Your search keyword '"Windshügel B"' showing total 42 results

1. LEADS-FRAG: A Benchmark Data Set for Assessment of Fragment Docking Performance

Author

Chachulski, L., Windshügel, B., and Publica

Abstract

Fragment-based drug design is a popular approach in drug discovery, which makes use of computational methods such as molecular docking. To assess fragment placement performance of molecular docking programs, we constructed LEADS-FRAG, a benchmark data set containing 93 high-quality protein-fragment complexes that were selected from the Protein Data Bank using a rational and unbiased process. The data set contains fully prepared protein and fragment structures and is publicly available. Moreover, we used LEADS-FRAG for evaluating the small-molecule docking programs AutoDock, AutoDock Vina, FlexX, and GOLD for their fragment docking performance. GOLD in combination with the scoring function ChemPLP and AutoDock Vina performed best and generated near-native conformations (root mean square deviation

Published

2020

2. Differential effects of clinically used derivatives and metabolites of artemisinin in the activation of constitutive androstane receptor isoforms

Author

Burk, O, Piedade, R, Ghebreghiorghis, L, Fait, J T, Nussler, A K, Gil, J P, Windshügel, B, and Schwab, M

Published

2012

3. Identification of novel CAR agonists by using two-step virtual screening together with in vitro assays: P178

Author

Vanamo, J, Windshügel, B, Jyrkkärinne, J, Poso, A, Sippl, W, and Honkakoski, P

Published

2008

4. Identification and Characterization of Approved Drugs and Drug-Like Compounds as Covalent Escherichia coli ClpP Inhibitors

Author

Sassetti, E., Durante Cruz, C., Tammela, P., Winterhalter, M., Augustyns, K., Gribbon, P., Windshügel, B., Division of Pharmaceutical Biosciences, Bioactivity Screening Group, Drug Research Program, and Publica

Subjects

ClpP, PROTEASE, 116 Chemical sciences, Escherichia coli, RECOGNITION, ANTIBIOTIC-RESISTANCE, high-throughput screening, FAMILY, inhibitor, lcsh:Chemistry, Chemistry, nitric oxide stress, lcsh:Biology (General), lcsh:QD1-999, 317 Pharmacy, covalent binding, ACID, 1182 Biochemistry, cell and molecular biology, Biology, lcsh:QH301-705.5, surface plasmon resonance

Abstract

The serine protease Caseinolytic protease subunit P (ClpP) plays an important role for protein homeostasis in bacteria and contributes to various developmental processes, as well as virulence. Therefore, ClpP is considered as a potential drug target in Gram-positive and Gram-negative bacteria. In this study, we utilized a biochemical assay to screen several small molecule libraries of approved and investigational drugs for Escherichia coli ClpP inhibitors. The approved drugs bortezomib, cefmetazole, cisplatin, as well as the investigational drug cDPCP, and the protease inhibitor 3,4-dichloroisocoumarin (3,4-DIC) emerged as ClpP inhibitors with IC50 values ranging between 0.04 and 31 &micro, M. Compound profiling of the inhibitors revealed cefmetazole and cisplatin not to inhibit the serine protease bovine &alpha, chymotrypsin, and for cefmetazole no cytotoxicity against three human cell lines was detected. Surface plasmon resonance studies demonstrated all novel ClpP inhibitors to bind covalently to ClpP. Investigation of the potential binding mode for cefmetazole using molecular docking suggested a dual covalent binding to Ser97 and Thr168. While only the antibiotic cefmetazole demonstrated an intrinsic antibacterial effect, cDPCP clearly delayed the bacterial growth recovery time upon chemically induced nitric oxide stress in a ClpP-dependent manner.

Published

2019

5. Identification of novel agonists by high-throughput screening and molecular modelling of human constitutive androstane receptor isoform 3

Author

Keminer, O., Windshügel, B., Essmann, F., Lee, S.M.L., Schiergens, T.S., Schwab, M., Burk, O., and Publica

Abstract

Prediction of drug interactions, based on the induction of drug disposition, calls for the identification of chemicals, which activate xenosensing nuclear receptors. Constitutive androstane receptor (CAR) is one of the major human xenosensors; however, the constitutive activity of its reference variant CAR1 in immortalized cell lines complicates the identification of agonists. The exclusively ligand-dependent isoform CAR3 represents an obvious alternative for screening of CAR agonists. As CAR3 is even more abundant in human liver than CAR1, identification of its agonists is also of pharmacological value in its own right. We here established a cellular high-throughput screening assay for CAR3 to identify ligands of this isoform and to analyse its suitability for identifying CAR ligands in general. Proof-of-concept screening of 2054 drug-like compounds at 10 µM resulted in the identification of novel CAR3 agonists. The CAR3 assay proved to detect the previously described CAR1 ligands in the screened libraries. However, we failed to detect CAR3-selective compounds, as the four novel agonists, which were selected for further investigations, all proved to activate CAR1 in different cellular and in vitro assays. In primary human hepatocytes, the compounds preferentially induced the expression of the prototypical CAR target gene CYP2B6. Failure to identify CAR3-selective compounds was investigated by molecular modelling, which showed that the isoform-specific insertion of five amino acids did not impact on the ligand binding pocket but only on heterodimerization with retinoid X receptor. In conclusion, we demonstrate here the usability of CAR3 for screening compound libraries for the presence of CAR agonists.

Published

2019

6. Electronic laboratory notebooks in a public-private partnership

Author

Vaas, L.A.I., Witt, G., Windshügel, B., Bosin, A., Serra, G., Bruengger, A., Winterhalter, M., Gribbon, P., Levy-Petelinkar, C.J., Kohler, M., and Publica

Abstract

This report shares the experience during selection, implementation and maintenance phases of an electronic laboratory notebook (ELN) in a public-private partnership project and comments on user's feedback. In particular, we address which time constraints for roll-out of an ELN exist in granted projects and which benefits and/or restrictions come with out-of-the-box solutions. We discuss several options for the implementation of support functions and potential advantages of open access solutions. Connected to that, we identified willingness and a vivid culture of data sharing as the major item leading to success or failure of collaborative research activities. The feedback from users turned out to be the only angle for driving technical improvements, but also exhibited high efficiency. Based on these experiences, we describe best practices for future projects on implementation and support of an ELN supporting a diverse, multidisciplinary user group based in academia, NGO s, and/or for-profit corporations located in multiple time zones.

Published

2016

7. LEADS-PEP: A benchmark data set for assessment of peptide docking performance

Author

Hauser, A.S., Windshügel, B., and Publica

Abstract

With increasing interest in peptide-based therapeutics also the application of computational approaches such as peptide docking has gained more and more attention. In order to assess the suitability of docking programs for peptide placement and to support the development of peptide specific docking tools, an independently constructed benchmark data set is urgently needed. Here we present the LEADS-PEP benchmark data set for assessing peptide docking performance. Using a rational and unbiased workflow, 53 protein-peptide complexes with peptide lengths ranging from 3 to 12 residues were selected. The data set is publicly accessible at www.leads-x.org. In a second step we evaluated several small molecule docking programs for their potential to reproduce peptide conformations as present in LEADS-PEP. While most tested programs were capable to generate native-like binding modes of small peptides, only Surflex-Dock and AutoDock Vina performed reasonably well for peptides consisting of more than five residues. Rescoring of docking poses with scoring functions ChemPLP, ChemScore, and ASP further increased the number of top-ranked near-native conformations. Our results suggest that small molecule docking programs are a good and fast alternative to specialised peptide docking programs.

Published

2016

8. Biophysical characterization of E. coli TolC interaction with the known blocker hexaamminecobalt

Author

Gilardi, A., primary, Bhamidimarri, S.P., additional, Brönstrup, M., additional, Bilitewski, U., additional, Marreddy, R.K.R., additional, Pos, K.M., additional, Benier, L., additional, Gribbon, P., additional, Winterhalter, M., additional, and Windshügel, B., additional

Published

2017

9. Biophysical characterization of E. coli TolC interaction with the known blocker hexaamminecobalt.

Author

Gribbon, P., Windshügel, B., Gilardi, A., Bhamidimarri, S.P., Benier, L., Winterhalter, M., Brönstrup, M., Bilitewski, U., Marreddy, R.K.R., and Pos, K.M.

Subjects

*ESCHERICHIA coli, *PHYSICAL biochemistry, *ANTIBIOTICS, *LIGANDS (Biochemistry), *ERYTHROMYCIN

Abstract

Background The tripartite efflux pump AcrAB-TolC in E. coli is involved in drug resistance by transporting antibiotics out of the cell. The outer membrane protein TolC can be blocked by various cations, including hexaamminecobalt, thereby TolC represents a potential target for reducing antimicrobial resistance as its blockage may improve efficacy of antibiotics. Methods We utilized single channel electrophysiology measurements for studying TolC conductance in the absence and presence of the known TolC blocker hexaamminecobalt. Association and dissociation constants of hexaamminecobalt were determined using surface plasmon resonance measurements. Minimum inhibitory concentration (MIC) assays in the absence and presence of antibiotics were carried out for investigating the antibacterial effect of hexaamminecobalt and its potential to reduce MICs. Results TolC gating in the absence of any ligand is voltage dependent and asymmetric at high applied voltages. Hexaamminecobalt binds to TolC with high affinity and kinetic data revealed fast association and dissociation rates. Despite potent binding to TolC, hexaamminecobalt does not possess an intrinsic antimicrobial activity against E. coli nor does it reduce MIC values of antibiotics erythromycin and fusidic acid. Conclusions TolC opening can be effectively blocked by small molecules. More potent channel blockers are needed in order to investigate the eligibility of TolC as drug target. General significance TolC, a potentially interesting pharmaceutical target can be addressed by small molecules, blocking the channel. Biophysical characterization of the binding processes will support future identification and optimisation of more potent TolC blockers in order to validate TolC as a pharmaceutical target. [ABSTRACT FROM AUTHOR]

Published

2017

10. Identification of novel CAR agonists for drug development

Author

Vanamo, J., primary, Windshügel, B., additional, Jyrkkärinne, J., additional, Poso, A., additional, Sippl, W., additional, and Honkakoski, P., additional

Published

2008

11. Molecular modeling of prostate specific antigen (PSA) and the design of compounds modulating its activity

Author

Härkönen, H.H., primary, Wallén, E.A.A., additional, Windshügel, B., additional, Lahtela-Kakkonen, M., additional, and Poso, A., additional

Published

2008

12. Substrate Analogues Entering the Lipoic Acid Salvage Pathway via Lipoate-Protein Ligase 2 Interfere with Staphylococcus aureus Virulence.

Author

Scattolini A, Grammatoglou K, Nikitjuka A, Jirgensons A, Mansilla MC, and Windshügel B

Subjects

Animals, Bacterial Proteins metabolism, Bacterial Proteins genetics, Caenorhabditis elegans, Peptide Synthases metabolism, Peptide Synthases genetics, Staphylococcal Infections microbiology, Staphylococcal Infections drug therapy, Virulence, Anti-Bacterial Agents pharmacology, Anti-Bacterial Agents chemistry, Staphylococcus aureus drug effects, Staphylococcus aureus enzymology, Staphylococcus aureus genetics, Thioctic Acid analogs & derivatives

Abstract

Lipoic acid (LA) is an essential cofactor in prokaryotic and eukaryotic organisms, required for the function of several multienzyme complexes such as oxoacid dehydrogenases. Prokaryotes either synthesize LA or salvage it from the environment. The salvage pathway in Staphylococcus aureus includes two lipoate-protein ligases, LplA1 and LplA2, as well as the amidotransferase LipL. In this study, we intended to hijack the salvage pathway by LA analogues that are transferred via LplA2 and LipL to the E2 subunits of various dehydrogenases, thereby resulting in nonfunctional enzymes that eventually impair viability of the bacterium. Initially, a virtual screening campaign was carried out to identify potential LA analogues that bind to LplA2. Three selected compounds affected S. aureus USA300 growth in minimal medium at concentrations ranging from 2.5 to 10 μg/mL. Further analysis of the most potent compound ( Lpl-004 ) revealed its transfer to E2 subunits of dehydrogenase complexes and a negative impact on its functionality. Growth impairment caused by Lpl-004 treatment was restored by adding products of the lipoate-dependent enzyme complexes. In addition, Caenorhabditis elegans infected with LpL-004 -treated USA300 demonstrated a significantly expanded lifespan compared to worms infected with untreated bacteria. Our results provide evidence that LA analogues exploiting the LA salvage pathway represent an innovative strategy for the development of novel antimicrobial substances.

Published

2024

13. Drug repurposing screen to identify inhibitors of the RNA polymerase (nsp12) and helicase (nsp13) from SARS-CoV-2 replication and transcription complex.

Author

Kuzikov M, Reinshagen J, Wycisk K, Corona A, Esposito F, Malune P, Manelfi C, Iaconis D, Beccari A, Tramontano E, Nowotny M, Windshügel B, Gribbon P, and Zaliani A

Subjects

Humans, Drug Repositioning, DNA-Directed RNA Polymerases, DNA Helicases genetics, DNA Helicases metabolism, Viral Nonstructural Proteins metabolism, SARS-CoV-2 metabolism, COVID-19

Abstract

Coronaviruses contain one of the largest genomes among the RNA viruses, coding for 14-16 non-structural proteins (nsp) that are involved in proteolytic processing, genome replication and transcription, and four structural proteins that build the core of the mature virion. Due to conservation across coronaviruses, nsps form a group of promising drug targets as their inhibition directly affects viral replication and, therefore, progression of infection. A minimal but fully functional replication and transcription complex was shown to be formed by one RNA-dependent RNA polymerase (nsp12), one nsp7, two nsp8 accessory subunits, and two helicase (nsp13) enzymes. Our approach involved, targeting nsp12 and nsp13 to allow multiple starting point to interfere with virus infection progression. Here we report a combined in-vitro repurposing screening approach, identifying new and confirming reported SARS-CoV-2 nsp12 and nsp13 inhibitors., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 The Authors. Published by Elsevier B.V. All rights reserved.)

Published

2024

14. Efflux Pump-Binding 4(3-Aminocyclobutyl)Pyrimidin-2-Amines Are Colloidal Aggregators.

Author

Szal T, Chauhan SS, Lewe P, Rachad FZ, Madre M, Paunina L, Witt S, Parthasarathi R, and Windshügel B

Subjects

Escherichia coli metabolism, Periplasm metabolism, Anti-Bacterial Agents pharmacology, Anti-Bacterial Agents metabolism, Multidrug Resistance-Associated Proteins metabolism, Membrane Transport Proteins metabolism, Escherichia coli Proteins metabolism

Abstract

Efflux pumps are a relevant factor in antimicrobial resistance. In E. coli , the tripartite efflux pump AcrAB-TolC removes a chemically diverse set of antibiotics from the bacterium. Therefore, small molecules interfering with efflux pump function are considered adjuvants for improving antimicrobial therapies. Several compounds targeting the periplasmic adapter protein AcrA and the efflux pump AcrB have been identified to act synergistically with different antibiotics. Among those, several 4(3-aminocyclobutyl)pyrimidin-2-amines have been shown to bind to both proteins. In this study, we intended to identify analogs of these substances with improved binding affinity to AcrA using virtual screening followed by experimental validation. While we succeeded in identifying several compounds showing a synergistic effect with erythromycin on E. coli , biophysical studies suggested that 4(3-aminocyclobutyl)pyrimidin-2-amines form colloidal aggregates that do not bind specifically to AcrA. Therefore, these substances are not suited for further development. Our study emphasizes the importance of implementing additional control experiments to identify aggregators among bioactive compounds.

Published

2023

15. Identification of Src as a Therapeutic Target in Oesophageal Adenocarcinoma through Functional Genomic and High-Throughput Drug Screening Approaches.

Author

McCabe NH, Stevenson L, Scanlon E, Douglas R, Kennedy S, Keminer O, Windshügel B, Zisterer D, Kennedy RD, Blayney JK, and Turkington RC

Abstract

Drug resistance limits the effectiveness of oesophageal adenocarcinoma (OAC) chemotherapies, leading to a poor prognosis for this disease. Elucidation of the underlying resistance mechanisms is key to enabling the identification of more effective treatments. This study, therefore, aims to identify novel therapeutic and/or chemotherapy sensitising drug targets in OAC. Transcriptional data from a cohort of 273 pre-treatment OAC biopsies, from patients who received neoadjuvant chemotherapy followed by surgical resection, were analysed using gene set enrichment analysis (GSEA) to determine differential gene expression between responding and non-responding OAC tumours. From this, 80 genes were selected for high-throughput siRNA screening in OAC cell lines with or without standard chemotherapy treatment. In parallel, cell viability assays were performed using a panel of FDA-approved drugs and combination index (CI) values were calculated to evaluate drug synergy with standard chemotherapy. Mechanisms of synergy were investigated using western blot, propidium iodide flow cytometry, and proliferation assays. Taken together, the screens identified that targeting Src, using either siRNA or the small molecule inhibitor dasatinib, enhanced the efficacy of chemotherapy in OAC cells. Further in vitro functional analysis confirmed Src inhibition to be synergistic with standard OAC chemotherapies, 5-fluorouracil (5-FU), and cisplatin (CDDP). In conclusion, a compound screen together with a functional genomic approach identified Src as a potential chemosensitising target in OAC, which could be assessed in a clinical study for poor prognosis OAC patients.

Published

2022

16. Development and Experimental Validation of Regularized Machine Learning Models Detecting New, Structurally Distinct Activators of PXR.

Author

Hirte S, Burk O, Tahir A, Schwab M, Windshügel B, and Kirchmair J

Subjects

Ligands, Machine Learning, Pregnane X Receptor, Xenobiotics, Receptors, Steroid metabolism

Abstract

The pregnane X receptor (PXR) regulates the metabolism of many xenobiotic and endobiotic substances. In consequence, PXR decreases the efficacy of many small-molecule drugs and induces drug-drug interactions. The prediction of PXR activators with theoretical approaches such as machine learning (ML) proves challenging due to the ligand promiscuity of PXR, which is related to its large and flexible binding pocket. In this work we demonstrate, by the example of random forest models and support vector machines, that classifiers generated following classical training procedures often fail to predict PXR activity for compounds that are dissimilar from those in the training set. We present a novel regularization technique that penalizes the gap between a model's training and validation performance. On a challenging test set, this technique led to improvements in Matthew correlation coefficients (MCCs) by up to 0.21. Using these regularized ML models, we selected 31 compounds that are structurally distinct from known PXR ligands for experimental validation. Twelve of them were confirmed as active in the cellular PXR ligand-binding domain assembly assay and more hits were identified during follow-up studies. Comprehensive analysis of key features of PXR biology conducted for three representative hits confirmed their ability to activate the PXR.

Published

2022

17. Structure-based discovery of small molecules improving stability of human broadly-neutralizing anti-HIV antibody 2F5 in plant suspension cells.

Author

Mandal MK, Kronenberger T, Zulka MI, Windshügel B, and Schiermeyer A

Subjects

Animals, HIV Envelope Protein gp41 metabolism, Humans, Mammals, Recombinant Proteins metabolism, Serine Proteases metabolism, Nicotiana genetics, Nicotiana metabolism, HIV Antibodies metabolism, HIV-1

Abstract

The production of biopharmaceuticals in engineered plant-based systems is a promising technology that has proven its suitability for the production of various recombinant glyco-proteins that are currently undergoing clinical trials. However, compared to mammalian cell lines, the productivity of plant-based systems still requires further improvement. A major obstacle is the proteolytic degradation of recombinant target proteins by endogenous plant proteases mainly from the subtilisin family of serine proteases. In the present study, the authors screened for putative small molecule inhibitors for subtilases that are secreted from tobacco BY-2 suspension cells using an in silico approach. The effectiveness of the substances identified in this screen was subsequently tested in degradation assays using the human broadly-neutralizing anti-HIV monoclonal antibody 2F5 (mAb2F5) and spent BY-2 culture medium as a model system. Among 16 putative inhibitors identified by in silico studies, three naphthalene sulfonic acid derivatives showed inhibitory activity in in vitro degradation assays and are similar to or even more effective than phenylmethylsulfonyl fluoride (PMSF), a classical inhibitor of serine proteases, which served as positive control., (© 2022 The Authors. Biotechnology Journal published by Wiley-VCH GmbH.)

Published

2022

18. Nelfinavir and Its Active Metabolite M8 Are Partial Agonists and Competitive Antagonists of the Human Pregnane X Receptor.

Author

Burk O, Kronenberger T, Keminer O, Lee SML, Schiergens TS, Schwab M, and Windshügel B

Subjects

ATP Binding Cassette Transporter, Subfamily B genetics, Binding Sites, Cytochrome P-450 CYP3A genetics, Dose-Response Relationship, Drug, Gene Expression Regulation drug effects, Hep G2 Cells, Hepatocytes cytology, Hepatocytes drug effects, Humans, Models, Molecular, Molecular Conformation, Molecular Docking Simulation, Nelfinavir chemistry, Pregnane X Receptor agonists, Pregnane X Receptor antagonists & inhibitors, Pregnane X Receptor chemistry, Primary Cell Culture, Hepatocytes metabolism, Nelfinavir analogs & derivatives, Nelfinavir pharmacology, Pregnane X Receptor metabolism

Abstract

The HIV protease inhibitor nelfinavir is currently being analyzed for repurposing as an anticancer drug for many different cancers because it exerts manifold off-target protein interactions, finally resulting in cancer cell death. Xenosensing pregnane X receptor (PXR), which also participates in the control of cancer cell proliferation and apoptosis, was previously shown to be activated by nelfinavir; however, the exact molecular mechanism is still unknown. The present study addresses the effects of nelfinavir and its major and pharmacologically active metabolite nelfinavir hydroxy- tert -butylamide (M8) on PXR to elucidate the underlying molecular mechanism. Molecular docking suggested direct binding to the PXR ligand-binding domain, which was confirmed experimentally by limited proteolytic digestion and competitive ligand-binding assays. Concentration-response analyses using cellular transactivation assays identified nelfinavir and M8 as partial agonists with EC 50 values of 0.9 and 7.3 µM and competitive antagonists of rifampin-dependent induction with IC 50 values of 7.5 and 25.3 µM, respectively. Antagonism exclusively resulted from binding into the PXR ligand-binding pocket. Impaired coactivator recruitment by nelfinavir as compared with the full agonist rifampin proved to be the underlying mechanism of both effects on PXR. Physiologic relevance of nelfinavir-dependent modulation of PXR activity was investigated in respectively treated primary human hepatocytes, which showed differential induction of PXR target genes and antagonism of rifampin-induced ABCB1 and CYP3A4 gene expression. In conclusion, we elucidate here the molecular mechanism of nelfinavir interaction with PXR. It is hypothesized that modulation of PXR activity may impact the anticancer effects of nelfinavir. SIGNIFICANCE STATEMENT: Nelfinavir, which is being investigated for repurposing as an anticancer medication, is shown here to directly bind to human pregnane X receptor (PXR) and thereby act as a partial agonist and competitive antagonist. Its major metabolite nelfinavir hydroxy- tert -butylamide exerts the same effects, which are based on impaired coactivator recruitment. Nelfinavir anticancer activity may involve modulation of PXR, which itself is discussed as a therapeutic target in cancer therapy and for the reversal of chemoresistance., (Copyright © 2021 by The Author(s).)

Published

2021

19. LEADS-FRAG: A Benchmark Data Set for Assessment of Fragment Docking Performance.

Author

Chachulski L and Windshügel B

Subjects

Ligands, Molecular Docking Simulation, Protein Binding, Benchmarking, Software

Abstract

Fragment-based drug design is a popular approach in drug discovery, which makes use of computational methods such as molecular docking. To assess fragment placement performance of molecular docking programs, we constructed LEADS-FRAG, a benchmark data set containing 93 high-quality protein-fragment complexes that were selected from the Protein Data Bank using a rational and unbiased process. The data set contains fully prepared protein and fragment structures and is publicly available. Moreover, we used LEADS-FRAG for evaluating the small-molecule docking programs AutoDock, AutoDock Vina, FlexX, and GOLD for their fragment docking performance. GOLD in combination with the scoring function ChemPLP and AutoDock Vina performed best and generated near-native conformations (root mean square deviation <1.5 Å) for more than 50% of the data set considering the top-ranked docking pose. Taking into account all docking poses, the tested programs generated near-native conformations for up to 86% of the fragments in LEADS-FRAG. By rescoring all docking poses with the GOLD scoring functions and the Protein-Ligand Informatics force field, the number of near-native conformations increased up to 40% with respect to the top-rescored poses. Our results show that conventional small-molecule docking programs achieve a satisfactory fragment docking performance when utilizing rescoring.

Published

2020

20. A tiered high-throughput screening approach for evaluation of estrogen and androgen receptor modulation by environmentally relevant bisphenol A substitutes.

Author

Keminer O, Teigeler M, Kohler M, Wenzel A, Arning J, Kaßner F, Windshügel B, and Eilebrecht E

Subjects

Endocrine Disruptors, Receptors, Androgen, Retrospective Studies, Benzhydryl Compounds chemistry, Phenols chemistry

Abstract

Bisphenol A (BPA) is a high production volume chemical with a broad application spectrum. As an endocrine disrupting chemical, mainly by modulation of nuclear receptors (NRs), BPA has an adverse impact on organisms and is identified as a substance of very high concern under the European REACH regulation. Various BPA substitution candidates have been developed in recent years, however, information concerning the endocrine disrupting potential of these substances is still incomplete or missing. In this study, we intended to investigate the endocrine potential of BPA substitution candidates used in environmentally relevant applications such as thermal paper or epoxy resins. Based on an extensive literature and patent search, 33 environmentally relevant BPA substitution candidates were identified. In order to evaluate the endocrine potential of the BPA replacements, a screening cascade consisting of biochemical and cell-based assays was employed to investigate substance binding to the NRs estrogen receptor α and β, as well as androgen receptor, co-activator recruitment and NR-mediated reporter gene activation. In addition, a computational docking approach for retrospective prediction of receptor binding was carried out. Our results show that some BPA substitution candidates, for which so far no or only very few data were available, possess a substantial endocrine disrupting potential (TDP, BPZ), while several substances (BPS, D-8, DD70, DMP-OH, TBSA, D4, CBDO, ISO, VITC, DPA, and DOPO) did not reveal any NR binding., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2019 The Author(s). Published by Elsevier B.V. All rights reserved.)

Published

2020

21. Structural insights into ligand-binding pocket formation in Nurr1 by molecular dynamics simulations.

Author

Windshügel B

Subjects

Binding Sites, Crystallography, X-Ray, Docosahexaenoic Acids chemistry, Ligands, Molecular Docking Simulation, Protein Domains, Structural Homology, Protein, Molecular Dynamics Simulation, Nuclear Receptor Subfamily 4, Group A, Member 2 chemistry

Abstract

The nuclear receptor Nurr1 (NR4A2) has been identified as a potential target for the treatment of Parkinson's disease. In contrast to most other nuclear receptors, the X-ray crystal structure of the Nurr1 ligand-binding domain (LBD) lacks any ligand-binding pocket (LBP). However, NMR spectroscopy measurements have revealed that the known Nurr1 agonist docosahexaenoic acid (DHA) binds to a region within the LBD that corresponds to the classical NR ligand-binding pocket (LBP). In order to investigate the structural dynamics of the Nurr1 LBD and to study potential LBP formation, the conformational space of the receptor was sampled using a molecular dynamics (MD) simulation. Docking of DHA into 50,000 LBD structures extracted from the simulation revealed the existence of a transient LBP that is capable to fully harbor the compound. The location of the identified pocket overlaps with the ligand-binding site suggested by NMR experiments. Structural analysis of the protein-ligand complex showed that only modest structural rearrangements within the Nurr1 LBD are required for LBP formation. These findings may support structure-based drug discovery campaigns for the development of receptor-specific agonists.

Published

2019

22. Activation of Caspase-6 Is Promoted by a Mutant Huntingtin Fragment and Blocked by an Allosteric Inhibitor Compound.

Author

Ehrnhoefer DE, Skotte NH, Reinshagen J, Qiu X, Windshügel B, Jaishankar P, Ladha S, Petina O, Khankischpur M, Nguyen YTN, Caron NS, Razeto A, Meyer Zu Rheda M, Deng Y, Huynh KT, Wittig I, Gribbon P, Renslo AR, Geffken D, Gul S, and Hayden MR

Subjects

Allosteric Regulation genetics, Animals, Apoptosis, COS Cells, Caspase 6 physiology, Chlorocebus aethiops, Huntingtin Protein metabolism, Huntington Disease pathology, Molecular Docking Simulation methods, Nerve Tissue Proteins metabolism, Neurons metabolism, Nuclear Proteins metabolism, Caspase 6 metabolism, Huntingtin Protein genetics, Huntington Disease metabolism

Abstract

Aberrant activation of caspase-6 (C6) in the absence of other hallmarks of apoptosis has been demonstrated in cells and tissues from patients with Huntington disease (HD) and animal models. C6 activity correlates with disease progression in patients with HD and the cleavage of mutant huntingtin (mHTT) protein is thought to strongly contribute to disease pathogenesis. Here we show that the mHTT 1-586 fragment generated by C6 cleavage interacts with the zymogen form of the enzyme, stabilizing a conformation that contains an active site and is prone to full activation. This shift toward enhanced activity can be prevented by a small-molecule inhibitor that blocks the interaction between C6 and mHTT 1-586 . Molecular docking studies suggest that the inhibitor binds an allosteric site in the C6 zymogen. The interaction of mHTT 1-586 with C6 may therefore promote a self-reinforcing, feedforward cycle of C6 zymogen activation and mHTT cleavage driving HD pathogenesis., (Copyright © 2019 Elsevier Ltd. All rights reserved.)

Published

2019

23. Identification of novel agonists by high-throughput screening and molecular modelling of human constitutive androstane receptor isoform 3.

Author

Keminer O, Windshügel B, Essmann F, Lee SML, Schiergens TS, Schwab M, and Burk O

Subjects

Cell Nucleus drug effects, Cell Nucleus metabolism, Clopidogrel pharmacology, Constitutive Androstane Receptor, Cytochrome P-450 CYP2B6 genetics, Gene Expression Regulation drug effects, HEK293 Cells, Hepatocytes physiology, Humans, Models, Molecular, Molecular Docking Simulation, Molecular Dynamics Simulation, Proof of Concept Study, Protein Isoforms, Protein Transport drug effects, Receptors, Cytoplasmic and Nuclear metabolism, Retinoid X Receptors chemistry, Retinoid X Receptors metabolism, Hepatocytes drug effects, High-Throughput Screening Assays methods, Receptors, Cytoplasmic and Nuclear agonists, Receptors, Cytoplasmic and Nuclear chemistry

Abstract

Prediction of drug interactions, based on the induction of drug disposition, calls for the identification of chemicals, which activate xenosensing nuclear receptors. Constitutive androstane receptor (CAR) is one of the major human xenosensors; however, the constitutive activity of its reference variant CAR1 in immortalized cell lines complicates the identification of agonists. The exclusively ligand-dependent isoform CAR3 represents an obvious alternative for screening of CAR agonists. As CAR3 is even more abundant in human liver than CAR1, identification of its agonists is also of pharmacological value in its own right. We here established a cellular high-throughput screening assay for CAR3 to identify ligands of this isoform and to analyse its suitability for identifying CAR ligands in general. Proof-of-concept screening of 2054 drug-like compounds at 10 µM resulted in the identification of novel CAR3 agonists. The CAR3 assay proved to detect the previously described CAR1 ligands in the screened libraries. However, we failed to detect CAR3-selective compounds, as the four novel agonists, which were selected for further investigations, all proved to activate CAR1 in different cellular and in vitro assays. In primary human hepatocytes, the compounds preferentially induced the expression of the prototypical CAR target gene CYP2B6. Failure to identify CAR3-selective compounds was investigated by molecular modelling, which showed that the isoform-specific insertion of five amino acids did not impact on the ligand binding pocket but only on heterodimerization with retinoid X receptor. In conclusion, we demonstrate here the usability of CAR3 for screening compound libraries for the presence of CAR agonists.

Published

2019

24. α-Amino Diphenyl Phosphonates as Novel Inhibitors of Escherichia coli ClpP Protease.

Author

Moreno-Cinos C, Sassetti E, Salado IG, Witt G, Benramdane S, Reinhardt L, Cruz CD, Joossens J, Van der Veken P, Brötz-Oesterhelt H, Tammela P, Winterhalter M, Gribbon P, Windshügel B, and Augustyns K

Subjects

Anti-Bacterial Agents chemistry, Anti-Bacterial Agents metabolism, Anti-Bacterial Agents pharmacology, Binding Sites, Biphenyl Compounds chemistry, Endopeptidase Clp metabolism, Escherichia coli drug effects, Escherichia coli Proteins metabolism, Inhibitory Concentration 50, Molecular Docking Simulation, Organophosphonates metabolism, Organophosphonates pharmacology, Protein Structure, Tertiary, Serine Proteinase Inhibitors metabolism, Serine Proteinase Inhibitors pharmacology, Structure-Activity Relationship, Endopeptidase Clp antagonists & inhibitors, Escherichia coli enzymology, Escherichia coli Proteins antagonists & inhibitors, Organophosphonates chemistry, Serine Proteinase Inhibitors chemistry

Abstract

Increased Gram-negative bacteria resistance to antibiotics is becoming a global problem, and new classes of antibiotics with novel mechanisms of action are required. The caseinolytic protease subunit P (ClpP) is a serine protease conserved among bacteria that is considered as an interesting drug target. ClpP function is involved in protein turnover and homeostasis, stress response, and virulence among other processes. The focus of this study was to identify new inhibitors of Escherichia coli ClpP and to understand their mode of action. A focused library of serine protease inhibitors based on diaryl phosphonate warheads was tested for ClpP inhibition, and a chemical exploration around the hit compounds was conducted. Altogether, 14 new potent inhibitors of E. coli ClpP were identified. Compounds 85 and 92 emerged as most interesting compounds from this study due to their potency and, respectively, to its moderate but consistent antibacterial properties as well as the favorable cytotoxicity profile.

Published

2019

25. On the relationship of anthranilic derivatives structure and the FXR (Farnesoid X receptor) agonist activity.

Author

Kronenberger T, Windshügel B, Wrenger C, Honorio KM, and Maltarollo VG

Subjects

Humans, Isoxazoles chemistry, Models, Molecular, Molecular Docking Simulation, Quantitative Structure-Activity Relationship, Receptors, Cytoplasmic and Nuclear chemistry, ortho-Aminobenzoates chemistry

Abstract

Farnesoid X receptor (FXR) is a nuclear receptor related to lipid and glucose homeostasis and is considered an important molecular target to treatment of metabolic diseases as diabetes, dyslipidemia, and liver cancer. Nowadays, there are several FXR agonists reported in the literature and some of it in clinical trials for liver disorders. Herein, a compound series was employed to generate QSAR models to better understand the structural basis for FXR activation by anthranilic acid derivatives (AADs). Furthermore, here we evaluate the inclusion of the standard deviation (SD) of EC 50 values in QSAR models quality. Comparison between the use of experimental variance plus average values in model construction with the standard method of model generation that considers only the average values was performed. 2D and 3D QSAR models based on the AAD data set including SD values showed similar molecular interpretation maps and quality (Q 2 LOO , Q 2 (F2) , and Q 2 (F3) ), when compared to models based only on average values. SD-based models revealed more accurate predictions for the set of test compounds, with lower mean absolute error indices as well as more residuals near zero. Additionally, the visual interpretation of different QSAR approaches agrees with experimental data, highlighting key elements for understanding the biological activity of AADs. The approach using standard deviation values may offer new possibilities for generating more accurate QSAR models based on available experimental data.

Published

2018

26. Identification of approved drugs as potent inhibitors of pregnane X receptor activation with differential receptor interaction profiles.

Author

Burk O, Kuzikov M, Kronenberger T, Jeske J, Keminer O, Thasler WE, Schwab M, Wrenger C, and Windshügel B

Subjects

Cell Line, Drug Approval, Hep G2 Cells, Hepatocytes cytology, Humans, Indazoles, Molecular Docking Simulation, Protein Binding, Pyrimidines administration & dosage, Sulfonamides administration & dosage, Tacrolimus administration & dosage, Tacrolimus pharmacology, Hepatocytes metabolism, Pregnane X Receptor antagonists & inhibitors, Pyrimidines pharmacology, Sulfonamides pharmacology, Tacrolimus analogs & derivatives

Abstract

Activation of pregnane X receptor (PXR) results in the induction of first-pass metabolism and drug efflux. Hereby, PXR may cause adverse drug reactions or therapeutic failure of drugs. PXR inhibition is thus an attractive option to minimise adverse effects or to improve therapeutic efficiencies; however, only a limited number of antagonists have been identified so far. We performed a cell-based high-throughput screen to identify PXR antagonists, using a library of approved and investigational drugs. Two approved drugs, pimecrolimus and pazopanib, emerged as novel potent antagonists of PXR activation, with IC 50 values of 1.2 and 4.1 µM, respectively. We further characterised these with respect to receptor specificity, assembly of the PXR ligand-binding domain (LBD) and interactions with co-factors. In vitro and in silico assays were carried out to identify the site(s) of interaction with the PXR LBD. Primary human hepatocytes were used to investigate antagonism of the induction of endogenous PXR target genes. Pimecrolimus and pazopanib did not affect the transcriptional activity of other nuclear receptors. Both induced the release of co-repressor from PXR and likewise interfered with agonist-induced recruitment of co-activator. Cumulative evidence from cellular and in vitro assays, as well as molecular docking, suggested additional or exclusive binding outside the PXR ligand-binding pocket for both. The compounds differentially antagonised the induction of PXR-regulated genes by rifampicin in primary human hepatocytes. In conclusion, we here have identified two approved drugs as novel potent PXR inhibitors with differential receptor interaction profiles and gene selectivity in primary human hepatocytes.

Published

2018

27. Human pregnane X receptor is activated by dibenzazepine carbamate-based inhibitors of constitutive androstane receptor.

Author

Jeske J, Windshügel B, Thasler WE, Schwab M, and Burk O

Subjects

Benzazepines chemistry, Constitutive Androstane Receptor, Gene Expression drug effects, Hep G2 Cells, Hepatocytes metabolism, Humans, Ligands, Molecular Docking Simulation, Pregnane X Receptor, Primary Cell Culture, Protein Binding, Receptors, Steroid genetics, Benzazepines pharmacology, Hepatocytes drug effects, Receptors, Cytoplasmic and Nuclear antagonists & inhibitors, Receptors, Steroid metabolism

Abstract

Unintentional activation of xenosensing nuclear receptors pregnane X receptor (PXR) and/or constitutive androstane receptor (CAR) by clinical drug use is known to produce severe side effects in patients, which may be overcome by co-administering antagonists. However, especially antagonizing CAR is hampered by the lack of specific inhibitors, which do not activate PXR. Recently, compounds based on a dibenzazepine carbamate scaffold were identified as potent CAR inhibitors. However, their potential to activate PXR was not thoroughly investigated, even if the lead compound was named "CAR inhibitor not PXR activator 1" (CINPA1). Thus, we performed a comprehensive analysis of the interaction of CINPA1 and four analogs with PXR. Cellular assays were used to investigate intra- and intermolecular interactions and transactivation activity of PXR as a function of the compounds. Modulation of PXR target gene expression was analyzed in primary human hepatocytes. Ligand binding to PXR was investigated by molecular docking and limited proteolytic digestion. We show here that CINPA1 induced the assembly of the PXR ligand-binding domain, released co-repressors from and recruited co-activators to the receptor. CINPA1 and its analogs induced the PXR-dependent activation of a CYP3A4 reporter gene and CINPA1 induced the expression of endogenous cytochrome P450 genes in primary hepatocytes, while not consistently inhibiting CAR-mediated induction. Molecular docking revealed favorable binding of CINPA1 and analogs to the PXR ligand-binding pocket, which was confirmed in vitro. Altogether, our data provide consistent evidence that compounds with a dibenzazepine carbamate scaffold, such as CINPA1 and its four analogs, bind to and activate PXR.

Published

2017

28. Structure of ThiM from Vitamin B1 biosynthetic pathway of Staphylococcus aureus - Insights into a novel pro-drug approach addressing MRSA infections.

Author

Drebes J, Künz M, Windshügel B, Kikhney AG, Müller IB, Eberle RJ, Oberthür D, Cang H, Svergun DI, Perbandt M, Betzel C, and Wrenger C

Subjects

Biosynthetic Pathways, Catalytic Domain, Databases, Chemical, Methicillin Resistance, Models, Molecular, Anti-Bacterial Agents chemistry, Phosphotransferases (Alcohol Group Acceptor) chemistry, Prodrugs chemistry, Staphylococcus aureus enzymology, Thiamine biosynthesis, Thiazoles chemistry

Abstract

Infections caused by the methicillin-resistant Staphylococcus aureus (MRSA) are today known to be a substantial threat for global health. Emerging multi-drug resistant bacteria have created a substantial need to identify and discover new drug targets and to develop novel strategies to treat bacterial infections. A promising and so far untapped antibiotic target is the biosynthesis of vitamin B1 (thiamin). Thiamin in its activated form, thiamin pyrophosphate, is an essential co-factor for all organisms. Therefore, thiamin analogous compounds, when introduced into the vitamin B1 biosynthetic pathway and further converted into non-functional co-factors by the bacterium can function as pro-drugs which thus block various co-factor dependent pathways. We characterized one of the key enzymes within the S. aureus vitamin B1 biosynthetic pathway, 5-(hydroxyethyl)-4-methylthiazole kinase (SaThiM; EC 2.7.1.50), a potential target for pro-drug compounds and analyzed the native structure of SaThiM and complexes with the natural substrate 5-(hydroxyethyl)-4-methylthiazole (THZ) and two selected substrate analogues.

Published

2016

29. Correction: Structural and Functional Similarity of Amphibian Constitutive Androstane Receptor with Mammalian Pregnane X Receptor.

Author

Mathäs M, Nusshag C, Burk O, Gödtel-Armbrust U, Herlyn H, Wojnowski L, and Windshügel B

Published

2016

30. Linker-Region Modified Derivatives of the Deoxyhypusine Synthase Inhibitor CNI-1493 Suppress HIV-1 Replication.

Author

Schröder M, Kolodzik A, Windshügel B, Krepstakies M, Priyadarshini P, Hartjen P, van Lunzen J, Rarey M, Hauber J, and Meier C

Subjects

Anti-HIV Agents chemical synthesis, Anti-HIV Agents pharmacology, Cell Line, Drug Stability, HIV-1 physiology, Humans, Hydrazones chemical synthesis, Hydrazones pharmacology, Hydrolysis, Mixed Function Oxygenases chemistry, Molecular Docking Simulation, Molecular Dynamics Simulation, Structure-Activity Relationship, Virus Replication, Anti-HIV Agents chemistry, HIV-1 drug effects, Hydrazones chemistry, Mixed Function Oxygenases antagonists & inhibitors

Abstract

The inhibition of cellular factors that are involved in viral replication may be an important alternative to the commonly used strategy of targeting viral enzymes. The guanylhydrazone CNI-1493, a potent inhibitor of the deoxyhypusine synthase (DHS), prevents the activation of the cellular factor eIF-5A and thereby suppresses HIV replication and a number of other diseases. Here, we report on the design, synthesis and biological evaluation of a series of CNI-1493 analogues. The sebacoyl linker in CNI-1493 was replaced by different alkyl or aryl dicarboxylic acids. Most of the tested derivatives suppress HIV-1 replication efficiently in a dose-dependent manner without showing toxic side effects. The unexpected antiviral activity of the rigid derivatives point to a second binding mode as previously assumed for CNI-1493. Moreover, the chemical stability of CNI-1493 was analysed, showing a successive hydrolysis of the imino bonds. By molecular dynamics simulations, the behaviour of the parent CNI-1493 in solution and its interactions with DHS were investigated., (© 2015 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2016

31. LEADS-PEP: A Benchmark Data Set for Assessment of Peptide Docking Performance.

Author

Hauser AS and Windshügel B

Subjects

Amino Acid Sequence, Benchmarking, Oligopeptides chemistry, Protein Binding, Protein Conformation, Proteins chemistry, Proteins metabolism, Molecular Docking Simulation methods, Oligopeptides metabolism

Abstract

With increasing interest in peptide-based therapeutics also the application of computational approaches such as peptide docking has gained more and more attention. In order to assess the suitability of docking programs for peptide placement and to support the development of peptide-specific docking tools, an independently constructed benchmark data set is urgently needed. Here we present the LEADS-PEP benchmark data set for assessing peptide docking performance. Using a rational and unbiased workflow, 53 protein-peptide complexes with peptide lengths ranging from 3 to 12 residues were selected. The data set is publicly accessible at www.leads-x.org . In a second step we evaluated several small molecule docking programs for their potential to reproduce peptide conformations as present in LEADS-PEP. While most tested programs were capable to generate native-like binding modes of small peptides, only Surflex-Dock and AutoDock Vina performed reasonably well for peptides consisting of more than five residues. Rescoring of docking poses with scoring functions ChemPLP, ChemScore, and ASP further increased the number of top-ranked near-native conformations. Our results suggest that small molecule docking programs are a good and fast alternative to specialized peptide docking programs.

Published

2016

32. Structural and functional similarity of amphibian constitutive androstane receptor with mammalian pregnane X receptor.

Author

Mathäs M, Nusshag C, Burk O, Gödtel-Armbrust U, Herlyn H, Wojnowski L, and Windshügel B

Subjects

Amphibian Proteins physiology, Animals, Binding Sites, COS Cells, Cell Line, Chlorocebus aethiops, Constitutive Androstane Receptor, Crystallography, X-Ray, Humans, Models, Molecular, Molecular Dynamics Simulation, Pregnane X Receptor, Receptors, Cytoplasmic and Nuclear physiology, Receptors, Steroid physiology, Xenopus laevis, Amphibian Proteins chemistry, Receptors, Cytoplasmic and Nuclear chemistry, Receptors, Steroid chemistry

Abstract

The nuclear receptors and xenosensors constitutive androstane receptor (CAR, NR1I3) and pregnane X receptor (PXR, NR1I2) induce the expression of xenobiotic metabolizing enzymes and transporters, which also affects various endobiotics. While human and mouse CAR feature a high basal activity and low induction upon ligand exposure, we recently identified two constitutive androstane receptors in Xenopus laevis (xlCARá and â) that possess PXR-like characteristics such as low basal activity and activation in response to structurally diverse compounds. Using a set of complementary computational and biochemical approaches we provide evidence for xlCARá being the structural and functional counterpart of mammalian PXR. A three-dimensional model of the xlCARá ligand-binding domain (LBD) reveals a human PXR-like L-shaped ligand binding pocket with a larger volume than the binding pockets in human and murine CAR. The shape and amino acid composition of the ligand-binding pocket of xlCAR suggests PXR-like binding of chemically diverse ligands which was confirmed by biochemical methods. Similarly to PXR, xlCARá possesses a flexible helix 11'. Modest increase in the recruitment of coactivator PGC-1á may contribute to the enhanced basal activity of three gain-of-function xlCARá mutants humanizing key LBD amino acid residues. xlCARá and PXR appear to constitute an example of convergent evolution.

Published

2014

33. Evolutionary history and functional characterization of the amphibian xenosensor CAR.

Author

Mathäs M, Burk O, Qiu H, Nusshag C, Gödtel-Armbrust U, Baranyai D, Deng S, Römer K, Nem D, Windshügel B, and Wojnowski L

Subjects

Amino Acid Sequence, Animals, Biological Evolution, Cell Line, Constitutive Androstane Receptor, Gene Expression Regulation, Humans, Molecular Sequence Data, Oligonucleotide Array Sequence Analysis, Phylogeny, Pregnane X Receptor, RNA, Messenger genetics, Receptors, Calcitriol metabolism, Receptors, Cytoplasmic and Nuclear metabolism, Receptors, Steroid metabolism, Sequence Alignment, Xenopus genetics, Xenopus metabolism, Evolution, Molecular, Receptors, Calcitriol genetics, Receptors, Cytoplasmic and Nuclear genetics, Receptors, Steroid genetics

Abstract

The xenosensing constitutive androstane receptor (CAR) is widely considered to have arisen in early mammals via duplication of the pregnane X receptor (PXR). We report that CAR emerged together with PXR and the vitamin D receptor from an ancestral NR1I gene already in early vertebrates, as a result of whole-genome duplications. CAR genes were subsequently lost from the fish lineage, but they are conserved in all taxa of land vertebrates. This contrasts with PXR, which is found in most fish species, whereas it is lost from Sauropsida (reptiles and birds) and plays a role unrelated to xenosensing in Xenopus. This role is fulfilled in Xenopus by CAR, which exhibits low basal activity and pronounced responsiveness to activators such as drugs and steroids, altogether resembling mammalian PXR. The constitutive activity typical for mammalian CAR emerged first in Sauropsida, and it is thus common to all fully terrestrial land vertebrates (Amniota). The constitutive activity can be achieved by humanizing just two amino acids of the Xenopus CAR. Taken together, our results provide a comprehensive reconstruction of the evolutionary history of the NR1I subfamily of nuclear receptors. They identify CAR as the more conserved and remarkably plastic NR1I xenosensor in land vertebrates. Nonmammalian CAR should help to dissect the specific functions of PXR and CAR in the metabolism of xeno- and endobiotics in humans. Xenopus CAR is a first reported amphibian xenosensor, which opens the way to toxicogenomic and bioaugmentation studies in this critically endangered taxon of land vertebrates.

Published

2012

34. The discovery of compounds that stimulate the activity of kallikrein-related peptidase 3 (KLK3).

Author

Härkönen HH, Mattsson JM, Määttä JA, Stenman UH, Koistinen H, Matero S, Windshügel B, Poso A, and Lahtela-Kakkonen M

Subjects

Binding Sites, Calorimetry, Differential Scanning, Drug Evaluation, Preclinical, Enzyme Activation drug effects, Humans, Kallikreins metabolism, Molecular Dynamics Simulation, Prostate-Specific Antigen, Protease Inhibitors pharmacology, Protein Structure, Tertiary, Small Molecule Libraries pharmacology, Kallikreins chemistry, Protease Inhibitors chemistry, Small Molecule Libraries chemistry

Abstract

Kallikrein-related peptidase 3 (KLK3), also known as prostate-specific antigen (PSA), is the most useful biomarker for prostate cancer (PCa). KLK3 is suggested to play a role in regulating cancer growth through anti-angiogenic activity in vivo and in vitro. This feature, together with its specificity for prostate tissue, makes KLK3 an intriguing target for the design of new therapies for PCa. 3D pharmacophores for KLK3-stimulating compounds were generated based on peptides that bind specifically to KLK3 and increase its enzymatic activity. As a result of pharmacophore-based virtual screening, four small, drug-like compounds with affinity for KLK3 were discovered and validated by capillary differential scanning calorimetry. One of the compounds also stimulated the activity of KLK3, and is therefore the first published small molecule with such an activity., (Copyright © 2011 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2011

35. New in vitro tools to study human constitutive androstane receptor (CAR) biology: discovery and comparison of human CAR inverse agonists.

Author

Küblbeck J, Jyrkkärinne J, Molnár F, Kuningas T, Patel J, Windshügel B, Nevalainen T, Laitinen T, Sippl W, Poso A, and Honkakoski P

Subjects

Animals, Antineoplastic Agents chemistry, Cell Line, Tumor, Constitutive Androstane Receptor, Humans, Isoquinolines chemistry, Models, Molecular, Molecular Dynamics Simulation, Drug Discovery, Methylurea Compounds chemistry, Receptors, Cytoplasmic and Nuclear agonists, Thiophenes chemistry

Abstract

The human constitutive androstane receptor (CAR, NR1I3) is one of the key regulators of xenobiotic and endobiotic metabolism. The unique properties of human CAR, such as the high constitutive activity and the complexity of signaling, as well as the lack of functional and predictive cell-based assays to study the properties of the receptor, have hindered the discovery of selective human CAR ligands. Here we report a novel human CAR inverse agonist, 1-[(2-methylbenzofuran-3-yl)methyl]-3-(thiophen-2-ylmethyl) urea (S07662), which suppresses human CAR activity, recruits the corepressor NCoR in cell-based assays, and attenuates the phenytoin- and 6-(4-chlorophenyl)imidazo[2,1-b][1,3]thiazole-5-carbaldehyde O-(3,4-dichlorobenzyl)oxime (CITCO)-induced expression of CYP2B6 mRNA in human primary hepatocytes. The properties of S07662 are also compared with those of known human CAR inverse agonists by using an array of different in vitro and in silico assays. The identified compound S07662 can be used as a chemical tool to study the biological functions of human CAR and also as a starting point for the development of new drugs for various conditions involving the receptor.

Published

2011

36. Constitutive activity and ligand-dependent activation of the nuclear receptor CAR-insights from molecular dynamics simulations.

Author

Windshügel B and Poso A

Subjects

Constitutive Androstane Receptor, Crystallography, X-Ray, Humans, Protein Binding, Molecular Dynamics Simulation, Receptors, Cytoplasmic and Nuclear chemistry, Receptors, Cytoplasmic and Nuclear metabolism

Abstract

The constitutive androstane receptor (CAR) possesses, unlike most other nuclear receptors, a pronounced basal activity in vitro whose structural basis is still not fully understood. Using comparative molecular dynamics simulations of CAR X-ray crystal structures, we evaluated the molecular basis for constitutive activity and ligand-dependent receptor activation. Our results suggest that a combination of van der Waals interactions and hydrogen bonds is required to maintain the activation helix in the active conformation also in absence of a ligand. Furthermore, we identified conformational rearrangements within the ligand-binding pocket upon agonist binding and an influence of CAR inducers pregnanedione and CITCO on the helical conformation of the activation helix. Based on the results a model for ligand-dependent CAR activation is suggested., (Copyright © 2011 John Wiley & Sons, Ltd.)

Published

2011

37. Insights into ligand-elicited activation of human constitutive androstane receptor based on novel agonists and three-dimensional quantitative structure-activity relationship.

Author

Jyrkkärinne J, Windshügel B, Rönkkö T, Tervo AJ, Küblbeck J, Lahtela-Kakkonen M, Sippl W, Poso A, and Honkakoski P

Subjects

Constitutive Androstane Receptor, Databases, Factual, Humans, Ligands, Models, Molecular, Molecular Structure, Receptors, Cytoplasmic and Nuclear chemistry, Transcription Factors chemistry, Pharmaceutical Preparations chemistry, Pharmaceutical Preparations metabolism, Quantitative Structure-Activity Relationship, Receptors, Cytoplasmic and Nuclear agonists, Receptors, Cytoplasmic and Nuclear metabolism, Transcription Factors agonists, Transcription Factors metabolism

Abstract

The human constitutive androstane receptor (CAR, NR1I3) is an important regulator of xenobiotic metabolism and other physiological processes. So far, only few CAR agonists are known and no explicit mechanism has been proposed for their action. Thus, we aimed to generate a 3D QSAR model that could explain the molecular determinants of CAR agonist action. To obtain a sufficient number of agonists that cover a wide range of activity, we applied a virtual screening approach using both structure- and ligand-based methods. We identified 27 novel human CAR agonists on which a 3D QSAR model was generated. The model, complemented by coregulator recruitment and mutagenesis results, suggests a potential activation mechanism for human CAR and may serve to predict potential activation of CAR for compounds emerging from drug development projects or for chemicals undergoing toxicological risk assessment.

Published

2008

38. Discovery of substituted sulfonamides and thiazolidin-4-one derivatives as agonists of human constitutive androstane receptor.

Author

Küblbeck J, Jyrkkärinne J, Poso A, Turpeinen M, Sippl W, Honkakoski P, and Windshügel B

Subjects

Cells, Cultured, Constitutive Androstane Receptor, Hepatocytes drug effects, Hepatocytes metabolism, Humans, Male, Middle Aged, Protein Binding drug effects, Protein Binding physiology, Receptors, Cytoplasmic and Nuclear chemistry, Sulfonamides pharmacology, Thiazolidines pharmacology, Transcription Factors chemistry, Receptors, Cytoplasmic and Nuclear agonists, Receptors, Cytoplasmic and Nuclear metabolism, Sulfonamides chemistry, Sulfonamides metabolism, Thiazolidines chemistry, Thiazolidines metabolism, Transcription Factors agonists, Transcription Factors metabolism

Abstract

The constitutive androstane receptor (CAR; NR1I3) is a nuclear receptor responsible for the recognition of potentially toxic endo- and exogenous compounds whose elimination from the body is accelerated by the CAR-mediated inducible expression of metabolizing enzymes and transporters. Despite the importance of CAR, few human agonists are known so far. Following a sequential virtual screening procedure using a 3D pharmacophore and molecular docking approach, we identified 17 novel agonists that could activate human CAR in vitro and enhance its association with the nuclear receptor co-activator SRC1. Selected agonists also increased the expression of the human CAR target CYP2B6 mRNA in primary hepatocytes. Composed of substituted sulfonamides and thiazolidin-4-one derivatives, these agonists represent two novel chemotypes capable of human CAR activation, thus broadening the agonist spectrum of CAR.

Published

2008

39. Comparison of homology models and X-ray structures of the nuclear receptor CAR: assessing the structural basis of constitutive activity.

Author

Windshügel B, Jyrkkärinne J, Vanamo J, Poso A, Honkakoski P, and Sippl W

Subjects

Amino Acid Sequence, Animals, Binding Sites, Computer Graphics, Computer Simulation, Coxsackie and Adenovirus Receptor-Like Membrane Protein, Crystallography, X-Ray, Humans, Mice, Molecular Sequence Data, Protein Structure, Secondary, Protein Structure, Tertiary, Receptors, Virus genetics, Receptors, Virus metabolism, Sequence Homology, Amino Acid, Thermodynamics, Models, Molecular, Receptors, Virus chemistry

Abstract

The constitutive androstane receptor (CAR) possesses an intrinsic basal activity whose structural basis has been analysed during the last decade. Recently, we published a homology model of the CAR ligand binding domain (LBD) based on the X-ray structures of the closely related pregnane X (PXR) and vitamin D (VDR) receptor. A detailed analysis of the homology model and molecular dynamics (MD) simulations afforded us to propose a potential mechanism underlying the constitutive activity of CAR. Almost simultaneously, X-ray structures of human and mouse CAR LBD were released. In the present study, a detailed analysis and comparison of homology model and X-ray structures is carried out in order to evaluate the quality and reliability of our homology modelling procedure. The hypothesis of the constitutive activity which we proposed on the basis of our modelling results was tested for consistency with the crystal structures. In addition, the features stated to be essential for the basal activity based on the X-ray data were investigated by means of molecular dynamics simulations. Our results show that the homology modelling procedure was able to predict the CAR LBD structure with high accuracy. Structural features that have been revealed as critical for constitutive activity in the model are also observed in the X-ray structures. Furthermore, the MD simulations of the CAR X-ray structures and a detailed analysis of other NRs clarify the role of distinct structural features that have been assigned an important role for the constitutive activity.

Published

2007

40. Structural mechanism of the recovery stroke in the myosin molecular motor.

Author

Fischer S, Windshügel B, Horak D, Holmes KC, and Smith JC

Subjects

Actins chemistry, Adenosine Triphosphatases chemistry, Adenosine Triphosphate chemistry, Animals, Binding Sites, Biophysics methods, Catalytic Domain, Crystallography, X-Ray, Dictyostelium, Hydrolysis, Kinetics, Ligands, Models, Molecular, Muscle Contraction, Mutation, Phenotype, Protein Binding, Protein Conformation, Protein Structure, Tertiary, Molecular Motor Proteins chemistry, Myosins chemistry

Abstract

The power stroke pulling myosin along actin filaments during muscle contraction is achieved by a large rotation ( approximately 60 degrees ) of the myosin lever arm after ATP hydrolysis. Upon binding the next ATP, myosin dissociates from actin, but its ATPase site is still partially open and catalytically off. Myosin must then close and activate its ATPase site while returning the lever arm for the next power stroke. A mechanism for this coupling between the ATPase site and the distant lever arm is determined here by generating a continuous series of optimized intermediates between the crystallographic end-states of the recovery stroke. This yields a detailed structural model for communication between the catalytic and the force-generating regions that is consistent with experimental observations. The coupling is achieved by an amplifying cascade of conformational changes along the relay helix lying between the ATPase and the domain carrying the lever arm.

Published

2005

41. Amino acids important for ligand specificity of the human constitutive androstane receptor.

Author

Jyrkkärinne J, Windshügel B, Mäkinen J, Ylisirniö M, Peräkylä M, Poso A, Sippl W, and Honkakoski P

Subjects

Amino Acid Sequence, Amino Acids genetics, Animals, Cell Line, Constitutive Androstane Receptor, Humans, Ligands, Mice, Models, Molecular, Molecular Sequence Data, Mutation genetics, Protein Binding, Protein Structure, Tertiary, Receptors, Cytoplasmic and Nuclear genetics, Sequence Alignment, Species Specificity, Substrate Specificity, Transcription Factors genetics, Amino Acids metabolism, Androstanes metabolism, Receptors, Cytoplasmic and Nuclear chemistry, Receptors, Cytoplasmic and Nuclear metabolism, Transcription Factors chemistry, Transcription Factors metabolism

Abstract

The human constitutive androstane receptor (CAR, NR1I3) is an important ligand-activated regulator of oxidative and conjugative enzymes and transport proteins. Because of the lack of a crystal structure of the ligand-binding domain (LBD), wide species differences in ligand specificity and the scarcity of well characterized ligands, the factors that determine CAR ligand specificity are not clear. To address this issue, we developed highly defined homology models of human CAR LBD to identify residues lining the ligand-binding pocket and to perform molecular dynamics simulations with known human CAR modulators. The roles of 22 LBD residues for basal activity, ligand selectivity, and interactions with co-regulators were studied using site-directed mutagenesis, mammalian co-transfection, and yeast two-hybrid assays. These studies identified several amino acids within helices 3 (Asn(165)), 5 (Val(199)), 11 (Tyr(326), Ile(330), and Gln(331)), and 12 (Leu(343) and Ile(346)) that contribute to the high basal activity of human CAR. Unique residues within helices 3 (Ile(164) and Asn(165)), 5 (Cys(202) and His(203)), and 7 (Phe(234) and Phe(238)) were found control the selectivity for CAR activators and inhibitors. A single residue in helix 7 (Phe(243)) appears to explain the human/mouse species difference in response of CAR to 17alpha-ethynyl-3,17beta-estradiol.

Published

2005

42. Molecular dynamics simulations of the human CAR ligand-binding domain: deciphering the molecular basis for constitutive activity.

Author

Windshügel B, Jyrkkärinne J, Poso A, Honkakoski P, and Sippl W

Subjects

Amino Acid Sequence, Binding Sites, Clotrimazole chemistry, Computational Biology, Constitutive Androstane Receptor, Gene Expression Regulation, Humans, Ligands, Molecular Sequence Data, Mutation, Pregnane X Receptor, Protein Structure, Tertiary, Receptors, Calcitriol chemistry, Receptors, Cytoplasmic and Nuclear genetics, Receptors, Steroid chemistry, Sequence Alignment, Structural Homology, Protein, Transcription Factors genetics, Models, Molecular, Receptors, Cytoplasmic and Nuclear chemistry, Transcription Factors chemistry

Abstract

The constitutive androstane receptor (CAR) belongs to the superfamily of nuclear-hormone receptors that function as ligand-activated transcription factors. CAR plays an essential role in the metabolism of xenobiotics and shows--in contrast to related receptors--constitutive activity. However, the molecular basis for the constitutive activity remains unclear. In the present study, homology models of the ligand binding domain (LBD) were generated based on the crystal structures of the related pregnane X (PXR) and the vitamin D receptor (VDR). The models were used to investigate the basal activity of CAR and the effect of coactivator binding. Molecular dynamics (MD) simulations of complexed and uncomplexed receptor revealed a hypothesis for the activation mechanism. The suggested mechanism is supported by experimental results from site-directed mutagenesis. The basal activity of CAR can be explained by specific van-der-Waals interactions between amino acids on the LBD and its C-terminal activation domain (AF-2). Docking studies with the GOLD program yielded the interaction modes of structurally diverse agonists, giving insight into mechanisms by which ligands enhance CAR activity.

Published

2005