Bone regeneration: The influence of composite HA/TCP scaffolds and electrical stimulation on TGF/BMP and RANK/RANKL/OPG pathways.

Júlia Venturini Helaehil, Boyang Huang, Paulo Bartolo, Milton Santamaria-Jr, Guilherme Ferreira Caetano
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Abstract

The repair of critical-sized bone defects represents significant clinical challenge. An alternative approach is the use of 3D composite scaffolds to support bone regeneration. Hydroxyapatite (HA) and tri-calcium phosphate (β-TCP), combined with polycaprolactone (PCL), offer promising mechanical resistance and biocompatibility. Bioelectrical stimulation (ES) at physiological levels is proposed to reestablishes tissue bioeletrocity and modulates cell signaling communication, such as the BMP/TGF-β and the RANK/RANK-L/OPG pathways. This study aimed to evaluate the use HA/TCP scaffolds and ES therapy for bone regeneration and their impact on the TGF-β/BMP pathway, alongside their relationship with the RANK/RANKL/OPG pathway in critical bone defects. The scaffolds were implanted at the bone defect in animal model (calvarial bone) and the area was subjected to ES application twice a week at 10 µA intensity of current for 5 min each session. Samples were collected for histomorphometry, immunohistochemistry, and molecular analysis. The TGF-β/BMP pathway study showed the HA/TCP+ES group increased BMP-7 gene expression at 30 and 60 days, and also greater endothelial vascular formation. Moreover, the HA/TCP and HA/TCP+ES groups exhibited a bone remodeling profile, indicated by RANKL/OPG ratio. HA/TCP scaffolds with ES enhanced vascular formation and mineralization initially, while modulation of the BMP/TGF pathway maintained bone homeostasis, controlling resorption via ES with HA/TCP.

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骨再生:HA/TCP复合支架和电刺激对TGF/BMP和RANK/RANKL/OPG通路的影响。
骨缺损的修复是临床面临的重大挑战。另一种方法是使用3D复合支架来支持骨再生。羟基磷灰石(HA)和磷酸三钙(β-TCP)与聚己内酯(PCL)结合,具有良好的机械抗性和生物相容性。生理水平的生物电刺激(ES)被认为可以重建组织生物电并调节细胞信号传导,如BMP/TGF-β和RANK/RANK- l /OPG通路。本研究旨在评估HA/TCP支架和ES治疗骨再生及其对TGF-β/BMP通路的影响,以及它们与严重骨缺损RANK/RANKL/OPG通路的关系。将支架植入动物模型骨缺损处(颅骨),每周2次,每次10µa电流,每次5 min。收集样本进行组织形态学、免疫组织化学和分子分析。TGF-β/BMP通路研究显示,HA/TCP+ES组在30和60 d时BMP-7基因表达增加,内皮血管形成增加。此外,HA/TCP和HA/TCP+ES组表现出骨重塑特征,由RANKL/OPG比值显示。带有ES的HA/TCP支架最初增强了血管形成和矿化,而BMP/TGF通路的调节维持了骨稳态,通过HA/TCP通过ES控制骨吸收。
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