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原位触发自收缩生物活性微凝胶组装通过激活机械转导和生化途径加速糖尿病皮肤伤口愈合。

In Situ Triggered Self-Contraction Bioactive Microgel Assembly Accelerates Diabetic Skin Wound Healing by Activating Mechanotransduction and Biochemical Pathway.

作者信息

Xie Qingqiao, Yan Chenchen, Liu Guohui, Bian Liming, Zhang Kunyu

机构信息

School of Biomedical Sciences and Engineering, Guangzhou International Campus, South China University of Technology, Guangzhou, 511442, P. R. China.

National Engineering Research Center for Tissue Restoration and Reconstruction, South China University of Technology, Guangzhou, 510006, P. R. China.

出版信息

Adv Mater. 2024 Sep;36(38):e2406434. doi: 10.1002/adma.202406434. Epub 2024 Jul 23.

DOI:10.1002/adma.202406434
PMID:39039968
Abstract

Chronic nonhealing skin wounds, characterized by reduced tissue contractility and inhibited wound cell survival under hyperglycemia and hypoxia, present a significant challenge in diabetic care. Here, an advanced self-contraction bioactive core-shell microgel assembly with robust tissue-adhesion (SMART-EXO) is introduced to expedite diabetic wound healing. The SMART-EXO dressing exhibits strong, reversible adhesion to damaged tissue due to abundant hydrogen and dynamic coordination bonds. Additionally, the core-shell microgel components and dynamic coordination bonds provide moderate rigidity, customizable self-contraction, and an interlinked porous architecture. The triggered in situ self-contraction of the SMART-EXO dressing enables active, tunable wound contraction, activating mechanotransduction in the skin and promoting the optimal fibroblast-to-myofibroblast conversion, collagen synthesis, and angiogenesis. Concurrently, the triggered contraction of SMART-EXO facilitates efficient loading and on-demand release of bioactive exosomes, contributing to re-epithelialization and wound microenvironment regulation in diabetic mice. RNA-seq results reveal the activation of critical signaling pathways associated with mechanosensing and exosome regulation, highlighting the combined biomechanical and biochemical mechanisms. These findings underscore SMART-EXO as a versatile, adaptable solution to the complex challenges of diabetic wound care.

摘要

慢性难愈合皮肤伤口的特点是在高血糖和缺氧条件下组织收缩性降低且伤口细胞存活率受抑制,这给糖尿病护理带来了重大挑战。在此,引入了一种具有强大组织粘附力的先进自收缩生物活性核壳微凝胶组件(SMART-EXO)以加速糖尿病伤口愈合。SMART-EXO敷料由于丰富的氢键和动态配位键而对受损组织表现出强的、可逆的粘附力。此外,核壳微凝胶组件和动态配位键提供适度的刚性、可定制的自收缩性以及相互连接的多孔结构。SMART-EXO敷料触发的原位自收缩能够实现主动的、可调节的伤口收缩,激活皮肤中的机械转导并促进成纤维细胞向肌成纤维细胞的最佳转化、胶原蛋白合成和血管生成。同时,SMART-EXO的触发收缩促进了生物活性外泌体的有效负载和按需释放,有助于糖尿病小鼠的再上皮化和伤口微环境调节。RNA测序结果揭示了与机械传感和外泌体调节相关的关键信号通路的激活,突出了联合的生物力学和生化机制。这些发现强调了SMART-EXO是应对糖尿病伤口护理复杂挑战的一种通用、适应性强的解决方案。

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