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4. Variations in the chemical profile and biological activities of licorice (Glycyrrhiza glabra L.), as influenced by harvest times

Author

Cheel, Jose, Tumova, L, Areche, C., Van Antwerpen, Pierre, Neve, Jean, Zouaoui Boudjeltia, Karim, San Martin, A., Vokral, I., Wsol, V., Neugebauerova, J., Cheel, Jose, Tumova, L, Areche, C., Van Antwerpen, Pierre, Neve, Jean, Zouaoui Boudjeltia, Karim, San Martin, A., Vokral, I., Wsol, V., and Neugebauerova, J.

Abstract

This study investigates the variations in the chemical profile, free radical scavenging, antioxidant and gastroprotective activities of licorice extracts (LE) from plants harvested during the months of February to November. Correlations between biological properties and the chemical composition of LE were also investigated. The results showed that the total contents of phenols, flavonoids and tannins in LE varied at different harvest times. Liquiritin and glycyrrhizin, the major components of LE, varied in the range of 28.65–62.80 and 41.84–114.33 mg g−1, respectively. The relative proportion of glycyrrhizin derivative (3), glabridin (4), glabrene (5) and liquiritigenin derivative (6), varied in the range of 0.88–11.38 %, 1.86–10.03 %, 1.80–18.40 % and 5.53–16.31 %, respectively. These fluctuations correlated positively with changes in the antioxidant and free radical scavenging activities of licorice. In general, the samples from May and November showed the most favorable free radical scavenging and antioxidant effects, whereas the best gastroprotective effect was in May. Liquiritin and glycyrrhizin, the major constituents in the February and May LE, appeared to contribute to the superoxide radical scavenging and gastroprotective effects. Glabridin and glabrene, the compounds with the highest relative proportion in the November LE, accounted for the antioxidant and DPPH scavenging activities of licorice. It is concluded that the chemical profile of licorice quantitatively varied at different harvest times and these fluctuations determined changes in its bioactivities. These data could pave the way to optimize harvesting protocols for licorice in relation with its health-promoting properties., SCOPUS: ar.j, info:eu-repo/semantics/published

Published
2013

5. Variations in the chemical profile, free radical scavenging, antioxidant and gastroprotective activities of licorice (Glycyrrhiza glabra L.): as influenced by harvest times

Author

Cheel, Jose, Areche, C., Van Antwerpen, Pierre, Neve, Jean, Zouaoui Boudjeltia, Karim, Tumova, L, San Martin, A., Vokral, I., Wsol, V., Neugebauerova, J., Cheel, Jose, Areche, C., Van Antwerpen, Pierre, Neve, Jean, Zouaoui Boudjeltia, Karim, Tumova, L, San Martin, A., Vokral, I., Wsol, V., and Neugebauerova, J.

Abstract

info:eu-repo/semantics/nonPublished

Published
2011

12. 11β-Hydroxysteroid dehydrogenase type 1: Purification from human liver and characterization as carbonyl reductase of xenobiotics

Author

Maser, E., Wsol, V., and Martin, H.-J.

Subjects
*DEHYDROGENASES, *GLUCOCORTICOID receptors, *XENOBIOTICS, *CARBONYL compounds, *HORMONES
Abstract

Abstract: 11β-Hydroxysteroid dehydrogenase type 1 (11β-HSD1) catalyzes the interconversion of 11-oxo glucocorticoids to their 11-hydroxy metabolites, thereby controlling access of glucocorticoid hormones to the glucocorticoid receptor. Interestingly, evidence is emerging that 11β-HSD1 fulfills an additional role in the metabolism of xenobiotic carbonyl compounds. In our studies, 11β-HSD1 was identified as a microsomal reductase that initiates the final detoxification of xenobiotics by reducing them to alcohols that are easier to conjugate and eliminate. With its pluripotent substrate specificities for glucocorticoids and xenobiotics, 11β-HSD1 adds to an expanding list of those hydroxysteroid dehydrogenases which, on the one hand, are capable of catalyzing the carbonyl reduction of non-steroidal carbonyl compounds, and which, on the other hand, exhibit great specificity to their physiological steroid substrates. It is conceivable that large interferences must occur between endogenous steroid metabolism and the detoxification of xenobiotic compounds on the level of hydroxysteroid dehydrogenases. [Copyright &y& Elsevier]

Published
2006
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13. Albendazole repeated administration induces cytochromes P4501A and accelerates albendazole deactivation in mouflon (Ovis musimon)

Author

Velik, J., Szotakova, B., Baliharova, V., Lamka, J., Savlik, M., Wsol, V., Snejdrova, E., and Skalova, L.

Abstract

Adult mouflon ewes (Ovis musimon) were treated repeatedly with therapeutic doses of albendazole (ABZ, p.o. 7.5 mg/kg of body weight/day, for five consecutive days). Animals (treated or control) were sacrificed 24 h after the fifth dose of ABZ and liver and small intestine were collected to prepare microsomes. The activities of several biotransformation enzymes were measured in both hepatic and intestinal microsomes. A significant increase in the activity and amount of cytochromes P4501A (CYP1A) was observed in both tissues of ABZ treated mouflons compared to control animals. No other biotransformation enzymes tested were affected by five ABZ doses. The in vitro biotransformation of ABZ was studied in hepatic and intestinal microsomes from ABZ treated and control mouflons. Concentrations of two main ABZ metabolites - pharmacologically active ABZ sulfoxide and pharmacologically inactive ABZ sulfone were analysed using HPLC. A significant increase in rate of formation of ABZ sulfone (which is catalysed by CYP1A) was observed in hepatic as well as in intestinal microsomes from ABZ treated animals. The enhancement of ABZ deactivation by its repeated administration may affect the anthelmintic efficacy of this drug and may contribute to the development of parasite resistance.

Published
2005
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14. 3-Phenyl-5-acyloxymethyl-2H,5H-furan-2-ones:  Synthesis and Biological Activity of a Novel Group of Potential Antifungal Drugs

Author

Pour, M., Spulak, M., Buchta, V., Kubanova, P., Voprsalova, M., Wsol, V., Fakova, H., Koudelka, P., Pourova, H., and Schiller, R.

Abstract

3-(Substituted phenyl)-5-acyloxymethyl-2H,5H-furan-2-ones related to the natural product (−)incrustoporine were synthesized and their in vitro antifungal activity evaluated. The compounds with halogen substituents on the phenyl ring displayed much higher antifungal effect against Aspergillus fumigatus than selected representatives of azole antifungal drugs. In particular, the activity (1.34 μg/mL) of the most promising derivative, 3-(3,4-dichlorophenyl)-5-pivaloyloxymethyl-2H,5H-furan-2-one, was comparable to that of amphotericin B (0.5 μg/mL). Preliminary evaluation of the toxicity of the compound was carried out as well. Considering the size and properties of these molecules in comparison with those of amphotericin B, further development of this novel group of antifungals may lead to substances with better pharmacological profiles than that of the standard anti-Aspergillus drug.

Published
2001

17. Acetylcholinesterase inhibitors and drugs acting on muscarinic receptors - potential crosstalk of cholinergic mechanisms during pharmacological treatment

Author

Soukup, O, Winder, M, Killi, UK, Wsol, V, Jun, D, Kuca, K, and Tobin, G

Subjects
Enzyme inhibitors, Business, international
Abstract

Abstract Pharmaceuticals with targets in the cholinergic transmission have been used for decades and are still fundamental treatments in many diseases and conditions today. Both the transmission and the effects [...]

Published
2016

31. Targeting Pharmacokinetic Drug Resistance in Acute Myeloid Leukemia Cells with CDK4/6 Inhibitors.

Author

Sorf A, Sucha S, Morell A, Novotna E, Staud F, Zavrelova A, Visek B, Wsol V, and Ceckova M

Abstract

Pharmacotherapy of acute myeloid leukemia (AML) remains challenging, and the disease has one of the lowest curability rates among hematological malignancies. The therapy outcomes are often compromised by the existence of a resistant AML phenotype associated with overexpression of ABCB1 and ABCG2 transporters. Because AML induction therapy frequently consists of anthracycline-like drugs, their efficiency may also be diminished by drug biotransformation via carbonyl reducing enzymes (CRE). In this study, we investigated the modulatory potential of the CDK4/6 inhibitors abemaciclib, palbociclib, and ribociclib on AML resistance using peripheral blood mononuclear cells (PBMC) isolated from patients with de novo diagnosed AML. We first confirmed inhibitory effect of the tested drugs on ABCB1 and ABCG2 in ABC transporter-expressing resistant HL-60 cells while also showing the ability to sensitize the cells to cytotoxic drugs even as no effect on AML-relevant CRE isoforms was observed. All tested CDK4/6 inhibitors elevated mitoxantrone accumulations in CD34 + PBMC and enhanced accumulation of mitoxantrone was found with abemaciclib and ribociclib in PBMC of FLT3-ITD - patients. Importantly, the accumulation rate in the presence of CDK4/6 inhibitors positively correlated with ABCB1 expression in CD34 + patients and led to enhanced apoptosis of PBMC in contrast to CD34 - samples. In summary, combination therapy involving CDK4/6 inhibitors could favorably target multidrug resistance, especially when personalized based on CD34- and ABCB1-related markers.

Published
2020
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32. Cyclin-dependent kinase inhibitors AZD5438 and R547 show potential for enhancing efficacy of daunorubicin-based anticancer therapy: Interaction with carbonyl-reducing enzymes and ABC transporters.

Author

Sorf A, Novotna E, Hofman J, Morell A, Staud F, Wsol V, and Ceckova M

Subjects
Animals, Antineoplastic Agents administration & dosage, Antineoplastic Agents therapeutic use, Binding Sites, Cell Line, Tumor, Cell Proliferation, Cloning, Molecular, Daunorubicin administration & dosage, Daunorubicin adverse effects, Daunorubicin analogs & derivatives, Dogs, Drug Resistance, Neoplasm drug effects, Gene Expression Regulation, Enzymologic drug effects, Heart Diseases chemically induced, Humans, Imidazoles administration & dosage, Protein Binding, Pyrimidines administration & dosage, ATP Binding Cassette Transporter, Subfamily G, Member 2 metabolism, Daunorubicin therapeutic use, Imidazoles pharmacology, Multidrug Resistance-Associated Proteins metabolism, Neoplasm Proteins metabolism, Pyrimidines pharmacology
Abstract

Daunorubicin (DAUN) has served as an anticancer drug in chemotherapy regimens for decades and is still irreplaceable in treatment of acute leukemias. The therapeutic outcome of DAUN-based therapy is compromised by its cardiotoxicity and emergence of drug resistance. This phenomenon is often caused by pharmacokinetic mechanisms such as efflux of DAUN from cancer cells through ATP-binding cassette (ABC) transporters and its conversion to less cytostatic but more cardiotoxic daunorubicinol (DAUN-OL) by carbonyl reducing enzymes (CREs). Here we aimed to investigate, whether two cyclin-dependent kinase inhibitors, AZD5438 and R547, can interact with these pharmacokinetic mechanisms and reverse DAUN resistance. Using accumulation assays, we revealed AZD5438 as potent inhibitor of ABCC1 showing also weaker inhibitory effect to ABCB1 and ABCG2. Combination index analysis, however, shown that inhibition of ABCC1 does not significantly contribute to synergism between AZD5438 and DAUN in MDCKII-ABCC1 cells, suggesting predominant role of other mechanism. Using pure recombinant enzymes, we found both tested drugs to inhibit CREs with aldo-keto reductase 1C3 (AKR1C3). This interaction was further confirmed in transfected HCT-116 cells. Moreover, these cells were sensitized to DAUN by both compounds as Chou-Talalay combination index analysis showed synergism in AKR1C3 transfected HCT-116, but not in empty vector transfected control cell line. In conclusion, we propose AZD5438 and R547 as modulators of DAUN resistance that can prevent AKR1C3-mediated DAUN biotransformation to DAUN-OL. This interaction could be beneficially exploited to prevent failure of DAUN-based therapy as well as the undesirable cardiotoxic effect of DAUN-OL., (Copyright © 2019 Elsevier Inc. All rights reserved.)

Published
2019
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33. Buparlisib is a novel inhibitor of daunorubicin reduction mediated by aldo-keto reductase 1C3.

Author

Bukum N, Novotna E, Morell A, Hofman J, and Wsol V

Subjects
Aldo-Keto Reductase Family 1 Member C3 antagonists & inhibitors, Aldo-Keto Reductase Family 1 Member C3 chemistry, Aldo-Keto Reductases antagonists & inhibitors, Aldo-Keto Reductases genetics, Aldo-Keto Reductases metabolism, Aminopyridines chemistry, Aminopyridines metabolism, Binding Sites, Catalytic Domain, HCT116 Cells, Humans, Inhibitory Concentration 50, Kinetics, Molecular Docking Simulation, Morpholines chemistry, Morpholines metabolism, Recombinant Proteins biosynthesis, Recombinant Proteins isolation & purification, Recombinant Proteins metabolism, Aldo-Keto Reductase Family 1 Member C3 metabolism, Aminopyridines pharmacology, Daunorubicin metabolism, Morpholines pharmacology
Abstract

Buparlisib is a pan-class I phosphoinositide 3-kinase (PI3K) inhibitor and is currently under clinical evaluation for the treatment of different cancers. Because PI3K signalling is related to cell proliferation and resistance to chemotherapy, new therapeutic approaches are focused on combining PI3K inhibitors with other anti-cancer therapeutics. Carbonyl-reducing enzymes catalyse metabolic detoxification of anthracyclines and reduce their cytotoxicity. In the present work, the effects of buparlisib were tested on six human recombinant carbonyl-reducing enzymes: AKR1A1, AKR1B1, AKR1B10, AKR1C3, and AKR7A2 from the aldo-keto reductase superfamily and CBR1 from the short-chain dehydrogenase/reductase superfamily, all of which participate in the metabolism of daunorubicin. Buparlisib exhibited the strongest inhibitory effect on recombinant AKR1C3, with a half-maximal inhibitory concentration (IC 50 ) of 9.5 μM. Its inhibition constant K i was found to be 14.0 μM, and the inhibition data best fitted a mixed-type mode with α = 0.6. The same extent of inhibition was observed at the cellular level in the human colorectal carcinoma HCT 116 cell line transfected with a plasmid encoding the AKR1C3 transcript (IC 50  = 7.9 μM). Furthermore, we performed an analysis of flexible docking between buparlisib and AKR1C3 and found that buparlisib probably occupies a part of the binding site for a cofactor most likely via the trifluoromethyl group of buparlisib interacting with catalytic residue Tyr55. In conclusion, our results show a novel PI3K-independent effect of buparlisib that may improve therapeutic efficacy and safety of daunorubicin by preventing its metabolism by AKR1C3., (Copyright © 2019 Elsevier B.V. All rights reserved.)

Published
2019
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34. Acetylcholinesterase Inhibitors and Drugs Acting on Muscarinic Receptors- Potential Crosstalk of Cholinergic Mechanisms During Pharmacological Treatment.

Author

Soukup O, Winder M, Killi UK, Wsol V, Jun D, Kuca K, and Tobin G

Subjects
Animals, Humans, Receptor Cross-Talk drug effects, Cholinesterase Inhibitors pharmacology, Receptors, Muscarinic drug effects
Abstract

Background: Pharmaceuticals with targets in the cholinergic transmission have been used for decades and are still fundamental treatments in many diseases and conditions today. Both the transmission and the effects of the somatomotoric and the parasympathetic nervous systems may be targeted by such treatments. Irrespective of the knowledge that the effects of neuronal signalling in the nervous systems may include a number of different receptor subtypes of both the nicotinic and the muscarinic receptors, this complexity is generally overlooked when assessing the mechanisms of action of pharmaceuticals., Methods: We have search of bibliographic databases for peer-reviewed research literature focused on the cholinergic system. Also, we have taken advantage of our expertise in this field to deduce the conclusions of this study., Results: Presently, the life cycle of acetylcholine, muscarinic receptors and their effects are reviewed in the major organ systems of the body. Neuronal and non-neuronal sources of acetylcholine are elucidated. Examples of pharmaceuticals, in particular cholinesterase inhibitors, affecting these systems are discussed. The review focuses on salivary glands, the respiratory tract and the lower urinary tract, since the complexity of the interplay of different muscarinic receptor subtypes is of significance for physiological, pharmacological and toxicological effects in these organs., Conclusion: Most pharmaceuticals targeting muscarinic receptors are employed at such large doses that no selectivity can be expected. However, some differences in the adverse effect profile of muscarinic antagonists may still be explained by the variation of expression of muscarinic receptor subtypes in different organs. However, a complex pattern of interactions between muscarinic receptor subtypes occurs and needs to be considered when searching for selective pharmaceuticals. In the development of new entities for the treatment of for instance pesticide intoxication, the muscarinic receptor selectivity needs to be considered. Reactivators generally have a muscarinic M2 receptor acting profile. Such a blockade may engrave the situation since it may enlarge the effect of the muscarinic M3 receptor effect. This may explain why respiratory arrest is the major cause for deaths by esterase blocking., (Copyright© Bentham Science Publishers; For any queries, please email at epub@benthamscience.org.)

Published
2017
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35. Inhibition of human anthracycline reductases by emodin - A possible remedy for anthracycline resistance.

Author

Hintzpeter J, Seliger JM, Hofman J, Martin HJ, Wsol V, and Maser E

Subjects
Anthraquinones pharmacology, Cell Line, Tumor, Cell Survival drug effects, Drug Synergism, Humans, Molecular Docking Simulation, Oxidoreductases metabolism, Antibiotics, Antineoplastic pharmacology, Daunorubicin pharmacology, Drug Resistance, Neoplasm drug effects, Emodin pharmacology, Oxidoreductases antagonists & inhibitors, Protein Kinase Inhibitors pharmacology
Abstract

The clinical application of anthracyclines, like daunorubicin and doxorubicin, is limited by two factors: dose-related cardiotoxicity and drug resistance. Both have been linked to reductive metabolism of the parent drug to their metabolites daunorubicinol and doxorubicinol, respectively. These metabolites show significantly less anti-neoplastic properties as their parent drugs and accumulate in cardiac tissue leading to chronic cardiotoxicity. Therefore, we aimed to identify novel and potent natural inhibitors for anthracycline reductases, which enhance the anticancer effect of anthracyclines by preventing the development of anthracycline resistance. Human enzymes responsible for the reductive metabolism of daunorubicin were tested for their sensitivity towards anthrachinones, in particular emodin and anthraflavic acid. Intense inhibition kinetic data for the most effective daunorubicin reductases, including IC50- and Ki-values, the mode of inhibition, as well as molecular docking, were compiled. Subsequently, a cytotoxicity profile and the ability of emodin to reverse daunorubicin resistance were determined using multiresistant A549 lung cancer and HepG2 liver cancer cells. Emodin potently inhibited the four main human daunorubicin reductases in vitro. Further, we could demonstrate that emodin is able to synergistically sensitize human cancer cells towards daunorubicin at clinically relevant concentrations. Therefore, emodin may yield the potential to enhance the therapeutic effectiveness of anthracyclines by preventing anthracycline resistance via inhibition of the anthracycline reductases. In symphony with its known pharmacological properties, emodin might be a compound of particular interest in the management of anthracycline chemotherapy efficacy and their adverse effects., (Copyright © 2016 Elsevier Inc. All rights reserved.)

Published
2016
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36. Flavones Inhibit the Activity of AKR1B10, a Promising Therapeutic Target for Cancer Treatment.

Author

Zemanova L, Hofman J, Novotna E, Musilek K, Lundova T, Havrankova J, Hostalkova A, Chlebek J, Cahlikova L, and Wsol V

Subjects
Aldehyde Reductase antagonists & inhibitors, Aldo-Keto Reductases, Apigenin pharmacology, Daunorubicin pharmacology, Enzyme Inhibitors chemistry, Flavones chemistry, Flavonoids pharmacology, HCT116 Cells, Humans, Luteolin pharmacology, Molecular Conformation, Molecular Structure, Aldehyde Reductase drug effects, Flavones pharmacology, Neoplasms drug therapy
Abstract

AKR1B10 is an NADPH-dependent reductase that plays an important function in several physiological reactions such as the conversion of retinal to retinol, reduction of isoprenyl aldehydes, and biotransformation of procarcinogens and drugs. A growing body of evidence points to the important role of the enzyme in the development of several types of cancer (e.g., breast, hepatocellular), in which it is highly overexpressed. AKR1B10 is regarded as a therapeutic target for the treatment of these diseases, and potent and specific inhibitors may be promising therapeutic agents. Several inhibitors of AKR1B10 have been described, but the area of natural plant products has been investigated sparingly. In the present study almost 40 diverse phenolic compounds and alkaloids were examined for their ability to inhibit the recombinant AKR1B10 enzyme. The most potent inhibitors-apigenin, luteolin, and 7-hydroxyflavone-were further characterized in terms of IC50, selectivity, and mode of action. Molecular docking studies were also conducted, which identified putative binding residues important for the interaction. In addition, cellular studies demonstrated a significant inhibition of the AKR1B10-mediated reduction of daunorubicin in intact cells by these inhibitors without a considerable cytotoxic effect. Although these compounds are moderately potent and selective inhibitors of AKR1B10, they constitute a new structural type of AKR1B10 inhibitor and may serve as a template for the development of better inhibitors.

Published
2015
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37. Pharmacokinetic interactions of breast cancer chemotherapeutics with human doxorubicin reductases.

Author

Hofman J, Skarka A, Havrankova J, and Wsol V

Subjects
3-Hydroxysteroid Dehydrogenases genetics, 3-Hydroxysteroid Dehydrogenases metabolism, Alcohol Oxidoreductases genetics, Alcohol Oxidoreductases metabolism, Aldehyde Reductase genetics, Aldehyde Reductase metabolism, Aldo-Keto Reductase Family 1 Member C3, Antineoplastic Combined Chemotherapy Protocols, Biotransformation, Docetaxel, Doxorubicin metabolism, Drug Interactions, Hep G2 Cells, Humans, Hydroxyprostaglandin Dehydrogenases genetics, Hydroxyprostaglandin Dehydrogenases metabolism, Isoenzymes genetics, Isoenzymes metabolism, Kinetics, Liver drug effects, Liver enzymology, MCF-7 Cells, Oxidation-Reduction, Recombinant Proteins genetics, Recombinant Proteins metabolism, Tamoxifen pharmacology, Antineoplastic Agents pharmacology, Cyclophosphamide pharmacology, Doxorubicin pharmacology, Fluorouracil pharmacology, Gene Expression Regulation, Neoplastic drug effects, Taxoids pharmacology
Abstract

Paclitaxel (PTX), docetaxel (DTX), 5-fluorouracil (5-FU), cyclophosphamide (CYC) or tamoxifen (TMX) are combined with doxorubicin (DOX) in first-line chemotherapy regimens that are indicated for breast cancer patients. Although the efficacies of these drugs in combination treatments have been demonstrated in clinical practice, their possible interference with DOX metabolism has not been described in detail to date. In the present study, we investigated the possible interactions of human carbonyl reducing enzymes with 5-FU, PTX, DTX, CYC and TMX. First, the reducing activities of carbonyl reducing enzymes toward DOX were tested using incubations with purified recombinant enzymes. In the subsequent studies, we investigated the possible effects of the tested anticancer agents on the DOX-reducing activities of the most potent enzymes (AKR1C3, CBR1 and AKR1A1) and on the DOX metabolism driven by MCF7, HepG2 and human liver cytosols. In both of these assays, we observed that CYC and its active metabolites inhibited DOX metabolism. In the final study, we tracked the changes in AKR1C3, CBR1 and AKR1A1 expression levels following exposure to the tested cytostatics in MCF7 and HepG2 cells. Consequently, no significant changes in the expression levels of tested enzymes were detected in either cell line. Based on these findings, it is feasible to presume that inhibition rather than induction plays a role in the interactions of the tested anticancer agents with DOX-reducing enzymes. In conclusion, our results describe important molecular events that occur during combination breast cancer therapies and might modulate pharmacokinetic DOX resistance and/or behaviour., (Copyright © 2015 Elsevier Inc. All rights reserved.)

Published
2015
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38. Isoquinoline alkaloids as a novel type of AKR1C3 inhibitors.

Author

Skarydova L, Hofman J, Chlebek J, Havrankova J, Kosanova K, Skarka A, Hostalkova A, Plucha T, Cahlikova L, and Wsol V

Subjects
Aldo-Keto Reductase Family 1 Member C3, Blotting, Western, Breast Neoplasms enzymology, Breast Neoplasms pathology, Cell Proliferation, Chromatography, High Pressure Liquid, Colorectal Neoplasms enzymology, Colorectal Neoplasms pathology, Female, Humans, Testosterone metabolism, Tumor Cells, Cultured, 3-Hydroxysteroid Dehydrogenases antagonists & inhibitors, Berberine Alkaloids pharmacology, Breast Neoplasms drug therapy, Cell Survival drug effects, Colorectal Neoplasms drug therapy, Enzyme Inhibitors pharmacology, Hydroxyprostaglandin Dehydrogenases antagonists & inhibitors
Abstract

AKR1C3 is an important human enzyme that participates in the reduction of steroids and prostaglandins, which leads to proliferative signalling. In addition, this enzyme also participates in the biotransformation of xenobiotics, such as drugs and procarcinogens. AKR1C3 is involved in the development of both hormone-dependent and hormone-independent cancers and was recently demonstrated to confer cell resistance to anthracyclines. Because AKR1C3 is frequently upregulated in various cancers, this enzyme has been suggested as a therapeutic target for the treatment of these pathological conditions. In this study, nineteen isoquinoline alkaloids were examined for their ability to inhibit a recombinant AKR1C3 enzyme. As a result, stylopine was demonstrated to be the most potent inhibitor among the tested compounds and exhibited moderate selectivity towards AKR1C3. In the follow-up cellular studies, stylopine significantly inhibited the AKR1C3-mediated reduction of daunorubicin in intact cells without considerable cytotoxic effects. This inhibitor could therefore be used as a model AKR1C3 inhibitor in research or evaluated as a possible therapeutic anticancer drug. Furthermore, based on our results, stylopine can serve as a model compound for the design and future development of structurally related AKR1C3 inhibitors., (Copyright © 2014 Elsevier Ltd. All rights reserved.)

Published
2014
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39. Anthracycline resistance mediated by reductive metabolism in cancer cells: the role of aldo-keto reductase 1C3.

Author

Hofman J, Malcekova B, Skarka A, Novotna E, and Wsol V

Subjects
3-Hydroxysteroid Dehydrogenases antagonists & inhibitors, 3-Hydroxysteroid Dehydrogenases genetics, Aldo-Keto Reductase Family 1 Member C3, Anthracyclines agonists, Anthracyclines metabolism, Antibiotics, Antineoplastic agonists, Antibiotics, Antineoplastic metabolism, Biotransformation, Cell Line, Tumor, Cell Survival drug effects, Daunorubicin agonists, Daunorubicin metabolism, Daunorubicin pharmacology, Doxorubicin metabolism, Doxorubicin pharmacology, Drug Synergism, Enzyme Induction drug effects, Enzyme Inhibitors pharmacology, Flavanones pharmacology, Humans, Hydroxyprostaglandin Dehydrogenases antagonists & inhibitors, Hydroxyprostaglandin Dehydrogenases genetics, Idarubicin agonists, Idarubicin metabolism, Idarubicin pharmacology, Kinetics, Neoplasm Proteins antagonists & inhibitors, Neoplasm Proteins genetics, Oxidation-Reduction, Recombinant Proteins chemistry, Recombinant Proteins metabolism, 3-Hydroxysteroid Dehydrogenases metabolism, Anthracyclines pharmacology, Antibiotics, Antineoplastic pharmacology, Carcinoma drug therapy, Drug Resistance, Neoplasm drug effects, Hydroxyprostaglandin Dehydrogenases metabolism, Neoplasm Proteins metabolism
Abstract

Pharmacokinetic drug resistance is a serious obstacle that emerges during cancer chemotherapy. In this study, we investigated the possible role of aldo-keto reductase 1C3 (AKR1C3) in the resistance of cancer cells to anthracyclines. First, the reducing activity of AKR1C3 toward anthracyclines was tested using incubations with a purified recombinant enzyme. Furthermore, the intracellular reduction of daunorubicin and idarubicin was examined by employing the transfection of A549, HeLa, MCF7 and HCT 116 cancer cells with an AKR1C3 encoding vector. To investigate the participation of AKR1C3 in anthracycline resistance, we conducted MTT cytotoxicity assays with these cells, and observed that AKR1C3 significantly contributes to the resistance of cancer cells to daunorubicin and idarubicin, whereas this resistance was reversible by the simultaneous administration of 2'-hydroxyflavanone, a specific AKR1C3 inhibitor. In the final part of our work, we tracked the changes in AKR1C3 expression after anthracycline exposure. Interestingly, a reciprocal correlation between the extent of induction and endogenous levels of AKR1C3 was recorded in particular cell lines. Therefore, we suggest that the induction of AKR1C3 following exposure to daunorubicin and idarubicin, which seems to be dependent on endogenous AKR1C3 expression, eventually might potentiate an intrinsic resistance given by the normal expression of AKR1C3. In conclusion, our data suggest a substantial impact of AKR1C3 on the metabolism of daunorubicin and idarubicin, which affects their pharmacokinetic and pharmacodynamic behavior. In addition, we demonstrate that the reduction of daunorubicin and idarubicin, which is catalyzed by AKR1C3, contributes to the resistance of cancer cells to anthracycline treatment., (Copyright © 2014 Elsevier Inc. All rights reserved.)

Published
2014
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40. In vitro functional interactions of acetylcholine esterase inhibitors and muscarinic receptor antagonists in the urinary bladder of the rat.

Author

Killi UK, Wsol V, Soukup O, Kuca K, Winder M, and Tobin G

Subjects
Animals, Atropine pharmacology, Diamines pharmacology, Dose-Response Relationship, Drug, Heart Atria enzymology, Heart Atria metabolism, In Vitro Techniques, Male, Methacholine Chloride pharmacology, Muscle Contraction drug effects, Obidoxime Chloride pharmacology, Physostigmine pharmacology, Rats, Receptor Cross-Talk, Urinary Bladder enzymology, Urinary Bladder metabolism, Cholinesterase Inhibitors pharmacology, Heart Atria drug effects, Muscarinic Antagonists pharmacology, Receptor, Muscarinic M2 antagonists & inhibitors, Receptor, Muscarinic M3 antagonists & inhibitors, Urinary Bladder drug effects
Abstract

Obidoxime, a weak acetylcholine-esterase (AChE) inhibitor, exerts muscarinic receptor antagonism with a significant muscarinic M2 receptor selective profile. The current examinations aimed to determine the functional significance of muscarinic M2 receptors in the state of AChE inhibition, elucidating muscarinic M2 and M3 receptor interaction. In the in vitro examinations, methacholine evoked concentration-dependent bladder contractile and atrial frequency inhibitory responses. Although atropine abolished both, methoctramine (1 μmol/L) only affected the cholinergic response in the atrial preparations. However, in the presence of methoctramine, physostigmine, an AChE inhibitor, increased the basal tension of the bladder strip preparations (+68%), as well as the contractile responses to low concentrations of methacholine (< 5 μmol/L; +90-290%). In contrast to physostigmine, obidoxime alone raised the basal tension (+58%) and the responses to low concentrations of methacholine (< 5 μmol/L; +80-450%). Physostigmine concentration-dependently increased methacholine-evoked responses, similarly to obidoxime at low concentrations. However, at large concentrations (> 5 μmol/L), obidoxime, because of its unselective muscarinic receptor antagonism, inhibited the methacholine bladder responses. In conclusion, the current results show that muscarinic M2 receptors inhibit muscarinic M3 receptor-evoked contractile responses to low concentrations of acetylcholine in the synaptic cleft. The muscarinic M2 and M3 receptor crosstalk could be a counteracting mechanism in the treatment of AChE inhibition when using reactivators, such as obidoxime., (© 2013 Wiley Publishing Asia Pty Ltd.)

Published
2014
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41. Biochemical properties of human dehydrogenase/reductase (SDR family) member 7.

Author

Stambergova H, Skarydova L, Dunford JE, and Wsol V

Subjects
11-beta-Hydroxysteroid Dehydrogenase Type 1 chemistry, 11-beta-Hydroxysteroid Dehydrogenase Type 1 metabolism, Amino Acid Sequence, Animals, Benzaldehydes metabolism, Blotting, Western, Fluorescent Antibody Technique, Humans, Intracellular Membranes metabolism, Isoenzymes chemistry, Isoenzymes metabolism, Kinetics, Microsomes, Liver enzymology, Molecular Sequence Data, NAD metabolism, NADP metabolism, Nitrosamines chemistry, Nitrosamines metabolism, Oxidoreductases chemistry, Sf9 Cells, Spectrophotometry, Substrate Specificity, Ultracentrifugation, Oxidoreductases metabolism
Abstract

Dehydrogenase/reductase (SDR family) member 7 (DHRS7, retSDR4, SDR34C1) is a previously uncharacterized member of the short-chain dehydrogenase/reductase (SDR) superfamily. While human SDR members are known to play an important role in various (patho)biochemical pathways including intermediary metabolism and biotransformation of xenobiotics, only 20% of them are considered to be well characterized. Based on phylogenetic tree and SDR sequence clusters analysis DHRS7 is a close relative to well-known SDR member 11β-hydroxysteroid dehydrogenase 1 (11β-HSD1) that participates in metabolism of endogenous and xenobiotic substances with carbonyl group. The aim of present study is to determine the basic biochemical properties of DHRS7 and its possible involvement in metabolism of substrates with carbonyl group. For the first time the computational predictions of this membrane protein and membrane topology were experimentally confirmed. DHRS7 has been demonstrated to be an integral protein facing the lumen of the endoplasmic reticulum with lack of posttranscriptional glycosylation modification. Subsequently, NADP(H) cofactor preference and enzymatic reducing activity of DHRS7 was determined towards endogenous substrates with a steroid structure (cortisone, 4-androstene-3,17-dion) and also toward relevant exogenous substances bearing a carbonyl group harmful to human health (1,2-naphtoquinone, 9,10-phenantrenequinone). In addition to 11β-HSD1, DHRS7 is another enzyme from SDR superfamily that have been proved, at least in vitro, to contribute to the metabolism of xenobiotics with carbonyl group., (Copyright © 2013 Elsevier Ireland Ltd. All rights reserved.)

Published
2014
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42. Inhibition of nitric oxide synthase prevents muscarinic and purinergic functional changes and development of cyclophosphamide-induced cystitis in the rat.

Author

Aronsson P, Vesela R, Johnsson M, Tayem Y, Wsol V, Winder M, and Tobin G

Subjects
Adenosine pharmacology, Adenosine Triphosphate pharmacology, Animals, Cyclophosphamide, Cystitis pathology, Immunohistochemistry, In Vitro Techniques, Male, Mast Cells drug effects, Mast Cells pathology, Methacholine Chloride pharmacology, Muscle Contraction drug effects, Nitric Oxide Synthase metabolism, Rats, Sprague-Dawley, Urinary Bladder drug effects, Urinary Bladder pathology, Urinary Bladder physiopathology, Cystitis drug therapy, Cystitis physiopathology, Enzyme Inhibitors pharmacology, Enzyme Inhibitors therapeutic use, Nitric Oxide Synthase antagonists & inhibitors, Receptors, Muscarinic metabolism, Receptors, Purinergic metabolism
Abstract

Nitric oxide (NO) has pivotal roles in cyclophosphamide- (CYP-) induced cystitis during which mucosal nitric oxide synthase (NOS) and muscarinic M5 receptor expressions are upregulated. In cystitis, urothelial muscarinic NO-linked effects hamper contractility. Therefore we wondered if a blockade of this axis also affects the induction of cystitis in the rat. Rats were pretreated with saline, the muscarinic receptor antagonist 4-DAMP (1 mg/kg ip), or the NOS inhibitor L-NAME (30 mg/kg ip) for five days. 60 h before the experiments the rats were treated with saline or CYP. Methacholine-, ATP-, and adenosine-evoked responses were smaller in preparations from CYP-treated rats than from saline-treated ones. Pretreatment with 4-DAMP did not change this relation, while pretreatment with L-NAME normalized the responses in the CYP-treated animals. The functional results were strengthened by the morphological observations; 4-DAMP pretreatment did not affect the parameters studied, namely, expression of muscarinic M5 receptors, P1A1 purinoceptors, mast cell distribution, or bladder wall enlargement. However, pretreatment with L-NAME attenuated the differences. Thus, the current study provides new insights into the complex mechanisms behind CYP-induced cystitis. The NO effects coupled to urothelial muscarinic receptors have a minor role in the development of cystitis. Inhibition of NOS may prevent the progression of cystitis.

Published
2014
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43. Deeper insight into the reducing biotransformation of bupropion in the human liver.

Author

Skarydova L, Tomanova R, Havlikova L, Stambergova H, Solich P, and Wsol V

Subjects
Alcohol Oxidoreductases genetics, Biotransformation, Bupropion analogs & derivatives, Chromatography, High Pressure Liquid, Cytosol enzymology, Humans, Hydroxysteroid Dehydrogenases genetics, Kinetics, Microsomes, Liver enzymology, Mitochondria, Liver enzymology, Oxidation-Reduction, Recombinant Proteins metabolism, Alcohol Oxidoreductases metabolism, Antidepressive Agents, Second-Generation metabolism, Bupropion metabolism, Hydroxysteroid Dehydrogenases metabolism, Liver enzymology
Abstract

Bupropion is widely used as an antidepressant drug and also as a smoking cessation aid. In humans, this drug is extensively metabolized to form several metabolites. Oxidised hydroxybupropion and two reduced metabolites, threohydrobupropion and erythrohydrobupropion, are major metabolites. All of these metabolites are considered to be active. Although the oxidative metabolic pathway and the central role of CYP2B6 are known, the enzymes that participate in the reduction have not been identified to date. The aim of this study was to confirm the role of human liver subcellular fractions in the metabolism of bupropion and elucidate the contribution of particular carbonyl-reducing enzymes. An HPLC method for the determination of bupropion metabolites was utilised. Bupropion is reduced to threohydrobupropion and less to erythrohydrobupropion in human liver cytosol, microsomes and also mitochondria. Surprisingly, intrinsic clearance for formation of both metabolites is the highest in mitochondrial fraction. Moreover this study provides the first direct evidence that 11β-hydroxysteroid dehydrogenase 1, AKR1C1, AKR1C2, AKR1C3 and CBR1 participate in the reducing biotransformation of bupropion in vitro. The enzyme kinetics of all of these reductases was investigated and kinetic parameters were calculated.

Published
2014
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44. A simple identification of novel carbonyl reducing enzymes in the metabolism of the tobacco specific carcinogen NNK.

Author

Skarydova L, Zverinova M, Stambergova H, and Wsol V

Subjects
Carcinogens metabolism, Humans, Microsomes, Liver metabolism, Smoking adverse effects, Smoking metabolism, Stereoisomerism, Alcohol Oxidoreductases metabolism, Chromatography, High Pressure Liquid methods, Nitrosamines analysis, Nitrosamines metabolism, Pyridines analysis
Abstract

Tobacco smoking is the most widely known cause of human cancer-related death worldwide. NNK is one of the proved human carcinogens contributing to the development of several types of cancer. The carcinogenic effect of NNK depends on the metabolic pathway. Reduction of NNK by carbonyl reducing enzymes leads to the formation of NNAL. This pathway is generally regarded as detoxification pathway although the conditions and circumstances are quite complicated - the process depends on a formed enantiomer of NNAL. In this study a novel method for the determination of the metabolite NNAL was developed. This makes it possible to findand characterize carbonyl reducing enzymes that are involved in NNK metabolism. This simple HPLC method uses conventional HPLC instrumentation and is designed mainly for biochemical laboratories. A new microsomal carbonyl reducing enzyme participating in the metabolism of NNK in vitro has been described. Its activity was compared with other carbonyl reducing enzymes taking part in the biotransformation of NNK.

Published
2012
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45. The potential of non-adrenergic, non-cholinergic targets in the treatment of interstitial cystitis/painful bladder syndrome.

Author

Vesela R, Aronsson P, Andersson M, Wsol V, and Tobin G

Subjects
Animals, Cystitis, Interstitial pathology, Humans, Urinary Bladder drug effects, Urinary Bladder innervation, Urinary Bladder metabolism, Urinary Tract drug effects, Urinary Tract innervation, Urinary Tract metabolism, Adrenergic Neurons drug effects, Cholinergic Neurons drug effects, Cystitis, Interstitial drug therapy, Cystitis, Interstitial metabolism
Abstract

Regulation of bladder function involves both divisions of the autonomic nervous system. However, in addition to the classical autonomic transmitters, noradrenaline and acetylcholine, other autonomic transmitters and other signalling components play important roles in physiology and pathophysiology of the lower urinary tract. Several substances of neuronal non-adrenergic, non-cholinergic (NANC) systems have already proven to considerably influence functional responses in the inflamed urinary bladder. Interstitial cystitis (IC) or painful bladder syndrome (PBS) is a chronic inflammatory bladder disease, characterized by urinary frequency, urgency and pelvic pain. IC/PBS is difficult to diagnose, especially because the etiology of the condition is largely unknown. Despite the unclear nature of the cause and manifestation of IC/PBS, it has been shown that the disease involves a significant NANC component. Here, we review the possible roles of ATP, adenosine, nitric oxide, vasoactive intestinal polypeptide, substance P, and pituitary adenylate cyclase-activating peptide in the contribution to IC/PBS development and manifestation of IC/PBS symptoms.

Published
2012

46. Studies on reduction of S-nitrosoglutathione by human carbonyl reductases 1 and 3.

Author

Staab CA, Hartmanová T, El-Hawari Y, Ebert B, Kisiela M, Wsol V, Martin HJ, and Maser E

Subjects
Alcohol Dehydrogenase metabolism, Alcohol Oxidoreductases chemistry, Alcohol Oxidoreductases genetics, Amino Acid Sequence, Animals, Biocatalysis, Catalytic Domain, Cysteine metabolism, Humans, Kinetics, Mice, Models, Molecular, Molecular Sequence Data, Mutagenesis, Site-Directed, Nitrosation, Oxidation-Reduction, Alcohol Oxidoreductases metabolism, S-Nitrosoglutathione metabolism
Abstract

Human carbonyl reductases 1 and 3 (CBR1 and CBR3) are monomeric NADPH-dependent enzymes of the short-chain dehydrogenase/reductase superfamily. Despite 72% identity in primary structure they exhibit substantial differences in substrate specificity. Recently, the endogenous low molecular weight S-nitrosothiol S-nitrosoglutathione (GSNO) has been added to the broad substrate spectrum of CBR1. The current study initially addressed whether CBR3 could equally reduce GSNO which was not the case. Neither the introduction of residues which contribute to glutathione binding in CBR1, i.e. K106Q and S97V/D98A, nor the exchange C143S, which prevents a theoretical disulfide bond with C227 in CBR3, could engender activity towards GSNO. However, exchanging amino acids 236-244 in CBR3 to correspond to CBR1 was sufficient to engender catalytic activity towards GSNO. Catalytic efficiency was further improved by the exchanges Q142M, C143S, P230W and H270S. Hence, the same residues previously reported as important for reduction of carbonyl compounds appear to be key to CBR1-mediated reduction of GSNO. Furthermore, for CBR1-mediated reduction of GSNO, considerable substrate inhibition at concentrations >5 K(m) was observed. Treatment of CBR1 with GSNO followed by removal of low molecular weight compounds decreased the GSNO reducing activity, suggesting a covalent modification. Treatment with dithiothreitol, but not with ascorbic acid, could rescue the activity, indicating S-glutathionylation rather than S-nitrosation as the underlying mechanism. As C227 has previously been identified as the reactive cysteine in CBR1, the variant CBR1 C227S was generated, which, in comparison to the wild-type protein, displayed a similar k(cat), but a 30-fold higher K(m), and did not show substrate inhibition. Collectively, the results clearly argue for a physiological role of CBR1, but not for CBR3, in GSNO reduction and thus ultimately in regulation of NO signaling. Furthermore, at higher concentrations, GSNO appears to work as a suicide inhibitor for CBR1, probably through glutathionylation of C227., (Copyright © 2011 Elsevier Ireland Ltd. All rights reserved.)

Published
2011
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47. Structural basis for substrate specificity in human monomeric carbonyl reductases.

Author

Pilka ES, Niesen FH, Lee WH, El-Hawari Y, Dunford JE, Kochan G, Wsol V, Martin HJ, Maser E, and Oppermann U

Subjects
Aldehyde Reductase, Aldo-Keto Reductases, Antineoplastic Agents pharmacology, Cloning, Molecular, Crystallography, X-Ray methods, Ethanolamines chemistry, Humans, Isoquinolines chemistry, Kinetics, Mutagenesis, Mutagenesis, Site-Directed, Structure-Activity Relationship, Substrate Specificity, Temperature, Xenobiotics chemistry, Alcohol Oxidoreductases chemistry
Abstract

Unlabelled: Carbonyl reduction constitutes a phase I reaction for many xenobiotics and is carried out in mammals mainly by members of two protein families, namely aldo-keto reductases and short-chain dehydrogenases/reductases. In addition to their capacity to reduce xenobiotics, several of the enzymes act on endogenous compounds such as steroids or eicosanoids. One of the major carbonyl reducing enzymes found in humans is carbonyl reductase 1 (CBR1) with a very broad substrate spectrum. A paralog, carbonyl reductase 3 (CBR3) has about 70% sequence identity and has not been sufficiently characterized to date. Screening of a focused xenobiotic compound library revealed that CBR3 has narrower substrate specificity and acts on several orthoquinones, as well as isatin or the anticancer drug oracin. To further investigate structure-activity relationships between these enzymes we crystallized CBR3, performed substrate docking, site-directed mutagenesis and compared its kinetic features to CBR1. Despite high sequence similarities, the active sites differ in shape and surface properties. The data reveal that the differences in substrate specificity are largely due to a short segment of a substrate binding loop comprising critical residues Trp229/Pro230, Ala235/Asp236 as well as part of the active site formed by Met141/Gln142 in CBR1 and CBR3, respectively. The data suggest a minor role in xenobiotic metabolism for CBR3., Enhanced Version: This article can also be viewed as an enhanced version in which the text of the article is integrated with interactive 3D representations and animated transitions. Please note that a web plugin is required to access this enhanced functionality. Instructions for the installation and use of the web plugin are available in Text S1.

Published
2009
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48. Inactivation of the anticancer drugs doxorubicin and oracin by aldo-keto reductase (AKR) 1C3.

Author

Novotna R, Wsol V, Xiong G, and Maser E

Subjects
3-Hydroxysteroid Dehydrogenases genetics, Aldo-Keto Reductase Family 1 Member C3, Humans, Hydroxyprostaglandin Dehydrogenases genetics, Recombinant Proteins biosynthesis, Recombinant Proteins isolation & purification, 3-Hydroxysteroid Dehydrogenases physiology, Antibiotics, Antineoplastic metabolism, Doxorubicin metabolism, Ethanolamines metabolism, Hydroxyprostaglandin Dehydrogenases physiology, Isoquinolines metabolism
Abstract

Resistance towards anticancer drugs is a general problem upon chemotherapy. Among the mechanisms of resistance, metabolic inactivation by carbonyl reduction is a major cause of chemotherapy failure that applies to drugs bearing a carbonyl moiety. Oracin is a promising anticancer drug which is presently in phase II clinical trials. Pharmacokinetic studies have revealed that oracin undergoes metabolic inactivation by carbonyl reduction. In the present study, we provide evidence that AKR1C3, a member of the aldo-keto reductase (AKR) superfamily, catalyzes the inactivation of oracin. Moreover, AKR1C3 does also mediate C13 carbonyl reduction of doxorubicin to its inactive hydroxy metabolite doxorubicinol. Doxorubicinol, however, has also been considered responsible for the cardiomyopathy observed upon doxorubicin chemotherapy. Since AKR1C3 is overexpressed in hormone-dependent malignancies like prostate and breast cancer, coadministration of AKR1C3 inhibitors might enhance the chemotherapeutic efficacy of oracin and doxorubicin, and simultaneously reduce the risk of cardiomyopathy upon doxorubicin treatment.

Published
2008
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49. Liquid chromatography-tandem mass spectrometry in chiral study of amlodipine biotransformation in rat hepatocytes.

Author

Suchanova B, Sispera L, and Wsol V

Abstract

A high proportion of drugs are chiral compounds used as racemic mixtures in a clinical practice. Very often only one of two enantiomers exhibits a desired pharmacological effect. Amlodipine, 2-[(2-aminoethoxy)methyl]-4-(2-chlorophenyl)-3-ethoxycarbonyl-5-methoxycarbonyl-6-methyl-1,4-dihydropyridine, is a chiral calcium channel blocker, currently used as a racemate in clinical practice. Racemic mixture is used even though it is known that R- and S-amlodipine do not have the same biological activity and only S-amlodipine possesses vasodilating properties. In this work a novel reversed phase liquid chromatography (RP-LC) separation method for amlodipine and its metabolites was developed. Based on this separation chiral aspects of amlodipine biotransformation were studied by incubation of amlodipine and its two individual enantiomers with primary culture of rat hepatocytes. Structure of the metabolites was elucidated using a liquid chromatography (LC) separation with ultraviolet (UV) and mass spectrometry (MS) detection. An LC-tandem MS (MS/MS) method was used to establish fragmentation pattern of amlodipine and its metabolites. Eight metabolites presented in the highest amount were identified and semiquantified by employing an LC separation. Basically two types of metabolites were detected, reduced type--dihydropyridine metabolites and oxidized type--pyridine metabolites. Other metabolic modification included changes of functional groups, e.g., methylester hydrolysis or acetylation of amino group. The results exhibited that R-amlodipine was stereoselectively metabolized by the respective biotransformation enzymes in rat liver hepatocytes and it is also demonstrated by greater extent of R-amlodipine conversion into metabolites where the values for R-amlodipine are for the most metabolites higher than those for metabolites of S-amlodipine.

Published
2006
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50. Purification and characterization of akr1b10 from human liver: role in carbonyl reduction of xenobiotics.

Author

Martin HJ, Breyer-Pfaff U, Wsol V, Venz S, Block S, and Maser E

Subjects
Aldo-Keto Reductases, Base Sequence, Electrophoresis, Polyacrylamide Gel, Escherichia coli genetics, Humans, Immunoblotting, Inactivation, Metabolic, Molecular Sequence Data, Oxidation-Reduction, Recombinant Proteins genetics, Recombinant Proteins isolation & purification, Spectrometry, Mass, Electrospray Ionization, Xenobiotics chemistry, Aldehyde Reductase genetics, Aldehyde Reductase isolation & purification, Aldehyde Reductase physiology, Liver enzymology, Xenobiotics pharmacokinetics
Abstract

Members of the aldo-keto reductase (AKR) superfamily have a broad substrate specificity in catalyzing the reduction of carbonyl group-containing xenobiotics. In the present investigation, a member of the aldose reductase subfamily, AKR1B10, was purified from human liver cytosol. This is the first time AKR1B10 has been purified in its native form. AKR1B10 showed a molecular mass of 35 kDa upon gel filtration and SDS-polyacrylamide gel electrophoresis. Kinetic parameters for the NADPH-dependent reduction of the antiemetic 5-HT3 receptor antagonist dolasetron, the antitumor drugs daunorubicin and oracin, and the carcinogen 4-methylnitrosamino-1-(3-pyridyl)-1-butanone (NNK) to the corresponding alcohols have been determined by HPLC. Km values ranged between 0.06 mM for dolasetron and 1.1 mM for daunorubicin. Enzymatic efficiencies calculated as kcat/Km were more than 100 mM-1 min-1 for dolasetron and 1.3, 0.43, and 0.47 mM-1 min-1 for daunorubicin, oracin, and NNK, respectively. Thus, AKR1B10 is one of the most significant reductases in the activation of dolasetron. In addition to its reducing activity, AKR1B10 catalyzed the NADP+-dependent oxidation of the secondary alcohol (S)-1-indanol to 1-indanone with high enzymatic efficiency (kcat/Km=112 mM-1 min-1). The gene encoding AKR1B10 was cloned from a human liver cDNA library and the recombinant enzyme was purified. Kinetic studies revealed lower activity of the recombinant compared with the native form. Immunoblot studies indicated large interindividual variations in the expression of AKR1B10 in human liver. Since carbonyl reduction of xenobiotics often leads to their inactivation, AKR1B10 may play a role in the occurrence of chemoresistance of tumors toward carbonyl group-bearing cytostatic drugs.

Published
2006
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