Interaction of 7-n-alkoxycoumarins with cytochrome <i>P</i>-4502 and their partitioning into liposomal membranes. Assessment of methods for determination of membrane partition coefficients

Vermeir, Marc; Boens, Noël; Heirwegh, Kpm

doi:10.1042/bj2840483

Cited by 12 publications

(8 citation statements)

References 47 publications

(35 reference statements)

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“…O-dealkylation rates of 7-alkoxycoumarins mediated by CYP2B4 in the rabbit: HOMO energies and log P data. Reference [18].…”

Section: Methodsmentioning

confidence: 99%

“…In addition, CYP2B-related activities for a series of 7-alkoxycoumarins [18] and of barbiturates [19] were retrieved from previously reported studies. Compound lipophilicities in the form of log P values were obtained from tabulations of experimental data [20,21] or calculated via the ClogP (BioByte, Pomona, CA) and Pallas (CompuDrug, Budapest, Hungary) software systems.…”

Section: Methodsmentioning

confidence: 99%

See 1 more Smart Citation

Quantitative structure-activity relationships (QSARs) for inhibitors and substrates of CYP2B enzymes: importance of compound lipophilicity in explanation of potency differences

Lewis

Ito

Lake

2010

Journal of Enzyme Inhibition and Medicinal Chemistry

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“…O-dealkylation rates of 7-alkoxycoumarins mediated by CYP2B4 in the rabbit: HOMO energies and log P data. Reference [18].…”

Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Quantitative structure-activity relationships (QSARs) for inhibitors and substrates of CYP2B enzymes: importance of compound lipophilicity in explanation of potency differences

Lewis

Ito

Lake

2010

Journal of Enzyme Inhibition and Medicinal Chemistry

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“…Until now, the ether O-dealkylation activities have been widely found in mammalian cytochrome P450 systems. Rates of cytochrome P450-catalyzed O-dealkylation reactions usually decrease with bulkier alkyl chains of alkyl and benzyl ethers [29][30][31], as similarly observed in strain DEE5151 [22]. Besides, there are reports that several members of the genera Rhodococcus and Corynebacterium possess cytochrome P450 systems catalyzing the O-dealkylation reactions of 2-alkoxyphenols and 7-ethoxycoumarin [26][27][28].…”

Section: Discussionmentioning

confidence: 66%

“…Besides, there are reports that several members of the genera Rhodococcus and Corynebacterium possess cytochrome P450 systems catalyzing the O-dealkylation reactions of 2-alkoxyphenols and 7-ethoxycoumarin [26][27][28]. Rates of cytochrome P450-catalyzed O-dealkylation reactions usually decrease with bulkier alkyl chains of alkyl and benzyl ethers [29][30][31], as similarly observed in strain DEE5151 [22]. In this study it is yet uncertain whether a cytochrome P450 enzyme system in strain DEE5151 is involved in the oxidation of diethyl ether, because it is difficult to interpret the inhibition studies resulting in no inhibitory effect, if the permeability barrier, e.g., mycolate layer, of the cell surface might exclude some inhibitors (e.g., carbon monoxide) from the cytoplasm.…”

Section: Discussionmentioning

confidence: 99%

Inhibition of diethyl ether degradation in Rhodococcus sp. strain DEE5151 by glutaraldehyde and ethyl vinyl ether

Kim

Engesser

2005

FEMS Microbiology Letters

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Alkyl ether-degrading Rhodococcus sp. strain DEE5151, isolated from activated sewage sludge, has an activity for the oxidation of a variety of alkyl ethers, aralkyl ethers and dibenzyl ether. The whole cell activity for diethyl ether oxidation was effectively inhibited by 2,3-dihydrofurane, ethyl vinyl ether and glutaraldehyde. Glutaraldehyde of less than 30 microM inhibited the activity by a competitive manner with the inhibition constant, K(I) of 7.07+/-1.36 microM. The inhibition type became mixed at higher glutaraldehyde concentrations >30 microM, probably due to the inactivation of the cell activity by the Schiff-base formation. Structurally analogous ethyl vinyl ether inhibited the diethyl ether oxidation activity in a mixed manner with decreasing the apparent maximum oxidation rate, v(max)(app), and increasing the apparent Michaelis-Menten constant, K(M)(app). The mixed type inhibition by ethyl vinyl ether seemed to be introduced not only by the structure similarity with diethyl ether, but also by the reactivity of the vinyl ether with cellular components in the whole cell system.

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“…These values can be determined from the fluorescence intensity depending on whether there is quenching or enhancement, as described in the Experimental section. [43][44][45] The increased emission intensity and blue-shift observed for P3TMAHT is common for CPEs when combined with phospholipids, 18,24 oppositely-charged, 19,51 or neutral surfactants. 51,52 Such changes have been attributed to the surfactant-induced break-up of the CPE clusters to form new surfactant-CPE aggregates, 52 where the conformation of the CPE changes from an aggregated to more extended state.…”

Section: Determination Of Partition Coefficients the Partition Coeffmentioning

confidence: 99%

Charge-Mediated Localization of Conjugated Polythiophenes in Zwitterionic Model Cell Membranes

et al. 2016

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The selective engineering of conjugated polyelectrolyte (CPE)-phospholipid interfaces is poised to play a key role in the design of advanced biomedical and biotechnological devices. Herein, we report a strategic study to investigate the relationship between the charge of the CPE side group and their association with zwitterionic phospholipid bilayers. The interaction of dipalmitoylphosphatidylcholine (DPPC) phospholipid vesicles with a series of poly(thiophene)s bearing zwitterionic, cationic, or anionic terminal groups (P3Zwit, P3TMAHT and P3Anionic, respectively) has been probed. Although all CPEs showed an affinity for the zwitterionic vesicles, the calculated partition coefficients determined using photoluminescence spectroscopy suggested preferential incorporation within the lipid bilayer in the order P3Zwit > P3Anionic ≫ P3TMAHT. The polarity probe Prodan was used to further qualify the position of the CPE inside the vesicle bilayers via Förster resonance energy transfer (FRET) studies. The varying proximity of the CPEs to Prodan was reflected in the Stern-Volmer quenching constants and decreased in the order P3Anionic > P3TMAHT ≫ P3Zwit. Dynamic light scattering measurements showed an increase in the hydrodynamic diameter of the DPPC vesicles upon addition of each poly(thiophene), but to the greatest extent for P3Anionic. Small-angle neutron scattering studies also revealed that P3Anionic specifically increased the thickness of the headgroup region of the phospholipid bilayer. Epifluorescence and atomic force microscopy imaging showed that P3TMAHT formed amorphous agglomerates on the vesicle surface, P3Zwit was buried throughout the bilayer, and P3Anionic formed a shell of protruding chains around the surface, which promoted vesicle fusion. The global data indicate three distinctive modes of interaction for the poly(thiophene)s within DPPC vesicles, whereby the nature of the association is ultimately controlled by the pendant charge group on each CPE chain. Our results suggest that charge-mediated self-assembly may provide a simple and effective route to design luminescent CPE probes capable of specific localization within phospholipid membranes.

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Interaction of 7-n-alkoxycoumarins with cytochrome P-4502 and their partitioning into liposomal membranes. Assessment of methods for determination of membrane partition coefficients

Cited by 12 publications

References 47 publications

Quantitative structure-activity relationships (QSARs) for inhibitors and substrates of CYP2B enzymes: importance of compound lipophilicity in explanation of potency differences

Quantitative structure-activity relationships (QSARs) for inhibitors and substrates of CYP2B enzymes: importance of compound lipophilicity in explanation of potency differences

Inhibition of diethyl ether degradation in Rhodococcus sp. strain DEE5151 by glutaraldehyde and ethyl vinyl ether

Charge-Mediated Localization of Conjugated Polythiophenes in Zwitterionic Model Cell Membranes

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