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机械刺激和卷曲形貌的协同作用刺激肌腱工程中天然胶原的生成。

Synergistic effects of mechanical stimulation and crimped topography to stimulate natural collagen development for tendon engineering.

机构信息

Department of Plastic and Reconstructive Surgery, Shanghai Ninth People's Hospital, Shanghai Jiao Tong University School of Medicine, Shanghai 200011, China; Shanghai Key Laboratory of Tissue Engineering Research, Shanghai 200011, China.

Department of Plastic and Reconstructive Surgery, Shanghai Ninth People's Hospital, Shanghai Jiao Tong University School of Medicine, Shanghai 200011, China; Shanghai Key Laboratory of Tissue Engineering Research, Shanghai 200011, China.

出版信息

Acta Biomater. 2022 Jun;145:297-315. doi: 10.1016/j.actbio.2022.04.026. Epub 2022 Apr 22.

Abstract

Suitable scaffold structures and mechanical loading are essential for functional tendon engineering. However, the bipolar fibril structure of native tendon collagen is yet to be recaptured in engineered tendons. This study compared the development of Achilles tendons of postnatal rats with and without (via surgical section) mechanical loading to define the mechanism of mechanical stimulation-mediated tendon development. The results demonstrated that the severed tendons weakened mechanically and exhibited disorganization without a bipolar fibril superstructure. Proteomic analysis revealed differentially expressed key regulatory molecules related to the collagen assembly process, including decreased fibromodulin, keratocan, fibroblast growth factor-1, and increased lumican and collagen5a1 in the severed tendons with immunohistochemical verification. Additionally, a complex regulatory network of mechanical stimulation-mediated collagen assembly in a spatiotemporal manner was also revealed using bioinformatics analysis, wherein PI3K-Akt and HDAC4 may be the predominant signaling pathways. A wavy microgrooved surface (Y = 5.47sin(0.015x)) that biomimics tendon topography was observed to enhance the expression of collagen assembly molecules under mechanical loading, and the aforementioned pathways are particularly involved and verified with their respective inhibitors of LY-294002 and LMK-235. Furthermore, an electrospun crimped nanofiber scaffold (approximately 2 μm fiber diameter and 0.12 crimpness) was fabricated to biomimic the tenogenic niche environment; this was observed to be more effective on enhancing collagen production and assembly under mechanical stimulation. In conclusion, the synergistic effect between topographical niche and mechanical stimulation was observed to be essential for collagen assembly and maturation and should be applied to functional tendon engineering in the future. STATEMENT OF SIGNIFICANCE: In biomaterial-mediated tendon regeneration, mechanical stimulation is essential for tendon collagen assembly. However, the underlying mechanisms remain not fully defined, leading to the failure of the native-like collagen regeneration. In this study, a mechanical stimulation deprivation model of rat tendon was established to reveal the mechanisms in tendon development and define the key regulatory molecules including small leucine-rich proteoglycans, lysyl oxidase and collagen V. After ensuring the importance of biomimetic structure in tendon remodeling, crimped nanofibers were developed to verify these regulatory molecules, and demonstrated that mechanical stimulation significantly enhanced collagen assembly via PIK3 and HDAC4 pathways in biomaterial-regulated tendon regeneration. This study provides more insightful perspectives in the physiologically remodeling progression of tendon collagen and design of tendon scaffolds.

摘要

合适的支架结构和机械加载对于功能性腱工程至关重要。然而,在工程腱中尚未重新捕获天然腱胶原的双极原纤维结构。本研究比较了出生后大鼠的跟腱有无机械加载(通过手术切开)的发育情况,以确定机械刺激介导腱发育的机制。结果表明,切断的腱在机械上变弱,并且没有双极原纤维超结构而表现出紊乱。蛋白质组学分析显示,在没有双极原纤维超结构的切断腱中,与胶原组装过程相关的关键调节分子的表达存在差异,包括纤维调节素、角膜蛋白聚糖、成纤维细胞生长因子-1 的减少,以及赖氨酰氧化酶和胶原 5a1 的增加,并用免疫组织化学验证。此外,通过生物信息学分析还揭示了机械刺激介导胶原组装的时空复杂调节网络,其中 PI3K-Akt 和 HDAC4 可能是主要的信号通路。观察到一种模仿腱拓扑结构的波浪形微槽表面(Y=5.47sin(0.015x))在机械加载下增强了胶原组装分子的表达,并且用各自的 LY-294002 和 LMK-235 抑制剂特别参与和验证了上述途径。此外,还制备了模仿腱生境环境的电纺卷曲纳米纤维支架(约 2μm 纤维直径和 0.12 卷曲度),观察到在机械刺激下更有效地增强胶原的产生和组装。总之,观察到拓扑生境和机械刺激的协同作用对于胶原组装和成熟至关重要,应该在未来应用于功能性腱工程。

意义声明

在生物材料介导的腱再生中,机械刺激对于腱胶原的组装是必不可少的。然而,其潜在机制仍未完全定义,导致天然样胶原再生失败。在这项研究中,建立了大鼠腱的机械刺激剥夺模型,以揭示腱发育的机制,并确定包括小富含亮氨酸的蛋白聚糖、赖氨酰氧化酶和胶原 V 在内的关键调节分子。在确保生物材料调节的腱再生中仿生结构的重要性之后,开发了卷曲纳米纤维来验证这些调节分子,并证明机械刺激通过 PIK3 和 HDAC4 途径显著增强了胶原组装。这项研究为腱胶原的生理重塑进展和腱支架的设计提供了更深入的视角。

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