Progressive Supranuclear Palsy (PSP) is now recognized as a spectrum disorder with multiple clinical phenotypes beyond the classic Richardson syndrome. These variants have distinct clinical presentations, pathological findings, and prognostic implications. Accurate phenotype classification is critical for patient counseling, clinical trial enrollment, and understanding disease mechanisms.
| Variant |
Key Features |
Prevalence |
Prognosis |
| PSP-RS (Richardson) |
Vertical gaze palsy, falls, axial rigidity |
40-50% |
Most rapid progression |
| PSP-P |
Parkinsonism, asymmetric onset |
20-30% |
Slower progression |
| PSP-PAGF |
Pure akinesia, gait freezing |
5-10% |
Variable |
| PSP-C |
Cerebellar ataxia prominent |
5-10% |
Variable |
| PSP-F |
Frontal dysfunction predominant |
5-15% |
Variable |
| PSP-CBS |
Corticobasal features |
5-10% |
Variable |
The classic presentation of PSP, also known as Steele-Richardson-Olszewski syndrome, is characterized by:
- Vertical supranuclear gaze palsy: Downgaze impairment typically appears first
- Postural instability: Falls within first year of symptoms
- Axial rigidity: Neck and trunk stiffness, progressive akinesia
- Frontal cognitive dysfunction: Executive impairment, behavioral changes
- Pseudobulbar affect: Emotional incontinence
- Neurofibrillary tangles concentrated in brainstem (especially substantia nigra, colliculi)
- Globose nuclei involvement
- 4R tau accumulation in neurons and glia
- Tufted astrocytes
A phenotype resembling Parkinson's disease but with PSP pathology:
- Asymmetric onset: Unlike classic PSP
- Resting tremor: Present in ~50% of cases
- Levodopa response: Transient or modest benefit
- Less prominent gaze palsy: May develop later
- Later onset of falls: Typically after 2-3 years
Key differences from Parkinson's disease:
- Earlier falls
- Vertical gaze abnormalities
- Axial-predominant rigidity
- Poor levodopa response
-对称起始
Generally slower progression than PSP-RS, with longer survival (10-15 years vs 5-7 years).
Characterized by progressive gait freezing and akinesia without other PSP features initially:
- Gait freezing: Difficulty initiating walking, episodic freezing
- Micrographia: Small handwriting
- Low voice: Hypophonia
- No gaze palsy initially: May develop later
- Minimal cognitive impairment: Initially preserved
- Midbrain atrophy on MRI
- Reduced FDG uptake in posterior cortical regions
- Preserved dopaminergic function on DAT imaging
A variant with prominent cerebellar involvement:
- Ataxia: Gait and limb ataxia
- Nystagmus: Horizontal gaze-evoked nystagmus
- Scanning speech: Dysarthria with cerebellar features
- Limb ataxia: Appendicular cerebellar signs
- Less prominent gaze palsy: May develop later
- Greater cerebellar involvement
- Purkinje cell loss
- pontine base involvement
Characterized by predominant frontal lobe symptoms:
- Behavioral changes: Disinhibition, apathy
- Executive dysfunction: Planning, organization deficits
- Language problems: Non-fluent aphasia
- Cognitive impairment: Prominent early
- Less motor signs: Initially subtle
May be confused with:
- Frontotemporal dementia
- Primary progressive aphasia
- Behavioral variant FTD
Some patients present with features of both PSP and corticobasal syndrome:
- Asymmetric rigidity: Corticobasal pattern
- Apraxia: Hand coordination deficits
- Alien limb phenomena: Rare
- Cortical sensory loss: Later features
- PSP features: Gaze palsy, falls develop
- Both are 4R tauopathies
- CBD and PSP share tau pathology patterns
- Some cases show mixed pathology
A variant with prominent cerebellar involvement:
- Progressive gait ataxia: Wide-based, unsteady gait
- Limb ataxia: Incoordination of arms and legs
- Scanning speech: Dysarthria with cerebellar qualities
- Nystagmus: Gaze-evoked horizontal nystagmus
- Ocular motor findings: May include downgaze palsy developing later
- Less prominent parkinsonism: May lack significant rigidity or tremor
- MRI: Significant pontine and cerebellar atrophy
- FDG-PET: Hypometabolism in cerebellar hemispheres and brainstem
- DTI: White matter degeneration in cerebellar peduncles
The cerebellar variant of PSP (PSP-C) can be challenging to distinguish from MSA-C (cerebellar variant of multiple system atrophy):
| Feature |
PSP-C |
MSA-C |
| Disease duration |
Typically longer |
Shorter progression |
| Eye movements |
Supranuclear gaze palsy |
Internuclear ophthalmoplegia |
| Autonomic failure |
Variable, less prominent |
Prominent early |
| Levodopa response |
May have transient response |
Poor response |
| Tau pathology |
4R tau deposits |
Alpha-synuclein deposits |
Population-based studies have estimated the distribution of PSP variants:
- PSP-RS (Richardson syndrome): 40-50% of all PSP cases — the most common variant
- PSP-P (Parkinsonism variant): 20-30% — second most common
- PSP-PAGF (Pure akinesia with gait freezing): 5-10%
- PSP-F (Frontal variant): 5-15%
- PSP-CBS (Corticobasal overlap): 5-10%
- PSP-C (Cerebellar variant): 5-10%
- Age of onset varies by variant: PSP-P tends to have later onset (mean 72 years) compared to PSP-RS (mean 63 years)
- Sex distribution is roughly equal across variants
- Disease duration ranges from 5-7 years (PSP-RS) to 10-15 years (PSP-P)
The International Parkinson and Movement Disorders Society (MDS) established criteria for PSP diagnosis:
Core clinical features:
- Vertical supranuclear gaze palsy
- Progressive gait impairment with falls within first year
- Early postural instability (Pull test score ≥2)
Supportive features:
- Early cognitive impairment (frontal executive dysfunction)
- Pseudobulbar affect
- Bradykinesia with axial rigidity
- Asymmetric onset of parkinsonism
- Resting tremor present in ~50%
- Transient levodopa response possible
- Less prominent gaze palsy (may develop after 2-3 years)
- Progressive gait freezing without other PSP features for ≥2 years
- No vertical gaze palsy initially
- No significant cognitive impairment at onset
- Prominent frontal behavioral changes (apathy, disinhibition)
- Early executive dysfunction
- Relative motor preservation initially
| Variant |
Levodopa Response |
Anticholinergics |
Botulinum Toxin |
| PSP-RS |
Poor |
Minimal |
For dystonia |
| PSP-P |
Transient |
May help |
For dystonia |
| PSP-PAGF |
Poor |
Variable |
Limited |
| PSP-F |
Poor |
Variable |
Limited |
| PSP-CBS |
Variable |
Variable |
For spasticity |
- Multidisciplinary care team
- Fall prevention strategies
- Speech and swallowing evaluation
- Eye movement aids (prism glasses)
- Trial of levodopa (may provide temporary benefit)
- Parkinson's disease medications for symptom management
- Standard PSP supportive care
- Physical therapy for gait training
- Assistive devices for mobility
- Speech therapy if needed
- Behavioral interventions
- Environmental modifications
- Caregiver support
- Cognitive enhancers (modest benefit)
The different PSP variants have distinct prognostic implications:
- PSP-RS: Mean survival 5-7 years from symptom onset
- PSP-P: Mean survival 10-15 years (slower progression)
- PSP-PAGF: Variable, often 7-12 years
- PSP-F: Variable, often 6-10 years
- PSP-CBS: Variable, often 6-9 years
- PSP-C: Variable, often 7-12 years
Disease progression follows variant-specific patterns:
- PSP-RS: Rapid progression, early loss of independence
- PSP-P: Slower functional decline, longer independent period
- PSP-F: Cognitive decline precedes motor disability
- PSP-CBS: Asymmetric progression, early apraxia
Recent studies have identified variant-specific biomarker patterns:
- Tau PET uptake patterns: Higher uptake in basal ganglia for PSP-RS, different patterns for PSP-CBS
- CSF p-tau181: Elevated across variants, but may differ in magnitude
- NfL (Neurofilament light chain): Elevated in all variants, highest in PSP-RS
Variant-specific genetic risk factors are emerging:
- MAPT H1 haplotype: Risk factor for all PSP variants
- PSP-P: May have stronger association with specific MAPT subhaplotypes
- Stereotypic variants: Some genetic variants may influence phenotype
¶ Tau Strain Biology and Variants
Different clinical variants may reflect distinct tau molecular strains:
- Cryo-EM studies: Have identified structural differences in tau filaments between variants
- PSP-RS: More compact tau filament structures
- PSP-CBS: May show intermediate structures
- Strain-specific seeding: Different variants may respond differently to anti-tau therapies
- Tau Seeding Activity: 4R-tau seeding activity reveals molecular subtypes in progressive supranuclear palsy[^recent1]
- PET Imaging: PET evaluation of cholinergic system differences in progressive supranuclear palsy and age-matched controls[^recent2]
- Clinical Variants: Corticobasal syndrome presenting as a progressive hemiparetic syndrome: a case report[^recent3]
- Molecular subtyping based on tau seeding activity may enable personalized therapeutic approaches
- Cholinergic system imaging shows distinct patterns in PSP compared to other parkinsonisms
- Early recognition of atypical presentations improves diagnostic accuracy