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Carboxyl-modified single-wall carbon nanotubes improve bone tissue formation in vitro and repair in an in vivo rat model

机译:羧基修饰的单壁碳纳米管可在体外改善骨骼组织的形成并在体内大鼠模型中进行修复

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摘要

The clinical management of bone defects caused by trauma or nonunion fractures remains a challenge in orthopedic practice due to the poor integration and biocompatibility properties of the scaffold or implant material. In the current work, the osteogenic properties of carboxyl-modified single-walled carbon nanotubes (COOH–SWCNTs) were investigated in vivo and in vitro. When human preosteoblasts and murine embryonic stem cells were cultured on coverslips sprayed with COOH–SWCNTs, accelerated osteogenic differentiation was manifested by increased expression of classical bone marker genes and an increase in the secretion of osteocalcin, in addition to prior mineralization of the extracellular matrix. These results predicated COOH–SWCNTs’ use to further promote osteogenic differentiation in vivo. In contrast, both cell lines had difficulties adhering to multi-walled carbon nanotube-based scaffolds, as shown by scanning electron microscopy. While a suspension of SWCNTs caused cytotoxicity in both cell lines at levels >20 μg/mL, these levels were never achieved by release from sprayed SWCNTs, warranting the approach taken. In vivo, human allografts formed by the combination of demineralized bone matrix or cartilage particles with SWCNTs were implanted into nude rats, and ectopic bone formation was analyzed. Histological analysis of both types of implants showed high permeability and pore connectivity of the carbon nanotube-soaked implants. Numerous vascularization channels appeared in the formed tissue, additional progenitor cells were recruited, and areas of de novo ossification were found 4 weeks post-implantation. Induction of the expression of bone-related genes and the presence of secreted osteopontin protein were also confirmed by quantitative polymerase chain reaction analysis and immunofluorescence, respectively. In summary, these results are in line with prior contributions that highlight the suitability of SWCNTs as scaffolds with high bone-inducing capabilities both in vitro and in vivo, confirming them as alternatives to current bone-repair therapies.
机译:由于支架或植入物材料的整合性和生物相容性较差,因此由外伤或不愈合骨折引起的骨缺损的临床管理仍是整形外科的挑战。在当前的工作中,在体内和体外研究了羧基修饰的单壁碳纳米管(COOH-SWCNTs)的成骨特性。当在喷有COOH-SWCNT的盖玻片上培养人成骨细胞和鼠类胚胎干细胞时,除了事先矿化细胞外基质外,经典骨标志物基因的表达增加和骨钙素的分泌增加表明了成骨分化的加速。这些结果表明,COOH-SWCNTs可用于进一步促进体内成骨分化。相比之下,如扫描电子显微镜所示,两种细胞系都难以粘附到基于多壁碳纳米管的支架上。尽管SWCNT的悬浮液在两种细胞系中均以> 20μg/ mL的水平引起细胞毒性,但从未从喷雾的SWCNT释放中达到这些水平,这保证了所采用的方法。在体内,将由脱矿质骨基质或软骨颗粒与SWCNT结合形成的人类同种异体移植物植入裸鼠,并分析异位骨的形成。两种类型植入物的组织学分析均显示,碳纳米管浸透的植入物具有较高的渗透性和孔连通性。在形成的组织中出现了许多血管形成通道,另外募集了祖细胞,并且在植入后4周发现了新生骨化区域。还通过定量聚合酶链反应分析和免疫荧光分别证实了诱导骨相关基因的表达和分泌骨桥蛋白。总而言之,这些结果与先前的研究结果相吻合,前者突出了SWCNT作为体外和体内具有高骨诱导能力的支架的适用性,证实了它们是当前骨修复疗法的替代品。

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