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用于大鼠开窗缺损模型引导性骨再生的序贯控释双药负载支架

Sequential controlled-released dual-drug loaded scaffold for guided bone regeneration in a rat fenestration defect model.

作者信息

Guo Zhenzhao, Bo Dongying, He Ping, Li Hong, Wu Gang, Li Zhizhong, Zhou Changren, Li Qiyan

机构信息

Department of Materials Science and Engineering, Jinan University, Guangzhou, China.

出版信息

J Mater Chem B. 2017 Oct 7;5(37):7701-7710. doi: 10.1039/c7tb00909g. Epub 2017 Sep 12.

DOI:10.1039/c7tb00909g
PMID:32264371
Abstract

A microbially-induced inflammatory periodontal disease is the main initiator to disrupt the periodontium. It is desirable to develop a newly guided bone regeneration (GBR) scaffold to accomplish the periodontal tissue regeneration for the concurrent control of inflammation. A novel therapeutic solution for GBR based on 3D multifunctional scaffolds, which combines the merits of osseous regeneration and local anti-inflammatory drug delivery, has been developed. The 3D dual-drug delivery scaffold (DDDS) loaded with parthenolide and naringin was successfully developed by thermally-induced phase separation techniques. The DDDS was hierarchically interconnected to the porous PLLA scaffold loaded with the hydrophobic parthenolide. In addition, the hydrophilic naringin loaded in chitosan microspheres was embedded in the scaffold. In vitro drug release profile results revealed that the DDDS showed an efficient sequential controlled release pattern with parthenolide delivered rapidly, followed by naringin delivered in a more sustained manner. Cell viability of MC3T3-E1 showed a combined effect of dual-drug delivery. Hemolysis of the DDDS was 1.84 ± 0.44%, which is less than that of the pure PLLA scaffold. To further evaluate the in vivo guided bone regeneration effect of the DDDS, a rat fenestration defect model was generated. The defects were harvested after 4 and 8 weeks for micro-CT and histological observation. The results suggested that the DDDS group had significantly increased the regenerated bone volume fraction compared to both the control and PLLA groups at 8 weeks, which was in parallel with the reduced expression of IL-6. This DDDS, as a GBR scaffold, might be utilized as a novel adjunctive treatment in periodontitis.

摘要

微生物诱导的炎性牙周病是破坏牙周组织的主要诱因。开发一种新型引导骨再生(GBR)支架以实现牙周组织再生并同时控制炎症是很有必要的。基于三维多功能支架的一种新型GBR治疗方案已经开发出来,该方案结合了骨再生和局部抗炎药物递送的优点。通过热致相分离技术成功制备了负载小白菊内酯和柚皮苷的三维双药递送支架(DDDS)。DDDS与负载疏水性小白菊内酯的多孔聚乳酸(PLLA)支架呈分层互连。此外,负载在壳聚糖微球中的亲水性柚皮苷被嵌入支架中。体外药物释放曲线结果显示,DDDS呈现出有效的顺序控释模式,小白菊内酯快速释放,随后柚皮苷以更持续的方式释放。MC3T3-E1细胞的活力显示出双药递送的联合效应。DDDS的溶血率为1.84±0.44%,低于纯PLLA支架。为了进一步评估DDDS在体内的引导骨再生效果,建立了大鼠开窗缺损模型。在4周和8周后采集缺损部位进行显微CT和组织学观察。结果表明,在8周时,与对照组和PLLA组相比,DDDS组的再生骨体积分数显著增加,这与白细胞介素-6表达的降低相一致。这种DDDS作为一种GBR支架,可能被用作牙周炎的一种新型辅助治疗方法。

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