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本文引用的文献

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Direct gene therapy for bone regeneration: gene delivery, animal models, and outcome measures.直接基因治疗骨再生:基因传递、动物模型和结果测量。
Tissue Eng Part B Rev. 2010 Feb;16(1):13-20. doi: 10.1089/ten.teb.2009.0156.
2
muCT-based measurement of cortical bone graft-to-host union.基于微计算机断层扫描(muCT)的皮质骨移植与宿主骨愈合情况测量
J Bone Miner Res. 2009 May;24(5):899-907. doi: 10.1359/jbmr.081232.
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Adverse events associated with anterior cervical spine surgery.与颈椎前路手术相关的不良事件。
J Am Acad Orthop Surg. 2008 Dec;16(12):729-38. doi: 10.5435/00124635-200812000-00005.
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Recent developments in the biology of fracture repair.骨折修复生物学的最新进展。
J Am Acad Orthop Surg. 2008 Nov;16(11):619-25. doi: 10.5435/00124635-200811000-00001.
5
Musculoskeletal allograft risks and recalls in the United States.美国肌肉骨骼同种异体移植的风险与召回情况。
J Am Acad Orthop Surg. 2008 Oct;16(10):559-65. doi: 10.5435/00124635-200810000-00001.
6
Self-complementary AAV vectors; advances and applications.自互补腺相关病毒载体:进展与应用
Mol Ther. 2008 Oct;16(10):1648-56. doi: 10.1038/mt.2008.171. Epub 2008 Aug 5.
7
The effect of surface demineralization of cortical bone allograft on the properties of recombinant adeno-associated virus coatings.皮质骨同种异体移植物表面脱矿质对重组腺相关病毒涂层性能的影响。
Biomaterials. 2008 Oct;29(28):3882-7. doi: 10.1016/j.biomaterials.2008.06.007. Epub 2008 Jun 30.
8
Chordin knockdown enhances the osteogenic differentiation of human mesenchymal stem cells.脊索蛋白敲低增强人间充质干细胞的成骨分化。
Arthritis Res Ther. 2008;10(3):R65. doi: 10.1186/ar2436. Epub 2008 Jun 4.
9
Runx2-mediated activation of the Bax gene increases osteosarcoma cell sensitivity to apoptosis.Runx2介导的Bax基因激活增加骨肉瘤细胞对凋亡的敏感性。
Oncogene. 2008 Jun 5;27(25):3605-14. doi: 10.1038/sj.onc.1211020. Epub 2008 Jan 28.
10
Freeze-dried tendon allografts as tissue-engineering scaffolds for Gdf5 gene delivery.冻干同种异体肌腱作为用于Gdf5基因递送的组织工程支架。
Mol Ther. 2008 Mar;16(3):466-73. doi: 10.1038/sj.mt.6300395. Epub 2008 Jan 8.

自互补 AAV2.5-BMP2 涂层同种异体股骨移植物介导的骨愈合优于具有与未骨折股骨相当生物力学的活自体移植物的小鼠。

Self-complementary AAV2.5-BMP2-coated femoral allografts mediated superior bone healing versus live autografts in mice with equivalent biomechanics to unfractured femur.

机构信息

The Center for Musculoskeletal Research, University of Rochester, Rochester, New York, USA.

出版信息

Mol Ther. 2011 Aug;19(8):1416-25. doi: 10.1038/mt.2010.294. Epub 2011 Jan 4.

DOI:10.1038/mt.2010.294
PMID:21206485
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3149158/
Abstract

Structural allografts used for critical bone defects have limited osteogenic properties for biointegration. Although ex vivo tissue-engineered constructs expressing bone morphogenetic protein-2 (BMP2) have demonstrated efficacy in critical defect models, similar success has not been achieved with off-the-shelf acellular approaches, including allografts coated with freeze-dried single-stranded adeno-associated virus (ssAAV-BMP2). To see whether the self-complementary AAV serotype 2.5 vector (scAAV2.5-BMP2) could overcome this, we performed side-by-side comparisons in vitro and in the murine femoral allograft model. Although ssAAV-BMP2 was unable to induce BMP2 expression and differentiation of C3H10T1/2 cells in culture, scAAV2.5-BMP2 transduction led to dose-dependent BMP2 expression and alkaline phosphatase activity, and displayed a 25-fold increased transduction efficiency in vivo. After 6 weeks, the ssAAV-BMP2 coating failed to demonstrate any significant effects. However, all allografts coated with 10(10) scAAV2.5-BMP2 formed a new cortical shell that was indistinguishable to that formed by live autografts. Additionally, coated allografts experienced reduced resorption resulting in a threefold increase in graft bone volume versus autograft. This led to biomechanical superiority versus both allografts and autografts, and equivalent torsional rigidity to unfractured femur. Collectively, these results demonstrate that scAAV2.5-BMP2 coating overcomes the major limitations of structural allografts, which can be used to heal critical defects of any size.

摘要

用于治疗临界骨缺损的结构性同种异体移植物的成骨性能有限,不利于生物整合。尽管表达骨形态发生蛋白-2(BMP2)的体外组织工程构建体在临界缺损模型中显示出了疗效,但现成的无细胞方法(包括用冻干单链腺相关病毒(ssAAV-BMP2)包被的同种异体移植物)并未取得类似的成功。为了观察自我互补的 AAV 血清型 2.5 载体(scAAV2.5-BMP2)是否能够克服这一问题,我们在体外和小鼠股骨同种异体移植模型中进行了并列比较。尽管 ssAAV-BMP2 不能诱导 C3H10T1/2 细胞在培养中的 BMP2 表达和分化,但 scAAV2.5-BMP2 转导导致 BMP2 表达和碱性磷酸酶活性呈剂量依赖性,并在体内显示出 25 倍的转导效率增加。6 周后,ssAAV-BMP2 涂层未能显示出任何显著效果。然而,所有用 10(10)scAAV2.5-BMP2 包被的同种异体移植物都形成了新的皮质壳,与活自体移植物形成的皮质壳无法区分。此外,包被的同种异体移植物经历了减少的吸收,导致移植物骨体积增加了三倍,而自体移植物的吸收则增加了三倍。这导致了与同种异体移植物和自体移植物相比的生物力学优势,以及与未骨折股骨相当的扭转刚度。总之,这些结果表明,scAAV2.5-BMP2 涂层克服了结构性同种异体移植物的主要局限性,可用于治疗任何大小的临界缺损。