Stereoselective accumulation of hydroxylated metabolites of amphetamine in rat striatum and hypothalamus

Stereoselective accumulation of hydroxylated metabolites of amphetamine in rat striatum and hypothalamus

1 The stereoselective accumulation of α‐methyl‐p‐tyramine (AMPT) and α‐methyl‐p‐octopamine (AMPO) in rat striatum and hypothalamus after acute and chronic administration of the (+)‐and (−)‐isomers of amphetamine (Amphet) and the acute administration of (+)‐ and (−)‐AMPT has been investigated by chem...

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Veröffentlicht in:British journal of pharmacology 1986-05, Vol.88 (1), p.285-290
Hauptverfasser: Dougan, D.F.H., Duffield, A.M., Duffield, P.H., Wade, D.N.
Format: Artikel
Sprache:eng
Schlagworte:
Amphetamine - metabolism
Amphetamine - pharmacology
Animals
Benzyl Compounds - metabolism
Biological and medical sciences
Corpus Striatum - metabolism
Half-Life
Hydroxylation
Hypothalamus - metabolism
Male
Medical sciences
Neuropharmacology
Octopamine - analogs & derivatives
Pharmacology. Drug treatments
Psychoanaleptics: cns stimulant, antidepressant agent, nootropic agent, mood stabilizer..., (alzheimer disease)
Psychology. Psychoanalysis. Psychiatry
Psychopharmacology
Rats
Stereoisomerism
Tyramine - analogs & derivatives
Tyramine - metabolism
Tyramine - pharmacology
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Zusammenfassung:1 The stereoselective accumulation of α‐methyl‐p‐tyramine (AMPT) and α‐methyl‐p‐octopamine (AMPO) in rat striatum and hypothalamus after acute and chronic administration of the (+)‐and (−)‐isomers of amphetamine (Amphet) and the acute administration of (+)‐ and (−)‐AMPT has been investigated by chemical ionization gas chromatography mass spectrometry (c.i.g.c.m.s.). 2 Two h after the administration of (+)‐ or (−)‐AMPT (5 mg kg−1 i.p.), the concentrations of the isomers in striatal tissue were approximately equal; 18 h later, the concentration of the (+)‐isomer was 10 times that of the (−)‐isomer. 3 The concentrations of AMPO in the striatum and hypothalamus 20 h after administration of (+)‐AMPT were 68 ng g−1 and 484 ng g−1 respectively. After the administration of the (−)‐isomer of AMPT, small quantities of AMPO were detected in both brain areas. 4 Twenty h after the last of 7 daily injections of (+)‐Amphet (5 mg kg−1, i.p.), the concentration of AMPO in the hypothalamus was 5.4 times the concentration at 20 h after one injection. In the striatum, the corresponding ratio for AMPO was 3.5 and for AMPT was 2.5. 5 These data indicate that, although both isomers of AMPT formed from Amphet administered systemically, cross the blood brain barrier, the (+)‐isomers AMPT and AMPO are preferentially stored in striatal and hypothalamic aminergic nerve terminals. 6 The accumulations of AMPT and AMPO in rat striatum and hypothalamus after chronic administration of Amphet demonstrates that these metabolites persist in neuronal storage in these brain areas for days after administration. The half‐lives of (+)‐AMPT and (+)‐AMPO in striatal neuronal storage, calculated from this data, were 1.5 days and 2.5 days, respectively. The corresponding half‐life for hypothalamic (+)‐AMPO was 7 days. 7 These findings suggest the involvement of accumulated AMPT and AMPO in the development of behavioural augmentation to repeated injections of Amphet (Randrup & Munkvad, 1970).
ISSN:0007-1188
1476-5381
DOI:10.1111/j.1476-5381.1986.tb09497.x