Differentials
Tardive dyskinesia
SIGNS / SYMPTOMS
Typically does not have a family history.
Can occur in patients treated with antipsychotic medications or metoclopramide.[34]
Tends to have a distinct oral, buccal, and lingual predominance, with speech and swallowing relatively unaffected.
Motor impersistence not seen.
Not progressive.
INVESTIGATIONS
The distinction between tardive dyskinesia and Huntington disease is primarily clinical.
In the unlikely event it is needed, CAG repeat testing is normal.
Referral to a movement disorders specialist would typically be more cost effective.
Dentatorubro-pallidoluysian atrophy (DRPLA)
SIGNS / SYMPTOMS
More common in Asian people but otherwise may be phenotypically indistinguishable from Huntington disease.[35]
In juvenile or early-onset cases, myoclonic epilepsy is a finding highly suggestive of DRPLA.
In black patients, DRPLA may manifest without myoclonic epilepsy.
INVESTIGATIONS
CAG repeat testing is normal, but testing for the gene for DRPLA (atrophin-1) will be positive.
In black patients, MRI may demonstrate globus pallidus microcalcifications with demyelination in the centrum semiovale (Haw River syndrome).
Neuroacanthocytosis
SIGNS / SYMPTOMS
Often has associated areflexia and distal amyotrophy with greater prominence of oral and lingual chorea with tics and tongue biting.[36]
May be phenotypically indistinguishable from Huntington disease, but inheritance is autosomal recessive.
INVESTIGATIONS
CAG repeat testing is normal.
Acanthocytes may be present on the peripheral blood smear, but repeated tests or dilution may be needed to discover them.
It is helpful to direct the laboratory to comment specifically on red blood cell morphology.
Creatine kinase is often elevated.
The genetic abnormality is a frameshift mutation in the gene coding for chorein.
Benign hereditary chorea
SIGNS / SYMPTOMS
An autosomal dominant disorder tending to be one of fairly early onset with very slow progression, without cognitive dysfunction or the other disabling features of Huntington disease.[37][38]
Atypical features, with some functional impairment, may occur.
INVESTIGATIONS
CAG repeat testing is normal.
An abnormality can be found in the gene coding for thyroid transcription factor 1 (TTF1).
McLeod syndrome (or McLeod myopathy)
SIGNS / SYMPTOMS
X-linked disorder; may be indistinguishable from Huntington disease.[39]
May have the additional features of axonal motor neuropathy, myopathy, cardiomyopathy, and anemia.
INVESTIGATIONS
Complete blood count testing reveals acanthocytes, hemolytic anemia.
Serum creatine kinase is elevated.
There is an abnormality in the gene XK (Kell erythrocyte antigen).
CAG repeat testing is normal.
Spinocerebellar ataxia 17
Huntington disease-like-1 (HDL1)
SIGNS / SYMPTOMS
A familial prion disorder that can be phenotypically indistinguishable from Huntington disease.[42]
INVESTIGATIONS
CAG repeat testing for Huntington disease is normal.
Genetic testing reveals a PRNP gene mutation.
Cerebellar atrophy and multicentric plaques that stain with anti-prion antibodies may be found at autopsy.
Huntington disease-like-2 (HDL2)
SIGNS / SYMPTOMS
Seen primarily in black patients.
Phenotypically identical to Huntington disease.[40]
INVESTIGATIONS
CAG repeat testing for Huntington disease is normal but a CAG/CTG repeat disorder is found in the gene for junctophilin-3.
Huntington disease-like-3 (HDL3)
Neurodegeneration with brain iron accumulation (NBIA; Hallervorden Spatz syndrome)
SIGNS / SYMPTOMS
Autosomal recessive disorder.[45]
May be phenotypically indistinguishable from Huntington disease.
INVESTIGATIONS
MRI scan shows a characteristic hypointense globus pallidus with foci of hyperintensity ("eye of the tiger" sign).
CAG repeat testing is normal.
PANK2 (pantothenate kinase) mutations are present on genetic testing.
Neuroferritinopathy (NBIA2)
SIGNS / SYMPTOMS
May be phenotypically indistinguishable from Huntington disease.[46]
Tends to have more facial action dystonia and more asymmetry of findings.
INVESTIGATIONS
MRI shows a T2 signal loss in the basal ganglia.
Serum ferritin may be decreased.
CAG repeat testing is normal; mutations for the ferritin light chain (FTL) are present.
Hyperthyroid chorea
SIGNS / SYMPTOMS
Chorea and behavioral abnormalities may be manifestations of thyrotoxicosis.[47]
INVESTIGATIONS
Elevated thyroid function tests will be seen.
CAG repeat testing is normal.
Chorea gravidarum
SIGNS / SYMPTOMS
Typically, this is a manifestation of the first trimester of pregnancy, is nonhereditary, is of acute onset, and is not associated with other features of Huntington disease.[48]
INVESTIGATIONS
Pregnancy testing is positive.
Sydenham chorea
SIGNS / SYMPTOMS
Typically seen in children or young adults.[49]
Subacute, sometimes asymmetric in onset, nonhereditary, and postinfectious.
INVESTIGATIONS
Antistreptolysin O titers are elevated.
Lupus cerebritis
SIGNS / SYMPTOMS
Rarely, chorea and/or cognitive impairment may be manifestations of central nervous system lupus erythematosus.[50]
It is not associated with other features of Huntington disease.
INVESTIGATIONS
Antinuclear antibody titers are elevated.
Antiphospholipid antibody syndrome
SIGNS / SYMPTOMS
May cause chorea in some patients and sometimes begins asymmetrically.[51]
It is not associated with other features of Huntington disease.
INVESTIGATIONS
Antiphospholipid antibodies are detected.
Wilson disease (hepatolenticular degeneration)
SIGNS / SYMPTOMS
Associated with a progressive (usually nonchoreiform) movement disorder, psychiatric and cognitive deficits, and progressive hepatic dysfunction.[52]
Resembles juvenile Huntington disease.
INVESTIGATIONS
CAG repeat testing is normal.
Serum ceruloplasmin is decreased. Serum and urine copper abnormalities, Kayser-Fleischer rings, and MRI abnormalities are readily apparent.
In early cases serum ceruloplasmin may be in the low-normal range.
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