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胶原蛋白包被的超弹性骨促进成骨细胞黏附与增殖。

Collagen-Coated Hyperelastic Bone Promotes Osteoblast Adhesion and Proliferation.

作者信息

Gresita Andrei, Raja Iman, Petcu Eugen, Hadjiargyrou Michael

机构信息

Department of Biomedical Sciences, College of Osteopathic Medicine, New York Institute of Technology, Old Westbury, NY 11568, USA.

Department of Biological & Chemical Sciences, New York Institute of Technology, Old Westbury, NY 11568, USA.

出版信息

Materials (Basel). 2023 Nov 1;16(21):6996. doi: 10.3390/ma16216996.

Abstract

Successfully reconstructing bone and restoring its dynamic function represents a significant challenge for medicine. Critical size defects (CSDs), resulting from trauma, tumor removal, or degenerative conditions, do not naturally heal and often require complex bone grafting. However, these grafts carry risks, such as tissue rejection, infections, and surgical site damage, necessitating the development of alternative treatments. Three-dimensional and four-dimensional printed synthetic biomaterials represent a viable alternative, as they carry low production costs and are highly reproducible. Hyperelastic bone (HB), a biocompatible synthetic polymer consisting of 90% hydroxyapatite and 10% poly(lactic-co-glycolic acid, PLGA), was examined for its potential to support cell adhesion, migration, and proliferation. Specifically, we seeded collagen-coated HB with MG-63 human osteosarcoma cells. Our analysis revealed robust cell adhesion and proliferation over 7 days in vitro, with cells forming uniform monolayers on the external surface of the scaffold. However, no cells were present on the core of the fibers. The cells expressed bone differentiation markers on days 3 and 5. By day 7, the scaffold began to degrade, developing microscopic fissures and fragmentation. In summary, collagen-coated HB scaffolds support cell adhesion and proliferation but exhibit reduced structural support after 7 days in culture. Nevertheless, the intricate 3D architecture holds promise for cellular migration, vascularization, and early osteogenesis.

摘要

成功重建骨骼并恢复其动态功能对医学来说是一项重大挑战。由创伤、肿瘤切除或退行性疾病导致的临界尺寸骨缺损(CSD)无法自然愈合,通常需要复杂的骨移植。然而,这些移植物存在组织排斥、感染和手术部位损伤等风险,因此需要开发替代治疗方法。三维和四维打印的合成生物材料是一种可行的替代方案,因为它们生产成本低且可高度复制。研究了超弹性骨(HB)这种由90%羟基磷灰石和10%聚乳酸-乙醇酸共聚物(PLGA)组成的生物相容性合成聚合物支持细胞黏附、迁移和增殖的潜力。具体而言,我们将MG-63人骨肉瘤细胞接种到胶原包被的HB上。我们的分析显示,在体外7天内细胞有强大的黏附和增殖能力,细胞在支架外表面形成均匀的单层。然而,纤维核心处没有细胞。细胞在第3天和第5天表达骨分化标志物。到第7天,支架开始降解,出现微观裂缝和破碎。总之,胶原包被的HB支架支持细胞黏附和增殖,但在培养7天后结构支撑能力下降。尽管如此,其复杂的三维结构在细胞迁移、血管生成和早期骨生成方面仍有前景。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3e30/10649997/06f6364ad123/materials-16-06996-g001.jpg

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