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By S.Bohlooli PhD  Neuroleptic: synonym for antipsychotic drug; originally indicated drug with antipsychotic efficacy but also neurologic (extrapyramidal motor) side effects  Typical neuroleptic: older agents fitting this description  Atypical neuroleptic: newer agents: antipsychotic efficacy with reduced or no neurologic side effects  TYPICAL NEUROLEPTICS:  PHENOTHIAZINES:  Chlorpromazine  Thioridazine  Fluphenazine  THIOXANTHENE  Thiothixene  BUTYROPHENONES  Haloperidol  ATYPICAL NEUROLEPTICS:  Risperidone  Clozapine  Olanzapine  Quetiapine  All neuroleptics are equally effective in treating psychoses, including schizophrenia, but differ in their tolerability.  All neuroleptics  block one or more types of DOPAMINE receptor, but differ in their other neurochemical effects.  show a significant delay before they become effective.  produce significant adverse effects.  The older, typical neuroleptics are effective antipsychotic agents with neurologic side effects involving the extrapyramidal motor system.  Typical neuroleptics block the dopamine-2 receptor.  Typical neuroleptics do not produce a general depression of the CNS, e.g. respiratory depression  Abuse, addiction, physical dependence do not develop to typical neuroleptics.  Typical neuroleptics are generally more effective against positive (active) symptoms of schizophrenia than the negative (passive) symptoms. thought disturbances, delusions, hallucinations  Positive/active symptoms include social withdrawal, loss of drive, diminished affect, paucity of speech. impaired personal hygiene  Negative/passive symptoms include  All appear equally effective; choice usually based on tolerability of side effects  Most common are haloperidol ,chlorpromazine and thioridazine  Latency to beneficial effects; 4-6 week delay until full response is common  70-80% of patients respond, but 30-40% show only partial response  Relapse, recurrence of symptoms is common ( approx. 50% within two years).  Noncompliance is common.  Adverse effects are common.  Anticholinergic (antimuscarinic) side effects:  Dry mouth, blurred vision, tachycardia, constipation, urinary retention, impotence  Antiadrenergic (Alpha-1) side effects:  Orthostatic hypotension , reflex tachycardia  Sedation  Antihistamine effect: sedation, weight gain DOPAMINE-2 RECEPTOR BLOCKADE IN THE BASAL GANGLIA RESULTS IN EXTRAPYRAMIDAL MOTOR SIDE EFFECTS (EPS).  DYSTONIA  NEUROLEPTIC MALIGNANT SYNDROME  PARKINSONISM  TARDIVE DYSKINESIA  AKATHISIA  Increased prolactin secretion (common with all; from dopamine blockade)  Weight gain (common, antihistamine effect?)  Photosensitivity (v. common w/ phenothiazines)  Lowered seizure threshold (common with all)  Leukopenia , agranulocytosis (rare; w/ phenothiazines)  Retinal pigmentopathy (rare; w/ phenothiazines)  Chlorpromazine and thioridazine produce marked autonomic side effects and sedation; EPS tend to be weak (thioridazine) or moderate (chlorpromazine).  Haloperidol, thiothixene and fluphenazine produce weak autonomic and sedative effects, but EPS are marked.  DOPAMINE-2 receptor blockade in meso- limbic and meso-cortical systems for antipsychotic effect.  DOPAMINE-2 receptor blockade in basal ganglia (nigro-striatal system) for EPS  DOPAMINE-2 receptor supersensitivity in nigrostriatal system for tardive dyskinesia  Dopamine neurons reduce activity.  Postsynaptic D-2 receptor numbers increase (compensatory response).  When D2 blockade is reduced, DA neurons resume firing and stimulate increased # of receptors >> hyperdopamine state >> tardive dyskinesia  Dystonia and parkinsonism: anticholinergic antiparkinson drugs  Neuroleptic malignant syndrome: muscle relaxants, DA agonists, supportive  Akathisia: benzodiazepines, propranolol  Tardive dyskinesia: increase neuroleptic dose; switch to clozapine  Adjunctive in acute manic episode  Tourette’s syndrome (Haloperidole )  Control of psychosis in depressed patient  Phenothiazines are effective anti-emetics,  Esp. prochlorperazine  Also, anti-migraine effect  Effective antipsychotic agents with greatly reduced or absent EPS, esp. reduced Parkinsonism and tardive dyskinesia  All atypical neuroleptics block dopamine and serotonin receptors; other neurochemical effects differ  Are effective against positive and negative symptoms of schizophrenia; and in patients refractory to typical neuroleptics  Combination of Dopamine-4 and Serotonin-2 receptor blockade in cortical and limbic areas for the “pines” like clozapine  Combination of Dopamine-2 and Serotonin-2 receptor blockade (esp. risperidone)  FDA-approved for patients not responding to other agents or with severe tardive dyskinesia  Effective against negative symptoms  Also effective in bipolar disorder  Little or no parkinsonism, tardive dyskinesia, PRL elevation, neuro-malignant syndrome; some akathisia  Blockade of alpha-1 adrenergic receptors  Blockade of muscarinic cholinergic receptors  Blockade of histamine-1 receptor  Other adverse effects;  Weight gain  Increased salivation  Increased risk of seizures  Risk of agranulocytosis requires continual monitoring  Olanzapine is clozapine without the agranulocytosis.  Same therapeutic effectiveness  Same side effect profile  Quetiapine is olanzapine without the anticholinergic effects.  Same therapeutic effectiveness  Same side effect profile  Highly effective against positive and negative symptoms  Adverse effects:  EPS incidence is dose-related  Alpha-1 receptor blockade  Little or no anticholinergic or antihistamine effects  Weight gain, PRL elevation  Use typical for:  1st acute episode w/ + or +/- symptoms  Switch to atypical if:  Breakthrough after Rx w/ typical  Use typical (depot prep) when:  Patient is noncompliant  If response is inadequate to:  Typical; switch to Atypical  Atypical; raise dose or switch to another Atypical  Typical and Atypical; switch to clozapine ®  For maintenance, lifetime Rx is required.