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首页> 外文期刊>RSC Advances >Short-term hypoxic preconditioning promotes prevascularization in 3D bioprinted bone constructs with stromal vascular fraction derived cells
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Short-term hypoxic preconditioning promotes prevascularization in 3D bioprinted bone constructs with stromal vascular fraction derived cells

机译:短期缺氧预处理可促进具有基质血管部分衍生细胞的3D生物打印骨构造中的血管生成

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Reconstruction of complex, craniofacial bone defects often requires autogenous vascularized bone grafts, and still remains a challenge today. In order to address this issue, we isolated the stromal vascular fraction (SVF) from adipose tissues and maintained the phenotypes and the growth of endothelial lineage cells within SVF derived cells (SVFC) by incorporating an endothelial cell medium. We 3D bioprinted SVFC within our hydrogel bioinks and conditioned the constructs in either normoxia or hypoxia. We found that short-term hypoxic conditioning promoted vascularization-related gene expression, whereas long-term hypoxia impaired cell viability and vascularization. 3D bioprinted bone constructs composed of polycaprolactone/hydroxyapatite (PCL/HAp) and SVFC-laden hydrogel bioinks were then implanted into athymic mice, after conditioning in normoxic or short-term hypoxic environments, in order to determine the in vitro and in vivo vascularization and osteogenic differentiation of the constructs. Short-term hypoxic conditioning promoted microvessel formation in vitro and in vivo and promoted integration with existing host vasculature, but did not affect osteogenic differentiation of SVFC. These findings demonstrate the benefit of short-term hypoxia and the potential for utilization of SVFC and 3D bioprinting for generating prevascularized 3D bioprinted bone constructs. Furthermore, the ability to custom design complex anatomical shapes has promising applications for the regeneration of both large and small craniofacial bone defects.
机译:复杂的颅面骨缺损的重建通常需要自体血管化的骨移植,并且仍然是当今的挑战。为了解决这个问题,我们从脂肪组织中分离出了间质血管部分(SVF),并通过整合内皮细胞培养基来维持SVF衍生细胞(SVFC)内的表型和内皮细胞谱系细胞的生长。我们在水凝胶生物墨水中对SVFC进行了3D生物打印,并在正常氧或缺氧条件下调节了构建体。我们发现短期缺氧条件促进血管生成相关的基因表达,而长期缺氧会损害细胞活力和血管生成。在常氧或短期低氧环境中进行调节后,将由聚己内酯/羟基磷灰石(PCL / HAp)和载有SVFC的水凝胶生物墨水组成的3D生物打印的骨骼构建体植入无胸腺小鼠中,以测定体外 体内的血管生成和成骨细胞分化。短期缺氧条件促进了体外和体外的微血管形成,促进了与现有宿主脉管系统的整合,但并未影响SVFC的成骨分化。这些发现证明了短期缺氧的益处以及利用SVFC和3D生物打印产生血管生成的3D生物打印骨构造的潜力。此外,定制设计复杂解剖形状的能力在大和小颅面骨缺损的再生中都具有广阔的应用前景。

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