结构控制的丝素蛋白涂层在骨科感染和原位成骨中的评价:体外和体内

Wenhao Zhou, Teng Zhang, Jianglong Yan, Qiyao Li, P. Xiong, Yangyang Li, Yan Cheng, Yufeng Zheng
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引用次数: 0

摘要

生物医学器械相关感染(BAI)和骨合成是骨科植入手术后的两个主要并发症,特别是当感染细菌形成成熟的生物膜时,它可以保护生物体免受宿主免疫系统和抗生素治疗的影响。与单一抗生素治疗方法相比,银纳米颗粒(AgNPs)与常规抗生素联合使用具有较高的抗菌活性。然而,极大限制AgNP/抗炎药潜在应用的一个主要问题是不受控制的释放。此外,成骨能力的缺乏也可能导致骨合成。因此,我们制备了一种结构控制的载药丝素(SF)涂层,可以实现AgNPs的大小和释放控制,并实现高效成骨。制备了三种比较的sf基涂层:α-结构涂层(α-helices占32.7%)、m-结构涂层(β-sheets占28.3%)和β-结构涂层(β-sheets占41%)。由于α-螺旋结构含量高,AgNPs较小(20 nm), α-结构涂层具有较好的蛋白质吸附和亲水性,并具有ph依赖性和长效抗菌性能。体外实验表明,α包被具有良好的生物相容性(细胞附着、扩散和增殖)、高ALP表达、高胶原分泌和高钙矿化。此外,在体内皮下植入一个月后,α结构涂层引起的炎症反应非常小。此外,在兔股骨缺损模型中,α-结构涂层对新生骨的生成和新骨与组织的结合有显著改善,表明骨整合快速持久。预期,这种优化的结构控制的sf基涂层可以成为当前骨科挑战的替代和前瞻性解决方案。
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Evaluation of Structure-Controlled Silk Fibroin Coatings for Orthopedic Infection and In-Situ Osteogenesis: In Vitro and In Vivo
Biomedical device-associated infections (BAI) and osteosynthesis are two main complications following the orthopedic implant surgery, especially while infecting bacteria form a mature biofilm, which can protect the organisms from the host immune system and antibiotic therapy. Comparing with the single antibiotics therapeutic method, the combination of silver nanoparticles (AgNPs) and conventional antibiotics exert a high level of antibacterial activity. Nevertheless, one major issue that extremely restricts the potential application of AgNP/antiviotics is the uncontrolled release. Moreover, the lack of osteogenic ability may cause the osteosynthesis. Thus, herein we fabricated a structure-controlled drug-loaded silk fibroin (SF) coating that can achieve the size and release control of AgNPs and high efficient osteogenesis. Three comparative SF-based coatings were fabricated: α-structured coating (α-helices 32.7%,), m-structured coating (β-sheets 28.3%) and β-structured coating (β-sheets 41%). Owning to the high content of α-helices structure and small AgNPs (20 nm), α-structured coating displayed better protein adsorption and hydrophilicity, as well as pH-dependent and long-lasting antibacterial performance. In vitro studies demonstrated that α coating showed good biocompatibility (cellular attachment, spreading and proliferation), high ALP expression, collagen secretion and calcium mineralization. Moreover, after one month subcutaneous implantation in vivo, α-structured coating elicited minimal, comparable inflammatory response. Additionally, in a rabbit femoral defect model, α-structured coating displayed a significant improvement on the generation of new-born bone and bonding between the new bone and the tissue, implying a rapid and durable osteointegration. Expectedly, this optimized structure-controlled SF-based coating can be an alternative and prospective solution for the current challenges in orthopedics.
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