CLC number: Q291
On-line Access: 2024-08-27
Received: 2023-10-17
Revision Accepted: 2024-05-08
Crosschecked: 2012-06-05
Cited: 7
Clicked: 7182
Bao-le Zhang, Ye Li, Jian-hua Ding, Fu-lu Dong, Yan-jun Hou, Bao-chun Jiang, Fang-xiong Shi, Yin-xue Xu. Sphingosine 1-phosphate acts as an activator for the porcine Gpr3 of constitutively active G protein-coupled receptors[J]. Journal of Zhejiang University Science B, 2012, 13(7): 555-566.
@article{title="Sphingosine 1-phosphate acts as an activator for the porcine Gpr3 of constitutively active G protein-coupled receptors",
author="Bao-le Zhang, Ye Li, Jian-hua Ding, Fu-lu Dong, Yan-jun Hou, Bao-chun Jiang, Fang-xiong Shi, Yin-xue Xu",
journal="Journal of Zhejiang University Science B",
volume="13",
number="7",
pages="555-566",
year="2012",
publisher="Zhejiang University Press & Springer",
doi="10.1631/jzus.B1100353"
}
%0 Journal Article
%T Sphingosine 1-phosphate acts as an activator for the porcine Gpr3 of constitutively active G protein-coupled receptors
%A Bao-le Zhang
%A Ye Li
%A Jian-hua Ding
%A Fu-lu Dong
%A Yan-jun Hou
%A Bao-chun Jiang
%A Fang-xiong Shi
%A Yin-xue Xu
%J Journal of Zhejiang University SCIENCE B
%V 13
%N 7
%P 555-566
%@ 1673-1581
%D 2012
%I Zhejiang University Press & Springer
%DOI 10.1631/jzus.B1100353
TY - JOUR
T1 - Sphingosine 1-phosphate acts as an activator for the porcine Gpr3 of constitutively active G protein-coupled receptors
A1 - Bao-le Zhang
A1 - Ye Li
A1 - Jian-hua Ding
A1 - Fu-lu Dong
A1 - Yan-jun Hou
A1 - Bao-chun Jiang
A1 - Fang-xiong Shi
A1 - Yin-xue Xu
J0 - Journal of Zhejiang University Science B
VL - 13
IS - 7
SP - 555
EP - 566
%@ 1673-1581
Y1 - 2012
PB - Zhejiang University Press & Springer
ER -
DOI - 10.1631/jzus.B1100353
Abstract: We cloned the complete coding sequences of porcine Gpr3, Gpr6, and Gpr12 genes. Further, on the basis of their high levels of sequence similarity, these genes are identified as a subfamily of g protein-coupled receptors. These putative protein sequences also showed high sequence identity with other mammalian orthologs, including several highly conserved motifs. A wide expression of the Gpr3 gene in pigs was observed through tissue distribution analysis by reverse transcriptase-polymerase chain reaction (RT-PCR) and real-time PCR, specially in the brain, pituitary, fat, liver and oocyte, where its strong expression was observed. The Gpr3 gene was found to be located on chromosome 6 and a single exon coded for the entire open-reading frame. Expression of porcine Gpr3 in HEK293 cells resulted in constitutive activation of adenylate cyclase (AC) similar in amplitude to that produced by fully stimulated Gs-coupled receptors. Moreover, sphingosine 1-phosphate (S1P) could increase AC activation via the constitutively active Gpr3 receptor. When a Gpr3-green fluorescent protein (GFP) construct was expressed in HEK293 cells, GFP-labeled Gpr3 protein was shown to be localized in the plasmalemma and subcellular membranes. After S1P treatment, agonist-mediated internalization could be visualized by confocal microscopy. In short, our findings suggest the porcine Gpr3, Gpr6, and Gpr12 genes as a subfamily of g protein-coupled receptors, and porcine Gpr3 was a constitutively active g protein-coupled receptor. Constitutive activation of AC and agonist-mediated internalization of Gpr3 receptor could be modulated by the S1P, suggesting that S1P might act as an activator for porcine Gpr3 receptor.
[1]Alewijnse, A.E., Timmerman, H., Jacobs, E.H., Smit, M.J., Roovers, E., Cotecchia, S., Leurs, R., 2000. The effect of mutations in the DRY motif on the constitutive activity and structural instability of the histamine H2 receptor. Mol. Pharmacol., 57(5):890-898.
[2]Clemens, J.J., Davis, M.D., Lynch, K.R., Macdonald, T.L., 2003. Synthesis of para-alkyl aryl amide analogues of sphingosine-1-phosphate: discovery of potent S1P receptor agonists. Bioorg. Med. Chem. Lett., 13(20):3401-3404.
[3]Conway, B.R., Minor, L.K., Xu, J.Z., Gunnet, J.W., DeBiasio, R., D′Andrea, M.R., Rubin, R., Giuliano, K., DeBiasio, L., Demarest, K.T., 1999. Quantification of G-protein coupled receptor internatilization using G-protein coupled receptor-green fluorescent protein conjugates with the ArrayScantrade mark high-content screening system. J. Biomol. Screen., 4(2):75-86.
[4]DiLuigi, A., Weitzman, V.N., Pace, M.C., Siano, L.J., Maier, D., Mehlmann, L.M., 2008. Meiotic arrest in human oocytes is maintained by a Gs signaling pathway. Biol. Reprod., 78(4):667-672.
[5]Hinckley, M., Vaccari, S., Horner, K., Chen, R., Conti, M., 2005. The G-protein-coupled receptors GPR3 and GPR12 are involved in cAMP signaling and maintenance of meiotic arrest in rodent oocytes. Dev. Biol., 287(2):249-261.
[6]Howard, A.D., McAllister, G., Feighner, S.D., Liu, Q., Nargund, R.P., van der Ploeg, L.H., Patchett, A.A., 2001. Orphan G-protein-coupled receptors and natural ligand discovery. Trends Pharmacol. Sci., 22(3):132-140.
[7]Ignatov, A., Lintzel, J., Hermans-Borgmeyer, I., Kreienkamp, H.J., Joost, P., Thomsen, S., Methner, A., Schaller, H.C., 2003a. Role of the G-protein-coupled receptor GPR12 as high-affinity receptor for sphingosylphosphorylcholine and its expression and function in brain development. J. Neurosci., 23(3):907-914.
[8]Ignatov, A., Lintzel, J., Kreienkamp, H.J., Schaller, H.C., 2003b. Sphingosine-1-phosphate is a high-affinity ligand for the G protein-coupled receptor GPR6 from mouse and induces intracellular Ca2+ release by activating the sphingosine-kinase pathway. Biochem. Biophys. Res. Commun., 311(2):329-336.
[9]Iismaa, T.P., Kiefer, J., Liu, M.L., Baker, E., Sutherland, G.R., Shine, J., 1994. Isolation and chromosomal localization of a novel human G-protein-coupled receptor (GPR3) expressed predominantly in the central nervous system. Genomics, 24(2):391-394.
[10]Joost, P., Methner, A., 2002. Phylogenetic analysis of 277 human G-protein-coupled receptors as a tool for the prediction of orphan receptor ligands. Genome Biol., 3(11):RESEARCH0063.
[11]Kabarowski, J.H., Zhu, K., Le, L.Q., Witte, O.N., Xu, Y., 2001. Lysophosphatidylcholine as a ligand for the immunoregulatory receptor G2A. Science, 293(5530):702-705.
[12]Ledent, C., Demeestere, I., Blum, D., Petermans, J., Hamalainen, T., Smits, G., Vassart, G., 2005. Premature ovarian aging in mice deficient for Gpr3. PNAS, 102(25):8922-8926.
[13]Mehlmann, L.M., Saeki, Y., Tanaka, S., Brennan, T.J., Evsikov, A.V., Pendola, F.L., Knowles, B.B., Eppig, J.J., Jaffe, L.A., 2004. The Gs-linked receptor GPR3 maintains meiotic arrest in mammalian oocytes. Science, 306(5703):1947-1950.
[14]Moller, S., Croning, M.D., Apweiler, R., 2001. Evaluation of methods for the prediction of membrane spanning regions. Bioinformatics, 17(7):646-653.
[15]Murakami, A., Takasugi, H., Ohnuma, S., Koide, Y., Sakurai, A., Takeda, S., Hasegawa, T., Sasamori, J., Konno, T., Hayashi, K., et al., 2010. Sphingosine 1-phosphate (S1P) regulates vascular contraction via S1P3 receptor: investigation based on a new S1P3 receptor antagonist. Mol. Pharmacol., 77(4):704-713.
[16]Nakai, K., Horton, P., 1999. PSORT: a program for detecting sorting signals in proteins and predicting their subcellular localization. Trends Biochem. Sci., 24(1):34-36.
[17]Padmanabhan, S., Myers, A.G., Prasad, B.M., 2009. Constitutively active GPR6 is located in the intracellular compartments. FEBS Lett., 583(1):107-112.
[18]Pyne, S., Pyne, N.J., 2000. Sphingosine 1-phosphate signalling in mammalian cells. Biochem. J., 349(Pt 2):385-402.
[19]Ruiz-Medina, J., Ledent, C., Valverde, O., 2011. GPR3 orphan receptor is involved in neuropathic pain after peripheral nerve injury and regulates morphine-induced antinociception. Neuropharmacology, 61(1-2):43-50.
[20]Saeki, Y., Ueno, S., Mizuno, R., Nishimura, T., Fujimura, H., Nagai, Y., Yanagihara, T., 1993. Molecular cloning of a novel putative G protein-coupled receptor (GPCR21) which is expressed predominantly in mouse central nervous system. FEBS Lett., 336(2):317-322.
[21]Tanaka, S., Ishii, K., Kasai, K., Yoon, S.O., Saeki, Y., 2007. Neural expression of G protein-coupled receptors GPR3, GPR6, and GPR12 up-regulates cyclic AMP levels and promotes neurite outgrowth. J. Biol. Chem., 282(14):10506-10515.
[22]Tanaka, S., Shaikh, I.M., Chiocca, E.A., Saeki, Y., 2009. The Gs-linked receptor GPR3 inhibits the proliferation of cerebellar granule cells during postnatal development. PLoS One, 4(6):e5922.
[23]Uhlenbrock, K., Gassenhuber, H., Kostenis, E., 2002. Sphingosine 1-phosphate is a ligand of the human gpr3, gpr6 and gpr12 family of constitutively active G protein-coupled receptors. Cell. Signal., 14(11):941-953.
[24]Valverde, O., Celerier, E., Baranyi, M., Vanderhaeghen, P., Maldonado, R., Sperlagh, B., Vassart, G., Ledent, C., 2009. GPR3 receptor, a novel actor in the emotional-like responses. PLoS One, 4(3):e4704.
[25]Whorton, M.R., Bokoch, M.P., Rasmussen, S.G., Huang, B., Zare, R.N., Kobilka, B.Sunahara, R.K., 2007. A monomeric G protein-coupled receptor isolated in a high-density lipoprotein particle efficiently activates its G protein. PNAS, 104(18):7682-7687.
[26]Wittenberger, T., Hellebrand, S., Munck, A., Kreienkamp, H.J., Schaller, H.C., Hampe, W., 2002. GPR99, a new G protein-coupled receptor with homology to a new subgroup of nucleotide receptors. BMC Genomics, 3(1):17.
[27]Xiao, M.F., Xu, J.C., Tereshchenko, Y., Novak, D., Schachner, M., Kleene, R., 2009. Neural cell adhesion molecule modulates dopaminergic signaling and behavior by regulating dopamine D2 receptor internalization. J. Neurosci., 29(47):14752-14763.
[28]Xu, Y., Zhu, K., Hong, G., Wu, W., Baudhuin, L.M., Xiao, Y., Damron, D.S., 2000. Sphingosylphosphorylcholine is a ligand for ovarian cancer G-protein-coupled receptor 1. Nat. Cell Biol., 2(5):261-267.
[29]Zhang, B., Ding, J., Li, Y., Wang, J., Zhao, Y., Wang, W., Shi, S., Dong, F., Zhang, Z., Shi, F., et al., 2012. The porcine Gpr3 gene: molecular cloning, characterization and expression level in tissues and cumulus-oocyte complexes during in vitro maturation. Mol. Biol. Rep., 39(5):5831-5839.
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