Vestibular agnosia in traumatic brain injury and its link to imbalance

Author:

Calzolari Elena1,Chepisheva Mariya1,Smith Rebecca M1,Mahmud Mohammad1ORCID,Hellyer Peter J2,Tahtis Vassilios13,Arshad Qadeer4,Jolly Amy5ORCID,Wilson Mark6,Rust Heiko1,Sharp David J5,Seemungal Barry M16ORCID

Affiliation:

1. Brain and Vestibular Group, Neuro-Otology Unit, Department of Brain Sciences, Charing Cross Hospital, Imperial College London, London, W6 8RF, UK

2. Centre for Neuroimaging Sciences, King’s College London, London WC2R 2LS, UK

3. King’s College Hospital NHS Foundation Trust, SE5 9RS, UK

4. InAmind Laboratory, Department of Neuroscience, Psychology and Behaviour, University of Leicester, Leicester, LE1 7RH, UK

5. C3NL, Department of Brain Sciences, Hammersmith Hospital, Imperial College London, London, W12 0NN, UK

6. St Mary’s Hospital Major Trauma Centre, Imperial College Healthcare NHS Trust, London, W2 1NY, UK

Abstract

Abstract Vestibular dysfunction, causing dizziness and imbalance, is a common yet poorly understood feature in patients with TBI. Damage to the inner ear, nerve, brainstem, cerebellum and cerebral hemispheres may all affect vestibular functioning, hence, a multi-level assessment—from reflex to perception—is required. In a previous report, postural instability was the commonest neurological feature in ambulating acute patients with TBI. During ward assessment, we also frequently observe a loss of vertigo sensation in patients with acute TBI, common inner ear conditions and a related vigorous vestibular-ocular reflex nystagmus, suggesting a ‘vestibular agnosia’. Patients with vestibular agnosia were also more unbalanced; however, the link between vestibular agnosia and imbalance was confounded by the presence of inner ear conditions. We investigated the brain mechanisms of imbalance in acute TBI, its link with vestibular agnosia, and potential clinical impact, by prospective laboratory assessment of vestibular function, from reflex to perception, in patients with preserved peripheral vestibular function. Assessment included: vestibular reflex function, vestibular perception by participants’ report of their passive yaw rotations in the dark, objective balance via posturography, subjective symptoms via questionnaires, and structural neuroimaging. We prospectively screened 918 acute admissions, assessed 146 and recruited 37. Compared to 37 matched controls, patients showed elevated vestibular-perceptual thresholds (patients 12.92°/s versus 3.87°/s) but normal vestibular-ocular reflex thresholds (patients 2.52°/s versus 1.78°/s). Patients with elevated vestibular-perceptual thresholds [3 standard deviations (SD) above controls’ average], were designated as having vestibular agnosia, and displayed worse posturography than non-vestibular-agnosia patients, despite no difference in vestibular symptom scores. Only in patients with impaired postural control (3 SD above controls’ mean), whole brain diffusion tensor voxel-wise analysis showed elevated mean diffusivity (and trend lower fractional anisotropy) in the inferior longitudinal fasciculus in the right temporal lobe that correlated with vestibular agnosia severity. Thus, impaired balance and vestibular agnosia are co-localized to the inferior longitudinal fasciculus in the right temporal lobe. Finally, a clinical audit showed a sevenfold reduction in clinician recognition of a common peripheral vestibular condition (benign paroxysmal positional vertigo) in acute patients with clinically apparent vestibular agnosia. That vestibular agnosia patients show worse balance, but without increased dizziness symptoms, explains why clinicians may miss treatable vestibular diagnoses in these patients. In conclusion, vestibular agnosia mediates imbalance in traumatic brain injury both directly via white matter tract damage in the right temporal lobe, and indirectly via reduced clinical recognition of common, treatable vestibular diagnoses.

Funder

The Medical Research Council

The Imperial Health Charity

NIHR Imperial Biomedical Research Centre

NIHR Clinical Doctoral Research Fellowship

The US Department of Defense - Congressionally Directed Medical Research Program

Publisher

Oxford University Press (OUP)

Subject

Neurology (clinical)

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