Lattanzi W, Parrilla C, Fetoni A, Logroscino G, Straface G, Pecorini G, Stigliano E, Tampieri A, Bedini R, Pecci R, Michetti F, Gambotto A, Robbins P D, Pola E
Department of Anatomy and Cell Biology, Università Cattolica del Sacro Cuore School of Medicine, Rome, Italy.
Gene Ther. 2008 Oct;15(19):1330-43. doi: 10.1038/gt.2008.116. Epub 2008 Jul 17.
Local gene transfer of the human Lim mineralization protein (LMP), a novel intracellular positive regulator of the osteoblast differentiation program, can induce efficient bone formation in rodents. To develop a clinically relevant gene therapy approach to facilitate bone healing, we have used primary dermal fibroblasts transduced ex vivo with Ad.LMP-3 and seeded on a hydroxyapatite/collagen matrix prior to autologous implantation. Here, we demonstrate that genetically modified autologous dermal fibroblasts expressing Ad.LMP-3 are able to induce ectopic bone formation following implantation of the matrix into mouse triceps and paravertebral muscles. Moreover, implantation of the Ad.LMP-3-modified dermal fibroblasts into a rat mandibular bone critical size defect model results in efficient healing, as determined by X-rays, histology and three-dimensional microcomputed tomography (3DmuCT). These results demonstrate the effectiveness of the non-secreted intracellular osteogenic factor LMP-3 in inducing bone formation in vivo. Moreover, the utilization of autologous dermal fibroblasts implanted on a biomaterial represents a promising approach for possible future clinical applications aimed at inducing new bone formation.
人Lim矿化蛋白(LMP)是成骨细胞分化程序中一种新型的细胞内正向调节因子,其局部基因转移可在啮齿动物中诱导高效的骨形成。为了开发一种与临床相关的促进骨愈合的基因治疗方法,我们使用经Ad.LMP - 3体外转导的原代真皮成纤维细胞,并在自体植入前接种到羟基磷灰石/胶原基质上。在此,我们证明,将表达Ad.LMP - 3的基因修饰自体真皮成纤维细胞植入基质到小鼠三头肌和椎旁肌后,能够诱导异位骨形成。此外,通过X射线、组织学和三维微计算机断层扫描(3DmuCT)确定,将经Ad.LMP - 3修饰的真皮成纤维细胞植入大鼠下颌骨临界尺寸缺损模型中可实现高效愈合。这些结果证明了非分泌型细胞内成骨因子LMP - 3在体内诱导骨形成的有效性。此外,利用植入生物材料上的自体真皮成纤维细胞代表了一种有前景的方法,有望用于未来旨在诱导新骨形成的临床应用。
