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首页> 外文期刊>Journal of biomedical materials research, Part A >Angiogenesis, Endothelial Cell Functions, and Tumor Cell Growth in Biodegradable and Nonbiodegradable Devices
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Angiogenesis, Endothelial Cell Functions, and Tumor Cell Growth in Biodegradable and Nonbiodegradable Devices

机译:可生物降解和非增生装置中的血管生成,内皮细胞功能和肿瘤细胞生长

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Development of tissue engineering creates multiple potentials for clinical treatment and scientific research. Biodegradable collagen matrices have been found to support simultaneous autotransplantation of hepatocytes after major liver resection. Dynamic angiogenesis in biodegradable devices (BDD) and nondegradable devices (NDD) transplanted into the renal subcapsule and subcutaneous tissue was measured by the distribution of radiolabeled red blood cells and serum albumin. The circulation, microvascular integrity, and capacities of endothelial cells (adhesion, proliferation, and migration) were investigated within 2 weeks after subcutaneous transplantation of both devices. Patterns of tumor cell growth in both devices were morphologically studied. After subcutaneous transplantation, significant angiogenesis was noted at 1 week in BDD implants and from 2 weeks and on in NDD implants, with an increase in implant blood and plasma volumes. Leakage index of radiolabeled albumin in NDD implants was significantly higher than in BDD implants, while the leakage index 2 weeks after BDD implant was similar to that in subcutaneous tissues. Adhesion, proliferation and migration rates of endothelial cells isolated from both devices were higher than from subcutaneous tissues. Endothelial proliferation and migration rates in BDD implants were significantly higher at 1 week, while in NDD at 2 weeks. Tumor cells migrated and grew on the top surface of NDD with a flattened shape, while growing within the BDD forming a round mass. Endothelial capacities, angiogenetic procedure, and biological and physical characteristics of the device contribute to patterns of tumor cell growth in the device. Biodegradable collagen matrix with three-dimensional structure is suitable for simultaneous transplantation with cells without prevascularization.
机译:组织工程的发展为临床治疗和科学研究产生了多种潜力。已经发现可生物降解的胶原蛋白基质支持主要肝切除后同时同时为肝细胞的固化性。通过放射性标记的红细胞和血清白蛋白的分布测量可生物降解装置(BDD)和非肾脏亚皮层和皮下组织中的可生物降解装置(BDD)和非致肾亚皮巾和皮下组织的动态血管生成。在两种装置的皮下移植后2周内研究了内皮细胞(粘附,增殖和迁移)的循环,微血管完整性和能力。两种装置的肿瘤细胞生长模式在形态学上研究。在皮下移植后,在BDD植入物的1周内并在NDD植入物中的1周和NDD植入物中提高了显着的血管生成,植入血液和血浆体积增加。 NDD植入物中放射性标记白蛋白的泄漏指数显着高于BDD植入物,而BDD植入后2周的泄漏指数与皮下组织中的泄漏指数相似。从两种装置中分离的内皮细胞的粘附,增殖和迁移率高于皮下组织。 BDD植入物的内皮增殖和迁移率在1周的1周明显高,而在2周内在NDD中均显着提高。肿瘤细胞在NDD的顶表面上迁移并以扁平的形状升高,同时在BDD内生长形成圆形质量。内皮容量,血管生成过程和器件的生物学和物理特性有助于装置中肿瘤细胞生长的模式。具有三维结构的可生物降解的胶原基质适用于在没有血血压的情况下同时移植细胞。

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