Prolonged analgesia induced by cathinone.
The role of stress and opioid and
nonopioid mechanisms
by
Nencini P, Ahmed AM, Anania MC, Moscucci M, Paroli E
Pharmacology 1984; 29(5):269-81
ABSTRACT
Cathinone, the active principle of Catha edulis (khat), shows long-lasting
analgesic effects when the tail-flick test is used in rats. The involvement of
monoamines, endogenous opioids and stress in this analgesic effect was tested.
Both early (30 min) and late (24 h) analgesic effects of cathinone were
prevented by reserpine or p-chlorophenylalanine, which deplete catecholamines or
serotonin, respectively, and by nomifensine, which prevents neuronal uptake of
biogenic amines and amphetamines. The same inhibitory effect was obtained with a
high dose (4 mg/kg) of naloxone. However, rats made tolerant to morphine
retained both early and late analgesic response to cathinone. The increase in
plasma ACTH induced by the tail-flick test at 30 min and 24 h was significantly
enhanced by cathinone, in a naloxone-reversible way. However, the analgesic
responses shown at these times were not prevented by either dexamethasone or
adrenalectomy. We conclude that the prolonged analgesia induced by cathinone is
primarily due to an amphetamine-like activation of monoaminergic pathways, but
requires the integrity of non-mu-opioid mechanisms. The involvement of the
adrenohypophyseal axis in this cathinone effect is less probable.
Khat
Coffee
Opioids
Insomnia
Adenosine
Ephedrine
Khat-chewing
Khat in Yemen
Amphetamines
Methylphenidate
Qat/khat in the UK
Methcathinone: structure
Hypersomnia and depression
Excessive daytime sleepiness
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