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通过重复局部应用胰岛素样生长因子-I(IGF-I)刺激类固醇抑制的皮肤愈合:基于IGF-I递送方式的不同作用机制。

Stimulation of steroid-suppressed cutaneous healing by repeated topical application of IGF-I: different mechanisms of action based upon the mode of IGF-I delivery.

作者信息

Beckert Stefan, Haack Sebastian, Hierlemann Helmut, Farrahi Farshid, Mayer Petra, Königsrainer Alfred, Coerper Stephan

机构信息

Department of General and Transplant Surgery, University of Tübingen, Tübingen, Germany.

出版信息

J Surg Res. 2007 May 15;139(2):217-21. doi: 10.1016/j.jss.2006.08.006. Epub 2006 Oct 27.

Abstract

BACKGROUND

Insulin-like growth factor-I (IGF-I) is accepted as a potent stimulus of wound healing when applied in combination with its binding proteins. However, there is only one study published that has investigated the effect of repeated topical application of unbound IGF-I on ischemic wound healing. The aim of this study was to show the effect of daily topical IGF-I therapy on cutaneous ulcer healing in a steroid-suppressed wound model.

MATERIALS AND METHODS

Full-thickness wounds were created on the back of 40 male Sprague-Dawley rats. Before surgery, animals received depot-steroids subcutaneously. Wounds were treated daily with either a standard hydrogel dressing (control), topical IGF-I dissolved in 0.2% methylcellulose gel (IGF-I gel), or a hydrogel dressing containing IGF-I (IGF-I dressing). After 7 days of treatment, wounds were excised and measured by photoplanimetry. SMA- and PCNA-expression as well as the formation of granulation tissue were assessed in tissue sections. Results are given as median(min-max). Differences between groups were calculated by the Mann-Whitney U test.

RESULTS

Subcutaneous injection of depot-steroids induced a significant delay in healing, as shown by an enlarged wound size [44(33-65) versus 25(20-35)] mm(2); P = 0.001). In steroid-treated rats, both IGF-I gel and IGF-I dressing enhanced excisional healing, as shown by a significant reduction in wound size (P = 0.0001), with IGF-I released from the dressing being even more effective than IGF-I gel (P = 0.03). However, in these animals only IGF-I released from the hydrogel dressing stimulated SMA- (P = 0.03) as well as PCNA-expression (P = 0.001) and increased granulation tissue formation (P = 0.018).

CONCLUSIONS

Our data indicate that a repeated application of topical IGF-I enhances cutaneous ulcer healing. In addition, only the controlled release of IGF-I from the hydrogel dressing is capable of reversing the steroid-induced delay of healing, suggesting different mechanisms of action with respect to the mode of IGF-I delivery.

摘要

背景

胰岛素样生长因子-I(IGF-I)与它的结合蛋白联合应用时被认为是伤口愈合的有力刺激因素。然而,仅有一项已发表的研究调查了重复局部应用未结合的IGF-I对缺血性伤口愈合的影响。本研究的目的是在类固醇抑制的伤口模型中显示每日局部应用IGF-I治疗对皮肤溃疡愈合的影响。

材料与方法

在40只雄性Sprague-Dawley大鼠背部制造全层伤口。手术前,动物皮下注射长效类固醇。伤口每日用标准水凝胶敷料(对照)、溶解于0.2%甲基纤维素凝胶的局部IGF-I(IGF-I凝胶)或含IGF-I的水凝胶敷料(IGF-I敷料)进行治疗。治疗7天后,切除伤口并用平面光度法测量。在组织切片中评估平滑肌肌动蛋白(SMA)和增殖细胞核抗原(PCNA)的表达以及肉芽组织的形成。结果以中位数(最小值-最大值)表示。组间差异通过Mann-Whitney U检验计算。

结果

皮下注射长效类固醇导致愈合显著延迟,伤口大小增大即可表明[44(33 - 65)对25(20 - 35)]平方毫米;P = 0.001)。在类固醇治疗的大鼠中,IGF-I凝胶和IGF-I敷料均促进切除后的愈合,伤口大小显著减小即可表明(P = 0.0001),从敷料中释放的IGF-I比IGF-I凝胶更有效(P = 0.03)。然而,在这些动物中,只有从水凝胶敷料中释放的IGF-I刺激了SMA表达(P = 0.03)以及PCNA表达(P = 0.001)并增加了肉芽组织形成(P = 0.018)。

结论

我们的数据表明,重复局部应用IGF-I可促进皮肤溃疡愈合。此外,只有从水凝胶敷料中控制释放IGF-I能够逆转类固醇诱导的愈合延迟,提示在IGF-I递送方式方面存在不同的作用机制。

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