In vitro DNA synthesis opposite oxazolone and repair of this DNA damage using modified oligonucleotides

doi:10.1093/nar/28.7.1555

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Nucleic Acids Research, 2000, Vol. 28, No. 7 1555-1563
© 2000 Oxford University Press

In vitro DNA synthesis opposite oxazolone and repair of this DNA damage using modified oligonucleotides

Victor Duarte, Didier Gasparutto, Michel Jaquinod¹ and Jean Cadet^*

Laboratoire des Lésions des Acides Nucléiques, Service de Chimie Inorganique et Biologique, Département de Recherche Fondamentale sur la Matière Condensée, UMR 5046, CEA Grenoble, 17 Rue des Martyrs, F-38054 Grenoble Cedex 9, France and ¹Laboratoire de Spectrométrie de Masse des Protéines, Institut de Biologie Structurale, 41 Rue des Martyrs, F-38027 Grenoble Cedex, France

Emphasis was placed in this work on the assessment of biologicalfeatures of 2,2,4-triaminooxazolone, a major one-electron and^·OH-mediated oxidation product of guanine. For this purpose,two oligonucleotides that contain a unique oxazolone residuewere synthesized. Herein we report the mutagenic potential ofoxazolone during in vitro DNA synthesis and its behavior towardsDNA repair enzymes. Nucleotide insertion opposite oxazolone,catalyzed by Klenow fragment exo^– and Taq polymerase indicatesthat the oxazolone lesion induces mainly dAMP insertion. Thissuggests that the formation of oxazolone in DNA may lead toG $->$ T transversions. On the other hand, oxazolone represents ablocking lesion when DNA synthesis is performed with DNA polymeraseß. Interestingly, DNA repair experiments carried out withformamidopyrimidine DNA N-glycosylase (Fpg) and endonucleaseIII (endo III) show that oxazolone is a substrate for both enzymes.Values of k_cat/K_m for the Fpg-mediated removal of oxidativeguanine lesions revealed that 8-oxo-7,8-dihydroguanine is onlya slightly better substrate than oxazolone. In the case of endoIII-mediated cleavage of modified bases, the present resultssuggest that oxazolone is a better substrate than 5-OHC, anoxidized pyrimidine base. Finally, MALDI-TOF-MS analysis ofthe DNA fragments released upon digestion of an oxazolone-containingoligonucleotide by Fpg gave insights into the enzymatic mechanismof oligonucleotide cleavage.

^* To whom correspondence should be addressed. Tel: +33 4 76 8849 87; Fax: +33 4 76 88 50 90; Email: cadet@drfmc.ceng.cea.fr

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