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通过微/介观分级多孔递送系统评估淫羊藿苷与骨形态发生蛋白2之间的协同成骨作用。

Evaluation of synergistic osteogenesis between icariin and BMP2 through a micro/meso hierarchical porous delivery system.

作者信息

Wang Qian, Cao Lingyan, Liu Yang, Zheng Ao, Wu Jiannan, Jiang Xinquan, Ji Ping

机构信息

Department of Oral and Maxillofacial Surgery, Stomatological Hospital of Chongqing Medical University.

Chongqing Key Laboratory of Oral Diseases and Biomedical Sciences.

出版信息

Int J Nanomedicine. 2017 Oct 19;12:7721-7735. doi: 10.2147/IJN.S141052. eCollection 2017.

Abstract

BMP2 is well known as an outstanding growth factor for inducing new bone formation. However, improvements are still required to use BMP2 effectively and expand its clinical application due to the potential side effects at high doses. In this study, icariin (IC), a type of traditional Chinese medicine, was originally proposed to be a cooperative factor for BMP2. An alkaline phosphatase (ALP) activity assay showed that IC promoted BMP2 osteogenesis in a concentration-dependent manner with significant enhancement at 38.4 µM versus that for BMP2 at 0.8 µg/mL. Furthermore, we developed a composite hierarchical porous scaffold (SF/SBA15; composed of micropores of silk fibroin [SF] scaffold and mesopores of SBA15) for the controlled delivery of BMP2 and IC. This composite scaffold was investigated by a series of physical characterizations and displayed good in vitro cell biocompatibility. In addition, the composite scaffold also showed the degradation rate of 12% dry weight loss and a slight change in the microstructures within 10 days. Moreover, BMP2 and IC were loaded into the SF and SBA15 structures, respectively, of the SF/SBA15 scaffold. This protein/drug loading system (SF/SBA15) provided delivery of BMP2 with an initial burst release of 60.9%±0.9% in the first 24 hours and a gradual release over the subsequent 6 days to 97.9%±0.8%, whereas IC exhibited a burst release of 64.2%±0.7% in the first 24 hours, followed by a sustained release to 92.4%±0.8% over 10 days. With the prolonged local retention and interaction duration of BMP2 and IC, the SF/SBA15 scaffold provided better osteogenic differentiation than other groups with different loading modes of BMP2 or IC, as determined by ALP staining and quantitation and Alizarin red staining. Finally, the results of quantitative real-time polymerase chain reaction analysis indicated that the SF/SBA15 scaffold induced a significantly higher increase in the , and expression levels of cocultured bone marrow mesenchymal stem cells than other payload composite scaffolds. This study suggests that a micro/meso hierarchical porous delivery system of BMP2 and IC ensures osteogenic synergy and demonstrates promise for bone tissue engineering.

摘要

骨形态发生蛋白2(BMP2)作为诱导新骨形成的杰出生长因子而广为人知。然而,由于高剂量时存在潜在副作用,仍需改进以有效使用BMP2并扩大其临床应用。在本研究中,淫羊藿苷(IC)这种传统中药最初被认为是BMP2的协同因子。碱性磷酸酶(ALP)活性测定表明,IC以浓度依赖性方式促进BMP2的成骨作用,在38.4 µM时的促进作用显著增强,而BMP2在0.8 µg/mL时才有此效果。此外,我们开发了一种复合分级多孔支架(SF/SBA15;由丝素蛋白[SF]支架的微孔和SBA15的介孔组成)用于BMP2和IC的控释。通过一系列物理表征对这种复合支架进行了研究,其在体外显示出良好的细胞生物相容性。此外,复合支架在10天内还显示出12%的干重损失降解率以及微观结构的轻微变化。而且,BMP2和IC分别负载到SF/SBA15支架的SF和SBA15结构中。这种蛋白质/药物负载系统(SF/SBA15)实现了BMP2的递送,在前24小时的初始突释率为60.9%±0.9%,在随后6天逐渐释放至97.9%±0.8%,而IC在前24小时的突释率为64.2%±0.7%,随后在10天内持续释放至92.4%±0.8%。随着BMP2和IC在局部的保留时间和相互作用时间延长,通过ALP染色和定量以及茜素红染色测定,SF/SBA15支架比其他具有不同BMP2或IC负载模式的组提供了更好的成骨分化。最后,定量实时聚合酶链反应分析结果表明,SF/SBA15支架诱导共培养的骨髓间充质干细胞的、和表达水平的升高显著高于其他负载复合支架。本研究表明,BMP2和IC的微/介观分级多孔递送系统确保了成骨协同作用,并在骨组织工程方面展现出前景。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/67fb/5656359/1425bd548874/ijn-12-7721Fig1.jpg

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