Micro-Nanostructured Polymeric Scaffolds for Bone Tissue Engineering.

Sama Abdulmalik, Suranji Wijekoon, Khadija Basiru Danazumi, Sai Sadhananth Srinivasan, Laxmi Vobbineni, Elifho Obopilwe, Sangamesh G Kumbar
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Abstract

While bone tissue allograft and autograft are commonly used in bone healing, their application is limited by factors such as availability, donor site morbidity, and immune response to the grafted tissue. Tissue-engineered implants, such as acellular or cellular polymeric structures, offer a promising alternative, and are a current trend in tissue engineering. Leveraging recent advancements in bone tissue engineering (BTE), we utilize 3D printing to develop biodegradable scaffolds that combine mechanical strength and bioactivity to facilitate bone repair and regeneration. This study focuses on the design and fabrication of mechanically competent 3D printed poly (L-lactic acid) (PLLA) micro-structured scaffolds. These scaffolds are enhanced with collagen type I nanofibrils to create bioactive scaffolds that promote tissue regeneration. The performance of these mechanically competent, micro-nanostructured polymeric matrices, in combination with bone marrow stromal cells (BMSCs), is evaluated in PLLA and PLLA-collagen scaffolds. The resulting micro-nanostructured PLLA-Collagen scaffolds mimic trabecular bone architecture, mechanical strength, and the extracellular matrix environment found in native bone tissue. The composite PLLA-collagen scaffolds exhibit mechanical properties in the mid-range of human trabecular bone. Both PLLA and PLLA-Collagen scaffolds support human BMSCs adhesion, proliferation, and osteogenic differentiation. A significantly higher number of implanted host cells are distributed in the PLLA-Collagen scaffolds with greater bone density, more uniform cell distribution, and attachment compared to the PLLA microstructure. Additionally, the biomimetic collagen nanostructure potently induces osteogenic transcription evidenced by increased alkaline phosphatase activity and upregulation of bone markers such as sialoprotein and collagen type I, ultimately guiding stem cell-mediated formation of a mature, mineralized bone matrix throughout the interconnected scaffold pores. This study underscores the benefits of micro-nanostructured scaffolds in successfully generating the inductive microenvironment of native bone extracellular matrix, triggering the cascade of cellular events required for functional bone regeneration, repairing critical-sized bone defects, and ultimately serving as an alternative material platform for bone regeneration, thereby instilling confidence in the potential of our research.

用于骨组织工程的微纳米结构聚合物支架。
同种异体骨组织和自体骨组织通常用于骨愈合,但它们的应用受到诸如可获得性、供体部位发病率和对移植物组织的免疫反应等因素的限制。组织工程植入物,如无细胞或细胞聚合物结构,提供了一个有前途的选择,是当前组织工程的趋势。利用骨组织工程(BTE)的最新进展,我们利用3D打印开发可生物降解的支架,结合机械强度和生物活性,促进骨修复和再生。本研究的重点是机械能力的3D打印聚乳酸(PLLA)微结构支架的设计和制造。这些支架与I型胶原纳米原纤维增强,形成促进组织再生的生物活性支架。这些具有机械性能的微纳米结构聚合物基质与骨髓基质细胞(BMSCs)结合,在PLLA和PLLA-胶原支架中进行了性能评估。由此产生的微纳米结构pla -胶原支架模拟小梁骨结构、机械强度和天然骨组织中的细胞外基质环境。pla -胶原复合支架在人小梁骨的中等范围内表现出力学性能。PLLA和PLLA-胶原支架均支持人骨髓间充质干细胞粘附、增殖和成骨分化。植入的宿主细胞数量明显高于PLLA- collagen支架,其骨密度更大,细胞分布更均匀,附着性更强。此外,仿生胶原纳米结构可以通过碱性磷酸酶活性的增加和唾液蛋白和I型胶原等骨标志物的上调来诱导成骨转录,最终引导干细胞介导的成熟矿化骨基质在相互连接的支架孔中形成。本研究强调了微纳米结构支架在成功产生天然骨细胞外基质诱导微环境,触发功能性骨再生所需的细胞事件级联,修复临界尺寸骨缺陷,最终作为骨再生的替代材料平台方面的益处,从而为我们的研究潜力注入了信心。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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