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298-46-4 molecular structure
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2-azatricyclo[9.4.0.0^{3,8}]pentadeca-1(11),3(8),4,6,9,12,14-heptaene-2-carboxamide

ChemBase ID: 446
Molecular Formular: C15H12N2O
Molecular Mass: 236.26858
Monoisotopic Mass: 236.09496301
SMILES and InChIs

SMILES:
O=C(N1c2c(C=Cc3c1cccc3)cccc2)N
Canonical SMILES:
NC(=O)N1c2ccccc2C=Cc2c1cccc2
InChI:
InChI=1S/C15H12N2O/c16-15(18)17-13-7-3-1-5-11(13)9-10-12-6-2-4-8-14(12)17/h1-10H,(H2,16,18)
InChIKey:
FFGPTBGBLSHEPO-UHFFFAOYSA-N

Cite this record

CBID:446 http://www.chembase.cn/molecule-446.html

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NAMES AND DATABASE IDS

NAMES AND DATABASE IDS

Names Database IDs
IUPAC name
2-azatricyclo[9.4.0.0^{3,8}]pentadeca-1(11),3(8),4,6,9,12,14-heptaene-2-carboxamide
2-azatricyclo[9.4.0.03,8]pentadeca-1(11),3(8),4,6,9,12,14-heptaene-2-carboxamide
2-azatricyclo[9.4.0.03,8]pentadeca-1(15),3,5,7,9,11,13-heptaene-2-carboxamide
2-azatricyclo[9.4.0.0^{3,8}]pentadeca-1(11),3,5,7,9,12,14-heptaene-2-carboxamide
IUPAC Traditional name
carbamazepine
2-azatricyclo[9.4.0.03,8]pentadeca-1(11),3(8),4,6,9,12,14-heptaene-2-carboxamide
Brand Name
Apo-Carbamazepine
Atretol
Biston
Calepsin
Carbamazepen
Carbatrol
Carbazepine
Carbelan
Epitol
Equetro
Finlepsin
Karbamazepin
Lexin
Neurotol
Novo-Carbamaz
Nu-Carbamazepine
Sirtal
Stazepin
Stazepine
Taro-Carbamazepine
Taro-Carbamazepine Cr
Tegretal
Tegretol
Tegretol Chewtabs
Tegretol Cr
Tegretol-Xr
Telesmin
Teril
Timonil
Synonyms
Carbamezepine
carbamazepine
Carbamazepine
5-Carbamoyl-5H-dibenz[b,f]azepine
Amizepin
CBZ
Carbamazepen
Carbamazepin
G 32883
Geigy 32883
Karbamazepin
Karbelex
Karberol
NSC 169864
Atretol
Carba
Carbagamma
Carbium
Epimaz
Neurotop
Prozine
Sirtal
Teril
Timonil
Trimonil
5H-Dibenzo[b,f]azepine-5-carboxamide
Epitol
Equetro
Tegretol
Biston
Calepsin
Carbamazepine
5H-Dibenz[b,f]azepine-5-carboxamide
5H-二苯并[b,f]氮杂卓-5-甲酰胺
卡马西平
CAS Number
298-46-4
EC Number
206-062-7
MDL Number
MFCD00005073
PubChem SID
24278084
24893120
160963909
46507583
PubChem CID
2554
CHEBI ID
3387
ATC CODE
N03AF01
CHEMBL
108
Chemspider ID
2457
DrugBank ID
DB00564
KEGG ID
D00252
Unique Ingredient Identifier
33CM23913M
Wikipedia Title
Carbamazepine
Medline Plus
a682237

CALCULATED PROPERTIES

CALCULATED PROPERTIES

JChem ALOGPS 2.1
Acid pKa 15.95836  H Acceptors
H Donor LogD (pH = 5.5) 2.7660303 
LogD (pH = 7.4) 2.7660303  Log P 2.7660303 
Molar Refractivity 71.888 cm3 Polarizability 26.949377 Å3
Polar Surface Area 46.33 Å2 Rotatable Bonds
Lipinski's Rule of Five true 
Log P 2.1  LOG S -3.19 
Solubility (Water) 1.52e-01 g/l 

PROPERTIES

PROPERTIES

Physical Property Safety Information Pharmacology Properties Product Information Bioassay(PubChem)
Solubility
17.7 mg/L expand Show data source
45% (w/v) aq 2-hydroxypropyl-β-cyclodextrin: soluble29 mg/mL expand Show data source
Dimethyl Sulfoxide expand Show data source
ethanol: soluble expand Show data source
H2O: insoluble expand Show data source
Methanol expand Show data source
propylene glycol: soluble expand Show data source
Apperance
powder expand Show data source
White Solid expand Show data source
Melting Point
190-192°C expand Show data source
191-192 °C(lit.) expand Show data source
191-193°C expand Show data source
Hydrophobicity(logP)
2.3 expand Show data source
Storage Condition
-20°C expand Show data source
Refrigerator expand Show data source
Room Temperature (15-30°C) expand Show data source
RTECS
HN8225000 expand Show data source
European Hazard Symbols
Harmful Harmful (Xn) expand Show data source
MSDS Link
Download expand Show data source
Download expand Show data source
Download expand Show data source
German water hazard class
2 expand Show data source
Risk Statements
22-42/43 expand Show data source
R:22-36/37/38 expand Show data source
Safety Statements
22-36/37/39 expand Show data source
S:25-26-36/37/39 expand Show data source
GHS Pictograms
GHS07 expand Show data source
GHS08 expand Show data source
GHS Signal Word
Danger expand Show data source
GHS Hazard statements
H302-H317-H334 expand Show data source
GHS Precautionary statements
P261-P280-P342 + P311 expand Show data source
Personal Protective Equipment
dust mask type N95 (US), Eyeshields, Faceshields, Gloves expand Show data source
Storage Temperature
2-8°C expand Show data source
Admin Routes
Oral expand Show data source
Bioavailability
80% expand Show data source
Excretion
2–3% excreted unchanged in urine expand Show data source
Half Life
25–65 hours (after several doses 12–17 hours) expand Show data source
Metabolism
Hepatic—by CYP3A4, to active epoxide form (carbamazepine-10,11 epoxide) expand Show data source
Protein Bound
76% expand Show data source
Legal Status
POM (UK) expand Show data source
Rx-only (US) expand Show data source
Pregnancy Category
D (US) expand Show data source
Gene Information
human ... BZRAP1(9256), GABRA1(2554), GABRA2(2555), GABRA3(2556), GABRA4(2557), GABRA5(2558), GABRA6(2559), GABRB1(2560), GABRB2(2561), GABRB3(2562), PRNP(5621), SCN5A(6331)rat ... Scn2a1(24766), Scnn1a(25122), Scnn1g(24768), Slc6a1(79212) expand Show data source
human ... PRNP(5621), SCN5A(6331)rat ... Scn2a1(24766), Scnn1a(25122), Scnn1g(24768), Slc6a1(79212) expand Show data source
Mechanism of Action
Apparent mode of action: posttetanic potentiation inhibitor expand Show data source
Exact mechanism unknown. expand Show data source
Reduces polysynaptic responses expand Show data source
Purity
95+% expand Show data source
Salt Data
Free Base expand Show data source
Certificate of Analysis
Download expand Show data source
Download expand Show data source
Suitability
meets USP testing specifications expand Show data source
Application(s)
Anticonvulsant expand Show data source
Used to treat trigeminal neuralgia expand Show data source
Pharmacopeia Traceability
traceable to PhEur C0450000 expand Show data source
traceable to USP 1093001 expand Show data source
Empirical Formula (Hill Notation)
C15H12N2O expand Show data source

DETAILS

DETAILS

DrugBank DrugBank Selleck Chemicals Selleck Chemicals Wikipedia Wikipedia Sigma Aldrich Sigma Aldrich TRC TRC
DrugBank - DB00564 external link
Item Information
Drug Groups approved; investigational
Description An anticonvulsant used to control grand mal and psychomotor or focal seizures. Its mode of action is not fully understood, but some of its actions resemble those of phenytoin; although there is little chemical resemblance between the two compounds, their three-dimensional structure is similar. [PubChem]
Indication For the treatment of epilepsy and pain associated with true trigeminal neuralgia.
Pharmacology Carbamazepine, an anticonvulsant structurally similar to tricyclic antidepressants, is used to treat partial seizures, tonic-clonic seizures, pain of neurologic origin such as trigeminal neuralgia, and psychiatric disorders including manic-depressive illness and aggression due to dementia.
Toxicity Mild ingestions cause vomiting, drowsiness, ataxia, slurred speech, nystagmus, dystonic reactions, and hallucinations. Severe intoxications may produce coma, seizures, respiratory depression, and hypotension
Affected Organisms
Humans and other mammals
Biotransformation Hepatic
Half Life 25-65 hours
Protein Binding Carbamazepine in blood is 76% bound to plasma proteins.
External Links
Wikipedia
RxList
Drugs.com
Selleck Chemicals - S1693 external link
Research Area
Description Neurological Disease
Biological Activity
Description Carbamazepine (Carbatrol) is a sodium channel blocker with IC50 of 131 μM in rat brain synaptosomes.
Targets Sodium channel
IC50 131 μM [1]
In Vitro Carbamazepine inhibits the binding of [3H]batrachotoxinin A 20-α-benzoate (BTX-B) to a receptor site of voltage-sensitive sodium channel with IC50 of 131 μM, to decrease the activation of sodium channel ion flux in rat brain synaptosomes. Carbamazepine reduces receptor affinity due to an increased rate of ligand dissociation from the receptor-ligand complex, without altering maximal binding capacity from the scatchard analysis of BTX-B binding to synaptosome, suggesting an indirect allosteric mechanism for anticonvulsant inhibition of BTX-B binding. Carbamazepine does not alter basal 125I-labeled scorpion toxin binding to synaptosomes in the absence of batrachotoxin, but when batrachotoxin (1.25 μM) added, Carbamazepine inhibits the batrachotoxin-dependent increase in scorpion toxin binding in a concentration-dependent manner with IC50 of 260 μM mediated at the alkaloid toxin binding site, none of which affects [3H]saxitoxin binding. [1]
In Vivo Carbamazepine at 25 mg/kg significantly increases extracellular levels of striatal and hippocampal dopamine (DA), 3,4-dihydroxyphenylalanine (DOPA), 3,4-dihydroxyphenylacetic acid (DOPAC) and homovanillic acid (HVA) in a dose dependent manner, while Carbamazepine at 50 mg/kg significantly decreases total levels of striatal DA and DOPA as well as hippocampal HVA, but has no effect on total levels of striatal DOPAC and HVA nor on hippocampal DA, DOPA and DOPAC. [2] Intraperitoneal administration of Carbamazepine (~100 mg/kg)to rats produces significant increases in the cerebral cortical concentrations of neuroactive steroids and neuroactive steroids in plasma in a dose and time dependent maner with DHEA formed as a result of side chain cleavage of pregnenolone not affected. [3]
Clinical Trials Phase III has been completed in the study of comparing the efficacy and safety of Zonisamide and Carbamazepine as monotherapy, in newly diagnosed partial epilepsy.
Features Carbamazepine is a most frequently prescribed first-line drug for the treatment of partial and generalized tonic-clonic epileptic seizures.
Protocol
Kinase Assay [1]
[3H]BTX-B binding assay [3H]BTX-B binding is studied by incubating synaptosomes (1.10 mg/mL) for 30 minutes at 36 °C in the standard incubation medium containing 25 mM KCl and 105 mM choline chloride plus [3H]BTX-B (10 nM), tetrodotoxin (1 μM), scorpion toxin (0.3 or 2 μM), BSA (1 mg/mL), and varying concentrations of Carbamazepine. Nonspecific binding of [3H]BTX-B is determined in the presence of 0.3 mM veratridine. Binding reactions are initiated by the addition of 25 μL of the synaptosomal suspension to 175 μL of the reaction mixture. Samples are rapidly mixed and, following incubation (10 minutes), the reaction is stopped by the addition of 3 mL of ice-cold wash medium consisting of choline chloride (163 mM), 5 mM Hepes-Tris (pH 7.4), CaCl2 (1.8 mM), MgSO4 (0.8 mM), and BSA (1 mg/mL). The synaptosomes are immediately collected on glassfiber filters under vacuum and washed three times with 3 mL of wash medium. Filters containing trapped synaptosomes are suspended in liquid scintillation fluid, and 3H bound is determined in a liquid scintifiation spectrometer. The IC50 determination is calculated by log-probit analysis according to the method of Finney.
Animal Study [2]
Animal Models Male Wistar rats
Formulation Dissolved in saline/DMSO (50/50 vol/vol)
Doses ~100 mg/kg
Administration Injected intraperitoneally (i.p.)
References
[1] Willow M, et al. Mol Pharmacol, 1982, 22(3), 627-635.
[2] Okada M, et al. Epilepsy Res, 1997, 28(2), 143-153.
[3] Serra M, et al. Neuropharmacology, 2000, 39(12), 2448-2456.
Sigma Aldrich - C4024 external link
Biochem/physiol Actions
抗惊厥药;GABAA 受体苯二氮卓调控位点的配体。
包装
1, 5, 10, 25 g in glass bottle
Sigma Aldrich - 49939 external link
Biochem/physiol Actions
Anticonvulsant; ligand for the GABAA receptor benzodiazepine modulatory site. Sodium channel inhibitor.
Sigma Aldrich - C8981 external link
Biochem/physiol Actions
抗惊厥药;GABAA 受体苯二氮卓调控位点的配体。
Toronto Research Chemicals - C175840 external link
Used in treatment of pain associated with trigeminal neuralgia. Anticonvulsant.

REFERENCES

REFERENCES

From Suppliers Google Scholar IconGoogle Scholar PubMed iconPubMed Google Books IconGoogle Books
  • • Willow M, et al. Mol Pharmacol, 1982, 22(3), 627-635.
  • • Okada M, et al. Epilepsy Res, 1997, 28(2), 143-153.
  • • Serra M, et al. Neuropharmacology, 2000, 39(12), 2448-2456.
  • • Stenger, E.G., et al.: Med. Exp., 11, 191 (1964)
  • • Pynnonen, S., et al.: Ther. Drug Monit., 1, 409 (1964)
  • • Sidebottom, A., et al.: J. Clin. Pharm. Ther., 20, 31 (1995)
  • • Schmutz, M., Handb. Exp. Pharmacol., 1985, 74, 479, (Carbamazepine, rev)
  • • Al-Showaier, I. et al., J. Het. Chem., 1986, 23, 731, (ms)
  • • Fromm, G.H., Drugs Control Epilepsy, 1992, 425, (Carbamazepine, rev)
  • • Negwer, M., Organic-Chemical Drugs and their Synonyms, 7th edn., Akademie-Verlag, 1994, 4398, (synonyms)
  • • Antiepileptic Drugs, (Eds., Levy, R.H. et al), 4th edn., Raven Press, 1995
  • • Tokmakov, G.P. et al., Tetrahedron, 1995, 51, 2091, (synth)
  • • Martindale, The Extra Pharmacopoeia, 32nd edn., Pharmaceutical Press, 1999, 339
  • • Lewis, R.J., Sax's Dangerous Properties of Industrial Materials, 8th edn., Van Nostrand Reinhold, 1992, DCV200
  • • Aldrich Library of FT-IR Spectra, 1st edn., 1985, 2, 681B, (ir)
  • • Aldrich Library of 13C and 1H FT NMR Spectra, 1992, 2, 1451A; 3, 164A, (nmr)
  • • Huisgen, R. et al., Chem. Ber., 1960, 93, 392, (synth)
  • • Bergmann, E.D. et al., J.O.C., 1960, 25, 827, (synth)
  • • Davis, M.A. et al., J. Med. Chem., 1964, 7, 88, (Carbamazepine)
  • • Aboul-Enein, H.Y. et al., Anal. Profiles Drug Subst., 1980, 9, 87, (rev, Carbamazepine)
  • • Himes, V.L. et al., Acta Cryst. B, 1981, 37, 2242, (Carbamazepine)
  • • Sinha, A.K. et al., Indian J. Chem., Sect. B, 1982, 21, 237, (synth, Carbamazepine)
  • • Harding, M.M., Acta Cryst. C, 1983, 39, 397, (cryst struct)
  • • Molock, F.F. et al., J. Het. Chem., 1983, 20, 109, (cmr)
  • • MacKichan, J.J., Appl. Ther. Drug Monit., 1984, 2, 73, (rev, anal, Carbamazepine)
  • • Hallberg, A. et al., J. Het. Chem., 1984, 21, 197, (pmr, cmr)
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