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使用动静脉袢对多孔基质进行轴向预血管化可促进移植的自体成骨细胞的存活和分化。

Axial prevascularization of porous matrices using an arteriovenous loop promotes survival and differentiation of transplanted autologous osteoblasts.

作者信息

Arkudas Andreas, Beier Justus P, Heidner Kristina, Tjiawi Jimmy, Polykandriotis Elias, Srour Safwan, Sturzl Michael, Horch Raymund E, Kneser Ulrich

机构信息

Department of Plastic and Hand Surgery, University of Erlangen Medical Center, Erlangen, Germany.

出版信息

Tissue Eng. 2007 Jul;13(7):1549-60. doi: 10.1089/ten.2006.0387.

Abstract

Generation of axially vascularized bioartificial bone might be performed using matrix neovascularization in connection with osteoblast injection. We sought to evaluate whether prevascularization of porous hard matrices using an arteriovenous (AV) loop promotes survival of transplanted osteoblasts. A processed bovine cancellous bone matrix was inserted into the AV loop. Six weeks later, 5 x 10(6) carboxyfluorescein diacetate-stained osteoblasts were injected into the matrix (group A, n = 34). Osteoblast-seeded matrices without prevascularization were implanted subcutaneously as controls (group B, n = 32). Specimens were subjected to histologic, morphometric, and molecular-biological analysis after 1, 4, 8, and 16 weeks. Upon cell injection, matrices were completely vascularized. An intense foreign body reaction was observed in matrices from both groups. Group A was significantly superior to group B in terms of osteoblast survival at any time point. Expression of bone-specific genes was detected in the AV loop group but not in the subcutaneous control. Bone formation was only detectable in 1 long-term animal of group A. This study demonstrates for the first time that axial prevascularization increases the survival of implanted osteoblasts in porous matrices. Matrices with optimized biocompatibility might eventually facilitate generation of axially vascularized bone tissue after injection of osteogenic cells in the AV loop model.

摘要

利用基质新生血管形成结合成骨细胞注射可能生成轴向血管化的生物人工骨。我们试图评估使用动静脉(AV)环对多孔硬基质进行预血管化是否能促进移植成骨细胞的存活。将经过处理的牛松质骨基质插入AV环中。六周后,将5×10⁶羧基荧光素二乙酸酯染色的成骨细胞注入该基质中(A组,n = 34)。未进行预血管化的接种有成骨细胞的基质作为对照皮下植入(B组,n = 32)。在1、4、8和16周后对标本进行组织学、形态计量学和分子生物学分析。细胞注射后,基质完全血管化。在两组的基质中均观察到强烈的异物反应。在任何时间点,A组在成骨细胞存活方面均显著优于B组。在AV环组中检测到骨特异性基因的表达,而皮下对照组未检测到。仅在A组的1只长期动物中检测到骨形成。本研究首次证明轴向预血管化可提高植入多孔基质中成骨细胞的存活率。具有优化生物相容性的基质最终可能有助于在AV环模型中注射成骨细胞后生成轴向血管化的骨组织。

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