Retroviral-Based BMP-4 In Vivo Gene Transfer Strategy with Intramedullary Viral Delivery Optimizes Transgene Expression in Rat Femur Fractures

The open tissue engineering and regenerative medicine journal Pub Date : 2008-11-05 DOI:10.2174/1875043500801010014

C. Rundle, Shin-Tai Chen, Ryan Porte, J. Wergedal, K. Lau

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引用次数: 2

Abstract

We have developed an intramedullary delivery strategy to administer retroviral vectors expressing a therapeutic gene to promote healing of a closed rat femur fracture. This strategy involves implantation of an indwelling catheter with the stabilizing Kirschner (K)-wire during the surgery prior to fracture of the femur by the three-point bending technique. It uses the openings in the bone that were already created for the stabilizing K-wire and the catheter insertion. In this study, transgene expression and callus bone formation induced by intramedullary delivery of MLV-based vectors expressing the bone morphogenetic protein-2/4 (BMP-2/4) hybrid gene or ￻-galactosidase (￻-gal) gene were compared with those pro- duced by percutaneous injections of the same vectors at the periosteum of the fracture site. The percutaneous injections of MLV-BMP-2/4 vector led to massive but asymmetric transgene expression in surrounding tissues within the fracture cal- lus and large amounts of supraperiosteal as well as asymmetric callus bone formation. In contrast, the intramedullary ad- ministration produced a robust and symmetric pattern of transgene expression at the fracture site with very minimal trans- duction at cells of surrounding tissues, resulting in normal subperiosteal bone development around the entire fracture cal- lus without supraperiosteal bone formation. In summary, we have developed an intramedullary retroviral vector delivery strategy with a rat femur fracture model that led to uniform transgene expression around the entire fracture site, which op- timizes the gene therapy-enhanced fracture repair. This strategy should readily be adapted to administer large dosages of any therapeutic vehicle (therapeutic molecules, peptides, or proteins, as well as viral or non-viral vectors) throughout much of early fracture repair, and thus it would be an ideal rat model for in vivo testing of various therapeutic agents to promote fracture repair.

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基于逆转录病毒的BMP-4体内基因转移策略与髓内病毒传递优化大鼠股骨骨折中的转基因表达

我们已经开发了一种髓内递送策略来管理表达治疗性基因的逆转录病毒载体，以促进闭合性大鼠股骨骨折的愈合。该策略包括在股骨骨折前通过三点弯曲技术在手术期间植入带有稳定克氏针(K)的留置导管。它利用骨头上已经形成的开口来稳定k针和导管的插入。本研究将表达骨形态发生蛋白-2/4 (BMP-2/4)杂交基因或￻-半乳糖苷酶(￻-gal)基因的基于mlv的载体髓内递送诱导的转基因表达和骨痂形成与在骨折部位骨膜经皮注射相同载体诱导的骨痂形成进行比较。经皮注射MLV-BMP-2/4载体可导致骨折骨痂周围组织大量但不对称的转基因表达和大量骨上骨痂形成。相比之下，髓内注射在骨折部位产生了稳健且对称的转基因表达模式，周围组织细胞的转导非常少，导致整个骨折骨周围正常的骨膜下骨发育，没有骨上骨形成。总之，我们在大鼠股骨骨折模型中开发了一种髓内逆转录病毒载体递送策略，该策略可以在整个骨折部位周围均匀表达转基因，从而优化基因治疗增强的骨折修复。在骨折早期修复过程中，这种策略可以很容易地适用于大剂量的任何治疗载体(治疗分子、多肽或蛋白质，以及病毒或非病毒载体)，因此它将是一种理想的大鼠模型，用于体内测试各种治疗药物以促进骨折修复。

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The open tissue engineering and regenerative medicine journal

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