Charge-driven tripod somersault on DNA for ratiometric fluorescence imaging of small molecules in the nucleus

Although fluorescence tracing of small bioactive molecules in living cells has been extensively studied, it is still a challenging task to detect their variations in the nucleus mainly due to the impermeable nuclear membrane and nucleic acid interference. Herein, we take advantage of the nucleic aci...

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Published inChemical science (Cambridge) Vol. 1; no. 43; pp. 153 - 164
Main Authors Wang, Kang-Nan, Cao, Qian, Liu, Liu-Yi, Zhao, Zi-Jian, Liu, Wenting, Zhou, Dan-Jie, Tan, Cai-Ping, Xia, Wei, Ji, Liang-Nian, Mao, Zong-Wan
Format Journal Article
LanguageEnglish
Published CAMBRIDGE Royal Soc Chemistry 21.11.2019
Royal Society of Chemistry
Subjects
Binding
Biocompatibility
Biological activity
Chemistry
Chemistry, Multidisciplinary
Crystallography
Deoxyribonucleic acid
Derivatives
DNA
Fluorescent indicators
Imaging
Physical Sciences
Science & Technology
Selectivity
Strategy
Titration
Toxicity
Tracing
SO2 DERIVATIVES
OXIDATIVE STRESS
LIVE-CELL
HYDROGEN-PEROXIDE
SENSORS
BISULFITE
PROBE
SULFUR-DIOXIDE DERIVATIVES
LIVING CELLS
SULFIDE
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Summary:Although fluorescence tracing of small bioactive molecules in living cells has been extensively studied, it is still a challenging task to detect their variations in the nucleus mainly due to the impermeable nuclear membrane and nucleic acid interference. Herein, we take advantage of the nucleic acid enriched environment in the nucleus to establish a strategy, named "charge-driven tripod somersault on DNA", for ratiometric fluorescence imaging of small bioactive molecules in the nucleus. Taking SO 2 derivatives as a typical target analyte, a tripodal probe has been constructed by conjugating two DNA binding groups containing a SO 2 derivative reaction site. Mechanism studies demonstrate that upon encountering and reacting with SO 3 2− /HSO 3 − , a charge variation occurs at the responsive arm of the tripodal probe, triggering a tripod somersault on DNA, resulting in the conformational rearrangement of the DNA binding modes with DNA-modulated fluorescence change, which allows the second emission feature to emerge. In this strategy, probe-DNA binding is not influenced by RNA or non-specific protein association, thus making it ideal for tracing nucleus-localized analytes. The application of this strategy has realized both in vitro and in vivo ratiometric fluorescence imaging of the variations of endogenous SO 2 derivatives in the nucleus for the first time, with high specificity and selectivity. Also, in theory, this strategy opens up a new avenue for the design of fluorescence probes for the nucleus-localized biological analytes. We have developed a strategy "charge-driven tripod somersault on DNA" realizing both in vitro and in vivo ratiometric fluorescence imaging of the variations of endogenous SO 2 derivatives in the nucleus for the first time.
Bibliography:For ESI and crystallographic data in CIF or other electronic format see DOI
1893794
Electronic supplementary information (ESI) available: Synthesis and characterization; DNA titration experiments, cytotoxicity of probes, and so on. CCDC
10.1039/c9sc03594j
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SourceType-Scholarly Journals-1
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ISSN:2041-6520
2041-6539
DOI:10.1039/c9sc03594j