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Attaching folic acid on gold nanoparticles using noncovalent interaction via different polyethylene glycol backbones and targeting of cancer cells

机译:通过不同的聚乙二醇骨架通过非共价相互作用将叶酸附着在金纳米颗粒上,并靶向癌细胞

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This article reports a simple one-step method of attaching folic acid (FA) to gold nanoparticles (AuNPs) and its fine tuning using different polyethylene glycol (PEG) backbones.PEG backbones used in this study are PEG-diamine with molecular weights 2000 (PAM2-2K) and 10,000 (PAM2-10K),PEG-tetramine with molecular weight 20,000 (PAM4-20K),and PEG-dithiol with molecular weight 2000 (PSH2-2K).The nanoconjugates were characterized with ultraviolet-visible spectroscopy,transmission electron microscopy (TEM),thermogravimetric analysis,Fourier transform infrared spectroscopy,inductively coupled plasma analysis,and radioactivity measurement with a scintillation counter.Attachment and release profiles of FAs from the nanoconjugates are done using ~3H-labelled FAs (~3FA).The binding of ~3FA follows the order Au-PAM4-20K > Au-PAM2-10K > Au-PAM2-2K > Au > Au-PSH2-2K,whereas its release profile follows the reverse order.Au-PAM4-20K-FA has been used for folate receptor (FR)-mediated targeting of AuNPs to cancer cells.Seven different cancer cell lines (SKOV-3,OVCAR-5,OV-202,OV-167,OPM-1,RPMI,and U266) were screened for expression of FRs.Among ovarian cancer cells,the expression pattern of FRs follows the order OV-167 > SKOV-3 > OV-202 > OVCAR-5,and multiple myeloma cell lines follow the order OPM-1 > U266 > RPMI.Intracellular uptakes of the nanoconjugates containing FA or no FA were monitored with digital optical photography and TEM.Quantitation of the internalization of nanoconjugates in different cell lines was determined by gold analysis with inductively coupled plasma.It is found that the uptake of the nanoconjugates correlates with FR expression.Maximum uptake is observed for OV-167,whereas it is minimum for OVCAR-5.TEM images of the cells treated with Au-PAM4-20K-FA confirm the endocytosis of the nanoconjugates.This study is an important step for targeted delivery of anticancer drugs as well as metal nanoparticles for targeted therapy,tumor imaging,and ablation exploiting the overexpression of FRs on cancer cells.
机译:本文报道了一种简单的一步法将叶酸(FA)附着在金纳米颗粒(AuNPs)上,并使用不同的聚乙二醇(PEG)骨架对其进行微调。本研究中使用的PEG骨架是分子量为2000的PEG-二胺。 PAM2-2K和10,000(PAM2-10K),分子量为20,000的PEG-四胺(PAM4-20K)和分子量为2000的PEG-二硫醇(PSH2-2K)。电子显微镜(TEM),热重分析,傅立叶变换红外光谱,电感耦合等离子体分析和具有闪烁计数器的放射性测量。使用〜3H标记的FAs(〜3FA)完成纳米复合物中FAs的附着和释放曲线。 〜3FA的结合遵循Au-PAM4-20K> Au-PAM2-10K> Au-PAM2-2K> Au> Au-PSH2-2K的顺序,而其释放曲线遵循相反的顺序.Au-PAM4-20K-FA具有被用于叶酸受体(FR)介导的AuN靶向筛选到癌细胞的Ps。筛选了7种不同的癌细胞系(SKOV-3,OVCAR-5,OV-202,OV-167,OPM-1,RPMI和U266)以表达FRs。在卵巢癌细胞中,其表达FRs的模式遵循OV-167> SKOV-3> OV-202> OVCAR-5的顺序,多发性骨髓瘤细胞系遵循OPM-1> U266> RPMI的顺序。监测含FA或不含FA的纳米复合物的细胞内吸收。用数字光学照相和TEM观察纳米偶联物在不同细胞系中的内在化程度,方法是通过电感耦合血浆的金分析确定,发现纳米偶联物的摄取与FR表达有关.OV-167的最大摄取Au-PAM4-20K-FA处理过的细胞的TEM图像证实了纳米缀合物的内吞作用。这项研究是靶向递送抗癌药物以及金属纳米粒子用于靶向治疗的重要步骤肿瘤的成像,消融FR在癌细胞上的过表达。

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