Chorea, Myoclonus & Tics

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Chorea, Myoclonus & Tics

Hyperkinetic movement disorders are characterized by excessive, involuntary movements. Three of the most commonly encountered phenomenologies — chorea, myoclonus, and tics — each have distinct clinical features that guide differential diagnosis and treatment. This article reviews the identification, etiologic workup, and management of these disorders, drawing primarily from the Continuum Movement Disorders issue (August 2025).

Bottom Line

Chorea: Random, purposeless, flowing movements; most common genetic cause in adults is Huntington disease; acute chorea workup should include glucose (nonketotic hyperglycemia), autoimmune panel, and brain MRI
Myoclonus: Brief, shock-like jerks (positive) or sudden loss of muscle tone (negative); classify by distribution, timing, and etiology to guide treatment; valproate, levetiracetam, and clonazepam are first-line for cortical myoclonus
Tics: Semivoluntary, suppressible movements with premonitory urge; CBIT is first-line treatment; only 3 FDA-approved medications (haloperidol, pimozide, aripiprazole); ecopipam is a promising new D1 antagonist
VMAT2 inhibitors: Tetrabenazine, deutetrabenazine, and valbenazine are FDA-approved for chorea in HD and tardive dyskinesia
Functional ticlike behavior (FTLB): Explosive onset at age ≥12, often linked to social media exposure during COVID-19 pandemic; treat with CBT, not antitic medications

Part 1: Chorea

Identification

Chorea describes involuntary movements that are random, purposeless, and unpredictable — brief and abrupt, free-flowing from one body part to another. Key examination features:

Motor impersistence: Inability to sustain posture (tongue protrusion for 10 seconds; "milkmaid's grip" with fluctuating handgrip intensity)
Parakinesia: Choreiform movements blended into purposeful movements (e.g., adjusting eyeglasses to mask an arm movement)
"Hung up" or pendular reflexes
Ballism: High-amplitude chorea involving proximal joints (flinging limb movements)
Athetosis: Continuous writhing movements of distal extremities ("piano-playing fingers"), often co-occurring with chorea

Examine patients without shoes and socks, with legs and feet suspended. Small-amplitude chorea is often best seen in the forehead and fingers.

Diagnostic Approach by Body Distribution

Distribution	Potential Causes
Orobuccolingual	Tardive dyskinesia, chorea-acanthocytosis, McLeod syndrome, Lesch-Nyhan, Wilson disease, neuroferritinopathy, NMDA receptor encephalitis
Forehead	Huntington disease (not pathognomonic but helps distinguish from TD)
Hemibody	With lesion: vascular insult, nonketotic hyperglycemia, infection, tuberous sclerosis. Without lesion: Sydenham chorea, polycythemia vera

Diagnostic Approach by Acuity

Acuity	Typical Causes	Key Workup
Acute / Subacute	Structural (stroke), drug-induced, infectious, autoimmune/paraneoplastic, metabolic/endocrine, nonketotic hyperglycemia	Serum glucose, CBC with smear, CMP, thyroid, ESR, ANA, antiphospholipid antibodies, lupus anticoagulant, paraneoplastic panel, brain MRI, pregnancy test
Subacute (children)	Sydenham chorea (most common acute chorea in children); post-streptococcal	ASO titer, anti-DNase B, throat culture; can recur with OCP use or pregnancy (chorea gravidarum)
Chronic / Progressive	Genetic etiologies: Huntington disease, HD phenocopies, neuroacanthocytosis, Wilson disease, benign hereditary chorea, NBIA	Brain MRI + CT (calcifications), genetic testing, ceruloplasmin (<50 years), acanthocyte smear, whole exome/genome if targeted testing negative

Huntington Disease

The most common inherited cause of chorea. Autosomal dominant; CAG trinucleotide repeat expansion on HTT gene (chromosome 4). US prevalence: ~5/100,000.

CAG Repeats	Clinical Significance
<26	Normal
27–35 (intermediate)	Normal (rare cases); risk of anticipation in offspring
36–39 (indeterminate)	Incomplete penetrance; later onset
≥40	Full penetrance; mean onset age 30–50
≥60	Juvenile onset; parkinsonism and seizures (Westphal variant)

Clinical triad: chorea + cognitive decline + neuropsychiatric symptoms. Psychiatric features (depression, irritability, impulsivity, psychosis) frequently precede motor onset. Suicidal ideation prevalence up to 30%; suicide is the third most common cause of death (6.6%). MRI shows caudate atrophy ("boxcar ventricles").

HD Phenocopies (HTT-negative)

C9orf72 disease: Most common HD phenocopy in White populations; hexanucleotide repeat; may have upper motor neuron signs/weakness; also causes FTD and ALS
SCA17 (HD-like 4): Second most common; CAG repeat in TBP gene; overlap of chorea and ataxia
HD-like 2: CTG/CAG repeat in JPH3; exclusively in sub-Saharan African descent
DRPLA: CAG repeat in ATN1; Japanese descent; seizures and myoclonus

Other Genetic Causes of Chorea

Disorder	Inheritance	Key Features	Diagnostic Clues
Neuroferritinopathy	AD; FTL gene	Prominent orofacial dystonia	Very low serum ferritin; MRI T2 hypointensity in basal ganglia
Aceruloplasminemia	AR; CP gene	Retinal degeneration	Absent ceruloplasmin, high ferritin; MRI iron accumulation
Chorea-acanthocytosis	AR; VPS13A	Feeding dystonia, tongue protrusion, seizures, neuropathy	Acanthocytes, elevated CK, absent chorein in RBCs
McLeod syndrome	X-linked; XK gene	Similar to chorea-acanthocytosis; males only	Reduced Kell antigen, acanthocytes, elevated CK/LFTs
Benign hereditary chorea	AD; NKX2-1	Brain-lung-thyroid syndrome; childhood onset, minimal progression	Congenital hypothyroidism, pulmonary disease; cancer screening
Wilson disease	AR; ATP7B	Treatable; variable movement disorders + liver disease	Low ceruloplasmin, elevated 24h urine Cu, KF rings, "face of giant panda" on MRI

Pharmacologic Management of Chorea

Agent	Mechanism	FDA Approved For	Key Considerations
Tetrabenazine	VMAT2 inhibitor	HD chorea (2008)	3x daily dosing; CYP2D6 metabolism; boxed warning for suicidality; parkinsonism, akathisia, depression
Deutetrabenazine	VMAT2 inhibitor (deuterated)	HD chorea; TD	Longer half-life, 2x daily; better tolerability than tetrabenazine; less depression risk
Valbenazine	VMAT2 inhibitor	TD; HD chorea (2024)	Once daily; newest approval for HD chorea
Antipsychotics	Postsynaptic D2 blockade	Off-label for chorea	Useful when psychiatric comorbidities coexist; risk of TD with long-term use; lower-cost option globally

Initial treatment for secondary chorea should always target the underlying cause. Mild chorea may not require pharmacologic treatment. Anosognosia may limit patient awareness, so care partners should be involved in treatment decisions.

Part 2: Myoclonus

Definition and Classification

Myoclonus is a fast, jerking movement with either gain of muscle tone (positive myoclonus) or sudden loss of muscle tone (negative myoclonus/asterixis). Unlike chorea, myoclonus lacks the flowing quality from one body part to another. Classification guides treatment:

Classification Axis	Categories
By distribution	Focal, segmental, multifocal, generalized
By timing	Spontaneous, action-induced, stimulus-sensitive (reflex), intention
By neuroanatomic origin	Cortical (most common treatable form), subcortical, brainstem (reticular reflex myoclonus), spinal, peripheral
By etiology	Physiologic (hiccups, sleep starts), essential, epileptic, symptomatic (secondary)

Key Etiologies

Category	Examples
Physiologic	Hiccups, sleep starts (hypnic jerks), exercise-induced, anxiety-related
Essential	Essential myoclonus (often hereditary, responds to alcohol); myoclonus-dystonia (SGCE mutations, AD)
Epileptic	Juvenile myoclonic epilepsy, progressive myoclonic epilepsies (Unverricht-Lundborg, Lafora body, neuronal ceroid lipofuscinosis), infantile spasms
Post-hypoxic	Lance-Adams syndrome (chronic post-hypoxic action myoclonus after cardiac arrest)
Metabolic	Uremia, hepatic failure (asterixis), hyponatremia, hypoglycemia, hypercalcemia
Toxic / Drug-induced	Opioids, SSRIs, lithium, bismuth, levodopa, anticonvulsants
Neurodegenerative	CJD (stimulus-sensitive), CBD (cortical reflex), DLB, MSA, AD, HD
Autoimmune	Opsoclonus-myoclonus syndrome (anti-Ri, neuroblastoma in children), stiff-person spectrum, NMDA receptor encephalitis
Spinal	Propriospinal myoclonus (axial jerks, worse supine); segmental spinal myoclonus (myelopathy, syrinx)

Evaluation

EEG with back-averaging: Cortical myoclonus shows a time-locked cortical potential preceding the jerk
Somatosensory evoked potentials (SSEPs): Giant SEPs suggest cortical myoclonus
EMG: Burst duration <75 ms suggests cortical origin; >200 ms suggests subcortical
MRI brain and spine (if spinal myoclonus suspected)
Metabolic workup: Renal/hepatic function, electrolytes, drug levels

Treatment of Myoclonus

Myoclonus Type	First-Line Treatment	Alternatives
Cortical myoclonus	Valproate, levetiracetam, clonazepam	Piracetam (not available in US), perampanel, zonisamide
Subcortical / Reticular	Clonazepam	Valproate, levetiracetam
Post-hypoxic (Lance-Adams)	Levetiracetam + clonazepam combination	Valproate, piracetam; sodium oxybate in severe cases
Myoclonus-dystonia (SGCE)	Alcohol (diagnostic clue); zonisamide, benzodiazepines	DBS (GPi) for refractory cases
Spinal myoclonus	Clonazepam	Treat underlying cause (myelopathy, tumor)
Metabolic (asterixis)	Correct the underlying metabolic derangement	—

Part 3: Tics and Tourette Syndrome

Epidemiology

Tourette syndrome global prevalence: 0.5% (0.77% in children, 0.05% in adults)
More common in boys (1.5:1 to 4:1 ratio); no racial/ethnic differences
Onset typically ages 3–8; peak severity ages 8–12; significant improvement or resolution in early adulthood
>85% of patients with Tourette syndrome have at least one psychiatric comorbidity (OCD 30–50%, ADHD 50–60%)

Clinical Features

Feature	Description
Simple motor tics	Blinking, nose twitching, neck snapping, tensing muscles
Complex motor tics	Copropraxia (rude gestures), echopraxia (mimicking), hitting, throwing
Simple phonic tics	Sniffing, throat clearing, grunting, squeaking
Complex phonic tics	Coprolalia (10–30%), echolalia, palilalia
Premonitory urge	82% report urge before tic; 57% find urge more bothersome than the tic itself
Suppressibility	Hallmark feature distinguishing tics from other hyperkinetic movements; urge builds during suppression
Waxing and waning	Tics fluctuate; new tics emerge, old tics fade; worsened by stress/sleep deprivation

Diagnosis

DSM-5 criteria for Tourette syndrome: ≥2 motor tics + ≥1 phonic tic, present for ≥1 year, onset before age 18. If only motor or only phonic: chronic motor/vocal tic disorder. If <1 year: provisional tic disorder.

Functional Ticlike Behavior (FTLB)

A significant increase in explosive acute-onset ticlike behavior occurred during the COVID-19 pandemic, often linked to social media exposure ("#tourette" viewed >5 billion times on TikTok). Diagnostic criteria (European Society for the Study of Tourette Syndrome, 2022):

Major criteria (all 3 required for "definite"): Age of onset ≥12 years; rapid symptom progression; ≥4 of 9 phenomenologic features
Key distinguishing features from Tourette: Onset in trunk/extremities (not face), complex tics at onset, 87% female (vs. 76% male in TS), associated with depression/anxiety rather than OCD/ADHD, no response to antitic medications, responsive to CBT

Treatment of Tics

Treatment Algorithm

Psychoeducation: All patients — explain natural history, waxing/waning course, expected improvement in adulthood; watchful waiting acceptable if tics are not functionally impairing
Treat comorbidities: OCD (CBT first-line > SSRIs), ADHD (stimulants do NOT worsen tics overall; guanfacine/clonidine help both), depression/anxiety
Behavioral intervention (CBIT): First-line treatment; 8 sessions over 10 weeks; combines habit reversal therapy + exposure/response prevention + psychoeducation; reduces tics 26–31% (similar to medications); benefits persist in 74% at 1 year
Pharmacotherapy: When CBIT unavailable/insufficient or tics are severe
Botulinum toxin: For focal tics, especially with strong premonitory urge
Neuromodulation/DBS: Pallidal or thalamic DBS for medication-refractory, severe tics

Pharmacologic Options for Tics

Class	Agents	Evidence Level	Key Notes
α2-Adrenergic agonists	Clonidine, guanfacine	Moderate / Low	First-line medication class; best tolerated; also help ADHD; monitor for bradycardia, hypotension; taper to avoid rebound HTN
Atypical antipsychotics	Aripiprazole (FDA-approved ages 6–17), risperidone, ziprasidone	Moderate	Aripiprazole has safest CV/metabolic profile; risperidone useful for comorbid aggression; monitor weight, metabolic syndrome, EPS
Typical antipsychotics	Haloperidol (FDA; age ≥3), pimozide (FDA; age ≥12), fluphenazine	Moderate / Low	Effective but more EPS and TD risk; pimozide requires ECG and CYP2D6 genotyping; reserve for refractory cases
GABAergic agents	Topiramate, clonazepam, baclofen, levetiracetam	Low / Very Low	Topiramate: avoid weight gain; baclofen: consider for dystonic tics; clonazepam: comorbid anxiety only, addiction risk
VMAT2 inhibitors	Deutetrabenazine, valbenazine, tetrabenazine	Failed primary endpoints	Clinical trials failed primary tic reduction endpoint but reported improved QoL; consider as add-on for refractory cases
Selective D1 antagonist	Ecopipam	D1AMOND trial positive	First-in-class; met primary endpoint for tic reduction; well-tolerated (headache, somnolence, insomnia); promising new option
Botulinum toxin	OnabotulinumtoxinA	Moderate	Focal tics (face, neck); targeting the area of the premonitory urge most beneficial

Distinguishing Hyperkinetic Movements

Feature	Chorea	Myoclonus	Tics
Quality	Random, flowing, dance-like	Sudden, shock-like jerk	Patterned, stereotyped
Speed	Brief but slower than myoclonus	Lightning-fast (<100 ms)	Variable; can be brief or sustained
Pattern	Unpredictable, non-stereotyped	Variable; may be patterned in epileptic forms	Stereotyped, repetitive
Suppressibility	Partially suppressible	Not suppressible	Suppressed for variable periods (hallmark)
Premonitory urge	No	No	Yes (82%)
Worsening with action	May worsen	Action myoclonus prominent	Worsens with stress, not typically with action

References

Continuum (Minneap Minn). August 2025; 31(4 Movement Disorders). Articles: Huntington Disease and Chorea (pp 1066–1087); Tourette Syndrome and Tic Disorders (pp 1120–1137).
Caviness JN. Treatment of myoclonus. Neurotherapeutics. 2014;11(1):188–200.
Zutt R, van Egmond ME, Elting JW, et al. A novel diagnostic approach to patients with myoclonus. Nat Rev Neurol. 2015;11(12):687–697.