Diabetic Ulcer Clinical Trial
Official title:
Endogenous Progenitors Cell Therapy for Diabetic Foot Ulcers
Diabetic foot ulcers, a complication of diabetes leading to 80.000 lower limb amputations annually in the US, are a significant burden to our health system, costing more than a billion dollars annually. Here, we propose a novel combination of two drugs (Mozobil® and Regranex®Gel) to mobilize a specific sub-type of stem cells (endothelial progenitor cells) from the bone marrow and traffic them toward the wound, increasing the blood supply that subsequently improves wound healing. Because we are using the human body's own resources to regenerate itself by targeting and correcting the underlying pathophysiology, we believe that this novel therapy yields great promise in the treatment of diabetic foot ulcers.
Because diabetes impairs wound healing by altering fibroblast function, promotes chronic
infection and diminishes blood supply to the skin, the lifetime risk of a person with
diabetes developing a diabetic foot ulcer (DFU) is as high as 25%. Current strategies focus
independently on the fibroblast dysfunction (growth factors such as PDGF/Regranex® Gel), on
the chronic infection (debridement, antibacterial dressings) or on the blood supply (VAC®).
This project is different from the other projects because we propose to combine two drugs in
a dual approach to first improve the fibroblast function using PDGF/Regranex® Gel and second
to induce neovascularization in DFU by recruiting progenitor cells into the wound through a
combination therapy of subcutaneous AMD3100 (Plerixafor/Mozobil®) with topical
PDGF/Regranex® Gel. By contrast to novel stem cell therapies where cells are extracted,
processed ex vivo and engrafted into the wound (exogenous stem cell therapy), here we
propose to keep the stem cells in vivo (endogenous stem cell therapy).
Specifically, the first aim of the study will be to launch a prospective evaluator-blind
pilot phase I/II safety and efficacy study to evaluate the clinical effect of AMD3100
(Plerixafor/Mozobil®) treatment with topical PDGF/Regranex® Gel compared to historical
controls (standard of care and PDGF). AMD3100 (240 µg/kg SC) will be administered daily for
2 weeks. Our primary endpoint will be the measure of the percentage of change in area of the
wound at 4 weeks (surrogate endpoint). In a second aim, we will measure the effect of
AMD3100 treatment with PDGF using a quality-of-life index dedicated to DFU (DFS-SF).
Because we are addressing the underlying physiopathology in a dual approach, because we are
avoiding the need for ex vivo processing and because both drugs are FDA approved, we believe
that this novel therapy yields great promise in the treatment of DFUs.
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Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Single Blind (Subject), Primary Purpose: Treatment
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