带血管的同源骨移植和骨髓有核细胞移植在修复临界大小骨缺损中促进血管生成的动物研究

M. Cavallo, M. Maglio, A. Parrilli, L. Martini, E. Guerra, S. Pagani, M. Fini, R. Rotini
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引用次数: 0

摘要

自体骨移植是临床修复骨缺损的标准方法,已取得良好的效果。自体带血管的骨移植是目前首选的方法,因为它具有较高的成骨潜能和抗重吸收能力。该方法的缺点包括供体部位有限,临床处理困难,失败率超过10%。同种异体移植物常用于大量骨丢失,但由于移植物植入后只有边缘部分新血管化,因此经常报道不愈合的骨折,并伴有移植物重吸收。为了克服这些问题,文献中的一些研究试图将骨移植与血管供应结合起来,并取得了令人鼓舞的结果。另一方面,文献中的一些研究报道了骨髓来源的细胞促进新血管形成的能力。事实上,骨髓不仅含有造血干细胞(hsc)和间充质干细胞作为再生组织的来源,还含有辅助细胞,通过产生多种生长因子来支持血管生成和血管生成。在这种情况下,我们开发了一种新的手术方法,包括在兔桡骨的一个临界大小的缺陷上进行异体骨移植,加上在正中动脉和静脉内部的偏差,并在胶原蛋白支架上补充自体骨髓浓缩物。24只新西兰公白兔(2500 ~ 3000 g)分为2组,每组12只。手术如下:组1(#12):同种异体骨移植(左桡骨)/同种异体骨移植+血管蒂+自体骨髓浓缩物(右桡骨);组2(#12):假手术(左桡骨)/同种异体骨移植+血管蒂(右桡骨)每组3个实验时间:8,4和2周(每次4只动物)。用作移植物的骨是先前从一项不相关的研究中收集的。所有病例均对骨髓浓缩液进行体外评估,并在牺牲时通过免疫组化检测VEGF、CD31和CD146进行组织学和组织形态学评估,以突出血管和内皮细胞的存在。所有病例均行显微ct分析及定量骨评价。骨髓浓缩物显示出分化成成骨、软骨和巨噬细胞谱系的显著能力。无感染或手术不耐受等并发症报告。在补充血管和骨髓浓缩物的组中,骨移植物仅表现出部分整合,主要集中在四肢,剩余骨良好健康。免疫组化显示同一组中VEGF表达升高。微CT分析显示,血管补充组的重塑活动更高,四肢整合面积随着牺牲时间的延长而增加。本研究提示,补充血管细胞和骨髓细胞对同种骨移植的新生血管生成和新生血管形成有积极的影响。需要更长时间的随访和手术技术的改进来验证手术的有效性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
VASCULARISED HOMOLOGOUS BONE GRAFT AND BONE MARROW NUCLEATED CELLS TRANSPLANTATION TO ENHANCE ANGIOGENESIS IN THE REPAIR OF CRITICAL SIZE BONE DEFECT: AN ANIMAL STUDY
Autologous bone grafting is a standard procedure for the clinical repair of skeletal defects, and good results have been obtained. Autologous vascularized bone grafting is currently the procedure of choice because of high osteogenic potential and resistance against reabsorption. Disadvantages of this procedure include limited availability of donor sites, clinical difficulty in handling, and a failure rate exceeding 10%. Allografts are often used for massive bone loss, but since only the marginal portion is newly vascularized after the implantation non healing fractures are often reported, along with a graft reabsorption. To overcome these problems, some studies in literature tried to conjugate bone graft and vascular supply, with encouraging results. On the other side, several studies in literature reported the ability of bone marrow derived cells to promote neo-vascularization. In fact, bone marrow contains not only hematopoietic stem cells (HSCs) and MSCs as a source for regenerating tissues but also accessory cells that support angiogenesis and vasculogenesis by producing several growth factors. In this scenario a new procedure was developed, consisting in an allogenic bone graft transplantation in a critical size defect in rabbit radius, plus a deviation at its inside of the median artery and vein with a supplement of autologous bone marrow concentrate on a collagen scaffold. Twenty-four New Zealand male white rabbits (2500–3000 g) were divided into 2 groups, each consisting of 12 animals. Surgeries were performed as follow: −Group 1 (#12): allogenic bone graft (left radius) / allogenic bone graft + vascular pedicle + autologous bone marrow concentrate (right radius) −Group 2 (#12): sham operated (left radius)/ allogenic bone graft + vascular pedicle (right radius) For each group, 3 experimental time: 8, 4 and 2 weeks (4 animals for each time). The bone used as graft was previously collected from an uncorrelated study. An in vitro evaluation of bone marrow concentrate was performed in all cases, and at the time of sacrifice histological and histomorphometrical assessment were performed with immunohistochemical assays for VEGF, CD31 e CD146 to highlight the presence of vessels and endothelial cells. Micro-CT Analysis with quantitative bone evaluation was performed in all cases. The bone marrow concentrate showed a marked capability to differentiate into osteogenic, chondrogenic and agipogenic lineages. No complications such as infection or intolerance to the procedure were reported. The bone grafts showed only a partial integration, mainly at the extremities in the group with vascular and bone marrow concentrate supplement, with a good and healthy residual bone. immunohistochemistry showed an interesting higher VEGF expression in the same group. Micro CT analysis showed a higher remodeling activities in the groups treated with vascular supplement, with an area of integration at the extremities increasing with the extension of the sacrifice time. The present study suggests that the vascular and marrow cells supplement may positively influence the neoangiogenesis and the neovascularization of the homologous bone graft. A longer time of follow up and improvement of the surgical technique are required to validate the procedure.
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