An active shrinkage and antioxidative hydrogel with biomimetic mechanics functions modulates inflammation and fibrosis to promote skin regeneration

IF 18 1区 医学 Q1 ENGINEERING, BIOMEDICAL Bioactive Materials Pub Date : 2024-11-27 DOI:10.1016/j.bioactmat.2024.11.028
Tao Zhang , Xin-Cao Zhong , Zi-Xuan Feng , Xiao-Ying Lin , Chun-Ye Chen , Xiao-Wei Wang , Kai Guo , Yi Wang , Jun Chen , Yong-Zhong Du , Ze-Ming Zhuang , Yong Wang , Wei-Qiang Tan
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Abstract

Achieving scar-free skin regeneration in clinical settings presents significant challenges. Key issues such as the imbalance in macrophage phenotype transition, delayed re-epithelialization, and excessive proliferation and differentiation of fibroblasts hinder wound healing and lead to fibrotic repair. To these, we developed an active shrinkage and antioxidative hydrogel with biomimetic mechanical functions (P&G@LMs) to reshape the healing microenvironment and effectively promote skin regeneration. The hydrogel's immediate hemostatic effect initiated sequential remodeling, the active shrinkage property sealed and contracted the wound at body temperature, and the antioxidative function eliminated ROS, promoting re-epithelialization. The spatiotemporal release of LMs (ACEI) during the inflammation phase regulated macrophage polarization towards the anti-inflammatory M2 phenotype, promoting progression to the proliferation phase. However, the profibrotic niche of macrophages induced a highly contractile α-SMA positive state in myofibroblasts, whereas the sustained LMs release could regulate this niche to control fibrosis and promote the correct biomechanical orientation of collagen. Notably, the biomimetic mechanics of the hydrogel mimicked the contraction characteristics of myofibroblasts, and the skin-like elastic modulus could accommodate the skin dynamic changes and restore the mechanical integrity of wound defect, partially substituting myofibroblasts' mechanical role in tissue repair. This study presents an innovative strategy for skin regeneration.

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具有生物仿生力学功能的活性收缩和抗氧化水凝胶可调节炎症和纤维化,促进皮肤再生
在临床环境中实现无疤痕皮肤再生是一项重大挑战。巨噬细胞表型转换失衡、再上皮化延迟、成纤维细胞过度增殖和分化等关键问题阻碍了伤口愈合并导致纤维化修复。为此,我们开发了一种具有生物模拟机械功能的主动收缩和抗氧化水凝胶(P&G@LMs),以重塑愈合微环境,有效促进皮肤再生。水凝胶的即时止血效果可启动顺序重塑,主动收缩特性可在体温下密封和收缩伤口,抗氧化功能可消除 ROS,促进皮肤再上皮化。在炎症阶段,LMs(ACEI)的时空释放调节巨噬细胞向抗炎的 M2 表型极化,促进向增殖阶段发展。然而,巨噬细胞的坏死龛位会诱导肌成纤维细胞出现高度收缩的α-SMA阳性状态,而持续释放的LMs可调节该龛位以控制纤维化并促进胶原蛋白的正确生物力学定向。值得注意的是,水凝胶的生物仿生力学模拟了肌成纤维细胞的收缩特性,类皮肤弹性模量可适应皮肤动态变化,恢复伤口缺损的力学完整性,部分替代了肌成纤维细胞在组织修复中的力学作用。这项研究提出了一种创新的皮肤再生策略。
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来源期刊
Bioactive Materials
Bioactive Materials Biochemistry, Genetics and Molecular Biology-Biotechnology
CiteScore
28.00
自引率
6.30%
发文量
436
审稿时长
20 days
期刊介绍: Bioactive Materials is a peer-reviewed research publication that focuses on advancements in bioactive materials. The journal accepts research papers, reviews, and rapid communications in the field of next-generation biomaterials that interact with cells, tissues, and organs in various living organisms. The primary goal of Bioactive Materials is to promote the science and engineering of biomaterials that exhibit adaptiveness to the biological environment. These materials are specifically designed to stimulate or direct appropriate cell and tissue responses or regulate interactions with microorganisms. The journal covers a wide range of bioactive materials, including those that are engineered or designed in terms of their physical form (e.g. particulate, fiber), topology (e.g. porosity, surface roughness), or dimensions (ranging from macro to nano-scales). Contributions are sought from the following categories of bioactive materials: Bioactive metals and alloys Bioactive inorganics: ceramics, glasses, and carbon-based materials Bioactive polymers and gels Bioactive materials derived from natural sources Bioactive composites These materials find applications in human and veterinary medicine, such as implants, tissue engineering scaffolds, cell/drug/gene carriers, as well as imaging and sensing devices.
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