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Download Anti-psychotic drugs 2006
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Antipsychotic drugs Anti-psychotic drugs • The CNS functionally is the most complex part of the body, and understanding drug effects is difficult • Understanding the effects of drugs on neurones does not predict the effect on the whole organ • In part this is due to complex interactions mediated by different neurotransmitters Dopamine • Important neurotransmitter • Present mainly in the nigrostriatal pathway • There are two main types of dopamine receptor: D1 and D2 . These stimulate and inhibit adenylate cyclase respectively. • D2 receptors are mainly responsible for the actions of anti-psychotic drugs Dopamine - functions • Motor control - nigrostriatal system. Deficiency results in rigidity, tremor and difficulty initiating movement • Behavioral effects - mesolimbic system. Overactivity in rats leads to abnormal behavior • Endocrine control - tubero-infundibular system. Dopamine and dopamine agonists suppress prolactin release, dopamine antagonists may stimulate it Schizophrenia - Dopamine hypothesis • Amphetamine can produce a syndrome similar to the ‘positive’ features of schizophrenia • Levodopa may aggravate the condition • Apomorphine and bromocriptine (D2 agonists) produce behavioral abnormalities in animals • D2 receptor antagonists are effective in controlling the positive features of the disorder • ? Increased D2 receptor binding in the brains of schizophrenic subjects. Evidence of genetic variation in the D4 receptor to which some anti-psychotic drugs have high affinity Anti-psychotic Drugs -5HT (serotonin) • Some drugs also act at 5-HT receptors (antagonists of 5HT2) • 5-HT has a modulatory effect on dopaminergic neurones • LSD which has mixed agonist/antagonist actions produces hallucinations and behavioral disturbance Anti-psychotic Drugs - Modes of Action • All anti-psychotic drugs have inhibitory effects on the D2 receptor • Some have actions against the D4 receptor • All have other effects - to varying degrees – Serotonin blockade (may improve negative symptoms) – Histamine H1 blockade (drowsiness) – Alpha adrenoceptor blockade (postural hypotension) How do we know they work? • mostly “accidentally” for early drugs designing drugs to reduce anxiety in surgical patients • clinical experience • clinical trials - especially more recent drugs • PET scanning showing blockade of central D2 receptors Anti-psychotic Drugs - Clinical Effects • Control the ‘positive’ features of the disease, but little effect on the ‘negative’ features (clozapine may be superior in this regard) • The main side-effects are on the extrapyramidal motor system - leading to rigidity, tremor, and loss of mobility and dyskinesia • Tardive dyskinesia is a late onset disorder characterised by repetitive abnormal movements of face and upper limbs. This may be due to proliferation of D2 receptors in the striatum Clinical Effects cont • Newer ‘atypical’ anti-psychotic drugs are less inclined to produce these effects possible due to their greater affinity for the mesolimbic over the striatal areas of the brain Anti-psychotic Drugs - Other Effects • some are effective anti-emetics • anti-muscarinic effects lead to dry mouth, blurred vision, difficulty with micturition • a antagonist effects lead to hypotension • antihistamine effects (H1 receptor) lead to drowsiness • prolactin stimulation may lead to breast development • agranulocytosis is fairly common with an ‘atypical’ drug - clozapine • ‘Neuroleptic malignant syndrome’ is a rare but serious effect leading to autonomic instability and hyperthermia Classification of anti-psychotic drugs • “classical/ typical” chlopromazine (gen) haloperidol (gen) fluphenazine (gen) thioridazine (auth) note: classification is based on fewer EPS sideeffects,fewer long-term ADRs, efficacy in treatment-resistant groups, negative symptoms • “atypical” clozapine (sec100) risperidone (auth) olanzapine (auth) quetiapine (auth) newer drugs • claims: – – – – lower doses reduced side effects more effective (especially negative symptoms) better compliance • evidence? – trials have been quite small and involved patients previously heavily treated and somewhat ‘resistant’ – trials have tended to show equivalent efficacy and better side effect profiles with newer drugs – head to head trials claimed superiority of olanzapine over risperidone (but company sponsored and controversial); some “parallel publications” • costs – Much higher with new drugs (10-40 times higher) Final Slide - summary of the actions of different anti-psychotic drugs at different receptors SEE CHAPTER 37 RANG DALE AND RITTER 5TH EDITION (NICE OVERVIEW) TABLE 37.1