Pain related channels are differentially expressed in neuronal and non-neuronal cells of glabrous skin of fabry knockout male mice.

[fabry disease]

Fabry disease (FD ) is one of the X-linked lysosomal storage disorders caused by deficient functioning of the alpha-galactosidase A (Î±-GalA ) enzyme . The Î±-GalA deficiency leads to multi-systemic clinical manifestations caused by the preferential accumulation of globotriaosylceramide in the endothelium and vascular smooth muscles . A hallmark symptom of FD patients is peripheral pain that appears in the early stage of the disease . Pain in FD patients is a peripheral small -fiber idiopathic neuropathy , with intra-epidermal fiber density and integrity being used for diagnosing FD in humans . However , the molecular correlates underlying pain sensation in FD remain elusive . Here , we have employed the Î±-GalA gene KO mouse as a model of FD in rodents to investigate molecular changes in their peripheral nervous system that may account for their algesic symptoms . The Î±-GalA null mice display neuropathic pain as evidenced by thermal hyperalgesia and mechanical allodynia , with histological analyses showing alterations in cutaneous innervation . Additionally , KO mice showed a decreased and scattered pattern of neuronal terminations consistent with the reduction in neuronal terminations in skin biopsies of patients with small fiber neuropathies . At the molecular level KO animals showed an increase in the expression of TRPV 1 and Nav 1 .8 , and a decrease in the expression of TRPM 8 . Notably , these alterations are observed in young animals . Taken together , our findings imply that the Î±-GalA KO mouse is a good model in which to study the peripheral small fiber neuropathy exhibited by FD patients , and provides molecular evidence for a hyperexcitability of small nociceptors in FD .

Diseases
Validation

Diseases presenting "peripheral small fiber neuropathy" symptom

fabry disease

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