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首页> 外文期刊>Journal of biomedical materials research. Part B, Applied biomaterials. >Engineering the tissue which encapsulates subcutaneous implants. II. Plasma-tissue exchange properties.
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Engineering the tissue which encapsulates subcutaneous implants. II. Plasma-tissue exchange properties.

机译:工程化封装皮下植入物的组织。二。血浆-组织交换特性。

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This study assesses the plasma-tissue exchange characteristics of the capsular tissue that forms around implants and how they are affected by implant porosity. The number of vessels and their permeability to rhodamine were measured by intravascular injection of the fluorophore tracer into Sprague-Dawley rats that hosted for 3-4 months polyvinyl alcohol (PVA) and polytetrafluoroethylene (PTFE) subcutaneous implants. Rats were implanted with four pore sizes of PVA--a nonporous PVA (PVA-skin), and 5, 60, and 700 micron mean pore sizes (PVA-5, PVA-60, and PVA-700, respectively)--and two pore sizes of PTFE: 0.50 (PTFE-0.5) and 5.0 (PTFE-5) mean micron pore sizes. Photodensitometric image analysis was used to quantify the local tracer extravasation and, hence the permeability coefficients of isolated vessels around the implants. The number of functional vessels within 100 microm of the implants highlighted by the lissamine-rhodamine tracer were counted with fluorescence microscopy and with H&E stained sections using brightfield microscopy. The permeability of vessels did not vary substantially with implant pore size but generally were lower than those measured for surrounding subcutis. Pore size, however, had a dramatic effect on the vascular density of tissue-encapsulating implants: the number of microvessels (under 10 microm in radius) within the tissue surrounding the porous implants was higher than the number around nonporous implants. Pore sizes on the order of cellular dimensions incited optimal neovascularization; the vascular density around PVA-60 implants was six times higher (p < .001) and three times higher (p < .001) than those around PVA-0 implants in the fluorescent images and in brightfield, respectively. Moreover, brightfield microscopy showed the number of vessels around PVA-60 implants was almost double those in normal subcutis. The results suggest that optimal vascular density around long-term implants, such as sensors, biofluid cell constructs, and immunoisolated cell systems, may be engineered with pore size.
机译:这项研究评估了在植入物周围形成的荚膜组织的血浆-组织交换特性,以及它们如何受到植入物孔隙度的影响。通过将荧光团示踪剂血管内注射到容纳3-4个月聚乙烯醇(PVA)和聚四氟乙烯(PTFE)皮下植入物的Sprague-Dawley大鼠中,测量血管的数量及其对罗丹明的渗透性。大鼠植入了四种孔径的PVA-无孔PVA(PVA-皮肤),5微米,60微米和700微米的平均孔径(分别为PVA-5,PVA-60和PVA-700)和PTFE的两种孔径:0.50(PTFE-0.5)和5.0(PTFE-5)的平均微米孔径。光密度计图像分析用于量化局部示踪剂外渗,从而量化植入物周围孤立血管的渗透系数。用荧光显微镜和通过H&E染色的切片使用明视野显微镜对由赖氨胺-罗丹明示踪剂强调的植入物100微米内的功能性血管数量进行计数。血管的渗透性并没有随植入物孔径的变化而变化,但通常低于对周围皮下组织的测量值。但是,孔的大小对包裹组织的植入物的血管密度有显着影响:多孔植入物周围的组织内的微血管(半径小于10微米)的数量高于无孔植入物周围的数量。孔尺寸在细胞尺寸上引起最佳的新生血管形成;在荧光图像和明场中,PVA-60植入物周围的血管密度分别比PVA-0植入物周围的血管密度高六倍(p <.001)和三倍(p <.001)。此外,明视野显微镜显示,PVA-60植入物周围的血管数量几乎是正常皮下组织的两倍。结果表明,可以通过孔径设计长期植入物(例如传感器,生物流体细胞构建体和免疫分离的细胞系统)周围的最佳血管密度。

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