Brainstem reflex testing provides a non-invasive method for assessing the integrity of brainstem neural circuits, particularly those involving the pons and medulla. These reflexes are particularly valuable in the evaluation of atypical parkinsonian syndromes, including [Corticobasal Syndrome (CBS)][/diseases/corticobasal-syndrome], as they can help differentiate between central and peripheral involvement patterns.
The blink reflex, startle reflex, and corneal reflex are the most commonly assessed brainstem reflexes in clinical practice. Each provides unique insights into specific brainstem pathways that may be differentially affected in CBS versus other parkinsonian disorders such as [Progressive Supranuclear Palsy (PSP)][/diseases/progressive-supranuclear-palsy].
¶ Anatomy and Physiology
The blink reflex is a triphasic reflex with two components:
-
R1 component: An early, oligosynaptic reflex arc involving the trigeminal nerve (afferent), the pons (facial nucleus), and the facial nerve (efferent). This component has a latency of approximately 30-40 ms and represents the most direct pathway.
-
R2 component: A longer-latency, polysynaptic reflex that involves more complex circuitry through the brainstem reticular formation. R2 latency is approximately 50-60 ms and shows habituation with repeated stimulation.
In [Corticobasal Syndrome][/diseases/corticobasal-syndrome], the blink reflex typically shows:
- Prolonged R1 latency: Reflects damage to the pontine portion of the reflex arc
- Reduced R2 amplitude: Indicating involvement of the reticular formation pathways
- Abnormal recovery curves: Suggests dysfunction in the inhibitory mechanisms that modulate the reflex
- Asymmetric findings: Common in CBS due to the typically asymmetric cortical-subcortical involvement
The blink reflex is particularly useful for differentiating CBS from [Parkinson's Disease (PD)][/diseases/parkinsons-disease], as PD patients typically show normal or near-normal blink reflex parameters, while CBS patients demonstrate more significant abnormalities.
| Parameter |
CBS |
PSP |
PD |
| R1 Latency |
Prolonged |
Normal or mildly prolonged |
Normal |
| R2 Amplitude |
Reduced |
Moderately reduced |
Normal |
| Asymmetry |
Marked (common) |
Mild-moderate |
None |
| Recovery Curve |
Abnormal |
Abnormal |
Normal |
¶ Anatomy and Physiology
The startle reflex is a polysensory response to sudden, unexpected stimuli (auditory, visual, or tactile). The primary pathway involves:
- Acoustic pathway: Via the cochlear nerve to the cochlear nuclei
- Brainstem integration: Through the nucleus reticularis pontis caudalis
- Motor output: Via the facial nucleus, trigeminal nucleus, and spinal motor neurons
Patients with CBS may show:
- Exaggerated startle responses: Due to loss of cortical inhibition
- Prolonged latencies: Indicating brainstem pathway involvement
- Abnormal habituation: Failure to suppress the response with repeated stimuli
¶ Anatomy and Physiology
The corneal reflex involves:
- Afferent: Ophthalmic division of the trigeminal nerve (V1)
- Central pathway: Pontine brainstem
- Efferent: Facial nerve (orbicularis oculi muscle)
The corneal reflex is typically preserved in early CBS but may show:
- Reduced amplitude: With disease progression
- Prolonged latency: With brainstem involvement
- Asymmetry: Correlating with the asymmetric clinical presentation
¶ Standard Blink Reflex Recording
| Parameter |
Specification |
| Stimulation |
Supraorbital nerve, 0.1-0.2 ms square wave pulses |
| Intensity |
2-3× sensory threshold |
| Recording |
Orbicularis oculi muscle (both sides) |
| Ground |
Forehead |
| Bandpass |
20-2000 Hz |
| Component |
Latency (ms) |
Amplitude (μV) |
| R1 |
30-40 |
200-500 |
| R2 |
50-60 |
200-600 |
- Prolonged R1 with normal R2: Peripheral facial nerve lesion
- Prolonged R1 and R2: Brainstem lesion (pons)
- Absent R2 with normal R1: Facial nerve lesion or severe brainstem involvement
- Prolonged R2 only: Extrapontine lesion
Brainstem reflex testing aids in differentiating:
- CBS from PD: CBS shows significant R1 prolongation and R2 abnormalities; PD typically shows normal reflexes
- CBS from PSP: Both may show abnormalities, but PSP tends toward more central (symmetric) involvement, while CBS shows asymmetric patterns
- CBS from Multiple System Atrophy (MSA): MSA often shows more severe brainstem involvement with early R2 changes
Serial brainstem reflex testing can track disease progression in CBS:
- Progressive R1 prolongation indicates worsening pontine involvement
- Declining R2 amplitudes reflect reticular formation dysfunction
- Development of asymmetry indicates lateralized disease progression
¶ Limitations and Considerations
- False negatives: Early CBS may have normal reflexes
- Medication effects: Antipsychotics and other drugs can alter reflex parameters
- Technical factors: Electrode placement and stimulus intensity must be standardized
- Complementary testing: Brainstem reflexes should be interpreted alongside other neurophysiological and neuroimaging findings
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