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Dopamine drugs prolonging action

MAO inhibitors (MAOIs) These drugs (eg, phenelzine, tranylcypromine, isocarboxazid) are stmcturally related to amphetamines and are orally active. They inhibit both MAO-A (which metabolizes norepinephrine, serotonin, and tyramine) and MAO-B (which metabolizes dopamine). Tranylcypromine is the fastest in onset of effect but has a shorter duration of action (about a week) than do other MAO inhibitors (with durations of 2-3 weeks). In spite of these prolonged actions, the MAO inhibitors are given daily. These drugs are inhibitors of hepatic drug-metabolizing enzymes and cause many drug interactions. [Pg.270]

These drugs are thought to prolong the effect of levodopa by blocking an enzyme, catechol-O-methyltransferase (COMT), which eliminates dopamine. When given with levodopa, the COMT inhibitors increase the plasma concentrations and duration of action of levodopa... [Pg.268]

As drugs of mixed action, amphetamines activate adrenergic receptors and simultaneously release endogenic catecholamines (norepinephrine and dopamine) from neurons of the brain and periphery. Sympathomimetic effects on the periphery are very similar to those of ephedrine. Amphetamine elevates systolic and diastolic blood pressure and has weakly expressed, broncholytic action. These effects are more prolonged, yet less expressed, than with epinephrine. The distinctive feature of amphetamines is their psychostimulatory activity. Larger doses can cause hallucinations and mental conditions similar to paranoid schizophrenia. As a sympathomimetic, amphetamine is sometimes used for uterine inertia. Synonyms of amphetamine are phenamine and benzedrine. [Pg.158]

Most antipsychotic drugs are highly lipid-soluble and protein-bound (92-99%). They tend to have large volumes of distribution (usually more than 7 L/kg). They generally have a much longer clinical duration of action than would be estimated from their plasma half-lives. This is paralleled by prolonged occupancy of D2 dopamine receptors in the brain by the typical antipsychotic drugs. [Pg.629]

Both approaches are effective in therapy and may usefully be combined. It therefore comes as no surprise that drugs which prolong the action of acetylcholine (anticholinesterases) or drugs which deplete dopamine stores (reserpine) or block dopamine receptors (antipsychotics, e.g. chlorpromazine) will exacerbate the symptoms of parkinsonism or induce a parkinson-like state. [Pg.423]


See other pages where Dopamine drugs prolonging action is mentioned: [Pg.273]    [Pg.165]    [Pg.338]    [Pg.471]    [Pg.90]    [Pg.33]    [Pg.221]    [Pg.247]    [Pg.317]    [Pg.84]    [Pg.248]    [Pg.54]    [Pg.715]    [Pg.251]    [Pg.22]    [Pg.31]    [Pg.221]    [Pg.247]    [Pg.181]    [Pg.103]    [Pg.96]    [Pg.98]    [Pg.165]    [Pg.338]    [Pg.251]    [Pg.532]    [Pg.611]    [Pg.567]    [Pg.191]    [Pg.310]    [Pg.70]    [Pg.421]    [Pg.837]    [Pg.254]    [Pg.22]    [Pg.31]    [Pg.221]    [Pg.41]    [Pg.96]    [Pg.139]    [Pg.250]    [Pg.154]    [Pg.165]   
See also in sourсe #XX -- [ Pg.423 ]




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