Therapeutic potential of gelatine methacrylate hydrogels loaded with macrophage-derived exosomes for accelerating angiogenesis and cutaneous wound healing

Jiajun Liu, Fuying Chen, Luoqiang Tian, Jinjie Wu, Keting Liu, Qiwen Wan, Bo Yuan, Xiangdong Zhu, Xuening Chen, Xingdong Zhang
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Abstract

Extensive studies demonstrate that macrophage response plays an important role in regulating angiogenesis via a paracrine way, which is crucial for skin wound repair. This study isolated and characterized nanosized exosomes from differently polarized macrophages (MΦ), including M0 (naïve), M1 (pro-inflammatory), and M2 (anti-inflammatory) macrophages, and further assessed their impacts on angiogenesis and skin regeneration. Our results indicated that compared to M0 and M1 counterparts, M2 macrophage-derived exosomes (M2-Exos) exhibited a pronounced ability to promote angiogenic ability of of human umbilical vein endothelial cells (HUVECs) by enhancing expression of angiogenic genes and proteins, increasing cell migration, and improving tubulogenesis. Bioinformatics analyses suggested that the distinct angiogenic potentials of three MΦ-Exos might be attributed to the differentially expressed angiogenesis-related miRNAs and their target genes such as Stat3, Smad 2, and Smad4. Moreover, these isolated MΦ-Exos were integrated with gelatine methacrylate (GelMA) hydrogels to achieve the sustained delivery at murine full-thickness cutaneous wound sites. In vivo results showed that Gel/M2-Exos significantly augmented angiogenesis, accelerated re-epithelialization, promoted collagen maturity, thereby promoting wound healing. In contrary, Gel/M1-Exos showed the opposite effects. Our findings provided compelling evidence that the polarization status of macrophages significantly affected angiogenesis and wound healing via the miRNA cargos of their derived exosomes. Moreover, this study opens a new avenue for developing nano-scale, cell-free exosome-based therapies in treating cutaneous wounds.

Graphical abstract

负载巨噬细胞外泌体的甲基丙烯酸明胶水凝胶在加速血管生成和皮肤伤口愈合方面的治疗潜力
大量研究表明,巨噬细胞反应通过旁分泌方式在调节血管生成方面发挥着重要作用,这对皮肤伤口修复至关重要。本研究从不同极化的巨噬细胞(MΦ)(包括M0(天真)、M1(促炎)和M2(抗炎)巨噬细胞)中分离并鉴定了纳米级外泌体,并进一步评估了它们对血管生成和皮肤再生的影响。我们的研究结果表明,与M0和M1对应物相比,M2巨噬细胞衍生的外泌体(M2-Exos)通过增强血管生成基因和蛋白的表达、增加细胞迁移和改善微管生成,表现出明显的促进人脐静脉内皮细胞(HUVECs)血管生成的能力。生物信息学分析表明,三种 MΦ-Exos 不同的血管生成潜能可能归因于血管生成相关 miRNA 及其靶基因(如 Stat3、Smad 2 和 Smad4)的不同表达。此外,这些分离出的 MΦ-Exos 与甲基丙烯酸明胶(GelMA)水凝胶结合,实现了在小鼠全厚皮肤伤口部位的持续递送。体内试验结果表明,Gel/M2-Exos能显著增强血管生成,加速再上皮化,促进胶原蛋白成熟,从而促进伤口愈合。相反,Gel/M1-Exos 则显示出相反的效果。我们的研究结果提供了令人信服的证据,表明巨噬细胞的极化状态会通过其衍生的外泌体所携带的 miRNA 显著影响血管生成和伤口愈合。此外,这项研究为开发基于纳米级无细胞外泌体的疗法治疗皮肤伤口开辟了一条新途径。
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来源期刊
Journal of Leather Science and Engineering
Journal of Leather Science and Engineering 工程技术-材料科学:综合
CiteScore
12.80
自引率
0.00%
发文量
29
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