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人骨组织衍生的细胞外基质水凝胶:通过加工参数控制物理化学、生物化学和生物学特性。

Human bone tissue-derived ECM hydrogels: Controlling physicochemical, biochemical, and biological properties through processing parameters.

作者信息

Kim Yang-Hee, Cidonio Gianluca, Kanczler Janos M, Oreffo Richard Oc, Dawson Jonathan I

机构信息

Bone and Joint Research Group, Centre for Human Development, Stem Cells and Regeneration, Institute of Developmental Sciences, University of Southampton, SO16 6YD, United Kingdom.

Department of Mechanical and Aerospace Engineering (DIMA), Sapienza University of Rome, Via Eudossiana 18, 00184, Rome, Italy.

出版信息

Bioact Mater. 2024 Sep 23;43:114-128. doi: 10.1016/j.bioactmat.2024.09.007. eCollection 2025 Jan.

Abstract

Decellularized tissues offer significant potential as biological materials for tissue regeneration given their ability to preserve the complex compositions and architecture of the native extracellular matrix (ECM). However, the evaluation and derivation of decellularized matrices from human bone tissue remains largely unexplored. We examined how the physiochemical and biological properties of ECM hydrogels derived from human bone ECM could be controlled by manipulating bone powder size (45-250 μm, 250-1000 μm, and 1000-2000 μm) and ECM composition through modulation of enzyme digestion time (3-5-7 days). A reduction in material bone powder size and an increase in ECM digestion time produced enhanced protein concentrations in the ECM hydrogels, accompanied by the presence of a diverse array of proteins and improved gelation strength. Human bone marrow-derived stromal cells (HBMSCs) cultured on ECM hydrogels from 45 to 250 μm bone powder, over 7 days, demonstrated enhanced osteogenic differentiation compared to hydrogels derived from larger bone powders and collagen gels confirming the potential of the hydrogels as biologically active materials for bone regeneration. Digestion time and bone powder size modulation enabled the generation of hydrogels with enhanced release of ECM proteins and appropriate gelation and rheological properties, offering new opportunities for application in bone repair.

摘要

鉴于其能够保留天然细胞外基质(ECM)的复杂组成和结构,脱细胞组织作为用于组织再生的生物材料具有巨大潜力。然而,从人骨组织中评估和获取脱细胞基质在很大程度上仍未得到探索。我们研究了如何通过控制骨粉大小(45 - 250μm、250 - 1000μm和1000 - 2000μm)以及通过调节酶消化时间(3 - 5 - 7天)来控制ECM组成,从而调控源自人骨ECM的ECM水凝胶的物理化学和生物学特性。骨粉大小的减小和ECM消化时间的增加使ECM水凝胶中的蛋白质浓度提高,同时伴有多种蛋白质的存在以及凝胶化强度的改善。与源自较大骨粉的水凝胶和胶原凝胶相比,在45至250μm骨粉的ECM水凝胶上培养7天的人骨髓间充质干细胞(HBMSCs)表现出增强的成骨分化,证实了这些水凝胶作为骨再生生物活性材料的潜力。消化时间和骨粉大小的调节能够生成具有增强的ECM蛋白释放以及合适的凝胶化和流变学特性的水凝胶,为骨修复应用提供了新的机会。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4e47/11456876/3ba9aacf4325/ga1.jpg

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