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      Functionalized tricyclic cytosine analogues provide nucleoside fluorophores with improved photophysical properties and a range of solvent sensitivities.

      Chemistry (Weinheim an Der Bergstrasse, Germany)
      Cytosine, analogs & derivatives, DNA, B-Form, analysis, Fluorescent Dyes, chemistry, Nucleic Acid Conformation, Nucleosides, Solvents

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          Abstract

          Tricyclic cytosines (tC and tC(O) frameworks) have emerged as a unique class of fluorescent nucleobase analogues that minimally perturb the structure of B-form DNA and that are not quenched in duplex nucleic acids. Systematic derivatization of these frameworks is a likely approach to improve on and diversify photophysical properties, but has not so far been examined. Synthetic methods were refined to improve on tolerance for electron-donating and electron-withdrawing groups, resulting in a series of eight new, fluorescent cytidine analogues. Photophysical studies show that substitution of the framework results in a pattern of effects largely consistent across tC and tC(O) and provides nucleoside fluorophores that are brighter than either parent. Moreover, a range of solvent sensitivities is observed, offering promise that this family of probes can be extended to new applications that require reporting on the local environment. Copyright © 2014 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.

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          Author and article information

          Journal
          24311229
          4020711
          10.1002/chem.201303410

          Chemistry
          Cytosine,analogs & derivatives,DNA, B-Form,analysis,Fluorescent Dyes,chemistry,Nucleic Acid Conformation,Nucleosides,Solvents

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