PSP Ocular Motor Examination

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PSP Ocular Motor Examination

Introduction

The ocular motor examination is a critical component in the diagnosis of Progressive Supranuclear Palsy (PSP), as eye movement abnormalities are among the earliest and most characteristic features of the disease. Vertical supranuclear gaze palsy, particularly affecting downgaze, is considered the hallmark clinical sign that distinguishes PSP from other Parkinsonian disorders[@steele1964]. The Movement Disorder Society (MDS) has established diagnostic criteria that incorporate specific ocular motor findings as essential or supportive features for PSP diagnosis[@hoglinger2017].

This page provides a comprehensive review of the ocular motor abnormalities observed in PSP, including the neuroanatomical basis, examination techniques, quantitative testing protocols, and the utility of these findings in differentiating PSP from related disorders such as Parkinson's disease (PD) and Corticobasal Syndrome (CBS).

Neuroanatomical Basis

Neural Pathways for Vertical Eye Movements

Vertical saccades are generated by a complex network of subcortical structures. The key components include:

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PSP Ocular Motor Examination

Introduction

Neuroanatomical Basis

Neural Pathways for Vertical Eye Movements

Vertical saccades are generated by a complex network of subcortical structures. The key components include:

Superior colliculus: Midbrain structure critical for initiating saccades, with separate maps for vertical and horizontal movements
Reticular formation: Contains burst neurons that trigger saccades and pause neurons that inhibit them
Posterior commisure: Acts as a conduit for vertical saccade signals
Rostral interstitial nucleus of MLF (riMLF): Key for vertical saccade generation, particularly for downward movements
Interstitial nucleus of Cajal: Involved in vertical gaze holding and torsional movements

In PSP, tau pathology preferentially affects these midbrain structures, particularly the superior colliculus and surrounding periaqueductal gray matter, leading to the characteristic vertical gaze impairment[@dickson2018].

Why Vertical Saccades Are Affected First

The selective vulnerability of vertical saccades in PSP relates to the topographical distribution of tau pathology. The neurofibrillary tangles in PSP show a predilection for:

Brainstem nuclei controlling vertical gaze (riMLF, interstitial nucleus of Cajal)
Pretectal area
Superior colliculus

Horizontal saccade pathways are relatively spared until later disease stages because they involve different brainstem circuits (paramedian pontine reticular formation) that are less affected by PSP pathology.

4R-Tauopathy and Vertical Gaze Vulnerability

The selective targeting of vertical saccade pathways in PSP reflects the unique pattern of 4-repeat (4R) tau pathology:

Molecular Mechanisms

Tau isoform expression: PSP brains show increased 4R tau relative to 3R tau. The 4R isoform has distinct binding properties that may preferentially affect certain neuronal populations.

Oligodendrocyte involvement: 4R tau pathology in oligodendrocytes (which produce 4R tau) may affect the white matter tracts connecting brainstem eye movement nuclei.

Neuronal vulnerability: Neurons in the riMLF and interstitial nucleus of Cajal express high levels of tau-phosphorylating kinases and have long axons with complex cytoskeletons — both factors increasing susceptibility to tau pathology.

Anatomical Predilection

The midbrain structures controlling vertical gaze have several characteristics that make them vulnerable to 4R tau:

| Structure | Function | Vulnerability Factor |
|------------|----------|---------------------|
| riMLF | Vertical saccade generation | High metabolic demand, long axons |
| Interstitial nucleus of Cajal | Vertical gaze holding | Continuous neural activity |
| Superior colliculus | Saccade initiation | Dense synaptic connections |
| Pretectal area | Pupillary control, gaze shifts | Complex integration requirements |

Progression Pattern

The hierarchical vulnerability in PSP follows a predictable pattern:

Earliest: Downward saccade slowing (riMLF neurons controlling downgaze are smaller and more vulnerable)

Early: Complete downgaze palsy

Mid-stage: Upgaze involvement

Late: Horizontal saccade impairment as pathology spreads to pontine reticular formation

This progression reflects the rostral-to-caudal spread of tau pathology in the brainstem, with the most rostral structures (controlling vertical gaze) affected first.

Key Ocular Motor Findings in PSP

1. Vertical Supranuclear Gaze Palsy

Description: The most characteristic finding in PSP, presenting as impaired vertical saccades with relatively preserved vertical eye movements on reflexive testing (e.g., oculocephalic maneuver).

Pathophysiology: The impairment represents a supranuclear (above the oculomotor nuclei) lesion. Patients can generate vertical eye movements when prompted by head impulses or caloric testing, indicating intact brainstem ocular motor nuclei and nerves.

Pattern:

Downgaze typically affected first — patients have difficulty looking downward
Upgaze affected later — progression to involve upward gaze
Horizontal saccades relatively preserved early — become impaired in later stages

Clinical significance: Vertical supranuclear gaze palsy is one of the most specific signs for PSP, present in 70-90% of patients with classic Richardson syndrome[@bhatt1993]. Its presence, especially when combined with early falls, strongly supports PSP over PD.

2. Slowing of Vertical Saccades

Quantitative finding: Reduced peak velocity of vertical saccades, even when the saccade can be completed.

Measurement:

Normal vertical saccade velocity: >300-400°/sec
PSP vertical saccade velocity: Often <200°/sec
Horizontal saccades typically remain >300°/sec in early PSP

Progression pattern:

First observed in downward saccades

Progresses to upward saccades

Eventually horizontal saccades become slow in moderate-to-severe PSP

Diagnostic utility: Slowing of vertical saccades can be detected before complete gaze palsy develops, making it valuable for early diagnosis. It is included in the MDS-PSP diagnostic criteria as a supportive finding.

3. Square Wave Jerks

Description: Involuntary, repetitive, horizontal saccadic movements that interrupt fixation. Each jerk consists of a saccade away from the target followed by a quick return.

Characteristics:

Amplitude: Typically 1-5° (small)
Frequency: 1-2 Hz
Occur during attempted fixation
More prominent in primary position

Pathophysiology: Related to impaired fixational stability due to frontal eye field and superior colliculus involvement. Reflects a failure of the saccadic suppression mechanism.

Differential diagnosis:

PSP: Prominent square wave jerks, especially as disease progresses
PD: Less prominent, usually in later stages
Huntington's disease: More prominent and higher amplitude
Normal aging: Occasional, low frequency

Clinical significance: Square wave jerks are common in PSP (present in 50-70% of patients) and contribute to the characteristic "staring" appearance. They are supportive of PSP diagnosis but not specific.

Other Saccadic Intrusions in PSP

While square wave jerks are the most common saccadic intrusion in PSP, several other patterns may be observed:

Glissadic Saccades

Glissades are small saccadic movements occurring at the end of primary saccades:

Characteristics: Small amplitude (1-3°), typically in the direction of the primary saccade
Prevalence: Present in 25-35% of PSP patients
Pathophysiology: Impaired cerebellar-mediated saccade termination
Clinical significance: More prominent than in PD, indicates cerebellar involvement

Antisaccade Deficits

The antisaccade task — where patients must look away from an appearing target — is particularly sensitive to PSP:

Error rate: PSP patients make errors 40-80% of the time (normal <15%)
Pathophysiology: Frontal lobe dysfunction affecting suppressive signals
Clinical significance: More severe deficits than in PD, reflects frontal/executive involvement

Saccadic Latency Prolongation

PSP patients demonstrate prolonged latency for:

Voluntary saccades: 300-500ms (normal 150-250ms)
Reflexive saccades: Relatively preserved
Clinical significance: Indicates cortical involvement vs. brainstem-only pathology

4. Eyelid Opening Apraxia (Blepharospasm)

Description: Inability to voluntarily open the eyes despite intact orbicularis oculi muscle function. Patients may use compensatory behaviors such as head tilt or eyebrow raising to open their eyes.

Clinical features:

Patients report "heavy eyelids" or inability to open eyes on command
May improve with sensory tricks (touching forehead or eyebrows)
Often accompanied by reduced blink rate
Can be present even when eyes are open

Pathophysiology: Related to degeneration of the pretectal area and frontal eye fields, which normally facilitate eyelid opening. The levator palpebrae superioris muscle is intact but cannot be activated voluntarily.

Differential from blepharospasm:

Blepharospasm: Involuntary orbicularis oculi contraction (closing)
Eyelid opening apraxia: Inability to initiate levator contraction (opening)
Can coexist in PSP

Clinical significance: Present in 30-50% of PSP patients, typically in moderate disease stages. Contributes to functional blindness and is a supportive feature for PSP diagnosis.

5. Reduced Blink Rate

Description: Decreased spontaneous blink frequency, typically <10-15 blinks per minute (normal: 15-20).

Clinical features:

Patients may report dry eyes, irritation
Contributes to corneal exposure risk
Often accompanies facial masking (hypomimia)

Pathophysiology: Related to reduced dopaminergic input to the frontal eye fields and basal ganglia circuits controlling blink generation.

6. Convergence Insufficiency

Description: Inability to maintain convergence, leading to diplopia at near.

Clinical features:

Difficulty reading or doing close work
May close one eye to compensate
Can be asymmetric

Pathophysiology: Related to midbrain involvement affecting the convergence center.

Additional Vergence Abnormalities in PSP

Beyond convergence insufficiency, PSP patients may exhibit:

Divergence Paresis

Pattern: Limited ability to diverge eyes for distance viewing
Clinical features: Intermittent diplopia at distance, may be mistaken for ocular motor palsy
Pathophysiology: Midbrain pretectal area involvement

Accommodative Dysfunction

Reduced accommodation: Difficulty focusing on near targets
Often coexists with convergence insufficiency
Contributes to: Reading difficulty, eye strain

Vergence Averages

| Vergence Type | PSP Finding | Clinical Impact |
|---------------|-------------|-----------------|
| Convergence | Reduced (50-70%) | Diplopia at near |
| Divergence | Variable (20-40%) | Diplopia at distance |
| Accommodative | Reduced (30-50%) | Difficulty reading |

Quantitative Testing

Research settings may assess:

Vergence facility: Ability to change focus between near and far
Vergence peak velocity: Speed of vergence movements
Vergence accuracy: Endpoint accuracy

Examination Protocol

Bedside Examination

A structured bedside ocular motor examination for suspected PSP should include:

1. Fixation Assessment

Observe patient at rest in primary gaze
Note: square wave jerks, blink rate, eyelid position
Duration: 30-60 seconds

2. Pursuit Testing

Test horizontal and vertical smooth pursuit
Use smooth, predictable targets
Note: catch-up saccades, impaired pursuit gain

3. Saccade Assessment (Key Test)

Horizontal saccades: Ask patient to look left-right between two targets
Vertical saccades: Ask patient to look up-down between targets
Test both spontaneous (self-paced) and reflexive saccades
Critical: Compare vertical vs. horizontal saccade velocity and accuracy

4. Gaze Holding

Test ability to hold eccentric gaze
Note: gaze-evoked nystagmus (suggests cerebellar involvement)

5. Head Impulse Test

Rapidly turn patient's head while they fixate on a target
Intact vestibulo-ocular reflex allows maintained fixation
Abnormal (corrective saccades) suggests peripheral vestibular issue

6. Oculocephalic Reflexes (Doll's Eyes)

Only performed when patient is unable to cooperate with voluntary testing
Test vertical and horizontal eye movements
Preserved in supranuclear gaze palsy (brainstem intact)

7. Convergence Testing

Test near target focus
Note: ability to converge, nystagmus

Quantitative Oculography Protocol

For research or detailed clinical assessment, quantitative measurements provide objective data:

Equipment

Infrared/video oculography (VOG)
Electrooculography (EOG)
Search coil technique (gold standard)

Standard Test Battery

Reflexive saccades: Random target jumps, 10-20° amplitude

Measure: latency, velocity, accuracy

2. Self-paced saccades: Alternating between two targets

Measure: velocity, timing

3. Antisaccades: Look away from target

Measure: error rate (reflects frontal lobe function)

4. Smooth pursuit: Sinusoidal target motion

Measure: gain, catch-up saccades

5. Blink rate: Measured during fixation

Normal Values (Adults)

| Parameter | Normal | PSP Finding |
|-----------|--------|-------------|
| Vertical saccade velocity | >300°/sec | <200°/sec |
| Horizontal saccade velocity | >300°/sec | Usually preserved early |
| Saccade latency | 150-250ms | May be prolonged |
| Antisaccade error rate | <15% | Elevated in PSP |
| Blink rate | 15-20/min | <10/min |

MDS-PSP Diagnostic Criteria

The 2017 MDS diagnostic criteria for PSP incorporate ocular motor findings as essential and supportive features[@hoglinger2017]:

Core Clinical Features

| Feature | PSP-RS | PSP-P |
|---------|--------|-------|
| Ocular motor dysfunction | Required | Supportive |
| Vertical supranuclear gaze palsy | Essential | — |
| Slow vertical saccades | Supportive | Supportive |
| Initiation failure | — | — |

Essential Feature for Probable PSP-RS

Age >40 years
Progressive disease
Vertical supranuclear gaze palsy OR
Slow vertical saccades AND prominent postural instability with falls within 3 years

Supportive Ocular Motor Features

Squared wave jerks during fixation
Eyelid opening apraxia
Reduced blink rate
Impaired convergence

Diagnostic Levels

Clinically definite PSP:

Pathological confirmation OR
Classic PSP-RS with 5+ years symptom duration

Probable PSP:

Required: Progressive disease, age >40, at least 2 core features OR
1 core feature + at least 2 supportives

Possible PSP:

Required: Progressive disease, at least 1 core feature or 2 supportives

Differential Diagnosis

PSP vs. Parkinson's Disease

| Feature | PSP | PD |
|---------|-----|-----|
| Vertical gaze palsy | Present early (70-90%) | Absent (unless advanced) |
| Vertical saccade slowing | Present early | Normal until late |
| Square wave jerks | Prominent | Mild/late |
| Eyelid opening apraxia | Common (30-50%) | Rare |
| Blink rate | Markedly reduced | Mildly reduced |
| Gaze palsy pattern | Downgaze first | None |

Key differentiators: Vertical supranuclear gaze palsy in PSP vs. normal vertical eye movements in PD is the single most important distinction. PSP patients also show saccade slowing in the vertical axis early, while PD patients maintain normal vertical saccade velocity until very late stages.

PSP vs. Corticobasal Syndrome (CBS)

| Feature | PSP-CBS | CBS |
|---------|---------|-----|
| Vertical gaze palsy | Variable (50-70%) | Uncommon |
| Square wave jerks | Present | May be present |
| Apraxia of eyelid opening | May be present | May be present |
| Ocular motor apraxia | Common | Common |

Overlap: PSP-CBS shows significant clinical overlap, as both can have ocular motor abnormalities. However:

PSP more consistently shows vertical supranuclear gaze palsy
CBS often has asymmetric apraxia of eyelid opening
Quantitative saccade testing may help differentiate

PSP vs. Multiple System Atrophy (MSA)

| Feature | PSP | MSA |
|---------|-----|-----|
| Vertical supranuclear gaze palsy | Common | Rare |
| Square wave jerks | Present | May be present |
| Ocular motor findings | Vertical > horizontal | Horizontal > vertical |

Early-Stage Diagnostic Challenges

In early disease (<3 years), the diagnosis can be challenging. Red flags suggesting PSP over PD:

Early vertical saccade slowing (even without complete gaze palsy)
Early falls or postural instability
Axial rigidity (neck/trunk) predominant over limb
Dysarthria prominent early
Reduced blink rate marked

Clinical Utility and Limitations

Advantages of Ocular Motor Examination

Non-invasive: No special equipment needed for bedside testing

Objective findings: Quantitative measures available

Early detection: Saccade slowing may precede gaze palsy

High specificity: Vertical supranuclear gaze palsy is fairly specific for PSP

Progression monitoring: Serial examinations track disease progression

Differential diagnosis: Helps distinguish PSP from PD, CBS, MSA

Limitations

Not pathologically specific: Similar findings can occur in other neurodegenerative conditions

Overlap with CBS: Significant clinical overlap in PSP-CBS variant

Patient cooperation required: Accurate assessment needs cooperative patient

Late onset in some variants: Some PSP variants (e.g., PSP-PAGF) may have minimal ocular findings early

Quantification needed: Subtle slowing requires quantitative testing for detection

Treatment Considerations

Symptomatic Management

While no disease-modifying treatments exist for PSP, some ocular motor symptoms can be managed:

Eyelid opening apraxia: Botulinum toxin injections to orbicularis oculi may provide partial relief
Blepharospasm: Botulinum toxin injections
Dry eye: Artificial tears, lubricating ointments
Convergence insufficiency: Prism glasses

Medication Effects

Dopaminergic medications (levodopa, dopamine agonists) provide minimal benefit for ocular motor symptoms in PSP, distinguishing it from PD where these medications often improve eye movements.

Summary

Ocular motor examination is a cornerstone of PSP diagnosis and monitoring. Key findings include:

Vertical supranuclear gaze palsy — the hallmark sign, affecting downgaze first

Slowed vertical saccades — detectable before complete gaze palsy

Square wave jerks — present in majority of patients

Eyelid opening apraxia — common in moderate disease

Reduced blink rate — contributes to functional impairment

These findings are incorporated into the MDS-PSP diagnostic criteria and help differentiate PSP from PD and other Parkinsonian syndromes. The examination can be performed at bedside with minimal equipment, though quantitative testing provides additional sensitivity for early diagnosis and research purposes.

References

[Steele JC, Richardson JC, Olszewski J, Progressive supranuclear palsy (1964)](https://pubmed.ncbi.nlm.nih.gov/14149684/)

[Hoglinger GU, Respondek G, Stamelou M, et al, Clinical diagnosis of progressive supranuclear palsy: The movement disorder society criteria (2017)](https://pubmed.ncbi.nlm.nih.gov/28467049/)

Dickson DW, Rademakers R, Hoggoth DM, Neuropathology of progressive supranuclear palsy (2018)

[Bhatt MH, Posner VH, Martin WR, et al, Longitudinal changes in eye movements in progressive supranuclear palsy (1993)](https://pubmed.ncbi.nlm.nih.gov/8334756/)

[MacDonald BK, Cockerell OA, Sander JW, Shorvon SD, The incidence and lifetime prevalence of neurological disorders in a prospective community-based study in the UK (2000)](https://pubmed.ncbi.nlm.nih.gov/10734001/)

[Dickson DW, Ahmed Z, Algom AA, et al, Neuropathology of older persons without cognitive impairment from two community-based studies (2016)](https://pubmed.ncbi.nlm.nih.gov/26962727/)

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