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PhTX-433

Names
IUPAC name N-[(2S)-1-[4-[3-(3-Aminopropylamino)propylamino]butylamino]-3-(4-hydroxyphenyl)-1-oxopropan-2-yl]butanamide
Identifiers
CAS Number	77108-00-0 Y
3D model (JSmol)	Interactive image
ChEMBL	ChEMBL1160514 N
ChemSpider	103077 N
PubChem CID	115201
InChI InChI=1S/C23H41N5O3/c1-2-7-22(30)28-21(18-19-8-10-20(29)11-9-19)23(31)27-17-4-3-13-25-15-6-16-26-14-5-12-24/h8-11,21,25-26,29H,2-7,12-18,24H2,1H3,(H,27,31)(H,28,30)/t21-/m0/s1 N Key: VRQNABCCOFCGJL-NRFANRHFSA-N N InChI=1/C23H41N5O3/c1-2-7-22(30)28-21(18-19-8-10-20(29)11-9-19)23(31)27-17-4-3-13-25-15-6-16-26-14-5-12-24/h8-11,21,25-26,29H,2-7,12-18,24H2,1H3,(H,27,31)(H,28,30)/t21-/m0/s1 Key: VRQNABCCOFCGJL-NRFANRHFBQ
SMILES CCCC(=O)N[C@@H](Cc1ccc(cc1)O)C(=O)NCCCCNCCCNCCCN
Properties
Chemical formula	C23H41N5O3
Molar mass	435.603 g/mol
Except where otherwise noted, data are given for materials in their standard state (at 25 °C [77 °F], 100 kPa). N verify (what is YN ?) Infobox references

Tracking categories (test):

• SizeSet

Chemical compound

European Beewolf female with paralyzed prey intended for her offspring

Philanthotoxins are components of the venom of the Egyptian solitary wasp Philanthus triangulum, commonly known as the European beewolf. Philanthotoxins are polyamine toxins, a group of toxins isolated from the venom of wasps and spiders which immediately but reversibly paralyze their prey.^[1] δ-philanthotoxin, also known as PhTX-433, is the most active philanthotoxin that can be refined from the venom.^[2] PhTX-433 functions by non-selectively blocking excitatory neurotransmitter ion channels^[3], including nicotinic acetylcholine receptors (NAChRs) and ionotropic glutamate receptors (iGluRs).^[4] Synthetic analogues, including PhTX-343 and PhTX-12, have been developed to improve selectivity^[3]. While the IC₅₀ values of philanthotoxins varies between analogues and receptor subunit composition, the IC₅₀ value of PhTX-433 at the iGluR AMPA receptor naturally expressed in locust leg muscle is 18 μM and the IC₅₀ value at rat nAChRs is 1 μM.^[5][6]

Biological Context

Nesting female Philanthus triangulum wasps utilize philanthotoxin-containing venom to paralyze prey (generally working honey bees Apis mellifera though other species may be collected) by stinging directly behind the front legs through the articular membranes. The female then carries the paralyzed prey to her nest burrow to be fed to her brood.^[7] The ability of the philanthotoxins in the venom to paralyze insect skeletal muscle through the blocking of glutamate receptor ion channels allows for this process to occur^[8]. Larval wasps rely on the paralyzed bees as a food source when they emerge. Paralyzed bee-prey may be stored for some length of time within the burrow and are regularly provisioned by the mother wasp to avoid spoiling due to fungal or bacterial infestation. In other predatory wasp species that paralyze instead of immediately killing the prey they provide their offspring, spoilage is deferred significantly by paralysis. Analysis of the provisioning of bee-prey by Beewolves, however, found that paralysis alone was not found to be sufficient to prevent spoilage, and that additional preservation methods were associated with treatment by the female wasp^[9].

Mechanism of Action

Philanthotoxins reversibly inhibit AMPA (also called the "quisqualate receptor"), kainate, and NMDA ionotropic glutamate receptors.^[4] Philanthotoxins have a hydrophobic aromatic head group and a hydrophilic polyamine tail, which allow them to inhibit iGluRs by binding within the ion channel.^[10] The nitrogen atoms of the polyamine tail have been proposed to interact with the negatively-charged or polar amino acids within the cation-selective channel pore. The aromatic head group anchors the molecule to the extracellular entrance to the channel.^[11] Inhibition may also occur via binding to an external allosteric polyamine binding site.^[6] Subunit composition of iGluRs heavily influences the efficacy of philanthotoxins. For example, AMPA receptors lacking the GluA2 subunit are highly sensitive to PhTX-433, whereas receptors containing the GluA2 subunit are nearly entirely insensitive.^[4] Study into the exact interactions that occur between the philanthotoxin molecules and the ion channels coupled with glutamate receptors has indicated that the molecules could bind to the narrowest region of the channel, thereby blocking ion flow, and that membrane potential is important to toxin-receptor interaction, making PhTXs highly voltage-dependent antagonists of iGluRs^[12]. PhTX-433 inhibits both vertebrate and insect nAChRs predominantly by non-competitively blocking the ion channel in its open conformation.^[13][14]

 

Philanthotoxins have four distinct regions that can be edited to produce a huge variety of synthetic analogs with varying efficacy and subunit selectivity. 4-3-3 describes number of methylenes separating nitrogens in the tail (thermospermine) region.

Isolation and synthesis

PhTX-433 was structurally elucidated and synthesized in 1988 by Eldefrawi and colleagues. For the isolation and structural identification of PhTX-433 female was venom glands were fractionated using reverse-phase HPLC and fractions were tested for pharmacological activity and the most pharmacologically active sample was re-fractioned using the same method. UV spectrum and H¹NMR analysis revealed that the structure consisted of a butyrl/tyrosil/polyamine sequence. Three isomers (PhTX-433, PhTX-343, and PhTX-334) were determined to be possible candidate structures and all three were synthesized_____ should I include details as to synthesis? I feel like it is to technical and anyone who cares will just go to the original paper? (See Figure__). PhTX-433 was found to be identical to the natural product isolated from the fractionalization and this structure in terms of H¹NMR, Mass Spectometry, CD (what does CD mean?), HPLC, and biological activity. PhTX-433 was therefore designated as the structure of the most biologically active naturally occurring philanthotoxin.^[15] Because PhTX-433 lacks strong receptor subtype selectivity, a variety of analogs have been synthesized as candidates for potential pharmacological exploitation.^[10] Philanthotoxins have four distinct regions that can be modified (see image at right); the number of nitrogens in the polyamine chain is the most common distinction between synthetic analogs.^[10] The most commonly synthesized and studied analogue is PhTX-343, which has similar properties to PhTX-433.^[10] Notably, philanthoxin and its synthetic analogues are smaller than similar polyamine toxins form orb-web spider venoms and argiotoxins and are easier to synthesize. ^[15]

Historical Context

Venoms from Hymenoptera species have been used in Chinese, Korean, and ancient Greek and Egyptian traditional medical practices since 1000-3000 BCE to treat a variety of ailments, including various neurological disorders^[12]. Valued in part for their pharmacological usefulness, bees and wasps feature heavily in the art and mythology of ancient Egypt, featured in hieroglyphs, amulets, and figurines^[16].

Modern Uses

Analogues with IC₅₀ values in the low nano-molar and pico-molar range have been identified and studied.^[10] Combined with the potential for precise receptor subtype selectivity, synthetic philanthotoxins could be used as highly potent and selective inhibitors for nAChRs and iGluRs. Glutamate is the main excitatory neurotransmitter in the mammalian brain and has been implicated in mediating neurological disorders such as epilepsy and neurodegenerative diseases such as Alzheimer's Disease and Huntington's disease.^[15] There is considerable interest in the therapeutic development of iGluR antagonists as anticonvulsants, muscle relaxants, and agents to protect from ischemic brain damage and possibly neurodegeneration.^[15] Study of philanthotoxins has therefore been largely focused on their potent antagonistic effect on iGlu receptorsin invertebrate and vertebrate nervous systems, as abnormal activation of these receptors is involved with Alzheimer's Disease, Stroke, Epilepsy, Neuropathic Pain, Parkinson's Disease, and Schizophrenia^[12]. By blocking open ionotropic receptor channels, philanthotoxins can moderate excessive opening associated with pathological neurological conditions and prevent a potentially damaging influx of calcium (Ca²⁺), resulting in neuroprotection. It is notable that this is a similar mechanism of action to the Alzheimer's drug Memantine, which has obtained good clinical results in the symptomatic treatment of Alzhiemer's Disease^[12]. In addition, because nAChRs are the major excitatory neurotransmitter gated ion channels in insects, philanthotoxins may be developed as insecticides. ^[11][10] The low specificity of the naturally occurring PhTX-433 has been the major obstacle in the development of PhTX-433 insecticides^[15]. Study of ionotropic glutamate (iGlu; AMPA) and nACh receptors using philanthotoxins as tools has been ongoing since the 1980s.^[12]

To Add to Wasp Page: Philanthus triangulum venom contains a class of compounds called Philanthoxins; these are polyamine toxins that allow the wasp to temporarily paralyze their prey^[1]. Philanthoxins have been explored as a source of insecticides as well as for therapeutic application in the treatment of neurological disorders due to their inhibitory effects on ionotropic glutamate (iGlu and AMPA) and nicotinic acetylcholine receptors. Study of these receptor types using philanthotoxins has been ongoing since the 1980s^[12].

References

1. Strømgaard, K.; Jensen, L. S.; Vogensen, S. B. (2005). "Polyamine toxins: development of selective ligands for ionotropic receptors". Toxicon. 45 (3): 249–254. doi:10.1016/j.toxicon.2004.11.013. PMID 15683862.
2. Piek, T. (1982). "δ-Philanthotoxin, a semi-irreversible blocker of ion-channels". Comparative Biochemistry and Physiology Part C: Comparative Pharmacology. 72 (2): 311–315. doi:10.1016/0306-4492(82)90098-3. PMID 6128152.
3. Kachel, Hamid S.; Franzyk, Henrik; Strømgaard, Kristian; Tikhonov, Denis B.; Mellor, Ian R. (2014-01). "Subunit-Dependent Inhibition of Neuronal Nicotinic Acetylcholine Receptors by Philanthotoxins". Biophysical Journal. 106 (2): 338a. doi:10.1016/j.bpj.2013.11.1935. ISSN 0006-3495. {{cite journal}}: Check date values in: |date= (help)
4. Kachel, H.S.; Patel, R.N.; Franzyk, H.; Mellor, I.R. (2016). "Block of nicotinic acetylcholine receptors by philanthotoxins is strongly dependent on their subunit composition". Scientific Reports. 6: 38116. doi:10.1038/srep38116. PMC 5128878. PMID 27901080.
5. Bruce, M.; Bukownik, R.; Eldefrawi, A. T.; Eldefrawi, M. E.; Goodnow, R.; Kallimopoulos, T.; Konno, K.; Nakanishi, K.; Niwa, M.; Usherwood, P. N. R. (1990). "Structure-activity relationships of analogues of the wasp toxin philanthotoxin: non-competitive antagonists of quisqualate receptors". Toxicon. 28 (11): 1333–1346. doi:10.1016/0041-0101(90)90098-r.
6. Anis, N.; Sherby, S.; Goodnow, R.; Niwa, M.; Konno, K.; Kallimopoulos, T.; Bukownik, R.; Nakanishi, K.; Usherwood, P.; Eldefrawi, A. (1990). "Structure-activity relationships of philanthotoxin analogs and polyamines on N-methyl-D-aspartate and nicotinic acetylcholine receptors". Journal of Pharmacology and Experimental Therapeutics. 254 (3).
7. "Philanthus triangulum (Fabricius,1775) | BWARS". www.bwars.com. Retrieved 2020-04-24.
8. Eldefrawi, Mohyee E.; Anis, Nabil A.; Eldefrawi, Amira T. (1993). "Glutamate receptor inhibitors as potential insecticides". Archives of Insect Biochemistry and Physiology. 22 (1–2): 25–39. doi:10.1002/arch.940220105. ISSN 0739-4462.
9. Strohm, Erhard; Linsenmair, K. Eduard (2001). "Females of the European beewolf preserve their honeybee prey against competing fungi". Ecological Entomology. 26 (2): 198–203. doi:10.1046/j.1365-2311.2001.00300.x. ISSN 1365-2311.
10. Kachel, H. (2015). Inhibition of mammalian nicotinic acetylcholine receptors by philanthotoxin analogues is strongly influenced by subunit composition. Nottingham ePrints.
11. Kachel, Hamid S; Buckingham, Steven D; Sattelle, David B (2018-12-01). "Insect toxins – selective pharmacological tools and drug/chemical leads". Current Opinion in Insect Science. Neuroscience * Insect bio-inspired micro and nanotechnologies. 30: 93–98. doi:10.1016/j.cois.2018.10.001. ISSN 2214-5745.
12. Silva, Juliana; Monge-Fuentes, Victoria; Gomes, Flávia; Lopes, Kamila; Anjos, Lilian; Campos, Gabriel; Arenas, Claudia; Biolchi, Andréia; Gonçalves, Jacqueline; Galante, Priscilla; Campos, Leandro (2015-08-18). "Pharmacological Alternatives for the Treatment of Neurodegenerative Disorders: Wasp and Bee Venoms and Their Components as New Neuroactive Tools". Toxins. 7 (8): 3179–3209. doi:10.3390/toxins7083179. ISSN 2072-6651. PMC 4549745. PMID 26295258.
13. Jayaraman, V.; Usherwood, P. N.; Hess, G. P. (1999). "Inhibition of nicotinic acetylcholine receptor by philanthotoxin-343: kinetic investigations in the microsecond time region using a laser-pulse photolysis technique". Biochemistry. 38 (35): 11406–11414. doi:10.1021/bi991219x. PMID 10471291.
14. Rozental, R.; Scoble, G. T.; Albuquerque, E. X.; Idriss, M.; Sherby, S.; Sattelle, D. B.; Nakanishi, K.; Konno, K.; Eldefrawi, A. T. (1989-04-01). "Allosteric inhibition of nicotinic acetylcholine receptors of vertebrates and insects by philanthotoxin". Journal of Pharmacology and Experimental Therapeutics. 249 (1): 123–130. ISSN 0022-3565. PMID 2468760.
15. Eldefrawi, A. T.; Eldefrawi, M. E.; Konno, K.; Mansour, N.A.; Nakanishi, E.; Oltz, E.; Usherwood, P. N. R. (1988). "Structure and synthesis of a potent glutamate receptor antagonist in wasp venom". Proc. Natl. Acad. Sci. U.S.A. 85 (13): 4910–4913. doi:10.1073/pnas.85.13.4910. PMC 280547. PMID 2838850.
16. Lobban, Richard (2013). "Commentary: Bees in Egypt" (PDF). ribeekeeper.org.

Glutamate receptor modulators

v t e Ionotropic glutamate receptor modulators AMPARTooltip α-Amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid receptor Agonists: Main site agonists: 5-Fluorowillardiine Acromelic acid (acromelate) AMPA BOAA Domoic acid Glutamate Ibotenic acid Proline Quisqualic acid Willardiine; Positive allosteric modulators: Aniracetam Cyclothiazide CX-516 CX-546 CX-614 Farampator (CX-691, ORG-24448) CX-717 CX-1739 CX-1942 Diazoxide Hydrochlorothiazide (HCTZ) IDRA-21 LY-392098 LY-395153 LY-404187 LY-451646 LY-503430 Mibampator (LY-451395) Nooglutyl ORG-26576 Oxiracetam PEPA Pesampator (BIIB-104, PF-04958242) Piracetam Pramiracetam S-18986 Tulrampator (S-47445, CX-1632) Antagonists: ACEA-1011 ATPO Becampanel Caroverine CNQX Dasolampanel DNQX Fanapanel (MPQX) GAMS Kaitocephalin Kynurenic acid Kynurenine Licostinel (ACEA-1021) NBQX PNQX Selurampanel Tezampanel Theanine Topiramate YM90K Zonampanel; Negative allosteric modulators: Barbiturates (e.g., pentobarbital, sodium thiopental) Cyclopropane Enflurane Ethanol (alcohol) Evans blue GYKI-52466 GYKI-53655 Halothane Irampanel Isoflurane Perampanel Pregnenolone sulfate Sevoflurane Talampanel; Unknown/unsorted antagonists: Minocycline KARTooltip Kainate receptor Agonists: Main site agonists: 5-Bromowillardiine 5-Iodowillardiine Acromelic acid (acromelate) AMPA ATPA Domoic acid Glutamate Ibotenic acid Kainic acid LY-339434 Proline Quisqualic acid SYM-2081; Positive allosteric modulators: Cyclothiazide Diazoxide Enflurane Halothane Isoflurane Antagonists: ACEA-1011 CNQX Dasolampanel DNQX GAMS Kaitocephalin Kynurenic acid Licostinel (ACEA-1021) LY-382884 NBQX NS102 Selurampanel Tezampanel Theanine Topiramate UBP-302; Negative allosteric modulators: Barbiturates (e.g., pentobarbital, sodium thiopental) Enflurane Ethanol (alcohol) Evans blue NS-3763 Pregnenolone sulfate NMDARTooltip N-Methyl-D-aspartate receptor Agonists: Main site agonists: AMAA Aspartate Glutamate Homocysteic acid (L-HCA) Homoquinolinic acid Ibotenic acid NMDA Proline Quinolinic acid Tetrazolylglycine Theanine; Glycine site agonists: β-Fluoro-D-alanine ACBD ACC (ACPC) ACPD AK-51 Apimostinel (NRX-1074) B6B21 CCG D-Alanine D-Cycloserine D-Serine DHPG Dimethylglycine Glycine HA-966 L-687414 L-Alanine L-Serine Milacemide Neboglamine (nebostinel) Rapastinel (GLYX-13) Sarcosine; Polyamine site agonists: Neomycin Spermidine Spermine; Other positive allosteric modulators: 24S-Hydroxycholesterol DHEATooltip Dehydroepiandrosterone (prasterone) DHEA sulfate (prasterone sulfate) Epipregnanolone sulfate Plazinemdor Pregnenolone sulfate SAGE-201 SAGE-301 SAGE-718 Antagonists: Competitive antagonists: AP5 (APV) AP7 CGP-37849 CGP-39551 CGP-39653 CGP-40116 CGS-19755 CPP Kaitocephalin LY-233053 LY-235959 LY-274614 MDL-100453 Midafotel (d-CPPene) NPC-12626 NPC-17742 PBPD PEAQX Perzinfotel PPDA SDZ-220581 Selfotel; Glycine site antagonists: 4-Cl-KYN (AV-101) 5,7-DCKA 7-CKA ACC ACEA-1011 ACEA-1328 Apimostinel (NRX-1074) AV-101 Carisoprodol CGP-39653 CNQX D-Cycloserine DNQX Felbamate Gavestinel GV-196771 Harkoseride Kynurenic acid Kynurenine L-689560 L-701324 Licostinel (ACEA-1021) LU-73068 MDL-105519 Meprobamate MRZ 2/576 PNQX Rapastinel (GLYX-13) ZD-9379; Polyamine site antagonists: Arcaine Co 101676 Diaminopropane Diethylenetriamine Huperzine A Putrescine; Uncompetitive pore blockers (mostly dizocilpine site): 2-MDP 3-HO-PCP 3-MeO-PCE 3-MeO-PCMo 3-MeO-PCP 4-MeO-PCP 8A-PDHQ 18-MC α-Endopsychosin Alaproclate Alazocine (SKF-10047) Amantadine Aptiganel Argiotoxin-636 Arketamine ARL-12495 ARL-15896-AR ARL-16247 Budipine Coronaridine Delucemine (NPS-1506) Dexoxadrol Dextrallorphan Dextromethadone Dextromethorphan Dextrorphan Dieticyclidine Diphenidine Dizocilpine Ephenidine Esketamine Etoxadrol Eticyclidine Fluorolintane Gacyclidine Ibogaine Ibogamine Indantadol Ketamine Ketobemidone Lanicemine Levomethadone Levomethorphan Levomilnacipran Levorphanol Loperamide Memantine Methadone Methorphan Methoxetamine Methoxphenidine Milnacipran Morphanol NEFA Neramexane Nitromemantine Noribogaine Norketamine Orphenadrine PCPr PD-137889 Pethidine (meperidine) Phencyclamine Phencyclidine Propoxyphene Remacemide Rhynchophylline Rimantadine Rolicyclidine Sabeluzole Tabernanthine Tenocyclidine Tiletamine Tramadol; Ifenprodil (NR2B) site antagonists: Besonprodil Buphenine (nylidrin) CO-101244 (PD-174494) Eliprodil Haloperidol Isoxsuprine Radiprodil (RGH-896) Rislenemdaz (CERC-301, MK-0657) Ro 8-4304 Ro 25-6981 Safaprodil Traxoprodil (CP-101606); NR2A-selective antagonists: MPX-004 MPX-007 TCN-201 TCN-213; Cations: Hydrogen Magnesium Zinc; Alcohols/volatile anesthetics/related: Benzene Butane Chloroform Cyclopropane Desflurane Diethyl ether Enflurane Ethanol (alcohol) Halothane Hexanol Isoflurane Methoxyflurane Nitrous oxide Octanol Sevoflurane Toluene Trichloroethane Trichloroethanol Trichloroethylene Urethane Xenon Xylene; Unknown/unsorted antagonists: ARR-15896 Bumetanide Caroverine Conantokin D-αAA Dexanabinol Flufenamic acid Flupirtine FPL-12495 FR-115427 Furosemide Hodgkinsine Ipenoxazone (MLV-6976) MDL-27266 Metaphit Minocycline MPEP Niflumic acid Pentamidine Pentamidine isethionate Piretanide Psychotridine Transcrocetin (saffron) Unsorted: Allosteric modulators: AGN-241751 See also: Receptor/signaling modulators Metabotropic glutamate receptor modulators Glutamate metabolism/transport modulators v t e Metabotropic glutamate receptor modulators Group I mGluR1Tooltip Metabotropic glutamate receptor 1 Agonists: ACPD DHPG Glutamate Ibotenic acid Quisqualic acid Ro01-6128 Ro67-4853 Ro67-7476 VU-71 Theanine Antagonists: BAY 36-7620 CPCCOEt Cyclothiazide LY-367,385 LY-456,236 MCPG NPS-2390 mGluR5Tooltip Metabotropic glutamate receptor 5 Agonists: ACPD ADX-47273 CDPPB CHPG DFB DHPG Glutamate Ibotenic acid Quisqualic acid VU-1545 Antagonists: CTEP DMeOB LY-344,545 Mavoglurant MCPG NPS-2390 Remeglurant SIB-1757 SIB-1893; Negative allosteric modulators: AZD9272 Basimglurant Dipraglurant Fenobam GRN-529 MPEP MTEP Raseglurant Group II mGluR2Tooltip Metabotropic glutamate receptor 2 Agonists: BINA CBiPES DCG-IV Eglumegad Glutamate Ibotenic acid LY-379,268 LY-404,039 (pomaglumetad) LY-487,379 LY-566,332 MGS-0028 Pomaglumetad methionil (LY-2140023) Talaglumetad; Positive allosteric modulators: JNJ-40411813 (ADX-71149) Antagonists: APICA CECXG EGLU HYDIA LY-307,452 LY-341,495 MCPG MGS-0039 PCCG-4; Negative allosteric modulators: Decoglurant RO4491533 mGluR3Tooltip Metabotropic glutamate receptor 3 Agonists: CBiPES DCG-IV Eglumegad Glutamate Ibotenic acid LY-379,268 LY-404,039 (pomaglumetad) LY-487,379 MGS-0028 Pomaglumetad methionil (LY-2140023) Talaglumetad Antagonists: APICA CECXG EGLU HYDIA LY-307,452 LY-341,495 MCPG MGS-0039; Negative allosteric modulators: Decoglurant RO4491533 Group III mGluR4Tooltip Metabotropic glutamate receptor 4 Agonists: Glutamate L-AP4 LSP2-9166 PHCCC VU-001,171 VU-0155,041; Positive allosteric modulators: Foliglurax MPEP Antagonists: CPPG MAP4 MPPG MSOP MTPG UBP-1112 mGluR6Tooltip Metabotropic glutamate receptor 6 Agonists: Glutamate L-AP4 Antagonists: CPPG MAP4 MPPG MSOP MTPG UBP-1112 mGluR7Tooltip Metabotropic glutamate receptor 7 Agonists: AMN082 Glutamate L-AP4 LSP2-9166 Antagonists: CPPG MAP4 MMPIP MPPG MSOP MTPG UBP-1112 XAP044; Negative allosteric modulators: ADX71743 mGluR8Tooltip Metabotropic glutamate receptor 8 Agonists: DCPG Glutamate L-AP4; Positive allosteric modulators: AZ12216052 Antagonists: CPPG MAP4 MPPG MSOP MTPG UBP-1112 See also: Receptor/signaling modulators • Ionotropic glutamate receptor modulators • Glutamate metabolism/transport modulators

Category:AMPA receptor antagonists Category:Ion channel toxins Category:Kainate receptor antagonists Category:Polyamines