硼硅酸盐生物活性玻璃三维纤维基质增加硼酸盐含量刺激愈合级联在慢性伤口。

Xingchen Zhao, Dong Zhai, Gavin Jell, Chengtie Wu, Huiling Gao, Julian R Jones
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引用次数: 0

摘要

糖尿病伤口再生受到细胞外基质(ECM)形成功能障碍、血管生成受损和炎症延长的阻碍。我们报道了第一个硼硅酸盐生物活性玻璃(BG)纳米纤维缠绕基质,其硼酸盐含量超过2 mol%,通过优化修饰的溶胶-凝胶静电纺丝参数,硼酸盐含量达到70 mol%。所得到的3D基质模拟了细胞外基质纤维的形态,纤维直径均匀在100-300纳米之间,可以通过释放治疗性钙离子和硼酸盐和硅酸盐来生物降解。重点研究硼酸盐含量对体外细胞反应的影响,以确定最佳硼硅酸盐组成;55SiO2-30CaO-15B2O3 (mol%, 55S30C15B)基质对成纤维细胞血管内皮生长因子和碱性成纤维细胞生长因子的促进作用最大,对内皮细胞代谢活性、蛋白表达和迁移的刺激作用最大。我们的体内研究(小鼠糖尿病模型)证实了55S30C15B伤口基质在改善伤口愈合、抗炎反应、血管生成、组织肉芽(α-SMA)和胶原沉积方面的功效,同时阐述了硼酸盐和纳米纤维结构的独特作用。所有证据表明,我们的基质在糖尿病伤口再生方面表现出巨大的潜力。意义声明:我们开发了一种用于伤口愈合的新支架;第一种硼硅BG纳米纤维(100 -300 nm),其硼酸盐含量超过2 mol%,硼含量高达70 mol%。我们确定了纤维输送的硼酸盐剂量对成纤维细胞和内皮细胞的影响。在体内模型中,模拟ecm的支架结构在伤口愈合级联的所有阶段都显示出功效。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Borosilicate bioactive glass 3D fibrous matrices with increased borate content stimulate healing cascades in chronic wounds.

Diabetic wound regeneration is hindered by dysfunctional extracellular matrix (ECM) formation, impaired angiogenesis and prolonged inflammation. We report the first borosilicate bioactive glass (BG) nanofiber wound matrices with borate content exceeding 2 mol%, achieving up to 70 mol% borate, by optimizing modified sol-gel electrospinning parameters. The resultant 3D matrices mimic the morphology of extracellular matrix fibers with homogeneous fiber diameters of 100-300 nm that can biodegrade with the release of therapeutic calcium ions and borate and silicate species. The focus was investigation of the impact of borate content on cellular response in vitro to identify the optimal borosilicate composition; 55SiO2-30CaO-15B2O3 (mol%, 55S30C15B) matrix promoted the greatest expression of vascular endothelial growth factor and basic fibroblast growth factor by fibroblasts and led to the highest stimulation metabolic activity, protein expression and migration of endothelial cells. Our in vivo study (mouse diabetic model) confirmed the efficacy of 55S30C15B wound matrix in improving wound closure, anti-inflammatory response, angiogenesis, tissue granulation (α-SMA), and collagen deposition, while elaborating the distinct roles of borates and nanofiber structure. All evidence suggests that our matrices exhibit great potential for diabetic wound regeneration. STATEMENT OF SIGNIFICANCE: We developed a new scaffold for wound healing; the first borosilicate BG nanofiber (100 -300 nm) mats with borate content in excess of 2 mol%, with boron content of up to 70 mol%. We identified the influence of borate dose delivered by the fibers on both fibroblasts and endothelial cells. Efficacy of the ECM-mimicking scaffold structure was shown across all stages of the wound healing cascade in an in vivo model.

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