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一种用于缺血预处理的新型小鼠岛状皮瓣。

A novel murine island skin flap for ischemic preconditioning.

作者信息

Tatlidede Soner, McCormack Michael C, Eberlin Kyle R, Nguyen John T, Randolph Mark A, Austen William G

机构信息

Plastic Surgery Research Laboratory, Division of Plastic Surgery, Massachusetts General Hospital, Harvard Medical School, Boston, Massachusetts 02114, USA.

出版信息

J Surg Res. 2009 Jun 1;154(1):112-7. doi: 10.1016/j.jss.2008.05.029. Epub 2008 Jun 20.

Abstract

BACKGROUND

Ischemia reperfusion injury is a well-known phenomenon affecting skin flap viability. One method to improve flap viability is ischemic preconditioning. Previous murine flap models used random flaps. We developed a single pedicle island skin flap which allows us to create true ischemia by clamping the single pedicle. Our first aim was to describe a novel murine skin flap model with a definable, reproducible injury. Our second aim was to test the usefulness of this model by demonstrating mitigation of injury via ischemic preconditioning.

MATERIALS AND METHODS

Dorsal lateral thoracic artery pedicle island skin flaps (3.5 x 1.5 cm) were elevated in 39 male C57/BL6 mice: a Control group (n = 7), 10 h of ischemia (n = 21), and Preconditioning (2 cycles of 20 min ischemia: 20 minutes reperfusion) + 10-h ischemia (n = 11). After flap elevation, a silicon sheet barrier was placed. The axial pedicles were occluded, and the flaps were inset with 6-0 prolene. In all mice, ischemia was followed by 1 wk of reperfusion. At 1 wk, percent necrosis was measured and an analysis of variance was performed.

RESULTS

The percent of flap necrosis was 1.1% +/- 1.11% in controls. Animals that were subjected to 10 h of ischemia developed 33.14% +/- 7.23% necrosis. Preconditioned animals that underwent 10 h of ischemia demonstrated a 43% reduction in necrosis (18.82% +/- 5.68%). There was a statistically significant difference among all groups (P < or = 0.001).

CONCLUSION

Rat models have been the standard for skin flap experiments. We have developed a novel murine single pedicle island skin flap model with reproducible injury. This model has numerous advantages, including ease of handling, low cost, appropriateness for biomedical studies, and the availability of genetically altered animals. We also confirmed this model's usefulness in a study of mitigation of ischemia reperfusion injury through ischemic preconditioning.

摘要

背景

缺血再灌注损伤是影响皮瓣存活的一种已知现象。改善皮瓣存活的一种方法是缺血预处理。先前的小鼠皮瓣模型使用的是随意皮瓣。我们开发了一种单蒂岛状皮瓣,通过钳夹单蒂可造成真正的缺血。我们的首要目标是描述一种具有可定义、可重复损伤的新型小鼠皮瓣模型。我们的第二个目标是通过证明缺血预处理可减轻损伤来测试该模型的实用性。

材料与方法

在39只雄性C57/BL6小鼠中掀起背外侧胸动脉蒂岛状皮瓣(3.5×1.5厘米):一个对照组(n = 7)、缺血10小时组(n = 21)以及预处理组(2个20分钟缺血:20分钟再灌注周期)+缺血10小时组(n = 11)。掀起皮瓣后,放置一块硅片屏障。阻断轴型蒂,用6-0普理灵缝合皮瓣。所有小鼠缺血后均进行1周的再灌注。在1周时,测量坏死百分比并进行方差分析。

结果

对照组皮瓣坏死百分比为1.1%±1.11%。经历10小时缺血的动物发生了33.14%±7.23%的坏死。经预处理后经历10小时缺血的动物坏死减少了43%(18.82%±5.68%)。所有组之间存在统计学显著差异(P≤0.001)。

结论

大鼠模型一直是皮瓣实验的标准。我们开发了一种具有可重复损伤的新型小鼠单蒂岛状皮瓣模型。该模型具有许多优点,包括易于操作、成本低、适用于生物医学研究以及可获得基因改造动物。我们还在一项通过缺血预处理减轻缺血再灌注损伤的研究中证实了该模型的实用性。

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