Etilamfetamine
Etilamfetamine, also known as N-ethylamphetamine and formerly sold under the brand names Apetinil and Adiparthrol, is a stimulant drug of the amphetamine family. It was invented in the early 20th century and was subsequently used as an anorectic or appetite suppressant in the 1950s, but was not as commonly used as other amphetamines such as amphetamine, methamphetamine, and benzphetamine, and was largely discontinued once newer drugs such as phenmetrazine were introduced.
Pharmacology
Pharmacodynamics
Monoamine releasing agent
Ethylamphetamine is a potent dopamine releasing agent in vitro, with an of 88.5nM. This is about 10-fold lower than the of dextroamphetamine. The values of ethylamphetamine for induction of norepinephrine and serotonin release were not reported. However, the values of its dextrorotatory enantiomer dextroethylamphetamine have been reported and were 44.1nM, 28.8nM, and 333nM for norepinephrine, dopamine, and serotonin, respectively. Hence, dextroethylamphetamine acts as a norepinephrine–dopamine releasing agent with weak effects on serotonin.In terms of structure–activity relationships, the potency of amphetamines as dopamine releasing agents and reuptake inhibitors decreases with increasing N-alkyl chain length. That is, the order of potency of N-alkylated amphetamines is as follows: amphetamine > methamphetamine > ethylamphetamine > propylamphetamine > butylamphetamine. Propylamphetamine is a weak dopamine reuptake inhibitor rather than releaser, whereas butylamphetamine is completely inactive as a dopamine releaser or reuptake inhibitor. The same relationship, for monoamine release and reuptake inhibition generally, has been shown with 4-methylamphetamine and its N-alkylated derivatives like 4-methylmethamphetamine and so forth.
Other actions
Ethylamphetamine is inactive as an agonist of the mouse and human trace amine-associated receptor 1, whereas findings in the case of the rat TAAR1 are conflicting. In one study, its Ki was 2,500nM and its was 880nM at the rat TAAR1, whereas its Ki and/or values at the mouse and human TAAR1 were >10,000nM. In another study however, ethylamphetamine showed very little capacity to activate the rat TAAR1.Pharmacokinetics
Ethylamphetamine can be N-dealkylated into amphetamine. As such, amphetamine may contribute to its effects in vivo.Chemistry
The molecular structure of ethylamphetamine is analogous to methamphetamine, with an ethyl group in place of the methyl group. It can also be considered a substituted amphetamine, with an ethyl group on the amphetamine backbone.Analogues of ethylamphetamine include amphetamine, methamphetamine, propylamphetamine, isopropylamphetamine, butylamphetamine, fenfluramine, dimethylamphetamine, and 3-fluoroethamphetamine, among others.