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Methods to follow intracellular trafficking of cell-penetrating peptides

机译:遵循细胞渗透肽的细胞内运输方法

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Cell-penetrating peptides (CPPs) are efficient vehicles to transport bioactive molecules into the cells. Despite numerous studies the exact mechanism by which CPPs facilitate delivery of cargo to its intracellular target is still debated. The current work presents methods that can be used for tracking CPP/pDNA complexes through endosomal transport and show the role of endosomal transport in the delivery of cargo. Separation of endosomal vesicles by differential centrifugation enables to pinpoint the localization of delivered cargo without labeling it and gives important quantitative information about pDNA trafficing in certain endosomal compartments. Single particle tracking (SPT) allows following individual CPP/cargo complex through endosomal path in live cells, using fluoresently labled cargo and green fluoresent protein expressing cells. These two different methods show similar results about tested NickFect/pDNA complexes intracellular trafficing. NF51 facilitates rapid internalization of complexes into the cells, prolongs their stay in early endosomes and promotes release to cytosol. NF1 is less capable to induce endosomal release and higher amount of complexes are routed to lysosomes for degradation. Our findings offer potential delivery vector for in vivo applications, NF51, where endosomal entrapment has been allayed. Furthermore, these methods are valuable tools to study other CPP-based delivery systems.
机译:细胞穿透肽(CPP)是将生物活性分子传送到细胞中的有效载体。尽管众多研究了CPP促进货物到其细胞内目标的确切机制仍然讨论。目前的工作介绍了通过内体运输跟踪CPP / PDNA复合物的方法,并显示内体运输在货物交付中的作用。通过差动离心分离内体囊泡使能够定位递送的货物的定位而不标记,并在某些内体隔室中提供关于PDNA交通的重要定量信息。单个粒子跟踪(SPT)允许通过活细胞中的内体路径允许单独的CPP /货物复合物,使用来自荧光致密的货物和绿色氟化蛋白表达细胞。这两种不同的方法显示了关于测试的尼克综合细胞内交通的测试的类似结果。 NF51促进复合物的快速内化进入细胞中,延长其在早期的胚胎中并促进释放到细胞溶胶。 NF1能够诱导诱导内体释放,并且较高量的络合物对溶质剂进行降解。我们的调查结果为体内应用提供了潜在的交付载体,NF51已经取代了内体夹紧。此外,这些方法是研究其他基于CPP的递送系统的有价值的工具。

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