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用肝素对多孔α-磷酸三钙颗粒进行表面改性,增强了其在大鼠颅骨缺损模型中的早期成骨能力。

Surface modification of porous alpha-tricalcium phosphate granules with heparin enhanced their early osteogenic capability in a rat calvarial defect model.

作者信息

Takeda Yoshihiro, Honda Yoshitomo, Kakinoki Sachiro, Yamaoka Tetsuji, Baba Shunsuke

机构信息

Department of Oral Implantology, Osaka Dental University.

Institute of Dental Research, Osaka Dental University.

出版信息

Dent Mater J. 2018 Jul 29;37(4):575-581. doi: 10.4012/dmj.2017-305. Epub 2018 Mar 27.

Abstract

Heparin binds to and modulates various growth factors, potentially augmenting the bone-forming capability of biomaterials. Here, α-tricalcium phosphate (α-TCP) granules were modified with peptide containing the marine mussel-derived adhesive sequence, which reacts with α-TCP surface, and cationic sequence, which binds to heparin (α-Ph). α-Ph retained the α-TCP phase and intergranule spaces after the surface modification. The existence of heparin on α-Ph granules was confirmed using X-ray photoelectron spectroscopy. Granules of α-TCP and α-Ph were implanted into critical-size defects in rat calvaria for 4 weeks. Micro-computed tomography, histological evaluation, and Alcian blue staining revealed that α-Ph induced superior bone formation compared with α-TCP. Newly formed bone on α-Ph was preferentially in contact with the Alcian blue-stained surfaces of granules. These results suggested that heparinization enhanced the early osteogenic capacity of α-TCP, possibly by modulating the secretion of Alcian blue-stained extracellular matrixes.

摘要

肝素与多种生长因子结合并对其进行调节,可能会增强生物材料的骨形成能力。在此,用含有海洋贻贝来源的粘附序列(可与α - 磷酸三钙(α-TCP)表面反应)和阳离子序列(可与肝素结合)的肽对α-TCP颗粒进行修饰(α-Ph)。表面修饰后,α-Ph保留了α-TCP相和颗粒间空间。使用X射线光电子能谱证实了α-Ph颗粒上存在肝素。将α-TCP和α-Ph颗粒植入大鼠颅骨的临界尺寸缺损处4周。微计算机断层扫描、组织学评估和阿尔新蓝染色显示,与α-TCP相比,α-Ph诱导了更好的骨形成。α-Ph上新形成的骨优先与颗粒的阿尔新蓝染色表面接触。这些结果表明,肝素化可能通过调节阿尔新蓝染色的细胞外基质的分泌来增强α-TCP的早期成骨能力。

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