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首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >Transport, resealing, and re-poration dynamics of two-pulse electroporation-mediated molecular delivery
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Transport, resealing, and re-poration dynamics of two-pulse electroporation-mediated molecular delivery

机译:两脉冲电穿孔介导的分子递送的运输,重新密封和再穿孔动力学

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摘要

Electroporation is of interest for many drug-delivery and gene-therapy applications. Prior studies have shown that a two-pulse-electroporation protocol consisting of a short-duration, high-voltage first pulse followed by a longer, low-voltage second pulse can increase delivery efficiency and preserve viability. In this work the effects of the field strength of the first and second pulses and the inter-pulse delay time on the delivery of two different-sized Fluorescein-Dextran (FD) conjugates are investigated. A series of two-pulse-electroporation experiments were performed on 3T3-mouse fibroblast cells, with an alternating-current first pulse to permeabilize the cell, followed by a direct-current second pulse. The protocols were rationally designed to best separate the mechanisms of permeabilization and electrophoretic transport. The results showed that the delivery of FD varied strongly with the strength of the first pulse and the size of the target molecule. The delivered FD concentration also decreased linearly with the logarithm of the inter-pulse delay. The data indicate that membrane resealing after electropermeabilization occurs rapidly, but that a non-negligible fraction of the pores can be reopened by the second pulse for delay times on the order of hundreds of seconds. The role of the second pulse is hypothesized to be more than just electrophoresis, with a minimum threshold field strength required to reopen nano-sized pores or defects remaining from the first pulse. These results suggest that membrane electroporation, sealing, and re-poration is a complex process that has both short-term and long-term components, which may in part explain the wide variation in membrane-resealing times reported in the literature. (C) 2015 Elsevier B.V. All rights reserved.
机译:电穿孔对于许多药物递送和基因治疗应用是令人感兴趣的。先前的研究表明,由短时间的高电压第一脉冲,然后是较长的低电压第二脉冲组成的两脉冲电穿孔方案可以提高输送效率并保持活力。在这项工作中,研究了第一和第二脉冲的场强以及脉冲间延迟时间对两种不同尺寸的荧光素-右旋糖酐(FD)结合物递送的影响。在3T3小鼠成纤维细胞上进行了一系列的两脉冲电穿孔实验,首先用交流电使细胞通透,然后用直流电第二脉冲。该协议经过合理设计,可以最好地分离通透性和电泳转运的机制。结果表明,FD的传递随第一个脉冲的强度和目标分子的大小而变化很大。输送的FD浓度也随脉冲间延迟的对数线性下降。数据表明,电渗透后膜的重新密封迅速发生,但是第二脉冲可将不可忽略的孔部分重新打开,延迟时间约为数百秒。假设第二脉冲的作用不只是电泳,其具有重新打开纳米尺寸的孔或从第一脉冲残留的缺陷所需的最小阈值场强。这些结果表明,膜电穿孔,密封和再穿孔是一个复杂的过程,具有短期和长期两个方面,这可能部分解释了文献中报道的膜重封时间的广泛差异。 (C)2015 Elsevier B.V.保留所有权利。

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