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用于体内血管化骨再生的含成骨细胞和血管生成细胞的氧张力控制基质

Oxygen Tension-Controlled Matrices with Osteogenic and Vasculogenic Cells for Vascularized Bone Regeneration In Vivo.

作者信息

Amini Ami R, Xu Thomas O, Chidambaram Ramaswamy M, Nukavarapu Syam P

机构信息

1 Oral and Maxillofacial Surgery, Massachusetts General Hospital , Boston, Massachusetts.

2 Institute for Regenerative Engineering, University of Connecticut Health Center , Farmington, Connecticut.

出版信息

Tissue Eng Part A. 2016 Apr;22(7-8):610-20. doi: 10.1089/ten.TEA.2015.0310. Epub 2016 Mar 22.

Abstract

Despite recent progress, segmental bone defect repair is still a significant challenge in orthopedic surgery. While bone tissue engineering approaches using biodegradable matrices along with bone/blood vessel forming cells offered improved possibilities, current regenerative strategies lack the ability to achieve vascularized bone regeneration in critical-sized/segmental bone defects. In this study, we introduced and evaluated a two-pronged approach for vascularized bone regeneration in vivo. The goal was to demonstrate vascularized bone formation using oxygen tension-controlled (OTC) matrices seeded with bone and blood vessel forming cells. OTC matrices were coimplanted with rabbit mesenchymal stem cells (MSCs) and peripheral blood-derived endothelial progenitor cells (PB-EPCs) to demonstrate the osteogenic and vasculogenic differentiation of these cells, postseeding on a matrix, especially deep inside the matrix pore structure. Matrices coimplanted with varied rabbit MSC and PB-EPC ratios (1:4, 1:1, and 4:1) were assessed in a nude mouse subcutaneous implantation model to determine a coimplantation ratio with superior osteogenic as well as vasculogenic properties. The implants were analyzed, at week 8, for endothelial (CD31 and Von Willebrand factor [vWF]) and osteogenic marker (RunX2 and Col I) staining qualitatively and collagen deposition and number of vessel formation quantitatively. Results from these experiments established MSC-to-PB-EPC ratio 1:1 as the best coimplantation ratio. OTC matrix with 1:1 coimplantation ratio was assessed for segmental bone defect repair in a rabbit critical-sized bone defect model. The group under investigation was OTC matrix, and the matrix was seeded with MSCs, EPCs, or MSCs:EPCs in a 1:1 ratio. Explants at week 12 were evaluated for bone defect repair via micro-CT and histology. Results from rabbit in vivo experiments show enhanced mineralization and vascularization for the 1:1 coimplantation group. Overall, the study establishes a two-pronged approach involving OTC matrix and effective progenitors for large-area and vascularized bone regeneration.

摘要

尽管近年来取得了进展,但节段性骨缺损修复仍是骨科手术中的一项重大挑战。虽然使用可生物降解基质以及骨/血管形成细胞的骨组织工程方法提供了更好的可能性,但目前的再生策略仍缺乏在临界尺寸/节段性骨缺损中实现血管化骨再生的能力。在本研究中,我们引入并评估了一种用于体内血管化骨再生的双管齐下方法。目标是使用接种了骨和血管形成细胞的氧张力控制(OTC)基质来证明血管化骨的形成。将OTC基质与兔间充质干细胞(MSC)和外周血来源的内皮祖细胞(PB-EPC)共同植入,以证明这些细胞在接种到基质上后,尤其是在基质孔结构深处的成骨和血管生成分化。在裸鼠皮下植入模型中评估与不同兔MSC和PB-EPC比例(1:4、1:1和4:1)共同植入的基质,以确定具有优异成骨和血管生成特性的共同植入比例。在第8周对植入物进行分析,定性检测内皮(CD31和血管性血友病因子[vWF])和成骨标记物(RunX2和I型胶原[Col I])染色,并定量检测胶原沉积和血管形成数量。这些实验结果确定MSC与PB-EPC比例为1:1是最佳共同植入比例。在兔临界尺寸骨缺损模型中评估共同植入比例为1:1的OTC基质用于节段性骨缺损修复。研究组为OTC基质,该基质接种了MSC、EPC或比例为1:1的MSC:EPC。在第12周通过微型计算机断层扫描(micro-CT)和组织学评估植入物的骨缺损修复情况。兔体内实验结果显示,1:1共同植入组的矿化和血管化增强。总体而言,该研究建立了一种涉及OTC基质和有效祖细胞的双管齐下方法,用于大面积和血管化骨再生。

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