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首页> 外文期刊>Wound repair and regeneration: official publication of the Wound Healing Society [and] the European Tissue Repair Society >Stromal-derived factor-1 delivered via hydrogel drug-delivery vehicle accelerates wound healing in vivo.
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Stromal-derived factor-1 delivered via hydrogel drug-delivery vehicle accelerates wound healing in vivo.

机译:Stromal-derived因子- 1通过水凝胶药物运输车辆加速伤口愈合体内。

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摘要

Topical treatment of superficial wounds has many advantages including decreased cost and increased ease of application compared with systemic treatments. Many of the advantages, however, are lost when it is necessary for repeated doses of topical medications to be given over an extended period of time. Therefore, a drug-delivery vehicle that delivers biologically appropriate doses in a sustained fashion would prove valuable. In this study, an alginate hydrogel scaffold impregnated with the angiogenic chemokine stromal-derived factor-1 was used to provide targeted, though short-term, delivery directly into the wound bed. Wounds were created on the dorsum of mice, and either a stromal-derived factor-1-impregnated or a saline-impregnated scaffold was applied. Wounds were explanted after 1, 3, 7 days, wound area was measured, and histology and immunohistochemistry for endothelial markers were performed. The remaining wound area in stromal-derived factor-1-treated wounds vs. controls was not significant 1 day after wounding (96.7 +/- 0.1 vs. 97.5 +/- 1.1%, p=0.317), but was significant after 3 days postwounding (46.7 +/- 0.1 vs. 82.3 +/- 2.4%, p=0.046) and 7 days postwounding (2.3 +/- 1.3 vs. 32.0 +/- 4.0%, p=0.049). Immunohistochemistry revealed a greater degree of endothelial cell invasion into the wound bed infiltration compared with controls. The results of this study suggest significant clinical promise for our hydrogel-delivery vehicle in the treatment of wounds.
机译:局部治疗表面的伤口有很多优势包括减少成本和增加方便应用程序与系统性治疗方法。当有必要重复剂量的丢失局部药物得到延长一段时间。车辆交付生物合适剂量持续的方式证明有价值的。与血管生成脚手架浸渍趋化因子stromal-derived因子- 1被用来提供有针对性的,虽然短期交付直接进入伤口床。在老鼠的背,要么stromal-derived factor-1-impregnated或saline-impregnated支架应用。是移植后1、3、7天,伤口面积测量和组织学和免疫组织化学内皮标记进行。剩余stromal-derived伤口面积不是factor-1-treated伤口与控制重大受伤后1天(96.7 + / - 0.1与97.5 + / - 1.1%,p = 0.317),但显著3天后postwounding(46.7 + / - 0.1和82.3+ / - 2.4%, p = 0.046), 7天postwounding (2.3+ / - 1.3 vs 32.0 + / - 4.0%), (p = 0.049)。免疫组织化学显示更大程度的内皮细胞入侵伤口床渗透与控制。本研究显示显著的临床承诺对我们hydrogel-delivery车辆治疗伤口。

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