首页> 美国卫生研究院文献>Journal of Burn Care Research: Official Publication of the American Burn Association >Concurrent In Vitro Release of Silver Sulfadiazine and Bupivacaine From Semi-Interpenetrating Networks for Wound Management
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Concurrent In Vitro Release of Silver Sulfadiazine and Bupivacaine From Semi-Interpenetrating Networks for Wound Management

机译:从半互穿性网络同时释放磺胺嘧啶银和布比卡因用于伤口处理。

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摘要

In situ photopolymerized semi-interpenetrating networks (sIPNs) composed of poly(ethylene glycol) and gelatin are promising multifunctional matrices for a regenerative medicine approach to dermal wound treatment. In addition to previously demonstrated efficacy in critical defects, sIPNs also function as drug delivery matrices for compounds loaded as either soluble or covalently linked components. Simultaneous release of silver sulfadiazine and bupivacaine from the sIPN would provide multiple-hit management of dermal wounds that minimizes infection, and manages pain along with sIPN absorption of exudates and facilitation of epidermal regrowth. We characterized the release of soluble silver sulfadiazine and bupivacaine and compared it with an established release model. Efficacy of released silver sulfadiazine was confirmed in vitro on Staphylococcus aureus, methicillin resistant S. aureus, and Pseudomonas aeruginosa. Bupivacaine loaded without silver sulfadiazine showed incomplete release, whereas simultaneous loading with silver sulfadiazine facilitated 100% bupivacaine release. Silver sulfadiazine released at 98% without bupivacaine and 96% with bupivacaine. Silver sulfadiazine released onto bacterial cultures inhibited all three strains dose dependently. sIPNs effectively release bupivacaine and silver sulfadiazine while maintaining the antimicrobial activity of silver sulfadiazine. Drug loaded sIPNs have potential to improve wound management by providing multi-drug delivery along with an effective wound treatment.
机译:由聚乙二醇和明胶组成的原位光聚合半互穿网络(sIPN)是用于皮肤伤口治疗的再生医学方法的有前途的多功能基质。除了先前证明的在关键缺陷中的功效外,sIPN还可作为负载为可溶性或共价连接组分的化合物的药物传递基质。从sIPN中同时释放磺胺嘧啶银和布比卡因可对皮肤伤口进行多次打击管理,从而最大程度地减少感染,并通过sIPN吸收渗出液和促进表皮再生来管理疼痛。我们表征了可溶性磺胺嘧啶银和布比卡因的释放,并将其与已建立的释放模型进行了比较。在体外证实了释放的磺胺嘧啶银对金黄色葡萄球菌,耐甲氧西林的金黄色葡萄球菌和铜绿假单胞菌的功效。没有磺胺嘧啶银装载的布比卡因显示不完全释放,而同时磺胺嘧啶银装载同时促进了100%布比卡因释放。磺胺嘧啶银在不使用布比卡因时的释放率为98%,在使用布比卡因时的释放率为96%。释放到细菌培养物中的磺胺嘧啶银抑制了这三个菌株的剂量依赖性。 sIPNs有效释放布比卡因和磺胺嘧啶银,同时保持磺胺嘧啶银的抗菌活性。通过提供多种药物以及有效的伤口治疗,载药的sIPN具有改善伤口管理的潜力。

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