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Potential Use of Folate-polyethylene glycol (PEG)-Appended Dendrimer (G3) Conjugate with alpha-Cyclodextrin as DNA Carriers to Tumor Cells

机译:叶酸-聚乙二醇(PEG)附加的树状聚合物(G3)与α-环糊精结合作为肿瘤细胞DNA载体的潜在用途

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摘要

We previously reported that polyamidoamine STARBURST dendrimer (generation 3, G3) (dendrimer) conjugate with alpha-cyclodextrin (alpha-CyD) having an average degree of substitution of 2.4 of alpha-CyD (alpha-CDE) provided remarkable aspects as novel carriers for DNA and siRNA. To develop novel alpha-CDE derivatives with tumor cell specificity, we prepared folate-appended alpha-CDEs (Fol-alpha-CDEs) and folate-polyethylene glycol (PEG)-appended alpha-CDEs (Fol-PalphaCs) with the various degrees of substitution of folate (DSF), and evaluated in vitro and in vivo gene transfer activity, cytotoxicity, cellular association and physicochemical properties. In vitro gene transfer activity of Fol-alpha-CDEs (G3, DSF 2, 5 or 7) was lower than that of α-CDE (G3) in KB cells, folate receptor (FR)-overexpressing cancer cells. Of the three Fol-PalphaCs (G3, DSF 2, 5 or 7), Fol-PalphaC (G3, DSF 5) had the highest gene transfer activity in KB cells. The activity of Fol-PalphaC (G3, DSF 5) was significantly higher than that of alpha-CDE (G3) in KB cells, but not in A549 cells, FR-negative cells. Negligible cytotoxicity of the pDNA complex with Fol-PalphaC (G3, DSF 5) was observed in KB cells or A549 cells up to a charge ratio of 100/1 (carrier/pDNA). The cellular association of the pDNA complex with Fol-PalphaC (G3, DSF 5) could be mediated by FR on KB cells, resulting in its efficient cellular uptake. Fol-PalphaC (G3, DSF 5) had higher binding affinity with folate binding protein (FBP) than alpha-CDE (G3), although the physicochemical properties of pDNA complex with Fol-PalphaC (G3, DSF 5) were almost comparable to that with alpha-CDE (G3), although the onset charge ratio and the compaction ability of Fol-PalphaC (G3, DSF 5) were slightly different. Fol-PalphaC (G3, DSF 5) tended to show higher gene transfer activity than alpha-CDE (G3) 12 h after intratumoral administration in mice. These results suggest that Fol-PalphaC (G3, DSF 5), not Fol-alpha-CDEs, could be potentially used as a FR-overexpressing cancer cell-selective DNA carrier.
机译:我们先前曾报道,聚酰胺酰胺STARBURST树状大分子(第3代,G3)(树状大分子)与平均取代度为2.4的α-CyD(α-CDE)的α-环糊精(α-CyD)共轭物,为新型载体提供了引人注目的方面DNA和siRNA。为了开发具有肿瘤细胞特异性的新型α-CDE衍生物,我们制备了叶酸添加的α-CDE(Fol-alpha-CDEs)和叶酸添加的聚乙二醇(PEG)添加的α-CDE(Fol-PalphaCs),叶酸(DSF)的替代,并评估了体内和体外的基因转移活性,细胞毒性,细胞缔合和理化特性。在过表达叶酸受体(FR)的KB细胞中,Fol-alpha-CDEs(G3,DSF 2、5或7)的体外基因转移活性低于α-CDE(G3)。在三个Fol-PalphaC(G3,DSF 2、5或7)中,Fol-PalphaC(G3,DSF 5)在KB细胞中具有最高的基因转移活性。在KB细胞中,Fol-PalphaC(G3,DSF 5)的活性明显高于α-CDE(G3),但在A549细胞,FR阴性细胞中则没有。在KB细胞或A549细胞中,电荷比高达100/1(载体/ pDNA)时,观察到pDNA复合物与Fol-PalphaC(G3,DSF 5)的细胞毒性微不足道。 pDNA复合物与Fol-PalphaC(G3,DSF 5)的细胞缔合可以通过FR介导KB细胞来介导,从而有效吸收细胞。 Fol-PalphaC(G3,DSF 5)与叶酸结合蛋白(FBP)的结合亲和力高于alpha-CDE(G3),尽管带有Fol-PalphaC的pDNA复合物(G3,DSF 5)的理化性质几乎与之相当使用α-CDE(G3)时,尽管Fol-PalphaC(G3,DSF 5)的起始电荷比率和压实能力略有不同。小鼠肿瘤内给药后12小时,Fol-PalphaC(G3,DSF 5)倾向于表现出比α-CDE(G3)更高的基因转移活性。这些结果表明,Fol-PalphaC(G3,DSF 5),而不是Fol-alpha-CDEs,有可能被用作过表达FR的癌细胞选择性DNA载体。

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