Sensory disturbances are part of the clinical picture of Parkinson’s disease. Abnormalities in sensory processing, through a basal ganglia involvement, are thought to be responsible for the sensory dysfunction since sensory nerve conduction velocity (NCV) is usually normal.However, NCVdoes not examine small fibres or terminal endings of large sensory fibres, whereas skin biopsy is more suitable for these purposes.To evaluate peripheral sensory nerves in Parkinson’s disease, we studied cutaneous free and encapsulated sensory nerve endings in 18 patients and 30 healthy controls using 3-mm punch biopsies from glabrous and hairy skin. Ten patients had additional skin biopsies fromthe contralateral side. Further evaluation included NCV and Quantitative Sensory Testing. Parkinson’s disease patients showed a significant increase in tactile and thermal thresholds (P<0.01), a significant reduction in mechanical pain perception (P<0.01) and significant loss of epidermal nerve fibres (ENFs) and Meissner corpuscles (MCs) (P<0.01). In patients with bilateral biopsies, loss of pain perception and ENFs was higher on the more affected side (P<0.01).We found evidence suggesting attempts at counteracting degenerative processes as increased branching, sprouting of nerves and enlargement of the vascular bed. Morphological and functional findings did not correlate with age or disease duration.Disease severity correlated with loss of MCs and reduction in cold perception and pain perception.We demonstrated a peripheral deafferentation in Parkinson’s disease that could play a major role in the pathogenesis of the sensory dysfunction.
Sensory deficit in Parkinson's disease: evidence of a cutaneous denervation / Nolano, M; Provitera, V; Estraneo, A; Selim, Mm; Caporaso, G; Stancanelli, A; Saltalamacchia, Am; Lanzillo, B; Santoro, Lucio. - In: BRAIN. - ISSN 0006-8950. - ELETTRONICO. - 131:7(2008), pp. 1903-1911.
Sensory deficit in Parkinson's disease: evidence of a cutaneous denervation
Nolano M;SANTORO, LUCIO
2008
Abstract
Sensory disturbances are part of the clinical picture of Parkinson’s disease. Abnormalities in sensory processing, through a basal ganglia involvement, are thought to be responsible for the sensory dysfunction since sensory nerve conduction velocity (NCV) is usually normal.However, NCVdoes not examine small fibres or terminal endings of large sensory fibres, whereas skin biopsy is more suitable for these purposes.To evaluate peripheral sensory nerves in Parkinson’s disease, we studied cutaneous free and encapsulated sensory nerve endings in 18 patients and 30 healthy controls using 3-mm punch biopsies from glabrous and hairy skin. Ten patients had additional skin biopsies fromthe contralateral side. Further evaluation included NCV and Quantitative Sensory Testing. Parkinson’s disease patients showed a significant increase in tactile and thermal thresholds (P<0.01), a significant reduction in mechanical pain perception (P<0.01) and significant loss of epidermal nerve fibres (ENFs) and Meissner corpuscles (MCs) (P<0.01). In patients with bilateral biopsies, loss of pain perception and ENFs was higher on the more affected side (P<0.01).We found evidence suggesting attempts at counteracting degenerative processes as increased branching, sprouting of nerves and enlargement of the vascular bed. Morphological and functional findings did not correlate with age or disease duration.Disease severity correlated with loss of MCs and reduction in cold perception and pain perception.We demonstrated a peripheral deafferentation in Parkinson’s disease that could play a major role in the pathogenesis of the sensory dysfunction.File | Dimensione | Formato | |
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