Advancing Scaffold Architecture for Bone Tissue Engineering: A Comparative Study of 3D-Printed β-TCP Constructs in Dynamic Culture with pBMSC.

IF 5.2 3区 医学 Q1 ENGINEERING, BIOMEDICAL
Yannick M Sillmann, Ana M P Baggio, Pascal Eber, Benjamin R Freedman, Cynthia Liu, Youssef Jounaidi, Alexander Schramm, Frank Wilde, Fernando P S Guastaldi
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Abstract

Scaffold architecture is a key determinant of cell behavior and tissue regeneration in bone tissue engineering, yet the influence of pore size under dynamic culture conditions remains incompletely understood. This study aimed to evaluate the effects of scaffold pore size on osteogenic differentiation of porcine bone marrow-derived mesenchymal stem cells (pBMSCs) cultured in a rotational oxygen-permeable bioreactor system (ROBS). Three-dimensionally (3D) printed beta-tricalcium phosphate (β-TCP) scaffolds with pore sizes of 500 µm and 1000 µm were seeded with pBMSC and cultured for 7 and 14 days under dynamic perfusion conditions. Gene expression analysis revealed significantly higher levels of osteogenic markers (Runx2, BMP-2, ALP, Osx, Col1A1) in the 1000 µm group, particularly at the early time point, with the later-stage marker Osteocalcin (Ocl) rising faster and higher in the 1000 µm group, after a lower expression at 7 days. ALP activity assays corroborated these findings. Despite having lower mechanical strength, the 1000 µm scaffolds supported a homogeneous cell distribution and high viability across all regions. These results suggest that larger pore sizes enhance early osteogenic commitment by improving nutrient transport and fluid flow in dynamic culture. These findings also support the use of larger-pore scaffolds in bioreactor-based preconditioning strategies and underscore the clinical importance of promoting early osteogenic differentiation to reduce in vitro culture time, an essential consideration for the timely preparation of implantable grafts in bone tissue engineering.

推进骨组织工程支架结构:3d打印β-TCP结构与pBMSC动态培养的比较研究。
在骨组织工程中,支架结构是细胞行为和组织再生的关键决定因素,但孔隙大小在动态培养条件下的影响尚不完全清楚。本研究旨在评估支架孔径对猪骨髓间充质干细胞(pBMSCs)在旋转透氧生物反应器(ROBS)中培养成骨分化的影响。将孔径分别为500µm和1000µm的三维打印β-磷酸三钙(β-TCP)支架植入pBMSC,在动态灌注条件下培养7天和14天。基因表达分析显示,在1000µm组中,成骨标志物(Runx2、BMP-2、ALP、Osx、Col1A1)水平显著升高,尤其是在早期时间点,后期标志物骨钙素(Ocl)在1000µm组中上升更快更高,在7天后表达较低。ALP活性测定证实了这些发现。尽管机械强度较低,但1000µm支架支持均匀的细胞分布和在所有区域的高活力。这些结果表明,在动态培养中,较大的孔隙大小通过改善营养物质的运输和流体流动来促进早期成骨承诺。这些发现也支持了大孔支架在生物反应器预处理策略中的应用,并强调了促进早期成骨分化以减少体外培养时间的临床重要性,这是骨组织工程中及时制备可植入移植物的重要考虑因素。
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来源期刊
Journal of Functional Biomaterials
Journal of Functional Biomaterials Engineering-Biomedical Engineering
CiteScore
4.60
自引率
4.20%
发文量
226
审稿时长
11 weeks
期刊介绍: Journal of Functional Biomaterials (JFB, ISSN 2079-4983) is an international and interdisciplinary scientific journal that publishes regular research papers (articles), reviews and short communications about applications of materials for biomedical use. JFB covers subjects from chemistry, pharmacy, biology, physics over to engineering. The journal focuses on the preparation, performance and use of functional biomaterials in biomedical devices and their behaviour in physiological environments. Our aim is to encourage scientists to publish their results in as much detail as possible. Therefore, there is no restriction on the length of the papers. The full experimental details must be provided so that the results can be reproduced. Several topical special issues will be published. Scope: adhesion, adsorption, biocompatibility, biohybrid materials, bio-inert materials, biomaterials, biomedical devices, biomimetic materials, bone repair, cardiovascular devices, ceramics, composite materials, dental implants, dental materials, drug delivery systems, functional biopolymers, glasses, hyper branched polymers, molecularly imprinted polymers (MIPs), nanomedicine, nanoparticles, nanotechnology, natural materials, self-assembly smart materials, stimuli responsive materials, surface modification, tissue devices, tissue engineering, tissue-derived materials, urological devices.
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