首页> 外文期刊>The Journal of Clinical Investigation: The Official Journal of the American Society for Clinical Investigation >Synergistic enhancement of bone formation and healing by stem cell-expressed VEGF and bone morphogenetic protein-4.
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Synergistic enhancement of bone formation and healing by stem cell-expressed VEGF and bone morphogenetic protein-4.

机译:通过干细胞表达的 VEGF 和骨形态发生蛋白-4 协同增强骨形成和愈合。

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摘要

We investigated the interaction between angiogenic and osteogenic factors in bone formation and bone healing with ex vivo gene therapy using muscle-derived stem cells genetically engineered to express human bone morphogenetic protein-4 (BMP4), VEGF, or VEGF-specific antagonist (soluble Flt1). Our results show that although VEGF alone did not improve bone regeneration, it acted synergistically with BMP4 to increase recruitment of mesenchymal stem cells, to enhance cell survival, and to augment cartilage formation in the early stages of endochondral bone formation. These early effects, coupled with accelerated cartilage resorption, eventually led to a significant enhancement of bone formation and bone healing. The beneficial effect of VEGF on bone healing elicited by BMP4 depends critically on the ratio of VEGF to BMP4, with an improper ratio leading to detrimental effects on bone healing. Finally, we show that soluble Flt1 inhibits bone formation elicited by BMP4. Thus, VEGF plays an important role in bone formation elicited by BMP4, and it can significantly enhance BMP4-elicited bone formation and regeneration through multiple mechanisms. This study has important implications for the formulation of new strategies to improve bone healing through increasing mesenchymal stem cell recruitment and survival, in combination with muscle-derived stem cell-based gene therapy.
机译:我们研究了血管生成和成骨因子在骨形成和骨愈合中的相互作用,使用经过基因工程改造以表达人骨形态发生蛋白-4 (BMP4)、VEGF 或 VEGF 特异性拮抗剂(可溶性 Flt1)的肌肉来源干细胞进行离体基因治疗。我们的结果表明,虽然单独使用VEGF并不能改善骨再生,但它与BMP4协同作用,增加间充质干细胞的募集,提高细胞存活率,并在软骨内骨形成的早期阶段增加软骨形成。这些早期效果,加上软骨吸收加速,最终导致骨形成和骨愈合的显着增强。VEGF对BMP4引起的骨愈合的有益作用主要取决于VEGF与BMP4的比例,比例不当会导致对骨愈合的不利影响。最后,我们发现可溶性 Flt1 抑制 BMP4 诱导的骨形成。因此,VEGF在BMP4诱导的骨形成中起重要作用,并且可以通过多种机制显著增强BMP4诱导的骨形成和再生。本研究对制定新策略具有重要意义,通过增加间充质干细胞募集和存活,结合基于肌肉的干细胞基因治疗来改善骨愈合。

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