首页> 外文期刊>Journal of tissue engineering and regenerative medicine >Perfusion bioreactor culture of human adipose-derived stromal cells on decellularized adipose tissue scaffolds enhances in vivo adipose tissue regeneration
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Perfusion bioreactor culture of human adipose-derived stromal cells on decellularized adipose tissue scaffolds enhances in vivo adipose tissue regeneration

机译:灌注生物反应器培养物脱脂型脂肪组织支架上的人脂肪衍生的基质细胞增强体内脂肪组织再生

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Tissue-engineering approaches hold promise to address the need in plastic and reconstructive surgery for new therapies that promote stable adipose tissue regeneration. Previous studies have demonstrated the potential of combining decellularized adipose tissue (DAT) scaffolds with adipose-derived stromal cells (ASCs) for volume augmentation applications. With the goal of enhancing in vivo angiogenesis and adipogenesis, this study evaluated the effects of culturing human ASCs on DAT scaffolds within a perfusion bioreactor. Using this system, the impact of both dynamic culture and hypoxic preconditioning were explored in vitro and in vivo. Initial studies compared the effects of 14 days of culture within the perfusion bioreactor under hypoxia (2% O-2) or normoxia (similar to 20% O-2) on human ASC expansion and expression of hypoxia inducible factor-1 alpha (HIF-1 alpha) in vitro relative to static cultured controls. The findings indicated that culturing within the bioreactor under hypoxia significantly increased ASC proliferation on the DAT, with a higher cell density observed in the scaffold periphery. Subsequent characterization in a subcutaneous implant model in athymic nude mice revealed that in vivo angiogenesis and adipogenesis were markedly enhanced when the ASCs were cultured on the DAT within the perfusion bioreactor under hypoxia for 14 days prior to implantation relative to the other culture conditions, as well as freshly seeded and unseeded DAT control groups. Overall, dynamic culture within the perfusion bioreactor system under hypoxia represents a promising approach for preconditioning ASCs on DAT scaffolds to enhance their capacity to stimulate angiogenesis and host-derived adipose tissue regeneration.
机译:组织工程方法有望解决整形和重建手术对促进稳定脂肪组织再生的新疗法的需求。先前的研究已经证明了脱细胞脂肪组织(DAT)支架与脂肪基质细胞(ASC)结合用于体积增大应用的潜力。为了增强体内血管生成和脂肪生成,本研究评估了在灌注生物反应器内DAT支架上培养人ASC的效果。利用该系统,在体外和体内探索了动态培养和低氧预处理的影响。初步研究比较了在缺氧(2%O-2)或常氧(类似于20%O-2)条件下,灌注生物反应器内培养14天对体外培养的人ASC扩增和缺氧诱导因子-1α(HIF-1α)表达的影响。研究结果表明,在缺氧条件下在生物反应器内培养显著增加了DAT上的ASC增殖,在支架周围观察到更高的细胞密度。在裸鼠皮下移植模型中的后续表征表明,相对于其他培养条件,以及新鲜种子和未种子DAT对照组,ASC在植入前在灌注生物反应器内的DAT上缺氧培养14天时,体内血管生成和脂肪生成显著增强。总的来说,在缺氧条件下灌注生物反应器系统内的动态培养代表了在DAT支架上预处理ASC以增强其刺激血管生成和宿主源性脂肪组织再生的能力的一种有希望的方法。

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