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体内可视化野生型/GFP 杂交模型中皮肤移植物血管生成的起源。

In vivo visualization of the origination of skin graft vasculature in a wild-type/GFP crossover model.

机构信息

Division of Plastic and Reconstructive Surgery, Department of Surgery, University Hospital Zurich, Rämistrasse 100, 8091 Zürich, Switzerland.

出版信息

Microvasc Res. 2011 Nov;82(3):237-45. doi: 10.1016/j.mvr.2011.07.003. Epub 2011 Jul 20.

Abstract

INTRODUCTION

Skin substitutes are increasingly produced in tissue engineering, but still the understanding of the physiological skin revascularization process is lacking. To study in vivo conditions we recently introduced a mouse model, in which we already characterized the angiogenic changes within the wound bed and the skin graft. The aim of this study was to identify the origination of the vasculature during skin graft revascularization in vivo and to track vessel development over time.

METHODS

We created a crossover wild-type/GFP skin transplantation model, in which each animal carried the graft from the other strain. The preparation of the modified dorsal skin fold chamber including cross-over skin grafting was performed in male C57BL/6J wild-type mice (n=5) and C57BL/6-Tg(ACTB-EGFP)1O sb/J mice (n=5). Intravital microscopy in 12 areas of wild-type and GFP skin grafts was performed daily over a time period of 10 days.

RESULTS

Graft reperfusion started after 48-72 h. After reperfusion GFP-positive structures from the wound bed were visible in the graft capillaries with the highest density in the center of the graft. Overall, we observed a replacement of existing graft capillaries with vessels from the wound bed in 68% of the vessels. Of note, vessel replacement occurred in almost 100% of graft vessels in the periphery. Additionally, vessels within the graft showed a temporary angiogenic response between days 3-8, which originated predominantly from the autochthonous graft vasculature, but also contained already grown-in vessels from the wound bed.

CONCLUSIONS

These in vivo data indicate an early in-growth of angiogenic bed vessels into the existing vascular channels of the graft and subsequent centripetal replacement. Additionally we observed a temporary angiogenic response of the autochthonous capillaries of the skin graft with contribution from bed vessels. These findings further support the theory that sprouting angiogenesis from the wound bed in combination with the replacement of existing graft vessels are the key factors in skin graft taking. Thus, manufacturing of skin substitutes should be aimed at providing pre-formed vascular channels within the construct to improve vascularization.

摘要

简介

皮肤替代物在组织工程中越来越多地被生产,但对生理皮肤再血管化过程的理解仍有所欠缺。为了研究体内情况,我们最近引入了一种小鼠模型,其中我们已经描述了创面床和皮片移植物中的血管生成变化。本研究的目的是确定体内皮片移植物再血管化过程中血管的起源,并跟踪随时间的血管发育。

方法

我们创建了一个野生型/GFP 皮肤移植的交叉模型,其中每个动物携带来自另一个品系的移植物。在雄性 C57BL/6J 野生型小鼠(n=5)和 C57BL/6-Tg(ACTB-EGFP)1O sb/J 小鼠(n=5)中进行了改良的背部皮肤折叠室的准备,包括交叉皮片移植。在 10 天的时间内,每天对 12 个野生型和 GFP 皮肤移植物区域进行活体显微镜检查。

结果

移植物再灌注在 48-72 小时后开始。再灌注后,在移植物毛细血管中可见来自创面床的 GFP 阳性结构,在移植物中心密度最高。总体而言,我们观察到在 68%的血管中,存在用来自创面床的血管替代现有移植物血管的情况。值得注意的是,在移植物的周边区域,血管替代几乎发生在 100%的移植物血管中。此外,移植物内的血管在第 3-8 天之间显示出短暂的血管生成反应,该反应主要来自移植物自身的血管,但也包含来自创面床的已生长的血管。

结论

这些体内数据表明,早期血管生成床血管向内生长到移植物现有的血管通道,并随后向中心进行替代。此外,我们观察到移植物自身毛细血管的短暂血管生成反应,其来源是床血管。这些发现进一步支持这样的理论,即来自创面床的发芽血管生成结合对现有移植物血管的替代是皮肤移植物成功的关键因素。因此,皮肤替代物的制造应旨在提供构建体中的预先形成的血管通道,以改善血管化。

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