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电刺激疗法和HA/TCP复合支架调节临界尺寸骨缺损再生中的Wnt信号通路。

Electrical Stimulation Therapy and HA/TCP Composite Scaffolds Modulate the Wnt Pathways in Bone Regeneration of Critical-Sized Defects.

作者信息

Helaehil Júlia Venturini, Helaehil Luiza Venturini, Alves Laryssa Fernanda, Huang Boyang, Santamaria-Jr Milton, Bartolo Paulo, Caetano Guilherme Ferreira

机构信息

Graduate Program in Biomedical Sciences, University Center of Hermínio Ometto Foundation, FHO, Araras 13607-339, Brazil.

Singapore Centre for 3D Printing, School of Mechanical and Aerospace Engineering, Nanyang Technological University, Singapore 639798, Singapore.

出版信息

Bioengineering (Basel). 2023 Jan 6;10(1):75. doi: 10.3390/bioengineering10010075.

Abstract

Critical bone defects are the most difficult challenges in the area of tissue repair. Polycaprolactone (PCL) scaffolds, associated with hydroxyapatite (HA) and tricalcium phosphate (TCP), are reported to have an enhanced bioactivity. Moreover, the use of electrical stimulation (ES) has overcome the lack of bioelectricity at the bone defect site and compensated the endogenous electrical signals. Such treatments could modulate cells and tissue signaling pathways. However, there is no study investigating the effects of ES and bioceramic composite scaffolds on bone tissue formation, particularly in the view of cell signaling pathway. This study aims to investigate the application of HA/TCP composite scaffolds and ES and their effects on the Wingless-related integration site (Wnt) pathway in critical bone repair. Critical bone defects (25 mm) were performed in rats, which were divided into four groups: PCL, PCL + ES, HA/TCP and HA/TCP + ES. The scaffolds were grafted at the defect site and applied with the ES application twice a week using 10 µA of current for 5 min. Bone samples were collected for histomorphometry, immunohistochemistry and molecular analysis. At the Wnt canonical pathway, HA/TCP and HA/TCP + ES groups showed higher and gene expression levels, especially HA/TCP. Moreover, HA/TCP + ES presented higher , and levels. At the Wnt non-canonical pathway, HA/TCP group showed higher voltage-gated calcium channel (), calmodulin-dependent protein kinase II, and genes expression, while HA/TCP + ES presented higher protein expression of VGCC and calmodulin (CaM) at the same period. The decrease in and genes expressions and the lower bone sialoprotein II in the HA/TCP + ES group may be related to the early bone remodeling. This study shows that the use of ES modulated the Wnt pathways and accelerated the osteogenesis with improved tissue maturation.

摘要

严重骨缺损是组织修复领域最具挑战性的难题。据报道,聚己内酯(PCL)支架与羟基磷灰石(HA)和磷酸三钙(TCP)结合后具有增强的生物活性。此外,电刺激(ES)的应用克服了骨缺损部位生物电的缺乏,并补偿了内源性电信号。这种治疗可以调节细胞和组织信号通路。然而,尚无研究探讨ES和生物陶瓷复合支架对骨组织形成的影响,特别是从细胞信号通路的角度。本研究旨在探讨HA/TCP复合支架和ES的应用及其在严重骨修复中对无翅相关整合位点(Wnt)通路的影响。在大鼠中制造25毫米的严重骨缺损,并将其分为四组:PCL、PCL + ES、HA/TCP和HA/TCP + ES。将支架植入缺损部位,并每周两次施加ES,电流为10 μA,持续5分钟。收集骨样本进行组织形态计量学、免疫组织化学和分子分析。在Wnt经典通路中,HA/TCP和HA/TCP + ES组显示出更高的 和 基因表达水平,尤其是HA/TCP组。此外,HA/TCP + ES组的 、 和 水平更高。在Wnt非经典通路中,HA/TCP组显示出更高的电压门控钙通道()、钙调蛋白依赖性蛋白激酶II和 基因表达,而HA/TCP + ES组在同一时期呈现出更高的VGCC和钙调蛋白(CaM)蛋白表达。HA/TCP + ES组中 和 基因表达的降低以及骨唾液蛋白II的减少可能与早期骨重塑有关。本研究表明,ES的使用调节了Wnt通路并加速了成骨过程,同时改善了组织成熟度。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8f88/9854456/1043ae5cec95/bioengineering-10-00075-g001.jpg

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