Abstract
Monocytes (Mo) and macrophages (Mϕ) play important roles in normal skin wound healing, and dysregulation of wound Mo/Mϕ leads to impaired wound healing in diabetes. Although skin wound Mϕ originate both from tissue resident Mϕ and infiltrating bone marrow-derived Mo, the latter play dominant roles during the inflammatory phase of wound repair. Increased production of bone marrow Mo caused by alterations of hematopoietic stem and progenitor cell (HSPC) niche and epigenetic modifications of HSPCs likely contributes to the enhanced number of wound Mϕ in diabetes. In addition, an impaired transition of diabetic wound Mϕ from “pro-inflammatory” to “pro-healing” phenotypes driven by the local wound environment as well as intrinsic changes in bone marrow Mo is also thought to be partly responsible for impaired diabetic wound healing. The current brief review describes the origin, heterogeneity and function of wound Mϕ during normal skin wound healing followed by discussion of how dysregulated wound Mϕ numbers and phenotype are associated with impaired diabetic wound healing. The review also highlights the possible links between altered bone marrow myelopoiesis and increased Mo production as well as extrinsic and intrinsic factors that drive wound macrophage dysregulation leading to impaired wound healing in diabetes.
Highlights
Skin wound healing involves distinct but overlapping phases of hemostasis, inflammation, proliferation, and remodeling (Eming et al, 2014)
A diverse set of cells such as platelets, mast cells, neutrophils, monocytes (Mo), macrophages (Mφ), lymphocytes, keratinocytes, fibroblasts, and endothelial cells all contribute to the process of skin wound healing (Canedo-Dorantes and Canedo-Ayala, 2019)
This brief review considers the origin, heterogeneity and function of wound Mφ during normal wound healing followed by discussion of how dysregulation of numbers and phenotypes of wound Mφ may lead to impaired diabetic wound healing
Summary
Macrophage Dysregulation and Impaired Skin Wound Healing in Diabetes. Front. Monocytes (Mo) and macrophages (Mφ) play important roles in normal skin wound healing, and dysregulation of wound Mo/Mφ leads to impaired wound healing in diabetes. Increased production of bone marrow Mo caused by alterations of hematopoietic stem and progenitor cell (HSPC) niche and epigenetic modifications of HSPCs likely contributes to the enhanced number of wound Mφ in diabetes. The current brief review describes the origin, heterogeneity and function of wound Mφ during normal skin wound healing followed by discussion of how dysregulated wound Mφ numbers and phenotype are associated with impaired diabetic wound healing. The review highlights the possible links between altered bone marrow myelopoiesis and increased Mo production as well as extrinsic and intrinsic factors that drive wound macrophage dysregulation leading to impaired wound healing in diabetes
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