首页> 美国卫生研究院文献>Journal of Burn Care Research: Official Publication of the American Burn Association >Sugar-coating wound repair: A review of FGF-10 and dermatan sulfate in wound healing and their potential application in burn wounds
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Sugar-coating wound repair: A review of FGF-10 and dermatan sulfate in wound healing and their potential application in burn wounds

机译:糖衣伤口修复:FGF-10和硫酸皮肤素在伤口愈合中的研究及其在烧伤伤口中的潜在应用

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摘要

Thousands of patients suffer from burn injuries each year, yet few therapies have been developed to accelerate the wound healing process. Most fibroblast growth factors (FGFs) have been extensively evaluated, but only a few have been found to participate in wound healing. In particular, FGF-10 is robustly increased in the wound microenvironment following injury and has demonstrated some ability to promote wound healing in vitro and in vivo. Glycosaminoglycans (GAGs) are linear carbohydrates that participate in wound repair by influencing cytokine/growth factor localization and interaction with cognate receptors. Dermatan sulfate (DS) is the most abundant GAG in human wound fluid and has been postulated to be directly involved in the healing process. Recently, the combination of FGF-10 and DS demonstrated the potential to accelerate wound healing via increased keratinocyte proliferation and migration. Based on these preliminary studies, DS may serve as a cofactor for FGF-10, and together, they are likely to expedite the healing process by stimulating keratinocyte activity. As a specific subtype of wounds, the overall healing process of burn injuries does not significantly differ from other types of wounds, where optimal repair results in matrix regeneration and complete re-epithelialization. At present, standard burn treatment primarily involves topical application of anti-microbial agents, while no routine therapies target acceleration of re-epithelialization, the key to wound closure. Thus, this novel therapeutic combination could be used in conjunction with some of the current therapies, but it would have the unique ability to initiate wound healing by stimulating keratinocyte epithelialization.
机译:每年有成千上万的患者遭受烧伤,但是很少有疗法可以加速伤口的愈合过程。大多数成纤维细胞生长因子(FGFs)已得到广泛评估,但仅发现少数几个参与伤口愈合。特别地,FGF-10在损伤后的伤口微环境中强烈增加,并已显示出一定的促进体外和体内伤口愈合的能力。糖胺聚糖(GAG)是线性碳水化合物,可通过影响细胞因子/生长因子的定位以及与同源受体的相互作用来参与伤口修复。硫酸皮肤素(DS)是人类伤口液中含量最丰富的GAG,据推测直接参与了愈合过程。最近,FGF-10和DS的组合显示出通过增加角质形成细胞增殖和迁移来加速伤口愈合的潜力。基于这些初步研究,DS可能是FGF-10的辅助因子,并且一起,它们可能通过刺激角质形成细胞的活性来加快愈合过程。作为伤口的特定亚型,烧伤的总体愈合过程与其他类型的伤口没有明显不同,在其他类型的伤口上,最佳修复可导致基质再生和完全上皮再生。目前,标准烧伤治疗主要涉及局部应用抗微生物剂,而没有常规疗法以加速上皮形成(伤口闭合的关键)为目标。因此,这种新颖的治疗组合可以与一些当前的治疗方法结合使用,但是它具有通过刺激角质形成细胞上皮化而启动伤口愈合的独特能力。

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