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Radiopacity endowed magnetic nanocomposite with hyperthermia and in vitro mineralization potential: a combinatorial therapeutic system for osteosarcoma

机译:辐射缺陷性具有高温和体外矿化潜力的磁性纳米复合材料:骨肉瘤的组合治疗系统

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The development of clinically advanced multifaceted therapeutic materials for osteosarcoma is at the forefront of cancer research. Accordingly, this work presents the design of a multifunctional magnetic nanocomposite composed of maghemite, strontium doped hydroxyapatite and silica nanoparticles prospectively holding indispensable therapeutic features such as magnetic hyperthermia, in vitro biomineralization, sustained drug release and intrinsic radiopacity for the treatment of osteosarcoma. The optimal composition has been identified by sequentially modulating the ratio of precursors of the magnetic nanocomposite synthesized by sol-gel technique. Structural and morphological characterization by x-ray diffraction, fourier transform infrared spectrum, Brunauer-Emmet-Teller and transmission electron microscopy analyses followed by VSM, hyperthermia and micro-CT analyses essentially assisted in the selective configuration of biofunctional properties. Results exemplify that MSHSr1 has a saturation magnetization of 47.4 emu g(-1) and attained hyperthermia temperature (42 degrees C) at a very low exposure time of 4 min. MSHSr1 is further unique with respect to its exceptional x-ray attenuation ability (contrast enhancement 154.5% in digital radiography; CT number 3100 HU), early biomimetic mineralization (in vitro) evident by the formation of spheroidal apatite layer (Ca/P ratio 1.33) harvested from FESEM-EDX analysis and controlled release of Doxorubicin, the clinically used chemotherapeutic drug: 87.7% at 120 h in tumour analogous pH (6.5) when compared to physiological pH (71.3% at 7.4). MTT assay complemented with cytoskeleton (F-actin) staining of human osteosarcoma (HOS) cells affirm biocompatibility of MSHSr1. In vitro biomineralization authenticated by Alizarin red S and von Kossa staining has been further corroborated by semi-quantitative calcium estimation of HOS cells cultured with MSHSr1 for two weeks. The results therefore validate the multifunctionality of MSHSr1, and hence could be proposed as a combinatorial therapeutic nanocomposite for osteosarcoma treatment.
机译:临床上先进的骨质瘤瘤治疗材料的开发是癌症研究的最前沿。因此,该工作介绍了由磁性热热磷灰石和二氧化硅纳米胺和二氧化硅纳米粒子组成的多功能磁性纳米复合材料的设计,例如磁性热热性,体外生物化,持续的药物释放,持续的药物释放,用于治疗骨肉瘤的不可或缺的药物释放。通过顺序调节通过溶胶技术合成的磁性纳米复合材料的前体的比例来鉴定最佳组合物。通过X射线衍射,傅里叶变换红外光谱,Brunauer-Emmet-kearer和透射电子显微镜分析,其次是VSM,热疗和微型CT分析的结构和形态学特性,基本上辅助生物功能性能的选择性配置。结果举例说明,MSHSR1具有47.4 emu g(-1)的饱和磁化强度,并在4分钟的非常低的曝光时间下实现高温温度(42℃)。 MSHSR1对其具有出色的X射线衰减能力(数码放射线照相中的造影154.5%; CT编号3100 HU),通过形成球形磷灰石层(CA / P比1.33 )从FeSem-EDX分析和受控释放的多柔比星,临床使用的化学治疗药:与生理pH(71.3%在7.4时)的肿瘤类似pH(6.5)中的120小时。 MTT测定与人骨瘤(HOS)细胞的细胞骨架(F-actin)染色相吻合MSHSR1的生物相容性。通过使用MSHSR1培养的肝细胞的半定量钙估计,通过茜素红S和von Kossa染色验证的体外生物矿化通过半定量钙估计两周。因此,结果验证了MSHSR1的多官能,因此可以提出作为骨肉瘤治疗的组合治疗纳米复合材料。

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