Your search keyword '"Walker, John K."' showing total 46 results

1. The Estrogen Receptor-Related Orphan Receptors Regulate Autophagy through TFEB.

Author

Losby M, Hayes M, Valfort A, Sopariwala DH, Sanders R, Walker JK, Xu W, Narkar VA, Zhang L, Billon C, and Burris TP

Subjects

Animals, Rats, Mice, Humans, Cell Line, ERRalpha Estrogen-Related Receptor, Rats, Sprague-Dawley, Basic Helix-Loop-Helix Leucine Zipper Transcription Factors metabolism, Basic Helix-Loop-Helix Leucine Zipper Transcription Factors genetics, Autophagy physiology, Receptors, Estrogen metabolism, Myocytes, Cardiac metabolism, Myocytes, Cardiac drug effects

Abstract

Autophagy is an essential self-degradative and recycling mechanism that maintains cellular homeostasis. Estrogen receptor-related orphan receptors (ERRs) are fundamental in regulating cardiac metabolism and function. Previously, we showed that ERR agonists improve cardiac function in models of heart failure and induce autophagy. Here, we characterized a mechanism by which ERRs induce the autophagy pathway in cardiomyocytes. Transcription factor EB (TFEB) is a master regulator of the autophagy-lysosome pathway and has been shown to be crucial regulator of genes that control autophagy. We discovered that TFEB is a direct ERR target gene whose expression is induced by ERR agonists. Activation of ERR results in increased TFEB expression in both neonatal rat ventricular myocytes and C 2 C 12 myoblasts. An ERR-dependent increase in TFEB expression results in increased expression of an array of TFEB target genes, which are critical for the stimulation of autophagy. Pharmacologically targeting ERR is a promising potential method for the treatment of many diseases where stimulation of autophagy may be therapeutic, including heart failure. SIGNIFICANCE STATEMENT: Estrogen receptor-related receptor agonists function as exercise mimetics and also display efficacy in animal models of metabolic disease, obesity, and heart failure., (Copyright © 2024 by The American Society for Pharmacology and Experimental Therapeutics.)

Published

2024

2. Computational structural prediction and chemical inhibition of the human mitochondrial pyruvate carrier protein heterodimer complex.

Author

Hadfield CM, Walker JK, Arnatt C, and McCommis KS

Abstract

The mitochondrial pyruvate carrier (MPC) plays a role in numerous diseases including neurodegeneration, metabolically dependent cancers, and the development of insulin resistance. Several previous studies in genetic mouse models or with existing inhibitors suggest that inhibition of the MPC could be used as a viable therapeutic strategy in these diseases. However, the MPC's structure is unknown, making it difficult to screen for and develop therapeutically viable inhibitors. Currently known MPC inhibitors would make for poor drugs due to their poor pharmacokinetic properties, or in the case of the thiazolidinediones (TZDs), off-target specificity for peroxisome-proliferator activated receptor gamma (PPARγ) leads to unwanted side effects. In this study, we develop several structural models for the MPC heterodimer complex and investigate the chemical interactions required for the binding of these known inhibitors to MPC and PPARγ. Based on these models, the MPC most likely takes on outward-facing (OF) and inward-facing (IF) conformations during pyruvate transport, and inhibitors likely plug the carrier to inhibit pyruvate transport. Although some chemical interactions are similar between MPC and PPARγ binding, there is likely enough difference to reduce PPARγ specificity for future development of novel, more specific MPC inhibitors., Competing Interests: Conflicts of Interest Statement None declared.

Published

2024

3. AdeIJK Pump-Specific Inhibitors Effective against Multidrug Resistant Acinetobacter baumannii .

Author

Tambat R, Kinthada RK, Saral Sariyer A, Leus IV, Sariyer E, D'Cunha N, Zhou H, Leask M, Walker JK, and Zgurskaya HI

Subjects

Humans, A549 Cells, Drug Synergism, Membrane Transport Proteins metabolism, Microbial Sensitivity Tests, Acinetobacter baumannii drug effects, Acinetobacter Infections microbiology, Acinetobacter Infections drug therapy, Anti-Bacterial Agents pharmacology, Anti-Bacterial Agents chemistry, Bacterial Proteins antagonists & inhibitors, Bacterial Proteins metabolism, Drug Resistance, Multiple, Bacterial drug effects

Abstract

Multidrug-resistant Acinetobacter baumannii is a serious threat pathogen rapidly spreading in clinics and causing a range of complicated human infections. The major contributor to A. baumannii antibiotic resistance is the overproduction of AdeIJK and AdeABC multidrug efflux pumps of the resistance-nodulation-division (RND) superfamily of proteins. The dominant role of efflux in antibiotic resistance and the relatively high permeability of the A. baumannii outer membrane to amphiphilic compounds make this pathogen a promising target for the discovery of clinically relevant efflux pump inhibitors. In this study, we identified 4,6-diaminoquoniline analogs with inhibitory activities against A. baumannii AdeIJK efflux pump and followed up on these compounds with a focused synthetic program to improve the target specificity and to reduce cytotoxicity. We identified several candidates that potentiate antibacterial activities of antibiotics erythromycin, tetracycline, and novobiocin not only in the laboratory antibiotic susceptible strain A. baumannii ATCC17978 but also in multidrug-resistant clinical isolates AB5075 and AYE. The best analogs potentiated the activities of antibiotics in low micromolar concentrations, did not have antibacterial activities on their own, inhibited AdeIJK-mediated efflux of its fluorescent substrate ethidium ion, and had low cytotoxicity in A549 human lung epithelial cells.

Published

2024

4. Predicting permeation of compounds across the outer membrane of P. aeruginosa using molecular descriptors.

Author

Manrique PD, Leus IV, López CA, Mehla J, Malloci G, Gervasoni S, Vargiu AV, Kinthada RK, Herndon L, Hengartner NW, Walker JK, Rybenkov VV, Ruggerone P, Zgurskaya HI, and Gnanakaran S

Abstract

The ability Gram-negative pathogens have at adapting and protecting themselves against antibiotics has increasingly become a public health threat. Data-driven models identifying molecular properties that correlate with outer membrane (OM) permeation and growth inhibition while avoiding efflux could guide the discovery of novel classes of antibiotics. Here we evaluate 174 molecular descriptors in 1260 antimicrobial compounds and study their correlations with antibacterial activity in Gram-negative Pseudomonas aeruginosa. The descriptors are derived from traditional approaches quantifying the compounds' intrinsic physicochemical properties, together with, bacterium-specific from ensemble docking of compounds targeting specific MexB binding pockets, and all-atom molecular dynamics simulations in different subregions of the OM model. Using these descriptors and the measured inhibitory concentrations, we design a statistical protocol to identify predictors of OM permeation/inhibition. We find consistent rules across most of our data highlighting the role of the interaction between the compounds and the OM. An implementation of the rules uncovered in our study is shown, and it demonstrates the accuracy of our approach in a set of previously unseen compounds. Our analysis sheds new light on the key properties drug candidates need to effectively permeate/inhibit P. aeruginosa, and opens the gate to similar data-driven studies in other Gram-negative pathogens., (© 2024. The Author(s).)

Published

2024

5. Inhibition of the C1s Protease and the Classical Complement Pathway by 6-(4-Phenylpiperazin-1-yl)Pyridine-3-Carboximidamide and Chemical Analogs.

Author

Xu X, Herdendorf TJ, Duan H, Rohlik DL, Roy S, Zhou H, Alkhateeb H, Khandelwal S, Zhou Q, Li P, Arepally GM, Walker JK, Garcia BL, and Geisbrecht BV

Subjects

Animals, Sheep, Peptide Hydrolases, Complement C1 metabolism, Endopeptidases, Pyridines pharmacology, Complement Pathway, Classical, Complement C1s

Abstract

The classical pathway (CP) is a potent mechanism for initiating complement activity and is a driver of pathology in many complement-mediated diseases. The CP is initiated via activation of complement component C1, which consists of the pattern recognition molecule C1q bound to a tetrameric assembly of proteases C1r and C1s. Enzymatically active C1s provides the catalytic basis for cleavage of the downstream CP components, C4 and C2, and is therefore an attractive target for therapeutic intervention in CP-driven diseases. Although an anti-C1s mAb has been Food and Drug Administration approved, identifying small-molecule C1s inhibitors remains a priority. In this study, we describe 6-(4-phenylpiperazin-1-yl)pyridine-3-carboximidamide (A1) as a selective, competitive inhibitor of C1s. A1 was identified through a virtual screen for small molecules that interact with the C1s substrate recognition site. Subsequent functional studies revealed that A1 dose-dependently inhibits CP activation by heparin-induced immune complexes, CP-driven lysis of Ab-sensitized sheep erythrocytes, CP activation in a pathway-specific ELISA, and cleavage of C2 by C1s. Biochemical experiments demonstrated that A1 binds directly to C1s with a Kd of ∼9.8 μM and competitively inhibits its activity with an inhibition constant (Ki) of ∼5.8 μM. A 1.8-Å-resolution crystal structure revealed the physical basis for C1s inhibition by A1 and provided information on the structure-activity relationship of the A1 scaffold, which was supported by evaluating a panel of A1 analogs. Taken together, our work identifies A1 as a new class of small-molecule C1s inhibitor and lays the foundation for development of increasingly potent and selective A1 analogs for both research and therapeutic purposes., (Copyright © 2024 by The American Association of Immunologists, Inc.)

Published

2024

6. A Synthetic ERR Agonist Alleviates Metabolic Syndrome.

Author

Billon C, Schoepke E, Avdagic A, Chatterjee A, Butler AA, Elgendy B, Walker JK, and Burris TP

Subjects

Mice, Animals, Obesity drug therapy, Obesity metabolism, Energy Metabolism, Receptors, Cytoplasmic and Nuclear, ERRalpha Estrogen-Related Receptor, Estrogens, Metabolic Syndrome drug therapy, Insulin Resistance

Abstract

Physical exercise induces physiologic adaptations and is effective at reducing the risk of premature death from all causes. Pharmacological exercise mimetics may be effective in the treatment of a range of diseases including obesity and metabolic syndrome. Previously, we described the development of SLU-PP-332, an agonist for the estrogen-related receptor (ERR) α , β, and γ nuclear receptors that activates an acute aerobic exercise program. Here we examine the effects of this exercise mimetic in mouse models of obesity and metabolic syndrome. Diet-induced obese or ob/ob mice were administered SLU-PP-332, and the effects on a range of metabolic parameters were assessed. SLU-PP-332 administration mimics exercise-induced benefits on whole-body metabolism in mice including increased energy expenditure and fatty acid oxidation. These effects were accompanied by decreased fat mass accumulation. Additionally, the ERR agonist effectively reduced obesity and improved insulin sensitivity in models of metabolic syndrome. Pharmacological activation of ERR may be an effective method to treat metabolic syndrome and obesity. SIGNIFICANCE STATEMENT: An estrogen receptor-related orphan receptor agonist, SLU-PP-332, with exercise mimetic activity, holds promise as a therapeutic to treat metabolic diseases by decreasing fat mass in mouse models of obesity., (Copyright © 2024 by The American Society for Pharmacology and Experimental Therapeutics.)

Published

2024

7. Novel Pan-ERR Agonists Ameliorate Heart Failure Through Enhancing Cardiac Fatty Acid Metabolism and Mitochondrial Function.

Author

Xu W, Billon C, Li H, Wilderman A, Qi L, Graves A, Rideb JRDC, Zhao Y, Hayes M, Yu K, Losby M, Hampton CS, Adeyemi CM, Hong SJ, Nasiotis E, Fu C, Oh TG, Fan W, Downes M, Welch RD, Evans RM, Milosavljevic A, Walker JK, Jensen BC, Pei L, Burris T, and Zhang L

Subjects

Mice, Animals, Cardiomegaly metabolism, Mitochondria metabolism, Myocytes, Cardiac metabolism, Receptors, Estrogen genetics, Receptors, Estrogen metabolism, Fatty Acids metabolism, Heart Failure

Abstract

Background: Cardiac metabolic dysfunction is a hallmark of heart failure (HF). Estrogen-related receptors ERRα and ERRγ are essential regulators of cardiac metabolism. Therefore, activation of ERR could be a potential therapeutic intervention for HF. However, in vivo studies demonstrating the potential usefulness of ERR agonist for HF treatment are lacking, because compounds with pharmacokinetics appropriate for in vivo use have not been available., Methods: Using a structure-based design approach, we designed and synthesized 2 structurally distinct pan-ERR agonists, SLU-PP-332 and SLU-PP-915. We investigated the effect of ERR agonist on cardiac function in a pressure overload-induced HF model in vivo. We conducted comprehensive functional, multi-omics (RNA sequencing and metabolomics studies), and genetic dependency studies both in vivo and in vitro to dissect the molecular mechanism, ERR isoform dependency, and target specificity., Results: Both SLU-PP-332 and SLU-PP-915 significantly improved ejection fraction, ameliorated fibrosis, and increased survival associated with pressure overload-induced HF without affecting cardiac hypertrophy. A broad spectrum of metabolic genes was transcriptionally activated by ERR agonists, particularly genes involved in fatty acid metabolism and mitochondrial function. Metabolomics analysis showed substantial normalization of metabolic profiles in fatty acid/lipid and tricarboxylic acid/oxidative phosphorylation metabolites in the mouse heart with 6-week pressure overload. ERR agonists increase mitochondria oxidative capacity and fatty acid use in vitro and in vivo. Using both in vitro and in vivo genetic dependency experiments, we show that ERRγ is the main mediator of ERR agonism-induced transcriptional regulation and cardioprotection and definitively demonstrated target specificity. ERR agonism also led to downregulation of cell cycle and development pathways, which was partially mediated by E2F1 in cardiomyocytes., Conclusions: ERR agonists maintain oxidative metabolism, which confers cardiac protection against pressure overload-induced HF in vivo. Our results provide direct pharmacologic evidence supporting the further development of ERR agonists as novel HF therapeutics., Competing Interests: Disclosures Dr Zhang is a cofounder of and consultant for Pelagos Pharmaceuticals Inc. The other authors report no conflicts of interest.

Published

2024

8. Estrogen-Related Receptor Agonism Reverses Mitochondrial Dysfunction and Inflammation in the Aging Kidney.

Author

Wang XX, Myakala K, Libby AE, Krawczyk E, Panov J, Jones BA, Bhasin K, Shults N, Qi Y, Krausz KW, Zerfas PM, Takahashi S, Daneshpajouhnejad P, Titievsky A, Taranenko E, Billon C, Chatterjee A, Elgendy B, Walker JK, Albanese C, Kopp JB, Rosenberg AZ, Gonzalez FJ, Guha U, Brodsky L, Burris TP, and Levi M

Subjects

Mice, Humans, Animals, Aged, Infant, Infant, Newborn, Estrogens metabolism, Mitochondria metabolism, Cytokines metabolism, Peroxisome Proliferator-Activated Receptor Gamma Coactivator 1-alpha metabolism, Kidney metabolism, Inflammation metabolism

Abstract

A gradual decline in renal function occurs even in healthy aging individuals. In addition to aging, per se, concurrent metabolic syndrome and hypertension, which are common in the aging population, can induce mitochondrial dysfunction and inflammation, which collectively contribute to age-related kidney dysfunction and disease. This study examined the role of the nuclear hormone receptors, the estrogen-related receptors (ERRs), in regulation of age-related mitochondrial dysfunction and inflammation. The ERRs were decreased in both aging human and mouse kidneys and were preserved in aging mice with lifelong caloric restriction (CR). A pan-ERR agonist, SLU-PP-332, was used to treat 21-month-old mice for 8 weeks. In addition, 21-month-old mice were treated with a stimulator of interferon genes (STING) inhibitor, C-176, for 3 weeks. Remarkably, similar to CR, an 8-week treatment with a pan-ERR agonist reversed the age-related increases in albuminuria, podocyte loss, mitochondrial dysfunction, and inflammatory cytokines, via the cyclic GMP-AMP synthase-STING and STAT3 signaling pathways. A 3-week treatment of 21-month-old mice with a STING inhibitor reversed the increases in inflammatory cytokines and the senescence marker, p21/cyclin dependent kinase inhibitor 1A (Cdkn1a), but also unexpectedly reversed the age-related decreases in PPARG coactivator (PGC)-1α, ERRα, mitochondrial complexes, and medium chain acyl coenzyme A dehydrogenase (MCAD) expression. These studies identified ERRs as CR mimetics and as important modulators of age-related mitochondrial dysfunction and inflammation. These findings highlight novel druggable pathways that can be further evaluated to prevent progression of age-related kidney disease., Competing Interests: Disclosure Statement None declared., (Copyright © 2023 American Society for Investigative Pathology. Published by Elsevier Inc. All rights reserved.)

Published

2023

9. International Union of Basic and Clinical Pharmacology CXIII: Nuclear Receptor Superfamily-Update 2023.

Author

Burris TP, de Vera IMS, Cote I, Flaveny CA, Wanninayake US, Chatterjee A, Walker JK, Steinauer N, Zhang J, Coons LA, Korach KS, Cain DW, Hollenberg AN, Webb P, Forrest D, Jetten AM, Edwards DP, Grimm SL, Hartig S, Lange CA, Richer JK, Sartorius CA, Tetel M, Billon C, Elgendy B, Hegazy L, Griffett K, Peinetti N, Burnstein KL, Hughes TS, Sitaula S, Stayrook KR, Culver A, Murray MH, Finck BN, and Cidlowski JA

Subjects

Humans, Receptors, Cytoplasmic and Nuclear metabolism, Transcription Factors metabolism, Carrier Proteins, Ligands, Pharmacology, Clinical

Abstract

The NR superfamily comprises 48 transcription factors in humans that control a plethora of gene network programs involved in a wide range of physiologic processes. This review will summarize and discuss recent progress in NR biology and drug development derived from integrating various approaches, including biophysical techniques, structural studies, and translational investigation. We also highlight how defective NR signaling results in various diseases and disorders and how NRs can be targeted for therapeutic intervention via modulation via binding to synthetic lipophilic ligands. Furthermore, we also review recent studies that improved our understanding of NR structure and signaling. SIGNIFICANCE STATEMENT: Nuclear receptors (NRs) are ligand-regulated transcription factors that are critical regulators of myriad physiological processes. NRs serve as receptors for an array of drugs, and in this review, we provide an update on recent research into the roles of these drug targets., (U.S. Government work not protected by U.S. copyright.)

Published

2023

10. Development and pharmacological evaluation of a new chemical series of potent pan-ERR agonists, identification of SLU-PP-915.

Author

Hampton CS, Sitaula S, Billon C, Haynes K, Avdagic A, Wanninayake U, Adeyemi CM, Chatterjee A, Griffett K, Banerjee S, Burris SL, Schoepke E, Boehm T, Bess A, de Vera IMS, Burris TP, and Walker JK

Subjects

Protein Isoforms, Estrogens

Abstract

Estrogen-related receptors (ERR) are an orphan nuclear receptor sub-family that play a critical role in regulating gene transcription for several physiological processes including mitochondrial function, cellular energy utilization and homeostasis. They have also been implicated to play a role in several pathological conditions. Herein, we report the identification, synthesis, structure-activity relationships and pharmacological evaluation of a new chemical series of potent pan-ERR agonists. This template was designed for ERRγ starting from the known acyl hydrazide template and compounds such as agonist GSK-4716 employing a structure-based drug design approach. This led to the preparation of a series of 2,5-disubstituted thiophenes from which several were found to be potent agonists of ERRγ in cell-based co-transfection assays. Additionally, direct binding to ERRγ was established through 1 H NMR protein-ligand binding experiments. Compound optimization revealed that the phenolic or aniline groups could be replaced with a boronic acid moiety, which was able to maintain activity and demonstrated improved metabolic stability in microsomal in vitro assays. Further pharmacological evaluation of these compounds showed that they had roughly equivalent agonist activity on ERR isoforms α and β representing an ERR pan-agonist profile. One potent agonist, SLU-PP-915 (10s), which contained a boronic acid moiety was profiled in gene expression assays and found to significantly upregulate the expression of ERR target genes such as peroxisome-proliferator activated receptor γ co-activators-1α, lactate dehydrogenase A, DNA damage inducible transcript 4 and pyruvate dehydrogenase kinase 4 both in vitro and in vivo., Competing Interests: Declaration of competing interest The authors declare the following financial interests/personal relationships which may be considered as potential competing interests:John K Walker reports financial support was provided by National Institutes of Health. Thomas P. Burris reports financial support was provided by National Institutes of Health. John K. Walker has patent #WO2019036562; Heteroaromatics as ERR inverse agonists and their preparation licensed to Myonid Therapeutics. Thomas P. Burris has patent #WO2019036562; Heteroaromatics as ERR inverse agonists and their preparation licensed to Myonid Therapeutics. Carissa Hampton has patent #WO2019036562; Heteroaromatics as ERR inverse agonists and their preparation licensed to Myonid Therapeutics. Keith Haynes has patent #WO2019036562; Heteroaromatics as ERR inverse agonists and their preparation licensed to Myonid Therapeutics. Kristine Griffett has patent #WO2019036562; Heteroaromatics as ERR inverse agonists and their preparation licensed to Myonid Therapeutics. Cyrielle Billon has patent #WO2019036562; Heteroaromatics as ERR inverse agonists and their preparation licensed to Myonid Therapeutics. Sadichha Situala has patent #WO2019036562; Heteroaromatics as ERR inverse agonists and their preparation licensed to Myonid Therapeutics. Founders in Myonid Therapeutics which is trying to develop ERR modulators as novel therapeutics (J.K.W. & T.P.B), (Copyright © 2023 Elsevier Masson SAS. All rights reserved.)

Published

2023

11. Identification and structure-activity relationships for a series of N, N-disubstituted 2-aminobenzothiazoles as potent inhibitors of S. aureus.

Author

Cao F, Kinthada R, Boehm T, D' Cunha N, Leus IV, Orth C, Zgurskaya HI, and Walker JK

Subjects

Microbial Sensitivity Tests, Anti-Bacterial Agents pharmacology, Anti-Bacterial Agents chemistry, Structure-Activity Relationship, Bacteria, Escherichia coli, Bacterial Proteins, Staphylococcus aureus, Methicillin-Resistant Staphylococcus aureus

Abstract

An internal collection of commercial and synthetically derived small molecule compounds was screened against several drug-resistant bacterial pathogens. Compound 1, a known N, N-disubstituted 2-aminobenzothiazole, was found to be a potent inhibitor of Staphylococcus aureus and several associated clinically relevant strains of methicillin-resistant S. aureus suggesting a possible novel mechanism of inhibition. It failed to show activity in any of the Gram-negative pathogens it was tested in. Evaluation in Escherichia coli BW25113 and Pseudomonas aeruginosa PAO1, as well as in their respective hyperporinated and efflux pump-deletion mutants revealed that activity in Gram-negative bacteria is diminished because this benzothiazole scaffold is a substrate for bacterial efflux pumps. Several analogs of 1 were synthesized to generate basic structure-activity relationships for the scaffold which highlighted that the N-propyl imidazole moiety was critical for the observed antibacterial activity., Competing Interests: Declaration of Competing Interest The authors declare the following financial interests/personal relationships which may be considered as potential competing interests: Some authors are inventors on a composition of matter patent that cover several of the compounds described here., (Copyright © 2023 Elsevier Ltd. All rights reserved.)

Published

2023

12. Synthetic ERRα/β/γ Agonist Induces an ERRα-Dependent Acute Aerobic Exercise Response and Enhances Exercise Capacity.

Author

Billon C, Sitaula S, Banerjee S, Welch R, Elgendy B, Hegazy L, Oh TG, Kazantzis M, Chatterjee A, Chrivia J, Hayes ME, Xu W, Hamilton A, Huss JM, Zhang L, Walker JK, Downes M, Evans RM, and Burris TP

Subjects

Animals, Mice, Muscle Fibers, Skeletal metabolism, Muscle, Skeletal metabolism, ERRalpha Estrogen-Related Receptor, Exercise Tolerance drug effects, Receptors, Estrogen drug effects, Receptors, Estrogen metabolism, Estrogens chemistry, Estrogens pharmacology

Abstract

Repetitive physical exercise induces physiological adaptations in skeletal muscle that improves exercise performance and is effective for the prevention and treatment of several diseases. Genetic evidence indicates that the orphan nuclear receptors estrogen receptor-related receptors (ERRs) play an important role in skeletal muscle exercise capacity. Three ERR subtypes exist (ERRα, β, and γ), and although ERRβ/γ agonists have been designed, there have been significant difficulties in designing compounds with ERRα agonist activity. Additionally, there are limited synthetic agonists that can be used to target ERRs in vivo . Here, we report the identification of a synthetic ERR pan agonist, SLU-PP-332, that targets all three ERRs but has the highest potency for ERRα. Additionally, SLU-PP-332 has sufficient pharmacokinetic properties to be used as an in vivo chemical tool. SLU-PP-332 increases mitochondrial function and cellular respiration in a skeletal muscle cell line. When administered to mice, SLU-PP-332 increased the type IIa oxidative skeletal muscle fibers and enhanced exercise endurance. We also observed that SLU-PP-332 induced an ERRα-specific acute aerobic exercise genetic program, and the ERRα activation was critical for enhancing exercise endurance in mice. These data indicate the feasibility of targeting ERRα for the development of compounds that act as exercise mimetics that may be effective in the treatment of numerous metabolic disorders and to improve muscle function in the aging.

Published

2023

13. Structural basis of synthetic agonist activation of the nuclear receptor REV-ERB.

Author

Murray MH, Valfort AC, Koelblen T, Ronin C, Ciesielski F, Chatterjee A, Veerakanellore GB, Elgendy B, Walker JK, Hegazy L, and Burris TP

Subjects

Heme metabolism, Ligands, Nuclear Receptor Subfamily 1, Group D, Member 1 genetics, Porphyrins pharmacology

Abstract

The nuclear receptor REV-ERB plays an important role in a range of physiological processes. REV-ERB behaves as a ligand-dependent transcriptional repressor and heme has been identified as a physiological agonist. Our current understanding of how ligands bind to and regulate transcriptional repression by REV-ERB is based on the structure of heme bound to REV-ERB. However, porphyrin (heme) analogues have been avoided as a source of synthetic agonists due to the wide range of heme binding proteins and potential pleotropic effects. How non-porphyrin synthetic agonists bind to and regulate REV-ERB has not yet been defined. Here, we characterize a high affinity synthetic REV-ERB agonist, STL1267, and describe its mechanism of binding to REV-ERB as well as the method by which it recruits transcriptional corepressor both of which are unique and distinct from that of heme-bound REV-ERB., (© 2022. The Author(s).)

Published

2022

14. Analysis of Orthogonal Efflux and Permeation Properties of Compounds Leads to the Discovery of New Efflux Pump Inhibitors.

Author

Moniruzzaman M, Cooper CJ, Uddin MR, Walker JK, Parks JM, and Zgurskaya HI

Subjects

Amines, Anti-Bacterial Agents chemistry, Anti-Bacterial Agents pharmacology, Porins, Escherichia coli, Membrane Transport Proteins chemistry

Abstract

Optimization of compound permeation into Gram-negative bacteria is one of the most challenging tasks in the development of antibacterial agents. Two permeability barriers─the passive diffusion barrier of the outer membrane (OM) and active drug efflux─act synergistically to protect cells from the antibacterial action of compounds. In Escherichia coli ( E. coli ) and relatives, these two barriers sieve compounds based on different physicochemical properties that are defined by their interactions with OM porins and efflux pumps, respectively. In this study, we critically tested the hypothesis that the best substrates and inhibitors of efflux pumps are compounds that can effectively permeate the OM and are available at relatively high concentrations in the periplasm. For this purpose, we filtered a large subset of the ZINC15 database of commercially available compounds for compounds containing a primary amine, a chemical feature known to facilitate the uptake through E. coli general porins. The assembled library was screened by ensemble docking to AcrA, the periplasmic component of the AcrAB-TolC efflux pump, followed by experimental testing of the top predicted binders for antibacterial activities, efflux recognition, and inhibition. We found that the filtered primary amine library is a rich source of compounds with efflux-inhibiting activities and identified efflux pump inhibitors with novel chemical scaffolds effective against E. coli AcrAB-TolC and efflux pumps of multidrug-resistant clinical isolates of Acinetobacter baumannii . However, primary amines are not required for the recognition of compounds by efflux pumps and their efflux-inhibitory activities.

Published

2022

15. Mechanistic Duality of Bacterial Efflux Substrates and Inhibitors: Example of Simple Substituted Cinnamoyl and Naphthyl Amides.

Author

D'Cunha N, Moniruzzaman M, Haynes K, Malloci G, Cooper CJ, Margiotta E, Vargiu AV, Uddin MR, Leus IV, Cao F, Parks JM, Rybenkov VV, Ruggerone P, Zgurskaya HI, and Walker JK

Subjects

Amides pharmacology, Escherichia coli genetics, Escherichia coli metabolism, Humans, Molecular Docking Simulation, Multidrug Resistance-Associated Proteins genetics, Escherichia coli Proteins genetics, Escherichia coli Proteins metabolism

Abstract

Antibiotic resistance poses an immediate and growing threat to human health. Multidrug efflux pumps are promising targets for overcoming antibiotic resistance with small-molecule therapeutics. Previously, we identified a diaminoquinoline acrylamide, NSC-33353, as a potent inhibitor of the AcrAB-TolC efflux pump in Escherichia coli . This inhibitor potentiates the antibacterial activities of novobiocin and erythromycin upon binding to the membrane fusion protein AcrA. It is also a substrate for efflux and lacks appreciable intrinsic antibacterial activity of its own in wild-type cells. Here, we have modified the substituents of the cinnamoyl group of NSC-33353, giving rise to analogs that retain the ability to inhibit efflux, lost the features of the efflux substrates, and gained antibacterial activity in wild-type cells. The replacement of the cinnamoyl group with naphthyl isosteres generated compounds that lack antibacterial activity but are both excellent efflux pump inhibitors and substrates. Surprisingly, these inhibitors potentiate the antibacterial activity of novobiocin but not erythromycin. Surface plasmon resonance experiments and molecular docking suggest that the replacement of the cinnamoyl group with naphthyl shifts the affinity of the compounds away from AcrA to the AcrB transporter, making them better efflux substrates and changing their mechanism of inhibition. These results provide new insights into the duality of efflux substrate/inhibitor features in chemical scaffolds that will facilitate the development of new efflux pump inhibitors.

Published

2021

16. A Repurposed Drug Screen Identifies Compounds That Inhibit the Binding of the COVID-19 Spike Protein to ACE2.

Author

Tsegay KB, Adeyemi CM, Gniffke EP, Sather DN, Walker JK, and Smith SEP

Abstract

Repurposed drugs that block the interaction between the SARS-CoV-2 spike protein and its receptor ACE2 could offer a rapid route to novel COVID-19 treatments or prophylactics. Here, we screened 2,701 compounds from a commercial library of drugs approved by international regulatory agencies for their ability to inhibit the binding of recombinant, trimeric SARS-CoV-2 spike protein to recombinant human ACE2. We identified 56 compounds that inhibited binding in a concentration-dependent manner, measured the IC 50 of binding inhibition, and computationally modeled the docking of the best inhibitors to the Spike-ACE2 binding interface. The best candidates were Thiostrepton, Oxytocin, Nilotinib, and Hydroxycamptothecin with IC50's in the 4-9 μM range. These results highlight an effective screening approach to identify compounds capable of disrupting the Spike-ACE2 interaction, as well as identify several potential inhibitors of the Spike-ACE2 interaction., Competing Interests: Seattle Children’s Research Institute has filed a provisional patent on the use of the inhibition assay for drug screening described herein., (Copyright © 2021 Tsegay, Adeyemi, Gniffke, Sather, Walker and Smith.)

Published

2021

17. A repurposed drug screen identifies compounds that inhibit the binding of the COVID-19 spike protein to ACE2.

Author

Tsegay KB, Adeyemi CM, Gniffke EP, Sather DN, Walker JK, and Smith SEP

Abstract

Repurposed drugs that block the interaction between the SARS-CoV-2 spike protein and its receptor ACE2 could offer a rapid route to novel COVID-19 treatments or prophylactics. Here, we screened 2701 compounds from a commercial library of drugs approved by international regulatory agencies for their ability to inhibit the binding of recombinant, trimeric SARS-CoV-2 spike protein to recombinant human ACE2. We identified 56 compounds that inhibited binding by <90%, measured the EC 50 of binding inhibition, and computationally modeled the docking of the best inhibitors to both Spike and ACE2. These results highlight an effective screening approach to identify compounds capable of disrupting the Spike-ACE2 interaction as well as identifying several potential inhibitors that could serve as templates for future drug discovery efforts.

Published

2021

18. Multidrug Efflux Pumps and the Two-Faced Janus of Substrates and Inhibitors.

Author

Zgurskaya HI, Walker JK, Parks JM, and Rybenkov VV

Subjects

ATP-Binding Cassette Transporters antagonists & inhibitors, ATP-Binding Cassette Transporters metabolism, Anti-Bacterial Agents metabolism, Anti-Bacterial Agents pharmacology, Bacterial Outer Membrane metabolism, Fluoroquinolones chemistry, Fluoroquinolones metabolism, Fluoroquinolones pharmacology, Gram-Negative Bacteria drug effects, Gram-Negative Bacteria metabolism, Gram-Positive Bacteria drug effects, Membrane Transport Proteins chemistry, Microbial Sensitivity Tests, Anti-Bacterial Agents chemistry, Membrane Transport Proteins metabolism

Abstract

Antibiotics are miracle drugs that can cure infectious bacterial diseases. However, their utility is challenged by antibiotic-resistant bacteria emerging in clinics and straining modern medicine and our ways of life. Certain bacteria such as Gram-negative (Gram(-)) and Mycobacteriales species are intrinsically resistant to most clinical antibiotics and can further gain multidrug resistance through mutations and plasmid acquisition. These species stand out by the presence of an additional external lipidic membrane, the outer membrane (OM), that is composed of unique glycolipids. Although formidable, the OM is a passive permeability barrier that can reduce penetration of antibiotics but cannot affect intracellular steady-state concentrations of drugs. The two-membrane envelopes are further reinforced by active efflux transporters that expel antibiotics from cells against their concentration gradients. The major mechanism of antibiotic resistance in Gram(-) pathogens is the active efflux of drugs, which acts synergistically with the low permeability barrier of the OM and other mutational and plasmid-borne mechanisms of antibiotic resistance.The synergy between active efflux and slow uptake offers Gram(-) bacteria an impressive degree of protection from potentially harmful chemicals, but it is also their Achilles heel. Kinetic studies have revealed that even small changes in the efficiency of either of the two factors can have dramatic effects on drug penetration into the cell. In line with these expectations, two major approaches to overcome this antibiotic resistance mechanism are currently being explored: (1) facilitation of antibiotic penetration across the outer membranes and (2) avoidance and inhibition of clinically relevant multidrug efflux pumps. Herein we summarize the progress in the latter approach with a focus on efflux pumps from the resistance-nodulation-division (RND) superfamily. The ability to export various substrates across the OM at the expense of the proton-motive force acting on the inner membrane and the engagement of accessory proteins for their functions are the major mechanistic advantages of these pumps. Both the RND transporters and their accessory proteins are being targeted in the discovery of efflux pump inhibitors, which in combination with antibiotics can potentiate antibacterial activities. We discuss intriguing relationships between substrates and inhibitors of efflux pumps, as these two types of ligands face similar barriers and binding sites in the transporters and accessory proteins and both types of activities often occur with the same chemical scaffold. Several distinct chemical classes of efflux inhibitors have been discovered that are as structurally diverse as the substrates of efflux pumps. Recent mechanistic insights, both empirical and computational, have led to the identification of features that distinguish OM permeators and efflux pump avoiders as well as efflux inhibitors from substrates. These findings suggest a path forward for optimizing the OM permeation and efflux-inhibitory activities in antibiotics and other chemically diverse compounds.

Published

2021

19. Predictive Rules of Efflux Inhibition and Avoidance in Pseudomonas aeruginosa.

Author

Mehla J, Malloci G, Mansbach R, López CA, Tsivkovski R, Haynes K, Leus IV, Grindstaff SB, Cascella RH, D'Cunha N, Herndon L, Hengartner NW, Margiotta E, Atzori A, Vargiu AV, Manrique PD, Walker JK, Lomovskaya O, Ruggerone P, Gnanakaran S, Rybenkov VV, and Zgurskaya HI

Subjects

Anti-Bacterial Agents chemical synthesis, Anti-Bacterial Agents metabolism, Bacterial Outer Membrane Proteins antagonists & inhibitors, Bacterial Outer Membrane Proteins genetics, Bacterial Outer Membrane Proteins metabolism, Binding Sites, Biological Transport drug effects, Gene Expression, Kinetics, Membrane Transport Proteins genetics, Membrane Transport Proteins metabolism, Microbial Sensitivity Tests, Models, Molecular, Peptidomimetics chemical synthesis, Peptidomimetics metabolism, Principal Component Analysis, Protein Binding, Protein Conformation, alpha-Helical, Protein Conformation, beta-Strand, Protein Interaction Domains and Motifs, Pseudomonas aeruginosa genetics, Pseudomonas aeruginosa metabolism, Structure-Activity Relationship, Thermodynamics, Anti-Bacterial Agents pharmacology, Bacterial Outer Membrane Proteins chemistry, Drug Resistance, Multiple, Bacterial drug effects, Membrane Transport Proteins chemistry, Models, Biological, Peptidomimetics pharmacology, Pseudomonas aeruginosa drug effects

Abstract

Antibiotic-resistant bacteria rapidly spread in clinical and natural environments and challenge our modern lifestyle. A major component of defense against antibiotics in Gram-negative bacteria is a drug permeation barrier created by active efflux across the outer membrane. We identified molecular determinants defining the propensity of small peptidomimetic molecules to avoid and inhibit efflux pumps in Pseudomonas aeruginosa , a human pathogen notorious for its antibiotic resistance. Combining experimental and computational protocols, we mapped the fate of the compounds from structure-activity relationships through their dynamic behavior in solution, permeation across both the inner and outer membranes, and interaction with MexB, the major efflux transporter of P. aeruginosa We identified predictors of efflux avoidance and inhibition and demonstrated their power by using a library of traditional antibiotics and compound series and by generating new inhibitors of MexB. The identified predictors will enable the discovery and optimization of antibacterial agents suitable for treatment of P. aeruginosa infections. IMPORTANCE Efflux pump avoidance and inhibition are desired properties for the optimization of antibacterial activities against Gram-negative bacteria. However, molecular and physicochemical interactions defining the interface between compounds and efflux pumps remain poorly understood. We identified properties that correlate with efflux avoidance and inhibition, are predictive of similar features in structurally diverse compounds, and allow researchers to distinguish between efflux substrates, inhibitors, and avoiders in P. aeruginosa The developed predictive models are based on the descriptors representative of different clusters comprising a physically intuitive combination of properties. Molecular shape (represented by acylindricity), amphiphilicity (anisotropic polarizability), aromaticity (number of aromatic rings), and the partition coefficient (LogD) are physicochemical predictors of efflux inhibitors, whereas interactions with Pro668 and Leu674 residues of MexB distinguish between inhibitors/substrates and efflux avoiders. The predictive models and efflux rules are applicable to compounds with unrelated chemical scaffolds and pave the way for development of compounds with the desired efflux interface properties., (Copyright © 2021 Mehla et al.)

Published

2021

20. GPR183-Oxysterol Axis in Spinal Cord Contributes to Neuropathic Pain.

Author

Braden, Giancotti LA, Chen Z, DeLeon C, Latzo N, Boehn T, D'Cunha N, Thompson BM, Doyle TM, McDonald JG, Walker JK, Kolar GR, Arnatt CK, and Salvemini D

Subjects

Animals, Female, HL-60 Cells, Humans, Male, Mice, Neuralgia drug therapy, Neuralgia pathology, Receptors, G-Protein-Coupled antagonists & inhibitors, Signal Transduction, Spinal Cord pathology, Neuralgia metabolism, Oxysterols metabolism, Receptors, G-Protein-Coupled metabolism, Spinal Cord metabolism

Abstract

Neuropathic pain is a debilitating public health concern for which novel non-narcotic therapeutic targets are desperately needed. Using unbiased transcriptomic screening of the dorsal horn spinal cord after nerve injury we have identified that Gpr183 (Epstein-Barr virus-induced gene 2) is upregulated after chronic constriction injury (CCI) in rats. GPR183 is a chemotactic receptor known for its role in the maturation of B cells, and the endogenous ligand is the oxysterol 7 α ,25-dihydroxycholesterol (7 α ,25-OHC). The role of GPR183 in the central nervous system is not well characterized, and its role in pain is unknown. The profile of commercially available probes for GPR183 limits their use as pharmacological tools to dissect the roles of this receptor in pathophysiological settings. Using in silico modeling, we have screened a library of 5 million compounds to identify several novel small-molecule antagonists of GPR183 with nanomolar potency. These compounds are able to antagonize 7 α ,25-OHC-induced calcium mobilization in vitro with IC 50 values below 50 nM. In vivo intrathecal injections of these antagonists during peak pain after CCI surgery reversed allodynia in male and female mice. Acute intrathecal injection of the GPR183 ligand 7 α ,25-OHC in naïve mice induced dose-dependent allodynia. Importantly, this effect was blocked using our novel GPR183 antagonists, suggesting spinal GPR183 activation as pronociceptive. These studies are the first to reveal a role for GPR183 in neuropathic pain and identify this receptor as a potential target for therapeutic intervention. SIGNIFICANCE STATEMENT: We have identified several novel GPR183 antagonists with nanomolar potency. Using these antagonists, we have demonstrated that GPR183 signaling in the spinal cord is pronociceptive. These studies are the first to reveal a role for GPR183 in neuropathic pain and identify it as a potential target for therapeutic intervention., (Copyright © 2020 by The American Society for Pharmacology and Experimental Therapeutics.)

Published

2020

21. A Selective ERRα/γ Inverse Agonist, SLU-PP-1072, Inhibits the Warburg Effect and Induces Apoptosis in Prostate Cancer Cells.

Author

Schoepke E, Billon C, Haynes KM, Avdagic A, Sitaula S, Sanders R, Adeyemi CM, Walker JK, and Burris TP

Subjects

Antineoplastic Agents chemical synthesis, Benzothiazoles chemical synthesis, Drug Inverse Agonism, Furans chemical synthesis, Gene Expression Regulation, Neoplastic drug effects, HEK293 Cells, Humans, PC-3 Cells, ERRalpha Estrogen-Related Receptor, Antineoplastic Agents pharmacology, Apoptosis drug effects, Benzothiazoles pharmacology, Furans pharmacology, Receptors, Estrogen antagonists & inhibitors, Warburg Effect, Oncologic drug effects

Abstract

The estrogen related receptors (ERRs) are a subgroup of nuclear receptors that play a role in regulation of cellular metabolism. Prostate cancer (PCa) cells display altered metabolic signatures, such as the Warburg effect, and the ERRs have been implicated in driving this phenotype. Despite the lack of a known endogenous ligand, synthetic ligands that target the ERRs have been discovered. For example, the ERRα inverse agonist XCT790 modulates metabolic pathways in PCa cells, but it also functions as a mitochondrial uncoupler independent of targeting ERRα. Here, we describe a novel dual ERRα/γ inverse agonist, SLU-PP-1072, derived from the GSK4716 ERRγ agonist scaffold that is distinct from the XCT790 scaffold. SLU-PP-1072 alters PCa cell metabolism and gene expression, resulting in cell cycle dysregulation and increased apoptosis without acute mitochondrial uncoupling activity. Our data suggest that inhibition of ERRα/γ may be beneficial in treatment of PCa, and SLU-PP-1072 provides a unique chemical tool to evaluate the pharmacology of ERRα and ERRγ.

Published

2020

22. Machine Learning Algorithm Identifies an Antibiotic Vocabulary for Permeating Gram-Negative Bacteria.

Author

Mansbach RA, Leus IV, Mehla J, Lopez CA, Walker JK, Rybenkov VV, Hengartner NW, Zgurskaya HI, and Gnanakaran S

Subjects

Algorithms, Gram-Negative Bacteria, Machine Learning, Pseudomonas aeruginosa, Anti-Bacterial Agents pharmacology, Vocabulary

Abstract

Drug discovery faces a crisis. The industry has used up the "obvious" space in which to find novel drugs for biomedical applications, and productivity is declining. One strategy to combat this is rational approaches to expand the search space without relying on chemical intuition, to avoid rediscovery of similar spaces. In this work, we present proof of concept of an approach to rationally identify a "chemical vocabulary" related to a specific drug activity of interest without employing known rules. We focus on the pressing concern of multidrug resistance in Pseudomonas aeruginosa by searching for submolecules that promote compound entry into this bacterium. By synergizing theory, computation, and experiment, we validate our approach, explain the molecular mechanism behind identified fragments promoting compound entry, and select candidate compounds from an external library that display good permeation ability.

Published

2020

23. Discovery of multidrug efflux pump inhibitors with a novel chemical scaffold.

Author

Green AT, Moniruzzaman M, Cooper CJ, Walker JK, Smith JC, Parks JM, and Zgurskaya HI

Subjects

Acinetobacter baumannii drug effects, Acinetobacter baumannii pathogenicity, Anti-Bacterial Agents adverse effects, Anti-Bacterial Agents pharmacology, Anti-Infective Agents chemistry, Carrier Proteins antagonists & inhibitors, Computational Biology methods, Drug Resistance, Bacterial drug effects, Drug Resistance, Bacterial genetics, Drug Synergism, Erythromycin chemistry, Erythromycin pharmacology, Escherichia coli Proteins antagonists & inhibitors, Gram-Negative Bacteria drug effects, Gram-Negative Bacteria pathogenicity, Gram-Negative Bacterial Infections microbiology, Gram-Negative Bacterial Infections pathology, Humans, Klebsiella pneumoniae, Lipoproteins antagonists & inhibitors, Molecular Docking Simulation, Multidrug Resistance-Associated Proteins antagonists & inhibitors, Novobiocin chemistry, Novobiocin pharmacology, Anti-Infective Agents pharmacology, Carrier Proteins chemistry, Escherichia coli Proteins chemistry, Gram-Negative Bacterial Infections drug therapy, Lipoproteins chemistry, Membrane Transport Proteins chemistry, Multidrug Resistance-Associated Proteins chemistry

Abstract

Multidrug efflux is a major contributor to antibiotic resistance in Gram-negative bacterial pathogens. Inhibition of multidrug efflux pumps is a promising approach for reviving the efficacy of existing antibiotics. Previously, inhibitors targeting both the efflux transporter AcrB and the membrane fusion protein AcrA in the Escherichia coli AcrAB-TolC efflux pump were identified. Here we use existing physicochemical property guidelines to generate a filtered library of compounds for computational docking. We then experimentally test the top candidate coumpounds using in vitro binding assays and in vivo potentiation assays in bacterial strains with controllable permeability barriers. We thus identify a new class of inhibitors of E. coli AcrAB-TolC. Six molecules with a shared scaffold were found to potentiate the antimicrobial activity of erythromycin and novobiocin in hyperporinated E. coli cells. Importantly, these six molecules were also active in wild-type strains of both Acinetobacter baumannii and Klebsiella pneumoniae, potentiating the activity of erythromycin and novobiocin up to 8-fold., 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 © 2020 Elsevier B.V. All rights reserved.)

Published

2020

24. Sphingosine-1-phosphate receptor 1 activation in astrocytes contributes to neuropathic pain.

Author

Chen Z, Doyle TM, Luongo L, Largent-Milnes TM, Giancotti LA, Kolar G, Squillace S, Boccella S, Walker JK, Pendleton A, Spiegel S, Neumann WL, Vanderah TW, and Salvemini D

Subjects

Animals, Drug Evaluation, Preclinical, Female, Interleukin-10 metabolism, Male, Mice, Neuralgia drug therapy, Neuralgia etiology, Rats, Sprague-Dawley, Sphingosine-1-Phosphate Receptors antagonists & inhibitors, Sulfones pharmacology, Triazoles pharmacology, Astrocytes metabolism, Neuralgia metabolism, Sphingosine-1-Phosphate Receptors metabolism, Sulfones therapeutic use, Triazoles therapeutic use

Abstract

Neuropathic pain afflicts millions of individuals and represents a major health problem for which there is limited effective and safe therapy. Emerging literature links altered sphingolipid metabolism to nociceptive processing. However, the neuropharmacology of sphingolipid signaling in the central nervous system in the context of chronic pain remains largely unexplored and controversial. We now provide evidence that sphingosine-1-phosphate (S1P) generated in the dorsal horn of the spinal cord in response to nerve injury drives neuropathic pain by selectively activating the S1P receptor subtype 1 (S1PR1) in astrocytes. Accordingly, genetic and pharmacological inhibition of S1PR1 with multiple antagonists in distinct chemical classes, but not agonists, attenuated and even reversed neuropathic pain in rodents of both sexes and in two models of traumatic nerve injury. These S1PR1 antagonists retained their ability to inhibit neuropathic pain during sustained drug administration, and their effects were independent of endogenous opioid circuits. Moreover, mice with astrocyte-specific knockout of S1pr1 did not develop neuropathic pain following nerve injury, thereby identifying astrocytes as the primary cellular substrate of S1PR1 activity. On a molecular level, the beneficial reductions in neuropathic pain resulting from S1PR1 inhibition were driven by interleukin 10 (IL-10), a potent neuroprotective and anti-inflammatory cytokine. Collectively, our results provide fundamental neurobiological insights that identify the cellular and molecular mechanisms engaged by the S1PR1 axis in neuropathic pain and establish S1PR1 as a target for therapeutic intervention with S1PR1 antagonists as a class of nonnarcotic analgesics., Competing Interests: Conflict of interest statement: D.S. is a cofounder of BioIntervene, Inc. that licensed related intellectual property from Saint Louis University.

Published

2019

25. Small Molecule Condensin Inhibitors.

Author

Zhao H, Petrushenko ZM, Walker JK, Baudry J, Zgurskaya HI, and Rybenkov VV

Subjects

Binding Sites, Chromosomal Proteins, Non-Histone genetics, Chromosomal Proteins, Non-Histone metabolism, Drug Evaluation, Preclinical, Escherichia coli genetics, Escherichia coli metabolism, Escherichia coli Proteins genetics, Escherichia coli Proteins metabolism, Isoquinolines chemistry, Isoquinolines pharmacology, Molecular Docking Simulation, Naphthalenes chemistry, Naphthalenes pharmacology, Repressor Proteins genetics, Repressor Proteins metabolism, Small Molecule Libraries pharmacology, Anti-Bacterial Agents chemistry, Anti-Bacterial Agents pharmacology, Chromosomal Proteins, Non-Histone antagonists & inhibitors, Escherichia coli drug effects, Escherichia coli Proteins antagonists & inhibitors, Repressor Proteins antagonists & inhibitors, Small Molecule Libraries chemistry

Abstract

Condensins play a unique role in orchestrating the global folding of the chromosome, an essential cellular process, and contribute to human disease and bacterial pathogenicity. As such, they represent an attractive and as yet untapped target for diverse therapeutic interventions. We describe here the discovery of small molecule inhibitors of the Escherichia coli condensin MukBEF. Pilot screening of a small diversity set revealed five compounds that inhibit the MukBEF pathway, two of which, Michellamine B and NSC260594, affected MukB directly. Computer-assisted docking suggested plausible binding sites for the two compounds in the hinge and head domains of MukB, and both binding sites were experimentally validated using mutational analysis and inspection of NSC260594 analogs. These results outline a strategy for the discovery of condensin inhibitors, identify druggable binding sites on the protein, and describe two small molecule inhibitors of condensins.

Published

2018

26. Molecular Properties That Define the Activities of Antibiotics in Escherichia coli and Pseudomonas aeruginosa.

Author

Cooper CJ, Krishnamoorthy G, Wolloscheck D, Walker JK, Rybenkov VV, Parks JM, and Zgurskaya HI

Subjects

Biological Transport, Active, Cell Membrane enzymology, Escherichia coli chemistry, Escherichia coli enzymology, Permeability, Pseudomonas aeruginosa chemistry, Pseudomonas aeruginosa enzymology, Anti-Bacterial Agents chemistry, Anti-Bacterial Agents pharmacology, Cell Membrane chemistry, Cell Membrane metabolism, Escherichia coli drug effects, Pseudomonas aeruginosa drug effects

Abstract

The permeability barrier of Gram-negative cell envelopes is the major obstacle in the discovery and development of new antibiotics. In Gram-negative bacteria, these difficulties are exacerbated by the synergistic interaction between two biochemically distinct phenomena, the low permeability of the outer membrane (OM) and active multidrug efflux. In this study, we used Pseudomonas aeruginosa and Escherichia coli strains with controllable permeability barriers, achieved through hyperporination of the OMs and varied efflux capacities, to evaluate the contributions of each of the barriers to protection from antibacterials. We analyzed antibacterial activities of β-lactams and fluoroquinolones, antibiotics that are optimized for targets in the periplasm and the cytoplasm, respectively, and performed a machine learning-based analysis to identify physicochemical descriptors that best classify their relative potencies. Our results show that the molecular properties selected by active efflux and the OM barriers are different for the two species. Antibiotic activity in P. aeruginosa was better classified by electrostatic and surface area properties, whereas topology, physical properties, and atom or bond counts best capture the behavior in E. coli. In several cases, descriptor values that correspond to active antibiotics also correspond to significant barrier effects, highlighting the synergy between the two barriers where optimizing for one barrier promotes strengthening of the other barrier. Thus, both barriers should be considered when optimizing antibiotics for favorable OM permeability, efflux evasion, or both.

Published

2018

27. The structural basis for inhibition of the classical and lectin complement pathways by S. aureus extracellular adherence protein.

Author

Woehl JL, Ramyar KX, Katz BB, Walker JK, and Geisbrecht BV

Subjects

Alanine chemistry, Alanine metabolism, Amino Acid Sequence, Amino Acid Substitution, Bacterial Proteins genetics, Bacterial Proteins metabolism, Binding Sites, Carbodiimides chemistry, Complement C4b genetics, Complement C4b metabolism, Complement Pathway, Classical, Complement Pathway, Mannose-Binding Lectin, Cross-Linking Reagents chemistry, Crystallography, X-Ray, Gene Expression, Glutamic Acid chemistry, Glutamic Acid metabolism, Host-Pathogen Interactions, Humans, Lysine metabolism, Models, Molecular, Mutation, Protein Binding, Protein Interaction Domains and Motifs, Protein Structure, Secondary, RNA-Binding Proteins genetics, RNA-Binding Proteins metabolism, Recombinant Proteins chemistry, Recombinant Proteins genetics, Recombinant Proteins metabolism, Sequence Alignment, Sequence Homology, Amino Acid, Bacterial Proteins chemistry, Complement C4b chemistry, Lysine chemistry, RNA-Binding Proteins chemistry, Staphylococcus aureus chemistry

Abstract

The extracellular adherence protein (Eap) plays a crucial role in pathogenesis and survival of Staphylococcus aureus by inhibiting the classical and lectin pathways of complement. We have previously shown that Eap binds with nanomolar affinity to complement C4b and disrupts the initial interaction between C4b and C2, thereby inhibiting formation of the classical and lectin pathway C3 pro-convertase. Although an underlying mechanism has been identified, the structural basis for Eap binding to C4b is poorly understood. Here, we show that Eap domains 3 and 4 each contain a low-affinity, but saturable binding site for C4b. Taking advantage of the high lysine content of Eap, we used a zero-length crosslinking approach to map the Eap binding site to both the α'- and γ-chains of C4b. We also probed the C4b/Eap interface through a chemical footprinting approach involving lysine modification, proteolytic digestion, and mass spectrometry. This identified seven lysines in Eap that undergo changes in solvent exposure upon C4b binding. We found that simultaneous mutation of these lysines to either alanine or glutamate diminished C4b binding and complement inhibition by Eap. Together, our results provide insight into Eap recognition of C4b, and suggest that the repeating domains that comprise Eap are capable of multiple ligand-binding modes., (© 2017 The Protein Society.)

Published

2017

28. Identification and Structure-Activity Relationships of Novel Compounds that Potentiate the Activities of Antibiotics in Escherichia coli.

Author

Haynes KM, Abdali N, Jhawar V, Zgurskaya HI, Parks JM, Green AT, Baudry J, Rybenkov VV, Smith JC, and Walker JK

Subjects

Cell Membrane Permeability, Cinnamates chemical synthesis, Cinnamates pharmacology, Computer Simulation, Databases, Chemical, Drug Resistance, Bacterial drug effects, Drug Synergism, Erythromycin pharmacology, Escherichia coli metabolism, Imidazoles chemical synthesis, Imidazoles pharmacology, Microbial Sensitivity Tests, Models, Molecular, Novobiocin pharmacology, Protein Binding, Structure-Activity Relationship, Anti-Bacterial Agents pharmacology, Carrier Proteins metabolism, Cinnamates chemistry, Escherichia coli drug effects, Escherichia coli Proteins metabolism, Imidazoles chemistry, Lipoproteins metabolism, Membrane Transport Proteins metabolism

Abstract

In Gram-negative bacteria, efflux pumps are able to prevent effective cellular concentrations from being achieved for a number of antibiotics. Small molecule adjuvants that act as efflux pump inhibitors (EPIs) have the potential to reinvigorate existing antibiotics that are currently ineffective due to efflux mechanisms. Through a combination of rigorous experimental screening and in silico virtual screening, we recently identified novel classes of EPIs that interact with the membrane fusion protein AcrA, a critical component of the AcrAB-TolC efflux pump in Escherichia coli. Herein, we present initial optimization efforts and structure-activity relationships around one of those previously described hits, NSC 60339 (1). From these efforts we identified two compounds, SLUPP-225 (17h) and SLUPP-417 (17o), which demonstrate favorable properties as potential EPIs in E. coli cells including the ability to penetrate the outer membrane, improved inhibition of efflux relative to 1, and potentiation of the activity of novobiocin and erythromycin.

Published

2017

29. Identification of C3b-Binding Small-Molecule Complement Inhibitors Using Cheminformatics.

Author

Garcia BL, Skaff DA, Chatterjee A, Hanning A, Walker JK, Wyckoff GJ, and Geisbrecht BV

Subjects

Complement Activation, Complement C3b chemistry, Complement Inactivating Agents therapeutic use, Crystallography, X-Ray, Drug Discovery, Drug Evaluation, Preclinical, Humans, Immunosuppressive Agents therapeutic use, Protein Binding, Proteolysis, Surface Plasmon Resonance, Autoimmune Diseases drug therapy, Complement C3b metabolism, Complement Inactivating Agents isolation & purification, Computational Biology, Immunosuppressive Agents isolation & purification, Neurodegenerative Diseases drug therapy, Small Molecule Libraries

Abstract

The complement system is an elegantly regulated biochemical cascade formed by the collective molecular recognition properties and proteolytic activities of more than two dozen membrane-bound or serum proteins. Complement plays diverse roles in human physiology, such as acting as a sentry against invading microorganisms, priming of the adaptive immune response, and removal of immune complexes. However, dysregulation of complement can serve as a trigger for a wide range of human diseases, which include autoimmune, inflammatory, and degenerative conditions. Despite several potential advantages of modulating complement with small-molecule inhibitors, small-molecule drugs are highly underrepresented in the current complement-directed therapeutics pipeline. In this study, we have employed a cheminformatics drug discovery approach based on the extensive structural and functional knowledge available for the central proteolytic fragment of the cascade, C3b. Using parallel in silico screening methodologies, we identified 45 small molecules that putatively bind C3b near ligand-guided functional hot spots. Surface plasmon resonance experiments resulted in the validation of seven dose-dependent C3b-binding compounds. Competition-based biochemical assays demonstrated the ability of several C3b-binding compounds to interfere with binding of the original C3b ligand that guided their discovery. In vitro assays of complement function identified a single complement inhibitory compound, termed cmp-5, and mechanistic studies of the cmp-5 inhibitory mode revealed it acts at the level of C5 activation. This study has led to the identification of a promising new class of C3b-binding small-molecule complement inhibitors and, to our knowledge, provides the first demonstration of cheminformatics-based, complement-directed drug discovery., (Copyright © 2017 by The American Association of Immunologists, Inc.)

Published

2017

30. Reviving Antibiotics: Efflux Pump Inhibitors That Interact with AcrA, a Membrane Fusion Protein of the AcrAB-TolC Multidrug Efflux Pump.

Author

Abdali N, Parks JM, Haynes KM, Chaney JL, Green AT, Wolloscheck D, Walker JK, Rybenkov VV, Baudry J, Smith JC, and Zgurskaya HI

Subjects

Bacterial Proteins genetics, Drug Design, Drug Discovery, Gene Expression Regulation, Bacterial drug effects, Membrane Transport Proteins chemistry, Membrane Transport Proteins genetics, Models, Molecular, Protein Conformation, Anti-Bacterial Agents pharmacology, Bacterial Proteins metabolism, Gram-Negative Bacteria drug effects, Gram-Negative Bacteria metabolism, Membrane Transport Proteins metabolism

Abstract

Antibiotic resistance is a major threat to human welfare. Inhibitors of multidrug efflux pumps (EPIs) are promising alternative therapeutics that could revive activities of antibiotics and reduce bacterial virulence. Identification of new druggable sites for inhibition is critical for the development of effective EPIs, especially in light of constantly emerging resistance. Here, we describe EPIs that interact with periplasmic membrane fusion proteins, critical components of efflux pumps that are responsible for the activation of the transporter and the recruitment of the outer-membrane channel. The discovered EPIs bind to AcrA, a component of the prototypical AcrAB-TolC pump, change its structure in vivo, inhibit efflux of fluorescent probes, and potentiate the activities of antibiotics in Escherichia coli and other Gram-negative bacteria. Our findings expand the chemical and mechanistic diversity of EPIs, suggest the mechanism for regulation of the efflux pump assembly and activity, and provide a promising path for reviving the activities of antibiotics in resistant bacteria.

Published

2017

31. Therapeutic Effect of a Synthetic RORα/γ Agonist in an Animal Model of Autism.

Author

Wang Y, Billon C, Walker JK, and Burris TP

Subjects

Animals, Ataxin-2 genetics, Ataxin-2 metabolism, Autism Spectrum Disorder complications, Autism Spectrum Disorder genetics, Autophagy-Related Protein-1 Homolog genetics, Brain drug effects, Brain metabolism, Cell Adhesion Molecules, Neuronal genetics, Cell Adhesion Molecules, Neuronal metabolism, Cell Line, Tumor, Disease Models, Animal, Dose-Response Relationship, Drug, Grooming drug effects, HEK293 Cells, Humans, Inositol 1,4,5-Trisphosphate Receptors genetics, Inositol 1,4,5-Trisphosphate Receptors metabolism, Intracellular Signaling Peptides and Proteins genetics, L-Lactate Dehydrogenase genetics, L-Lactate Dehydrogenase metabolism, Mice, Mice, Inbred Strains, Neuroblastoma pathology, Nuclear Receptor Subfamily 1, Group F, Member 1 genetics, REM Sleep Behavior Disorder drug therapy, REM Sleep Behavior Disorder etiology, Autism Spectrum Disorder drug therapy, Benzamides therapeutic use, Gene Expression Regulation drug effects, Nuclear Receptor Subfamily 1, Group F, Member 1 agonists, Nuclear Receptor Subfamily 1, Group F, Member 1 metabolism

Abstract

Autism is a developmental disorder of the nervous system associated with impaired social communication and interactions as well excessive repetitive behaviors. There are no drug therapies that directly target the pathology of this disease. The retinoic acid receptor-related orphan receptor α (RORα) is a nuclear receptor that has been demonstrated to have reduced expression in many individuals with autism spectrum disorder (ASD). Several genes that have been shown to be downregulated in individuals with ASD have also been identified as putative RORα target genes. Utilizing a synthetic RORα/γ agonist, SR1078, that we identified previously, we demonstrate that treatment of BTBR mice (a model of autism) with SR1078 results in reduced repetitive behavior. Furthermore, these mice display increased expression of ASD-associated RORα target genes in both the brains of the BTBR mice and in a human neuroblastoma cell line treated with SR1078. These data suggest that pharmacological activation of RORα may be a method for treatment of autism.

Published

2016

32. Discovery and characterization of atropisomer PH-797804, a p38 MAP kinase inhibitor, as a clinical drug candidate.

Author

Xing L, Devadas B, Devraj RV, Selness SR, Shieh H, Walker JK, Mao M, Messing D, Samas B, Yang JZ, Anderson GD, Webb EG, and Monahan JB

Subjects

Animals, Arthritis drug therapy, Benzamides pharmacology, Benzamides therapeutic use, Computer Simulation, Crystallography, X-Ray, Drug Evaluation, Preclinical, Enzyme Activation drug effects, Female, Lipopolysaccharides toxicity, Male, Protein Kinase Inhibitors pharmacology, Protein Kinase Inhibitors therapeutic use, Protein Structure, Tertiary, Pyridones pharmacology, Pyridones therapeutic use, Quantum Theory, Rats, Receptors, Cell Surface, p38 Mitogen-Activated Protein Kinases metabolism, Benzamides chemistry, Protein Kinase Inhibitors chemistry, Pyridones chemistry, p38 Mitogen-Activated Protein Kinases antagonists & inhibitors

Abstract

PH-797804 ((aS)-3-{3-bromo-4-[(2,4-difluorobenzyl)oxy]-6-methyl-2-oxopyridin-1(2H)-yl}-N,4-dimethylbenzamde) is a diarylpyridinone inhibitor of p38 mitogen-activated protein (MAP) kinase derived from a racemic mixture as the more potent atropisomer (aS), first proposed by molecular modeling and subsequently confirmed by experiments. Due to steric constraints imposed by the pyridinone carbonyl group and the 6- and 6'-methyl substituents of PH-797804, rotation around the connecting bond of the pyridinone and the N-phenyl ring is restricted. Density functional theory predicts a remarkably high rotational energy barrier of >30 kcal mol(-1), corresponding to a half-life of more than one hundred years at room temperature. This gives rise to discrete conformational spaces for the N-phenylpyridinone group, and as a result, two atropic isomers that do not interconvert under ambient conditions. Molecular modeling studies predict that the two isomers should differ in their binding affinity for p38α kinase; whereas the atropic S (aS) isomer binds favorably, the opposite aR isomer incurs significant steric interference with p38α kinase. The two isomers were subsequently identified and separated by chiral chromatography. IC50 values from p38α kinase assays confirm that one atropisomer is >100-fold more potent than the other. It was ultimately confirmed by small-molecule X-ray diffraction that the more potent atropisomer, PH-797804, is the aS isomer of the racemic pair. Extensive pharmacological characterization supports that PH-797804 carries most activity both in vitro and in vivo, and it has a stability profile compatible with oral formulation and delivery options., (Copyright © 2012 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2012

33. Investigation of the pyrazinones as PDE5 inhibitors: evaluation of regioisomeric projections into the solvent region.

Author

Hughes RO, Maddux T, Joseph Rogier D, Lu S, Walker JK, Jon Jacobsen E, Rumsey JM, Zheng Y, Macinnes A, Bond BR, and Han S

Subjects

Crystallography, X-Ray, Inhibitory Concentration 50, Models, Molecular, Phosphodiesterase 5 Inhibitors chemistry, Phosphodiesterase 5 Inhibitors pharmacokinetics, Pyrazines chemistry, Pyrazines pharmacokinetics, Solvents chemistry, Phosphodiesterase 5 Inhibitors pharmacology, Pyrazines pharmacology

Abstract

We describe the design, synthesis and profiling of a novel series of PDE5 inhibitors. We take advantage of an alternate projection into the solvent region to identify compounds with excellent potency, selectivity and pharmacokinetic profiles., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2011

34. Design, synthesis and activity of a potent, selective series of N-aryl pyridinone inhibitors of p38 kinase.

Author

Selness SR, Boehm TL, Walker JK, Devadas B, Durley RC, Kurumbail R, Shieh H, Xing L, Hepperle M, Rucker PV, Jerome KD, Benson AG, Marrufo LD, Madsen HM, Hitchcock J, Owen TJ, Christie L, Promo MA, Hickory BS, Alvira E, Naing W, Blevis-Bal R, Devraj RV, Messing D, Schindler JF, Hirsch J, Saabye M, Bonar S, Webb E, Anderson G, and Monahan JB

Subjects

Animals, Disease Models, Animal, Enzyme Activation drug effects, Enzyme Inhibitors chemistry, Humans, Inhibitory Concentration 50, Male, Microsomes, Liver enzymology, Molecular Structure, Pyridazines chemistry, Pyridazines pharmacology, Pyridones chemistry, Pyrimidines chemistry, Pyrimidines pharmacology, Rats, Rats, Sprague-Dawley, Drug Design, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors pharmacology, Pyridones chemical synthesis, Pyridones pharmacology, p38 Mitogen-Activated Protein Kinases antagonists & inhibitors

Abstract

A series of N-aryl pyridinone inhibitors of p38 mitogen activated protein (MAP) kinase were designed and prepared based on the screening hit SC-25028 (1) and structural comparisons to VX-745 (5). The focus of the investigation targeted the dependence of potency and metabolic stability on the benzyloxy connectivity, the role of the C-6 position and the substitution pattern on the N-phenyl ring. Further optimization produced the highly selective and potent pyridinones 2 and 3. These inhibitors exhibited activity in both acute and chronic models of inflammation., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2011

35. Discovery of PH-797804, a highly selective and potent inhibitor of p38 MAP kinase.

Author

Selness SR, Devraj RV, Devadas B, Walker JK, Boehm TL, Durley RC, Shieh H, Xing L, Rucker PV, Jerome KD, Benson AG, Marrufo LD, Madsen HM, Hitchcock J, Owen TJ, Christie L, Promo MA, Hickory BS, Alvira E, Naing W, Blevis-Bal R, Messing D, Yang J, Mao MK, Yalamanchili G, Vonder Embse R, Hirsch J, Saabye M, Bonar S, Webb E, Anderson G, and Monahan JB

Subjects

Animals, Benzamides chemistry, Disease Models, Animal, Dogs, Enzyme Activation drug effects, Enzyme Inhibitors chemistry, Humans, Inhibitory Concentration 50, Macaca fascicularis, Male, Molecular Structure, Pyridones, Pyrones chemistry, Rats, Rats, Sprague-Dawley, Structure-Activity Relationship, p38 Mitogen-Activated Protein Kinases chemistry, p38 Mitogen-Activated Protein Kinases pharmacology, Benzamides chemical synthesis, Benzamides pharmacology, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors pharmacology, Pyrones chemical synthesis, Pyrones pharmacology, p38 Mitogen-Activated Protein Kinases antagonists & inhibitors

Abstract

The synthesis and SAR studies of a novel N-aryl pyridinone class of p38 kinase inhibitors are described. Systematic structural modifications to the HTS lead, 5, led to the identification of (-)-4a as a clinical candidate for the treatment of inflammatory diseases. Additionally, the chiral synthesis and properties of (-)-4a are described., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2011

36. Acute lymphoid and gastrointestinal toxicity induced by selective p38alpha map kinase and map kinase-activated protein kinase-2 (MK2) inhibitors in the dog.

Author

Morris DL, O'Neil SP, Devraj RV, Portanova JP, Gilles RW, Gross CJ, Curtiss SW, Komocsar WJ, Garner DS, Happa FA, Kraus LJ, Nikula KJ, Monahan JB, Selness SR, Galluppi GR, Shevlin KM, Kramer JA, Walker JK, Messing DM, Anderson DR, Mourey RJ, Whiteley LO, Daniels JS, Yang JZ, Rowlands PC, Alden CL, Davis JW 2nd, and Sagartz JE

Subjects

Animals, B-Lymphocytes metabolism, Blotting, Western, Cell Proliferation drug effects, Cells, Cultured, Colon drug effects, Colon pathology, Dogs, Female, Gastrointestinal Diseases pathology, Gastrointestinal Hemorrhage chemically induced, Humans, Immunohistochemistry, Intracellular Signaling Peptides and Proteins metabolism, Linear Models, Lymph Nodes drug effects, Lymph Nodes pathology, Lymphatic Diseases pathology, Macaca fascicularis, Male, Mice, Protein Serine-Threonine Kinases metabolism, Rats, Rats, Sprague-Dawley, Spleen cytology, Spleen metabolism, T-Lymphocytes metabolism, Toxicity Tests, Acute, p38 Mitogen-Activated Protein Kinases metabolism, Gastrointestinal Diseases chemically induced, Intracellular Signaling Peptides and Proteins antagonists & inhibitors, Lymphatic Diseases chemically induced, Protein Kinase Inhibitors toxicity, Protein Serine-Threonine Kinases antagonists & inhibitors, p38 Mitogen-Activated Protein Kinases antagonists & inhibitors

Abstract

Exposure to moderately selective p38alpha mitogen-activated protein kinase (MAPK) inhibitors in the Beagle dog results in an acute toxicity consisting of mild clinical signs (decreased activity, diarrhea, and fever), lymphoid necrosis and depletion in the gut-associated lymphoid tissue (GALT), mesenteric lymph nodes and spleen, and linear colonic and cecal mucosal hemorrhages. Lymphocyte apoptosis and necrosis in the GALT is the earliest and most prominent histopathologic change observed, followed temporally by neutrophilic infiltration and acute inflammation of the lymph nodes and spleen and multifocal mucosal epithelial necrosis and linear hemorrhages in the colon and cecum. These effects are not observed in the mouse, rat, or cynomolgus monkey. To further characterize the acute toxicity in the dog, a series of in vivo, in vitro, and immunohistochemical studies were conducted to determine the relationship between the lymphoid and gastrointestinal (GI) toxicity and p38 MAPK inhibition. Results of these studies demonstrate a direct correlation between p38alpha MAPK inhibition and the acute lymphoid and gastrointestinal toxicity in the dog. Similar effects were observed following exposure to inhibitors of MAPK-activated protein kinase-2 (MK2), further implicating the role of p38alpha MAPK signaling pathway inhibition in these effects. Based on these findings, the authors conclude that p38alpha MAPK inhibition results in acute lymphoid and GI toxicity in the dog and is unique among the species evaluated in these studies.

Published

2010

37. 1-(2-(2,2,2-trifluoroethoxy)ethyl-1H-pyrazolo[4,3-d]pyrimidines as potent phosphodiesterase 5 (PDE5) inhibitors.

Author

Tollefson MB, Acker BA, Jacobsen EJ, Hughes RO, Walker JK, Fox DN, Palmer MJ, Freeman SK, Yu Y, and Bond BR

Subjects

Animals, Antihypertensive Agents chemical synthesis, Antihypertensive Agents pharmacokinetics, Cyclic Nucleotide Phosphodiesterases, Type 5 metabolism, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors pharmacokinetics, Humans, Microsomes, Liver metabolism, Patch-Clamp Techniques, Pyrimidines chemical synthesis, Pyrimidines pharmacokinetics, Rats, Structure-Activity Relationship, Antihypertensive Agents chemistry, Enzyme Inhibitors chemistry, Phosphodiesterase 5 Inhibitors, Pyrimidines chemistry

Abstract

1H-Pyrazolo[4,3-d]pyrimidines were previously disclosed as a potent second generation class of phosphodiesterase 5 (PDE5) inhibitors. This work explores the advancement of more selective and potent PDE5 inhibitors resulting from the substitution of 2-(2,2,2-trifluoroethoxy)ethyl at the 1 position in the so-called alkoxy pocket., (Copyright 2010 Elsevier Ltd. All rights reserved.)

Published

2010

38. Discovery of 5-substituted-N-arylpyridazinones as inhibitors of p38 MAP kinase.

Author

Jerome KD, Hepperle ME, Walker JK, Xing L, Devraj RV, Benson AG, Baldus JE, and Selness SR

Subjects

Anti-Infective Agents chemical synthesis, Anti-Infective Agents pharmacology, Binding Sites, Computer Simulation, Drug Discovery, Mitogen-Activated Protein Kinase 14 metabolism, Protein Kinase Inhibitors chemical synthesis, Protein Kinase Inhibitors pharmacology, Pyridazines chemical synthesis, Pyridazines pharmacology, Structure-Activity Relationship, Anti-Infective Agents chemistry, Mitogen-Activated Protein Kinase 14 antagonists & inhibitors, Protein Kinase Inhibitors chemistry, Pyridazines chemistry

Abstract

The synthesis, structure-activity relationship and modeling of a series of 5-substituted-N-aryl pyridazinone based p38alpha inhibitors are described. In comparing the series to the similar N-aryl pyridinone series, it was found that the pyridazinones maintained a weaker interaction to the p38 enzyme, and therefore showed generally weaker binding than the pyridinones., (Copyright 2010 Elsevier Ltd. All rights reserved.)

Published

2010

39. 1-(2-Ethoxyethyl)-1H-pyrazolo[4,3-d]pyrimidines as potent phosphodiesterase 5 (PDE5) inhibitors.

Author

Tollefson MB, Acker BA, Jacobsen EJ, Hughes RO, Walker JK, Fox DN, Palmer MJ, Freeman SK, Yu Y, and Bond BR

Subjects

Animals, Cyclic Nucleotide Phosphodiesterases, Type 5 metabolism, Dogs, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors pharmacokinetics, Humans, Microsomes, Liver metabolism, Pyrimidines chemical synthesis, Pyrimidines pharmacokinetics, Structure-Activity Relationship, Enzyme Inhibitors chemistry, Phosphodiesterase 5 Inhibitors, Pyrimidines chemistry

Abstract

1H-Pyrazolo[4,3-d]pyrimidines are a class of potent and selective second generation phosphodiesterase 5 (PDE5) inhibitors. This work explores the potency, selectivity and efficacy of 1-(2-ethoxyethyl)-1H-pyrazolo[4,5-d]pyrimidines as PDE5 inhibitors resulting in the advancement of a clinical candidate.

Published

2010

40. Identification of SD-0006, a potent diaryl pyrazole inhibitor of p38 MAP kinase.

Author

Walker JK, Selness SR, Devraj RV, Hepperle ME, Naing W, Shieh H, Kurambail R, Yang S, Flynn DL, Benson AG, Messing DM, Dice T, Kim T, Lindmark RJ, Monahan JB, and Portanova J

Subjects

Animals, Catalytic Domain, Humans, Models, Molecular, p38 Mitogen-Activated Protein Kinases metabolism, Protein Kinase Inhibitors pharmacology, Pyrazoles pharmacology, Pyrimidines pharmacology, p38 Mitogen-Activated Protein Kinases antagonists & inhibitors

Abstract

Starting from an initial HTS screening lead, a novel series of C(5)-substituted diaryl pyrazoles were developed that showed potent inhibition of p38alpha kinase. Key to this outcome was the switch from a pyridyl to pyrimidine at the C(4)-position leading to analogs that were potent in human whole blood based cell assay as well as in a number of animal efficacy models for rheumatoid arthritis. Ultimately, we identified a clinical candidate from this substrate; SD-0006., (Copyright 2010 Elsevier Ltd. All rights reserved.)

Published

2010

41. Design, synthesis, and biological evaluation of 3-[4-(2-hydroxyethyl)piperazin-1-yl]-7-(6-methoxypyridin-3-yl)-1-(2-propoxyethyl)pyrido[3,4-b]pyrazin-2(1H)-one, a potent, orally active, brain penetrant inhibitor of phosphodiesterase 5 (PDE5).

Author

Hughes RO, Rogier DJ, Jacobsen EJ, Walker JK, Macinnes A, Bond BR, Zhang LL, Yu Y, Zheng Y, Rumsey JM, Walgren JL, Curtiss SW, Fobian YM, Heasley SE, Cubbage JW, Moon JB, Brown DL, Acker BA, Maddux TM, Tollefson MB, Mischke BV, Owen DR, Freskos JN, Molyneaux JM, Benson AG, and Blevis-Bal RM

Subjects

Administration, Oral, Animals, Biological Availability, Blood Pressure drug effects, Cyclic Nucleotide Phosphodiesterases, Type 5 metabolism, Dose-Response Relationship, Drug, Drug Design, Humans, Male, Models, Chemical, Molecular Structure, Phosphodiesterase Inhibitors pharmacokinetics, Pyrazines pharmacokinetics, Pyridines pharmacokinetics, Rats, Rats, Inbred SHR, Rats, Sprague-Dawley, Brain metabolism, Phosphodiesterase 5 Inhibitors, Phosphodiesterase Inhibitors chemical synthesis, Phosphodiesterase Inhibitors pharmacology, Pyrazines chemical synthesis, Pyrazines pharmacology, Pyridines chemical synthesis, Pyridines pharmacology

Abstract

We recently described a novel series of aminopyridopyrazinones as PDE5 inhibitors. Efforts toward optimization of this series culminated in the identification of 3-[4-(2-hydroxyethyl)piperazin-1-yl]-7-(6-methoxypyridin-3-yl)-1-(2-propoxyethyl)pyrido[3,4-b]pyrazin-2(1H)-one, which possessed an excellent potency and selectivity profile and demonstrated robust in vivo blood pressure lowering in a spontaneously hypertensive rat (SHR) model. Furthermore, this compound is brain penetrant and will be a useful agent for evaluating the therapeutic potential of central inhibition of PDE5. This compound has recently entered clinical trials.

Published

2010

42. Discovery of N-substituted pyridinones as potent and selective inhibitors of p38 kinase.

Author

Selness SR, Devraj RV, Monahan JB, Boehm TL, Walker JK, Devadas B, Durley RC, Kurumbail R, Shieh H, Xing L, Hepperle M, Rucker PV, Jerome KD, Benson AG, Marrufo LD, Madsen HM, Hitchcock J, Owen TJ, Christie L, Promo MA, Hickory BS, Alvira E, Naing W, and Blevis-Bal R

Subjects

Administration, Oral, Animals, Anti-Inflammatory Agents chemical synthesis, Anti-Inflammatory Agents pharmacokinetics, Binding Sites, Catalytic Domain, Crystallography, X-Ray, Drug Discovery, Humans, JNK Mitogen-Activated Protein Kinases antagonists & inhibitors, JNK Mitogen-Activated Protein Kinases metabolism, Male, Microsomes, Liver metabolism, Protein Kinase Inhibitors chemical synthesis, Protein Kinase Inhibitors pharmacokinetics, Pyridones chemical synthesis, Pyridones pharmacokinetics, Rats, Rats, Sprague-Dawley, Structure-Activity Relationship, p38 Mitogen-Activated Protein Kinases metabolism, Anti-Inflammatory Agents chemistry, Protein Kinase Inhibitors chemistry, Pyridones chemistry, p38 Mitogen-Activated Protein Kinases antagonists & inhibitors

Abstract

The identification and evolution of a series of potent and selective p38 inhibitors is described. p38 inhibitors based on a N-benzyl pyridinone high-throughput screening hit were prepared and their SAR explored. Their design was guided by ligand bound co-crystals of p38alpha. These efforts resulted in the identification of 12r and 19 as orally active inhibitors of p38 with significant efficacy in both acute and chronic models of inflammation.

Published

2009

43. Optimization of the aminopyridopyrazinones class of PDE5 inhibitors: discovery of 3-[(trans-4-hydroxycyclohexyl)amino]-7-(6-methoxypyridin-3-yl)-1-(2-propoxyethyl)pyrido[3,4-b]pyrazin-2(1H)-one.

Author

Hughes RO, Walker JK, Rogier DJ, Heasley SE, Blevis-Bal RM, Benson AG, Jacobsen EJ, Cubbage JW, Fobian YM, Owen DR, Freskos JN, Molyneaux JM, Brown DL, Acker BA, Maddux TM, Tollefson MB, Moon JB, Mischke BV, Rumsey JM, Zheng Y, MacInnes A, Bond BR, and Yu Y

Subjects

Animals, Cyclic Nucleotide Phosphodiesterases, Type 5 metabolism, Cyclic Nucleotide Phosphodiesterases, Type 6 antagonists & inhibitors, Cyclic Nucleotide Phosphodiesterases, Type 6 metabolism, Dogs, Drug Discovery, Humans, Phosphodiesterase Inhibitors chemical synthesis, Phosphodiesterase Inhibitors pharmacokinetics, Protein Isoforms antagonists & inhibitors, Protein Isoforms metabolism, Pyrazines chemical synthesis, Pyrazines pharmacokinetics, Pyridines chemical synthesis, Pyridines pharmacokinetics, Rats, Rats, Inbred SHR, Structure-Activity Relationship, Phosphodiesterase 5 Inhibitors, Phosphodiesterase Inhibitors chemistry, Pyrazines chemistry, Pyridines chemistry

Abstract

We describe efforts to improve the pharmacokinetic profile of the aminopyridopyrazinone class of PDE5 inhibitors. These efforts led to the discovery of 3-[(trans-4-hydroxycyclohexyl)amino]-7-(6-methoxypyridin-3-yl)-1-(2-propoxyethyl)pyrido[3,4-b]pyrazin-2(1H)-one, a potent and selective inhibitor of PDE5 with an excellent PK profile.

Published

2009

44. Investigation of aminopyridiopyrazinones as PDE5 inhibitors: Evaluation of modifications to the central ring system.

Author

Hughes RO, Walker JK, Cubbage JW, Fobian YM, Rogier DJ, Heasley SE, Blevis-Bal RM, Benson AG, Owen DR, Jacobsen EJ, Freskos JN, Molyneaux JM, Brown DL, Stallings WC, Acker BA, Maddux TM, Tollefson MB, Williams JM, Moon JB, Mischke BV, Rumsey JM, Zheng Y, Macinnes A, Bond BR, and Yu Y

Subjects

Administration, Oral, Aminopyridines pharmacology, Animals, Chemistry, Pharmaceutical methods, Cyclic GMP chemistry, Cyclic Nucleotide Phosphodiesterases, Type 5 chemistry, Drug Design, Humans, Hydrogen-Ion Concentration, Hypertension drug therapy, Microsomes drug effects, Models, Chemical, Phosphodiesterase Inhibitors pharmacology, Pyrazines pharmacology, Rats, Rats, Sprague-Dawley, Solubility, Aminopyridines chemical synthesis, Phosphodiesterase 5 Inhibitors, Phosphodiesterase Inhibitors chemical synthesis, Pyrazines chemical synthesis

Abstract

Efforts to improve the potency and physical properties of the aminopyridiopyrazinone class of PDE5 inhibitors through modification of the core ring system are described. Five new ring systems are evaluated and features that impart improved potency and improved solubility are delineated.

Published

2009

45. Identification, synthesis and SAR of amino substituted pyrido[3,2b]pyrazinones as potent and selective PDE5 inhibitors.

Author

Owen DR, Walker JK, Jon Jacobsen E, Freskos JN, Hughes RO, Brown DL, Bell AS, Brown DG, Phillips C, Mischke BV, Molyneaux JM, Fobian YM, Heasley SE, Moon JB, Stallings WC, Joseph Rogier D, Fox DN, Palmer MJ, Ringer T, Rodriquez-Lens M, Cubbage JW, Blevis-Bal RM, Benson AG, Acker BA, Maddux TM, Tollefson MB, Bond BR, Macinnes A, and Yu Y

Subjects

3',5'-Cyclic-GMP Phosphodiesterases, Animals, Catalytic Domain, Chemistry, Pharmaceutical methods, Crystallography, X-Ray methods, Cyclic Nucleotide Phosphodiesterases, Type 6 antagonists & inhibitors, Cyclic Nucleotide Phosphodiesterases, Type 6 chemistry, Drug Design, Humans, Hydrogen-Ion Concentration, Inhibitory Concentration 50, Phosphodiesterase Inhibitors chemical synthesis, Phosphodiesterase Inhibitors pharmacology, Phosphoric Diester Hydrolases chemistry, Protein Structure, Tertiary, Pyrazines pharmacology, Rats, Structure-Activity Relationship, Cyclic Nucleotide Phosphodiesterases, Type 5 chemistry, Phosphodiesterase 5 Inhibitors, Pyrazines chemical synthesis

Abstract

A new class of potent and selective PDE5 inhibitors is disclosed. Guided by X-ray crystallographic data, optimization of an HTS lead led to the discovery of a series of 2-aryl, (N8)-alkyl substituted-6-aminosubstituted pyrido[3,2b]pyrazinones which show potent inhibition of the PDE5 enzyme. Synthetic details and some structure-activity relationships are also presented.

Published

2009

46. Structural bioinformatics-based prediction of exceptional selectivity of p38 MAP kinase inhibitor PH-797804.

Author

Xing L, Shieh HS, Selness SR, Devraj RV, Walker JK, Devadas B, Hope HR, Compton RP, Schindler JF, Hirsch JL, Benson AG, Kurumbail RG, Stegeman RA, Williams JM, Broadus RM, Walden Z, and Monahan JB

Subjects

Benzamides chemistry, Crystallography, X-Ray, Humans, Hydrogen Bonding, Models, Molecular, Molecular Structure, Phosphorylation, Protein Kinase Inhibitors chemistry, Pyridones, Pyrones chemistry, Substrate Specificity, p38 Mitogen-Activated Protein Kinases metabolism, Benzamides pharmacology, Computational Biology, Protein Kinase Inhibitors pharmacology, Pyrones pharmacology, p38 Mitogen-Activated Protein Kinases antagonists & inhibitors

Abstract

PH-797804 is a diarylpyridinone inhibitor of p38alpha mitogen-activated protein (MAP) kinase derived from a racemic mixture as the more potent atropisomer (aS), first proposed by molecular modeling and subsequently confirmed by experiments. On the basis of structural comparison with a different biaryl pyrazole template and supported by dozens of high-resolution crystal structures of p38alpha inhibitor complexes, PH-797804 is predicted to possess a high level of specificity across the broad human kinase genome. We used a structural bioinformatics approach to identify two selectivity elements encoded by the TXXXG sequence motif on the p38alpha kinase hinge: (i) Thr106 that serves as the gatekeeper to the buried hydrophobic pocket occupied by 2,4-difluorophenyl of PH-797804 and (ii) the bidentate hydrogen bonds formed by the pyridinone moiety with the kinase hinge requiring an induced 180 degrees rotation of the Met109-Gly110 peptide bond. The peptide flip occurs in p38alpha kinase due to the critical glycine residue marked by its conformational flexibility. Kinome-wide sequence mining revealed rare presentation of the selectivity motif. Corroboratively, PH-797804 exhibited exceptionally high specificity against MAP kinases and the related kinases. No cross-reactivity was observed in large panels of kinase screens (selectivity ratio of >500-fold). In cellular assays, PH-797804 demonstrated superior potency and selectivity consistent with the biochemical measurements. PH-797804 has met safety criteria in human phase I studies and is under clinical development for several inflammatory conditions. Understanding the rationale for selectivity at the molecular level helps elucidate the biological function and design of specific p38alpha kinase inhibitors.

Published

2009