Study of Cellular Uptake of Modified Oligonucleotides by Using Time-Resolved Microspectrofluorimetry and Florescence Imaging

P. Praus, E. Kočišová, P. Mojzeš, J. Štěpánek, F. Sureau
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引用次数: 2

Abstract

Fluorescence microimaging and homodyne phase-resolved confocal microspectrofluorimetry were used to monitor the transport of antisense oligonucleotide into cancer MCF7 cells and the subsequent intracellular distribution. Phosphorothioate analog of 15-mer oligoadenylate (dA15) labeled by ATTO 425 was complexed with 5,10,15,20-tetrakis (1-methyl-4-pyridyl) porphyrin (H2TMPyP4) as an uptake-mediating agent. Fluorescence lifetime data within a broad spectral range have revealed properties of both components inside the cell. H2TMPyP4 lifetime inside the cell is not influenced in this malignant cell line, while the lifetime of modified oligonucleotide was found to be slightly shortened.
用时间分辨显微荧光法和荧光成像技术研究修饰寡核苷酸的细胞摄取
采用荧光显微成像和同差相分辨共聚焦显微荧光法监测反义寡核苷酸在肿瘤MCF7细胞内的转运及细胞内分布。ATTO 425标记的15-聚寡腺苷酸(dA15)的硫代类似物与5,10,15,20-四(1-甲基-4-吡啶基)卟啉(H2TMPyP4)络合作为摄取介质。宽光谱范围内的荧光寿命数据揭示了细胞内两种成分的特性。在该恶性细胞系中,H2TMPyP4在细胞内的寿命不受影响,而修饰寡核苷酸的寿命略有缩短。
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