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Article Publish Status: FREE
Abstract Title:

Combination of low level light therapy and nitrosyl-cobinamide accelerates wound healing.

Abstract Source:

J Biomed Opt. 2015 May ;20(5):051022. PMID: 25562608

Abstract Author(s):

Ryan Spitler, Hsiang Ho, Frederique Norpetlian, Xiangduo Kong, Jingjing Jiang, Kyoko Yokomori, Bogi Andersen, Gerry R Boss, Michael W Berns

Article Affiliation:

Ryan Spitler

Abstract:

Low level light therapy (LLLT) has numerous therapeutic benefits, including improving wound healing, but the precise mechanisms involved are not well established; in particular, the underlying role of cytochrome C oxidase (C-ox) as the primary photoacceptor and the associated biochemical mechanisms still require further investigation. We previously showed the nitric oxide (NO) donating drug nitrosyl-cobinamide (NO-Cbi) enhances wound healing through a cGMP/cGMP-dependent protein kinase/ERK1/2 mechanism. Here, we show that the combination of LLLT and NO-Cbi markedly improves wound healing compared to either treatment alone. LLLT-enhanced wound healing proceeded through an electron transport chain-C-ox-dependent mechanism with a reduction of reactive oxygen species and increased adenosine triphosphate production. C-ox was validated as the primary photoacceptor by three observations: increased oxygen consumption, reduced wound healing in the presence of sodium azide, and disassociation of cyanide, a known C-ox ligand, following LLLT. We conclude that LLLT and NO-Cbi accelerate wound healing through two independent mechanisms, the electron transport chain-C-ox pathway and cGMP signaling, respectively, with both resulting in ERK1/2 activation.

Study Type : In Vitro Study
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