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使用聚己内酯支架在流动条件下对用于血管内应用的原代人成骨细胞培养物进行钙化。

Calcification of primary human osteoblast cultures under flow conditions using polycaprolactone scaffolds for intravascular applications.

作者信息

Zhu Beili, Bailey Steven R, Agrawal C Mauli

机构信息

Department of Biomedical Engineering, College of Engineering, University of Texas at San Antonio, TX, USA.

Janey Briscoe Center for Cardiovascular Research, Janey and Dolph Briscoe Division of Cardiology, Department of Medicine, University of Texas Health Science Center at San Antonio, TX, USA.

出版信息

J Tissue Eng Regen Med. 2012 Oct;6(9):687-95. doi: 10.1002/term.472. Epub 2011 Sep 20.

Abstract

Total atherosclerotic occlusion is a leading cause of death. Recent animal models of this disease are devoid of cell-mediated calcification and arteries are often not occluded gradually. This study is part of a project with the objective of developing a new model featuring the above two characteristics, using a tissue-engineering scaffold. The amount and distribution of calcium deposits in primary human osteoblast (HOB) cultures on polycaprolactone (PCL) scaffolds under flow conditions were investigated. HOBs were cultured on PCL scaffolds with TGF-β1 loadings of 0 (control), 5 and 50 ng. HOB-PCL constructs were cultured in spinner flasks. Under flow conditions, cell numbers present in HOB cultures on PCL scaffolds increased from day 7 to day 14, and most calcification was induced at day 21. TGF-β1 loadings of 5 and 50 ng did not show a significant difference in ALP activity, cell numbers and amount of calcium deposited in HOB cultures, but calcium staining showed that 50 ng TGF-β1 had higher calcium deposited on both days 21 and 28 under flow conditions compared with 5 ng of loading. Amount of calcium deposited by HOBs on day 28 showed a decrease from their levels on day 21. PCL degradation may be a factor contributing to this loss. The results indicate that cell-induced calcification can be achieved on PCL scaffolds under flow conditions. In conclusion, TGFβ1-HOB loaded PCL can be applied to create a model for total atherosclerotic occlusion with cell-deposited calcium in animal arteries.

摘要

完全动脉粥样硬化闭塞是主要的死亡原因。该疾病的近期动物模型缺乏细胞介导的钙化,且动脉通常不会逐渐闭塞。本研究是一个项目的一部分,该项目旨在利用组织工程支架开发一种具有上述两个特征的新模型。研究了在流动条件下原代人成骨细胞(HOB)在聚己内酯(PCL)支架上培养时钙沉积的量和分布。将HOB接种在TGF-β1负载量分别为0(对照)、5和50 ng的PCL支架上。HOB-PCL构建体在旋转瓶中培养。在流动条件下,PCL支架上HOB培养物中的细胞数量从第7天到第14天增加,并且在第21天诱导出最多的钙化。5和50 ng的TGF-β1负载量在HOB培养物中的碱性磷酸酶活性、细胞数量和钙沉积量方面没有显示出显著差异,但钙染色显示,在流动条件下,与5 ng负载量相比,50 ng TGF-β1在第21天和第28天均有更高的钙沉积。HOB在第28天沉积的钙量比第21天有所减少。PCL降解可能是导致这种损失的一个因素。结果表明,在流动条件下,PCL支架上可实现细胞诱导的钙化。总之,负载TGFβ1-HOB的PCL可用于创建动物动脉中细胞沉积钙的完全动脉粥样硬化闭塞模型。

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