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颅骨腔室——一种用于活体评估骨质血管生成的新模型。

Calvaria bone chamber--a new model for intravital assessment of osseous angiogenesis.

机构信息

Department of Oral and Maxillofacial Surgery, Hannover Medical School, Hannover, Germany.

出版信息

J Biomed Mater Res A. 2011 Nov;99(2):151-7. doi: 10.1002/jbm.a.32955. Epub 2011 Aug 16.

Abstract

The faith of tissue engineered bone replacing constructs depends on their early supply with oxygen and nutrients, and thus on a rapid vascularization. Although some models for direct observation of angiogenesis are described, none of them allows the observation of new vessel formation in desmal bone. Therefore, we developed a new chamber model suitable for quantitative in vivo assessment of the vascularization of bone substitutes by intravital fluorescence microscopy. In the parietal calvaria of 32 balb/c mice a critical size defect was set. Porous 3D-poly(L-lactide-co-glycolide) (PLGA)-blocks were inserted into 16 osseous defects (groups 3 and 4) while other 16 osseous defects remained unequipped (groups 1 and 2). By placing a polyethylene membrane onto the dura mater, the angiogenesis was mainly restricted to the osseous margins (groups 2 and 4). Microvascular density, angiogenesis, and microcirculatory parameters were evaluated repetitively during 22 days. In all animals, only a mild inflammatory reaction was observed with a climax after 2 weeks. The implantation of PLGA scaffolds resulted in a vascular growth directed towards the center of the defect as demonstrated by the significantly (p < 0.05) enhanced central microvascular densitiy from day 3 to day 22 when compared with unequipped chambers. The additional application of polyethylene membrane was found to reduce significantly the microvessel density mainly in the center of both scaffolds and defects. The present calvaria bone chamber allows for the first time to assess quantitatively the angiogenesis arising from desmal bone directly in vivo. Therefore, this chronic model may support the future research in the biological adequacy of bone substitutes.

摘要

组织工程骨替代物的构建体的形成依赖于其早期氧和营养物质的供应,因此依赖于快速的血管生成。尽管已经描述了一些用于直接观察血管生成的模型,但它们都不允许观察到骨膜中的新血管形成。因此,我们开发了一种新的室模型,适用于通过活体荧光显微镜对骨替代物的血管化进行定量的体内评估。在 32 只 balb/c 小鼠的顶骨颅骨上设置了一个临界尺寸缺陷。将多孔 3D-聚(L-丙交酯-co-乙交酯)(PLGA)块插入 16 个骨质缺损中(第 3 组和第 4 组),而其他 16 个骨质缺损则没有配备(第 1 组和第 2 组)。通过将聚乙烯膜放置在硬脑膜上,血管生成主要限制在骨质边缘(第 2 组和第 4 组)。在 22 天内重复评估微血管密度、血管生成和微循环参数。在所有动物中,仅观察到轻微的炎症反应,2 周后达到高峰。PLGA 支架的植入导致血管生长朝向缺陷的中心,与未配备腔室的支架相比,从第 3 天到第 22 天,中央微血管密度显著增加(p < 0.05)。发现额外应用聚乙烯膜主要减少了支架和缺陷中心的微血管密度。目前的颅骨骨室首次允许直接在体内定量评估来自骨膜的血管生成。因此,这种慢性模型可能支持骨替代物的未来生物学评估研究。

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