Abstract
IntroductionHypoxia-inducible factor (HIF)-1α, part of the heterodimeric transcription factor that mediates the cellular response to hypoxia, is critical for the expression of multiple angiogenic growth factors, cell motility, and the recruitment of endothelial progenitor cells. Inhibition of the oxygen-dependent negative regulator of HIF-1α, prolyl hydroxylase domain-2 (PHD-2), leads to increased HIF-1α and mimics various cellular and physiological responses to hypoxia. The roles of PHD-2 in the epidermis and dermis have not been clearly defined in wound healing.MethodsEpidermal and dermal specific PHD-2 knockout (KO) mice were developed in a C57BL/6J (wild type) background by crossing homozygous floxed PHD-2 mice with heterozygous K14-Cre mice and heterozygous Col1A2-Cre-ER mice to get homozygous floxed PHD-2/heterozygous K14-Cre and homozygous floxed PHD-2/heterozygous floxed Col1A2-Cre-ER mice, respectively. Ten to twelve-week-old PHD-2 KO and wild type (WT) mice were subjected to wounding and ischemic pedicle flap model. The amount of healing was grossly quantified with ImageJ software. Western blot and qRT-PCR was run on protein and RNA from primary cells cultured in vitro.ResultsqRT-PCR demonstrated a significant decrease of PHD-2 in keratinocytes and fibroblasts derived from tissue specific KO mice relative to control mice (*p<0.05). Western blot analysis showed a significant increase in HIF-1α and VEGF protein levels in PHD-2 KO mice relative to control mice (*p<0.05). PHD-2 KO mice showed significantly accelerated wound closure relative to WT (*p<0.05). When ischemia was analyzed at day nine post-surgery in a flap model, the PHD-2 tissue specific knockout mice showed significantly more viable flaps than WT (*p<0.05).ConclusionsPHD-2 plays a significant role in the rates of wound healing and response to ischemic insult in mice. Further exploration shows PHD-2 KO increases cellular levels of HIF-1α and this increase leads to the transcription of downstream angiogenic factors such as VEGF.
Highlights
Hypoxia-inducible factor (HIF)-1a, part of the heterodimeric transcription factor that mediates the cellular response to hypoxia, is critical for the expression of multiple angiogenic growth factors, cell motility, and the recruitment of endothelial progenitor cells
Numerous treatment options for chronic wounds currently exist, including treatment of the underlying pathology, systemic treatment aimed at improving the local wound environment and local treatment aimed at improving the wound environment [2,3,4]
Transcription of prolyl hydroxylase domain-2 (PHD-2) should be severely depressed and that of HIF-1a mRNA should not be altered since PHD-2 regulates HIF-1a at the protein level
Summary
Hypoxia-inducible factor (HIF)-1a, part of the heterodimeric transcription factor that mediates the cellular response to hypoxia, is critical for the expression of multiple angiogenic growth factors, cell motility, and the recruitment of endothelial progenitor cells. Inhibition of the oxygen-dependent negative regulator of HIF-1a, prolyl hydroxylase domain-2 (PHD-2), leads to increased HIF-1a and mimics various cellular and physiological responses to hypoxia. The increasing incidence and prevalence of chronic wounds has made them a prominent public health concern; slow healing of chronic wounds, such as ulcers, can lead to infection, sepsis, and eventually amputation. The wide array of treatment modalities currently used in the treatment of chronic wounds belies the deficiency of each individual approach to provide an optimal solution. Left untreated, these wounds can lead to serious
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