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在成年瘢痕形成模型中,白细胞介素-10的过表达可减少炎症介质并促进再生愈合。

IL-10 overexpression decreases inflammatory mediators and promotes regenerative healing in an adult model of scar formation.

作者信息

Peranteau William H, Zhang Liping, Muvarak Nidal, Badillo Andrea T, Radu Antoneta, Zoltick Philip W, Liechty Kenneth W

机构信息

Department of Surgery, The Center for Fetal Research, The Children's Hospital of Philadelphia, Philadelphia, Pennsylvania 19104-4318, USA.

出版信息

J Invest Dermatol. 2008 Jul;128(7):1852-60. doi: 10.1038/sj.jid.5701232. Epub 2008 Jan 17.

Abstract

Adult wound healing is characterized by an exuberant inflammatory response and scar formation. In contrast, scarless fetal wound healing has diminished inflammation, a lack of fibroplasia, and restoration of normal architecture. We have previously shown that fetal wounds produce less inflammatory cytokines, and the absence of IL-10, an anti-inflammatory cytokine, results in fetal scar formation. We hypothesized that increased IL-10 would decrease inflammation and create an environment conducive for regenerative healing in the adult. To test this hypothesis, a lentiviral vector expressing IL-10 and green fluorescent protein (GFP) (Lenti-IL-10) or GFP alone (Lenti-GFP) was injected at the wound site 48 hours before wounding. We found that both Lenti-IL-10 and Lenti-GFP were expressed in the wounds at 1 and 3 days post wounding. At 3 days, Lenti-IL-10-treated wounds demonstrated decreased inflammation and decreased quantities of all proinflammatory mediators analyzed with statistically different levels of IL-6, monocyte chemoattractant protein-1, and heat-shock protein 47. At 3 weeks, Lenti-GFP wounds demonstrated scar formation. In contrast, wounds injected with Lenti-IL-10 demonstrated decreased inflammation, a lack of abnormal collagen deposition, and restoration of normal dermal architecture. We conclude that lentivirus-mediated overexpression of IL-10 decreases the inflammatory response to injury, creating an environment conducive for regenerative adult wound healing.

摘要

成人伤口愈合的特点是炎症反应旺盛和瘢痕形成。相比之下,胎儿伤口无瘢痕愈合的炎症反应减弱,缺乏纤维组织增生,且能恢复正常结构。我们之前已经表明,胎儿伤口产生的炎性细胞因子较少,而抗炎细胞因子白细胞介素-10(IL-10)的缺失会导致胎儿瘢痕形成。我们推测,增加IL-10的表达会减轻炎症,并为成人创造有利于再生愈合的环境。为了验证这一假设,在受伤前48小时将表达IL-10和绿色荧光蛋白(GFP)的慢病毒载体(Lenti-IL-10)或仅表达GFP的慢病毒载体(Lenti-GFP)注射到伤口部位。我们发现,在受伤后1天和3天,Lenti-IL-10和Lenti-GFP均在伤口中表达。在第3天,经Lenti-IL-10处理的伤口炎症减轻,所有分析的促炎介质数量均减少,白细胞介素-6、单核细胞趋化蛋白-1和热休克蛋白47的水平具有统计学差异。在第3周时,Lenti-GFP处理的伤口出现瘢痕形成。相比之下,注射Lenti-IL-10的伤口炎症减轻,无异常胶原沉积,真皮结构恢复正常。我们得出结论,慢病毒介导的IL-10过表达可减轻对损伤的炎症反应,为成人再生性伤口愈合创造有利环境。

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