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首页> 外文期刊>Biomaterials >The ability of a collagen/calcium phosphate scaffold to act as its own vector for gene delivery and to promote bone formation via transfection with VEGF(165).
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The ability of a collagen/calcium phosphate scaffold to act as its own vector for gene delivery and to promote bone formation via transfection with VEGF(165).

机译:胶原蛋白/磷酸钙支架作为自身载体进行基因传递并通过VEGF转染促进骨形成的能力(165)。

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摘要

Collagen/calcium phosphate scaffolds have been used for bone reconstruction due to their inherent similarities to the bone extracellular matrix. Calcium phosphate alone has also been used as a non-viral vector for gene delivery. The aim of this study was to determine the capability of a collagen/calcium phosphate scaffold to deliver naked plasmid DNA and mediate transfection in vivo. The second goal of the study was to deliver a plasmid encoding vascular endothelial growth factor(165) (pVEGF(165)) to promote angiogenesis, and hence bone formation, in a mouse intra-femoral model. The delivery of naked plasmid DNA resulted in a 7.6-fold increase in mRNA levels of beta-Galactosidase compared to the delivery of plasmid DNA complexed with a partially degraded PAMAM dendrimer (dPAMAM) in a subcutaneous murine model. When implanted in a muirne intra-femoral model, the delivery of pVEGF(165) resulted in a 2-fold increase in bone volume at the defect site relative to control scaffolds without pVEGF(165). It was concluded that a collagen/calcium phosphate scaffold can mediate transfection without the use of additional transfection vectors and can promote bone formation in a mouse model via the delivery of pVEGF(165).
机译:由于胶原/磷酸钙支架与骨细胞外基质的内在相似性,它们已被用于骨重建。单独的磷酸钙也已经用作基因递送的非病毒载体。这项研究的目的是确定胶原蛋白/磷酸钙支架传递裸质粒DNA并介导体内转染的能力。该研究的第二个目标是在小鼠股骨内模型中提供编码血管内皮生长因子(165)(pVEGF(165))的质粒,以促进血管生成,从而促进骨形成。与在皮下鼠模型中与部分降解的PAMAM树状大分子(dPAMAM)复合的质粒DNA的递送相比,裸质粒DNA的递送导致β-半乳糖苷酶的mRNA水平增加7.6倍。当植入muirne股内模型中时,相对于没有pVEGF(165)的对照支架,pVEGF(165)的递送导致缺损部位骨体积增加2倍。结论是,胶原蛋白/磷酸钙支架可以在不使用其他转染载体的情况下介导转染,并且可以通过递送pVEGF促进小鼠模型中的骨形成(165)。

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