Analysis of G-Protein Coupled Receptor 12

Analysis of G-Protein conjugate sensory sensory sense organ 12 hookG-Protein couple receptor 12 (GPR12) belongs to the orphan GPCR family which is the same of the GPR3 and GPR6. homophilelogy model for the protein GPR12 was gene hooked from the SWISS-MODEL website which portrayed an every(prenominal) important motif with seven transmembrane -helix interconnected by loops. GPR12 acts through the cyclical Adenosine monophosphate (cAMP) channel and promotes neurite outgrowth in primary neurons which can be utilise to slow down the onward motion of neurodegene sellive diseases. The gene of GPR12 is located in the chromosome 13q12.13 for homo, 12p11 for rat and 5 5 G3 for a snarf with the size of 5.6 kbp, 3.4 kbp, and 4.3 kbp. Four menstruum ongoing clinical trials studies on GPR12 was found on clinicaltrials.gov.G-Protein Coupled Receptor 12 (GPR12) belongs to the orphan GPCR family which is the same of the GPR3 and GPR6 (Ignatov et al., 2003a Ignatov et al., 2003b). G PR 12 family members are constitutively activated and pop the cAMP signaling cascades (Ignatov et al., 2003a). It is reported that GPR12 promote neurite extension in primary neurons (Ignatov et al., 2003a). The chronological sequence identity of GPR12 is standardised to GPCR S1P5 by 34%, GPR3 by 57% and GPR6 by 58% (Ignatov et al., 2003a Ignatov et al., 2003b). Hence, it is hypothesized that the orphan receptors might share mutual ligands and also have similar physiological draws (Uhlenbrock et al., 2002 Tanaka et al., 2007). GPR12 has a high bandaging affinity towards Sphingosylphosphorylcholine (SPC) (Uhlenbrock et al., 2002). GPR 12 also binds with Sphingosine-1-phosphate (S1P) with low affinity (Uhlenbrock et al., 2002). GPR12 family members are always activated and cAMP downstream signaling cascades initiated (Uhlenbrock et al., 2002 Ignatov et al., 2003a). This persistent activating promotes neurite extension in primary neurons (Tanaka et al., 2007).GPR12 belongs to t he orphan GPCR family which is the same of the GPR3 and GPR6 (Ignatov et al., 2003a Ignatov et al., 2003b). According to pierce et al., GPR12 belongs to the GPCRs, Class A Rhodopsin-like subfamily with any different Orphan GPCR receptors ( bird of night et al., 2003).2.1. StructureA search was conducted for GPR12 in the RCSB protein data bank to identify the protein structure of G-Protein Coupled Receptor 12. There were no matches found in the search which is basen in figure 1. Hence, a Homology model for the protein was generated from the SWISS-MODEL website, 27.41% sequence identity was indicated for Cannabinoid receptor 1 (Flavodoxin). Flavodoxin, Cannabinoid receptor one was chosen as the template, and a 3D morphological model was generated for GPR12 from the template which is shown in the figures 2a and 2b. The GMQE (Global Model Quality Estimation) and Q-Mean value for the generated protein 0.56 and -4.28. The generated protein showed an all alpha motif with seven transme mbrane -helix interconnected by loops forming quaternity extra boothular topological domains and quaternity cytoplasmic topological domains. The alignment of protein sequence amid Human GPR12 and GPR12 of new(prenominal) species like computer mouse and rat showed very slight variation which indicates the protein is hold amid these species(UniProtKB UniProtKB UniProtKB). The protein alignment is shown in figure 3.2.2. PathwayAccording to Horn et al., GPR12 belongs to the GPCRs, Class A Rhodopsin-like subfamily with all other Orphan GPCR receptors (Horn et al., 2003). GPR12 acts through the cyclic Adenosine monophosphate (cAMP) pathway (Tanaka et al., 2007). Since, GPR12 is an orphan receptor where its natural ligand is unknown (Ignatov et al., 2003a). When the ligand such as S1P or SPC binds to the GPR12, the G-Protein gets activated due to the binding of GTP (Ignatov et al., 2003a). Thus, G-Protein activates Adenylate cyclase which converts the Adenosine triphosphate (ATP) into cAMP, and the cAMP activates Protein Kinase A (Ignatov et al., 2003a). The excited Protein Kinase A activates the cellular reaction such as neurite extension in primary neurons (Ignatov et al., 2003a). Refer figure 42.3. Gene and Evolutionary aspects of GPR12The alignment of protein sequence between Human GPR12 and GPR12 of other species like mouse and rat showed very less variation which indicates the protein is conserved between these species (UniProtKB UniProtKB UniProtKB). The protein alignment is shown in figure 3. The gene location of GPR12 in the chromosomes locus is nearly the same for human and rat, provided it is different in mouse (NCBI-Gene NCBI-Gene NCBI-Gene). The gene of GPR12 is located in the chromosome 13q12.13 for human, 12p11 for rat and 5 5 G3 for mouse (NCBI-Gene NCBI-Gene NCBI-Gene). The GPR12 gene contains two exons in humans, common chord exons in rat and three exons in Mouse separating the intron sequence and the evolutionary association of the gene sequence of GPR12 between the species and between GPCR family is shown in figure 5a and 5b (NCBI-Gene NCBI-Gene NCBI-Gene). The GPR12 gene size for a human is 5.6 kbp, for rat it is 3.4 kbp, and for the mouse, it is 4.3 kbp (NCBI-Gene NCBI-Gene NCBI-Gene Stevens et al., 2013).GPR12 magnetic variation mice showed an effect in their emotionality was moved(p) due to the mutation in GPR12 which was no significant change (Frank et al., 2012). GPR12 overexpressed in neurons upregulate cAMP levels and promotes neurite outgrowth in primary neurons which can be used to slow down the progression of neurodegenerative diseases like Alzheimers disease, Parkinsons disease, Huntingtons disease, etc. (Tanaka et al., 2007). GPR12 is also involved in the regulation of cell survival and cell proliferation which may vary during the diseased condition which causes astrocytes to grow at a faster rate and results in inflammation (Lu et al., 2012).A search was done for G-Protein coupled receptor 12 on clinicaltrails.gov website which showed four current ongoing clinical trials studies on GPR12. The studies were different from each other such as Platelet reactivity (ClinicalTrials.gov), Stoke (ClinicalTrials.gov), Metastatic Lung Adenocarcinomas (ClinicalTrials.gov) and sick headache (ClinicalTrials.gov).GPR12 belongs to the GPCRs, Class A Rhodopsin-like subfamily with all other Orphan GPCR receptors. The gene code for GPR12 is conserved between Humans, Rats, and Mouse which indicates the existence of similar roles and function in these three animals. GPR12 is still in the stages of primary research where its structure, signaling pathways, function, and roles are still waiting to be found. GPR12 has recently assumed to be associated with uneasy disorders and diseases. Clinical trials have been successfully conducted for GPR12 for many diseases one of which is depression.ReferencesClinicalTrials.gov Is There a Transient Rebound Effect of Platelet Reactivity Following utmost of Dual Antiplatelet Therapy With Ticagrelor a Single Center Prospective Observational Trial. Journal, https//clinicaltrials.gov/ct2/show/NCT02808039?term=G-Protein%2BCoupled%2BReceptor%2B12recr=Openrank=1, January 25, 2017.ClinicalTrials.gov Platelet Reactivity in Acute Non-disabling Cerebrovascular Events (PRINCE). Journal, https//clinicaltrials.gov/ct2/show/NCT02506140?term=G-Protein+Coupled+Receptor+12recr=Openrank=2, January 25, 2017.ClinicalTrials.gov Retrospective Analysis of the Expression of the Neurotensin Receptor by Metastatic Lung Adenocarcinomas (NTS). Journal, https//clinicaltrials.gov/ct2/show/NCT02891733?term=G-Protein%2BCoupled%2BReceptor%2B12recr=Openrank=4, January 25, 2017.ClinicalTrials.gov Ticagrelor Therapy for RefrACTORy Migraine deal (TRACTOR). Journal, https//clinicaltrials.gov/ct2/show/NCT02518464?term=G-Protein%2BCoupled%2BReceptor%2B12recr=Openrank=3, January 25, 2017.Frank, E., Wu, Y., Piyaratna, N., Body, W.J., Snikeris, P., South, T., Gerdin, A.K., Bj ursell, M., Bohlooly, Y.M., Storlien, L. Huang, X.F. (2012) Metabolic parameters and emotionality are little affected in G-protein coupled receptor 12 (Gpr12) mutant mice. PLoS One, 7, e42395.Horn, F., Bettler, E., Oliveira, L., Campagne, F., Cohen, F.E. Vriend, G. (2003) GPCRDB information corpse for G protein-coupled receptors. Nucleic acids research, 31, 294-297.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. Journal of Neuroscience, 23, 907-914.Ignatov, A., Lintzel, J., Kreienkamp, H.-J. Chica Schaller, H. (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. Biochemical and Biophysical Research Communica tions, 311, 329-336.Lu, X., Zhang, N., Meng, B., Dong, S. Hu, Y. (2012) pastime of GPR12 in the regulation of cell proliferation and survival. Mol Cell Biochem, 366, 101-110.NCBI-Gene Gpr12 G-protein coupled receptor 12 Mus brawn (house mouse) Gene NCBI. Journal, https//www.ncbi.nlm.nih.gov/gene/14738, January/25/2017.NCBI-Gene GPR12 G protein-coupled receptor 12 Homo sapiens (human) Gene NCBI. Journal, https//www.ncbi.nlm.nih.gov/gene/2835, January/25/2017.NCBI-Gene Gpr12 G protein-coupled receptor 12 Rattus norvegicus (Norway rat) Gene NCBI. Journal, https//www.ncbi.nlm.nih.gov/gene/80840, January/25/2017.Stevens, R.C., Cherezov, V., Katritch, V., Abagyan, R., Kuhn, P., Rosen, H. Wuthrich, K. (2013) The GPCR Network a large-scale collaboration to determine human GPCR structure and function. Nat Rev Drug Discov, 12, 25-34.Tanaka, S., Ishii, K., Kasai, K., Yoon, S.O. Saeki, Y. (2007) nervous expression of G protein-coupled receptors GPR3, GPR6, and GPR12 up-regulates cyc lic AMP levels and promotes neurite outgrowth. J Biol Chem, 282, 10506-10515.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. Cellular signalling, 14, 941-953.UniProtKB GPR12 G-protein coupled receptor 12 Homo sapiens (Human) GPR12 gene protein. Journal, http//www.uniprot.org/uniprot/P47775, January 25, 2017.UniProtKB Gpr12 G-protein coupled receptor 12 Mus musculus (Mouse) Gpr12 gene protein. Journal, http//www.uniprot.org/uniprot/P35412, January 25, 2017.UniProtKB Gpr12 G-protein coupled receptor 12 Rattus norvegicus (Rat) Gpr12 gene protein. Journal, http//www.uniprot.org/uniprot/P30951, January 25, 2017. count on 1 No structure was found for the protein GPR12 in RCSB Protein data bank. visit 2a Side view of the GPR12 structure which was generated by SWISS-MODEL. The protein is presentation an all alpha motif with seven transmembrane -helix interconnected by loops forming four extracellular topological domains and four cytoplasmic topological domains.Figure 2b Top view of the GPR12 structure which was generated by SWISS-MODEL. The protein is showing an all alpha motif with seven transmembrane -helix interconnected by loops forming four extracellular topological domains and four cytoplasmic topological domains.Figure 3 GPR12 protein alignment for the species Human, mouse and rat generated from ClustalW. * (asterisk) indicates positions which have a single, fully conserved residue, (colon) indicates conservation between groups of strongly similar residue properties, . (period) indicates conservation between groups of weakly similar residue properties.Figure 4 GPR12 proteins complete intracellular signaling pathwayFigure 5a Phylogenetic/evolutionary tree of GPCR family members (Stevens et al., 2013)Figure 5b Phylogenetic/evolutionary tree of GPR12 showing evolutionary difference between human, rat, and mouse G-P rotein Coupled Receptor (GPR12) ProteinAgonistAntagonistSphingosine-1-phosphateSuraminSphingosyl-phosphocholineTable 1 GPR12 agonist and obstructer with structure and name