Drug-Induced Movement Disorders

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Drug-Induced Movement Disorders

Drug-induced movement disorders (DIMDs) encompass a range of motor abnormalities caused by medications that affect dopaminergic, serotonergic, or other neurotransmitter systems. They are among the most common movement disorders encountered in clinical practice and are largely preventable. This article reviews the major categories: tardive syndromes, drug-induced parkinsonism, acute dystonic reactions, akathisia, neuroleptic malignant syndrome, serotonin syndrome, and drug-induced chorea/tremor.

Bottom Line

Tardive dyskinesia: VMAT2 inhibitors (deutetrabenazine, valbenazine) are FDA-approved first-line treatments; prevention by minimizing dopamine blocker exposure is key
Drug-induced parkinsonism: Second most common cause of parkinsonism; clinically indistinguishable from PD; typically resolves within weeks to months of stopping the offending agent, but may unmask prodromal PD
Akathisia: Often misdiagnosed as anxiety or psychotic agitation; propranolol and benzodiazepines are first-line; dose reduction of the offending agent is essential
NMS: Medical emergency (mortality 5–20%); immediate discontinuation of causative agent + supportive care + dantrolene/bromocriptine
Serotonin syndrome: Clinical triad of altered mental status + autonomic instability + neuromuscular hyperactivity; cyproheptadine is the specific antidote

Tardive Syndromes

Epidemiology and Risk Factors

Tardive syndromes develop after prolonged exposure (≥3 months; ≥1 month in patients >60 years) to dopamine receptor-blocking agents (DRBAs). Prevalence: 20–30% of patients on long-term antipsychotic therapy.

Risk Factor	Details
Age >55 years	Strongest risk factor; 5x higher incidence
Female sex	Higher risk, especially postmenopausal
African American descent	Higher risk (pharmacogenetic factors)
Duration of DRBA exposure	Cumulative dose-dependent
First-generation > second-generation antipsychotics	Typical antipsychotics have higher risk; clozapine has lowest risk
Mood disorders (vs. schizophrenia)	Patients with affective disorders at higher risk
Diabetes mellitus	Independent risk factor
Early EPS	Drug-induced parkinsonism or akathisia predicts higher TD risk

Causative Agents

Any DRBA can cause tardive syndromes. Commonly implicated agents beyond antipsychotics:

Antiemetics: Metoclopramide (most common non-psychiatric cause; FDA boxed warning for >12 weeks), prochlorperazine, promethazine
Antidepressants: Amoxapine (D2 blocking properties)
Atypical antipsychotics: All carry risk, though lower; quetiapine, olanzapine, risperidone; clozapine has the lowest risk and may actually treat TD

Clinical Subtypes

Subtype	Description	Key Features
Tardive dyskinesia (TD)	Repetitive, stereotyped, purposeless movements	Classic orobuccolingual: lip smacking, tongue protrusion, chewing, lateral jaw movements; may also involve limbs and trunk
Tardive dystonia	Sustained or intermittent muscle contractions causing abnormal postures	More disabling than TD; retrocollis, opisthotonus, trunk extension; more common in younger males; often persists after DRBA withdrawal
Tardive akathisia	Persistent restlessness persisting >3 months after stable dose	Distinguished from acute akathisia by persistence; often coexists with TD
Tardive tremor	Postural/kinetic tremor, 3–5 Hz	Rare; may mimic essential tremor
Tardive tics / tourettism	Ticlike movements after DRBA exposure	Rare; may have premonitory urge
Tardive myoclonus	Brief jerking movements	Rare; may be generalized

Assessment

The Abnormal Involuntary Movement Scale (AIMS) is the standard instrument: 12-item clinician-rated scale assessing facial/oral, extremity, and trunk movements, plus global severity and patient awareness. Total score range 0–40.

Treatment of Tardive Dyskinesia

TD Treatment Algorithm

Prevention: Use lowest effective dose of DRBA for shortest duration; monitor with AIMS every 3–6 months (every 12 months for atypical antipsychotics)
Reduce or discontinue DRBA if clinically feasible (risk of psychiatric decompensation; TD may initially worsen on withdrawal — "withdrawal dyskinesia")
Switch to lower-risk antipsychotic: Consider clozapine or quetiapine if antipsychotic is still needed
VMAT2 inhibitor therapy (first-line):
- Valbenazine 40–80 mg daily (FDA approved for TD, 2017)
- Deutetrabenazine 12–48 mg/day in divided doses (FDA approved for TD, 2017)
- Both have Class I evidence; significant reduction in AIMS scores vs. placebo
Adjunctive options (limited evidence): Tetrabenazine (off-label), clonazepam, ginkgo biloba extract (EGb-761), amantadine, vitamin B6

Drug-Induced Parkinsonism (DIP)

DIP is the second most common cause of parkinsonism after Parkinson disease, accounting for ~10–20% of parkinsonism cases. It can be clinically indistinguishable from PD.

Feature	Details
Onset	Days to months after starting the offending agent; most within 1–3 months
Clinical features	Bilateral and symmetric (vs. asymmetric in PD); tremor may be absent or postural rather than resting; bradykinesia and rigidity prominent; may coexist with other DIMDs (akathisia, TD)
Causative agents	Antipsychotics (typical > atypical), antiemetics (metoclopramide, prochlorperazine), calcium channel blockers (flunarizine, cinnarizine), lithium, valproate, amiodarone, SSRIs
Resolution	Typically resolves within weeks to months of stopping the agent; may take up to 12 months. Persistence beyond 12 months suggests unmasking of underlying PD
DaTscan	Normal in pure DIP (intact presynaptic dopamine terminals); abnormal if underlying PD has been unmasked

DIP vs. Parkinson Disease

Up to 15–20% of patients diagnosed with DIP are later diagnosed with PD. DIP may unmask prodromal PD by challenging an already compromised dopaminergic system. Any patient with persistent parkinsonism >6–12 months after drug withdrawal should be evaluated for underlying PD (consider DaTscan or clinical follow-up).

Acute Dystonic Reactions

Onset: Usually within 24–96 hours of DRBA initiation (90% within first 5 days)
Risk factors: Young age (children and young adults), male sex, high-potency antipsychotics, cocaine use
Presentations: Oculogyric crisis (forced upward eye deviation), torticollis, trismus, tongue protrusion, opisthotonos, laryngospasm (potentially life-threatening)
Treatment: IM or IV diphenhydramine (50 mg) or benztropine (1–2 mg); response typically within minutes. Continue oral anticholinergic for 48–72 hours to prevent recurrence
Causative agents: Haloperidol, fluphenazine, metoclopramide, prochlorperazine; less common with atypical antipsychotics

Akathisia

A subjective sense of inner restlessness with an urge to move, typically manifesting as inability to sit still, rocking, pacing, or shifting weight. Often overlooked or misdiagnosed as anxiety, psychotic agitation, or RLS.

Subtype	Timing	Features
Acute akathisia	Hours to days after starting/increasing DRBA	Most common; resolves with dose reduction or discontinuation
Tardive akathisia	≥3 months on stable DRBA dose	Persists or worsens after DRBA withdrawal; often coexists with TD
Withdrawal akathisia	Within 6 weeks of DRBA discontinuation/dose reduction	Self-limited (usually 6 weeks)

Assessment: Barnes Akathisia Rating Scale (BARS) — 4-item clinician-rated scale.

Treatment of Akathisia

Step 1: Reduce dose of the offending agent or switch to a lower-risk agent (quetiapine, clozapine)
Step 2: Propranolol 20–80 mg/day (most evidence; lipophilic beta-blocker preferred)
Step 3: Benzodiazepines (lorazepam, clonazepam)
Other options: Mirtazapine (5-HT2A antagonist properties), cyproheptadine, amantadine
Anticholinergics: Less effective for akathisia than for other EPS; do NOT use as monotherapy

Neuroleptic Malignant Syndrome (NMS)

Medical Emergency

NMS is an idiosyncratic, life-threatening reaction to DRBAs, characterized by hyperthermia, severe rigidity, autonomic instability, and altered mental status. Mortality has declined from ~30% to 5–20% with earlier recognition and treatment.

Feature	Details
Cardinal features	Hyperthermia (>38°C, often >40°C), severe "lead-pipe" rigidity, altered mental status (confusion → coma), autonomic instability (tachycardia, labile BP, diaphoresis)
Lab findings	Elevated CK (often >1,000 IU/L, can exceed 100,000), leukocytosis, elevated LDH, metabolic acidosis, myoglobinuria, acute kidney injury
Onset	Usually within 2 weeks of DRBA initiation or dose increase (90% within 10 days); can occur at any time
Risk factors	High-potency typical antipsychotics, rapid dose escalation, dehydration, agitation, IM administration, previous NMS episode (17–30% recurrence risk)
Causative agents	All antipsychotics; metoclopramide; also rapid withdrawal of dopaminergic agents in PD patients

NMS Treatment

Immediately discontinue the causative agent
Aggressive supportive care: ICU admission, IV fluids, cooling measures, monitoring for renal failure, DVT, PE, DIC
Dantrolene 1–2.5 mg/kg IV q6h (muscle relaxant; reduces rigidity and hyperthermia)
Bromocriptine 2.5–10 mg PO/NG q8h (dopamine agonist; restores dopaminergic tone)
Benzodiazepines for agitation and muscle rigidity
ECT for refractory cases

Rechallenge: If antipsychotic is needed, wait ≥2 weeks, use a low-potency or atypical agent (clozapine, quetiapine), start at low dose, titrate slowly.

Serotonin Syndrome

A potentially life-threatening drug reaction caused by excessive serotonergic activity, most commonly from combining serotonergic agents.

Domain	Features
Neuromuscular hyperactivity	Clonus (spontaneous, inducible, or ocular), hyperreflexia, myoclonus, tremor, rigidity (lower > upper extremity)
Autonomic instability	Hyperthermia, tachycardia, diaphoresis, diarrhea, mydriasis, labile BP
Altered mental status	Agitation, confusion, delirium

Serotonin Syndrome vs. NMS

Feature	Serotonin Syndrome	NMS
Onset	Rapid (hours)	Gradual (days)
Tone	Clonus, hyperreflexia (neuromuscular excitation)	Lead-pipe rigidity (bradykinetic)
Pupils	Mydriasis (dilated)	Normal
Bowel sounds	Hyperactive	Normal or decreased
CK	Mildly elevated (usually <1,000)	Markedly elevated (often >1,000–100,000)
Causative drugs	Serotonergic agents (SSRIs, SNRIs, MAOIs, tramadol, linezolid, triptans)	Dopamine receptor blockers
Treatment	Cyproheptadine (5-HT2A antagonist) + benzodiazepines	Dantrolene + bromocriptine
Resolution	24–72 hours (rapid after drug removal)	Days to weeks

Drug-Induced Chorea

Multiple drug classes can induce choreiform movements:

Drug Class	Examples
Antiparkinsonism	Levodopa (peak-dose dyskinesia in PD), dopamine agonists, anticholinergics
Dopamine antagonists	Tardive syndromes (see above)
Antiseizure medications	Phenytoin, carbamazepine, lamotrigine, gabapentin, valproic acid
Antidepressants	TCAs, SSRIs
Stimulants	Cocaine, amphetamines
Oral contraceptives	Chorea gravidarum; recurrence of Sydenham chorea
Others	Baclofen, calcium channel blockers, digoxin, fluoroquinolones, steroids, methadone

Drug-Induced Tremor

Tremor Type	Common Causative Agents
Enhanced physiologic tremor	Sympathomimetics (albuterol, theophylline), caffeine, lithium, valproate, thyroid hormones, SSRIs
Parkinsonian tremor	Antipsychotics, metoclopramide, valproate (may cause both action and resting tremor)
Cerebellar/intention tremor	Lithium (toxicity), phenytoin, carbamazepine, 5-FU, cytarabine

Management: Dose reduction or discontinuation of the causative agent is the primary intervention. For essential lithium or valproate therapy, propranolol may reduce tremor amplitude. Dose fractionation or switching to extended-release formulations can also help.

References

Continuum (Minneap Minn). August 2025; 31(4 Movement Disorders). Huntington Disease and Chorea (pp 1066–1087).
Caroff SN, Campbell EC. Drug-induced extrapyramidal syndromes. Psychiatr Clin North Am. 2016;39(3):391–411.
Ricciardi L, Pringsheim T, Barnes TRE, et al. Treatment recommendations for tardive dyskinesia. Can J Psychiatry. 2019;64(6):388–399.
Ware MR, Feller DB, Hall KL. Neuroleptic malignant syndrome: diagnosis and management. Prim Care Companion CNS Disord. 2018;20(1):17r02185.
Boyer EW, Shannon M. The serotonin syndrome. N Engl J Med. 2005;352(11):1112–1120.