Abstract
A common presentation of inherited prion disease is Gerstmann-Sträussler-Scheinker syndrome, typically presenting with gait ataxia and painful dysaesthesiae in the legs evolving over 2-5 years. The most frequent molecular genetic diagnosis is a P102L mutation of the prion protein gene (PRNP). There is no explanation for why this clinical syndrome is so distinct from Creutzfeldt-Jakob disease, and biomarkers of the early stages of disease have not been developed. Here we aimed, first, at determining if quantitative neurophysiological assessments could predict clinical diagnosis or disability and monitor progression and, second, to determine the neuropathological basis of the initial clinical and neurophysiological findings. We investigated subjects known to carry the P102L mutation in the longitudinal observational UK National Prion Monitoring Cohort study, with serial assessments of clinical features, peripheral nerve conduction, H and F components, threshold tracking and histamine flare and itch response and neuropathological examination in some of those who died. Twenty-three subjects were studied over a period of up to 12 years, including 65 neurophysiological assessments at the same department. Six were symptomatic throughout and six became symptomatic during the study. Neurophysiological abnormalities were restricted to the lower limbs. In symptomatic patients around the time of, or shortly after, symptom onset the H-reflex was lost. Lower limb thermal thresholds were at floor/ceiling in some at presentation, in others thresholds progressively deteriorated. Itch sensation to histamine injection was lost in most symptomatic patients. In six patients with initial assessments in the asymptomatic stage of the disease, a progressive deterioration in the ability to detect warm temperatures in the feet was observed prior to clinical diagnosis and the onset of disability. All of these six patients developed objective abnormalities of either warm or cold sensation prior to the onset of significant symptoms or clinical diagnosis. Autopsy examination in five patients (including two not followed clinically) showed prion protein in the substantia gelatinosa, spinothalamic tracts, posterior columns and nuclei and in the neuropil surrounding anterior horn cells. In conclusion, sensory symptoms and loss of reflexes in Gerstmann-Sträussler-Scheinker syndrome can be explained by neuropathological changes in the spinal cord. We conclude that the sensory symptoms and loss of lower limb reflexes in Gerstmann-Sträussler-Scheinker syndrome is due to pathology in the caudal spinal cord. Neuro-physiological measures become abnormal around the time of symptom onset, prior to diagnosis, and may be of value for improved early diagnosis and for recruitment and monitoring of progression in clinical trials.
Highlights
Prion diseases, or transmissible spongiform encephalopathies, are a group of fatal neurodegenerative disorders affecting humans and animals (Collinge, 2001)
The situation is even more difficult in the inherited prion diseases because age at onset variation is high, and criteria are not optimized for an early diagnosis
Systematic history taking, rating scale analysis and review of clinical letters defined three milestones: (i) onset of any symptom that subsequently developed into part of the Gerstmann-StrausslerScheinker syndrome; (ii) onset of disability, defined as an MRC Prion Disease Rating Scale score 520; and (iii) the time at which the National Prion Clinic (NPC) clinician confirmed the diagnosis of Gerstmann-Straussler-Scheinker with patient and family
Summary
Transmissible spongiform encephalopathies, are a group of fatal neurodegenerative disorders affecting humans and animals (Collinge, 2001). The central mechanism of prion diseases is the conversion of host encoded prion protein (PrPC) to a misfolded multimeric state (Prusiner, 1982). Human prion diseases occur in sporadic, acquired and inherited forms. The majority develop progressive neurodegeneration with cognitive impairment and other neurological deficits primarily, but not exclusively, due to CNS dysfunction. Sporadic and acquired prion diseases generally follow a rapid course lasting less than 2 years. Not all, hereditary forms the duration of the disease is much longer ranging from 2 years, to more than 20 years
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