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首页> 外文期刊>Journal of plastic, reconstructive & aesthetic surgery: JPRAS >EPO reverses defective wound repair in hypercholesterolaemic mice by increasing functional angiogenesis
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EPO reverses defective wound repair in hypercholesterolaemic mice by increasing functional angiogenesis

机译:EPO通过增加功能性血管生成逆转高胆固醇血症小鼠的创面修复不良

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This study aims to elucidate the effect of erythropoietin (EPO) on the microcirculation during wound healing in mice genetically depleted of apolipoprotein E (ApoE -/-). The skinfold chamber in mice was used for intravital microscopy, whereby an incisional wound was created within the chamber. Animals received Recormon ? 1000 U kg -1 body weight (BW) intra-peritoneally (i.p.) at day 1, 3, 5, 7, 9 and 11 post-wounding at a concentration of 100 U ml -1 (n = 42). Normal healing and vehicle-treated wild type animals (WT) served as controls. The microcirculation of the wound was analysed quantitatively in vivo using epi-illumination intravital fluorescence microscopy. Microtomography (micro-CT) analysis of casted wound microvessels was performed allowing three-dimensional (3D) histomorphometric analysis. Tissue samples were examined ex vivo for wound scoring and for expression analysis of EPO-Receptor (Epo-R) and endothelial nitric oxide synthase (eNOS). Upon EPO treatment, the total wound score in ApoE -/- mice was increased by 23% on day 3, by 26% on day 7 and by 18% on day 13 when compared to untreated ApoE -/- mice (all P 0.05 vs. vehicle). Improved wound healing was accompanied with a significant increase of functional angiogenetic density and angiogenetic red blood cell perfusion on days 5, 7, 9 and 11 post-wounding. 3D histomorphometric analysis revealed an increase of vessel thickness (1.7-fold), vessel volume (2.4-fold) and vessel surface (1.7-fold) (all P 0.05 vs. vehicle). In addition, improved wound healing was associated with enhanced Epo-R expression (4.6-fold on day 3 and 13.5-fold on day 7) and eNOS expression (2.4-fold on day 7) (all P 0.05 vs. vehicle). Our data demonstrate that repetitive systemic EPO treatment reverses microvascular dysfunction during wound healing in hypercholesterolaemic mice by inducing new vessel formation and by providing the wound with more oxygen.
机译:这项研究旨在阐明促红细胞生成素(EPO)对基因缺失载脂蛋白E(ApoE-/-)的小鼠伤口愈合过程中微循环的影响。小鼠的皮褶腔用于活体显微镜检查,从而在腔内形成切开伤口。动物收到了Recormon?伤口后第1、3、5、7、9和11天腹膜内(腹腔)1000 U kg -1体重(BW),浓度为100 U ml -1(n = 42)。正常愈合和经媒介物处理的野生型动物(WT)用作对照。使用落射照明活体荧光显微镜在体内定量分析伤口的微循环。对铸造的伤口微血管进行了显微断层扫描(micro-CT)分析,从而可以进行三维(3D)组织形态分析。离体检查组织样品的伤口评分以及EPO-受体(Epo-R)和内皮型一氧化氮合酶(eNOS)的表达分析。经EPO治疗后,与未经治疗的ApoE-/-小鼠相比,ApoE-/-小鼠的总伤口评分在第3天增加了23%,在第7天增加了26%,在第13天增加了18%(所有P <0.05与车辆)。伤口愈合的改善在伤口后第5、7、9和11天伴随着功能性血管生成密度和血管生成红细胞灌注的显着增加。 3D组织形态计量学分析显示血管厚度(1.7倍),血管体积(2.4倍)和血管表面(1.7倍)增加(相对于溶媒,所有P <0.05)。此外,改善的伤口愈合与增强的Epo-R表达(第3天为4.6倍,第7天为13.5倍)和eNOS表达(第7天为2.4倍)相关(相对于赋形剂,所有P <0.05)。我们的数据表明,通过诱导新血管的形成并为伤口提供更多的氧气,重复的全身性EPO治疗可逆转高胆固醇血症小鼠伤口愈合过程中的微血管功能障碍。

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