Presentation is loading. Please wait.

Presentation is loading. Please wait.

1 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital Risks of Psychotropics.

Published byAmice Moore Modified over 9 years ago

Similar presentations

Presentation on theme: "1 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital Risks of Psychotropics."— Presentation transcript:

1 1 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital Risks of Psychotropics

2 2 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital The Risks  Antidepressants  Antipsychotics  Adverse Effects  Toxicity  Significant Interactions

3 3 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital Tricyclic antidepressants  Mechanism of action –Block reuptake of noradrenaline seratonin. –Dose dependent increase in seratonin, noradrenaline and dopamine. –Also alpha blockade antihistamine actions and anticholinergic actions.  Pharmacokinetics –Highly lipid soluble –large volume of distribution –rapid absorption –Polymorphic hepatic metabolism.

4 4 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital TCAs: Pharmacokinetic Interactions Elevated [TCAs] Cimetidine Ethanal acute ingestion Haloperidol Phenothiazine Propoxyphene Fluoxetine Lower [TCAs] Chronic ethanol Barbiturates Carbamazepine Elevated [Interacting Drugs] Phenytoin Warfarin

5 5 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital TCAs: Pharmacodynamic Interactions  Decreased antihypertensive effect. –Methyldopa Clonidine –Disulfiram - acute organic brain syndrome  Classic monoamine oxidase inhibitors increase therapeutic and toxic effects of both drugs. Hypertension, delirium, seizures.

6 6 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital Toxicity in overdose  Not all are equipotent  CNS –Sedation & coma –Seizures –Anticholinergic delirium  Cardiovascular –Supraventricular and ventricular arrhythmias –Conduction defects –Sinus tachycardia –Hypotension

7 7 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital MAO-A inhibitors: Moclobemide  Mechanism –reversible competitive blockade of monoamine oxidase A enzymes decreasing breakdown of monoamines.  Pharmacokinetics l polymorphic P450 hepatic metabolism - active metabolites l half life 1 - 1½ hours l low volume of distribution l 50% protein bound l high bioavailabilty 90% with repeated doses l Inhibition of monoamine oxidase 12 to 16 hours.

8 8 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital MAO-A inhibitors: Moclobemide  Dosage –300 to 600mg per day.  Side effects –Nausea (for possibly 5%)  Drug interactions –No clear evidence for dietary restrictions. – Reduced clearance by cimetidine.

9 9 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital MAO-A inhibitors: Moclobemide  Toxicity –Minimal toxicity in overdose –CNS depression and confusion, nausea, hyperreflexia, hypotension and occasional hyperthermia.

10 10 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital Fluoxetine  Mechanism –Inhibition of presynaptic seratonin reuptake plus probably altering sensitivity to serotonin.

11 11 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital Fluoxetine  Pharmacokinetics –High bioavailability and volume of distribution –High protein binding. –P450 hepatic metabolism, less than 5% renal metabolism. –Half life of fluoxetine approximately 70 hours. –Half life of active metabolite desmethylfluoxetine 330 hours, therefore steady state concentrations take 2 to 4 weeks.

12 12 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital Fluoxetine  Efficacy –In moderate depression similar to tricyclic antidepressants –some analgesic and anorectic effects, no sedative effects or alpha effects.  Not proarrhythmic.  No evidence of psychomotor changes subjectively or objectively

13 13 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital Fluoxetine  Side effects –Approximately 20% of patients experience nervousness, insomnia or nausea. Treatment failure due to side effects approximately 5%.  Drug interaction –Kinetic: Increased concentration of TCA, carbamazepine, haloperidol, metoprolol & terfenadine  Toxicity –Minimal cardiotoxicity, ataxia, CNS depression, occasional seizures.

14 14 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital Antipsychotics:Phenothiazines and butyrophenones  Mechanism –Antipsychotic effect probably due to dopamine blockade. –Dirty drugs with alpha effects, antihistamine effects, anticholinergic effects (except haloperidol) direct membrane stabilising effects.

15 15 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital Antipsychotics:Phenothiazines and butyrophenones  Metabolism –Predominantly Polymorphic hepatic P450 enzyme metabolism. –Conjugation –High volume of distribution, long half life

16 16 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital Antipsychotics:Phenothiazines and butyrophenones  Side effects –Similar to those of tricyclic antidepressants –Attributed to dopamine blockade l Parkinsonian states l Tardive dyskinesia l Neuroleptic malignant syndrome l Acute dystonia (early) l Akathesia

17 17 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital Antipsychotics:Phenothiazines and butyrophenones –Lowered seizure threshold –Hypersensitivity reactions –Hyperpigmentation –Retinal toxicity (especially thioridazine >800mg/day) –Lowered seizure threshold for phenothiazines –Endocrine

18 18 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital Antipsychotics:Phenothiazines and butyrophenones  Drug interactions –Enzyme inducers some self induction. –Heavy smoking may decrease levels. –Antipsychotics may inhibit antidepressant metabolism. –Inhibits phenytoin metabolism.

19 19 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital Neuroleptic Malignant Syndrome  ESSENTIAL CRITERIA (need 1 of the following) –Receiving or recently received a neuroleptic drug –Receiving other dopamine antagonist (eg metoclopramide) –Recently stopped therapy with a dopamine agonist (eg levodopa)

20 20 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital Neuroleptic Malignant Syndrome  MAJOR –Fever > 37.5OC (no other cause) –Autonomic dysfunction –Extrapyramidal syndrome

21 21 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital Neuroleptic Malignant Syndrome  MINOR CRITERIA –CPK rise –Altered sensorium –Leucocytosis >15000 –Other possible cause for fever (delete leucocytosis) –Low serum iron –Therapeutic response (Sequence)

22 22 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital Neuroleptic Malignant Syndrome  TREATMENT –Withdrawal –Specific –Bromocriptine. –L-Dopa –Dantrolene. –Anticholinergics and benzodiazepines –ECT –Nifedipine

23 23 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital Neuroleptic Malignant Syndrome  Recommencement of Neuroleptics. – with caution after complete recovery from NMS

24 24 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital Clozapine –A Diebenzodizepine Antipsychotic –A Low Affinity Dopamine Antagonist –A High Affinity Serotonin Antagonist  Indications –Treatment Resistant Schizophrenia

25 25 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital Clozapine  Pharmacokinetics –Bioavailability 50% –Protein Binding 95% –Half Life 12 Hours –Hepatic Metabolism

26 26 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital Clozapine  Adverse Effects –Neuroleptic Malignanct Syndrome –Seizures 5% of Patients > 600 Mg a Day –Hypersalivation –Agranulocytosis l 0.8% In One Year (95% in First Six Months) l Increased Risk in the Elderly and Female l Increased Risk in Ashkenazi Jews

27 27 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital Clozapine  Drug Interactions –Enhance Sedation With Other Sedatives –Metabolism Inhibited by Cimetidine Leading to Clozapine Toxicity –Clozapine Metabolism Induced by Phenytoin

28 28 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital Clozapine  Overdose –Delirium, Coma, Seizures –Tachycardia, Hypotension –Respiratory Depression –Hypersalivation

29 29 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital Risperidone - a benzisoxazole derivative  Indications –schizophrenia l Negative symptoms l Movement disorders on conventional therapy  Mechanism –Low affinity D2 antagonism –High affinity 5H2 antagonism –Some alpha 1 and antihistamine effect

30 30 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital Risperidone - a benzisoxazole derivative  Pharmacokinetics –rapid absorption and high bioavailability –risperidone metabolised to 9 hydroxy resperidone –P450 to D6 half life of risperidone (fast acetylators 2-4 hours) –Half life hydroxyrisperidone (fast acetylators 27 hours) –Protein binding (albumin and alpha glycoprotein) l risperidone 88%, 9 hydroxyrisperidone 77%

31 31 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital Risperidone - a benzisoxazole derivative  Side effects –postural hypotension –weight gain –hyperprolactinaemia asthaenia  Drug interactions –pharmacodynamic l dopamine l augmented affect of TCAs and phenothiazines

32 32 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital Selectivity of antidepressants 0.001 0.01 0.1 1 10 100 1000 Nisoxetine Nomifensine Maprotiline (approx) Desipramine Imipramine Nortriptyline Amitriptyline Clomipramine Trazodone Zimelidine Fluoxetine Citalopram (approx) NA- selective Non- selective 5-HT- selective Ratio NA: 5-HT uptake inhibition

Download ppt "1 Clinical Toxicology & Pharmacology Newcastle Mater Misericordiae Hospital Risks of Psychotropics."

Similar presentations

Drugs acting on the CNSI

Drugs acting on the CNSI
Connecting Pharmacology with Therapeutics Clive Roberts.

Connecting Pharmacology with Therapeutics Clive Roberts.
Antipsychotic drugs.

Antipsychotic drugs.
Monoamine oxidase inhibitors Monoamine Oxidase Inhibitors (MAOIs) are a class of powerful antidepressant drugs. They are particularly effective in treating.

Monoamine oxidase inhibitors Monoamine Oxidase Inhibitors (MAOIs) are a class of powerful antidepressant drugs. They are particularly effective in treating.
psychoterapeutic Drugs

psychoterapeutic Drugs
Antipsychotic Drugs Department of Pharmacology Zhang Yan-mei.

Antipsychotic Drugs Department of Pharmacology Zhang Yan-mei.
Clinical Toxicology & Pharmacology, Newcastle Mater Misericordiae Hospital Relative toxicity of venlafaxine and serotonin specific reuptake inhibitors.

Clinical Toxicology & Pharmacology, Newcastle Mater Misericordiae Hospital Relative toxicity of venlafaxine and serotonin specific reuptake inhibitors.
Copyright © 2013, 2010 by Saunders, an imprint of Elsevier Inc. Chapter 32 Antidepressants.

Copyright © 2013, 2010 by Saunders, an imprint of Elsevier Inc. Chapter 32 Antidepressants.
Antidepressant agents By Bohlooli S., Ph.D. School of Medicine, Ardabil University of Medical Sciences.

Antidepressant agents By Bohlooli S., Ph.D. School of Medicine, Ardabil University of Medical Sciences.
Mosby items and derived items © 2007 by Mosby, Inc., an affiliate of Elsevier Inc. Chapter 17 Psychotherapeutic Agents.

Mosby items and derived items © 2007 by Mosby, Inc., an affiliate of Elsevier Inc. Chapter 17 Psychotherapeutic Agents.
1- Affective Psychoses: a- Mania b- Depression c- Manic-depressive illness ( bipolar affective disorder ) 2- Schizophrenia.

1- Affective Psychoses: a- Mania b- Depression c- Manic-depressive illness ( bipolar affective disorder ) 2- Schizophrenia.
Copyright © 2013, 2010 by Saunders, an imprint of Elsevier Inc. Chapter 31 Antipsychotic Agents and Their Use in Schizophrenia.

Copyright © 2013, 2010 by Saunders, an imprint of Elsevier Inc. Chapter 31 Antipsychotic Agents and Their Use in Schizophrenia.
SSRIs & Antidepressants

SSRIs & Antidepressants
Aripiprazole in the treatment of acute manic or mixed episodes in patients with bipolar I disorder:

Aripiprazole in the treatment of acute manic or mixed episodes in patients with bipolar I disorder:
Pharmacotherapy of Functional Mental Illness in the Elderly. Virupakshi Jalihal Locum Consultant Psychiatrist Cornwall Partnership NHS Foundation Trust.

Pharmacotherapy of Functional Mental Illness in the Elderly. Virupakshi Jalihal Locum Consultant Psychiatrist Cornwall Partnership NHS Foundation Trust.
for the Psychiatry Clerkship is proud to present And Now Here Is The Host... Insert Name Here.

for the Psychiatry Clerkship is proud to present And Now Here Is The Host... Insert Name Here.
1 ANTI DEPRESSANT DRUGS. 2 3 DEPRESSION INTENSE FEELINGS OF SADNESS INTENSE FEELINGS OF SADNESS HOPELESSNESS HOPELESSNESS DESPAIR DESPAIR INABILITY TO.

1 ANTI DEPRESSANT DRUGS. 2 3 DEPRESSION INTENSE FEELINGS OF SADNESS INTENSE FEELINGS OF SADNESS HOPELESSNESS HOPELESSNESS DESPAIR DESPAIR INABILITY TO.
Antidepressants & Neuroleptics Lesson 20. Unipolar Depression n Major Depressive Disorder n Extreme sadness & despair l extent & duration important n.

Antidepressants & Neuroleptics Lesson 20. Unipolar Depression n Major Depressive Disorder n Extreme sadness & despair l extent & duration important n.
Management Of Depressive Disorders Pharmacologic Treatments For Depression Copyright © 2011. World Psychiatric Association.

Management Of Depressive Disorders Pharmacologic Treatments For Depression Copyright © World Psychiatric Association.
Antipsychotic drugs. Anti-psychotic drugs The CNS functionally is the most complex part of the body, and understanding drug effects is difficult Understanding.

Antipsychotic drugs. Anti-psychotic drugs The CNS functionally is the most complex part of the body, and understanding drug effects is difficult Understanding.

Similar presentations

Ads by Google