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Theranostic liposomes loaded with quantum dots and apomorphine for brain targeting and bioimaging

机译:装有量子点和阿扑吗啡的神经治疗脂质体,用于脑靶向和生物成像

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Abstract: Quantum dots (QDs) and apomorphine were incorporated into liposomes to eliminate uptake by the liver and enhance brain targeting. We describe the preparation, physicochemical characterization, in vivo bioimaging, and brain endothelial cell uptake of the theranostic liposomes. QDs and the drug were mainly located in the bilayer membrane and inner core of the liposomes, respectively. Spherical vesicles with a mean diameter of ~140 nm were formed. QDs were completely encapsulated by the vesicles. Nearly 80% encapsulation percentage was achieved for apomorphine. A greater fluorescence intensity was observed in mouse brains treated with liposomes compared to free QDs. This result was further confirmed by ex vivo imaging of the organs. QD uptake by the heart and liver was reduced by liposomal incorporation. Apomorphine accumulation in the brain increased by 2.4-fold after this incorporation. According to a hyperspectral imaging analysis, multifunctional liposomes but not the aqueous solution carried QDs into the brain. Liposomes were observed to have been efficiently endocytosed into bEND3 cells. The mechanisms involved in the cellular uptake were clathrin- and caveola-mediated endocytosis, which were energy-dependent. To the best of our knowledge, our group is the first to develop liposomes with a QD-drug hybrid for the aim of imaging and treating brain disorders.
机译:摘要:将量子点(QDs)和阿扑吗啡掺入脂质体中,以消除肝脏的摄取并增强脑靶向性。我们描述了制备,理化特性,体内生物成像,和治疗性脂质体的脑内皮细胞摄取。量子点和药物主要位于脂质体的双层膜和内核中。形成平均直径约为140 nm的球形囊泡。 QD被囊泡完全包裹。阿扑吗啡的包封率接近80%。与游离QD相比,在用脂质体处理的小鼠大脑中观察到更大的荧光强度。通过器官的离体成像进一步证实了该结果。脂质体的掺入减少了心脏和肝脏对QD的吸收。合并后,阿扑吗啡在大脑中的积累增加了2.4倍。根据高光谱成像分析,多功能脂质体而不是水溶液将QD携带到大脑中。观察到脂质体已被有效内吞入bEND3细胞。参与细胞摄取的机制是网格蛋白和小窝介导的内吞作用,它们是能量依赖的。据我们所知,我们的团队是第一个开发具有QD-药物杂合体的脂质体,以成像和治疗脑部疾病的方法。

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