首页> 外文期刊>Journal of biomedical materials research, Part A >Optimization of Microencapsulated Recombinant CHO Cell Growth, Endostatin Production, and Stability of Microcapsule In Vivo
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Optimization of Microencapsulated Recombinant CHO Cell Growth, Endostatin Production, and Stability of Microcapsule In Vivo

机译:微囊化重组CHO细胞生长,内皮抑素生产和微囊体内稳定性的优化

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Microencapsulation of recombinant cells secreting endostatin offers a promising approach to tumor gene therapy in which therapeutic protein is delivered in a sustainable and long-term fashion by encapsulated recombinant cells. However, the studies of cell growth and protein production in vivo are very limited. In this study, the effects of microencapsulation parameters on in vivo cell growth, endostatin production, and microcapsule stability after implantation in the peritoneal cavity of mice were for the first time investigated. Microcapsules with liquid core reached higher cell density and endostatin production at day 18 than microcapsules with solid core. There was no significant difference in stability whether the core of the microcapsule was solid or liquid. Decrease in microcapsule size increased the stability of microcapsule. The microcapsules kept intact in the peritoneal cavity of mice after 36 days of implantation when the microcapsules size was 240 mu m in diameter, which gave rise to high endostatin production as well. The optimized microencapsulation conditions for in vivo implantation are liquid core and 240 mu m in diameter. This study provides useful information for antiangiogenic gene therapy to tumors using microencapsulated recombinant cells.
机译:分泌内皮抑素的重组细胞的微囊化为肿瘤基因治疗提供了一种有希望的方法,其中通过封装的重组细胞以可持续和长期的方式递送治疗性蛋白质。然而,体内细胞生长和蛋白质生产的研究非常有限。在这项研究中,首次研究了微囊化参数对小鼠腹膜腔内植入后体内细胞生长,内皮抑素产生和微囊稳定性的影响。具有液体核心的微胶囊在第18天比具有固体核心的微胶囊达到更高的细胞密度和内皮抑素生产。无论微胶囊的核心是固体还是液体,稳定性都没有显着差异。微胶囊尺寸的减小增加了微胶囊的稳定性。植入36天后,当微胶囊的直径为240μm时,微胶囊在小鼠的腹膜腔中保持完整,这也引起了高内皮抑素的产生。用于体内植入的最佳微囊包封条件是液芯,直径为240μm。该研究为使用微囊化重组细胞对肿瘤的抗血管生成基因治疗提供了有用的信息。

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