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首页> 外文期刊>Plastic and reconstructive surgery >Stimulation of the follicular bulge lgr5+ and lgr6+ stem cells with the gut-derived human alpha defensin 5 results in decreased bacterial presence, enhanced wound healing, and hair growth from tissues devoid of adnexal structures
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Stimulation of the follicular bulge lgr5+ and lgr6+ stem cells with the gut-derived human alpha defensin 5 results in decreased bacterial presence, enhanced wound healing, and hair growth from tissues devoid of adnexal structures

机译:肠道来源的人α防御素5刺激卵泡凸起的lgr5 +和lgr6 +干细胞导致细菌减少,伤口愈合增强以及无附件结构的头发生长

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BACKGROUND:: Discovery of leucine-rich repeat-containing G-protein-coupled receptors 5 and 6 (LGR5 and LGR6) as markers of adult epithelial stem cells of the skin and intestine permits researchers to draw on the intrinsic cellular fundamentals of wound healing and proliferation dynamics of epithelial surfaces. In this study, the authors use the intestine-derived human alpha defensin 5 to stimulate epithelial proliferation, bacterial reduction, and hair production in burn wound beds to provide the field with initial insight on augmenting wound healing in tissues devoid of adnexal stem cells. METHODS:: Murine third-degree burn wound beds were treated with (1) intestine-derived human alpha defensin 5, (2) skin-derived human beta defensin 1, and (3) sulfadiazine to determine their roles in wound healing, bacterial reduction, and hair growth. RESULTS:: The human alpha defensin 5 peptide significantly enhanced wound healing and reduced basal bacterial load compared with human beta defensin 1 and sulfadiazine. Human alpha defensin 5 was the only therapy to induce LGR stem cell migration into the wound bed. In addition, gene heat mapping showed significant mRNA up-regulation of key wound healing and Wnt pathway transcripts such as Wnt1 and Wisp1. Ex vivo studies showed enhanced cell migration in human alpha defensin 5-treated wounds compared with controls. CONCLUSIONS:: Application of human alpha defensin 5 increases LGR stem cell migration into wound beds, leading to enhanced healing, bacterial reduction, and hair production through the augmentation of key Wnt and wound healing transcripts. These findings can be used to derive gut protein-based therapeutics in wound healing.
机译:背景:发现富含亮氨酸的重复序列的G蛋白偶联受体5和6(LGR5和LGR6)作为皮肤和肠成人上皮干细胞的标志物,使研究人员可以利用伤口愈合和修复的内在细胞基础上皮表面的增殖动力学。在这项研究中,作者使用肠道来源的人α防御素5刺激烧伤创面中的上皮增殖,细菌减少和毛发生长,为增强无附件干细胞组织伤口愈合的领域提供了初步见识。方法:用(1)肠源性人α防御素5,(2)皮肤源性人β防御素1和(3)磺胺嘧啶治疗鼠三度烧伤创面,以确定它们在伤口愈合,细菌减少中的作用。和头发生长。结果:与人β防御素1和磺胺嘧啶相比,人α防御素5肽可显着增强伤口愈合并降低基础细菌负荷。人α防御素5是诱导LGR干细胞迁移到创面的唯一疗法。此外,基因热图谱显示关键伤口愈合和Wnt通路转录物(例如Wnt1和Wisp1)的mRNA显着上调。离体研究显示,与对照相比,人α防御素5处理的伤口中细胞迁移增强。结论:人α防御素5的应用增加了LGR干细胞向伤口床的迁移,从而通过增强关键的Wnt和伤口愈合转录本而增强了愈合,减少细菌并产生了毛发。这些发现可用于在伤口愈合中获得基于肠蛋白的疗法。

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