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Reducing Confusion in Naming Antipsychotics: Pharmacology, Not Clinical Target for Nomenclature Stephen M. Stahl, MD, PhD Professor of Psychiatry, University of California, San Diego Honorary Senior Visiting Fellow University of Cambridge, United Kingdom Copyright © 2011 Neuroscience Education Institute. All rights reserved. Learning Objectives • To discuss how antipsychotic nomenclature can be confusing by using names based upon clinical actions • To propose nomenclature based upon pharmacologic mechanisms no matter what the clinical use • To reduce confusion by addressing: – When is an antipsychotic not an antipsychotic? – When is a non antipsychotic an antipsychotic? Copyright © 2011 Neuroscience Education Institute. All rights reserved. Question 1 • Why are antipsychotics antipsychotics? – – – – 1. Because they reduce psychosis 2. Because they block D2 dopamine receptors 3. Both 4. Neither Copyright © 2011 Neuroscience Education Institute. All rights reserved. Current Nomenclature for Conventional (First-Generation) Antipsychotics D2 • • • • • • • D2 antagonists Dopamine blockers Neuroleptics Psycholeptics Conventional antipsychotics First Generation antipsychotics Major tranquilizers Stahl SM. Stahl’s Essential Psychopharmacology. 4th Ed. Cambridge University Press, 2013. Copyright © 2011 Neuroscience Education Institute. All rights reserved. Current Nomenclature for Atypical (Second-Generation) Antipsychotics • • • • • • • • • D2/5HT2A antagonists Serotonin dopamine antagonists Antipsychotics Anti-manics Mood Stabilizers Anti-depressants Treatment resistant antidepressants Antidepressant augmenting agents Bipolar antidepressants Stahl SM. Stahl’s Essential Psychopharmacology. 4th Ed. Cambridge University Press, 2013. Copyright © 2011 Neuroscience Education Institute. All rights reserved. Muscarinic Acetylcholine Receptors: M1 M2 M3 M4 Histamine Receptors: H1 Adrenergic Alpha Receptors: 1 2A 2B 2C Transporters SERT NET D2 Dopamine Receptors: D1 Serotonin Receptors: 5HT1A 2A 5-1 1B 1D 2B 2C 1E 3 5 6 7 Copyright © 2011 Neuroscience Education Institute. All rights reserved. D2 D3 D4 Question 2 • Why are antipsychotics antidepressants? – – – – – – – 1. Because they improve depression 2. Because they block dopamine D2 receptors 3. Because of other pharmacologic actions 4. All of the above 5. None of the above 6. 1 and 2 7. 1 and 3 Copyright © 2011 Neuroscience Education Institute. All rights reserved. Lurasidone 5HT7 5-59 D4 D2 5HT 2A 2C 5HT 1A 2A 1 5HT 2C Copyright © 2011 Neuroscience Education Institute. All rights reserved. Lurasidone Axis I Class : dopamine multifunctional Relevant Mechanism: dopamine and serotonin receptor antagonist Axis 2 Indications: schizophrenia (USA, Canada, UK, Europe); major depressive episodes associated with bipolar I disorder (USA and Canada) Axis 3 Efficacy: Improvement of psychotic symptoms, improvement in depressive symptoms Side Effects: sedation, dizziness, EPS, galactorrhea (low), weight gain (low). Risk of diabetes (low) but monitoring recommended as a class warning; class warning for increased mortality in elderly dementia patients and for tardive dyskinesia and NMS Committee notes: Serotonin 7, serotonin 1A and alpha 2 actions may be relevant especially in bipolar depression Copyright © 2011 Neuroscience Education Institute. All rights reserved. Lurasidone (cont’d) Axis 4 Neurobiological description Neurotransmitter actions: Dopamine and serotonin receptor antagonist Preclinical: Antagonist at D2 and D3, 5HT2A, 5HT7, NE alpha2 receptors; partial agonist at 5HT1A receptor Human: Blocks central D2 receptors (PET; human) Physiological: Preclinical: Catalepsy, improves cognition in animal models Copyright © 2011 Neuroscience Education Institute. All rights reserved. Pimavanserin Copyright © 2011 Neuroscience Education Institute. All rights reserved. Pimavanserin • 5HT2A inverse agonist antagonist – Blocks intrinsic activity when no agonist is present and blocks the agonist when present • Recently approved for psychosis in Parkinson’s disease (PD) – Reduction in psychotic symptoms – Unlike antipsychotics, pimavanserin does not impair motor function or reduce the efficacy of L-DOPA Significant improvement on the Scale for the Assessment of Positive Symptoms –Parkinson’s Disease (SAPS-PD) Cummings et al. The Lancet 2014;383:533-40; Friedman JH. Expert Opin Pharmacother 2013;14(14):1969-75; Goldman, Holden. Curr Treat Options Neurol 2014;16:281; McFarland et al. Beh Pharmacol 2011;22:681-92; Meltzer HY et al. Neuropsychopharmacol 2010;35:881-92; Meltzer, Roth. J Clin Invest 2013;123(12):4986-91. Copyright © 2011 Neuroscience Education Institute. All rights reserved. Question 3 • If an agent like pimavanserin improves psychosis but doesn’t block D2 dopamine receptors, should it be classified as an antipsychotic? – 1. yes – 2. no Copyright © 2011 Neuroscience Education Institute. All rights reserved. Question 4 • If an agent improves psychosis but doesn’t block D2 dopamine receptors like pimavanserin, should it get class warnings for antipsychotics (weight gain, diabetes, tardive dyskinesia, NMS, mortality in elderly dementia, etc), be classified as “other antipsychotic” and be used only second line after other antipsychotics fail? – 1. yes – 2. no Copyright © 2011 Neuroscience Education Institute. All rights reserved. Question 5 If pimavanserin improves sleep and improves behavioral symptoms of dementia as well as psychosis in Parkinson’s disease what should it be called? 1. hypnotic 2. antipsychotic hypnotic 3. Parkinsonian antipsychotic 4. anti-dementia agent 5. Antipsychotic for Parkinson’s disease that is not an antipsychotic because it doesn’t block D2 receptors and doesn’t have EPS, or other warnings, thus the nonantipsychotic antipsychotic hypnotic antidementia agent Copyright © 2011 Neuroscience Education Institute. All rights reserved. Question 6 How about calling pimavanserin a selective serotonin receptor antagonist? 1. yes 2. no Copyright © 2011 Neuroscience Education Institute. All rights reserved. Summary • We propose that it is no longer appropriate to name all drugs that treat psychosis only as “antipsychotics” • A multi axial classification system is proposed to use for drugs that treat psychosis, mania and depression based on pharmacologic mechanism of action • Mechanism based nomenclature may clarify these differing mechanisms for individual agents rather than class effects for all atypical antipsychotics, especially for actions in psychosis versus mood disorders • This approach has the potential to better inform those who work with drugs that treat depression and other conditions to prevent confusion with other drugs that treat both psychosis and multiple additional disorders such as depression and sexual dysfunction • This approach is also a strategy for naming novel drugs yet to be discovered that target novel mechanisms of action Copyright © 2011 Neuroscience Education Institute. All rights reserved.
