首页> 外文期刊>Advances in skin & wound care >Infected wound model development of an in vitro biomaterial-protected wound infection model to study microbial activity and antimicrobial treatment through microdialysis.
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Infected wound model development of an in vitro biomaterial-protected wound infection model to study microbial activity and antimicrobial treatment through microdialysis.

机译:建立体外生物材料保护的伤口感染模型的感染伤口模型,以研究微生物活性和通过微透析进行的抗菌治疗。

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OBJECTIVE: Skin injuries provide a favorable environment for microbial infection if left untreated. This is problematic especially in nosocomial situations having a high prevalence of Staphylococcus aureus that can cause suppuration of wounds, systemic disease, and toxic shock. The objective of this investigation was to use a wound model system to study the interactions between microbial activity, host tissue, therapeutic treatments, and wound biomaterials. DESIGN: An in vitro wound model was developed using Sykes-Moore chambers filled with 1 of 2 biomaterials used for wound treatment (1% alginate and dialyzed HyFil hydrogel (B. Braun Medical, Inc, Bethlehem, Pennsylvania) and seeded with fibroblasts. The chambers were inoculated with S aureus, and half were later treated with antibiotics through in situ microdialysis tubing. MAIN OUTCOME MEASURES: The chambers were monitored by obtaining fluid samples and biomaterial samples at specific time intervals (0, 2, 8, and 24 hours) and were analyzed for (1) S aureus protein A (SPA) concentration, (2) viable S aureus numbers, and (3) fibroblast numbers and viability. Chambers containing each biomaterial with and without antibiotics were compared to controls. MAIN RESULTS: There was an inverse relationship between postinfection S aureus numbers and fibroblast viability. S aureus numbers were usually consistent with SPA concentration, which may have been underestimated because of SPA interactions with the biomaterials. CONCLUSION: This wound model may be useful to gain an understanding about the interactions between microbial activity, host tissue, therapeutic treatments, and wound biomaterials. Hypotheses about wound treatments derived by means of this model may direct future in vivo studies.
机译:目的:如果不及时治疗,皮肤损伤为微生物感染提供了良好的环境。这尤其在有金黄色葡萄球菌的高流行率的医院情况下是有问题的,这可能引起伤口化脓,全身性疾病和中毒性休克。这项研究的目的是使用伤口模型系统研究微生物活性,宿主组织,治疗方法和伤口生物材料之间的相互作用。设计:使用填充有2种用于伤口处理的生物材料中的1种(1%海藻酸盐和透析过的HyFil水凝胶(B. Braun Medical,Inc,伯利恒,宾夕法尼亚州))并用成纤维细胞接种的Sykes-Moore腔室开发了体外伤口模型。主要观察指标:通过在特定时间间隔(0、2、8和24小时)获得体液样本和生物材料样本,对腔室进行监测,对腔室进行监测。结果包括:(1)金黄色葡萄球菌蛋白A(SPA)浓度,(2)活金黄色葡萄球菌数量和(3)成纤维细胞数量和生存力,将装有和不使用抗生素的每种生物材料的培养箱与对照组进行比较。是感染后金黄色葡萄球菌数量与成纤维细胞活力之间的反比关系,金黄色葡萄球菌数量通常与SPA浓度一致,这可能是由于SPA相互作用而被低估了生物材料。结论:该伤口模型可能有助于了解微生物活性,宿主组织,治疗方法和伤口生物材料之间的相互作用。通过这种模型得出的有关伤口治疗的假设可能会指导未来的体内研究。

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