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The Use of Amnion-Derived Cellular Cytokine Solution to Improve Healing in Acute and Chronic Wound Models

机译:使用羊膜来源的细胞因子溶液改善急性和慢性伤口模型的愈合

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摘要

>Objective: Growth factors demonstrate mixed results improving wound healing. Amnion-derived multipotent cells release physiologic levels of growth factors and tissue inhibitors of metalloproteinases. This solution was tested in models of acute and chronic wound healing. >Methods: Acute model: Sprague-Dawley rats underwent laparotomy incisions. The midline fascia was primed with phosphate-buffered saline, unconditioned media, or amnion-derived cellular cytokine suspension prior to incision. Breaking strength of laparotomy wounds was tested with an Instron tensiometer. Incisional hernia formation was measured after 28 days. Chronic model: Chronic, infected granulating wounds were produced in rats by excising full thickness burn eschars inoculated with Escherica coli. Granulating wounds were treated with unconditioned media or amnion-derived cellular cytokine suspension. Treatments were applied either on day 0 and day 7 or day 0 and then every other day. Wounds were traced every 72 hours and biopsied for quantitative bacteriology. >Results: Acute model: Priming with amnion-derived cellular cytokine suspension increased the breaking strength of laparotomy incisions in comparison with phosphate-buffered saline or unconditioned media (P < .05). Acute wound failure and incisional hernia formation was 100% in the phosphate-buffered saline and unconditioned media groups and 18% in the amnion-derived cellular cytokine suspension–treated group (P <.05). Chronic model: The rate of wound closure was accelerated in amnion-derived cellular cytokine suspension–treated chronic wounds (P < .05). Multidosing improved the effect. >Conclusions: A physiologic solution of cytokines and tissue inhibitors of metalloproteinases improves healing in models of acute and chronic wounds. Such a cocktail can be produced from amnion-derived multipotent progenitor cells.
机译:>目标:生长因子显示出改善伤口愈合的好坏参半。羊膜来源的多能细胞释放生理水平的生长因子和金属蛋白酶的组织抑制剂。该解决方案已在急性和慢性伤口愈合模型中进行了测试。 >方法:急性模型:对Sprague-Dawley大鼠进行剖腹手术切口。切口前,中线筋膜用磷酸盐缓冲液,无条件培养基或羊膜来源的细胞因子悬浮液灌注。用Instron张力计测试剖腹手术伤口的断裂强度。 28天后测量切口疝的形成。慢性模型:通过切除接种大肠杆菌的全层烧伤焦糖,在大鼠中产生慢性感染的肉芽伤口。用无条件培养基或羊膜来源的细胞因子悬浮液治疗肉芽伤口。在第0天和第7天或第0天,然后每隔一天进行治疗。每72小时追踪一次伤口,并对其进行活检以进行定量细菌学检查。 >结果:急性模型:羊膜来源的细胞因子悬浮液引发的开腹手术与磷酸盐缓冲液或无条件培养基相比,增加了剖腹切口的断裂强度(P <.05)。在磷酸盐缓冲液和无条件培养基组中,急性伤口衰竭和切开疝的形成为100%,在羊膜来源的细胞因子悬浮液治疗组中为18%(P <.05)。慢性模型:在羊膜来源的细胞因子悬浮液治疗的慢性伤口中,伤口闭合的速度加快(P <.05)。多剂量改善了效果。 >结论:一种细胞因子和金属蛋白酶组织抑制剂的生理溶液可改善急性和慢性伤口模型的愈合。这种混合物可以由羊膜来源的多能祖细胞产生。

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