Antimycotic ciclopirox olamine in the diabetic environment promotes angiogenesis and enhances wound healing

Sae Hee Ko; Allison Nauta; Shane D. Morrison; Hongyan Zhou; Andrew Zimmermann; Geoffrey C. Gurtner; Sheng Ding; Michael T. Longaker

doi:10.1371/journal.pone.0027844

Antimycotic ciclopirox olamine in the diabetic environment promotes angiogenesis and enhances wound healing

Sae Hee Ko, Allison Nauta, Shane D. Morrison, Hongyan Zhou, Andrew Zimmermann, Geoffrey C. Gurtner, Sheng Ding, Michael T. Longaker

Research output: Contribution to journal › Article › peer-review

26 Scopus citations

Abstract

Diabetic wounds remain a major medical challenge with often disappointing outcomes despite the best available care. An impaired response to tissue hypoxia and insufficient angiogenesis are major factors responsible for poor healing in diabetic wounds. Here we show that the antimycotic drug ciclopirox olamine (CPX) can induce therapeutic angiogenesis in diabetic wounds. Treatment with CPX in vitro led to upregulation of multiple angiogenic genes and increased availability of HIF-1α. Using an excisional wound splinting model in diabetic mice, we showed that serial topical treatment with CPX enhanced wound healing compared to vehicle control treatment, with significantly accelerated wound closure, increased angiogenesis, and increased dermal cellularity. These findings offer a promising new topical pharmacologic therapy for the treatment of diabetic wounds.

Original language	English (US)
Article number	e27844
Journal	PloS one
Volume	6
Issue number	11
DOIs	https://doi.org/10.1371/journal.pone.0027844
State	Published - Nov 18 2011
Externally published	Yes

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title = "Antimycotic ciclopirox olamine in the diabetic environment promotes angiogenesis and enhances wound healing",

abstract = "Diabetic wounds remain a major medical challenge with often disappointing outcomes despite the best available care. An impaired response to tissue hypoxia and insufficient angiogenesis are major factors responsible for poor healing in diabetic wounds. Here we show that the antimycotic drug ciclopirox olamine (CPX) can induce therapeutic angiogenesis in diabetic wounds. Treatment with CPX in vitro led to upregulation of multiple angiogenic genes and increased availability of HIF-1α. Using an excisional wound splinting model in diabetic mice, we showed that serial topical treatment with CPX enhanced wound healing compared to vehicle control treatment, with significantly accelerated wound closure, increased angiogenesis, and increased dermal cellularity. These findings offer a promising new topical pharmacologic therapy for the treatment of diabetic wounds.",

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AU - Ko, Sae Hee

AU - Nauta, Allison

AU - Morrison, Shane D.

AU - Zhou, Hongyan

AU - Zimmermann, Andrew

AU - Gurtner, Geoffrey C.

AU - Ding, Sheng

AU - Longaker, Michael T.

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AB - Diabetic wounds remain a major medical challenge with often disappointing outcomes despite the best available care. An impaired response to tissue hypoxia and insufficient angiogenesis are major factors responsible for poor healing in diabetic wounds. Here we show that the antimycotic drug ciclopirox olamine (CPX) can induce therapeutic angiogenesis in diabetic wounds. Treatment with CPX in vitro led to upregulation of multiple angiogenic genes and increased availability of HIF-1α. Using an excisional wound splinting model in diabetic mice, we showed that serial topical treatment with CPX enhanced wound healing compared to vehicle control treatment, with significantly accelerated wound closure, increased angiogenesis, and increased dermal cellularity. These findings offer a promising new topical pharmacologic therapy for the treatment of diabetic wounds.

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Antimycotic ciclopirox olamine in the diabetic environment promotes angiogenesis and enhances wound healing

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