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Enhancing the photoluminescence and cellular uptake of fluorescent carbon nanodots via cubosome lipid nanocarriers

机译:通过立方体脂质纳米载体增强荧光碳纳米点的光致发光和细胞摄取

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Carbon nanodots (C-dots) have attracted much attention for their use in the fields of bioimaging, drug delivery, and sensing due to their excellent fluorescent and photoluminescent properties, photostability, biocompatibility, and amenability to surface modification. Herein, we report a nanocomposite formulation of C-dots (<5 nm) encapsulated in lipid-based lyotropic liquid crystalline nanoparticles (∼250 nm) via either passive diffusion or electrostatic mechanisms. The physicochemical properties of the nanocomposite formulation including particle size, surface charge, internal cubic nanostructures, and pH-dependent fluorescent properties were characterised. Upon loading of C-dots into lipid nanoparticles, the highly ordered inverse bicontinuous cubic mesophase existed in the internal phase of the nanoparticles, demonstrated by synchrotron small angle X-ray scattering, molecular dynamic simulation and cryogenic transmission electron microscopy. The pH-dependent fluorescent property of the C-dots was modified via electrostatic interaction between the C-dots and cationic lipid nanoparticles, which further enhanced the brightness of C-dots through self-quenching prevention. The cytotoxicity and cellular uptake efficiency of the developed nanocomposites were also examined in an epithelial gastric adenocarcinoma cell line (AGS) and a macrophage cell line (stimulated THP-1). Compared to free C-dots, the uptake and cell imaging potential of the C-dot nanocomposites was significantly improved, by several orders of magnitude as demonstrated by cytoplasmic fluorescent intensities using confocal microscopy. Loading C-dots into mesoporous lipid nanocarriers presents a new way of modifying C-dot physicochemical and fluorescent properties, alternative to direct chemical surface modification, and advances the bioimaging potential of C-dots by enhancing cellular uptake efficiency and converging C-dot light emission.
机译:碳nanodots (C-dots)吸引了为他们的使用领域的关注bioimaging、药物输送和遥感由于他们的优秀的荧光和发光性能、耐光性、生物相容性和表面改性的顺从。报告的纳米复合材料配方C-dots (< 5海里)封装在lipid-based易溶的液体通过纳米晶体(∼250海里)被动扩散或静电机制。的物理化学性质纳米复合材料配方包括粒子大小、表面电荷、内部立方纳米结构和pH-dependent荧光属性特征。C-dots脂质纳米粒子,高度命令逆双连续立方中间相存在于内部的阶段纳米颗粒,证明了同步加速器小角x射线散射、分子动态模拟和低温透射电子显微镜。通过静电C-dots的修改C-dots和阳离子脂质之间的相互作用纳米颗粒,进一步增强亮度C-dots通过自灭预防。纳米复合材料开发的效率还研究了胃上皮腺癌细胞系(AGS)和巨噬细胞细胞系(刺激THP-1)。C-dots,吸收和细胞成像的潜力C-dot纳米复合材料是显著的改善,由好几个数量级证明了胞质荧光使用共焦显微镜强度。C-dots到介孔脂质人们提出了一种新的方式修改C-dot物理化学和荧光性质,选择直接化学表面bioimaging修改和进步的潜力C-dots通过提高细胞吸收效率和收敛C-dot发光。

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