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聚富马酸丙二醇酯/β-磷酸三钙可注射复合支架的体内降解

In vivo degradation of a poly(propylene fumarate)/beta-tricalcium phosphate injectable composite scaffold.

作者信息

Peter S J, Miller S T, Zhu G, Yasko A W, Mikos A G

机构信息

Institute of Biosciences and Bioengineering and Department of Chemical Engineering, Rice University, Houston, Texas 77005-1892, USA.

出版信息

J Biomed Mater Res. 1998 Jul;41(1):1-7. doi: 10.1002/(sici)1097-4636(199807)41:1<1::aid-jbm1>3.0.co;2-n.

Abstract

This study was designed to investigate the in vivo biodegration and biocompatibility of a poly(propylene fumarate) (PPF)-based orthopedic biomaterial. The effects of varying the PPF to N-vinyl pyrrolidinone ratio and PPF to beta-tricalcium phosphate content were studied. The composite mechanical properties and local tissue interactions were analyzed over 12 weeks. An initial increase in both compressive modulus and strength was seen for composite formulations that incorporated beta-tricalcium phosphate. The samples incorporating a higher PPF to N-vinyl pyrrolidinone ratio reached a maximal compressive strength of 7.7 MPa and a maximal compressive modulus of 191.4 MPa at 3 weeks. The lower PPF to N-vinyl pyrrolidinone ratio samples gained a maximum compressive strength of 7.5 MPa initially and a compressive modulus of 134.0 MPa at 1 week. At 6 weeks, all samples for formulations incorporating beta-tricalcium phosphate crumbled upon removal and were not mechanically tested. Samples that did not incorporate beta-tricalcium phosphate were very weak and insufficient for bone replacement at the 4-day time point and beyond. Tissue interactions resulted in a mild inflammatory response at the initial time points and mature fibrous encapsulation by 12 weeks.

摘要

本研究旨在调查基于聚富马酸丙二醇酯(PPF)的骨科生物材料的体内生物降解性和生物相容性。研究了改变PPF与N-乙烯基吡咯烷酮比例以及PPF与β-磷酸三钙含量的影响。在12周内分析了复合材料的力学性能和局部组织相互作用。对于掺入β-磷酸三钙的复合配方,观察到压缩模量和强度最初均有所增加。PPF与N-乙烯基吡咯烷酮比例较高的样品在3周时达到最大抗压强度7.7MPa和最大压缩模量191.4MPa。PPF与N-乙烯基吡咯烷酮比例较低的样品最初获得最大抗压强度7.5MPa,在1周时获得压缩模量134.0MPa。在6周时,所有掺入β-磷酸三钙的配方样品在取出时破碎,未进行力学测试。未掺入β-磷酸三钙的样品在4天及以后非常脆弱,不足以用于骨替代。组织相互作用在初始时间点导致轻度炎症反应,到12周时形成成熟的纤维包裹。

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