The Extracellular Matrix Promotes Diabetic Oral Wound Healing by Modulating the Microenvironment.

IF 9.6 Q1 ENGINEERING, BIOMEDICAL Biomaterials research Pub Date : 2025-03-19 eCollection Date: 2025-01-01 DOI:10.34133/bmr.0169
Zhongke Wang, Li Wang, Sihan Wang, Hongmei Chen, Danni Wang, Aodi Li, Ying Huang, Yifan Pu, Xinlei Xiong, Xiangrui Lui, Yuwen Huang, Ling Guo
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Abstract

Oral wounds in diabetes mellitus (DM) often delay healing due to reduced angiogenesis and increased inflammatory response in the local microenvironment, even leading to graft necrosis and implant failure. Therefore, developing an effective program to promote healing is of great clinical value. Much of the current research is focused on promoting wound healing through surface adhesive materials that exert a pro-angiogenic, anti-inflammatory effect. However, the application of surface bonding materials in the oral cavity is very limited due to the humid and friction-prone environment. Decellularized extracellular adipose tissue (DAT) is an easily accessible and biocompatible material derived from adipose tissue. To further explore the potential of DAT, we used multi-omics to analyze its composition and possible mechanisms. Proteomic studies revealed that DAT contains anti-inflammatory, pro-angiogenic proteins that promote DM tissue regeneration. To adapt to the moist and chewing friction environment of the mouth, we modified DAT into a temperature-sensitive hydrogel material that can be injected intramucosally. DAT hydrogel has been verified to promote angiogenesis and exert anti-inflammatory effects through macrophage phenotypic transformation. Meanwhile, transcriptome analysis suggested that the inhibitory effect of DAT on the interleukin 17 signaling pathway might be a key factor in promoting DM oral wound healing. In conclusion, after multi-omic analysis, DAT hydrogel can exert good pro-angiogenic and anti-inflammatory effects through the interleukin 17 signaling pathway and can be adapted to the specific environment of the oral cavity. This provides a potential way to promote DM oral wound healing in a clinical setting.

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细胞外基质通过调节微环境促进糖尿病口腔伤口愈合。
糖尿病(DM)口腔伤口由于血管生成减少和局部微环境炎症反应增加而延迟愈合,甚至导致移植物坏死和种植失败。因此,制定一个有效的方案来促进愈合具有重要的临床价值。目前的许多研究都集中在通过表面粘附材料来促进伤口愈合,这种材料具有促血管生成、抗炎的作用。然而,由于口腔环境的潮湿和易发生摩擦,表面粘合材料在口腔中的应用非常有限。脱细胞细胞外脂肪组织(DAT)是一种来源于脂肪组织的易获取的生物相容性材料。为了进一步探索DAT的潜力,我们利用多组学分析了它的组成和可能的机制。蛋白质组学研究显示,DAT含有抗炎、促血管生成蛋白,可促进糖尿病组织再生。为了适应口腔的潮湿和咀嚼摩擦环境,我们将DAT改造成一种温度敏感的水凝胶材料,可以注射到粘膜内。DAT水凝胶已被证实通过巨噬细胞表型转化促进血管生成并发挥抗炎作用。同时,转录组分析提示,DAT对白细胞介素17信号通路的抑制作用可能是促进DM口腔创面愈合的关键因素。综上所述,经多组学分析,DAT水凝胶能够通过白细胞介素17信号通路发挥良好的促血管生成和抗炎作用,能够适应口腔的特定环境。这提供了一个潜在的途径,促进口腔伤口愈合的糖尿病在临床设置。
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