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Preparation and characterization of folate conjugated N-trimethyl chitosan nanoparticles as protein carrier targeting folate receptor: in vitro studies

机译:叶酸偶联的N-三甲基壳聚糖纳米粒的制备及表征作为靶向叶酸受体的蛋白载体:体外研究

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Folate conjugated N-trimethyl chitosan (folate-TMC) was synthesized and characterized using Fourier transform infrared (FTIR) and H spectroscopy. The fluorescein isothiocyanate conjugated bovine serum albumin (FITC-BSA) loaded TMC-nanoparticle (FB-TMC-NP) and FITC-BSA loaded folate-TMC-nanoparticle (FB-f-TMC-NP) were prepared by ionic cross-linking of TMC or folate-TMC with sodium alginate. Single factor analysis method was used to optimize the formulation of nanoparticles. The encapsulating efficiencies of FB-TMC-NP and FB-f-TMC-NP produced by optimal formulation were 98.3+-1.9% and 98.7+-2.7% (n=3), respectively. In addition, the mean diameters of FB-TMC-NP and FB-f-TMC-NP were 184.3 +-8.3 nm and 176.1 +-5.0 nm (n = 3), respectively. Transmission electron microscope (TEM) showed that the nanoparticles were of spherical shapes. The intracellular uptake of FB-f-TMC-NP by SKOV3 cells (folate receptor overexpressing cells) was 3.7-fold more than that of FB-TMC-NP and could be inhibited by the presence of 1 mM folate in the culture medium, although there was no significant difference between the intracellular uptake of FB-f-TMC-NP in A549 cells (folate receptor-deficient cells) and that of FB-TMC-NP in the same cells. In conclusion, the enhancement of cellular uptake of FB-f-TMC-NP by SKOV3 cells in a specific way was attributed to the folate receptor-mediated endocytosis. FB-TMC-NP was a promising carrier for protein.
机译:合成了叶酸共轭N-三甲基壳聚糖(folate-TMC),并使用傅里叶变换红外(FTIR)和H光谱进行了表征。通过离子交联制备负载了异硫氰酸荧光素的荧光素偶联牛血清白蛋白(FITC-BSA)和负载了叶酸-TMC纳米颗粒(FB-f-TMC-NP)的TMC-纳米颗粒。 TMC或叶酸-TMC与海藻酸钠。使用单因素分析方法来优化纳米颗粒的配方。通过最佳配方生产的FB-TMC-NP和FB-f-TMC-NP的包封效率分别为98.3 + -1.9%和98.7 + -2.7%(n = 3)。此外,FB-TMC-NP和FB-f-TMC-NP的平均直径分别为184.3±-8.3 nm和176.1±-5.0 nm(n = 3)。透射电子显微镜(TEM)显示纳米颗粒为球形。尽管SKOV3细胞(叶酸受体过表达细胞)对FB-f-TMC-NP的细胞内摄取比FB-TMC-NP高3.7倍,但培养基中1 mM叶酸的存在可以抑制该摄取。 A549细胞(叶酸受体缺陷型细胞)中的FB-f-TMC-NP的细胞内摄取与相同细胞中的FB-TMC-NP的细胞内摄取之间没有显着差异。总之,SKOV3细胞以特定方式增强细胞对FB-f-TMC-NP的吸收归因于叶酸受体介导的内吞作用。 FB-TMC-NP是有前途的蛋白质载体。

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