Intracellular Monitoring of AS1411 Aptamer by Time-Resolved Microspectrofluorimetry and Fluorescence Imaging

Time-resolved microspectrofluorimetry and fluorescence microscopy imaging—two complementary fluorescence techniques—provide important information about the intracellular distribution, level of uptake and binding/interactions inside living cell of the labeled molecule of interest. They were employed...

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Bibliographic Details
Published inJournal of fluorescence Vol. 25; no. 5; pp. 1245 - 1250
Main Authors Kočišová, Eva, Praus, Petr, Bok, Jiří, Bonneau, Stéphanie, Sureau, Franck
Format Journal Article
LanguageEnglish
Published New York Springer US 01.09.2015
Springer Verlag
Subjects
Analytical Chemistry
Aptamers, Nucleotide - metabolism
Base Sequence
Biochemistry
Bioengineering
Biological and Medical Physics
Biological Physics
Biomedical and Life Sciences
Biomedicine
Biophysics
Biotechnology
Cell Line, Tumor
Humans
Imaging
Intracellular Space - genetics
Intracellular Space - metabolism
Life Sciences
Microscopy, Fluorescence - methods
Oligodeoxyribonucleotides - genetics
Oligodeoxyribonucleotides - metabolism
Original Article
Physics
Spectrometry, Fluorescence - methods
Time Factors
Fluorescence microscopy imaging
Aptamer
AS1411 aptamer
Phase-modulation lifetime measurement
Intracellular fluorescence
intracellular fluorescence
phase modulation fluorescence lifetime 2
aptamer
micro imaging
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Summary:Time-resolved microspectrofluorimetry and fluorescence microscopy imaging—two complementary fluorescence techniques—provide important information about the intracellular distribution, level of uptake and binding/interactions inside living cell of the labeled molecule of interest. They were employed to monitor the “fate” of AS1411 aptamer labeled by ATTO 425 in human living cells. Confocal microspectrofluorimeter adapted for time-resolved intracellular fluorescence measurements by using a phase-modulation principle with homodyne data acquisition was employed to obtain emission spectra and to determine fluorescence lifetimes in U-87 MG tumor brain cells and Hs68 non–tumor foreskin cells. Acquired spectra from both the intracellular space and the reference solutions were treated to observe the aptamer localization and its interaction with biological structures inside the living cell. The emission spectra and the maximum emission wavelengths coming from the cells are practically identical, however significant lifetime lengthening was observed for tumor cell line in comparison to non–tumor one.
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ISSN:1053-0509
1573-4994
DOI:10.1007/s10895-015-1612-3