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Multifunctional liposomal drug delivery with dual probes of magnetic resonance and fluorescence imaging

机译:多功能脂质体药物递送磁共振和荧光成像的双重探针

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Many liposomal drug carriers have shown great promise in the clinic. To ensure the efficient preclinical development of drug-loaded liposomes, the drug retention and circulation properties of these systems should be characterized. Iron oxide (Fe3O4) magnetic nanoparticles (MNPs) are used as T2 contrast agents in magnetic resonance imaging (MRI). Gold nanoclusters (GNCs) contain tens of atoms with subnanometer dimensions; they have very low cytotoxicity and possess superb red emitting fluorescent properties, which prevents in vivo background autofluorescence. The aim of this study was to develop dual imaging, nanocomposite, multifunctional liposome drug carriers (Fe3O4-GNCs) comprising MNPs of iron oxide and GNCs. First, MNPs of iron oxide were synthesized by co-precipitation. The MNP surfaces were modified with amine groups using 3-aminopropyltriethoxysilane (APTES). Second, GNCs were synthesized by reducing HAuCl4 center dot 3H(2)O with NaBH4 in the presence of lipoic acid (as a stabilizer and nanosynthetic template). The GNCs were grown by adsorption onto particles to control the size and stability of the resultant colloids. Subsequently, dual Fe3O4-GNCs imaging probes were fabricated by conjugating the iron oxide MNPs with the GNCs via amide bonds. Finally, liposome nanocarriers were used to enclose the Fe3O4-GNCs in an inner phase (liposome@Fe3O4-GNCs) by reverse phase evaporation. These nanocarriers were characterized by dynamic light scattering (DLS), fluorescence spectroscopy, X-ray diffraction (XRD), transmission electron microscopy (TEM), Fourier transform infrared (FT-IR) spectrophotometry, superconducting quantum interference device (SQUID), nuclear magnetic resonance (NMR) imaging and in vivo imaging systems (IVIS). These multifunctional liposomal drug delivery systems with dual probes are expected to prove useful in preclinical trials for cancer diagnosis and therapy.
机译:许多脂质体药物载体在临床上表现出很好的希望。为了确保药物脂质体的有效临床前发育,应表征这些系统的药物保留和循环性能。氧化铁(Fe3O4)磁性纳米颗粒(MNP)用作磁共振成像(MRI)中的T2造影剂。金纳米板(GNC)含有数十个原子,具有亚域尺寸;它们具有非常低的细胞毒性并具有精湛的红色发射荧光特性,这可防止体内背景自发荧光。本研究的目的是开发含有MnP的氧化铁和GNC的双成像,纳米复合材料,多功能脂质体药物载体(Fe3O4-GNC)。首先,通过共沉淀合成氧化铁的MNP。使用3-氨基丙基三乙氧基硅烷(Aptes)用胺基进行改性MNP表面。其次,通过在硫辛酸存在(作为稳定剂和纳米合成模板)存在下用NaBH 4减少Haucl4中心点3h(2)o来合成GNC。通过吸附到颗粒上以控制所得胶体的尺寸和稳定性的GNC。随后,通过通过酰胺键将氧化铁MNP与GNC缀合来制造双Fe3O4-GNCS成像探针。最后,使用脂质体纳米载体通过反相蒸发将Fe3O4-GNC包围内相(脂质体@ Fe 3 O 4 -GNC)。这些纳米载体的特征在于通过动态光散射(DLS),荧光光谱,X射线衍射(XRD),透射电子显微镜(TEM),傅里叶变换红外(FT-IR)分光光度法,超导量子干涉装置(鱿鱼),核磁共振(NMR)成像和体内成像系统(IVIS)。这些具有双重探针的多功能脂质体药物递送系统预计将在癌症诊断和治疗的临床前试验中证明。

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