缺氧间充质干细胞来源的小细胞外囊泡通过 miR-210-3p/EFNA3/PI3K 通路促进血管化骨再生。

Small extracellular vesicles derived from hypoxic mesenchymal stem cells promote vascularized bone regeneration through the miR-210-3p/EFNA3/PI3K pathway.

机构信息

Department of Oral and Cranio-Maxillofacial Surgery, Shanghai Ninth People's Hospital, Shanghai Jiao Tong University School of Medicine, College of Stomatology, Shanghai Jiao Tong University, China; National Center for Stomatology, National Clinical Research Center for Oral Diseases, Shanghai Key Laboratory of Stomatology, Research Unit of Oral and Maxillofacial Regenerative Medicine, Chinese Academy of Medical Sciences, Shanghai 200011, China.

出版信息

Acta Biomater. 2022 Sep 15;150:413-426. doi: 10.1016/j.actbio.2022.07.015. Epub 2022 Jul 16.

DOI:10.1016/j.actbio.2022.07.015

PMID:35850484

Abstract

Angiogenesis is closely coupled with osteogenesis and has equal importance. Thus, promoting angiogenesis during the bone repair process is vital for ideal bone regeneration. As important mediators of cell-cell communication and biological homeostasis, mesenchymal stem cell-derived small extracellular vesicles (MSC-sEVs) have been proved to be highly involved in bone and vascular regeneration. Because hypoxia microenvironment promotes the proangiogenic activity of MSCs, in the present study, we investigate the effect and underlying molecular mechanisms of sEVs from hypoxia-preconditioned MSCs (hypo-sEVs) on angiogenesis and develop an effective strategy to promote vascularized bone regeneration. Compared to sEVs from normoxia MSCs (nor-sEVs), hypo-sEVs promoted the proliferation, migration, and angiogenesis of HUVECs and ultimately enhanced bone regeneration and new blood vessel reconstruction in a critical-size calvarial bone defect model. miRNA sequence and the verified results showed that miR-210-3p in hypo-sEVs was increased via HIF-1α under hypoxia. The upregulated miR-210-3p in hypo-sEVs promoted angiogenesis by downregulating EFNA3 expression and enhancing the phosphorylation of the PI3K/AKT pathway. Thus, this study suggests a successful strategy to enhance vascularized bone regeneration by utilizing hypo-sEVs via the miR-210-3p/EFNA3/PI3K/AKT pathway. STATEMENT OF SIGNIFICANCE: Considering the significance of vascularization in ideal bone regeneration, strategies to promote angiogenesis during bone repair are required. Hypoxia microenvironment can promote the proangiogenic potential of mesenchymal stem cells (MSCs). Nonetheless, the therapeutic effect of small extracellular vesicles (sEVs) from hypoxia-preconditioned MSCs on cranio-maxillofacial bone defect remains unknown, and the underlying mechanism is poorly understood. This study shows that hypo-sEVs significantly enhance the proliferation, migration, and angiogenesis of HUVECs as well as promote vascularized bone formation. Moreover, this work indicates that HIF-1α can induce overexpression of miR-210-3p under hypoxia, and miR-210-3p can hinder EFNA3 expression and subsequently activate the PI3K/AKT pathway. The application of hypo-sEVs provides a facile and promising strategy to promote vascularized bone regeneration in a critical-size bone defect model.

摘要

血管生成与成骨密切相关，具有同等重要性。因此，在骨修复过程中促进血管生成对于理想的骨再生至关重要。作为细胞间通讯和生物稳态的重要介质，间充质干细胞衍生的小细胞外囊泡 (MSC-sEVs) 已被证明高度参与骨和血管再生。由于低氧微环境促进 MSC 的促血管生成活性，因此在本研究中，我们研究了低氧预处理 MSC 的 sEVs (hypo-sEVs) 对血管生成的影响及其潜在的分子机制，并开发了一种促进血管化骨再生的有效策略。与来自常氧 MSC 的 sEVs (nor-sEVs) 相比，hypo-sEVs 促进了 HUVEC 的增殖、迁移和血管生成，并最终增强了临界大小颅骨骨缺损模型中的骨再生和新血管重建。miRNA 序列和验证结果表明，低氧条件下 HIF-1α 使 hypo-sEVs 中的 miR-210-3p 增加。hypo-sEVs 中上调的 miR-210-3p 通过下调 EFNA3 表达和增强 PI3K/AKT 通路的磷酸化来促进血管生成。因此，这项研究通过利用 miR-210-3p/EFNA3/PI3K/AKT 通路，利用 hypo-sEVs 提出了一种增强血管化骨再生的成功策略。

意义声明

考虑到血管化在理想骨再生中的重要性，需要在骨修复过程中促进血管生成的策略。低氧微环境可以促进间充质干细胞 (MSCs) 的促血管生成潜力。尽管如此，来自低氧预处理 MSC 的 sEVs 对颅面骨缺损的治疗效果尚不清楚，其潜在机制也知之甚少。本研究表明 hypo-sEVs 可显著增强 HUVEC 的增殖、迁移和血管生成，并促进血管化骨形成。此外，这项工作表明 HIF-1α 可以在低氧下诱导 miR-210-3p 的过表达，而 miR-210-3p 可以抑制 EFNA3 的表达，进而激活 PI3K/AKT 通路。hypo-sEVs 的应用为在临界大小骨缺损模型中促进血管化骨再生提供了一种简便而有前景的策略。

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缺氧间充质干细胞来源的小细胞外囊泡通过 miR-210-3p/EFNA3/PI3K 通路促进血管化骨再生。

Small extracellular vesicles derived from hypoxic mesenchymal stem cells promote vascularized bone regeneration through the miR-210-3p/EFNA3/PI3K pathway.

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