Uptake and quantification of intracellular concentration of lipophilic pro-oligonucleotides in HeLa cells.

J. Bologna, E. Vivés, J. Imbach, F. Morvan
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引用次数: 24

Abstract

Several lipophilic prodrugs of oligonucleotides (T12 and T20) bearing enzymolabile protecting groups and labeled with fluorescein were synthesized. Their cellular uptake was studied by three different approaches using fluorescence: fluorescence microscopy, flow cytometry and spectrofluorometry. The corresponding prooligonucleotides (pro-oligos) were rapidly and efficiently taken up by HeLa cells and were found homogeneously in the cytoplasm and in the nucleus. The uptake was proportional to their relative lipophilicity and likely proceeded through a passive diffusion mechanism. Uptake followed a dose-response curve. This prooligo approach led to a 2-log increase of uptake in comparison with a T20 phosphorothioate oligonucleotide. Finally, an intracellular concentration of pro-oligo was estimated between 4 and 6 microM for an external concentration of 1 microM and up to 27 microM for an incubation at 10 microM.
HeLa细胞中亲脂性前寡核苷酸的摄取和细胞内浓度的定量。
合成了几种具有酶促保护基团并以荧光素标记的寡核苷酸(T12和T20)亲脂性前药。他们的细胞摄取研究了三种不同的方法使用荧光:荧光显微镜,流式细胞术和荧光光谱法。相应的前寡核苷酸(pro-oligos)被HeLa细胞快速有效地吸收,并均匀地存在于细胞质和细胞核中。摄取与它们的相对亲脂性成正比,并可能通过被动扩散机制进行。摄取遵循剂量-反应曲线。与T20硫代寡核苷酸相比,这种原寡核苷酸的摄取增加了2倍。最后,细胞内的前寡核苷酸浓度估计在1微米的外部浓度为4至6微米之间,在10微米的孵育下高达27微米。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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