Abstract

Bacterial infection of pressure ulcers (PUs) are a notable source of hospitalization for individuals with diabetes. This study evaluated the safety profile and efficacy of auranofin to treat diabetic PUs infected with methicillin-resistant Staphylococcus aureus (MRSA). PUs were infected with MRSA in diabetic TALLYHO/JngJ mice and then treated with topical auranofin (2%), topical mupirocin (2%), or oral clindamycin (30 mg/kg) for four days. PUs were harvested post-treatment to enumerate bacterial burden and determine expression of cytokines/growth factors. Landrace cross pigs were exposed topically to auranofin (1%, 2%, and 3%) for 4–14 days and evaluated for signs of localized or systemic toxicity. Auranofin eradicated MRSA in PUs within four days (7.92-log10 reduction) in contrast to mupirocin (2.15-log10 reduction) and clindamycin (0.73-log10 reduction). Additionally, auranofin treatment resulted in decreased expression of pro-inflammatory cytokines and increased expression of biomarkers associated with re-epithelization of wounded tissue, confirmed with histopathologic analysis. No significant histopathologic lesions were present on porcine skin sites exposed to topical auranofin. Additionally, minimal accumulation of plasma gold and no systemic toxicity was observed in pigs exposed to topical auranofin. Auranofin appears to be a potent and safe topical agent to further investigate for treatment of mild-to-moderate MRSA-infected diabetic PUs.

Highlights

  • Bacterial infection of pressure ulcers (PUs) are a notable source of hospitalization for individuals with diabetes

  • TALLYHO/JngJ mice exhibiting moderate methicillin-resistant Staphylococcus aureus (MRSA)-infected pressure ulcers were treated with oral clindamycin (30 mg/kg) q.d. or topically with auranofin (2%), mupirocin (2%), or vehicle alone b.i.d. for four days

  • Complete eradication of MRSA (7.92-log[10] reduction) was observed in PUs treated with auranofin, which was superior to clindamycin (P = 0.0181)

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Summary

Introduction

Bacterial infection of pressure ulcers (PUs) are a notable source of hospitalization for individuals with diabetes. This study evaluated the safety profile and efficacy of auranofin to treat diabetic PUs infected with methicillin-resistant Staphylococcus aureus (MRSA). Auranofin appears to be a potent and safe topical agent to further investigate for treatment of mild-to-moderate MRSA-infected diabetic PUs. Diabetes is a significant global public health challenge that affects approximately 9% of all adults (463 million people) and is associated with 4.2 million deaths each y­ ear[1,2]. The objectives of the present study were to evaluate auranofin in the treatment of MRSA-infected pressure ulcers in diabetic mice and to evaluate the safety profile of auranofin as a topical agent when applied to porcine skin. Addressing efficacy and safety in these animal models is an important pre-clinical step to repurpose auranofin for the treatment of mild-to-moderate MRSA-infected pressure ulcers in diabetic patients

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