What s new in Mental Health?

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What s new in Mental Health? Sheri Andrews BSc.(Pharm) MSc.(EBP) Mental Health Program SERHA (RHA B) CSHP-NB AGM 2008 May 24, 2008 Countdown to delivery: 155 days Objectives Highlight new medications available for treating mental illness, including duloxetine (Cymbalta ) and ziprasidone (Zeldox ). Assess options for switching pharmacological treatment for psychosis and depression Review risks and benefits of smoking cessation options with respect to patients with mental illness. Case 1 LB has recently started treatment with paroxetine (titrated to 40 mg/d over 2 months) for an episode of MDD. She notes improvement in some symptoms such as sleep and anxiety but wishes to achieve greater improvement in her mood. As well, she has experienced decreased libido since starting paroxetine. LK inquires about the benefits of Cymbalta (duloxetine). duloxetine New antidepressant available in Canada Indicated for major depressive disorder (MDD) and neuropathic pain associated with diabetic peripheral neuropathy Acts as a SNRI, similar to venlafaxine (serotonin and norepinephrine) duloxetine Duloxetine: drug interactions Taken once daily (60 mg) Drug Effect Mechanism Very important to take with food initially Fluvoxamine duloxetine 1A2 inhibition Marketing: fast onset, immediate dual action, low incidence sexual dysfunction Ciprofloxacin Paroxetine duloxetine duloxetine 1A2 inhibition 2D6 inhibition Substrate of: 2D6 and 1A2 Triptans Serotonin syndrome Additive effect Inhibitor of: 2D6 (moderate), 1A2 (potential, based on in vitro studies) Warfarin Smoking INR duloxetine Not stated? 1A2 induction Alcohol Liver injury? 1

Efficacy vs. antidepressants Efficacy: paroxetine vs duloxetine SNRI vs. SSRI: No studies adequately powered to detect differences between paroxetine and duloxetine. 10,11,12 SNRI vs. SNRI: More patients treated with venlafaxine (150 mg/d) completed the study (P< 0.038) and more patients treated with duloxetine (60mg/d) experienced adverse effects (P< 0.032) 13 Study Detke 2004 10 Goldstein 2004 11 Perahia 2006 12 Outcome Response rate (50% HAMD) at 8 wks Total HAMD score (8 wks) Change in HAMD (8 wks) Results Placebo 44% Duloxetine 80 mg/d 65% Duloxetine 120 mg/d 71% Paroxetine 20 mg/d 74% Duloxetine 80 mg/d more effective than paroxetine 20 mg/d; caution re: dose and lack of power Both doses of duloxetine (80 and 120 mg/d) better than placebo (P<0.05); paroxetine no sig. diff from placebo (P=0.089) Tolerability: sexual dysfunction Tolerability: duloxetine Detke 10 Goldstein 11 Perahia 12 Perahia 12 8 weeks 8 weeks 8 weeks 6 months Duloxetine 46.5% Paroxetine 62.8% (P=NS) Placebo 16.7% Duloxetine 28.6% Paroxetine 34.4% (P=NS) Placebo 9.6% Duloxetine 80 mg/d 63.1%** Duloxetine 120 mg/d 30.1% Paroxetine 64.1%** P<0.05, vs. placebo Placebo 24.7% Duloxetine 80 mg/d 25% Duloxetine 120 mg/d 20.7% Paroxetine 24.7% Common adverse effects include: Nausea (take with food!) Insomnia Dizziness Caution with elevated blood pressure and liver dysfunction, alcohol use Making the switch To switch from a SSRI to a SNRI, no washout is required but a taper is recommended. 9 Should decrease the 1 st drug over 3-7 days, then initiate the 2 nd drug (consider lower dose). Individualize based on individual concern of relapse, intolerance, safety. Making the switch Consider (not only 1 way to make switch): paroxetine to 30 mg/d for 3 days paroxetine to 20 mg/d + duloxetine 30 mg/d (reduced dose) for 7 days Discontinue paroxetine and duloxetine to 60 mg/d. Monitor for serotonin side effects (e.g. nausea, vomiting, ) 2

Case 2 DM is a 45 year male with a history of paranoid schizophrenia. He is currently treated with olanzapine (30 mg/d); recent blood work reveals elevated glucose (Hb A1C =7.9%; FPG=7.4mmol/L) and cholesterol (total=6.2 mmol/l; LDL=4.5mmol/L; TG=1.97mmol/L). Though DM s symptoms improved, his psychiatrist wishes to change treatment to ziprasidone due to metabolic concerns. ziprasidone New atypical antipsychotic available in Canada Indicated for treatment of schizophrenia and related psychotic disorders Dosed twice daily (40-160 mg/d) Less weight gain and risk of increased cholesterol Can increase QT c interval significance?? Adverse effects: Somnolence (14%) ziprasidone Extrapyramidal side effects (14%) Respiratory tract infection (8%) Hypotension Dry mouth Dizziness ziprasidone Mechanism D 2 and 5HT 2 antagonism (therapeutic effect) H 1 antagonism (somnolence) α 1 antagonism (orthostatic hypotension) Drug interactions Substrate: 3A4 and 1A2 (minor pathway) Ziprasidone: drug interactions Drug Carbamazepine Valproate, lamotrigine Oral contraceptive Lithium Alcohol smoking Effect ziprasidone? No effect No effect Additive sedation No significant effects Mechanism 3A4 induction Not studied Note: only 40 mg/d studied Consider cardiac conduction changes Caution with CNS depressants Consider 1A2 pathway minor Efficacy: olanzapine vs. ziprasidone Studies ranging from 6-28 weeks indicate comparable efficacy between olanzapine and ziprasidone with a trend toward greater efficacy for olanzapine treatment Results dependent on dose (OLZ 15 or 20 mg/d), sponsor (Lilly vs. Pfizer), and outcome (depressive symptoms ). 1,2,3,4 3

Safety: olanzapine vs. ziprasidone Glucose Short studies (6-8 weeks): olanzapine group experiences increased insulin levels or Hb AIC 1,4 Longer studies (28 wks): NO significant difference between olanzapine and ziprasidone 2,3 Case reports: Diabetes associated with ziprasidone 5 and olanzapine-induced hyperglycemia resolving after switch to ziprasidone reported. 6 Safety: olanzapine vs. ziprasidone Cholesterol Significant increases in cholesterol, triglycerides, and weight have been observed with olanzapine (vs. ziprasidone). 1,2,3,4 Significant decreases in total cholesterol and triglycerides were observed 6 weeks after switch to ziprasidone from other antipsychotics, independent of weight changes (n=37). 7 Safety: Cardiac Risk A 6 week, double-blind trial reported that MEN treated with olanzapine had a mean increase of 7.69% in their Framingham risk score (FRS) vs. a decrease of 11% in patients treated with ziprasidone. (P=0.09). Women did not demonstrate a significant difference, though there was a trend favoring treatment with ziprasidone. 8 4 options 9 Making the switch Washout/start: increased risk of relapse Stop/start: risk of relapse and withdrawal symptoms. Consider if serious adverse effect from drug #1. Cross-taper over 1-4 weeks: increased risk of adverse effects; can be expensive. Delayed withdrawal: Start 2 nd drug (therapeutic dose) prior to decreasing 1 st drug Another atypical antipsychotic: paliperidone (Invega ) Active metabolite of risperidone; No direct comparisons to risperidone. Available as oral tab; IM (depot) formulation in future? Efficacy: doses greater than 3 mg/d comparable to olanzapine 10 mg/d 16 tachycardia and prolactin compared to placebo Back to DM Cardiac risk factors: 1) Male gender X 2) Increased age 3) Diabetes X 4) Smoking status X 5) Cholesterol level X Less weight gain than olanzapine 4

Options for smoking cessation Cold turkey Nicotine replacement Varenicline (Champix ) Cigarette smoking Can induce CYP 1A2 9 Decrease clozapine * levels by % Decrease olanzapine levels by % Caution if client stops smoking during therapy. Increased risk of toxicity from antipsychotic agent. *clozapine levels not routinely ordered Varenicline (Chantix ) NOT tested in patients with mental illness By Nov 2007, Health Canada had received notice of 46 psychiatric adverse reactions attributed to varenicline. 15 Fourteen of these included depression and suicidal thinking or tendencies. In some cases, the patient had a history of depression. 15 Varenicline (Champix ) Public Health Advisory Important Information on Chantix (varenicline) FDA is issuing this public health advisory to alert patients, caregivers, and healthcare professionals to important changes to Chantix prescribing information. Chantix is a medicine used to help patients stop smoking. At the request of FDA, Pfizer, the manufacturer of Chantix, has updated the Chantix prescribing information to include warnings about the possibility of severe changes in mood and behavior in patients taking Chantix. FDA is highlighting the following related important safety information on Chantix: Patients should tell their doctor about any history of psychiatric illness prior to starting Chantix. Chantix may cause worsening of a current psychiatric illness even if it is currently under control and may cause an old psychiatric illness to reoccur. http://www.fda.gov/cder/drug/advisory/varenicline.htm (last accessed May 13, 2008) Varenicline (Chantix ) Healthcare professionals, patients, patients families, and caregivers should be alert to and monitor for changes in mood and behavior in patients treated with Chantix. Symptoms may include anxiety, nervousness, tension, depressed mood, unusual behaviors and thinking about or attempting suicide. In most cases, neuropsychiatric symptoms developed during Chantix treatment, but in others, symptoms developed following withdrawal of varenicline therapy. Patients taking Chantix should immediately report changes in mood and behavior to their doctor. Patients taking Chantix may experience vivid, unusual, or strange dreams. Patients taking Chantix may experience impairment of the ability to drive or operate heavy machinery. While Chantix has demonstrated clear evidence of efficacy, it is important to consider these safety concerns and alert patients that they are possible. http://www.fda.gov /cder/drug/adv isory/v arenicline.htm (last accessed May 13, 2008) Summary New options for treatment of: Depression: duolxetine Psychosis: ziprasidone, paliperidone Switching treatment requires individual approach Pateints with mental illness may not be included in trials assessing new meds caution. 5

1) Simpson GM, Glick ID, Weiden PJ, Romano SJ, Siu CO. Randomized, controlled, double-blind multicenter comparison of the efficacy and tolerability of ziprasidone and olanzapine in acutely ill inpatients with schizophrenia or schizoaffective disorder. Am J psychiatry 2004; 161:1837-47. 2) Simpson GM, Weiden P, Pigott T, Murray S, Siu CO. Six-month blinded, multicenter continuation study of ziprasidone versus olanzapine in schizophrenia. Am J Psychiatry 2005;162(8):1535-8. 3) Breier A, Berg PH, Thakore JH, Naber D, Gattaz WF. Olanzapine versus ziprasidone: results of a 28 week double-blind study in patients with schizophrenia. Am J Psychiatry 2005;162(10):1879-87. 4) Kinon BJ, Lipkovich I, Edwards SB, Adams DH, Ascher-Svanum H. A 24 week randomized study of olanzapine vs. ziprasidone in the treatment of schizophrenia or schizoaffective disorder in patients with prominent depressive symptoms. J Clin Psychopharmacology 2006;26(2):157-62. 5) Sanchez-Barranco P. New onset of diabetes mellitus with ziprasidone: A case report. J Clin Psychiatry 66(2):268-9. 6) Spivak B, Alamy SS, Jarskog LF, Sheitman BB, Lieberman JA. Ziprasidone alternative for olanzapine-induced hyperglycemia. Am J Psychiatry 2002;159(9):1606. 7) Kingsbury SJ, Fayek M, Trufasiu D, Zada J, Simpson GM. The apparent effects of ziprasidone on plasma lipids and glucose. J Clin Psychiatry 2001;62(5):347-9. 8) Del Valle MC, Loebel AD, Murray S, Yang R, Harrison DJ. Change in framingham risk score in patients with schizophrenia: a post hoc analysis of a randomized, double-blind, 6-week trial of ziprasidone and olanzapine Prim Care Companion J Clin Psychiatry. 2006;8(6):329-33 9) Bezchlibnyk-Butler KZ, Jeffries JJ, Virani AS (Eds.) Clinical Handbook of Psychotropic Drugs (2007). Hogrefe & Huber Publishers, 17 th ed. 10) Detke MJ, Wiltse CG, Mallinckrodt CH, McNamara RK, Demitrack MA. Duloxetine in the acute and long-term treatment of major depressive disorder: a placebo- and paroxetine-controlled trial. European Neuropsychopharmacology 2004;14:457-70. 11) Goldstein DJ, Lu Y, Detke MJ, Wiltse C, Mallinckrodt C. Duloxetine in the treatment of depression: A double-blind placebocontrolled comparison with paroxetine. J Clin Psychopharmacology 2004;24(4):389-99. 12) Perahia DGS, Wang F, Mallinckrodt CH, Walker DJ, Detke MJ. Duloxetine in the treatment of major depressive disorder: a placebo- and paroxetine-controlled trial. European Psychiatry 2006;21:367-78. 13) Perahia DGS, Pritchett YL, Kajadasz DK, Bauer M, Jain R. A randomized, double-blind comparison of duloxetine and venlafaxine in the treatment of patients with major depressive disorder. J Psychiatric Research 2008;42:22-34. 14) Framingham risk reference 15) Canadian Adverse Reaction Newsletter Volume 18 Issue 2 April 2008 16) Nussbaum A. Paliperidone for schizophrenia. Cochrane Database Syst Rev. 2008 Apr 16;(2):CD006369 Thank you! 6