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    Activation of the pro-oxidant PKC?IIp66Shc Signaling pathway contributes to pericyte dysfunction in skeletal muscles of patients with diabetes with critical limb Ischemia

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    Date
    2016
    Author
    Vono, Rosa
    Fuoco, Claudia
    Testa, Stefano
    Pirro, Stefano
    Maselli, David
    Ferl, David
    McCollough
    Sangalli, Elena
    Pintus, Gianfranco
    Giordo, Roberta
    Finzi, Giovanna
    Sessa, Fausto
    Cardani, Rosanna
    Gotti, Ambra
    Losa, Sergio
    Cesareni, Gianni
    Rizzi, Roberto
    Bearzi, Claudia
    Cannata, Stefano
    Spinetti, Gaia
    Gargioli, Cesare
    Madeddu, Paolo
    ...show more authors ...show less authors
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    Abstract
    Critical limb ischemia (CLI), foot ulcers, former amputation, and impaired regeneration are independent risk factors for limb amputation in subjects with diabetes. The present work investigates whether and by which mechanism diabetes negatively impacts on functional properties of muscular pericytes (MPs), which are resident stem cells committed to reparative angiomyogenesis. We obtained muscle biopsy samples from patients with diabetes who were undergoing major limb amputation and control subjects. Diabetic muscles collected at the rim of normal tissue surrounding the plane of dissection showed myofiber degeneration, fat deposition, and reduction of MP vascular coverage. Diabetic MPs (D-MPs) display ultrastructural alterations, a differentiation bias toward adipogenesis at the detriment of myogenesis and an inhibitory activity on angiogenesis. Furthermore, they have an imbalanced redox state, with downregulation of the antioxidant enzymes superoxide dismutase 1 and catalase, and activation of the pro-oxidant protein kinase C isoform -II (PKCII)- dependent p66Shc signaling pathway. A reactive oxygen species scavenger or, even more effectively, clinically approved PKCII inhibitors restore D-MP angiomyogenic activity. Inhibition of the PKCII-dependent p66Shc signaling pathway could represent a novel therapeutic approach for the promotion of muscle repair in individuals with diabetes.
    DOI/handle
    http://dx.doi.org/10.2337/db16-0248
    http://hdl.handle.net/10576/18194
    Collections
    • Biomedical Sciences [‎462‎ items ]
    • Health Sciences-CAS (pre 2016) [‎139‎ items ]

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