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The involvement of microtubules and actin filaments in the intracellular transport of non-viral gene delivery system.

机译:微管和肌动蛋白丝参与非病毒基因传递系统的细胞内运输。

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摘要

It is known that two cytoskeleton components, microtubules and actins filaments, are required for efficient endocytosis. The relative importance of these two components in the cellular uptake of 2-(dimethylamino)ethyl methacrylate (DMAEMA)-DNA polyplexes was investigated in this study by applying microtubule depolymerising agent, colchicine, and actin polymerising inhibitor, cytochalasin D, in a cell transfection study. The effect of colchicine on transfection efficiency of polyplexes was found to be a time-dependent phenomenon, whereby the level of gene expression was inhibited at early stage, presumably to the disruption of a transport of vesicles along microtubules by colchicine. As time progressed, the level of gene expression was significantly enhanced relative to the control, possibly due to the failure in transport of vesicles from endosomes to late lysosomes, or due to the breakdown of nuclear membrane when mitosis was arrested at metaphase by colchicine. On the other hand, transfection efficiency was significantly reduced at all time points by cytochalasin D, which is considered to primarily affects invagination of vesicles at the early stage of endocytosis by inhibiting actin polymerisation. Further investigation to identify the endocytotic route of DMAEMA polyplexes was conducted applying clathrin- and caveolae- pathways inhibitors in cell transfection study. The results indicate that DMAEMA polyplexes were internalized primarily through clathrin-mediated pathway, with a minor fraction possibly entering cells via a caveolae-mediated pathway.
机译:已知有效的胞吞作用需要两个细胞骨架成分,微管和肌动蛋白丝。在这项研究中,通过在细胞转染中应用微管解聚剂秋水仙碱和肌动蛋白聚合抑制剂细胞松弛素D,研究了这两种成分在甲基丙烯酸2-(二甲基氨基)乙基酯(DMAEMA)-DNA多聚体的细胞摄取中的相对重要性。研究。发现秋水仙碱对多聚体转染效率的影响是时间依赖性的现象,由此基因表达的水平在早期受到抑制,大概是秋水仙碱破坏了沿着微管的囊泡运输。随着时间的流逝,基因表达水平相对于对照显着提高,这可能是由于囊泡从内体向后期溶酶体的转运失败,或者是由于秋水仙碱将有丝分裂停在中期而使核膜破裂。另一方面,细胞松弛素D在所有时间点均显着降低了转染效率,细胞松弛素D被认为主要是通过抑制肌动蛋白的聚合作用而在内吞作用的早期阶段影响囊泡的内陷。在细胞转染研究中应用网格蛋白和小窝途径抑制剂进行了进一步的研究,以确定DMAEMA多聚体的内吞途径。结果表明,DMAEMA多聚体主要通过网格蛋白介导的途径内在化,而一小部分可能通过小窝介导的途径进入细胞。

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