Federal Employee Program 1310 G Street, N.W. Washington, D.C. 20005 202.942.1000 Fax 202.942.1125 Subject: Xenazine Page: 1 of 5 Last Review Date: June 12, 2014 Xenazine Description Xenazine (tetrabenazine) Background Xenazine is the first FDA approved medication for treatment of chorea associated with Huntington's disease (HD) (1). Huntington's disease is a rare inherited neurological disorder. The disease results from genetically programmed degeneration of brain cells. The deterioration causes uncontrolled movements, loss of intellectual faculties, and emotional disturbance (2). Xenazine decreases the amount of dopamine available to work at relevant synapses in the brain. Dopamine is a chemical that communicates between certain nerve cells in the brain. In patients with Huntington's disease, this system is overactive and results in the abnormal movements called chorea. Xenazine decreases the amount of dopamine available to interact with certain nerve cells, thereby decreasing the involuntary movements (2). Xenazine is a presynaptic dopamine depletor that may have considerable efficacy in tardive kyskinesia (TD), especially tardive dystonia (3,6), tic associated with Tourette s syndrome (4,6), dystonia (5), other choreas (6), and facial dystonia/dyskinesia (6). Regulatory Status FDA-approved indication: Xenazine is a vesicular monoamine transporter 2 (VMAT) inhibitor indicated for the treatment of chorea associated with Huntington s disease (1). Xenazine carries a boxed warning regarding the increased risk of depression and suicidal
Subject: Xenazine Page: 2 of 5 thoughts and behavior (suicidality) in patients with Huntington disease. The risks of depression and suicidality should be balanced with the clinical need of Xenazine therapy for the control of choreiform movements. Xenazine is contraindicated in patients who are actively suicidal, and in patients with untreated or inadequately treated depression (1). Prescribers should periodically re-evaluate the need for Xenazine in their patients by assessing the beneficial effect on chorea and possible adverse effects, including depression, cognitive decline, parkinsonism, dysphagia, sedation/somnolence, akathisia, restlessness and disability. It may be difficult to distinguish between drug induced side-effects and progression of the underlying disease; decreasing the dose or stopping the drug may help the clinician distinguish between the two possibilities. In some patients, underlying chorea itself may improve over time, decreasing the need for Xenazine (1). Xenazine is contraindicated in patients with impaired hepatic function (1). Xenazine is contraindicated in patients taking MAOIs or reserpine. Concurrent use of reserpine and xenazine may result in elevated catecholamine levels. When switching a patient from reserpine to xenazine, wait for chorea to re-emerge and at least 20 days after stopping reserpine before initiating tetrabenazine to avoid overdose and significant depletion of norepinephrine and serotonin in the CNS (1). Patients requiring doses above 50 mg per day should be genotyped for the drug metabolizing enzyme CYP2D6 to determine if the patient is a poor metabolizer (PM) or an extensive metabolizer (EM). The maximum daily dose in PMs is 50mg with a maximum single dose of 25 mg. The maximum daily dose in EMs and intermediate metabolizers (IMs) is 100mg with a maximum single dose of 37.5 mg (1). Xenazine should be avoided in patients with congenital long QT syndrome and in patients with a history of cardiac arrhythmias. Certain circumstances may increase the risk of the occurrence of torsade de pointes and/or sudden death in association with the use of drugs that prolong the QTc interval (1). Xenazine therapy should be discontinued if Neuroleptic Malignant Syndrome (NMS) develops. If treatment with Xenazine is needed after recovery from NMS, patients should be monitored for signs of recurrence (1).
Subject: Xenazine Page: 3 of 5 Related policies Policy This policy statement applies to clinical review performed for pre-service (Prior Approval, Precertification, Advanced Benefit Determination, etc.) and/or post-service claims. Xenazine may be considered medically necessary in patients with Tourette s disorder, Huntington s Chorea or other Chorea; acute dystonia due to drugs; orofacial dyskinesia; subacute dyskinesia due to drugs; or dystonia. Xenazine may be considered investigational for all other indications. Prior-Approval Requirements Diagnoses Patient must have ONE of the following: 1. Tourette's disorder 2. Huntington s Chorea 3. Other Chorea 4. Acute Dystonia Due to Drugs 5. Orofacial Dyskinesia 6. Subacute Dyskinesia Due to Drugs (Tardive Dyskinesia or TD) 7. Dystonia AND NONE of the following: 1. Actively suicidal 2. Untreated or inadequately treated depression 3. Concomitant use of a MAOI (monoamine oxidase inhibitor) or reserpine (must be >20 days post discontinuing therapy) 4. Severe hepatic impairment. Prior Approval Renewal Requirements Same as above Policy Guidelines
Subject: Xenazine Page: 4 of 5 Pre - PA Allowance None Prior - Approval Limits Quantity Duration 12.5mg - 720 tablets per 90 days 25 mg 360 tablets per 90 days 12 months Prior Approval Renewal Limits Same as above Rationale Summary Xenazine is the first FDA approved medication for treatment of chorea associated with Huntington's disease (HD). Xenazine is a presynaptic dopamine depletor that may have considerable efficacy in tardive kyskinesia (TD), especially tardive dystonia, tic associated with Tourette s syndrome, dystonia, other choreas, and facial dystonia/dyskinesia. Xenazine carries a boxed warning regarding the increased risk of depression and suicidal thoughts and behavior (suicidality) in patients. Xenazine is contraindicated in patients with impaired hepatic function and is contraindicated in patients taking MAOIs or reserpine. Prior authorization is required to ensure the safe, clinically appropriate and cost effective use of Xenazine while maintaining optimal therapeutic outcomes. References 1. Xenazine. Prescribing Information. Deerfield, IL. Lundbeck Inc. September 2012. 2. FDA News Release. FDA Approves First Drug for Treatment of Chorea in Huntington s Disease. August 15, 2008. http://www.fda.gov/newsevents/newsroom/pressannouncements/2008/ucm116936.htm 3. Tarsy D. Tardive dyskinesia. Curr Treatment Options Neurol. 2000 May;2(3): 205 214.
Subject: Xenazine Page: 5 of 5 4. Fasano, A, Bentivoglio, AR. Tetrabenazine. Expert Opin Pharmacother. 2009 Dec;10(17):2883-96. 5. Kenney C, Hunter C, Jankovic J. Long-term tolerability of tetrabenazine in the treatment of hyperkinetic movement disorders. Mov Disord. 2007 Jan;22(2):193-7. 6. Paleacu, D, Giladi, N, Moore, O, Stern, A, Honigman, S, Badarny, S. Tetrabenazine treatment in movement disorders. Clin Neuropharmacol. 2004 Sep; 27(5):230-3. Policy History Date June 2010 December 2011 December 2012 June 2014 Action The use of Xenazine to treat dyskinetic movement disorders has been demonstrated to be safe and effective. The clinical literature supports the use of Xenazine in tardive dyskinesia, chorea not associated with HD, orofacial dyskinesia and Tourette's syndrome. (3,4,5,6) Practicing neurologists consulted also report the use of Xenazine for these indications as generally accepted medical practice. Annual review Annual review Annual editorial review and reference update. Keywords This policy was approved by the FEP Pharmacy and Medical Policy Committee on June 12, 2014 and is effective July 1, 2014. Signature on File Deborah M. Smith, MD, MPH