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基于细胞的血管内皮生长因子基因治疗对节段性骨缺损愈合的影响。

Effect of cell-based VEGF gene therapy on healing of a segmental bone defect.

作者信息

Li Ru, Stewart Duncan J, von Schroeder Herbert P, Mackinnon Erin S, Schemitsch Emil H

机构信息

St. Michael's Hospital, University of Toronto, Ontario, Canada.

出版信息

J Orthop Res. 2009 Jan;27(1):8-14. doi: 10.1002/jor.20658.

DOI:10.1002/jor.20658
PMID:18634016
Abstract

Fracture healing requires coordinated coupling between osteogenesis and angiogenesis in which vascular endothelial growth factor (VEGF) plays a key role. We hypothesized that targeted over-expression of angiogenic and osteogenic factors within the fracture would promote bone healing by inducing development of new blood vessels and stimulating/affecting proliferation, survival, and activity of skeletal cells. Using a cell-based method of gene transfer, without viral vector, 5.0 x 10(6) fibroblasts transfected with VEGF were delivered to a 10-mm bone defect in rabbit tibiae (Group 1) (n = 9); control groups were treated with fibroblasts (Group 2) (n = 7), or saline (Group 3) (n = 7) only. After 12 weeks, eight tibial fractures healed in Group 1, compared to four each in Groups 2 and 3. In Group 1, ossification was seen across the entire defect; in Groups 2 and 3, the defects were fibrous and sparsely ossified. Group 1 had more positively stained (CD31) vessels than Groups 2 and 3. MicroCT 3-D showed complete bridging of the new bone for Group 1, but incomplete healing for Groups 2 and 3. MicroCT bone structural parameters showed significant differences between VEGF treatment and control groups (p < 0.05). These results indicate that the cell-based VEGF gene therapy has significant angiogenic and osteogenic effects to enhance healing of a segmental defect in the long bone of rabbits.

摘要

骨折愈合需要成骨作用与血管生成之间的协调配合,其中血管内皮生长因子(VEGF)起着关键作用。我们假设,在骨折部位靶向过表达血管生成和成骨因子,通过诱导新血管生成以及刺激/影响骨骼细胞的增殖、存活和活性,将促进骨愈合。采用无病毒载体的基于细胞的基因转移方法,将5.0×10⁶个转染了VEGF的成纤维细胞植入兔胫骨10毫米的骨缺损处(第1组)(n = 9);对照组分别用成纤维细胞处理(第2组)(n = 7)或仅用生理盐水处理(第3组)(n = 7)。12周后,第1组的8处胫骨骨折愈合,而第2组和第3组各有4处愈合。在第1组中,整个缺损处均可见骨化;在第2组和第3组中,缺损处为纤维性且骨化稀疏。第1组中阳性染色(CD31)的血管比第2组和第3组更多。MicroCT三维成像显示第1组新骨完全桥接,但第2组和第3组愈合不完全。MicroCT骨结构参数显示VEGF治疗组与对照组之间存在显著差异(p < 0.05)。这些结果表明,基于细胞的VEGF基因治疗对增强兔长骨节段性缺损的愈合具有显著的血管生成和成骨作用。

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