How protonation and deprotonation of 9-methylguanine alter its singlet O sub(2) addition path: about the initial stage of guanine nucleoside oxidation

How protonation and deprotonation of 9-methylguanine alter its singlet O sub(2) addition path: about the initial stage of guanine nucleoside oxidation

Mutagenicity of singlet O sub(2) is due to its oxidatively generated damage to the guanine nucleobases of DNA. Oxidation of neutral guanosine has been assumed to be initiated by the formation of a transient 4,8-endoperoxide viaa Diels-Alder cycloaddition of singlet O sub(2). Protonation and deproton...

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Veröffentlicht in:Physical chemistry chemical physics : PCCP 2016-06, Vol.18 (22), p.15223-15234
Hauptverfasser: Lu, Wenchao, Teng, Huayu, Liu, Jianbo
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Sprache:eng
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Cycloaddition
Damage
Guanines
Guanosines
Mathematical models
Nucleosides
Oxidation
Protonation
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Teng, Huayu
Liu, Jianbo
description Mutagenicity of singlet O sub(2) is due to its oxidatively generated damage to the guanine nucleobases of DNA. Oxidation of neutral guanosine has been assumed to be initiated by the formation of a transient 4,8-endoperoxide viaa Diels-Alder cycloaddition of singlet O sub(2). Protonation and deprotonation of guanosine represent another factor related to DNA damage and repair. Herein, 9-methylguanine was utilized as a model substrate to mimic the correlation between singlet O sub(2) oxidation of the nucleoside and its ionization states, both in the absence and in the presence of water ligands. We used guided-ion-beam scattering tandem mass spectrometry to detect and quantify transient intermediates at room temperature. To provide a reliable description of reaction potential surfaces, different levels of theory including restricted and unrestricted density functional theory, CCSD(T), MP2, and multi-reference CASSCF and CASMP2 were applied. By means of molecular potential, kinetic and direct dynamics simulations, two reaction pathways were identified and neither follows the mechanism for neutral guanosine. Singlet O sub(2) oxidation of protonated 9-methylguanine begins by a concerted cycloaddition; but it is mediated by a 5,8-endoperoxide. By contrast, a concerted cycloaddition does not occur for deprotonated 9-methylguanine. The latter involves a stepwise addition starting with the formation of an 8-peroxide, which subsequently evolves to a 4,8-endoperoxide. This dichotomy implies that acidic and basic media may lead to different chemistries for guanosine oxidation in aqueous solutions, starting from initial stage. The comparison with oxidation of protonated/deprotonated guanine illustrates the different mechanisms and products and particularly the suppressed oxidizability of 9-methylguanine vs.free guanine.
doi_str_mv 10.1039/c6cp01350c
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Oxidation of neutral guanosine has been assumed to be initiated by the formation of a transient 4,8-endoperoxide viaa Diels-Alder cycloaddition of singlet O sub(2). Protonation and deprotonation of guanosine represent another factor related to DNA damage and repair. Herein, 9-methylguanine was utilized as a model substrate to mimic the correlation between singlet O sub(2) oxidation of the nucleoside and its ionization states, both in the absence and in the presence of water ligands. We used guided-ion-beam scattering tandem mass spectrometry to detect and quantify transient intermediates at room temperature. To provide a reliable description of reaction potential surfaces, different levels of theory including restricted and unrestricted density functional theory, CCSD(T), MP2, and multi-reference CASSCF and CASMP2 were applied. By means of molecular potential, kinetic and direct dynamics simulations, two reaction pathways were identified and neither follows the mechanism for neutral guanosine. Singlet O sub(2) oxidation of protonated 9-methylguanine begins by a concerted cycloaddition; but it is mediated by a 5,8-endoperoxide. By contrast, a concerted cycloaddition does not occur for deprotonated 9-methylguanine. The latter involves a stepwise addition starting with the formation of an 8-peroxide, which subsequently evolves to a 4,8-endoperoxide. This dichotomy implies that acidic and basic media may lead to different chemistries for guanosine oxidation in aqueous solutions, starting from initial stage. 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By means of molecular potential, kinetic and direct dynamics simulations, two reaction pathways were identified and neither follows the mechanism for neutral guanosine. Singlet O sub(2) oxidation of protonated 9-methylguanine begins by a concerted cycloaddition; but it is mediated by a 5,8-endoperoxide. By contrast, a concerted cycloaddition does not occur for deprotonated 9-methylguanine. The latter involves a stepwise addition starting with the formation of an 8-peroxide, which subsequently evolves to a 4,8-endoperoxide. This dichotomy implies that acidic and basic media may lead to different chemistries for guanosine oxidation in aqueous solutions, starting from initial stage. 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source Royal Society Of Chemistry Journals 2008-; Alma/SFX Local Collection
subjects Cycloaddition
Damage
Guanines
Guanosines
Mathematical models
Nucleosides
Oxidation
Protonation
title How protonation and deprotonation of 9-methylguanine alter its singlet O sub(2) addition path: about the initial stage of guanine nucleoside oxidation
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