- Phenibut
ambox
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text =This article has been summarily "reverted" by a from a [fullurl:Phenibut|oldid=199785883 prior version] due to an obvious and major [http://www.bulknutrition.com/?ingredients_id=64 copyright violation] that is contrary to the expressed wishes of the authors. It must be "re-written" if it is to return to its previous level of usefulness and quality.drugbox
IUPAC_name = 4-amino-3-phenyl-butanoic acid
CAS_number = 1078-21-3
ATC_prefix =
ATC_suffix =
PubChem = 14113
DrugBank =
synonyms = Fenibut, Phenybut, PhGABA
chemical_formula =
C=10|H=13|N=1|O=2
smiles = C1=lCC=lC(C=lC1)C(CC(=lO)O)CN
molecular_weight = 179.216 g/mol
bioavailability =
protein_bound =
metabolism =
elimination_half-life = 5 hours
excretion =
melting_point = 253
pregnancy_AU =
pregnancy_US =
pregnancy_category=
legal_AU =
legal_CA =
legal_UK =
legal_US = OTC
legal_status =
routes_of_administration = OralBeta-phenyl-gamma-aminobutyric acid, better known as Phenibut or less commonly Fenibut or Phenybut, is natural derivative of the relaxing neurotransmitter GABA (Gamma amino butyric acid). Sold as a dietary supplement in the US while in Russia sold as a neuropsychotropic drug that is capable of passing the
blood-brain barrier . Phenibut is cited as anootropic for its ability to improve neurological functions. It was discovered in Russia in the 1960's, and has since been used there to treat a wide range of ailments including anxiety and insomnia.The name Phenibut, along with many of the other names for the compound, comes directly from the chemical name for the compound, beta-phenyl-gamma-aminobutyric acid.
Structurally, phenibut is similar to
baclofen andphenethylamine , although it is not considered a phenethylamine. Phenibut is a GABAB receptor agonist, with slight activity at GABAA receptors. The pharmacological effects of phenibut are virtually identical to baclofen.Fact|date=September 2007Phenibut should be used with extreme caution as it can have unpleasant withdrawal symptoms. Side effects can include acute
anxiety andinsomnia that can last for up to two weeks afterwards. Withdrawal symptoms, however, are almost always associated with cessation after prolonged usage. Tolerance to phenibut can develop quite rapidly.Fact|date=September 2007Phenibut should never be mixed with alcohol, sedatives or prescription medication without consulting with a healthcare professional.
Persons on MAO inhibitors or epilepsy medications like
carbamazepine oroxcarbazepine should consult with their psychiatrist/physician prior to supplementation with phenibut. Clinical research has demonstrated that phenibut can potentate or inhibit the function of some epilepsy medications.Fact|date=September 2007Commonly recommended doses are 250-3,000 mg as needed or daily with weekly cycling off during weekends.
Phenibut is a phenylethylamine antagonist and thus reduces the effects of phenylethylamine and other compounds that raise phenylethylamine levels.
References
1. Pavlov J Biol Sci. 1986 Oct-Dec;21(4):129-40. On neurotransmitter mechanisms of reinforcement and internal inhibition. Shulgina GI.
2. Arch Immunol Ther Exp (Warsz). 1975;23(6):733-46. Pharmacological properties of gamma-animobutyric acid and it derivatives. IV. Aryl gaba derivatives and their respective lactams. Chojnacka-Wojcik E, Hano J, Sieroslawska J, Sypniewska M.
3. Lapin I. Phenibut (beta-phenyl-GABA): a tranquilizer and nootropic drug. CNS Drug Rev. 2001 Winter;7(4):471-81.
4. Neurosci Behav Physiol. 2003 Mar;33(3):255-61. Neurochemical characteristics of the ventromedial hypothalamus in mediating the antiaversive effects of anxiolytics in different models of anxiety. Talalaenko AN, Pankrat'ev DV, Goncharenko NV.
5. Eksp Klin Farmakol. 2002 Sep-Oct;65(5):22-6. [Monoaminergic and aminoacidergic mechanisms of the posterior hypothalamus in realization of the antiaversive effects of anxiosedative and anxioselective agents in various anxiety models] [Article in Russian] . Talalaenko AN, Pankrat'ev DV, Goncharenko NV.
6. Ross Fiziol Zh Im I M Sechenova. 2001 Sep;87(9):1217-26. [Neurochemical characteristics of the ventromedial hypothalamus and anti-aversive effects of anxiolytic agents in various anxiety models] [Article in Russian] . Talalaenko AN, Pankrat'ev DV, Goncharenko NV.
7. Ukr Biokhim Zh. 1984 Nov-Dec;56(6):637-41. [Mg2+-ATPase activity of brain mitochondria fractions in chronic stress and its correction by psychotropic agents] [Article in Russian] . Kresiun VI.
8. Farmakol Toksikol. 1991 Sep-Oct;54(5):14-6. [The adequacy of a new method for assessing the vestibular protective effect of biologically active substances] [Article in Russian] . Karkishchenko NN, Dimitriadi NA.
External links
* [http://chem.sis.nlm.nih.gov/chemidplus/jsp/common/ChemFull.jsp?MW=179.218 NLM/NIH]
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