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首页> 外文期刊>Journal of Controlled Release: Official Journal of the Controlled Release Society >Protein kinase C alpha-specific peptide substrate graft-type copolymer for cancer cell-specific gene regulation systems
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Protein kinase C alpha-specific peptide substrate graft-type copolymer for cancer cell-specific gene regulation systems

机译:用于癌细胞特异性基因调控系统的蛋白激酶Cα特异性肽底物接枝型共聚物

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摘要

We recently proposed a novel gene regulation system responding to specifically and abnormally activated intracellular enzymes in diseased cells. In the present study, we focused on protein kinase C(PKC)alpha, which is hyper-activated in most tumor cells, as a trigger for transgene regulation. We prepared cationic copolymers comprising hydrophilic and neutral polymers in main chains and cationic peptide substrates with different contents in side chains. Our copolymer with high peptide content (>3 mol%) condensed with pDNA more weakly than with poly(L-lysine) (pLL) having a similar molecular weight, but gene suppression was nearly identical to that of pLL. probably due to the steric hindrance of the main chains in our copolymer. Steric hindrance of the main chains barely affected the phosphorylation reaction of the pendant peptide. In cell and mouse experiments, higher gene expression was observed in complexes of pDNA with copolymers pended PKC alpha-specific substrate peptide than that in complexes with negative copolymers pended peptide substituted phosphorylation site of serine residues with alanine. These results indicate that our system can recognize intracellular PKC alpha as a trigger to regulate transgene expression, and may be useful for tumor gene therapy.
机译:我们最近提出了一种新的基因调节系统,该系统可对患病细胞中特异性和异常激活的细胞内酶作出反应。在本研究中,我们集中于蛋白激酶C(PKC)alpha,它在大多数肿瘤细胞中被过度激活,作为转基因调控的触发。我们制备了在主链中包含亲水性和中性聚合物以及在侧链中具有不同含量的阳离子肽底物的阳离子共聚物。与具有相似分子量的聚L-赖氨酸(pLL)相比,我们的具有高肽含量(> 3 mol%)的共聚物与pDNA的缩合作用更弱,但基因抑制与pLL几乎相同。可能是由于共聚物中主链的空间位阻。主链的位阻几乎不影响侧链肽的磷酸化反应。在细胞和小鼠实验中,观察到pDNA与共轭PKCα特异性底物肽的共聚物中的基因表达高于与负共聚物共聚肽取代的丝氨酸残基与丙氨酸的磷酸化位点的基因表达。这些结果表明我们的系统可以识别细胞内PKCα作为调节转基因表达的触发因素,可能对肿瘤基因治疗有用。

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