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脱细胞富血小板纤维蛋白负载锌掺杂磷酸镁支架的多尺度孔隙率在骨再生中的作用。

Effects of the multiscale porosity of decellularized platelet-rich fibrin-loaded zinc-doped magnesium phosphate scaffolds in bone regeneration.

机构信息

Department of Veterinary Surgery and Radiology, West Bengal University of Animal and Fishery Sciences, Kolkata, 700037, India.

School of Minerals, Metallurgical and Materials Engineering, Indian Institute of Technology Bhubaneswar, Argul, 752050, India.

出版信息

J Mater Chem B. 2024 Jun 19;12(24):5869-5883. doi: 10.1039/d3tb02981f.

Abstract

In recent years, metallic ion-doped magnesium phosphate (MgP)-based degradable bioceramics have emerged as alternative bone substitute materials owing to their excellent biocompatibility, bone-forming ability, bioactivity, and controlled degradability. Conversely, incorporating a biomolecule such as decellularized platelet-rich fibrin (d-PRF) on scaffolds has certain advantages for bone tissue regeneration, particularly in enhanced osteogenesis and angiogenesis. The present study focuses on the impact of d-PRF-loaded multiscale porous zinc-doped magnesium phosphate (Zn-MgP) scaffolds on biodegradability, biocompatibility, and bone regeneration. Scaffolds were fabricated through the powder-metallurgy route utilizing naphthalene as a porogen (porosity = 5-43%). With the inclusion of a higher porogen, a higher fraction of macro-porosity (>20 μm) and pore interconnectivity were observed. X-ray diffraction (XRD) studies confirmed the formation of the farringtonite phase. The developed scaffolds exhibited a minimum ultimate compressive strength (UCS) of 8.5 MPa (for 40 Naph), which lies within the range of UCS of the cancellous bone of humans (2-12 MPa). The assessment immersion in physiological fluid yielded a higher deposition of the calcium phosphate (CaP) compound in response to increased macro-porosity and interconnectivity (40 Naph). Cytocompatibility assessed using MC3T3-E1 cells showed that the incorporation of d-PRF coupled with increased porosity resulted the highest cell attachment, proliferation, and viability. For further evaluation, the developed scaffolds were implanted in rabbit femur condylar defects. Radiography, SEM, OTC labelling, and histology analysis after 2 months of implantation revealed the better invasion of mature osteoblastic cells into the scaffolds with enhanced angiogenesis and superior and accelerated healing of bone defects in d-PRF-incorporated higher porosity scaffolds (40 Naph). Finally, it is hypothesized that the combination of d-PRF incorporation with multiscale porosity and increased interconnectivity facilitated better bone-forming ability, good biocompatibility, and controlled degradability within and around the Zn-doped MgP scaffolds.

摘要

近年来,由于具有优异的生物相容性、成骨能力、生物活性和可控降解性,金属离子掺杂的磷酸镁(MgP)基可降解生物陶瓷已成为替代骨替代材料。相反,在支架上掺入生物分子如脱细胞富血小板纤维蛋白(d-PRF)对于骨组织再生具有一定的优势,特别是在增强成骨和血管生成方面。本研究重点研究了负载脱细胞富血小板纤维蛋白的多尺度多孔锌掺杂磷酸镁(Zn-MgP)支架对生物降解性、生物相容性和骨再生的影响。支架通过粉末冶金工艺利用萘作为造孔剂(孔隙率为 5-43%)制备。随着造孔剂含量的增加,观察到较大的宏观孔隙率(>20μm)和孔连通性的比例更高。X 射线衍射(XRD)研究证实了 farringtonite 相的形成。所开发的支架的最小极限抗压强度(UCS)为 8.5MPa(对于 40Naph),这处于人类松质骨的 UCS 范围内(2-12MPa)。在生理液中的评估表明,随着宏观孔隙率和连通性的增加,钙磷(CaP)化合物的沉积更高(40Naph)。使用 MC3T3-E1 细胞进行细胞相容性评估表明,d-PRF 的掺入与增加的孔隙率相结合,导致最高的细胞附着、增殖和活力。为了进一步评估,将开发的支架植入兔股骨髁缺损中。植入 2 个月后的射线照相、SEM、OTC 标记和组织学分析显示,具有更高孔隙率的掺入 d-PRF 的支架中成熟成骨细胞更好地侵入,血管生成增强,骨缺损的愈合更好且更快。最后,假设 d-PRF 掺入与多尺度孔隙率和增加的连通性相结合,促进了 Zn 掺杂 MgP 支架内和周围更好的成骨能力、良好的生物相容性和可控降解性。

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