Effects of N-propargyl-1-(R)aminoindan (rasagiline)
in models of motor and
cognition disorders
by
Speiser Z, Levy R, Cohen S
Department of Physiology and Pharmacology,
Tel Aviv University, Israel.
J Neural Transm Suppl 1998; 52:287-300
ABSTRACT
N-propargyl-1-(R)aminoindan (rasagiline) is a new and selective irreversible
MAO-B inhibitor, currently being considered as the mesylate salt for potential
therapy in certain neurological disorders. It has been studied in animal models
of cognition and motor dysfunction. Its ability to restore normal motor activity
was determined in models of acute drug-induced dopaminergic dysfunction: Its
effects in improving cognition and memory deficits was studied in adult and
senescent rats that had been exposed to prolonged hypoxia, then subjected to the
passive and active avoidance tests. In alpha-methyl-p-tyrosine
(alpha-MpT)-induced hypokinesia (100-120 mg/kg, i.p.) pretreatment with
rasagiline at 2.5 mg/kg i.p. restored motor activity to control level. But
pretreatment with reserpine abolished the protective effect of rasagiline.
Rasagiline at 0.5 mg/kg/day was protective against alpha-MpT also in
hypoxia-lesioned rats. In haloperidol-induced catalepsy in rats (1.5 mg/kg,
s.c.) or mice (4-6 mg/kg s.c.), rasagiline improved recovery of normal
locomotion, gait and coordination at 0.4-2.4 mg/kg i.p. and 1.8-1.5 mg/kg i.p.,
respectively. In amphetamine-induced stereotypy (0.6 mg/kg s.c., rasagiline
potentiated this effect at 1.5 mg/kg i.p. In hypoxia-induced impairment of
memory and learning, rasagiline at 0.32-0.5 mg/kg/day per os improved
performance of adult rats in passive and active avoidance, and of senescent rats
in active avoidance. Selegiline was either ineffective or less effective at
equivalent doses. Racemic N-propargyl-1-aminoindan (AGN-1135), besides being of
lower potency, had a different dose-dependency than rasagiline in antagonizing
haloperidol-induced catalepsy or alpha-MpT-induced hypokinesia. 1-(R)aminoindan
((R)AI), a metabolite of rasagiline, in relatively high doses produced effects
that were distinct in certain respects from those of rasagiline.
MAO
Piribedil
Selegiline
Levodopa
Dopamine
Rasagiline
Amphetamines
Rasagiline.com
Propargylamines
Rasagiline: prospects
Imidazolines and MAO-b
Rasagiline and the amines
Parkinson's disease and depression
Refs
HOME
HedWeb
Future Opioids
BLTC Research
Paradise-Engineering
Utopian Pharmacology
The Hedonistic Imperative
When Is It Best To Take Crack Cocaine?
The Good Drug Guide
The Responsible Parent's Guide
To Healthy Mood Boosters For All The Family