Your search keyword '"Ruth Lehr"' showing total 12 results

1. Discovery of a First-in-Class Receptor Interacting Protein 1 (RIP1) Kinase Specific Clinical Candidate (GSK2982772) for the Treatment of Inflammatory Diseases

Author

Xiaoyang Dong, Anna Vossenkämper, Attiq Rahman, Viera Kasparcova, Robert Singhaus, Joshua N. Finger, Bryan W. King, Patrick M. Eidam, Michael Reilly, David D. Wisnoski, Scott B. Berger, John D. Lich, James Kang, Michael T. Ouellette, Lauren Dare, Philip A. Harris, Julie A. Cox, Nathan A. Miller, John Bertin, Michelle C. Schaeffer, Deepak Bandyopadhyay, Daohua Zhang, Alan R. Rendina, Clark A. Sehon, Sandra J. Hoffman, Peter J. Gough, Rachel D. Totoritis, Thomas T. MacDonald, Yunfeng Lan, Paris Ward, Barbara A. Swift, Robert W. Marquis, Lara Kathryn Leister, Rakesh Nagilla, Elizabeth J. Rivera, Helen H. Sun, Carol A. Capriotti, Nino Campobasso, Ruth Lehr, Christina S. Pao, and Jae U. Jeong

Subjects

0301 basic medicine, Swine, Necroptosis, Anti-Inflammatory Agents, Inflammation, Pharmacology, Mice, 03 medical and health sciences, Dogs, 0302 clinical medicine, Psoriasis, Drug Discovery, medicine, Animals, Humans, Potency, Protein Kinase Inhibitors, Tumor Necrosis Factor-alpha, Chemistry, Kinase, Haplorhini, Benzazepines, medicine.disease, Ulcerative colitis, Rats, Molecular Docking Simulation, 030104 developmental biology, Receptor-Interacting Protein Serine-Threonine Kinases, 030220 oncology & carcinogenesis, Rheumatoid arthritis, Cytokines, Swine, Miniature, Molecular Medicine, Colitis, Ulcerative, Rabbits, medicine.symptom, RECEPTOR-INTERACTING PROTEIN

Abstract

RIP1 regulates necroptosis and inflammation and may play an important role in contributing to a variety of human pathologies, including immune-mediated inflammatory diseases. Small-molecule inhibitors of RIP1 kinase that are suitable for advancement into the clinic have yet to be described. Herein, we report our lead optimization of a benzoxazepinone hit from a DNA-encoded library and the discovery and profile of clinical candidate GSK2982772 (compound 5), currently in phase 2a clinical studies for psoriasis, rheumatoid arthritis, and ulcerative colitis. Compound 5 potently binds to RIP1 with exquisite kinase specificity and has excellent activity in blocking many TNF-dependent cellular responses. Highlighting its potential as a novel anti-inflammatory agent, the inhibitor was also able to reduce spontaneous production of cytokines from human ulcerative colitis explants. The highly favorable physicochemical and ADMET properties of 5, combined with high potency, led to a predicted low oral dose in humans.

Published

2017

2. DNA-Encoded Library Screening Identifies Benzo[b][1,4]oxazepin-4-ones as Highly Potent and Monoselective Receptor Interacting Protein 1 Kinase Inhibitors

Author

Michelle C. Schaeffer, Peter J. Gough, James Kang, Viera Kasparcova, Jae U. Jeong, LaShadric C. Grady, Joshua N. Finger, Paris Ward, Daohua Zhang, Robert W. Marquis, Lauren Dare, Michael T. Ouellette, Deepak Bandyopadhyay, Rakesh Nagilla, Xiaoyang Dong, Carol A. Capriotti, Christina S. Pao, Nino Campobasso, Rachel D. Totoritis, Philip A. Harris, Ruth Lehr, Jennifer Summerfield, Bryan W. King, Ami S. Lakdawala, Julie A. Cox, Barbara A. Swift, Aming Zhang, Scott B. Berger, John Bertin, Dean E. McNulty, Alan R. Rendina, and Sandra J. Hoffman

Subjects

0301 basic medicine, Models, Molecular, Crystallography, X-Ray, 01 natural sciences, Small Molecule Libraries, 03 medical and health sciences, chemistry.chemical_compound, Mice, Structure-Activity Relationship, Cell Line, Tumor, Drug Discovery, Structure–activity relationship, Potency, Animals, Humans, Protein Kinase Inhibitors, U937 cell, Dose-Response Relationship, Drug, Molecular Structure, 010405 organic chemistry, Chemistry, Kinase, DNA, Isoxazoles, U937 Cells, 0104 chemical sciences, Oxazepines, 030104 developmental biology, Biochemistry, Cell culture, Receptor-Interacting Protein Serine-Threonine Kinases, Molecular Medicine, Tumor necrosis factor alpha, HT29 Cells

Abstract

The recent discovery of the role of receptor interacting protein 1 (RIP1) kinase in tumor necrosis factor (TNF)-mediated inflammation has led to its emergence as a highly promising target for the treatment of multiple inflammatory diseases. We screened RIP1 against GSK's DNA-encoded small-molecule libraries and identified a novel highly potent benzoxazepinone inhibitor series. We demonstrate that this template possesses complete monokinase selectivity for RIP1 plus unique species selectivity for primate versus nonprimate RIP1. We elucidate the conformation of RIP1 bound to this benzoxazepinone inhibitor driving its high kinase selectivity and design specific mutations in murine RIP1 to restore potency to levels similar to primate RIP1. This series differentiates itself from known RIP1 inhibitors in combining high potency and kinase selectivity with good pharmacokinetic profiles in rodents. The favorable developability profile of this benzoxazepinone template, as exemplified by compound 14 (GSK'481), makes it an excellent starting point for further optimization into a RIP1 clinical candidate.

Published

2016

3. On the Catalytic Mechanism of Human ATP Citrate Lyase

Author

Thomas D. Meek, Frank M. Raushel, Hongwei Qi, Huizhen Zhao, Joseph Boyer, Benjamin Schwartz, Taylor L. Graham, Howard J. Williams, Fan Fan, and Ruth Lehr

Subjects

Oxaloacetic Acid, ATP citrate lyase, Stereochemistry, Coenzyme A, ATP Citrate (pro-S)-Lyase, Biochemistry, chemistry.chemical_compound, Biosynthesis, Acetyl Coenzyme A, Catalytic Domain, Oxaloacetic acid, Humans, Citrate synthase, Histidine, Phosphorylation, Conserved Sequence, biology, Chemistry, Deuterium Exchange Measurement, Active site, musculoskeletal system, Mutation, Biocatalysis, biology.protein

Abstract

ATP citrate lyase (ACL) catalyzes an ATP-dependent biosynthetic reaction which produces acetyl-coenzyme A and oxaloacetate from citrate and coenzyme A (CoA). Studies were performed with recombinant human ACL to ascertain the nature of the catalytic phosphorylation that initiates the ACL reaction and the identity of the active site residues involved. Inactivation of ACL by treatment with diethylpyrocarbonate suggested the catalytic role of an active site histidine (i.e., His760), which was proposed to form a phosphohistidine species during catalysis. The pH-dependence of the pre-steady-state phosphorylation of ACL with [γ-(33)P]-ATP revealed an ionizable group with a pK(a) value of ~7.5, which must be unprotonated for the catalytic phosphorylation of ACL to occur. Mutagenesis of His760 to an alanine results in inactivation of the biosynthetic reaction of ACL, in good agreement with the involvement of a catalytic histidine. The nature of the formation of the phospho-ACL was further investigated by positional isotope exchange using [γ-(18)O(4)]-ATP. The β,γ-bridge to nonbridge positional isotope exchange rate of [γ-(18)O(4)]-ATP achieved its maximal rate of 14 s(-1) in the absence of citrate and CoA. This rate decreased to 5 s(-1) when citrate was added, and was found to be 10 s(-1) when both citrate and CoA were present. The rapid positional isotope exchange rates indicated the presence of one or more catalytically relevant, highly reversible phosphorylated intermediates. Steady-state measurements in the absence of citrate and CoA showed that MgADP was produced by both wild type and H760A forms of ACL, with rates at three magnitudes lower than that of k(cat) for the full biosynthetic reaction. The ATPase activity of ACL, along with the small yet significant positional isotope exchange rate observed in H760A mutant ACL (~150 fold less than wild type), collectively suggested the presence of a second, albeit unproductive, phosphoryl transfer in ACL. Mathematical analysis and computational simulation suggested that the desorption of MgADP at a rate of ~7 s(-1) was the rate-limiting step in the biosynthesis of AcCoA and oxaloacetate.

Published

2012

4. Crystal structure of the kinase domain of serum and glucocorticoid-regulated kinase 1 in complex with AMP-PNP

Author

Tanya Randall, Thau F. Ho, Ruth Lehr, Kathleen Maley, Christine G. Schnackenberg, Martha S. Head, Angela Smallwood, Kristin K. Koretke, and Baoguang Zhao

Subjects

Models, Molecular, Protein Conformation, Adenylyl Imidodiphosphate, Molecular Sequence Data, Serine threonine protein kinase, Protein Serine-Threonine Kinases, Crystallography, X-Ray, Biochemistry, Protein Structure, Secondary, SH3 domain, Immediate-Early Proteins, MAP2K7, Adenosine Triphosphate, Catalytic Domain, Humans, Amino Acid Sequence, c-Raf, Protein kinase A, Molecular Biology, Serine/threonine-specific protein kinase, Binding Sites, Molecular Structure, urogenital system, Chemistry, Protein Structure, Tertiary, Protein Structure Report, Biophysics, Cyclin-dependent kinase complex, Casein kinase 2, Dimerization, Hydrophobic and Hydrophilic Interactions, Sequence Alignment

Abstract

Serum and glucocorticoid-regulated kinase 1 (SGK1) is a serine/threonine protein kinase of the AGC family which participates in the control of epithelial ion transport and is implicated in proliferation and apoptosis. We report here the 1.9 A crystal structure of the catalytic domain of inactive human SGK1 in complex with AMP-PNP. SGK1 exists as a dimer formed by two intermolecular disulfide bonds between Cys258 in the activation loop and Cys193. Although most of the SGK1 structure closely resembles the common protein kinase fold, the structure around the active site is unique when compared to most protein kinases. The alphaC helix is not present in this inactive form of SGK1 crystal structure; instead, the segment corresponding to the C helix forms a beta-strand that is stabilized by the N-terminal segment of the activation loop through a short antiparallel beta-sheet. Since the differences from other kinases occur around the ATP binding site, this structure can provide valuable insight into the design of selective and highly potent ATP-competitive inhibitors of SGK1 kinase.

Published

2007

5. Inhibition of T Lymphocyte Actnation by a Novel p56lckTyrosine Kinase Inhibitor

Author

Patricia Mauvais, Jay Sarup, Deborah Ann Miller, Susan Hoekstra, Bruce Gauvin, Paul Juniewicz, Su Wang, Ruth Lehr, Wen Xie, John Reid, Dennis J. Murphy, David G. Sawutz, and Connie R. Faltynek

Subjects

CD3 Complex, medicine.drug_class, T-Lymphocytes, Protein tyrosine phosphatase, Biochemistry, Tropomyosin receptor kinase C, Antibodies, Piperazines, Receptor tyrosine kinase, Tyrosine-kinase inhibitor, medicine, Humans, Enzyme Inhibitors, Phosphorylation, Cells, Cultured, biology, Chemistry, Molecular biology, Kinetics, src-Family Kinases, Lymphocyte Specific Protein Tyrosine Kinase p56(lck), CD4 Antigens, ROR1, Quinolines, Cancer research, biology.protein, Tyrosine, Molecular Medicine, Tyrosine kinase, Platelet-derived growth factor receptor, Proto-oncogene tyrosine-protein kinase Src

Abstract

A new p56idk tyrosine kinase inhibitor WIN 61651 [1,4-dihydro-7-(4-methyl-1-piperizinyl)-1-(4-(4-methyl-1-piperizinyl))phenyl-4-oxo-3-quinolinecarboxamide) is described. WIN 61651, which is competitive with AP, demonstrates selectivity for the lymphoid restricted tyrosine kinase p56lck over serine/threonine kinases, such as protein kinase C and protein kinase A, and over some other tyrosine kinases, including erbB2, epidermal growth factor receptor, and insulin receptor; however, it is equipotent for inhibition of p56lck and the platelet derived growth factor receptor tyrosine kinases. WIN 61651 inhibits p56lck activity in cell-free assays, tyrosine kinase activity in a T lymphocytic cell line, and T cell activation, as measured by IL-2 production by purified CD4 positive peripheral blood T lymphocytes and the mixed lymphocyte reaction. WIN 61651 constitutes a new tool for studies on the role for tyrosine kinases in lymphocyte function.

Published

1995

6. Kinetic mechanism and rate-limiting steps of focal adhesion kinase-1

Author

James P. Villa, Kang Yan, Angela Smallwood, Khyati Oza, Robert B. Kirkpatrick, Jessica L. Schneck, Sara H. Thrall, Baoguang Zhao, Patrick McDevitt, Jacques Briand, Stephanie Chen, Ruth Lehr, Nestor O. Concha, and Thomas D. Meek

Subjects

Models, Molecular, Stereochemistry, Kinetics, Adenylyl Imidodiphosphate, Molecular Sequence Data, chemistry.chemical_element, Kinetic energy, Crystallography, X-Ray, Biochemistry, Oxygen, Models, Biological, Catalysis, chemistry.chemical_compound, Adenosine Triphosphate, Humans, Amino Acid Sequence, Phosphorylation, Autophosphorylation, Solvent, Crystallography, chemistry, Focal Adhesion Kinase 1, Peptides, Adenosine triphosphate, Protein Binding

Abstract

Steady-state kinetic analysis of focal adhesion kinase-1 (FAK1) was performed using radiometric measurement of phosphorylation of a synthetic peptide substrate (Ac-RRRRRRSETDDYAEIID-NH(2), FAK-tide) which corresponds to the sequence of an autophosphorylation site in FAK1. Initial velocity studies were consistent with a sequential kinetic mechanism, for which apparent kinetic values k(cat) (0.052 +/- 0.001 s(-1)), K(MgATP) (1.2 +/- 0.1 microM), K(iMgATP) (1.3 +/- 0.2 microM), K(FAK-tide) (5.6 +/- 0.4 microM), and K(iFAK-tide) (6.1 +/- 1.1 microM) were obtained. Product and dead-end inhibition data indicated that enzymatic phosphorylation of FAK-tide by FAK1 was best described by a random bi bi kinetic mechanism, for which both E-MgADP-FAK-tide and E-MgATP-P-FAK-tide dead-end complexes form. FAK1 catalyzed the betagamma-bridge:beta-nonbridge positional oxygen exchange of [gamma-(18)O(4)]ATP in the presence of 1 mM [gamma-(18)O(4)]ATP and 1.5 mM FAK-tide with a progressive time course which was commensurate with catalysis, resulting in a rate of exchange to catalysis of k(x)/k(cat) = 0.14 +/- 0.01. These results indicate that phosphoryl transfer is reversible and that a slow kinetic step follows formation of the E-MgADP-P-FAK-tide complex. Further kinetic studies performed in the presence of the microscopic viscosogen sucrose revealed that solvent viscosity had no effect on k(cat)/K(FAK-tide), while k(cat) and k(cat)/K(MgATP) were both decreased linearly at increasing solvent viscosity. Crystallographic characterization of inactive versus AMP-PNP-liganded structures of FAK1 showed that a large conformational motion of the activation loop upon ATP binding may be an essential step during catalysis and would explain the viscosity effect observed on k(cat)/K(m) for MgATP but not on k(cat)/K(m) for FAK-tide. From the positional isotope exchange, viscosity, and structural data it may be concluded that enzyme turnover (k(cat)) is rate-limited by both reversible phosphoryl group transfer (k(forward) approximately 0.2 s(-1) and k(reverse) approximately 0.04 s(-1)) and a slow step (k(conf) approximately 0.1 s(-1)) which is probably the opening of the activation loop after phosphoryl group transfer but preceding product release.

Published

2010

7. Characterization of PI3K class IA isoforms with regulatory subunit p55alpha using a scintillation proximity assay

Author

Jeffrey D. Carson, Lusong Luo, Robert H. Sinnamon, Peter J. Tummino, Ruth Lehr, Glenn S. Van Aller, Christine Fernandes, and Robert B. Kirkpatrick

Subjects

Protein subunit, Biophysics, Drug Evaluation, Preclinical, Biology, P110α, Biochemistry, Wortmannin, chemistry.chemical_compound, Phosphatidylinositol 3-Kinases, Humans, Kinase activity, Enzyme Inhibitors, Molecular Biology, Phosphoinositide-3 Kinase Inhibitors, Biological Products, Phosphoinositide 3-kinase, Dose-Response Relationship, Drug, Assay, Titrimetry, Cell Biology, Hydrogen-Ion Concentration, Molecular biology, Microspheres, Isoenzymes, Protein Subunits, Scintillation proximity assay, chemistry, P110δ, biology.protein, Biocatalysis, Scintillation Counting

Abstract

Differential activation of the phosphoinositide 3-kinase (PI3K)/AKT pathway has been linked to cancer. Activation occurs through gene amplification and activating mutations. High-frequency mutations in the gene encoding the p110alpha catalytic subunit of PI3K (PIK3CA) have been observed in a variety of tumors including colon, brain, breast, ovarian, and gastric. Inhibition of PI3K kinase activity may provide a specific way to treat multiple types of human cancer. A scintillation proximity assay (SPA) was developed to detect phosphatidylinositol 3-kinase catalytic activity. Using this assay format, steady-state kinetic parameters were compared for the PI3K class IA enzymes p110alpha, p110beta, and p110delta, each coexpressed with the regulatory subunit p85alpha or splice variant p55alpha. Inhibition by the natural product wortmannin and LY294002 was detected with potencies consistent with alternate assay formats. Other biochemical assay formats have been described for phosphoinositide 3-kinases but each has its unique limitations. The simple, inexpensive, sensitive high-throughput nature of the SPA format has advanced our knowledge of isoform-specific enzymology and will facilitate the discovery of novel PI3K inhibitors.

Published

2008

8. Effects of oncogenic p110alpha subunit mutations on the lipid kinase activity of phosphoinositide 3-kinase

Author

Glenn S. Van Aller, Kurt R. Auger, Robert H. Sinnamon, Dashyant Dhanak, Ruth Lehr, Robert A. Copeland, Robert B. Kirkpatrick, Lusong Luo, Jeffrey D. Carson, Richard R. Gontarek, and Peter J. Tummino

Subjects

Class I Phosphatidylinositol 3-Kinases, Lipid kinase activity, Mitogen-activated protein kinase kinase, Biochemistry, MAP2K7, Phosphatidylinositol 3-Kinases, Adenosine Triphosphate, Catalytic Domain, Tumor Cells, Cultured, Humans, ASK1, Phosphorylation, Molecular Biology, Alleles, Adaptor Proteins, Signal Transducing, MAP kinase kinase kinase, biology, Cyclin-dependent kinase 4, Cyclin-dependent kinase 2, Cell Biology, Oncogenes, Molecular biology, Recombinant Proteins, Enzyme Activation, Kinetics, Mutation, biology.protein, Insulin Receptor Substrate Proteins, Cyclin-dependent kinase 9

Abstract

The PIK3CA gene, encoding the p110α catalytic subunit of Class IA PI3Ks (phosphoinositide 3-kinases), is frequently mutated in many human tumours. The three most common tumour-derived alleles of p110α, H1047R, E542K and E545K, were shown to potently activate PI3K signalling in human epithelial cells. In the present study, we examine the biochemical activity of the recombinantly purified PI3K oncogenic mutants. The kinetic characterizations of the wt (wild-type) and the three ‘hot spot’ PI3K mutants show that the mutants all have approx. 2-fold increase in lipid kinase activities. Interestingly, the phosphorylated IRS-1 (insulin receptor substrate-1) protein shows activation of the lipid kinase activity for the wt and H1047R but not E542K and E545K PI3Kα, suggesting that these mutations represent different mechanisms of lipid kinase activation and hence transforming activity in cancer cells.

Published

2007

9. Interleukin-1F7B (IL-1H4/IL-1F7) is processed by caspase-1 and mature IL-1F7B binds to the IL-18 receptor but does not induce IFN-gamma production

Author

Andrea Gambotto, Charles Hanning, Michael T. Lotze, Ruth Lehr, David J. Rieman, Michael Brigham-Burke, Wentao Gao, John C. Lee, Frank J. Lynch, Robert B. Kirkpatrick, Sanjay S. Khandekar, Sanjay Kumar, and Gilbert F. Scott

Subjects

DNA, Complementary, Recombinant Fusion Proteins, Immunology, Caspase 1, Biochemistry, Cell Line, Interferon-gamma, Immunology and Allergy, Humans, Amino Acid Sequence, Binding site, Receptor, Molecular Biology, Peptide sequence, Caspase, Receptors, Interleukin-18, Binding Sites, biology, HEK 293 cells, Interleukin-18, Hematology, Receptors, Interleukin, Fusion protein, Molecular biology, Cell biology, Cell culture, Caspases, biology.protein, Interleukin-18 Receptor alpha Subunit, Interleukin-1

Abstract

We have recently reported the identification of four novel members of the interleukin-1 (IL-1) family which we designated as IL-1 homologue 1-4 (IL-1H1-4). These proteins exhibit significant sequence homology to other members of the IL-1 family. Of these homologues, only IL-1H4 (renamed IL-1F7b) was predicted to contain a propeptide domain and a caspase cleavage site. We now report that caspase-1 cleaves IL-1F7b at the predicted site to generate mature IL-1F7b. Caspase-4 was also able to process IL-1F7b, albeit inefficiently. Other caspases and Granzyme-B did not cleave IL-1F7b. Furthermore, adenovirus-mediated expression of IL-1F7b in HEK 293 cells led to in situ processing and secretion of mature IL-1F7b. In a screen to identify a potential receptor, both pro and mature IL-1F7b bound to the soluble IL-18 receptor alpha-Fc (IL-18Ralpha-Fc) but not to the soluble IL-1R-Fc or ST2R-Fc fusion proteins. Mature IL-1F7b bound to the IL-18Ralpha-Fc protein with higher affinity than the pro form, although the affinities for both proteins were significantly lower than that observed for IL-18. Consistent with this observation, only IL-18 and not IL-1F7b induced IFN-gamma production by KG1a cells. We also report that pro and mature IL-1F7b form homodimers with association constants of 4 microM and 5 nM, respectively, suggesting biological relevance to IL-1F7b processing. Finally, we have localized the expression of IL-1F7b protein in discrete cell populations including plasma cells and tumor cells. These data suggest that IL-1F7b may be involved in immune response, inflammatory diseases and/or cancer.

Published

2002

10. Inhibition of transforming growth factor (TGF)-beta1-induced extracellular matrix with a novel inhibitor of the TGF-beta type I receptor kinase activity: SB-431542

Author

Barbara A. Olson, Ruth Lehr, J. Bomberger, C. Tweed, S. Butter, Eugene T. Grygielko, Nicholas J. Laping, W. Martin, John D. Harling, Laramie Mary Gaster, James A. Fornwald, James F. Callahan, and A. Mathur

Subjects

MAPK/ERK pathway, Pyridines, Receptor, Transforming Growth Factor-beta Type I, SMAD, Dioxoles, Protein Serine-Threonine Kinases, p38 Mitogen-Activated Protein Kinases, Collagen Type I, Thrombospondin 1, Transforming Growth Factor beta1, chemistry.chemical_compound, Transforming Growth Factor beta, Plasminogen Activator Inhibitor 1, Extracellular, Tumor Cells, Cultured, Humans, RNA, Messenger, Kinase activity, Enzyme Inhibitors, Protein kinase A, Pharmacology, biology, Chemistry, Kinase, Imidazoles, Molecular biology, Extracellular Matrix, Fibronectins, Fibronectin, Benzamides, biology.protein, Molecular Medicine, SB-431542, Mitogen-Activated Protein Kinases, Activin Receptors, Type I, Receptors, Transforming Growth Factor beta

Abstract

Transforming growth factor beta1 (TGF-beta1) is a potent fibrotic factor responsible for the synthesis of extracellular matrix. TGF-beta1 acts through the TGF-beta type I and type II receptors to activate intracellular mediators, such as Smad proteins, the p38 mitogen-activated protein kinase (MAPK), and the extracellular signal-regulated kinase pathway. We expressed the kinase domain of the TGF-beta type I receptor [activin receptor-like kinase (ALK)5] and the substrate, Smad3, and determined that SB-431542 is a selective inhibitor of Smad3 phosphorylation with an IC50 of 94 nM. It inhibited TGF-beta1-induced nuclear Smad3 localization. The p38 mitogen-activated protein kinase inhibitors SB-203580 and SB-202190 also inhibit phosphorylation of Smad3 by ALK5 with IC50 values of 6 and 3 microM, respectively. This suggests that these p38 MAPK inhibitors must be used at concentrations of less than 10 microM to selectively address p38 MAPK mechanisms. However, the p38 MAPK inhibitor SB-242235 did not inhibit ALK5. To evaluate the relative contribution of Smad signaling and p38 MAPK signaling in TGF-beta1-induced matrix production, the effect of SB-431542 was compared with that of SB-242235 in renal epithelial carcinoma A498 cells. All compounds inhibited TGF-beta1-induced fibronectin (FN) mRNA, indicating that FN synthesis is mediated in part via the p38 MAPK pathway. In contrast, SB-431542, but not the selective p38 MAPK inhibitor SB-242235, inhibited TGF-beta1-induced collagen Ialpha1 (col Ialpha1). These data indicate that some matrix markers that are stimulated by TGF-beta1 are mediated via the p38 MAPK pathway (i.e., FN), whereas others seem to be activated via ALK5 signaling independent of the p38 MAPK pathway (i.e., col Ialpha1).

Published

2002

11. Identification of novel inhibitors of the transforming growth factor beta1 (TGF-beta1) type 1 receptor (ALK5)

Author

Joseph Weinstock, A. Mathur, Chet Kwon, Barbara A. Olson, James A. Fornwald, Ruth Lehr, Jag Paul Heer, Nicholas J. Laping, John D. Harling, James F. Callahan, Laramie Mary Gaster, Joelle Lorraine Burgess, and Harrington Frank Peter

Subjects

Receptor, Transforming Growth Factor-beta Type I, Protein Serine-Threonine Kinases, p38 Mitogen-Activated Protein Kinases, Structure-Activity Relationship, Drug Discovery, Tumor Cells, Cultured, Humans, RNA, Messenger, Smad3 Protein, Enzyme Inhibitors, Cytotoxicity, Receptor, biology, Chemistry, Imidazoles, Activin receptor, Molecular biology, Fibronectins, Fibronectin, DNA-Binding Proteins, Biochemistry, Cell culture, Enzyme inhibitor, biology.protein, Trans-Activators, Molecular Medicine, Signal transduction, Mitogen-Activated Protein Kinases, Activin Receptors, Type I, Receptors, Transforming Growth Factor beta, Transforming growth factor

Abstract

Screening of our internal compound collection for inhibitors of the transforming growth factor beta1 (TGF-beta1) type I receptor (ALK5) identified several hits. Optimization of the dihydropyrroloimidazole hit 2 by introduction of a 2-pyridine and 3,4-methylenedioxyphenyl group gave 7, a selective ALK5 inhibitor. With this information, optimization of the triarylimidazole hit 8 gave the selective inhibitor 14, which inhibits TGF-beta1-induced fibronectin mRNA formation while displaying no measurable cytotoxicity in the 48 h XTT assay.

Published

2002

12. Identification and initial characterization of four novel members of the interleukin-1 family

Author

Grace I. Wells, M. N. Tzimas, Peter R. Young, Elizabeth A. Capper, Michael L. Doyle, Ruth Tal-Singer, Peter C. McDonnell, Sanjay Kumar, Lauren A. Tierney, Ruth Lehr, and Don E. Griswold

Subjects

Keratinocytes, Protein Folding, Molecular Sequence Data, Sequence alignment, Herpesvirus 1, Human, Biology, Fibroblast growth factor, Biochemistry, Epithelium, Protein Structure, Secondary, Mice, Protein structure, Cell surface receptor, Animals, Humans, Protein Isoforms, Amino Acid Sequence, RNA, Messenger, Cloning, Molecular, Receptor, Molecular Biology, Peptide sequence, Cells, Cultured, Genetics, Regulation of gene expression, Expressed sequence tag, Sequence Homology, Amino Acid, Circular Dichroism, Oxazolone, Herpes Simplex, Cell Biology, Recombinant Proteins, Cell biology, Gene Expression Regulation, Sequence Alignment, Interleukin-1

Abstract

Interleukin-1 (IL-1), fibroblast growth factors (FGFs), and their homologues are secreted factors that share a common beta-barrel structure and act on target cells by binding to cell surface receptors with immunoglobulin-like folds in their extracellular domain. While numerous members of the FGF family have been discovered, the IL-1 family has remained small and outnumbered by IL-1 receptor homologues. From expressed sequence tag data base searches, we have now identified four additional IL-1 homologues, IL-1H1, IL-1H2, IL-1H3, and IL-1H4. Like most other IL-1/FGFs, these proteins do not contain a hydrophobic leader sequence. IL-1H4 has a propeptide sequence, while IL-1H1, IL-1H2, and IL-1H3 encode only the mature protein. Circular dichroism spectra and thermal stability analysis suggest that IL-1H1 folds similarly to IL-1ra. The novel homologues are not widely expressed in mammals. IL-1H1 is constitutively expressed only in placenta and the squamous epithelium of the esophagus. However, IL-1H1 could be induced in vitro in keratinocytes by interferon-gamma and tumor necrosis factor-alpha and in vivo via a contact hypersensitivity reaction or herpes simplex virus infection. This suggests that IL-1H1 may be involved in pathogenesis of immune mediated disease processes. The addition of four novel IL-1 homologues suggests that the IL-1 family is significantly larger than previously thought.

Published

2000