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甘露糖基化树枝状大分子/α-环糊精共轭物介导的基因递送的改善

Improvement of gene delivery mediated by mannosylated dendrimer/alpha-cyclodextrin conjugates.

作者信息

Wada Koki, Arima Hidetoshi, Tsutsumi Toshihito, Chihara Yuko, Hattori Kenjiro, Hirayama Fumitoshi, Uekama Kaneto

机构信息

Graduate School of Pharmaceutical Sciences, Kumamoto University, 5-1 Oe-honmachi, Kumamoto 862-0973, Japan.

出版信息

J Control Release. 2005 May 18;104(2):397-413. doi: 10.1016/j.jconrel.2005.02.016. Epub 2005 Apr 26.

Abstract

The purpose of this study is to evaluate in vitro and in vivo gene delivery efficiency of polyamidoamine (PAMAM) starburst dendrimer (generation 2, G2) conjugate with alpha-cyclodextrin (alpha-CDE conjugate (G2)) bearing mannose (Man-alpha-CDE conjugates) with the various degrees of substitution of the mannose moiety (DSM) as a novel non-viral vector in a variety of cells. Man-alpha-CDE conjugates (DSM 3.3 and 4.9) were found to have much higher gene transfer activity than dendrimer, alpha-CDE conjugate and Man-alpha-CDE conjugates (DSM 1.1 and 8.3) in various cells, which are independent of the expression of cell surface mannose receptors. Cellular association of pDNA complexes with dendrimer, alpha-CDE conjugate and Man-alpha-CDE conjugate (DSM 3.3) and their cytotoxic effects differed only very slightly. Surface plasmon resonance study demonstrated that the specific binding activity of Man-alpha-CDE conjugates to concanavalin A was not very strong. Much more conjugation of the mannose moiety to alpha-CDE conjugates provided unfavorable physicochemical properties of pDNA complexes for gene transfer, e.g. the low interaction with pDNA, the low enzymatic stability of pDNA and the lack of pDNA compaction. Man-alpha-CDE conjugate (DSM 3.3) provided gene transfer activity higher than dendrimer and alpha-CDE conjugate in kidney 12 h after intravenous injection in mice. These results suggest the potential use of Man-alpha-CDE conjugate (DSM 3.3) as a non-viral vector.

摘要

本研究的目的是评估聚酰胺-胺(PAMAM)第2代星型树枝状聚合物(G2)与带有不同甘露糖取代度(DSM)的α-环糊精共轭物(α-CDE共轭物(G2))结合甘露糖(Man-α-CDE共轭物)作为新型非病毒载体在多种细胞中的体外和体内基因传递效率。发现在多种细胞中,Man-α-CDE共轭物(DSM 3.3和4.9)比树枝状聚合物、α-CDE共轭物以及Man-α-CDE共轭物(DSM 1.1和8.3)具有更高的基因转移活性,且这与细胞表面甘露糖受体的表达无关。pDNA复合物与树枝状聚合物、α-CDE共轭物以及Man-α-CDE共轭物(DSM 3.3)的细胞结合及其细胞毒性作用仅存在非常轻微的差异。表面等离子体共振研究表明,Man-α-CDE共轭物与伴刀豆球蛋白A的特异性结合活性不是很强。更多甘露糖部分与α-CDE共轭物的共轭作用为基因传递提供了不利于pDNA复合物的物理化学性质,例如与pDNA的低相互作用、pDNA的低酶稳定性以及缺乏pDNA压缩。在小鼠静脉注射12小时后,Man-α-CDE共轭物(DSM 3.3)在肾脏中的基因转移活性高于树枝状聚合物和α-CDE共轭物。这些结果表明Man-α-CDE共轭物(DSM 3.3)具有作为非病毒载体的潜在用途。

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