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用于骨组织工程的负载多能成体祖细胞的脱矿骨基质

Multipotent adult progenitor cell-loaded demineralized bone matrix for bone tissue engineering.

作者信息

Supronowicz Peter, Gill Elise, Trujillo Angelica, Thula Taili, Zhukauskas Rasa, Perry Robert, Cobb Ronald R

机构信息

Biotechnology Development Department, RTI Biologics, Alachua, FL, USA.

Sports Medicine Group, RTI Biologics, Alachua, FL, USA.

出版信息

J Tissue Eng Regen Med. 2016 Apr;10(4):275-83. doi: 10.1002/term.1706. Epub 2013 Feb 15.

Abstract

Multipotent adult progenitor cells (MAPCs) from bone marrow have been shown to be capable of forming bone, cartilage and other connective tissues. In addition, MAPCs differentiate into lineages that are different from their germ layers of origin. Previous studies showed the ability of MAPCs to improve cardiac function and control allogenic-reactive responses associated with acute graft versus host disease. In the current study, we evaluated the ability of MAPCs to produce bone matrix on demineralized bone allograft substrates. Specifically, MAPCs expressed alkaline phosphatase, produced extracellular matrix proteins and deposited calcium-containing mineral on demineralized bone matrices. Furthermore, the addition of MAPCs on demineralized bone matrix (DBM) scaffolds enhanced osteoinductivity of the carrier in a rat ectopic pouch model. These results demonstrated the potential of MAPCs as a new approach for bone repair in tissue-engineering applications.

摘要

来自骨髓的多能成体祖细胞(MAPCs)已被证明能够形成骨、软骨和其他结缔组织。此外,MAPCs能分化成与其起源胚层不同的谱系。先前的研究表明,MAPCs具有改善心脏功能以及控制与急性移植物抗宿主病相关的同种异体反应的能力。在本研究中,我们评估了MAPCs在脱矿骨同种异体移植基质上产生骨基质的能力。具体而言,MAPCs表达碱性磷酸酶,产生细胞外基质蛋白,并在脱矿骨基质上沉积含钙矿物质。此外,在大鼠异位袋模型中,将MAPCs添加到脱矿骨基质(DBM)支架上可增强载体的骨诱导活性。这些结果证明了MAPCs作为组织工程应用中骨修复新方法的潜力。

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