Volume 21 | March 2026

Patient-Forward Approaches for Tardive Dyskinesia: From Differential Diagnosis to Appropriate Treatment

EXPERT COMMENTARY
Expert Commentary With Henry Nasrallah, MD, and Daniel Dees, MD
Expert Commentary With Henry Nasrallah, MD, and Daniel Dees, MD
This newsletter is produced by Teva Pharmaceuticals. Drs Henry Nasrallah and Daniel Dees were compensated by Teva for their insights.
Antipsychotics are an essential treatment option for patients with psychotic and/or mood disorders, but it is equally important to recognize that these medications and other dopamine receptor blocking agents (DRBAs) can cause drug-induced movement disorders (DIMDs), including acute dystonia, acute akathisia, drug-induced parkinsonism (DIP), and tardive dyskinesia (TD). In this conversation, Drs Nasrallah and Dees discuss the nuances of recognizing and treating DIMDs and their experience with TD diagnosis, assessment, and treatment.

Q1.
How do you differentiate TD from other DIMDs?
Dr Dees

Put simply, TD is a hyperkinetic movement disorder—too much movement; DIP is a hypokinetic movement disorder—too little movement. However, it is also critical to understand the phenomenology associated with different movement disorders. Let’s consider TD and DIP, the most common DIMDs, as an example.

TD can be associated with chorea, athetosis and, in some cases, dystonia. So, let’s define those phenomenologies. Chorea is randomly flowing movements from one body part to another. Athetosis is slow, writhing movements also flowing from one body part to another. Dystonia is defined as sustained involuntary muscle contractions. TD most often affects the orofacial region, but in greater than half of all patients affects all extremities and even the trunk as well. Common symptoms include lip puckering, facial grimacing, tongue protrusions, excessive blinking, and “piano playing” in the fingers or toes. TD movements are irregular, nonpredictable, and constantly flowing.

DIP, on the other hand, is characterized by an overall paucity of movement and associated with bradykinesia and rigidity. Bradykinesia is a primary symptom of DIP and is defined as small, slow movements. The patient will feel as if they are trying to make big movements but are unable to do so, resulting in difficulty with common activities such as standing from a chair with no armrests. Rigidity is muscle stiffness resulting in resistance to movement. Additionally, 75% of patients with DIP will have tremor at rest, although 25% of patients with DIP will have no tremor. Tremor typically occurs in the jaw, hands, and feet. These 3 phenomenologies are indicative of DIP; however, more advanced DIP may have postural instability and falls. Common additional symptoms include “masked face” with reduced blinking, shuffling gait, and lack of arm swing.

By defining these phenomenologies, we can determine whether our patient’s symptoms are due to TD, DIP, or both.

Dr Nasrallah

TD and DIP can also be differentiated based on the onset of symptoms. DIP has acute onset, often starting days to weeks after initiating treatment with or increasing the dose of an antipsychotic. TD, on the other hand, is a late-onset movement disorder, occurring after long-term exposure to an antipsychotic. That’s why we refer to it as “tardive.”

Q2.
Why is it important to distinguish TD from other DIMDs—particularly DIP?
Dr Dees

Learning to make the distinction between TD and DIP is essential because they require different treatments. DIP can be treated with anticholinergics, but these medications don’t help with the flowing movements associated with TD and can actually make movement worse, especially in older patients. A correct diagnosis determines the appropriate course of treatment.

Dr Nasrallah

I agree. These movements have different underlying causes. Acute DIP results from hypodopaminergic state in the brain while TD results from hyperdopaminergic state. Anticholinergics increase dopamine activity and thus help reduce the severity of DIP, but will worsen TD movements. The American Psychiatric Association (APA) recommends vesicular monoamine transporter 2 (VMAT2) inhibitors, which are the only US Food and Drug Administration (FDA)-approved treatment for TD that has an impact on the patient.

DIP can be treated with anticholinergics, but these medications don’t help with TD and can actually make movements worse.
Q3.
Less than 6% of patients with TD are treated with VMAT2 inhibitors, and ~40% of psychiatry health care professionals prescribe benztropine, a common anticholinergic, to treat TD. What explains the persistent use of anticholinergics for TD despite warnings that it worsens symptoms?
Dr Nasrallah

The challenge we encounter in psychiatry is the continued use of terms like extrapyramidal symptoms (EPS) to describe any DIMD experienced by a patient taking antipsychotics. This umbrella term doesn’t adequately differentiate between the movement disorders, like TD and DIP, that require different treatments.

In the 1950s, antipsychotic medications were discovered as a treatment option for various psychiatric conditions. However, some patients receiving these medications developed abnormal movements that were reminiscent of parkinsonism. At the time, anticholinergic medications were commonly used to treat parkinsonism, and clinicians began using them to alleviate the drug-induced movements experienced by patients on antipsychotics. It became common practice to prescribe anticholinergics alongside antipsychotics to address these side effects.

When TD was recognized as a distinct movement disorder associated with long-term antipsychotic use, it was initially grouped together with DIP under the broader classification of EPS. As a result, both conditions were treated with anticholinergics despite the differences in their underlying mechanisms.

For many years, no effective treatment existed for TD, leading to the continued use of the term EPS and the reliance on anticholinergics. This practice has become entrenched in clinical settings despite the approval of VMAT2 inhibitors for the treatment of TD in 2017, and it remains a significant barrier to overcome.

Q4.
How would you discuss discontinuing an anticholinergic with a patient?
Dr Dees

This can be a challenging conversation to have with patients, but it is extremely important. I’ve encountered patients who do not want to discontinue their anticholinergic medication, especially if they have been taking it for a long period of time. This scenario is where I think that patient education is absolutely critical. I want the patient to understand why we are discontinuing the anticholinergic—namely, that it may be making their symptoms worse. I want to engage in a conversation to develop a treatment plan that addresses all of their concerns, including their TD. For my patients with TD, I will explain that anticholinergics are not an appropriate treatment, but VMAT2 inhibitors have been approved by the FDA for the treatment of TD.

I want the patient to understand why we are discontinuing the anticholinergic—namely, that it may be making their TD symptoms worse.
Q5.
How do clinical practice guidelines inform the way you manage patients on antipsychotics and at risk of developing TD?
Dr Nasrallah

The APA guidelines, which contribute to the standard of care, state that patients taking antipsychotics should be assessed for movements during a clinical evaluation at every visit. Further, a structured assessment should be conducted annually or every 6 months in high-risk patients, such as elderly patients, postmenopausal females, patients with a mood disorder, and those with a previous movement disorder.

The Abnormal Involuntary Movement Scale (AIMS) is the standard scale for systematically assessing and quantifying the severity of TD movements. It assesses 7 items—4 regions of the face, where TD most often occurs, upper extremities, lower extremities, and trunk.

By adhering to clinical practice guidelines and the standard of care, we can ensure that TD is identified and treated appropriately. It is worth noting that patients may score a 0 on the AIMS for years while taking an antipsychotic before developing movements. We want to identify and document when a patient’s score jumps plus 1 or plus 2. If movements are detected, we should then ask about impact.

At every clinical encounter, I ask my patients taking antipsychotics if they have noticed movements that they don’t like in their face or body. If they mention or have movements, I ask about impact. Does it bother or embarrass them? And then, importantly, I will ask about treatment. Are they willing to take medication to address it? The APA guidelines recommend treatment for TD that has an impact on the patient, regardless of the severity of movements.

AIMS is the standard scale for systematically assessing and quantifying the severity of TD movements.
Q6.
Why is it important to recognize TD and its impact on patients and address the abnormal movements?
Dr Nasrallah

TD can have a profound impact on patients physically, socially, and psychologically. Patients may not be able to properly use their hands, chew their food, or button their shirts. They may isolate themselves from others, and TD can also make it more difficult to manage the patient’s underlying mental health condition. The biopsychosocial impact of TD can be distressing for patients.

Dr Dees

I’d add that nobody wants to be the person that the other people on the bus don’t want to sit next to. It’s an instinct probably ingrained into us since childhood. TD can make you feel socially ostracized. And for many patients, these movements have an added impact to an already distressing mental health condition. So, the impetus to treat is impact. Does this bother you enough to start taking a pill every day to make it better?

Dr Nasrallah

In my clinical experience, I have found that it is important to initiate treatment for TD, regardless of severity of movements, as soon as possible once a diagnosis has been made if it has an impact on the patient. In fact, the FDA trials for both VMAT2 inhibitors in the market included patients with mild, moderate, or severe TD.

Even mild movements can have a substantial impact, depending on the individual patient’s circumstances. My brief advice to my colleagues would be to be vigilant for DIMDs in patients taking antipsychotics, diagnose TD early and understand the impact of movements on your patient’s life, and consider clinical practice guidelines, which recommend treatment with a VMAT2 inhibitor for TD that impacts the patient.

In my clinical experience, I have found that it is important to initiate treatment for TD, regardless of severity of movements, as soon as possible once a diagnosis has been made if it has an impact on the patient.
Q7.
What are the features of AUSTEDO XR® (deutetrabenazine) that are most important to you or to your patients?
Dr Nasrallah

First, AUSTEDO has a demonstrated efficacy and safety profile, which was established in 2 randomized, placebo-controlled clinical trials. The most common adverse reactions reported in patients with TD treated with AUSTEDO (>3% and greater than placebo) were nasopharyngitis and insomnia. Second, increasing improvement in AIMS total score was observed through 3 years in an open-label extension (OLE) study, with 71% of patients at Week 145 seeing improvement relative to Week 15.

A very important factor for my patients is a reduction in movements and the resulting improvement in their social and emotional well-being. Teva conducted a survey to assess satisfaction among patients taking AUSTEDO XR. Patients reported greater self-esteem and feeling more comfortable with social activities, including spending time with family or working. When discussing treatments, my goal is to help patients understand how reduction of their movements could subsequently help to reduce the impact of TD on their lives.

Dr Dees

When starting AUSTEDO XR, all patients with TD begin with a 12-mg dose, which may be increased at weekly intervals by 6 mg/day until the desired symptom control is tolerably achieved. It is important that we find that reasonable dose to achieve therapeutic effect. That is why we increase the dose until we are able to see symptom control. AUSTEDO XR is available in doses from 12 mg to 48 mg, which allows providers to individualize the treatment to the patient’s needs.

AUSTEDO has a demonstrated efficacy and safety profile, which was established in 2 randomized, placebo-controlled clinical trials.
Q8.
How has management of TD changed over time, and what do you see as the most important challenge for clinicians today?
Dr Nasrallah

I would like to reiterate that using outdated terms like EPS that do not differentiate between movement disorders doesn't just delay diagnosis, but it can really impact the patient. We know that TD can lead to biopsychosocial repercussions for our patients, so it’s really important to understand that TD is distinct from other DIMDs and to identify TD early and treat it with a VMAT2 inhibitor.

Dr Dees

I agree. There used to be nothing we, as providers, could do to effectively treat TD. Now, we are equipped with VMAT2 inhibitors, such as once-daily AUSTEDO XR, that can help control the symptoms of TD, and I find that really inspiring. What we need to remain focused on is accurately identifying TD from other DIMDs, like DIP, to ensure that appropriate treatment can be prescribed, and the patient can see the benefit.

Select References
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American Psychiatric Association. The American Psychiatric Association Practice Guideline for the Treatment of Patients With Schizophrenia. 3rd ed. American Psychiatric Association; 2021. Accessed November 12, 2025. https://psychiatryonline.org/doi/pdf/10.1176/appi.books.9780890424841

Anderson KE, Stamler D, Davis MD, et al. Deutetrabenazine for treatment of involuntary movements in patients with tardive dyskinesia (AIM-TD): a double-blind, randomised, placebo-controlled, phase 3 trial. Lancet Psychiatry. 2017;4(8):595-604.

AUSTEDO XR® (deutetrabenazine) extended-release tablets/AUSTEDO® current Prescribing Information. Parsippany, NJ: Teva Neuroscience, Inc.

Bhidayasiri R, Jitkritsadakul O, Friedman JH, Fahn S. Updating the recommendations for treatment of tardive syndromes: a systematic review of new evidence and practical treatment algorithm. J Neurol Sci. 2018;389:67-75.

Caroff SN. Overcoming barriers to effective management of tardive dyskinesia. Neuropsychiatr Dis Treat. 2019;15:785-794.

Caroff SN, Davis VG, Miller DD, et al. Treatment outcomes of patients with tardive dyskinesia and chronic schizophrenia. J Clin Psychiatry. 2011;72(3):295-303.

Caroff SN, Yeomans K, Lenderking WR, et al. RE-KINECT: a prospective study of the presence and healthcare burden of tardive dyskinesia in clinical practice settings. J Clin Psychopharmacol. 2020;40(3):259-268.

Chepke C, Benning B, Cicero S, et al. Investigating real-world benztropine usage patterns in movement disorders: claims analysis and health care provider survey results. Prim Care Companion CNS Disord. 2023;25(4):22m03472.

Data on file. Teva Neuroscience, Inc. Parsippany, NJ.

Duma SR, Fung VSC. Drug-induced movement disorders. Aust Prescr. 2019;42(2):56-61.

Fahn S, Jankovic J, Hallet M, eds. Principles and Practice of Movement Disorders. 2nd ed. Elsevier, Inc; 2011.

Fernandez HH, Factor SA, Hauser RA, et al. Randomized controlled trial of deutetrabenazine for tardive dyskinesia: the ARM-TD study. Neurology. 2017;88(21):2003-2010.

Finkbeiner S, Konings M, Henegar M, et al. Multidimensional impact of tardive dyskinesia: interim analysis of clinician-reported measures in the IMPACT-TD Registry. Presented at: Psych Congress Elevate; May 30-June 2, 2024; Las Vegas, NV.

Guy W. ECDEU Assessment Manual for Psychopharmacology: Revised. Rockville, MD: US Department of Health, Education and Welfare, Public Health Service, Alcohol, Drug Abuse and Mental Health Administration, NIMH Psychopharmacology Research Branch, Division of Extramural Research Programs; 1976:534-537. DHEW publication number ADM 76-338.

Hauser RA, Meyer JM, Factor SA, et al. Differentiating tardive dyskinesia: a video-based review of antipsychotic-induced movement disorders in clinical practice. CNS Spectr. 2022;27(2):208-217.

Ingrezza® (valbenazine) capsules. Prescribing Information. San Diego, CA: Neurocrine Biosciences, Inc.

Jain R, Konings M, Thompson S, et al. Real-world evidence of patient experience with once-daily deutetrabenazine extended-release tablets for tardive dyskinesia and chorea in Huntington disease in the United States. Poster presented at: The Annual Psych Congress; October 29-November 2, 2024; Boston, MA.

Miller JJ. Everyone please stop (EPS). Psychiatric Times. 2022;39(8). Accessed November 12, 2025. https://www.psychiatrictimes.com/view/everyone-please-stop-eps-

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Vasan S, Padhy RK. Tardive Dyskinesia. In: StatPearls [Internet]. StatPearls Publishing; 2025. Accessed November 12, 2025. https://www.ncbi.nlm.nih.gov/books/NBK448207/

Prev ARTICLE
Treatment
Understanding AUSTEDO XR®: A Once-Daily Treatment Option for Adult Patients With Tardive Dyskinesia
Volume 20
On the Front Line: Helping Advanced Practice Providers to Recognize, Assess, and Treat Tardive Dyskinesia
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Volume 19
Unmasking the Impact of Tardive Dyskinesia on Patients’ Lives
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Volume 18
Is the EPS Diagnosis Leading Us Astray? The Importance of Differentiating Tardive Dyskinesia
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Volume 17
When Patients With Mood Disorders Develop TD: Considerations for Assessment and Treatment
Read more
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IMPORTANT SAFETY INFORMATION
Depression and Suicidality in Patients with Huntington's Disease: AUSTEDO XR® and AUSTEDO® can increase the risk of depression and suicidal thoughts and behavior (suicidality) in patients with Huntington's disease. Balance the risks of depression and suicidality with the clinical need for treatment of chorea. Closely monitor patients for the emergence or worsening of depression, suicidality, or unusual changes in behavior. Inform patients, their caregivers, and families of the risk of
IMPORTANT SAFETY INFORMATION
Depression and Suicidality in Patients with Huntington's Disease: AUSTEDO XR® and AUSTEDO® can increase the risk of depression
INDICATIONS AND USAGE

AUSTEDO XR® (deutetrabenazine) extended-release tablets and AUSTEDO® (deutetrabenazine) tablets are indicated in adults for the treatment of chorea associated with Huntington's disease and for the treatment of tardive dyskinesia.

IMPORTANT SAFETY INFORMATION
Depression and Suicidality in Patients with Huntington's Disease: AUSTEDO XR® and AUSTEDO® can increase the risk of depression and suicidal thoughts and behavior (suicidality) in patients with Huntington's disease. Balance the risks of depression and suicidality with the clinical need for treatment of chorea. Closely monitor patients for the emergence or worsening of depression, suicidality, or unusual changes in behavior. Inform patients, their caregivers, and families of the risk of depression and suicidality and instruct them to report behaviors of concern promptly to the treating physician. Exercise caution when treating patients with a history of depression or prior suicide attempts or ideation. AUSTEDO XR and AUSTEDO are contraindicated in patients who are suicidal, and in patients with untreated or inadequately treated depression.
Contraindications: AUSTEDO XR and AUSTEDO are contraindicated in patients with Huntington's disease who are suicidal, or have untreated or inadequately treated depression. AUSTEDO XR and AUSTEDO are also contraindicated in: patients with hepatic impairment; patients taking reserpine or within 20 days of discontinuing reserpine; patients taking monoamine oxidase inhibitors (MAOIs), or within 14 days of discontinuing MAOI therapy; and patients taking tetrabenazine or valbenazine.
Clinical Worsening and Adverse Events in Patients with Huntington's Disease: AUSTEDO XR and AUSTEDO may cause a worsening in mood, cognition, rigidity, and functional capacity. Prescribers should periodically re-evaluate the need for AUSTEDO XR or AUSTEDO in their patients by assessing the effect on chorea and possible adverse effects.
QTc Prolongation: AUSTEDO XR and AUSTEDO may prolong the QT interval, but the degree of QT prolongation is not clinically significant when AUSTEDO XR or AUSTEDO is administered within the recommended dosage range. AUSTEDO XR and AUSTEDO should be avoided in patients with congenital long QT syndrome and in patients with a history of cardiac arrhythmias.
Neuroleptic Malignant Syndrome (NMS), a potentially fatal symptom complex reported in association with drugs that reduce dopaminergic transmission, has been observed in patients receiving tetrabenazine. The risk may be increased by concomitant use of dopamine antagonists or antipsychotics. The management of NMS should include immediate discontinuation of AUSTEDO XR and AUSTEDO; intensive symptomatic treatment and medical monitoring; and treatment of any concomitant serious medical problems.
Akathisia, Agitation, and Restlessness: AUSTEDO XR and AUSTEDO may increase the risk of akathisia, agitation, and restlessness. The risk of akathisia may be increased by concomitant use of dopamine antagonists or antipsychotics. If a patient develops akathisia, the AUSTEDO XR or AUSTEDO dose should be reduced; some patients may require discontinuation of therapy.
Parkinsonism: AUSTEDO XR and AUSTEDO may cause parkinsonism in patients with Huntington's disease or tardive dyskinesia. Parkinsonism has also been observed with other VMAT2 inhibitors. The risk of parkinsonism may be increased by concomitant use of dopamine antagonists or antipsychotics. If a patient develops parkinsonism, the AUSTEDO XR or AUSTEDO dose should be reduced; some patients may require discontinuation of therapy.
Sedation and Somnolence: Sedation is a common dose-limiting adverse reaction of AUSTEDO XR and AUSTEDO. Patients should not perform activities requiring mental alertness, such as operating a motor vehicle or hazardous machinery, until they are on a maintenance dose of AUSTEDO XR or AUSTEDO and know how the drug affects them. Concomitant use of alcohol or other sedating drugs may have additive effects and worsen sedation and somnolence.
Hyperprolactinemia: Tetrabenazine elevates serum prolactin concentrations in humans. If there is a clinical suspicion of symptomatic hyperprolactinemia, appropriate laboratory testing should be done and consideration should be given to discontinuation of AUSTEDO XR and AUSTEDO.
Binding to Melanin-Containing Tissues: Deutetrabenazine or its metabolites bind to melanin-containing tissues and could accumulate in these tissues over time. Prescribers should be aware of the possibility of long-term ophthalmologic effects.
Common Adverse Reactions: The most common adverse reactions for AUSTEDO (>8% and greater than placebo) in a controlled clinical study in patients with Huntington's disease were somnolence, diarrhea, dry mouth, and fatigue. The most common adverse reactions for AUSTEDO (4% and greater than placebo) in controlled clinical studies in patients with tardive dyskinesia were nasopharyngitis and insomnia. Adverse reactions with AUSTEDO XR extended-release tablets are expected to be similar to AUSTEDO tablets.
Please see accompanying full Prescribing Information, including Boxed Warning.
INDICATIONS AND USAGE

AUSTEDO XR® (deutetrabenazine) extended-release tablets and AUSTEDO® (deutetrabenazine) tablets are indicated in adults for the treatment of chorea associated with Huntington's disease and for the treatment of tardive dyskinesia.

IMPORTANT SAFETY INFORMATION
Depression and Suicidality in Patients with Huntington's Disease: AUSTEDO XR® and AUSTEDO® can increase the risk of depression and suicidal thoughts and behavior (suicidality) in patients with Huntington's disease. Balance the risks of depression and suicidality with the clinical need for treatment of chorea. Closely monitor patients for the emergence or worsening of depression, suicidality, or unusual changes in behavior. Inform patients, their caregivers, and families of the risk of depression and suicidality and instruct them to report behaviors of concern promptly to the treating physician. Exercise caution when treating patients with a history of depression or prior suicide attempts or ideation. AUSTEDO XR and AUSTEDO are contraindicated in patients who are suicidal, and in patients with untreated or inadequately treated depression.
Contraindications: AUSTEDO XR and AUSTEDO are contraindicated in patients with Huntington's disease who are suicidal, or have untreated or inadequately treated depression. AUSTEDO XR and AUSTEDO are also contraindicated in: patients with hepatic impairment; patients taking reserpine or within 20 days of discontinuing reserpine; patients taking monoamine oxidase inhibitors (MAOIs), or within 14 days of discontinuing MAOI therapy; and patients taking tetrabenazine or valbenazine.
Clinical Worsening and Adverse Events in Patients with Huntington's Disease: AUSTEDO XR and AUSTEDO may cause a worsening in mood, cognition, rigidity, and functional capacity. Prescribers should periodically re-evaluate the need for AUSTEDO XR or AUSTEDO in their patients by assessing the effect on chorea and possible adverse effects.
QTc Prolongation: AUSTEDO XR and AUSTEDO may prolong the QT interval, but the degree of QT prolongation is not clinically significant when AUSTEDO XR or AUSTEDO is administered within the recommended dosage range. AUSTEDO XR and AUSTEDO should be avoided in patients with congenital long QT syndrome and in patients with a history of cardiac arrhythmias.
Neuroleptic Malignant Syndrome (NMS), a potentially fatal symptom complex reported in association with drugs that reduce dopaminergic transmission, has been observed in patients receiving tetrabenazine. The risk may be increased by concomitant use of dopamine antagonists or antipsychotics. The management of NMS should include immediate discontinuation of AUSTEDO XR and AUSTEDO; intensive symptomatic treatment and medical monitoring; and treatment of any concomitant serious medical problems.
Akathisia, Agitation, and Restlessness: AUSTEDO XR and AUSTEDO may increase the risk of akathisia, agitation, and restlessness. The risk of akathisia may be increased by concomitant use of dopamine antagonists or antipsychotics. If a patient develops akathisia, the AUSTEDO XR or AUSTEDO dose should be reduced; some patients may require discontinuation of therapy.
Parkinsonism: AUSTEDO XR and AUSTEDO may cause parkinsonism in patients with Huntington's disease or tardive dyskinesia. Parkinsonism has also been observed with other VMAT2 inhibitors. The risk of parkinsonism may be increased by concomitant use of dopamine antagonists or antipsychotics. If a patient develops parkinsonism, the AUSTEDO XR or AUSTEDO dose should be reduced; some patients may require discontinuation of therapy.
Sedation and Somnolence: Sedation is a common dose-limiting adverse reaction of AUSTEDO XR and AUSTEDO. Patients should not perform activities requiring mental alertness, such as operating a motor vehicle or hazardous machinery, until they are on a maintenance dose of AUSTEDO XR or AUSTEDO and know how the drug affects them. Concomitant use of alcohol or other sedating drugs may have additive effects and worsen sedation and somnolence.
Hyperprolactinemia: Tetrabenazine elevates serum prolactin concentrations in humans. If there is a clinical suspicion of symptomatic hyperprolactinemia, appropriate laboratory testing should be done and consideration should be given to discontinuation of AUSTEDO XR and AUSTEDO.
Binding to Melanin-Containing Tissues: Deutetrabenazine or its metabolites bind to melanin-containing tissues and could accumulate in these tissues over time. Prescribers should be aware of the possibility of long-term ophthalmologic effects.
Common Adverse Reactions: The most common adverse reactions for AUSTEDO (>8% and greater than placebo) in a controlled clinical study in patients with Huntington's disease were somnolence, diarrhea, dry mouth, and fatigue. The most common adverse reactions for AUSTEDO (4% and greater than placebo) in controlled clinical studies in patients with tardive dyskinesia were nasopharyngitis and insomnia. Adverse reactions with AUSTEDO XR extended-release tablets are expected to be similar to AUSTEDO tablets.
Please see accompanying full Prescribing Information, including Boxed Warning.