首页> 外文期刊>Bioconjugate Chemistry >Bioreducible Comb-Shaped Conjugates Composed of Secondary Amine and Hydroxyl Group-Containing Backbones and Disulfide-Linked Side Chains with Tertiary Amine Groups for Facilitating Gene Delivery
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Bioreducible Comb-Shaped Conjugates Composed of Secondary Amine and Hydroxyl Group-Containing Backbones and Disulfide-Linked Side Chains with Tertiary Amine Groups for Facilitating Gene Delivery

机译:可生物还原的梳状共轭物,由仲胺和含羟基的主链和二硫键连接的侧链与叔胺基组成,可促进基因传递

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Comb-shaped polymeric vectors (SS-PGEADMs) consisting of ethanolamine/cystamine-functionalized poly-(glycidyl methacrylate) (SS-PGEA-NH2) backbones and bioreducible poly((2-dimethyl amino)ethyl methacrylate) (PDMEAMA) side chains were prepared by a combination of the ring-opening reaction and atom transfer radical polymerization (ATRP). The SS-PGEA-NH2 backbones, which were prepared via the ring-opening reaction of the pendant epoxide groups of poly(glycidyl methacrylate) with the amine moieties of ethanolamine/cystamine, possess plentiful flanking secondary amine and hydroxyl groups and some flanking disulfide bond-containing cystmine derivatives. The primary amine groups of the cystamine derivatives were activated to produce bromoisobutylryl-terminated SS-PGEA (SS-PGEA-Br) as multifunctional initiators for subsequent ATRP of DMAEMA The resultant disulfide-linked short PDMEAMA side chains possess pendant tertiary amine groups and are biocleavable. Such SS-PGEADMs can effectively condense pDNA The cytotoxicity of SS-PGEADMs could be controlled by adjusting the grafting amount of PDMEAMA side chains. In comparison with the pristine SS-PGEA-NH2, the moderate introduction of PDMEAMA side chains can further enhance the gene transfection efficiency in different cell lines. The present approach to well-defined comb-shaped vectors with multifunctional groups could provide a versatile means for tailoring the functional structures of advanced gene/drug vectors.
机译:由乙醇胺/胱胺官能化的聚甲基丙烯酸缩水甘油酯(SS-PGEA-NH2)骨架和生物可还原的聚(甲基丙烯酸2-二甲基氨基乙酯)(PDMEAMA)侧链组成的梳状聚合物载体(SS-PGEADM)为通过开环反应和原子转移自由基聚合(ATRP)的组合制备。 SS-PGEA-NH2主链是通过聚甲基丙烯酸缩水甘油酯的侧基环氧基与乙醇胺/胱胺的胺基的开环反应制得的,具有丰富的侧链仲胺和羟基和一些侧链二硫键含胱氨酸衍生物。激活了胱胺衍生物的伯胺基团,生成了溴异丁基ryl端基的SS-PGEA(SS-PGEA-Br),作为随后DMAEMA的ATRP的多功能引发剂。 。这样的SS-PGEADM可以有效地缩合pDNA。可以通过调节PDMEAMA侧链的接枝量来控制SS-PGEADM的细胞毒性。与原始SS-PGEA-NH2相比,适度引入PDMEAMA侧链可以进一步提高不同细胞系中的基因转染效率。具有多功能基团的明确定义的梳形载体的本方法可以提供用于修饰高级基因/药物载体的功能结构的通用手段。

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