Carbon-13 nuclear magnetic resonance of 5-substituted uracils

Pd, Ellis; Rb, Dunlap; Al, Pollard; Seidman, Kurt; Ad, Cardin

doi:10.1021/ja00794a042

Cited by 51 publications

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“…The N-3, N-5 and N-6 substituted uridines and cytidines included in our present study shown 6(H-6) and 6(H-5) variations which closely parallel the substituent effects observed in the bases. The following upfield and downfield shifts of 6(H-6), relative to the unsubstituted nucleosides, are observed upon C-5 substitution : produced by base substitution reflect electron density changes originating in the C(5) = C(6) half of the pyrimidine itself, in accord with theoretical considerations, I3C nuclear magnetic resonance [34] and photoelectron spectroscopic measurements [35], which agree that uracil is not an aromatic system but that C(5)=C(6) must be regarded as a substituted ethylene or enamine unit. The nucleosides derived from methylated or halogenated uracil and cytosine may then be treated together with unsubstituted uridines and cytidines in the following discussion.…”

Section: Pyrimidine Structuresupporting

confidence: 64%

Pyrimidine Nucleosides in Solution

Follmann¹,

Pfeil²,

Witzel³

1977

European Journal of Biochemistry

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Proton magnetic resonance (PMR) spectra of 45 nucleoside and nucleotide derivatives of uracil, thymine, cytosine, 5-methylcytosine, and other substituted pyrimidines in water or dimethyl sulfoxide solutions have been analysed in order to correlate structure variations with molecular conformations and to gain insight into the nature of intramolecular forces which are responsible for the 'rigidity' of the molecules. Irrespective of thc structure of pyrimidine base and the absolute chemical shift values (6) the C(6)-H and, to a lesser degree, the C(5)-H and C(5)-CH3 resonances are shifted downfield by very similar amounts ( A S ) in the regular nucleosides or in the presence of charged or polar C-4' substituents. In detail, the following conformation-determining effects are seen.1. Ribose vs 2-deoxyribose substitution of a pyrimidine makes little difference for the chemical environment of base hydrogens but an intact pentofuranose ring (4'-0) and the exocyclic 5'-OH group are essential for a nucleoside to assume a specific conformation.2. Profound shielding or deshielding of H-6 by exocyclic nitrate, halogen, hydroxyl, phosphate, and carboxylate substituents indicates preference for the anti and gauche,gauche conformation ranges in all compounds except in the case of C-6 substitution.3. Halogen atoms and the hydroxyl group ( A 6 = 0.30 -0.40 ppm) interact with pyrimidine bases by induced polarisation of the C(5)=C(6) double bond, phosphate anions ( A 6 % 0.50 ppm) interact by the electrostatic attraction mechanism previously described, and in nucleoside 5'-carboxylates ( A 6 > 0.90 ppm) a hydrogen bond between -COO-and H-6 is formed.4. The deshielding effects caused by a 5'-OH group and monoanionic 5'-phosphate are similar ( A 6 % 0.35 -0.45 ppm), supporting the view that intramolecular rigidity of nucleosides and the nucleotide unit is not fundamentally different.This systematic survey, together with our previous studies of adenosine derivatives, provides a rationale for why the majority of both pyrimidine and purine nucleosides and nucleotides in solution exhibit closely comparable conformations, which in turn explain the group specificity of certain key enzymes in nucleic acid metabolism.Enzymes which act upon nucleosides or nucleotides usually show stringent specificities with respect to the conformation of the heterocyclic base, furanose moiety, and exocyclic hydroxyl or phosphate group of their substrates. For example, modified ribonucleotides in which the base deviates from a regular anti position are poor substrates of ribonucleases [l], RNA polymerase [2], or ribonucleotide reductase (H. Follmann and W. Ludwig, unpublished). 'H and13C nuclear magnetic resonance spectra are excellent tools to study This paper is part 3 of a series entitled Forces Stabilizing the Conformation of Nucleosides in Solution.Abbreviations. PMR, proton magnetic resonance. The IUPAC-IUB abbreviations are used for nucleic acid constituents. these three-dimensional structures in solutions, and in recent years have provided description...

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Section: Pyrimidine Structuresupporting

confidence: 64%

Pyrimidine Nucleosides in Solution

Follmann¹,

Pfeil²,

Witzel³

1977

European Journal of Biochemistry

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“…Compounds 2-16 were identified as lumichrome (2), 5) chrysoeriol (3), 6) genistein (4), 7) adenosine (5), 8) guanosine (6), 9) uracil (7), 10) acetovanillone (8), 11) vanillin (9), 11) vanillic acid (10), 12) 6-methoxy-benzoxazolinone (11), 13) stigmast-4-en-3-one (12), 14) b-sitosterol (13), 15) stigmasterol (14), 16) stigmastanone (15), 17) and 7a-hydroxysitosterol (16) 18) based on comparison of their NMR spectral data with published spectral data.…”

mentioning

confidence: 99%

Chemical Constituents of the Style of Zea mays L. with Glycation Inhibitory Activity

et al. 2007

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“…The calculations predict that almost 90% of the difference in the u + H electron density at the 6 position that occurs between uracil and 5-fluorouracil arises from the difference in electron density of the orbital. Table I also contains chemical shift data from CI3 N M R studies of the C(6) atom in uracil, thymine, 5-fluorouracil, and CF3U [43]. As the magnitude of the chemical shift decreases, the electron shielding at the C(6) atom is expected to decrease.…”

Section: Resultsmentioning

confidence: 99%

“…In a preliminary attempt to predict the relative susceptibility of uracil and substituted uracils to nucleophilic attack the magnitude of the total electron density at the 6 position has been considered [43]. From this point of view the INDO calculations and the N M R results predict that the susceptibility to nucleophilic attack of the C(6) atom in the molecules studied increases in the order 5-fluorouracil < thymine < uracil < CF,U.…”

Section: Resultsmentioning

confidence: 99%

Ultraviolet photoelectron studies of 5-trifluoromethyluracil: Electronic susceptibility of substituted uracils to nucleophilic attack

Peng

Lin

Shahbaz

et al. 2009

Int. J. Quantum Chem.

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U V photoelectron spectroscopy has been employed to investigate the electronic structure of 5-trifluoromethyluracil. Band assignments have been made by comparison with photoelectron results from uracil. thymine, 5-fluorouracil, and I-methyl-5-trifluoromethyluracil. Spectroscopically mcasured ionization potentials have also been compared with energy levels predicted by INDO molecular orbital (MO) calculations. The calculations predict the ordering and the spacing of the four uppermost orbitals in 5-trifluoromethyluracil with good accuracy. They also give a good reprcsentition of the shifts observed in the ionization potentials of these orbitals when spectra of uracil, thymine, 5-fluorouracil, 5-trifluoromethyluracil, and 1 -methyl-5-trifluoromethyluracil are compared.Descriptions of electronic structure provided by the photoelectron results and the INDO calculations have been examined in conjunction with results from kinetic and equilibrium studies of sulfite attack at thc 6 position of uracil and substituted uracils. Results of the comparison indicate that while rcsonance effects cause 5-fluorouracil to exhibit greater electron density at the 6 position than thymine or uracil. the order of reactivity is 5-fluorouracil1 uracil > thymine. The enhanced reactivity of 5-fluorouracil over that expected from considerations of electron density may be ascribed in part to inductive electron withdrawing effects of the F atom, which oppose resonance effects and which stabilize the transition state involved in the addition of an SO:-ion.

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Carbon-13 nuclear magnetic resonance of 5-substituted uracils

Cited by 51 publications

References 1 publication

Pyrimidine Nucleosides in Solution

Pyrimidine Nucleosides in Solution

Chemical Constituents of the Style of Zea mays L. with Glycation Inhibitory Activity

Ultraviolet photoelectron studies of 5-trifluoromethyluracil: Electronic susceptibility of substituted uracils to nucleophilic attack

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