Mechanically activated mesenchymal-derived bone cells drive vessel formation via an extracellular vesicle mediated mechanism.

IF 6.7 1区 工程技术 Q1 CELL & TISSUE ENGINEERING
N Shen, M Maggio, I Woods, M C Lowry, R Almasri, C Gorgun, K F Eichholz, E Stavenschi, K Hokamp, F M Roche, L O'Driscoll, D A Hoey
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引用次数: 1

Abstract

Blood vessel formation is an important initial step for bone formation during development as well as during remodelling and repair in the adult skeleton. This results in a heavily vascularized tissue where endothelial cells and skeletal cells are constantly in crosstalk to facilitate homeostasis, a process that is mediated by numerous environmental signals, including mechanical loading. Breakdown in this communication can lead to disease and/or poor fracture repair. Therefore, this study aimed to determine the role of mature bone cells in regulating angiogenesis, how this is influenced by a dynamic mechanical environment, and understand the mechanism by which this could occur. Herein, we demonstrate that both osteoblasts and osteocytes coordinate endothelial cell proliferation, migration, and blood vessel formation via a mechanically dependent paracrine mechanism. Moreover, we identified that this process is mediated via the secretion of extracellular vesicles (EVs), as isolated EVs from mechanically stimulated bone cells elicited the same response as seen with the full secretome, while the EV-depleted secretome did not elicit any effect. Despite mechanically activated bone cell-derived EVs (MA-EVs) driving a similar response to VEGF treatment, MA-EVs contain minimal quantities of this angiogenic factor. Lastly, a miRNA screen identified mechanoresponsive miRNAs packaged within MA-EVs which are linked with angiogenesis. Taken together, this study has highlighted an important mechanism in osteogenic-angiogenic coupling in bone and has identified the mechanically activated bone cell-derived EVs as a therapeutic to promote angiogenesis and potentially bone repair.

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机械活化的间充质骨细胞通过细胞外囊泡介导机制驱动血管形成。
血管的形成是成人骨骼发育、重塑和修复过程中骨形成的重要初始步骤。这导致了一个血管化程度很高的组织,内皮细胞和骨骼细胞不断地相互作用,以促进体内平衡,这一过程是由许多环境信号介导的,包括机械负荷。这种交流的中断可导致疾病和/或骨折修复不良。因此,本研究旨在确定成熟骨细胞在调节血管生成中的作用,这是如何受到动态机械环境的影响,并了解其发生的机制。在此,我们证明成骨细胞和骨细胞通过机械依赖的旁分泌机制协调内皮细胞增殖、迁移和血管形成。此外,我们发现这一过程是通过细胞外囊泡(EVs)的分泌介导的,因为从机械刺激的骨细胞中分离出的EVs引起了与完整分泌组相同的反应,而ev耗尽的分泌组则没有引起任何影响。尽管机械活化的骨细胞源性EVs (MA-EVs)对VEGF治疗有类似的反应,但MA-EVs含有极少量的这种血管生成因子。最后,miRNA筛选鉴定了包装在ma - ev中的机械反应性miRNA,这些miRNA与血管生成有关。综上所述,本研究强调了骨中成骨-血管生成耦合的重要机制,并确定了机械激活的骨细胞来源的EVs作为促进血管生成和潜在骨修复的治疗方法。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Journal of Tissue Engineering
Journal of Tissue Engineering Engineering-Biomedical Engineering
CiteScore
11.60
自引率
4.90%
发文量
52
审稿时长
12 weeks
期刊介绍: The Journal of Tissue Engineering (JTE) is a peer-reviewed, open-access journal dedicated to scientific research in the field of tissue engineering and its clinical applications. Our journal encompasses a wide range of interests, from the fundamental aspects of stem cells and progenitor cells, including their expansion to viable numbers, to an in-depth understanding of their differentiation processes. Join us in exploring the latest advancements in tissue engineering and its clinical translation.
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