骨生物学中基质硬度对免疫细胞的影响

Ting Jiang , Meng-Ting Zheng , Ruo-Mei Li , Ning-Juan Ouyang
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摘要

骨细胞和免疫细胞通常居住在同一微环境中,并相互影响,共同执行 "骨免疫系统 "的功能。建立一个和谐持久的骨免疫系统能显著促进骨再生,因此必须维持骨和免疫的平衡。近来,机械生物学在骨组织工程中引起了越来越多的关注,基质硬度作为一个关键参数受到了广泛研究。基质硬度对骨稳态的影响仍然相对明确。软基质往往会严重影响骨髓间充质干细胞的软骨分化,而增加基质硬度则有利于成骨分化。增加硬度会增加破骨细胞的分化和活性。此外,人们越来越重视免疫平衡,这就需要免疫细胞之间进行动态交流。免疫细胞在启动骨再生和驱动早期炎症反应方面至关重要。基质硬度引起的功能变化是决定工程组织模拟结果的关键。然而,由于基质硬度范围、测量方法和其他因素的不同,关于不同免疫细胞对基质硬度反应的研究结果不一致且不可比,这可能会令人困惑。因此,本研究旨在全面综述基质硬度对不同免疫细胞的具体影响,尤其关注其对骨再生的影响,这将为大段骨缺损的治疗提供理论依据,并有助于新工程策略的临床开发。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
The effects of matrix stiffness on immune cells in bone biology

Bone and immune cells typically inhabit the same microenvironment and engage in mutual interactions to collectively execute the functions of the “osteoimmune system.” Establishing a harmonized and enduring osteoimmune system significantly enhances bone regeneration, necessitating the maintenance of bone and immune homeostasis. Recently, mechanobiology has garnered increasing interest in bone tissue engineering, with matrix stiffness emerging as a crucial parameter that has been extensively investigated. The effect of matrix stiffness on bone homeostasis remains relatively clear. Soft substrates tend to significantly affect the chondrogenic differentiation of bone marrow mesenchymal stem cells, whereas increasing matrix stiffness is advantageous for osteogenic differentiation. Increased stiffness increases osteoclast differentiation and activity. Additionally, there is increasing emphasis on immune homeostasis, which necessitates dynamic communication between immune cells. Immune cells are crucial in initiating bone regeneration and driving early inflammatory responses. Functional changes induced by matrix stiffness are pivotal for determining the outcomes of engineered tissue mimics. However, inconsistent and incomparable findings regarding the responses of different immune cells to matrix stiffness can be perplexing owing to variations in the stiffness range, measurement methods, and other factors. Therefore, this study aimed to provide a comprehensive review of the specific effects of matrix stiffness on diverse immune cells, with a particular focus on its implications for bone regeneration, which would offer theoretical insights into the treatment of large segmental bony defects and assist in the clinical development of new engineering strategies.

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