Identification
- Generic Name
- Metocurine
- DrugBank Accession Number
- DB01336
- Background
Dimethyltubocurarinium (INN) or metocurine (USAN), also known as dimethyltubocurarine, is a non-depolarizing muscle relaxant. Patients on chronic anticonvulsant drugs are relatively resistant to metocurine. 1
- Type
- Small Molecule
- Groups
- Approved
- Structure
Structure for Metocurine (DB01336)
- Weight
- Average: 652.8189
Monoisotopic: 652.351237278 - Chemical Formula
- C40H48N2O6
- Synonyms
- Dimethylchondrocurarine
- O,O-Dimethylchondrocurarine
- External IDs
- BRN 3583380
Pharmacology
- Indication
Metocurine is a muscle relaxant.
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Prevent Adverse Drug Events TodayTap into our Clinical API for life-saving information on contraindications & blackbox warnings, population restrictions, harmful risks, & more.Avoid life-threatening adverse drug events with our Clinical API- Pharmacodynamics
Not Available
- Mechanism of action
Metocurine antagonizes the neurotransmitter action of acetylcholine by binding competitively with cholinergic receptor sites on the motor end-plate. This antagonism is inhibited, and neuromuscular block reversed, by acetylcholinesterase inhibitors such as neostigmine, edrophonium, and pyridostigmine.
Target Actions Organism ANeuronal acetylcholine receptor subunit alpha-2 antagonistHumans UMuscarinic acetylcholine receptor M2 antagonistHumans - Absorption
Not Available
- Volume of distribution
Not Available
- Protein binding
Not Available
- Metabolism
- Not Available
- Route of elimination
Not Available
- Half-life
Not Available
- Clearance
Not Available
- Adverse Effects
Improve decision support & research outcomesWith structured adverse effects data, including: blackbox warnings, adverse reactions, warning & precautions, & incidence rates. View sample adverse effects data in our new Data Library!Improve decision support & research outcomes with our structured adverse effects data.- Toxicity
Not Available
- Pathways
- Not Available
- Pharmacogenomic Effects/ADRs Browse all" title="About SNP Mediated Effects/ADRs" id="snp-actions-info" class="drug-info-popup" href="javascript:void(0);">
- Not Available
Interactions
- Drug Interactions Learn More" title="About Drug Interactions" id="structured-interactions-info" class="drug-info-popup" href="javascript:void(0);">
- This information should not be interpreted without the help of a healthcare provider. If you believe you are experiencing an interaction, contact a healthcare provider immediately. The absence of an interaction does not necessarily mean no interactions exist.
Drug Interaction Integrate drug-drug
interactions in your software1,2-Benzodiazepine The risk or severity of CNS depression can be increased when Metocurine is combined with 1,2-Benzodiazepine. Acetazolamide The risk or severity of CNS depression can be increased when Acetazolamide is combined with Metocurine. Acetophenazine The risk or severity of CNS depression can be increased when Acetophenazine is combined with Metocurine. Acetyldigitoxin The risk or severity of Cardiac Arrhythmia can be increased when Metocurine is combined with Acetyldigitoxin. Aclidinium The risk or severity of adverse effects can be increased when Metocurine is combined with Aclidinium. - Food Interactions
- Not Available
Products
Drug product information from 10+ global regionsOur datasets provide approved product information including:dosage, form, labeller, route of administration, and marketing period.Access drug product information from over 10 global regions.- Product Ingredients
Ingredient UNII CAS InChI Key Metocurine chloride 15BE4G33H2 33335-58-9 IRPSJVWFSWAZSZ-OIUSMDOTSA-L
Categories
- Drug Categories
- Agents producing tachycardia
- Alkaloids
- Amines
- Anticholinergic Agents
- Benzylisoquinolines
- Central Nervous System Depressants
- Curare Alkaloids
- Heterocyclic Compounds, Fused-Ring
- Isoquinolines
- Muscarinic Antagonists
- Muscle Relaxants
- Muscle Relaxants, Peripherally Acting Agents
- Musculo-Skeletal System
- Neuromuscular Agents
- Neuromuscular Blocking Agents
- Neuromuscular-Blocking Agents (Nondepolarizing)
- Nicotinic Antagonists
- Onium Compounds
- Peripheral Nervous System Agents
- Quaternary Ammonium Compounds
- Tetrahydroisoquinolines
- Chemical TaxonomyProvided by Classyfire
- Description
- This compound belongs to the class of organic compounds known as diarylethers. These are organic compounds containing the dialkyl ether functional group, with the formula ROR', where R and R' are aryl groups.
- Kingdom
- Organic compounds
- Super Class
- Organic oxygen compounds
- Class
- Organooxygen compounds
- Sub Class
- Ethers
- Direct Parent
- Diarylethers
- Alternative Parents
- Tetrahydroisoquinolines / Anisoles / Aralkylamines / Alkyl aryl ethers / Tetraalkylammonium salts / Oxacyclic compounds / Azacyclic compounds / Organopnictogen compounds / Organic salts / Hydrocarbon derivatives show 1 more
- Substituents
- Alkyl aryl ether / Amine / Anisole / Aralkylamine / Aromatic heteropolycyclic compound / Azacycle / Benzenoid / Diaryl ether / Hydrocarbon derivative / Organic cation show 9 more
- Molecular Framework
- Aromatic heteropolycyclic compounds
- External Descriptors
- isoquinolines (CHEBI:6900)
- Affected organisms
- Not Available
Chemical Identifiers
- UNII
- V0M92G2U26
- CAS number
- 5152-30-7
- InChI Key
- JFXBEKISTKFVAB-AJQTZOPKSA-N
- InChI
- InChI=1S/C40H48N2O6/c1-41(2)17-15-27-22-34(44-6)36-24-30(27)31(41)19-25-9-12-29(13-10-25)47-40-38-28(23-37(45-7)39(40)46-8)16-18-42(3,4)32(38)20-26-11-14-33(43-5)35(21-26)48-36/h9-14,21-24,31-32H,15-20H2,1-8H3/q+2/t31-,32+/m0/s1
- IUPAC Name
- (1S,16R)-9,10,21,25-tetramethoxy-15,15,30,30-tetramethyl-7,23-dioxa-15,30-diazaheptacyclo[22.6.2.2^{3,6}.1^{8,12}.1^{18,22}.0^{27,31}.0^{16,34}]hexatriaconta-3,5,8(34),9,11,18(33),19,21,24,26,31,35-dodecaene-15,30-diium
- SMILES
- [H][C@@]12CC3=CC=C(OC4=C5C(CC[N+](C)(C)[C@]5([H])CC5=CC(OC6=C(OC)C=C(CC[N+]1(C)C)C2=C6)=C(OC)C=C5)=CC(OC)=C4OC)C=C3
References
- General References
- Spacek A, Neiger FX, Krenn CG, Hoerauf K, Kress HG: Rocuronium-induced neuromuscular block is affected by chronic carbamazepine therapy. Anesthesiology. 1999 Jan;90(1):109-12. [Article]
- External Links
- Human Metabolome Database
- HMDB0015429
- KEGG Compound
- C07919
- PubChem Compound
- 21233
- PubChem Substance
- 46508044
- ChemSpider
- 19961
- BindingDB
- 50237609
- 29950
- ChEBI
- 6900
- ChEMBL
- CHEMBL1259
- ZINC
- ZINC000004097448
- Therapeutic Targets Database
- DAP000352
- PharmGKB
- PA164749507
- PDBe Ligand
- CU9
- Wikipedia
- Dimethyltubocurarinium
- PDB Entries
- 3peo
Clinical Trials
- Clinical Trials Learn More" title="About Clinical Trials" id="clinical-trials-info" class="drug-info-popup" href="javascript:void(0);">
Phase Status Purpose Conditions Count
Pharmacoeconomics
- Manufacturers
- Not Available
- Packagers
- Not Available
- Dosage Forms
- Not Available
- Prices
- Not Available
- Patents
- Not Available
Properties
- State
- Solid
- Experimental Properties
- Not Available
- Predicted Properties
Property Value Source Water Solubility 6.42e-06 mg/mL ALOGPS logP 2.36 ALOGPS logP -1.8 Chemaxon logS -8 ALOGPS pKa (Strongest Acidic) 12.99 Chemaxon pKa (Strongest Basic) -3.4 Chemaxon Physiological Charge 2 Chemaxon Hydrogen Acceptor Count 4 Chemaxon Hydrogen Donor Count 0 Chemaxon Polar Surface Area 55.38 Å2 Chemaxon Rotatable Bond Count 4 Chemaxon Refractivity 211.94 m3·mol-1 Chemaxon Polarizability 73.08 Å3 Chemaxon Number of Rings 7 Chemaxon Bioavailability 1 Chemaxon Rule of Five No Chemaxon Ghose Filter No Chemaxon Veber's Rule No Chemaxon MDDR-like Rule No Chemaxon - Predicted ADMET Features
Property Value Probability Human Intestinal Absorption - 0.871 Blood Brain Barrier + 0.9597 Caco-2 permeable + 0.7462 P-glycoprotein substrate Substrate 0.8469 P-glycoprotein inhibitor I Non-inhibitor 0.6124 P-glycoprotein inhibitor II Non-inhibitor 0.82 Renal organic cation transporter Non-inhibitor 0.533 CYP450 2C9 substrate Non-substrate 0.8465 CYP450 2D6 substrate Non-substrate 0.5836 CYP450 3A4 substrate Substrate 0.6987 CYP450 1A2 substrate Non-inhibitor 0.9391 CYP450 2C9 inhibitor Non-inhibitor 0.9626 CYP450 2D6 inhibitor Non-inhibitor 0.908 CYP450 2C19 inhibitor Non-inhibitor 0.9468 CYP450 3A4 inhibitor Non-inhibitor 0.8976 CYP450 inhibitory promiscuity Low CYP Inhibitory Promiscuity 0.976 Ames test AMES toxic 0.6059 Carcinogenicity Non-carcinogens 0.9074 Biodegradation Not ready biodegradable 0.8898 Rat acute toxicity 2.7086 LD50, mol/kg Not applicable hERG inhibition (predictor I) Weak inhibitor 0.8306 hERG inhibition (predictor II) Non-inhibitor 0.6067
Spectra
- Mass Spec (NIST)
- Not Available
- Spectra
- Not Available
- Chromatographic Properties
Collision Cross Sections (CCS)
Adduct CCS Value (Å2) Source type Source [M-H]- 258.6727996 predictedDarkChem Lite v0.1.0 [M-H]- 263.7884378 predictedDarkChem Lite v0.1.0 [M-H]- 260.6469996 predictedDarkChem Lite v0.1.0 [M-H]- 245.55089 predictedDeepCCS 1.0 (2019) [M+H]+ 259.2324996 predictedDarkChem Lite v0.1.0 [M+H]+ 264.6774378 predictedDarkChem Lite v0.1.0 [M+H]+ 260.2161996 predictedDarkChem Lite v0.1.0 [M+H]+ 247.37576 predictedDeepCCS 1.0 (2019) [M+Na]+ 260.4555996 predictedDarkChem Lite v0.1.0 [M+Na]+ 264.6814378 predictedDarkChem Lite v0.1.0 [M+Na]+ 260.8482996 predictedDarkChem Lite v0.1.0 [M+Na]+ 253.08101 predictedDeepCCS 1.0 (2019)
Targets
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- Kind
- Protein
- Organism
- Humans
- Pharmacological action
- Yes
- Actions
- Antagonist
- General Function
- Drug binding
- Specific Function
- After binding acetylcholine, the AChR responds by an extensive change in conformation that affects all subunits and leads to opening of an ion-conducting channel across the plasma membrane.
- Gene Name
- CHRNA2
- Uniprot ID
- Q15822
- Uniprot Name
- Neuronal acetylcholine receptor subunit alpha-2
- Molecular Weight
- 59764.82 Da
References
- Liu M, Dilger JP: Synergy between pairs of competitive antagonists at adult human muscle acetylcholine receptors. Anesth Analg. 2008 Aug;107(2):525-33. doi: 10.1213/ane.0b013e31817b4469. [Article]
- Liu M, Dilger JP: Site selectivity of competitive antagonists for the mouse adult muscle nicotinic acetylcholine receptor. Mol Pharmacol. 2009 Jan;75(1):166-73. doi: 10.1124/mol.108.051060. Epub 2008 Oct 8. [Article]
- Groebe DR, Dumm JM, Abramson SN: Irreversible inhibition of nicotinic acetylcholine receptors by the bipinnatins. Toxin activation and kinetics of receptor inhibition. J Biol Chem. 1994 Mar 25;269(12):8885-91. [Article]
- Wang HL, Gao F, Bren N, Sine SM: Curariform antagonists bind in different orientations to the nicotinic receptor ligand binding domain. J Biol Chem. 2003 Aug 22;278(34):32284-91. Epub 2003 Jun 10. [Article]
- Chen X, Ji ZL, Chen YZ: TTD: Therapeutic Target Database. Nucleic Acids Res. 2002 Jan 1;30(1):412-5. [Article]
- Kind
- Protein
- Organism
- Humans
- Pharmacological action
- Unknown
- Actions
- Antagonist
- General Function
- G-protein coupled acetylcholine receptor activity
- Specific Function
- The muscarinic acetylcholine receptor mediates various cellular responses, including inhibition of adenylate cyclase, breakdown of phosphoinositides and modulation of potassium channels through the...
- Gene Name
- CHRM2
- Uniprot ID
- P08172
- Uniprot Name
- Muscarinic acetylcholine receptor M2
- Molecular Weight
- 51714.605 Da
References
- Son SL, Waud DR: Effects of non-depolarizing neuromuscular blocking agents on the cardiac vagus nerve in the guineapig. Br J Anaesth. 1980 Oct;52(10):981-7. [Article]
Drug created at June 30, 2007 18:07 / Updated at June 12, 2020 16:51