小鼠背侧皮褶腔模型。

IF 1 Q3 SURGERY
Jeannine Schreiter, Sophia Meyer, Christian Schmidt, Ronny M Schulz, Stefan Langer
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引用次数: 21

摘要

背景/目的:在过去的八十年中,背侧皮肤褶腔模型的使用大大提高了对病理生理学中微血管化的理解。它允许在连续一段时间内对血管化进行体内病理生理研究。背侧皮肤褶腔是一种有吸引力的技术,用于监测自体或异体移植、伤口愈合、肿瘤发生和生物材料植入物的相容性。为了进一步减少动物携带背皮褶腔时的不适,我们开发了一个更小的腔(Leipzig背皮褶腔),并总结了商业上可用的腔模型。此外,我们还将我们的模型与普通腔室进行了比较。方法:采用莱比锡背侧皮褶实验箱对66只平均体重22 g的C57Bl/6雌性小鼠进行实验。在Axio显微镜下观察注射异硫氰酸葡聚糖荧光素后背皮肤折叠腔内血管生成情况。在21天的时间内,在5个不同的时间点评估背侧皮褶腔内的平均血管密度。将获得的数据与先前使用更大和更重的小鼠背皮肤褶模型的结果进行比较。通过PubMed检索和专利检索,对2006年1月1日至2015年12月31日所有与“背侧皮肤褶腔”相关的论文进行评估,评估背侧皮肤褶腔模型及其技术改进。主要模型进行了描述,并与我们的钛莱比锡背皮肤折叠室模型进行了比较。结果:莱比锡背侧皮褶实验室在减少对小鼠的刺激的同时,满足了以往实验室模型的连续体内模型的所有要求。已经确定了五种不同的腔室模型,显示出很大的区域差异。新制作的钛背皮肤折叠腔可能取代德国目前使用的钛腔模型,因为它比以前的更小,更轻。然而,新的燃烧室没有达到亚洲和美国现有的燃烧室模型的优势,这些模型更小、更轻。结论:设计一个更小更轻的背侧皮褶腔,可以对较小的动物进行研究,减少动物携带腔体时的不适。应该进行更多的研究交流,以推广使用更小、更轻的腔室模型。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Dorsal skinfold chamber models in mice.

Dorsal skinfold chamber models in mice.

Dorsal skinfold chamber models in mice.

Dorsal skinfold chamber models in mice.

Background/purpose: The use of dorsal skinfold chamber models has substantially improved the understanding of micro-vascularisation in pathophysiology over the last eight decades. It allows in vivo pathophysiological studies of vascularisation over a continuous period of time. The dorsal skinfold chamber is an attractive technique for monitoring the vascularisation of autologous or allogenic transplants, wound healing, tumorigenesis and compatibility of biomaterial implants. To further reduce the animals' discomfort while carrying the dorsal skinfold chamber, we developed a smaller chamber (the Leipzig Dorsal Skinfold Chamber) and summarized the commercial available chamber models. In addition we compared our model to the common chamber. Methods: The Leipzig Dorsal Skinfold Chamber was applied to 66 C57Bl/6 female mice with a mean weight of 22 g. Angiogenesis within the dorsal skinfold chamber was evaluated after injection of fluorescein isothiocyanate dextran with an Axio Scope microscope. The mean vessel density within the dorsal skinfold chamber was assessed over a period of 21 days at five different time points. The gained data were compared to previous results using a bigger and heavier dorsal skinfold model in mice. A PubMed and a patent search were performed and all papers related to "dorsal skinfold chamber" from 1st of January 2006 to 31st of December 2015 were evaluated regarding the dorsal skinfold chamber models and their technical improvements. The main models are described and compared to our titanium Leipzig Dorsal Skinfold Chamber model. Results: The Leipzig Dorsal Skinfold Chamber fulfils all requirements of continuous in vivo models known from previous chamber models while reducing irritation to the mice. Five different chamber models have been identified showing substantial regional diversity. The newly elaborated titanium dorsal skinfold chamber may replace the pre-existing titanium chamber model used in Germany so far, as it is smaller and lighter than the former ones. However, the new chamber does not reach the advantages of already existing chamber models used in Asia and the US, which are smaller and lighter. Conclusion: Elaborating a smaller and lighter dorsal skinfold chamber allows research studies on smaller animals and reduces the animals' discomfort while carrying the chamber. Greater research exchange should be done to spread the use of smaller and lighter chamber models.

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