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用于细胞限制诱导早期成骨的图案化 PCL-胶原纳米纤维支架的制备。

Fabrication of micropatterned PCL-collagen nanofibrous scaffold for cellular confinement induced early osteogenesis.

机构信息

Biomaterials & Biomimetics Laboratory, School of Life Sciences, Central University of Gujarat, Gandhinagar 382030, Gujarat, India.

Department of Materials Science and Solar Energy Research Center MIBSOLAR University of Milano-Biococca, and INSTM Milano-Biococca Research Unit Via Cozzi 55, I-20125 Milano, Italy.

出版信息

Biomater Adv. 2024 Nov;164:213991. doi: 10.1016/j.bioadv.2024.213991. Epub 2024 Aug 10.

Abstract

The intricate interaction of the scaffold's architecture/geometry and with the cells is essential for tissue engineering and regenerative medicine. Cells sense their surrounding dynamic cues such as biophysical, biomechanical, and biochemical, and respond to them differently. Numerous studies have recently explored and reported the effect of contact guidance by culturing various types of cells on different types of micropatterned substrates such as microgrooves, geometric (square and triangle) micropattern, microstrips, micropatterned nanofibers. Amongst all of these micropatterned polymeric substrates; electrospun nanofibers have been regarded as a suitable substrate as it mimics the native ECM architectures. Therefore, in the present study; stencil-assisted electrospun Grid-lined micropatterned PCL-Collagen nanofibers (GLMPCnfs) were fabricated and its influence on the alignment and differentiation of pre-osteoblast cells (MC3T3-E1) was investigated. The randomly orientated Non-patterned PCL-Collagen nanofibers (NPPCnfs) were used as control. The patterns were characterized for their geometrical features such as area and thickness of deposition using surface profiler and scanning electron microscopy. A 61 % decrease in the overall area of GLMPCnfs as compared to the stencil area demonstrated the potential of electrofocusing phenomenon in the process of patterning electrospun nanofibers into various micron-scale structures. The MC3T3-E1 cells were confined and aligned in the direction of GLMPCnfs as confirmed by a high cellular aspect ratio (AR = 5.41), lower cellular shape index (CSI = 0.243), and cytoskeletal reorganization assessed through the F-actin filament immunocytochemistry (ICC) imaging. The aligned cells along the GLMPCnfs exhibited elevated alkaline phosphatase activity and enhanced mineralization. Furthermore, the gene expression profiling revealed upregulation of key osteogenic markers, such as ALP, OCN, OPN, COL1A1, and osteocyte markers DMP1, and SOST. Consequently, the research highlights the impact of GLMPCnfs on the cellular behaviour that results to the pre-osteoblast differentiation and the potential for stimulant-free early osteogenesis. These results offer an extensive understanding and mechanistic insight into how scaffold topography can be modified to influence cellular responses for effective bone regeneration strategies.

摘要

支架的结构/几何形状与细胞的复杂相互作用对于组织工程和再生医学至关重要。细胞感知周围的动态线索,如生物物理、生物力学和生物化学,并对此做出不同的反应。最近有许多研究探索并报道了在不同类型的微图案化基底上培养各种类型的细胞的接触导向的影响,例如微沟、几何(方形和三角形)微图案、微条、微图案化纳米纤维。在所有这些微图案化聚合物基底中;静电纺纳米纤维被认为是一种合适的基底,因为它模拟了天然 ECM 结构。因此,在本研究中;使用模板辅助静电纺丝制备了 Grid-lined 微图案化 PCL-胶原蛋白纳米纤维(GLMPCnfs),并研究了其对前成骨细胞(MC3T3-E1)的排列和分化的影响。使用随机取向的非图案化 PCL-胶原蛋白纳米纤维(NPPCnfs)作为对照。使用表面轮廓仪和扫描电子显微镜对图案进行了几何特征(如沉积面积和厚度)的表征。与模板面积相比,GLMPCnfs 的总面积减少了 61%,这表明在将静电纺纳米纤维图案化为各种微米级结构的过程中,电聚焦现象具有潜力。通过高细胞纵横比(AR=5.41)、低细胞形状指数(CSI=0.243)和通过 F-肌动蛋白丝免疫细胞化学(ICC)成像评估的细胞骨架重排,证实 MC3T3-E1 细胞被限制并沿 GLMPCnfs 排列。沿着 GLMPCnfs 排列的细胞表现出碱性磷酸酶活性的升高和矿化的增强。此外,基因表达谱分析显示关键成骨标志物(如 ALP、OCN、OPN、COL1A1 和骨细胞标志物 DMP1 和 SOST)的上调。因此,该研究强调了 GLMPCnfs 对细胞行为的影响,从而导致前成骨细胞分化,并为无刺激的早期成骨提供了潜力。这些结果提供了对支架形貌如何被修改以影响细胞反应以实现有效骨再生策略的广泛理解和机制见解。

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