Publication | Closed Access
Template-Directed Fluorogenic Oligonucleotide Ligation Using “Click” Chemistry: Detection of Single Nucleotide Polymorphism in the Human p53 Tumor Suppressor Gene
33
Citations
36
References
2013
Year
Single Nucleotide PolymorphismMolecular BiologyUpstream Oligonucleotide ProbeChemical BiologyTumor BiologyComplementary TemplateNucleic Acid ChemistryAntisense TherapyMolecular DiagnosticsRadiation OncologyBiochemistryOligonucleotideDna ReplicationCancer GeneticsAzide-modified OligonucleotideNatural SciencesCancer GenomicsMedicineGenome Editing
A novel nonfluorescent alkyne-modified coumarin phosphoramidite was synthesized and successfully incorporated into oligonucleotides, which were then used in highly efficient DNA interstrand cross-linking and ligation reactions via "click" chemistry. The template-directed fluorogenic ligation "click" chemistry reaction was used for single nucleotide polymorphism analysis, where the target DNA catalyzes the ligation of two nonfluorescent probes to generate a fluorescent product. The upstream oligonucleotide probe is a nonfluorescent alkyne-modified coumarin and the downstream probe is an azide-modified oligonucleotide. When bound to a fully complementary template, the oligonucleotides ligated to produce a fluorescent product with a fluorophore at the ligation point. Wild-type and mutant p53 alleles were used to demonstrate that template-directed fluorogenic oligonucleotide ligation is sequence-specific and is capable of single nucleotide discrimination under mild conditions, even without the removal of unreacted probes.
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