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电纺聚己内酯支架的基质结合骨细胞衍生细胞外囊泡功能化促进成骨细胞分化和矿化。

Functionalization of Electrospun Polycaprolactone Scaffolds with Matrix-Binding Osteocyte-Derived Extracellular Vesicles Promotes Osteoblastic Differentiation and Mineralization.

机构信息

Trinity Centre for Biomedical Engineering, Trinity Biomedical Sciences Institute, Trinity College Dublin, Dublin, Ireland.

Department of Mechanical, Manufacturing, and Biomedical Engineering, School of Engineering, Trinity College Dublin, Dublin, Ireland.

出版信息

Ann Biomed Eng. 2021 Dec;49(12):3621-3635. doi: 10.1007/s10439-021-02872-2. Epub 2021 Oct 18.

Abstract

Synthetic polymeric materials have demonstrated great promise for bone tissue engineering based on their compatibility with a wide array of scaffold-manufacturing techniques, but are limited in terms of the bioactivity when compared to naturally occurring materials. To enhance the regenerative properties of these materials, they are commonly functionalised with bioactive factors to guide growth within the developing tissue. Extracellular matrix vesicles (EVs) play an important role in facilitating endochondral ossification during long bone development and have recently emerged as important mediators of cell-cell communication coordinating bone regeneration, and thus represent an ideal target to enhance the regenerative properties of synthetic scaffolds. Therefore, in this paper we developed tools and protocols to enable the attachment of MLO-Y4 osteocyte-derived EVs onto electrospun polycaprolactone (PCL) scaffolds for bone repair. Initially, we optimize a method for the functionalization of PCL materials with collagen type-1 and fibronectin, inspired by the behaviour of matrix vesicles during endochondral ossification, and demonstrate that this is an effective method for the adhesion of EVs to the material surface. We then used this functionalization process to attach osteogenic EVs, collected from mechanically stimulated MLO-Y4 osteocytes, to collagen-coated electrospun PCL scaffolds. The EV-functionalized scaffold promoted osteogenic differentiation (measured by increased ALP activity) and mineralization of the matrix. In particular, EV-functionalised scaffolds exhibited significant increases in matrix mineralization particularly at earlier time points compared to uncoated and collagen-coated controls. This approach to matrix-based adhesion of EVs provides a mechanism for incorporating vesicle signalling into polyester scaffolds and demonstrates the potential of osteocyte derived EVs to enhance the rate of bone tissue regeneration.

摘要

合成聚合物材料在与广泛的支架制造技术兼容方面表现出了巨大的潜力,基于此,它们在骨组织工程中具有广阔的应用前景,但与天然材料相比,其生物活性有限。为了增强这些材料的再生性能,通常会用生物活性因子对其进行功能化处理,以引导组织内的生长。细胞外基质囊泡(EVs)在长骨发育过程中的软骨内骨化中起着重要作用,并且最近已成为协调骨再生的细胞间通讯的重要介质,因此代表了增强合成支架再生性能的理想目标。因此,在本文中,我们开发了工具和方案,以使 MLO-Y4 成骨细胞衍生的 EVs 附着到电纺聚己内酯(PCL)支架上,以用于骨修复。最初,我们受基质囊泡在软骨内骨化过程中的行为启发,优化了一种用胶原蛋白 I 型和纤连蛋白对 PCL 材料进行功能化的方法,证明这是一种将 EV 附着到材料表面的有效方法。然后,我们使用该功能化过程将从机械刺激的 MLO-Y4 成骨细胞中收集的成骨 EVs 附着到胶原蛋白涂覆的电纺 PCL 支架上。EV 功能化支架促进了成骨分化(通过增加碱性磷酸酶活性来衡量)和基质矿化。特别是,与未涂覆和涂覆胶原蛋白的对照相比,EV 功能化支架在早期时显示出基质矿化的显著增加。这种基于基质的 EV 附着方法为将囊泡信号纳入聚酯支架提供了一种机制,并证明了成骨细胞衍生的 EV 增强骨组织再生速度的潜力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4380/8671272/ea01146e05d6/10439_2021_2872_Fig1_HTML.jpg

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