在共聚物支架中接种骨髓基质细胞来递送 VEGFA 可增强血管生成,但与在皮下小鼠模型中双重递送 VEGFA 和 BMP2 相比,其成骨作用不足。
Delivery of VEGFA in bone marrow stromal cells seeded in copolymer scaffold enhances angiogenesis, but is inadequate for osteogenesis as compared with the dual delivery of VEGFA and BMP2 in a subcutaneous mouse model.
机构信息
Department of Clinical Dentistry, Centre for Clinical Dental Research, University of Bergen, 5020, Bergen, Norway.
Department of Oral Biology, Faculty of Dentistry, University of Oslo, 0316, Oslo, Norway.
出版信息
Stem Cell Res Ther. 2018 Jan 31;9(1):23. doi: 10.1186/s13287-018-0778-4.
BACKGROUND
In bone tissue engineering (BTE), extensive research into vascular endothelial growth factor A (VEGFA)-mediated angiogenesis has yielded inconsistent results. The aim of this study was to investigate the influence on angio- and osteogenesis of adenoviral-mediated delivery of VEGFA alone or in combination with bone morphogenetic protein 2 (BMP2) in bone marrow stromal cells (BMSC) seeded onto a recently developed poly(LLA-co-CL) scaffold.
METHODS
Human BMSC were engineered to express VEGFA alone or in combination with BMP2 and seeded onto poly(LLA-co-CL) scaffolds. Changes in angiogenic and osteogenic gene and protein levels were examined by quantitative reverse-transcription polymerase chain reaction (RT-PCR), PCR array, and alkaline phosphatase assay. An in vivo subcutaneous mouse model was used to investigate the effect on angio- and osteogenesis of VEGFA alone or in combination with BMP2, using microcomputed tomography (μCT), histology, immunohistochemistry, and immunofluorescence.
RESULTS
Combined delivery of a lower ratio (1:3) of VEGFA and BMP2 (ad-BMP2 + VEGFA) led to upregulation of osteogenic and angiogenic genes in vitro at 3 and 14 days, compared with mono-delivery of VEGFA (ad-VEGFA) and other controls. In vivo, in a subcutaneous mouse model, both ad-VEGFA and ad-BMP2 + VEGFA scaffold explants exhibited increased angiogenesis at 2 weeks. Enhanced angiogenesis was largely related to the recruitment and differentiation of mouse progenitor cells to the endothelial lineage and, to a lesser extent, to endothelial differentiation of the implanted BMSC. μCT and histological analyses revealed enhanced de novo bone formation only in the ad-BMP2 + VEGFA group, corresponding at the molecular level to the upregulation of genes related to osteogenesis, such as ALPL, RUNX2, and SPP1.
CONCLUSIONS
Although BMSC expressing VEGFA alone or in combination with BMP2 significantly induced angiogenesis, VEGFA alone failed to demonstrate osteogenic activity both in vitro and in vivo. These results not only call into question the use of VEGFA alone in bone regeneration, but also highlight the importance in BTE of appropriately formulated combined delivery of VEGFA and BMP2.
背景
在骨组织工程(BTE)中,广泛研究血管内皮生长因子 A(VEGFA)介导的血管生成,得到的结果并不一致。本研究旨在探讨单独或联合骨形态发生蛋白 2(BMP2)转染腺病毒载体在骨髓基质细胞(BMSC)种植于新型聚(LLA-co-CL)支架上对血管生成和成骨的影响。
方法
通过定量逆转录聚合酶链反应(RT-PCR)、PCR 阵列和碱性磷酸酶测定,检测单独或联合 BMP2 转染 VEGFA 对人 BMSC 血管生成和成骨基因和蛋白水平的影响。使用微计算机断层扫描(μCT)、组织学、免疫组织化学和免疫荧光,在体内皮下小鼠模型中,检测单独转染 VEGFA 或联合转染 BMP2 和 VEGFA 对血管生成和成骨的影响。
结果
与单独转染 VEGFA(ad-VEGFA)和其他对照组相比,在第 3 和 14 天,较低比例(1:3)的 VEGFA 和 BMP2 联合转染(ad-BMP2+VEGFA)可上调成骨和成血管基因。在体内皮下小鼠模型中,2 周时,ad-VEGFA 和 ad-BMP2+VEGFA 支架标本均表现出血管生成增加。增强的血管生成主要与小鼠祖细胞募集和向内皮谱系分化有关,在较小程度上与植入 BMSC 的内皮分化有关。μCT 和组织学分析仅显示 ad-BMP2+VEGFA 组有新骨形成增加,这与骨形成相关基因(如 ALPL、RUNX2 和 SPP1)的上调相对应。
结论
尽管单独或联合转染 BMSC 表达 VEGFA 显著诱导了血管生成,但单独转染 VEGFA 无论是在体外还是体内都未能显示出成骨活性。这些结果不仅对单独使用 VEGFA 进行骨再生提出了质疑,而且强调了在 BTE 中适当配方联合转染 VEGFA 和 BMP2 的重要性。
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