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27 results on '"Thomas J. Stout"'

1. Liver X Receptor (LXR) partial agonists: Biaryl pyrazoles and imidazoles displaying a preference for LXRβ

Author

Thomas J. Stout, Brett B. Busch, Todd G. Kirchgessner, Michael Charles Nyman, Tie-Lin Wang, Ruth R. Wexler, Lam Nguyen, Ellen K. Kick, Brandee L. Wagner, Grace Yan, Yinong Xie, Edwin J. Schweiger, Artur Plonowski, Ira G. Schulman, Brenton T. Flatt, Jacek Ostrowski, Max H. Nanao, Richard Martin, Raju Mohan, and Xiao-Hui Gu

Subjects
Models, Molecular, medicine.medical_specialty, Clinical Biochemistry, Pharmaceutical Science, Pyrazole, Biochemistry, Partial agonist, Mice, Plasma, Structure-Activity Relationship, chemistry.chemical_compound, Internal medicine, Drug Discovery, medicine, Animals, Humans, Tissue Distribution, Sulfones, Liver X receptor, Molecular Biology, Triglycerides, Liver X Receptors, Whole blood, Molecular Structure, biology, Chemistry, Organic Chemistry, Imidazoles, Transporter, Orphan Nuclear Receptors, Drug Partial Agonism, Endocrinology, Liver, ABCG1, Nuclear receptor, ABCA1, biology.protein, Pyrazoles, Molecular Medicine, lipids (amino acids, peptides, and proteins), ATP Binding Cassette Transporter 1
Abstract

A series of biaryl pyrazole and imidazole Liver X Receptor (LXR) partial agonists has been synthesized displaying LXRβ selectivity. The LXRβ selective partial agonist 18 was identified with potent induction of ATP binding transporters ABCA1 and ABCG1 in human whole blood (EC50 = 1.2 μM, 55% efficacy). In mice 18 displayed peripheral induction of ABCA1 at 3 and 10 mpk doses with no significant elevation of plasma or hepatic triglycerides at these doses, showing an improved profile compared to a full pan-agonist.

Published
2015

2. The design, synthesis, and biological evaluation of potent receptor tyrosine kinase inhibitors

Author

Erick Wang Co, John M. Nuss, Stefan Engst, Monica Rodriquez, Jason Chen, Xiang Wu, Moon Hwan Kim, Peiwen Yu, Fawn Qian, Yeping Zhao, Morrison B. Mac, Peter Lamb, Wei Cheng, Wei Xu, Kwang-Ai Won, Frauke Bentzien, Wentao Zhang, Thomas J. Stout, Dana T. Aftab, Jason Jevious Parks, Jeffrey H. Till, Amy Lew Tsuhako, Rhett Ronald Klein, Levina Goon, Donna T. Le, and F. Michael Yakes

Subjects
Indoles, Transplantation, Heterologous, Clinical Biochemistry, Pharmaceutical Science, Pharmacology, Crystallography, X-Ray, Biochemistry, Receptor tyrosine kinase, Mice, Structure-Activity Relationship, chemistry.chemical_compound, Piperidines, Cell Line, Tumor, Neoplasms, Drug Discovery, Animals, Cytochrome P-450 CYP3A, Humans, Transferase, Structure–activity relationship, Oxindole, Lung, Protein Kinase Inhibitors, Molecular Biology, ADME, Binding Sites, biology, Organic Chemistry, Receptor Protein-Tyrosine Kinases, Protein Structure, Tertiary, Rats, Transplantation, chemistry, Drug Design, biology.protein, Molecular Medicine, Female, Piperidine, Platelet-derived growth factor receptor, Half-Life
Abstract

Variously substituted indolin-2-ones were synthesized and evaluated for activity against KDR, Flt-1, FGFR-1 and PDGFR. Extension at the 5-position of the oxindole ring with ethyl piperidine (compound 7i) proved to be the most beneficial for attaining both biochemical and cellular potencies. Further optimization of 7i to balance biochemical and cellular potencies with favorable ADME/ PK properties led to the identification of 8h, a compound with a clean CYP profile, acceptable pharmacokinetic and toxicity profiles, and robust efficacy in multiple xenograft tumor models.

Published
2012

3. The design, synthesis, and biological evaluation of PIM kinase inhibitors

Author

John M. Nuss, Gordon Mark Stott, Hongwang Du, E.S. Koltun, A.D Laird, I Ngan, Amy Lew Tsuhako, Adam A. Galan, Ping Huang, Thomas J. Stout, Patrick Kearney, Chan, Stuart Johnston, W. Zhang, R Lin, Stefan Engst, Peiwen Zhou, L Mock, Maurizio Franzini, Brown S David, Moon Hwan Kim, Brian Kane, Naing Aay, Arlyn Arcalas, Wei Xu, Michael Pack, Peiwen Yu, and Cristiana A. Zaharia

Subjects
Clinical Biochemistry, Pharmaceutical Science, Pyrimidinones, Crystallography, X-Ray, Biochemistry, Structure-Activity Relationship, chemistry.chemical_compound, Proto-Oncogene Proteins c-pim-1, hemic and lymphatic diseases, Drug Discovery, Transferase, Computer Simulation, Furans, Protein Kinase Inhibitors, Molecular Biology, Cell permeability, Alkyl, Biological evaluation, chemistry.chemical_classification, Binding Sites, Kinase, Aryl, Organic Chemistry, Combinatorial chemistry, Protein Structure, Tertiary, chemistry, Design synthesis, Drug Design, Molecular Medicine, Selectivity
Abstract

A series of substituted benzofuropyrimidinones with pan-PIM activities and excellent selectivity against a panel of diverse kinases is described. Initial exploration identified aryl benzofuropyrimidinones that were potent, but had cell permeability limitation. Using X-ray crystal structures of the bound PIM-1 complexes with 3, 5m, and 6d, we were able to guide the SAR and identify the alkyl benzofuropyrimidinone (6l) with good PIM potencies, permeability, and oral exposure.

Published
2012

4. Discovery of XL413, a potent and selective CDC7 inhibitor

Author

Arlyn Arcalas, Richards Steven J, Amy Lew Tsuhako, Naing Aay, Kim Ferguson, Arthur Plonowski, Gordon Mark Stott, Wei Xu, Jenny Young, Peiwen Yu, Wentao Zhang, Charles R. Holst, Kevin Noson, Cristiana A. Zaharia, Brown S David, Hongwang Du, Manisha Mohan, Ping Huang, Thomas J. Stout, Adam A. Galan, Patrick Kearney, David W. Markby, Stefan Engst, Maurizio Franzini, Peiwen Zhou, John M. Nuss, Brian Kane, Kenneth J. Shaw, Elena S. Koltun, Scott Robertson, Moon Hwan Kim, Vicky Chan, and Jia Li

Subjects
Cell cycle checkpoint, Transplantation, Heterologous, Clinical Biochemistry, Pharmaceutical Science, Cell Cycle Proteins, Pyrimidinones, Protein Serine-Threonine Kinases, Biochemistry, Serine, Mice, Structure-Activity Relationship, In vivo, Cell Line, Tumor, Neoplasms, Drug Discovery, Animals, Humans, Computer Simulation, Threonine, Protein Kinase Inhibitors, Molecular Biology, Binding Sites, Kinase, Chemistry, Organic Chemistry, DNA replication, Cell Cycle Checkpoints, In vitro, Protein Structure, Tertiary, Rats, Up-Regulation, Cell biology, Cell culture, Molecular Medicine
Abstract

CDC7 is a serine/threonine kinase that has been shown to be required for the initiation and maintenance of DNA replication. Up-regulation of CDC7 is detected in multiple tumor cell lines, with inhibition of CDC7 resulting in cell cycle arrest. In this paper, we disclose the discovery of a potent and selective CDC7 inhibitor, XL413 (14), which was advanced into Phase 1 clinical trials. Starting from advanced lead 3, described in a preceding communication, we optimized the CDC7 potency and selectivity to demonstrate in vitro CDC7 dependent cell cycle arrest and in vivo tumor growth inhibition in a Colo-205 xenograft model.

Published
2012

5. Crystal Structures of a Unique Thermal-Stable Thymidylate Synthase from Bacillus subtilis

Author

Daniel V. Santi, Robert M. Stroud, Thomas J. Stout, and Ute Schellenberger

Subjects
Models, Molecular, Lactobacillus casei, Hot Temperature, Stereochemistry, Dimer, Molecular Sequence Data, Sequence alignment, Crystal structure, Bacillus subtilis, Crystallography, X-Ray, medicine.disease_cause, Biochemistry, chemistry.chemical_compound, Enzyme Stability, Escherichia coli, medicine, Amino Acid Sequence, Sequence Homology, Amino Acid, biology, Mutagenesis, Lactococcus lactis, Thymidylate Synthase, biology.organism_classification, Recombinant Proteins, Isoenzymes, Solutions, chemistry, Crystallization
Abstract

Unlike all other organisms studied to date, Bacillus subtilis expresses two different thymidylate synthases: bsTS-A and bsTS-B. bsTS-A displays enhanced enzymatic and structural thermal stability uncharacteristic of most TSs. Despite the high level of TS conservation across most species, bsTS-A shares low sequence identity (

Published
1998

6. The complex of the anti-cancer therapeutic, BW1843U89, with thymidylate synthase at 2.0 å resolution: implications for a new mode of inhibition

Author

Robert M. Stroud and Thomas J. Stout

Subjects
Models, Molecular, Indoles, Protein Conformation, Stereochemistry, Antineoplastic Agents, Isoindoles, Crystallography, X-Ray, Binding, Competitive, Thymidylate synthase, Structural Biology, Escherichia coli, medicine, Enzyme Inhibitors, Binding site, Molecular Biology, Ternary complex, chemistry.chemical_classification, Binding Sites, Molecular Structure, biology, Cooperative binding, Active site, Thymidylate Synthase, Ligand (biochemistry), Enzyme, chemistry, Mechanism of action, Biochemistry, Drug Design, Quinazolines, biology.protein, Folic Acid Antagonists, medicine.symptom, Deoxyuracil Nucleotides, Protein Binding
Abstract

Background: Thymidylate synthase (TS) is critical to DNA synthesis as it catalyzes the rate limiting step in the only biosynthetic pathway for deoxythymidine monophosphate (dTMP) production. TS is therefore an important target for anti-proliferative and anti-cancer drug design. The TS enzymatic mechanism involves the reductive methylation of the substrate, deoxyuridine monophosphate (dUMP), by transfer of a methylene group from the co-factor, methylenetetrahydrofolate (CH 2 H 4 folate), resulting in the production of deoxythymidine monophosphate (dTMP) and dihydrofolate (H 2 folate). Previous drug design efforts based on co-factor analogues have produced good inhibitors of TS, but poor bioavailability and toxicity have limited their usefulness. BW1843U89, a folate analogue, is a recently developed compound which is an exceptionally strong inhibitor (K i =0.09 nM), has good bioavailability and in clinical trials thus far has not demonstrated significant toxicity. Results We report the crystal structure of E. coli TS in ternary complex with dUMP and BW1843U89 at 2.0 a resolution. Although the benzoquinazoline ring system of the inhibitor binds to TS in much the same manner as previously determined for H 2 folate and CB3717, the larger size of the ligand is accommodated by the enzyme through a local distortion of the active site, that is not strictly conserved in both monomers in the asymmetric unit. Several conserved waters that had been previously implicated in mechanistic roles have been displaced. Conclusion BW1843U89 forms a ternary complex with dUMP and competes with CH 2 H 4 folate at the active site. Inhibition of TS by BW1843U89 shows four unique aspects in its mechanism of action. BW1843U89 prevents the Michael addition of dUMP to Cys146, in contrast to the mechanisms implicated from crystallography of other quinazoline based inhibitors; displaces a catalytic water from the active site; reorders a peptide loop (Leu72–Trp83) in the active site; and is unique amongst the antifolates in inactivating TS at a stoichiometric ratio of one molecule per TS dimer. Thus, it exploits the principles of negative cooperativity that are increasingly being recognized in the catalytic mechanism of the enzyme per se . The structure suggests that this ‘half-the-sites' effect is catalytic and not related to ligand binding. Therefore BW1843U89 is both a competitive inhibitor (at the binding site) and a non-competitive inhibitor at the other site.

Published
1996

7. An Essential Role for Water in an Enzyme Reaction Mechanism: The Crystal Structure of the Thymidylate Synthase Mutant E58Q

Author

C.R. Sage, Thomas J. Stout, Robert M. Stroud, and Earl E. Rutenber

Subjects
Models, Molecular, Protein Conformation, Stereochemistry, Dimer, Mutant, Glutamic Acid, Crystallography, X-Ray, Biochemistry, Thymidylate synthase, chemistry.chemical_compound, Folic Acid, Protein structure, Escherichia coli, Point Mutation, Transferase, Amino Acid Sequence, Enzyme Inhibitors, Binding site, Binding Sites, biology, Hydrogen bond, Water, Active site, Hydrogen Bonding, Thymidylate Synthase, Recombinant Proteins, chemistry, Mutagenesis, Site-Directed, Quinazolines, biology.protein, Crystallization, Deoxyuracil Nucleotides
Abstract

A water-mediated hydrogen bond network coordinated by glutamate 60(58) appears to play an important role in the thymidylate synthase (TS) reaction mechanism. We have addressed the role of glutamate 60(58) in the TS reaction by cocrystalizing the Escherichia coli TS mutant E60(58)Q with dUMP and the cofactor analog CB3717 and have determined the X-ray crystal structure to 2.5 A resolution with a final R factor of 15.2% (Rfree = 24.0%). Using difference Fourier analysis, we analyzed directly the changes that occur between wild-type and mutant structures. The structure of the mutant enzyme suggests that E60(58) is not required to properly position the ligands in the active site and that the coordinated hydrogen bond network has been disrupted in the mutant, providing an atomic resolution explanation for the impairment of the TS reaction by the E60(58)Q mutant and confirming the proposal that E60(58) coordinates this conserved hydrogen bond network. The structure also provides insight into the role of specific waters in the active site which have been suggested to be important in the TS reaction. Finally, the structure shows a unique conformation for the cofactor analog, CB3717, which has implications for structure-based drug design and sheds light on the controversy surrounding the previously observed enzymatic nonidentity between the chemically identical monomers of the TS dimer.

Published
1996

8. Stereochemical and Conformational Effects on the Cycloaromatization of Dynemicin A-Related Molecules

Author

Daniel Elbaum, Stuart L. Schreiber, Thomas J. Stout, Jon Clardy, and John A. Porco

Subjects
Steric effects, Conformational change, Dynemicin A, Stereochemistry, Aromatization, Epoxide, General Chemistry, Biochemistry, Molecular mechanics, Catalysis, chemistry.chemical_compound, Colloid and Surface Chemistry, chemistry, Molecule, Reactivity (chemistry)
Abstract

A series of compounds was investigated in order to determine the factors that govem the cycloaromatization reaction exhibited by dynemicin A and related molecules. It was determined that the stereochemistry at ClOa dictated the thermal reactivity of compounds equipped with an exo-epoxide. Structures containing an a-substituent were unreactive while those possessing a P-substituent underwent cyclization at 80 "C. Molecular mechanics and dynamics calculations indicate that this reactivity difference is due to a steric interaction that develops as the a-substituted compounds undergo a conformational change that appears to be necessary for aromatization to occur. Additionally, a C 10a a-substituted endo-epoxide was synthesized and shown to undergo cycloaromatization under mild acidic conditions via an epoxide opening.

Published
1995

9. SAR and in vivo evaluation of 4-aryl-2-aminoalkylpyrimidines as potent and selective Janus kinase 2 (JAK2) inhibitors

Author

Matthew Sangyup Lee, Robin Tammie Noguchi, John M. Nuss, Peiwen Zu, Jeff Chen, Brian Kane, Naing Aay, Jia Li, Xian Shi, Brian Hugh Ridgway, Craig Stacy Takeuchi, Elena S. Koltun, Lisa E. Meyr, Henry Johnson, Timothy Patrick Forsyth, Sergey Epshteyn, Brown S David, Byung Gyu Kim, Stefan Engst, Adam A. Galan, Arlyn Arcalas, Gary L. Lewis, Jean-Francois Martini, Vicky Chan, Thomas J. Stout, Robert Kassees, Shwu-Hwa Lin, James W. Leahy, Wentao Zhang, Grace Mann, Philip Tong, Ron Aoyama, Patrick Kearney, Michael Pack, Peiwen Yu, Steven Brian Gendreau, Tai P. Huynh, John Woolfrey, Hongwang Du, and Mohamed Abdulkader Ibrahim

Subjects
Models, Molecular, Proline, High-throughput screening, Clinical Biochemistry, Pharmaceutical Science, Mice, Nude, Antineoplastic Agents, Apoptosis, Pharmacology, Crystallography, X-Ray, Biochemistry, chemistry.chemical_compound, Mice, Structure-Activity Relationship, Dogs, Mouse xenograft, In vivo, Drug Discovery, High-Throughput Screening Assays, Structure–activity relationship, Animals, Molecular Biology, Protein Kinase Inhibitors, Cell Proliferation, Janus kinase 2, biology, Dose-Response Relationship, Drug, Molecular Structure, Chemistry, Aryl, Organic Chemistry, Haplorhini, Neoplasms, Experimental, Janus Kinase 2, Xenograft Model Antitumor Assays, Rats, Pyrimidines, biology.protein, Molecular Medicine
Abstract

We report the discovery of a series of 4-aryl-2-aminoalkylpyrimidine derivatives as potent and selective JAK2 inhibitors. High throughput screening of our in-house compound library led to the identification of hit 1, from which optimization resulted in the discovery of highly potent and selective JAK2 inhibitors. Advanced lead 10d demonstrated a significant dose-dependent pharmacodynamic and antitumor effect in a mouse xenograft model. Based upon the desirable profile of 10d (XL019) it was advanced into clinical trials.

Published
2012

11. New cembradiene diterpenoids from an undescribed Caribbean gorgonian of the genus Eunicea

Author

William Fenical, Thomas J. Stout, Jongheon Shin, and Jon Clardy

Subjects
Plexauridae, chemistry.chemical_compound, Gorgonian, biology, Genus, Chemistry, Stereochemistry, Organic Chemistry, Drug Discovery, Diterpene, biology.organism_classification, Biochemistry
Abstract

Five new cembradiene diterpenoids (1–5) and two previously known compounds (7 and 8) have been isolated from an undescribed Caribbean gorgonian of the genus Eunicea. The structures of these compounds were assigned on the basis of chemical and spectral studies, and the relative stereochemistry of cembradiene 3 was defined by X-ray crystallographic methods.

Published
1993

13. Emeniveol; A new pollen growth inhibitor from the fungus, Emericella nivea

Author

Takashi Hamasaki, Yasuo Kimura, Norihiro Shigemitsu, Masahiko Nishibe, Fumio Sugawara, Hiromitsu Nakajima, Jon Clardy, and Thomas J. Stout

Subjects
biology, Stereochemistry, Chemistry, Pollen, Organic Chemistry, Drug Discovery, medicine, Fungus, biology.organism_classification, medicine.disease_cause, Emericella nivea, Biochemistry
Abstract

Emeniveol (1), a new pollen growth inhibitor, was isolated from the fungus, Emericella nivea. The structure was elucidated from the X-ray crystallographic analysis as well as homonuclear decoupling, COSY, COLOC and HMBC experiments, and chemical reaction.

Published
1992

14. Aplasmomycin c: Structural studies of a marine antibiotic

Author

William Penical, Jon Clardy, Thomas J. Stout, and I. Charles Pathirana

Subjects
Diffraction, Crystallography, Solution state, Chemistry, Organic Chemistry, Drug Discovery, X-ray crystallography, health occupations, Aplasmomycin, Biochemistry, Single crystal
Abstract

The solid and solution state structures of aplasmomycin C, a boroncontaining antibiotic, were studied by single crystal X-ray diffraction and NMR techniques. This unusual antibiotic was shown to have a complex and as yet imperfectly understood series of conformations.

Published
1991

15. Studies on the solution- and solid-state structure of patellin 2

Author

Mark P. Foster, T. Mark Zabriskie, Thomas J. Stout, Jon Clardy, and Chris M. Ireland

Subjects
Crystallography, Colloid and Surface Chemistry, Nuclear magnetic resonance, Chemistry, X-ray crystallography, General Chemistry, Nuclear magnetic resonance spectroscopy, Crystal structure, Biochemistry, Solid state structure, Catalysis
Published
1990

16. Total synthesis of the macrolide antibiotic cytovaricin

Author

Jon Clardy, Todd K. Jones, Stephen W. Kaldor, David A. Evans, and Thomas J. Stout

Subjects
chemistry.chemical_classification, Stereochemistry, medicine.drug_class, Antibiotics, Enantioselective synthesis, Glycoside, Total synthesis, General Chemistry, Alkylation, Biochemistry, Catalysis, Colloid and Surface Chemistry, Polyol, chemistry, Aldol reaction, medicine, Lactone
Abstract

A convergent asymmetric synthesis of the antinoeplastic macrolide antibiotic cytovaricin has been achieved through the synthesis and coupling of the illustrated spiroketal and polyol glycoside subunits. All absolute steroechemical relationships within the target structure were ultimately controlled by the use of asymmetric aldol, alkylation, or epoxidation methodology. Union of the two subnits was accomplished by Julia-Lythgoe trans olefination, providing direct access to a suitable macrolactonization substrate

Published
1990

17. Crystal structures of the phosphorylated and unphosphorylated kinase domains of the Cdc42-associated tyrosine kinase ACK1

Author

Polly Mak, Rui-Hong Chen, Julie Lougheed, and Thomas J. Stout

Subjects
Materials science, Protein Conformation, Molecular Sequence Data, Protein tyrosine phosphatase, SH2 domain, Crystallography, X-Ray, Biochemistry, SH3 domain, Receptor tyrosine kinase, MAP2K7, Apoenzymes, CDC2 Protein Kinase, Humans, Amino Acid Sequence, Phosphorylation, Molecular Biology, biology, Cyclin-dependent kinase 2, Cell Biology, Protein-Tyrosine Kinases, Peptide Fragments, Cell biology, biology.protein, Cyclin-dependent kinase 9, Proto-oncogene tyrosine-protein kinase Src
Abstract

ACK1 is a multidomain non-receptor tyrosine kinase that is an effector of the Cdc42 GTPase. Members of the ACK family have a unique domain ordering and are the only tyrosine kinases known to interact with Cdc42. In contrast with many protein kinases, ACK1 has only a modest increase in activity upon phosphorylation. We have solved the crystal structures of the human ACK1 kinase domain in both the unphosphorylated and phosphorylated states. Comparison of these structures reveals that ACK1 adopts an activated conformation independent of phosphorylation. Furthermore, the unphosphorylated activation loop is structured, and its conformation resembles that seen in activated tyrosine kinases. In addition to the apo structure, complexes are also presented with a non-hydrolyzable nucleotide analog (adenosine 5'-(beta,gamma-methylenetriphosphate)) and with the natural product debromohymenialdisine, a general inhibitor of many protein kinases. Analysis of these structures reveals a typical kinase fold, a pre-organization into the activated conformation, and an unusual substrate-binding cleft.

Published
2004

18. Vinylogous polypeptides: an alternative peptide backbone

Author

Jon Clardy, Neville J. Anthony, Stuart L. Schreiber, Thomas J. Stout, and Masahiko Hagihara

Subjects
Steric effects, Chemistry, Stereochemistry, Hydrogen bond, Solid-state, Pulse sequence, General Chemistry, Nuclear magnetic resonance spectroscopy, Biochemistry, Catalysis, Crystallography, Colloid and Surface Chemistry, Peptide backbone, X-ray crystallography, Chemical solution
Published
1992

19. Structures of active and latent PAI-1: a possible stabilizing role for chloride ions

Author

David J. Matthews, Hugh Graham, Douglas I. Buckley, and Thomas J. Stout

Subjects
Models, Molecular, Protein Conformation, Mutant, DNA, Recombinant, Serpin, In Vitro Techniques, Crystallography, X-Ray, Biochemistry, Chloride, chemistry.chemical_compound, Protein structure, Chlorides, Drug Stability, Plasminogen Activator Inhibitor 1, medicine, Humans, Binding site, Reactive center, Binding Sites, Base Sequence, Chemistry, Mutagenesis, Recombinant Proteins, Crystallography, Plasminogen activator inhibitor-1, Mutagenesis, Site-Directed, medicine.drug
Abstract

Serpins exhibit a range of physiological roles and can contribute to certain disease states dependent on their various conformations. Understanding the mechanisms of the large-scale conformational reorganizations of serpins may lead to a better understanding of their roles in various cardiovascular diseases. We have studied the serpin, plasminogen activator inhibitor 1 (PAI-1), in both the active and the latent state and found that anionic halide ions may play a role in the active-to-latent structural transition. Crystallographic analysis of a stable mutant form of active PAI-1 identified an anion-binding site between the central beta-sheet and a small surface domain. A chloride ion was modeled in this site, and its identity was confirmed by soaking crystals in a bromide-containing solution and calculating a crystallographic difference map. The anion thus located forms a 4-fold ligated linchpin that tethers the surface domain to the central beta-sheet into which the reactive center loop must insert during the active-to-latent transition. Timecourse experiments measuring active PAI-1 stability in the presence of various halide ions showed a clear trend for stabilization of the active form with F(-)Cl(-)Br(-)I(-). We propose that the "stickiness" of this pin (i.e., the electronegativity of the anion) contributes to the energetics of the active-to-latent transition in the PAI-1 serpin.

Published
2000

20. Structure-based design of inhibitors specific for bacterial thymidylate synthase

Author

M. Rinaldi, Robert M. Stroud, Maria Paola Costi, Thomas J. Stout, Daniel V. Santi, Brian K. Shoichet, D. Barlocco, P. Pecorari, Irwin D. Kuntz, and Donatella Tondi

Subjects
Drug, Models, Molecular, Lactobacillus casei, Methyltransferase, Stereochemistry, media_common.quotation_subject, Phenolphthalein, Crystallography, X-Ray, Biochemistry, Thymidylate synthase, Substrate Specificity, drug design, specific inhibitors, crystallography, synthesis, Bacterial Proteins, Species Specificity, Humans, Computer Simulation, Binding site, Enzyme Inhibitors, media_common, chemistry.chemical_classification, Binding Sites, biology, DNA synthesis, Thymidylate Synthase, biology.organism_classification, Lacticaseibacillus casei, Enzyme, chemistry, Amino Acid Substitution, biology.protein, Mutagenesis, Site-Directed, Structure based
Abstract

Thymidylate synthase is an attractive target for antiproliferative drug design because of its key role in the synthesis of DNA. As such, the enzyme has been widely targeted for anticancer applications. In principle, TS should also be a good target for drugs used to fight infectious disease. In practice, TS is highly conserved across species, and it has proven to be difficult to develop inhibitors that are selective for microbial TS enzymes over the human enzyme. Using the structure of TS from Lactobacillus casei in complex with the nonsubstrate analogue phenolphthalein, inhibitors were designed to take advantage of features of the bacterial enzyme that differ from those of the human enzyme. Upon synthesis and testing, these inhibitors were found to be up to 40-fold selective for the bacterial enzyme over the human enzyme. The crystal structures of two of these inhibitors in complex with TS suggested the design of further compounds. Subsequent synthesis and testing showed that these second-round compounds inhibit the bacterial enzyme at sub-micromolar concentrations, while the human enzyme was not inhibited at detectable levels (selectivities of 100-1000-fold or greater). Although these inhibitors share chemical similarities, X-ray crystal structures reveal that the analogues bind to the enzyme in substantially different orientations. Site-directed mutagenesis experiments suggest that the individual inhibitors may adopt multiple configurations in their complexes with TS.

Published
1999

21. D221 in thymidylate synthase controls conformation change, and thereby opening of the imidazolidine

Author

Robert M. Nissen, Robert M. Stroud, C.R. Sage, Thomas J. Stout, Janet Finer-Moore, D. Biermann, and Michelitsch

Subjects
Models, Molecular, Conformational change, Stereochemistry, Macromolecular Substances, Protein Conformation, Ring (chemistry), Crystallography, X-Ray, Biochemistry, Cofactor, Substrate Specificity, chemistry.chemical_compound, Folic Acid, Imidazolidine, Escherichia coli, Fluorodeoxyuridylate, Pterin, Tetrahydrofolates, Cofactor binding, Aspartic Acid, Binding Sites, biology, Hydrogen bond, Imidazoles, Hydrogen Bonding, Thymidylate Synthase, chemistry, Covalent bond, biology.protein, Mutagenesis, Site-Directed, Quinazolines, Asparagine, Protein Binding
Abstract

In thymidylate synthase (TS), the invariant residue Asp-221 provides the only side chain that hydrogen bonds to the pterin ring of the cofactor, 5,10-methylene-5,6,7,8-tetrahydrofolate. All mutants of D221 except cysteine abolish activity. We have determined the crystal structures of two ternary complexes of the Escherichia coli mutant D221N. In a complex with dUMP and the antifolate 10- propargyl-5,8-dideazafolate (CB3717), dUMP is covalently bound to the active site cysteine, as usual. CB3717, which has no imidazolidine ring, is also bound in the usual productive orientation, but is less ordered than in wild-type complexes. The side chain of Asn-221 still hydrogen bonds to N3 of the quinazoline ring of CB3717, which must be in the enol form. In contrast, the structure of D221N with 5-fluoro-dUMP and 5,10-methylene-5,6,7,8-tetrahydrofolate shows the cofactor bound in two partially occupied, nonproductive binding sites. In both binding modes, the cofactor has a closed imidazolidine ring and adopts the solution conformation of the unbound cofactor. In one of the binding sites, the pterin ring is turned around such that Asn-221 hydrogen bonds to the unprotonated N1 instead of the protonated N3 of the cofactor. This orientation blocks the conformational change required for forming covalent ternary complexes. Taken together, the two crystal structures suggest that the hydrogen bond between the side chain of Asp-221 and N3 of the cofactor is most critical during the early steps of cofactor binding, where it enforces the correct orientation of the pterin ring. Proper orientation of the cofactor appears to be a prerequisite for opening the imidazolidine ring prior to formation of the covalent steady-state intermediate in catalysis.

Published
1998

22. Erratum to 'Discovery of XL413, a potent and selective CDC7 inhibitor' [Bioorg. Med. Chem. Lett. 22 (2012) 3727–3731]

Author

Stefan Engst, Manisha Mohan, Jenny Young, Jia Li, Naing Aay, Patrick Kearney, Arlyn Arcalas, Wei Xu, Brian Kane, Peiwen Yu, Wentao Zhang, Scott Robertson, Charles R. Holst, Moon Hwan Kim, Kim Ferguson, Richards Steven J, Gordon M. Stott, Cristiana A. Zaharia, John M. Nuss, Arthur Plonowski, Maurizio Franzini, Amy Lew Tsuhako, Peiwen Zhou, Kevin Noson, Kenneth J. Shaw, Vicky Chan, Ping Huang, Thomas J. Stout, Elena S. Koltun, Hongwang Du, David W. Markby, Brown S David, and Adam A. Galan

Subjects
Chemistry, Organic Chemistry, Clinical Biochemistry, Drug Discovery, Pharmaceutical Science, Molecular Medicine, Theology, Molecular Biology, Biochemistry
Abstract

Erratum to ‘‘Discovery of XL413, a potent and selective CDC7 inhibitor’’ [Bioorg. Med. Chem. Lett. 22 (2012) 3727–3731] Elena S. Koltun ⇑, Amy Lew Tsuhako, David S. Brown, Naing Aay, Arlyn Arcalas, Vicky Chan, Hongwang Du, Stefan Engst, Kim Ferguson, Maurizio Franzini, Adam Galan, Charles R. Holst, Ping Huang, Brian Kane, Moon H. Kim, Jia Li, David Markby, Manisha Mohan, Kevin Noson, Arthur Plonowski, Steven J. Richards, Scott Robertson, Kenneth Shaw, Gordon Stott, Thomas J. Stout, Jenny Young, Peiwen Yu, Cristiana A. Zaharia, Wentao Zhang, Peiwen Zhou, John M. Nuss, Wei Xu, Patrick C. Kearney

Published
2012

23. Salinamides A and B: anti-inflammatory depsipeptides from a marine streptomycete

Author

Jacqueline A. Trischman, Paul R. Jensen, Jon Clardy, Chris M. Ireland, Tawnya C. McKee, William Fenical, Dianne M. Tapiolas, Ryan H. Dwight, and Thomas J. Stout

Subjects
Depsipeptide, biology, Chemistry, Stereochemistry, medicine.drug_class, Streptomycetaceae, Biological activity, General Chemistry, biology.organism_classification, Biochemistry, Streptomyces, Catalysis, Anti-inflammatory, Colloid and Surface Chemistry, medicine, Actinomycetales, Bacteria
Published
1994

24. The three-dimensional structure of neohalicholactone, an unusual fatty acid metabolite from the marine sponge halichondria okadai kadota

Author

Hideo Kigoshi, Jon Clardy, Kiyoyuki Yamada, Haruki Niwa, and Thomas J. Stout

Subjects
chemistry.chemical_classification, biology, Stereochemistry, Metabolite, Organic Chemistry, Fatty acid, biology.organism_classification, Biochemistry, Neohalicholactone, chemistry.chemical_compound, Sponge, Three dimensional shape, chemistry, Drug Discovery, Lactone, Halichondria okadai
Abstract

The three-dimensional structure of the unusual fatty acid metabolite neohalicholactone, isolated from the marine sponge Halinchondria okadai Kadota, has been determined by X-ray crystallography.

Published
1991

26. Transannular Diels-Alder route to systems related to dynemicin A

Author

Jon Clardy, Frank J. Schoenen, Stuart L. Schreiber, John A. Porco, and Thomas J. Stout

Subjects
chemistry.chemical_classification, chemistry.chemical_compound, Colloid and Surface Chemistry, Polycyclic compound, Dynemicin A, chemistry, Diels alder, Organic chemistry, General Chemistry, Biochemistry, Catalysis, Lactone
Published
1990

27. Ohioensin-A: a novel benzonaphthoxanthenone from Polytrichum ohioense

Author

John M. Cassady, Jon Clardy, Ching Jer Chang, Guo Qiang Zheng, and Thomas J. Stout

Subjects
chemistry.chemical_classification, biology, Chemistry, Stereochemistry, General Chemistry, biology.organism_classification, Biochemistry, Catalysis, Polytrichaceae, Colloid and Surface Chemistry, Polycyclic compound, Organic chemistry, Molecule, Polytrichum ohioense
Published
1989

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