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聚乙二醇化α-环糊精/聚酰胺-胺树枝状大分子的多假轮烷与环糊精作为 DNA 的缓释系统。

Polypseudorotaxanes of pegylated α-cyclodextrin/polyamidoamine dendrimer conjugate with cyclodextrins as a sustained release system for DNA.

机构信息

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

出版信息

Bioorg Med Chem. 2012 Feb 15;20(4):1425-33. doi: 10.1016/j.bmc.2011.12.060. Epub 2012 Jan 9.

DOI:10.1016/j.bmc.2011.12.060
PMID:22277591
Abstract

Nonviral gene delivery suffers from a number of limitations including short transgene expression times and low transfection efficiency. In this study, we examined whether polypseudorotaxanes (PPRXs) of polyethylene glycol (PEG, molecular weight: 2,000)-grafted α-cyclodextrin (α-CyD)/polyamidoamine dendrimer conjugate (PEG-α-CDE) with CyDs have the potential for the novel sustained release systems for plasmid DNA (pDNA). The PEG-α-CDE/pDNA complex formed PPRXs with α-CyD and γ-CyD solutions, but not with β-CyD solution. In the PEG-α-CDE/CyDs PPRX systems, 20.6mol of α-CyD and 11.8mol of γ-CyD were involved in the PPRXs formation with one PEG chain by α-CyD and γ-CyD, respectively, consistent with in the PEG-dendrimer/CyDs systems. PEG-α-CDE/pDNA/α-CyD PPRX and PEG-α-CDE/pDNA/γ-CyD PPRX formed hexagonal and tetragonal columnar channels in the crystalline phase, respectively. In addition, the CyDs PPRX provided the sustained release of pDNA from PEG-α-CDE complex with pDNA at least 72 h in vitro. The release of pDNA from CyDs PPRX retarded as the volume of dissolution medium decreased. Furthermore, the PEG-α-CDE/γ-CyD PPRX system showed sustained transfection efficiency after intramuscular injection to mice at least for 14days. These results suggest that the PEG-α-CDE/CyD PPRX systems are useful for novel sustained DNA release systems.

摘要

非病毒基因传递受到多种限制,包括转基因表达时间短和转染效率低。在这项研究中,我们研究了聚乙二醇(PEG,分子量:2000)接枝α-环糊精(α-CyD)/聚酰胺-胺树枝状大分子缀合物(PEG-α-CDE)与 CyD 的聚轮烷(PPRXs)是否具有质粒 DNA(pDNA)新型持续释放系统的潜力。PEG-α-CDE/pDNA 复合物与 α-CyD 和 γ-CyD 溶液形成 PPRXs,但不与β-CyD 溶液形成 PPRXs。在 PEG-α-CDE/CyDs PPRX 系统中,20.6mol 的 α-CyD 和 11.8mol 的 γ-CyD 分别与一个 PEG 链结合形成 PPRXs,与 PEG-树枝状大分子/CyDs 系统一致。PEG-α-CDE/pDNA/α-CyD PPRX 和 PEG-α-CDE/pDNA/γ-CyD PPRX 分别在结晶相中形成六方和四方柱状孔道。此外,CyD PPRX 提供了 PEG-α-CDE 复合物与 pDNA 的 pDNA 的持续释放,至少在体外 72 小时。随着溶解介质体积的减少,pDNA 的释放从 CyD PPRX 中延迟。此外,PEG-α-CDE/γ-CyD PPRX 系统在向小鼠肌肉内注射后至少 14 天内显示出持续的转染效率。这些结果表明,PEG-α-CDE/CyD PPRX 系统是新型持续 DNA 释放系统的有用工具。

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