mature to the metaphase II stage by a preovulatory luteinizing hormone (LH) surge that occurs with each reproductive cycle. Small, growing oocytes are not competent to mature into fertilizable eggs because they do not possess adequate amounts of cell cycle regulatory proteins, particularly cyclin-dependent kinase 1 (CDK1). As oocytes grow, they synthesize CDK1 and acquire the ability to mature. After oocytes achieve meiotic competence, meiotic arrest at the prophase stage is dependent on high levels of cAMP that are generated in the oocyte under the control of the constitutively active Gs-coupled receptor, GPR3. In this study, we examined the switch between GPR3-independent and GPR3-dependent meiotic arrest. We found that the ability of oocytes to mature, as well as oocyte CDK1 levels, were dependent on follicle size, but CDK1 expression in oocytes from preantral follicles was not acutely altered by the activity of follicle stimulating hormone (FSH). Gpr3 was expressed and active in incompetent oocytes within early stage follicles, well before cAMP is required to maintain meiotic arrest. Oocytes from Gpr3-/- mice were less competent to mature than oocytes from Gpr3+/+ mice, as assessed by the time course of germinal vesicle breakdown. Correspondingly, Gpr3-/- oocytes contained significantly lower CDK1 levels than their Gpr3+/+ counterparts that were at the same stage of follicle development. These results demonstrate that GPR3 potentiates meiotic competence, most likely by raising cAMP.

Published

2017

45. GPR3 and GPR6, novel molecular targets for cannabidiol

Author

Zhao-Hui Song and Alyssa S. Laun

Subjects

0301 basic medicine, endocrine system, Cannabinoid receptor, Drug Inverse Agonism, Biophysics, GPR3, Pharmacology, Biology, Biochemistry, Receptors, G-Protein-Coupled, 03 medical and health sciences, Structure-Activity Relationship, medicine, Inverse agonist, Cannabidiol, Humans, Receptor, Molecular Biology, Orphan receptor, Cell Biology, Endocannabinoid system, beta-Arrestin 2, 030104 developmental biology, GPR6, Cancer research, medicine.drug

Abstract

GPR3 and GPR6 are members of a family of constitutively active, Gs protein-coupled receptors. Previously, it has been reported that GPR3 is involved in Alzheimer's disease whereas GPR6 plays potential roles in Parkinson's disease. GPR3 and GPR6 are considered orphan receptors because there are no confirmed endogenous agonists for them. However, GPR3 and GPR6 are phylogenetically related to the cannabinoid receptors. In this study, the activities of endocannabinoids and phytocannabinoids were tested on GPR3 and GPR6 using a β-arrestin2 recruitment assay. Among the variety of cannabinoids tested, cannabidiol (CBD), the major non-psychoactive component of marijuana, significantly reduced β-arrestin2 recruitment to both GPR3 and GPR6. In addition, the inhibitory effects of CBD on β-arrestin2 recruitment were concentration-dependent for both GPR3 and GPR6, with a higher potency for GPR6. These data show that CBD acts as an inverse agonist at both GPR3 and GPR6 receptors. These results demonstrate for the first time that both GPR3 and GPR6 are novel molecular targets for CBD. Our discovery that CBD acts as a novel inverse agonist on both GPR3 and GPR6 indicates that some of the potential therapeutic effects of CBD (e.g. treatment of Alzheimer's disease and Parkinson's disease) may be mediated through these important receptors.

Published

2017

46. A New Understanding on the Regulation of Oocyte Meiotic Prophase Arrest and Resumption

Author

Meijia Zhang

Subjects

0301 basic medicine, endocrine system, 030219 obstetrics & reproductive medicine, media_common.quotation_subject, Phosphodiesterase, GPR3, Biology, Oocyte, NPR2, Cell biology, Adenylyl cyclase, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, chemistry, Follicular phase, medicine, Luteinizing hormone, Ovulation, media_common

Abstract

In mammals, oocyte maturation must be remained precisely in synchrony with ovulation for normal female fertility. Signals from ovarian somatic cells prevent precocious resumption of meiosis until a surge of luteinizing hormone (LH) from the pituitary stimulates oocyte maturation and ovulation. Natriuretic peptide type C (NPPC) produced by mural granulosa cells stimulates the generation of cyclic guanosine 3′,5′-monophosphate (cGMP) by natriuretic peptide receptor 2 (NPR2) of cumulus cells. The cGMP then diffuses into oocytes and arrests meiotic progression by inhibiting oocyte-specific phosphodiesterase 3A (PDE3A) activity and cyclic adenosine 3′,5′-monophosphate (cAMP) hydrolysis. Intraoocyte cAMP is produced by G-protein-coupled receptor GPR3/12 activation of adenylyl cyclase endogenous to the oocyte. Oocyte itself also promotes cumulus cell expression of NPR2 and inosine monophosphate dehydrogenase (IMPDH) to elevate cGMP levels for meiotic arrest. Follicle-stimulating hormone (FSH), through estradiol (E2), enhances NPPC/NPR2 expression to ensure meiotic arrest during antral follicular development. LH-induced epidermal growth factor (EGF)-like growth factors decrease NPPC content and NPR2 activity, resulting in cGMP decrease and meiotic resumption. A better understanding of these signaling networks on the regulation of oocyte meiotic progress will provide new opportunities for the manipulation of follicular functions for contraception or the treatment of infertility.

Published

2017

47. Role for endocytosis of a constitutively active GPCR (GPR185) in releasing vertebrate oocyte meiotic arrest

Author

Khaled Machaca, Rashmi P. Kulkarni, Maya Dib, Arwa Daalis, and Nancy Nader

Subjects

Endosome, media_common.quotation_subject, Blotting, Western, Green Fluorescent Proteins, GPR3, Xenopus Proteins, Biology, Endocytosis, Models, Biological, Receptors, G-Protein-Coupled, Xenopus laevis, Prophase, Meiosis, Cyclic AMP, medicine, Animals, Internalization, Molecular Biology, DNA Primers, media_common, G protein-coupled receptor, Cell Cycle Checkpoints, Cell Biology, Oocyte, Cell biology, Luminescent Proteins, medicine.anatomical_structure, Microscopy, Fluorescence, Oocytes, Developmental Biology

Abstract

Vertebrate oocytes are naturally arrested at prophase of meiosis I for sustained periods of time before resuming meiosis in a process called oocyte maturation that prepares the egg for fertilization. Members of the constitutively active GPR3/6/12 family of G-protein coupled receptors represent important mediators of meiotic arrest. In the frog oocyte the GPR3/12 homolog GPRx (renamed GPR185) has been shown to sustain meiotic arrest by increasing intracellular cAMP levels through GαSβγ. Here we show that GPRx is enriched at the cell membrane (~80%), recycles through an endosomal compartment at steady state, and loses its ability to signal once trapped intracellularly. Progesterone-mediated oocyte maturation is associated with significant internalization of both endogenous and overexpressed GPRx. Furthermore, a GPRx mutant that does not internalize in response to progesterone is significantly more efficient than wild-type GPRx at blocking oocyte maturation. Collectively our results argue that internalization of the constitutively active GPRx is important to release oocyte meiotic arrest.

Published

2014

48. Developmental expression of GPR3 in rodent cerebellar granule neurons is associated with cell survival and protects neurons from various apoptotic stimuli

Author

Masayasu Matsumoto, Yoshinaga Saeki, Tatsuhiro Miyagi, Takahiro Seki, E. Antonio Chiocca, Eisuke Dohi, Yusuke Sotomaru, Norio Sakai, Izumi Hide, and Shigeru Tanaka

Subjects

endocrine system, Cardiotonic Agents, Neurite, Cell Survival, MAP Kinase Signaling System, Cerebellar granular neurons, Apoptosis, Biology, Neuronal protection, lcsh:RC321-571, Receptors, G-Protein-Coupled, Brain ischemia, Mice, chemistry.chemical_compound, Ischemia, cAMP, Cerebellum, Animals, LY294002, Cyclic adenosine monophosphate, Enzyme Inhibitors, Rats, Wistar, Receptor, lcsh:Neurosciences. Biological psychiatry. Neuropsychiatry, Protein kinase B, GPR3, Mice, Knockout, Neurons, Colforsin, Age Factors, Gene Expression Regulation, Developmental, KT5720, Rats, Cell biology, Mice, Inbred C57BL, Disease Models, Animal, Neurology, chemistry, GPR6, Culture Media, Conditioned, Signal transduction, Signal Transduction

Abstract

G-protein coupled receptor 3 (GPR3), GPR6, and GPR12 belong to a family of constitutively active Gs-coupled receptors that activate 3′-5′-cyclic adenosine monophosphate (cAMP) and are highly expressed in the brain. Among these receptors, the endogenous expression of GPR3 in cerebellar granule neurons (CGNs) is increased following development. GPR3 is important for neurite outgrowth and neural maturation; however, the physiological functions of GPR3 remain to be fully elucidated. Here, we investigated the survival and antiapoptotic functions of GPR3 under normal and apoptosis-inducing culture conditions. Under normal culture conditions, CGNs from GPR3-knockout mice demonstrated lower survival than did CGNs from wild-type or GPR3-heterozygous mice. Cerebellar sections from GPR3−/− mice at P7, P14, and P21 revealed more caspase-3-positive neurons in the internal granular layer than in cerebellar sections from wild-type mice. Conversely, in a potassium-deprivation model of apoptosis, increased expression of these three receptors promoted neuronal survival. The antiapoptotic effect of GPR3 was also observed under hypoxic (1% O2/5% CO2) and reactive oxygen species (ROS)-induced apoptotic conditions. We further investigated the signaling pathways involved in the GPR3-mediated antiapoptotic effect. The addition of the PKA inhibitor KT5720, the MAP kinase inhibitor U0126, and the PI3 kinase inhibitor LY294002 abrogated the GPR3-mediated antiapoptotic effect in a potassium-deprivation model of apoptosis, whereas the PKC inhibitor Gö6976 did not affect the antiapoptotic function of GPR3. Furthermore, downregulation of endogenous GPR3 expression in CGNs resulted in a marked reduction in the basal levels of ERK and Akt phosphorylation under normal culture conditions. Finally, we used a transient middle cerebral artery occlusion (tMCAO) model in wild-type and GPR3-knockout mice to determine whether GPR3 expression modulates neuronal survival after brain ischemia. After tMCAO, GPR3-knockout mice exhibited a significantly larger infarct area than did wild-type mice. Collectively, these in vitro and in vivo results suggest that the developmental expression of constitutively active Gs-coupled GPR3 activates the ERK and Akt signaling pathways at the basal level, thereby protecting neurons from apoptosis that is induced by various stimuli.

Published

2014

49. G protein-coupled receptor 3: a key factor in the regulation of the nervous system and follicle development

Author

Dianshuai Gao, Bao-Le Zhang, and Yin-Xue Xu

Subjects

Nervous system, endocrine system, medicine.medical_specialty, Sphingosine, GPR3, General Medicine, Biology, medicine.disease, Premature ovarian failure, Cell biology, Follicle, chemistry.chemical_compound, Endocrinology, medicine.anatomical_structure, chemistry, Cell surface receptor, Internal medicine, medicine, Receptor, G protein-coupled receptor

Abstract

G protein-coupled receptors (GPCRs), the largest cell surface receptor superfamily, are involved in many physiological and pathological processes. G protein-coupled receptor 3 (Gpr3) is a newly discovered sphingosine 1-phosphate receptor, which directly or indirectly takes part in regulating the processes of nervous system and follicle development in the vertebrates. As a potential therapeutic drug target for a variety of neurological diseases and premature ovarian failure, its physiological function and biological mechanisms deserve further studies. In this paper, we reviewed the functions of Gpr3 in the processes of nervous system development and ovarian follicular development in the vertebrates.

Published

2013

50. Neuro-psychopharmacological perspective of Orphan receptors of Rhodopsin (class A) family of G protein-coupled receptors

Author

Muhammad Zahid Khan and Ling He

Subjects

0301 basic medicine, Pharmacology, Rhodopsin, Mental Disorders, Brain, GPR3, Class C GPCR, Neurodegenerative Diseases, Biology, Ligands, Orphan Nuclear Receptors, Rhodopsin-like receptors, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, GPR55, GPR6, GPR62, Animals, Humans, Receptor, Neuroscience, Endoplasmic Reticulum Chaperone BiP, 030217 neurology & neurosurgery, G protein-coupled receptor

Abstract

In the central nervous system (CNS), G protein-coupled receptors (GPCRs) are the most fruitful targets for neuropsychopharmacological drug development. Rhodopsin (class A) is the most studied class of GPCR and includes orphan receptors for which the endogenous ligand is not known or is unclear. Characterization of orphan GPCRs has proven to be challenging, and the production pace of GPCR-based drugs has been incredibly slow. Determination of the functions of these receptors may provide unexpected insight into physiological and neuropathological processes. Advances in various methods and techniques to investigate orphan receptors including in situ hybridization and knockdown/knockout (KD/KO) showed extensive expression of these receptors in the mammalian brain and unmasked their physiological and neuropathological roles. Due to these rapid progress and development, orphan GPCRs are rising as a new and promising class of drug targets for neurodegenerative diseases and psychiatric disorders. This review presents a neuropsychopharmacological perspective of 26 orphan receptors of rhodopsin (class A) family, namely GPR3, GPR6, GPR12, GPR17, GPR26, GPR35, GPR39, GPR48, GPR49, GPR50, GPR52, GPR55, GPR61, GPR62, GPR63, GPR68, GPR75, GPR78, GPR83, GPR84, GPR85, GPR88, GPR153, GPR162, GPR171, and TAAR6. We discussed the expression of these receptors in mammalian brain and their physiological roles. Furthermore, we have briefly highlighted their roles in neurodegenerative diseases and psychiatric disorders including Alzheimer’s disease, Parkinson’s disease, neuroinflammation, inflammatory pain, bipolar and schizophrenic disorders, epilepsy, anxiety, and depression.

Published

2016