Quantum chemical simulation of cytochrome P450 catalyzed aromatic oxidation: Metabolism, toxicity, and biodegradation of benzene derivatives

D’yachkov, P. N.; Харчевникова, Н. В.; Дмитриев, А. В.; Kuznetsov, A. V.; Poroikov, Vladimir

doi:10.1002/qua.21416

Cited by 9 publications

(9 citation statements)

References 56 publications

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“…In summary, taking into account our previous results 18, we conclude that the oxenoid model together with semiempirical quantum chemical calculations can reasonably explain the in vivo and in vitro experimental data on the positions of the enzyme‐mediated oxidation, rate of substrate biotransformation, as well as toxicity, and carcinogenicity of the mono‐ and disubstituted benzene derivatives.…”

Section: Discussionsupporting

confidence: 68%

“…The oxens readily react with substrates 16, 17. The relationships between the nature of substituents from one side and biological oxidation and acute toxicity of the benzene derivatives from another side as well as the features of metabolism of di‐ and trichlorinated biphenyls by bacteria were studied using an oxenoid model in our recent paper 18.…”

Section: Introductionmentioning

confidence: 99%

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Assessing utility values in rheumatoid arthritis: A comparison between time trade‐off and the EuroQol

Ariza‐Ariza

Hernández‐Cruz

Carmona

et al. 2006

Arthritis & Rheumatism

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At baseline, the EQ-5D scores were highly correlated with the HAQ (r ‫؍‬ ؊0.74) and moderately correlated with the DAS28 (r ‫؍‬ ؊0.47), whereas the TTO correlated poorly with both the HAQ and DAS28. Correlation between the mean change in the EQ-5D and in the HAQ was moderate (r ‫؍‬ ؊0.55). Conclusion. TTO and EQ-5D do not yield the same utility values. The results suggest that the EQ-5D is more representative of RA status than the TTO, a valuable conclusion when addressing economic evaluations in RA.

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Section: Discussionsupporting

confidence: 68%

Section: Introductionmentioning

confidence: 99%

Assessing utility values in rheumatoid arthritis: A comparison between time trade‐off and the EuroQol

Ariza‐Ariza

Hernández‐Cruz

Carmona

et al. 2006

Arthritis & Rheumatism

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“…The results at the AM1 level are rather poor ( r 2 = 0.55 for BDE cat alone, excluding nonaromatic oxidations, and r 2 = 0.60 for our full data set with both descriptors). However, it is significantly better and faster than energies obtained for the intermediate with the methoxy-radical model ( r 2 = 0.35−0.45), a method that has been used in several previous studies. ,,, …”

Section: Resultsmentioning

confidence: 99%

“…It has previously been shown that the methoxy radical can be used as a model for compound I when studying the hydroxylation of aliphatic carbon atoms , as well as in semiempirical studies of hydroxylation of aromatic carbon atoms. ,,, Therefore, we also tested how well the activation energies and the energies of the tetrahedral intermediate, calculated with the methoxy radical could reproduce the energies in Table . As is shown in part a of Figure and Table , the activation energies calculated with the methoxy radical at the B3LYP/6−31G(d) level correlate well with the final DFT energies calculated with the full compound I model.…”

Section: Resultsmentioning

confidence: 99%

Prediction of Activation Energies for Aromatic Oxidation by Cytochrome P450

2008

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We have estimated the activation energy for aromatic oxidation by compound I in cytochrome P450 for a diverse set of 17 substrates using state-of-the-art density functional theory (B3LYP) with large basis sets. The activation energies vary from 60 to 87 kJ/mol. We then test if these results can be reproduced by computationally less demanding methods. The best methods (a B3LYP calculation of the activation energy of a methoxy-radical model or a partial least-squares model of the semiempirical AM1 bond dissociation energies and spin densities of the tetrahedral intermediate for both a hydroxyl-cation and a hydroxyl-radical model) give correlations with r(2) of 0.8 and mean absolute deviations of 3 kJ/mol. Finally, we apply these simpler methods on several sets of reactions for which experimental data are available and show that we can predict the reactive sites by combining calculations of the activation energies with the solvent-accessible surface area of each site.

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“…Quantitative relationships between structure and metabolism rates have been investigated for a limited number of closely related compounds, even though their applicability to PBPK modeling has not been demonstrated (e.g., QSPR models for K cat and 1/ K m [ 87 ]). Other works in this area relate to the development of quantum chemical or quantum dynamic methods for prediction of activation energy or enthalpy of activation of P450 mediated reactions [ 20 , 25 , 26 , 31 , 36 , 38 , 88 – 91 ], which have not been used to derive metabolism constants for direct incorporation within rodent or human PBPK models.…”

Section: Discussionmentioning

confidence: 99%

Quantitative Property-Property Relationship for Screening-Level Prediction of Intrinsic Clearance of Volatile Organic Chemicals in Rats and Its Integration within PBPK Models to Predict Inhalation Pharmacokinetics in Humans

Peyret

Krishnan²

2012

Journal of Toxicology

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The objectives of this study were (i) to develop a screening-level Quantitative property-property relationship (QPPR) for intrinsic clearance (CLint) obtained from in vivo animal studies and (ii) to incorporate it with human physiology in a PBPK model for predicting the inhalation pharmacokinetics of VOCs. CLint, calculated as the ratio of the in vivo V max (μmol/h/kg bw rat) to the K m (μM), was obtained for 26 VOCs from the literature. The QPPR model resulting from stepwise linear regression analysis passed the validation step (R 2 = 0.8; leave-one-out cross-validation Q 2 = 0.75) for CLint normalized to the phospholipid (PL) affinity of the VOCs. The QPPR facilitated the calculation of CLint (L PL/h/kg bw rat) from the input data on log P ow, log blood: water PC and ionization potential. The predictions of the QPPR as lower and upper bounds of the 95% mean confidence intervals (LMCI and UMCI, resp.) were then integrated within a human PBPK model. The ratio of the maximum (using LMCI for CLint) to minimum (using UMCI for CLint) AUC predicted by the QPPR-PBPK model was 1.36 ± 0.4 and ranged from 1.06 (1,1-dichloroethylene) to 2.8 (isoprene). Overall, the integrated QPPR-PBPK modeling method developed in this study is a pragmatic way of characterizing the impact of the lack of knowledge of CLint in predicting human pharmacokinetics of VOCs, as well as the impact of prediction uncertainty of CLint on human pharmacokinetics of VOCs.

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Quantum chemical simulation of cytochrome P450 catalyzed aromatic oxidation: Metabolism, toxicity, and biodegradation of benzene derivatives

Cited by 9 publications

References 56 publications

Assessing utility values in rheumatoid arthritis: A comparison between time trade‐off and the EuroQol

Assessing utility values in rheumatoid arthritis: A comparison between time trade‐off and the EuroQol

Prediction of Activation Energies for Aromatic Oxidation by Cytochrome P450

Quantitative Property-Property Relationship for Screening-Level Prediction of Intrinsic Clearance of Volatile Organic Chemicals in Rats and Its Integration within PBPK Models to Predict Inhalation Pharmacokinetics in Humans

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