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Targeting epigenetic mechanisms in diabetic wound healing.

Citation
Dekker, A. den, et al. “Targeting Epigenetic Mechanisms In Diabetic Wound Healing.”. Translational Research : The Journal Of Laboratory And Clinical Medicine, pp. 39-50.
Center University of Michigan
Author Aaron den Dekker, Frank M Davis, Steve L Kunkel, Katherine A Gallagher
Abstract

Impaired wound healing is a major secondary complication of type 2 diabetes that often results in limb loss and disability. Normal tissue repair progresses through discrete phases including hemostasis, inflammation, proliferation, and remodeling. In diabetes, normal progression through these phases is impaired resulting in a sustained inflammatory state and dysfunctional epithelialization in the wound. Due to their plasticity, macrophages play a critical role in the transition from the inflammation phase to the proliferation phase. Diabetes disrupts macrophage function by impairing monocyte recruitment to the wound, reducing phagocytosis, and prohibiting the transition of inflammatory macrophages to an anti-inflammatory state. Diabetes also impedes keratinocyte and fibroblast function during the later phases resulting in impaired epithelialization of the wound. Several recent studies suggest that altered epigenetic regulation of both immune and structural cells in wounds may influence cell phenotypes and healing, particularly in pathologic states, such as diabetes. Specifically, it has been shown that macrophage plasticity during wound repair is partly regulated epigenetically and that diabetes alters this epigenetic regulation and contributes to a sustained inflammatory state. Epigenetic regulation is also known to regulate keratinocyte and fibroblast function during wound repair. In this review, we provide an introduction to the epigenetic mechanisms that regulate tissue repair and highlight recent findings that demonstrate, how epigenetic events are altered during the course of diabetic wound healing.

Year of Publication
2019
Journal
Translational research : the journal of laboratory and clinical medicine
Volume
204
Number of Pages
39-50
Date Published
12/2019
ISSN Number
1878-1810
DOI
10.1016/j.trsl.2018.10.001
Alternate Journal
Transl Res
PMID
30392877
PMCID
PMC6331222
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