Integrative miRNA–mRNA profiling of human epidermis: unique signature of SCN9A painful neuropathy, 2022, Andelic et al.

Discussion in ''Conditions related to ME/CFS' news and research' started by SNT Gatchaman, Apr 16, 2023.

  1. SNT Gatchaman

    SNT Gatchaman Senior Member (Voting Rights)

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    Integrative miRNA–mRNA profiling of human epidermis: unique signature of SCN9A painful neuropathy
    Andelic, Mirna; Salvi, Erika; Marcuzzo, Stefania; Marchi, Margherita; Lombardi, Raffaella; Cartelli, Daniele; Cazzato, Daniele; Mehmeti, Elkadia; Gelemanovic, Andrea; Paolini, Matilde; Pardo, Carlotta; D’Amato, Ilaria; Hoeijmakers, Janneke G J; Dib-Hajj, Sulayman; Waxman, Stephen G; Faber, Catharina G; Lauria, Giuseppe

    Personalized management of neuropathic pain is an unmet clinical need due to heterogeneity of the underlying aetiologies, incompletely understood pathophysiological mechanisms and limited efficacy of existing treatments.

    Recent studies on microRNA in pain preclinical models have begun to yield insights into pain-related mechanisms, identifying nociception-related species differences and pinpointing potential drug candidates.

    With the aim of bridging the translational gap towards the clinic, we generated a human pain-related integrative miRNA and mRNA molecular profile of the epidermis, the tissue hosting small nerve fibres, in a deeply phenotyped cohort of patients with sodium channel-related painful neuropathy not responding to currently available therapies.

    We identified four miRNAs strongly discriminating patients from healthy individuals, confirming their effect on differentially expressed gene targets driving peripheral sensory transduction, transmission, modulation and post-transcriptional modifications, with strong effects on gene targets including NEDD4.

    We identified a complex epidermal miRNA–mRNA network based on tissue-specific experimental data suggesting a cross-talk between epidermal cells and axons in neuropathy pain. Using immunofluorescence assay and confocal microscopy, we observed that Nav1.7 signal intensity in keratinocytes strongly inversely correlated with NEDD4 expression that was downregulated by miR-30 family, suggesting post-transcriptional fine tuning of pain-related protein expression.

    Our targeted molecular profiling advances the understanding of specific neuropathic pain fine signatures and may accelerate process towards personalized medicine in patients with neuropathic pain.

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  2. SNT Gatchaman

    SNT Gatchaman Senior Member (Voting Rights)

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  3. SNT Gatchaman

    SNT Gatchaman Senior Member (Voting Rights)

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    See also Targeting a Peripheral Sodium Channel to Treat Pain (2023, New England Journal of Medicine), which talks about new drugs targeting a similar sodium channel (Nav1.8) with the trial paper being Selective Inhibition of NaV1.8 with VX-548 for Acute Pain (2023, New England Journal of Medicine).

     
    Last edited: Aug 4, 2023
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    SNT Gatchaman Senior Member (Voting Rights)

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    Last edited: Aug 4, 2023
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