Your search keyword '"Henke BR"' showing total 34 results

1. Human cardiovascular disease model predicts xanthine oxidase inhibitor cardiovascular risk.

Author

Feaver RE, Bowers MS, Cole BK, Hoang S, Lawson MJ, Taylor J, LaMoreaux BD, Zhao L, Henke BR, Johns BA, Nyborg AC, Wamhoff BR, and Figler RA

Subjects

United States, Humans, Xanthine Oxidase, Febuxostat pharmacology, Risk Factors, Enzyme Inhibitors adverse effects, Heart Disease Risk Factors, Cardiovascular Diseases chemically induced

Abstract

Some health concerns are often not identified until late into clinical development of drugs, which can place participants and patients at significant risk. For example, the United States Food and Drug Administration (FDA) labeled the xanthine oxidase inhibitor febuxostat with a"boxed" warning regarding an increased risk of cardiovascular death, and this safety risk was only identified during Phase 3b clinical trials after its approval. Thus, better preclinical assessment of drug efficacy and safety are needed to accurately evaluate candidate drug risk earlier in discovery and development. This study explored whether an in vitro vascular model incorporating human vascular cells and hemodynamics could be used to differentiate the potential cardiovascular risk associated with molecules that have similar on-target mechanisms of action. We compared the transcriptomic responses induced by febuxostat and other xanthine oxidase inhibitors to a database of 111 different compounds profiled in the human vascular model. Of the 111 compounds in the database, 107 are clinical-stage and 33 are FDA-labelled for increased cardiovascular risk. Febuxostat induces pathway-level regulation that has high similarity to the set of drugs FDA-labelled for increased cardiovascular risk. These results were replicated with a febuxostat analog, but not another structurally distinct xanthine oxidase inhibitor that does not confer cardiovascular risk. Together, these data suggest that the FDA warning for febuxostat stems from the chemical structure of the medication itself, rather than the target, xanthine oxidase. Importantly, these data indicate that cardiovascular risk can be evaluated in this in vitro human vascular model, which may facilitate understanding the drug candidate safety profile earlier in discovery and development., Competing Interests: Authors RE Feaver, PhD, BK Cole, PhD, S Hoang, PhD, MJ Lawson, PhD, J Taylor, BS, BR Henke, PhD, BA Johns, PhD, BR Wamhoff, PhD, RA Figler, PhD have financial interest, including employment and stock ownership at HemoShear Therapeutics. Authors MS Bowers, PhD, BD LaMoreaux, MD, L Zhao, PhD, AC Nyborg have financial interest, including employment and stock ownership at Horizon Therapeutics. This does not alter our adherence to PLOS ONE policies on sharing data and materials., (Copyright: © 2023 Feaver et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.)

Published

2023

2. A novel small molecule approach for the treatment of propionic and methylmalonic acidemias.

Author

Armstrong AJ, Collado MS, Henke BR, Olson MW, Hoang SA, Hamilton CA, Pourtaheri TD, Chapman KA, Summar MM, Johns BA, Wamhoff BR, Reardon JE, and Figler RA

Subjects

Acyl Coenzyme A metabolism, Amino Acid Metabolism, Inborn Errors genetics, Amino Acid Metabolism, Inborn Errors pathology, Carnitine metabolism, Cell Line, Citrates metabolism, Hepatocytes drug effects, Humans, Methylmalonyl-CoA Mutase deficiency, Propionic Acidemia genetics, Propionic Acidemia pathology, Amino Acid Metabolism, Inborn Errors drug therapy, Methylmalonyl-CoA Decarboxylase genetics, Methylmalonyl-CoA Mutase genetics, Propionic Acidemia drug therapy, Small Molecule Libraries pharmacology

Abstract

Propionic Acidemia (PA) and Methylmalonic Acidemia (MMA) are inborn errors of metabolism affecting the catabolism of valine, isoleucine, methionine, threonine and odd-chain fatty acids. These are multi-organ disorders caused by the enzymatic deficiency of propionyl-CoA carboxylase (PCC) or methylmalonyl-CoA mutase (MUT), resulting in the accumulation of propionyl-coenzyme A (P-CoA) and methylmalonyl-CoA (M-CoA in MMA only). Primary metabolites of these CoA esters include 2-methylcitric acid (MCA), propionyl-carnitine (C3), and 3-hydroxypropionic acid, which are detectable in both PA and MMA, and methylmalonic acid, which is detectable in MMA patients only (Chapman et al., 2012). We deployed liver cell-based models that utilized PA and MMA patient-derived primary hepatocytes to validate a small molecule therapy for PA and MMA patients. The small molecule, HST5040, resulted in a dose-dependent reduction in the levels of P-CoA, M-CoA (in MMA) and the disease-relevant biomarkers C3, MCA, and methylmalonic acid (in MMA). A putative working model of how HST5040 reduces the P-CoA and its derived metabolites involves the conversion of HST5040 to HST5040-CoA driving the redistribution of free and conjugated CoA pools, resulting in the differential reduction of the aberrantly high P-CoA and M-CoA. The reduction of P-CoA and M-CoA, either by slowing production (due to increased demands on the free CoA (CoASH) pool) or enhancing clearance (to replenish the CoASH pool), results in a net decrease in the CoA-derived metabolites (C3, MCA and MMA (MMA only)). A Phase 2 study in PA and MMA patients will be initiated in the United States., Competing Interests: Conflict of interest The following authors have units of ownership in HemoShear Therapeutics, Inc.: Allison J Armstrong, Maria Sol Collado, Matthew W Olson, Stephen A Hoang, Christin A Hamilton, Brian A Johns, Brian R Wamhoff, John E Reardon, and Robert A Figler. Author, Kimberly A Chapman, is the PI on the HemoShear Therapeutics' sponsored HERO (Helping Reduce Organic Acids) Clinical Trial at Children's National Medical Center, Washington DC., (Copyright © 2021 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2021

3. Identification of 2,2-Dimethylbutanoic Acid (HST5040), a Clinical Development Candidate for the Treatment of Propionic Acidemia and Methylmalonic Acidemia.

Author

Armstrong AJ, Henke BR, Collado MS, Taylor JM, Pourtaheri TD, Dillberger JE, Roper TD, Wamhoff BR, Olson MW, Figler RA, Hoang SA, Reardon JE, and Johns BA

Subjects

Acyl Coenzyme A metabolism, Amino Acid Metabolism, Inborn Errors pathology, Animals, Area Under Curve, Butyrates chemistry, Butyrates metabolism, Cells, Cultured, Dogs, Drug Evaluation, Preclinical, Half-Life, Hepatocytes cytology, Hepatocytes metabolism, Humans, Mice, Models, Biological, Propionic Acidemia pathology, ROC Curve, Rats, Structure-Activity Relationship, Amino Acid Metabolism, Inborn Errors drug therapy, Butyrates therapeutic use, Propionic Acidemia drug therapy

Abstract

Propionic acidemia (PA) and methylmalonic acidemia (MMA) are rare autosomal recessive disorders of propionyl-CoA (P-CoA) catabolism, caused by a deficiency in the enzymes P-CoA carboxylase and methylmalonyl-CoA (M-CoA) mutase, respectively. PA and MMA are classified as intoxication-type inborn errors of metabolism because the intramitochondrial accumulation of P-CoA, M-CoA, and other metabolites results in secondary inhibition of multiple pathways of intermediary metabolism, leading to organ dysfunction and failure. Herein, we describe the structure-activity relationships of a series of short-chain carboxylic acids which reduce disease-related metabolites in PA and MMA primary hepatocyte disease models. These studies culminated in the identification of 2,2-dimethylbutanoic acid ( 10 , HST5040) as a clinical candidate for the treatment of PA and MMA. Additionally, we describe the in vitro and in vivo absorption, distribution, metabolism, and excretion profile of HST5040, data from preclinical studies, and the synthesis of the sodium salt of HST5040 for clinical trials.

Published

2021

4. Inhibitor Mimetic Mutations in the Pseudomonas aeruginosa PqsE Enzyme Reveal a Protein-Protein Interaction with the Quorum-Sensing Receptor RhlR That Is Vital for Virulence Factor Production.

Author

Taylor IR, Paczkowski JE, Jeffrey PD, Henke BR, Smith CD, and Bassler BL

Subjects

Pseudomonas aeruginosa enzymology, Pseudomonas aeruginosa pathogenicity, Molecular Mimicry, Mutation, Pseudomonas aeruginosa genetics, Quorum Sensing, Virulence Factors biosynthesis

Abstract

Pseudomonas aeruginosa is an opportunistic human pathogen that causes fatal infections. There exists an urgent need for new antimicrobial agents to combat P. aeruginosa . We conducted a screen for molecules that bind the virulence-controlling protein PqsE and characterized hit compounds for inhibition of PqsE enzymatic activity. The binding conformations of two inhibitory molecules, BB391 and BB393, were identified by crystallography, and inhibitor binding was mimicked by the substitution of PqsE residues E182 and S285 with tryptophan. Comparison of the inhibitor-mimetic mutations to the catalytically inactive PqsE D73A protein demonstrated that catalysis is not responsible for the role PqsE plays in driving virulence factor production. Rather, the PqsE E182W protein fails to interact with the quorum-sensing receptor, RhlR, and our results suggest that it is this interaction that is responsible for promoting virulence factor production in P. aeruginosa . These findings provide a new route for drug discovery efforts targeting PqsE.

Published

2021

5. Mechanism underlying autoinducer recognition in the Vibrio cholerae DPO-VqmA quorum-sensing pathway.

Author

Huang X, Duddy OP, Silpe JE, Paczkowski JE, Cong J, Henke BR, and Bassler BL

Subjects

Bacterial Proteins chemistry, Bacterial Proteins genetics, Binding Sites, Crystallography, X-Ray, DNA chemistry, DNA metabolism, Gene Expression Regulation, Bacterial, Ligands, Molecular Dynamics Simulation, Mutagenesis, Site-Directed, Protein Binding, Pyrazoles chemistry, Structure-Activity Relationship, Transcription Factors chemistry, Transcription Factors genetics, Bacterial Proteins metabolism, Pyrazoles metabolism, Quorum Sensing, Signal Transduction, Transcription Factors metabolism, Vibrio cholerae metabolism

Abstract

Quorum sensing is a bacterial communication process whereby bacteria produce, release, and detect extracellular signaling molecules called autoinducers to coordinate collective behaviors. In the pathogen Vibrio cholerae , the quorum-sensing autoinducer 3,5-dimethyl-pyrazin-2-ol (DPO) binds the receptor and transcription factor VqmA. The DPO-VqmA complex activates transcription of vqmR , encoding the VqmR small RNA, which represses genes required for biofilm formation and virulence factor production. Here, we show that VqmA is soluble and properly folded and activates basal-level transcription of its target vqmR in the absence of DPO. VqmA transcriptional activity is increased in response to increasing concentrations of DPO, allowing VqmA to drive the V. cholerae quorum-sensing transition at high cell densities. We solved the DPO-VqmA crystal structure to 2.0 Å resolution and compared it with existing structures to understand the conformational changes VqmA undergoes upon DNA binding. Analysis of DPO analogs showed that a hydroxyl or carbonyl group at the 2'-position is critical for binding to VqmA. The proposed DPO precursor, a linear molecule, N -alanyl-aminoacetone (Ala-AA), also bound and activated VqmA. Results from site-directed mutagenesis and competitive ligand-binding analyses revealed that DPO and Ala-AA occupy the same binding site. In summary, our structure-function analysis identifies key features required for VqmA activation and DNA binding and establishes that, whereas VqmA binds two different ligands, VqmA does not require a bound ligand for folding or basal transcriptional activity. However, bound ligand is required for maximal activity., (© 2020 Huang et al.)

Published

2020

6. Discovery of PqsE Thioesterase Inhibitors for Pseudomonas aeruginosa Using DNA-Encoded Small Molecule Library Screening.

Author

Valastyan JS, Tota MR, Taylor IR, Stergioula V, Hone GAB, Smith CD, Henke BR, Carson KG, and Bassler BL

Subjects

Benzamides chemical synthesis, Benzamides pharmacology, Enzyme Inhibitors chemical synthesis, Microbial Sensitivity Tests, Molecular Structure, Phthalic Acids chemical synthesis, Phthalic Acids pharmacology, Pseudomonas aeruginosa enzymology, Small Molecule Libraries chemical synthesis, Structure-Activity Relationship, Bacterial Proteins antagonists & inhibitors, DNA chemistry, Enzyme Inhibitors pharmacology, Pseudomonas aeruginosa drug effects, Small Molecule Libraries pharmacology, Thiolester Hydrolases antagonists & inhibitors

Abstract

Pseudomonas aeruginosa is a leading cause of hospital-acquired infections in the United States. PqsE, a thioesterase enzyme, is vital for virulence of P. aeruginosa , making PqsE an attractive target for inhibition. Neither the substrate nor the product of PqsE catalysis has been identified. A library of 550 million DNA-encoded drug-like small molecules was screened for those that bind to the purified PqsE protein. The structures of the bound molecules were identified by high throughput sequencing of the attached DNA barcodes. Putative PqsE binders with the strongest affinity features were examined for inhibition of PqsE thioesterase activity in vitro . The most potent inhibitors were resynthesized off DNA and examined for the ability to alter PqsE thermal melting and for PqsE thioesterase inhibition. Here, we report the synthesis, biological activity, mechanism of action, and early structure-activity relationships of a series of 2-(phenylcarbamoyl)benzoic acids that noncompetitively inhibit PqsE. A small set of analogs designed to probe initial structure-activity relationships showed increases in potency relative to the original hits, the best of which has an IC 50 = 5 μM. Compound refinement is required to assess their in vivo activities as the current compounds do not accumulate in the P. aeruginosa cytosol. Our strategy validates DNA-encoded compound library screening as a rapid and effective method to identify catalytic inhibitors of the PqsE protein, and more generally, for discovering binders to bacterial proteins revealed by genetic screening to have crucial in vivo activities but whose biological functions have not been well-defined.

Published

2020

7. An Autoinducer Analogue Reveals an Alternative Mode of Ligand Binding for the LasR Quorum-Sensing Receptor.

Author

Paczkowski JE, McCready AR, Cong JP, Li Z, Jeffrey PD, Smith CD, Henke BR, Hughson FM, and Bassler BL

Subjects

4-Butyrolactone chemistry, 4-Butyrolactone metabolism, Amino Acids chemistry, Escherichia coli drug effects, Ligands, Molecular Structure, Mutation, Protein Binding, Pseudomonas aeruginosa drug effects, Signal Transduction, Structure-Activity Relationship, 4-Butyrolactone analogs & derivatives, Bacterial Proteins metabolism, Quorum Sensing drug effects, Trans-Activators metabolism

Abstract

Bacteria use a cell-cell communication process called quorum sensing to coordinate collective behaviors. Quorum sensing relies on production and group-wide detection of extracellular signal molecules called autoinducers. Here, we probe the activity of the Pseudomonas aeruginosa LasR quorum-sensing receptor using synthetic agonists based on the structure of the native homoserine lactone autoinducer. The synthetic compounds range from low to high potency, and agonist activity tracks with the ability of the agonist to stabilize the LasR protein. Structural analyses of the LasR ligand binding domain complexed with representative synthetic agonists reveal two modes of ligand binding, one mimicking the canonical autoinducer binding arrangement, and the other with the lactone head group rotated approximately 150°. Iterative mutagenesis combined with chemical synthesis reveals the amino acid residues and the chemical moieties, respectively, that are key to enabling each mode of binding. Simultaneous alteration of LasR residues Thr75, Tyr93, and Ala127 converts low-potency compounds into high-potency compounds and converts ligands that are nearly inactive into low-potency compounds. These results show that the LasR binding pocket displays significant flexibility in accommodating different ligands. The ability of LasR to bind ligands in different conformations, and in so doing, alter their potency as agonists, could explain the difficulties that have been encountered in the development of competitive LasR inhibitors.

Published

2019

8. Structural determinants driving homoserine lactone ligand selection in the Pseudomonas aeruginosa LasR quorum-sensing receptor.

Author

McCready AR, Paczkowski JE, Henke BR, and Bassler BL

Subjects

4-Butyrolactone metabolism, Bacterial Proteins genetics, Blotting, Western, Ligands, Mutagenesis, Site-Directed, Protein Structure, Quaternary, Pseudomonas aeruginosa physiology, Structure-Activity Relationship, Trans-Activators genetics, 4-Butyrolactone analogs & derivatives, Bacterial Proteins metabolism, Pseudomonas aeruginosa metabolism, Quorum Sensing, Trans-Activators metabolism

Abstract

Quorum sensing is a cell-cell communication process that bacteria use to orchestrate group behaviors. Quorum sensing is mediated by signal molecules called autoinducers. Autoinducers are often structurally similar, raising questions concerning how bacteria distinguish among them. Here, we use the Pseudomonas aeruginosa LasR quorum-sensing receptor to explore signal discrimination. The cognate autoinducer, 3OC 12 homoserine lactone (3OC 12 HSL), is a more potent activator of LasR than other homoserine lactones. However, other homoserine lactones can elicit LasR-dependent quorum-sensing responses, showing that LasR displays ligand promiscuity. We identify mutants that alter which homoserine lactones LasR detects. Substitution at residue S129 decreases the LasR response to 3OC 12 HSL, while enhancing discrimination against noncognate autoinducers. Conversely, the LasR L130F mutation increases the potency of 3OC 12 HSL and other homoserine lactones. We solve crystal structures of LasR ligand-binding domains complexed with noncognate autoinducers. Comparison with existing structures reveals that ligand selectivity/sensitivity is mediated by a flexible loop near the ligand-binding site. We show that LasR variants with modified ligand preferences exhibit altered quorum-sensing responses to autoinducers in vivo. We suggest that possessing some ligand promiscuity endows LasR with the ability to optimally regulate quorum-sensing traits., Competing Interests: The authors declare no conflict of interest.

Published

2019

9. 2,4-Diamino-8-quinazoline carboxamides as novel, potent inhibitors of the NAD hydrolyzing enzyme CD38: Exploration of the 2-position structure-activity relationships.

Author

Deaton DN, Haffner CD, Henke BR, Jeune MR, Shearer BG, Stewart EL, Stuart JD, and Ulrich JC

Subjects

ADP-ribosyl Cyclase 1 metabolism, Amides metabolism, Amides pharmacokinetics, Animals, Binding Sites, Enzyme Inhibitors metabolism, Enzyme Inhibitors pharmacokinetics, Half-Life, Humans, Mice, Molecular Docking Simulation, NAD chemistry, Protein Structure, Tertiary, Structure-Activity Relationship, ADP-ribosyl Cyclase 1 antagonists & inhibitors, Amides chemistry, Enzyme Inhibitors chemistry, NAD metabolism, Quinazolines chemistry

Abstract

Starting from 4-amino-8-quinoline carboxamide lead 1a and scaffold hopping to the chemically more tractable quinazoline, a systematic exploration of the 2-substituents of the quinazoline ring, utilizing structure activity relationships and conformational constraint, resulted in the identification of 39 novel CD38 inhibitors. Eight of these analogs were 10-100-fold more potent human CD38 inhibitors, including the single digit nanomolar inhibitor 1am. Several of these molecules also exhibited improved therapeutic indices relative to hERG activity. A representative analog 1r exhibited suitable pharmacokinetic parameters for in vivo animal studies, including moderate clearance and good oral bioavailability. These inhibitor compounds will aid in the exploration of the enzymatic functions of CD38, as well as furthering the study of the therapeutic implications of NAD enhancement in metabolic disease models., (Copyright © 2018 Elsevier Ltd. All rights reserved.)

Published

2018

10. Flavonoids Suppress Pseudomonas aeruginosa Virulence through Allosteric Inhibition of Quorum-sensing Receptors.

Author

Paczkowski JE, Mukherjee S, McCready AR, Cong JP, Aquino CJ, Kim H, Henke BR, Smith CD, and Bassler BL

Subjects

Allosteric Regulation, Biofilms drug effects, Biofilms growth & development, Pseudomonas aeruginosa growth & development, Quorum Sensing drug effects, Small Molecule Libraries pharmacology, Structure-Activity Relationship, Bacterial Proteins antagonists & inhibitors, Flavonoids pharmacology, Pseudomonas aeruginosa drug effects, Quorum Sensing physiology, Trans-Activators antagonists & inhibitors, Virulence drug effects

Abstract

Quorum sensing is a process of cell-cell communication that bacteria use to regulate collective behaviors. Quorum sensing depends on the production, detection, and group-wide response to extracellular signal molecules called autoinducers. In many bacterial species, quorum sensing controls virulence factor production. Thus, disrupting quorum sensing is considered a promising strategy to combat bacterial pathogenicity. Several members of a family of naturally produced plant metabolites called flavonoids inhibit Pseudomonas aeruginosa biofilm formation by an unknown mechanism. Here, we explore this family of molecules further, and we demonstrate that flavonoids specifically inhibit quorum sensing via antagonism of the autoinducer-binding receptors, LasR and RhlR. Structure-activity relationship analyses demonstrate that the presence of two hydroxyl moieties in the flavone A-ring backbone are essential for potent inhibition of LasR/RhlR. Biochemical analyses reveal that the flavonoids function non-competitively to prevent LasR/RhlR DNA binding. Administration of the flavonoids to P. aeruginosa alters transcription of quorum sensing-controlled target promoters and suppresses virulence factor production, confirming their potential as anti-infectives that do not function by traditional bacteriocidal or bacteriostatic mechanisms., (© 2017 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2017

11. Discovery of Novel Small Molecules that Activate Satellite Cell Proliferation and Enhance Repair of Damaged Muscle.

Author

Billin AN, Bantscheff M, Drewes G, Ghidelli-Disse S, Holt JA, Kramer HF, McDougal AJ, Smalley TL, Wells CI, Zuercher WJ, and Henke BR

Subjects

3T3 Cells, Animals, Cells, Cultured, Drug Discovery, Humans, Mice, Muscle, Skeletal cytology, Muscle, Skeletal injuries, Pyrimidines pharmacokinetics, Stem Cells cytology, Stem Cells drug effects, Cell Proliferation drug effects, Muscle, Skeletal drug effects, Muscle, Skeletal physiology, Pyrimidines chemistry, Pyrimidines pharmacology, Regeneration drug effects

Abstract

Skeletal muscle progenitor stem cells (referred to as satellite cells) represent the primary pool of stem cells in adult skeletal muscle responsible for the generation of new skeletal muscle in response to injury. Satellite cells derived from aged muscle display a significant reduction in regenerative capacity to form functional muscle. This decrease in functional recovery has been attributed to a decrease in proliferative capacity of satellite cells. Hence, agents that enhance the proliferative abilities of satellite cells may hold promise as therapies for a variety of pathological settings, including repair of injured muscle and age- or disease-associated muscle wasting. Through phenotypic screening of isolated murine satellite cells, we identified a series of 2,4-diaminopyrimidines (e.g., 2) that increased satellite cell proliferation. Importantly, compound 2 was effective in accelerating repair of damaged skeletal muscle in an in vivo mouse model of skeletal muscle injury. While these compounds were originally prepared as c-Jun N-terminal kinase 1 (JNK-1) inhibitors, structure-activity analyses indicated JNK-1 inhibition does not correlate with satellite cell activity. Screening against a broad panel of kinases did not result in identification of an obvious molecular target, so we conducted cell-based proteomics experiments in an attempt to identify the molecular target(s) responsible for the potentiation of the satellite cell proliferation. These data provide the foundation for future efforts to design improved small molecules as potential therapeutics for muscle repair and regeneration.

Published

2016

12. Elimination of a cholecystokinin receptor agonist 'trigger' in an effort to develop positive allosteric modulators without intrinsic agonist activity.

Author

Desai AJ, Henke BR, and Miller LJ

Subjects

Animals, Benzodiazepines chemistry, CHO Cells, Cricetulus, Dose-Response Relationship, Drug, Humans, Molecular Structure, Structure-Activity Relationship, Allosteric Regulation drug effects, Benzodiazepines pharmacology, Receptors, Cholecystokinin agonists

Abstract

Cholecystokinin (CCK) acts at the type 1 cholecystokinin receptor (CCK1R) to elicit satiety and is a well-established drug target for obesity. To date, small molecule agonists have been developed, but have failed to demonstrate adequate efficacy in clinical trials, and concerns about side effects and potential toxicity have limited further development of full agonists. The use of positive allosteric modulators (PAMs) without intrinsic agonist activity that are active only for a brief period of time after a meal might represent a safer alternative. Here, we propose a possible novel strategy to develop such compounds by modifying the agonist 'trigger' of an existing small molecule agonist. We have studied analogues of the 1,5-benzodiazepine agonist, GI181771X, in which the N1-isopropyl agonist 'trigger' was modified. While agonist activity was greatly reduced in these compounds, they acted as negative, rather than positive modulators. The parent drug was also found to exhibit no positive modulation of CCK action. Receptor structure-activity relationship studies demonstrated that the mode of docking these derivatives was distinct from that of the parent compound, perhaps explaining their action as negative allosteric modulators. We conclude that this outcome is likely characteristic of the parental agonist, and that this strategy may be more successfully utilized with a parental ago-PAM, possessing intrinsic positive modulatory activity., (Copyright © 2015 Elsevier Ltd. All rights reserved.)

Published

2015

13. Discovery, Synthesis, and Biological Evaluation of Thiazoloquin(az)olin(on)es as Potent CD38 Inhibitors.

Author

Haffner CD, Becherer JD, Boros EE, Cadilla R, Carpenter T, Cowan D, Deaton DN, Guo Y, Harrington W, Henke BR, Jeune MR, Kaldor I, Milliken N, Petrov KG, Preugschat F, Schulte C, Shearer BG, Shearer T, Smalley TL Jr, Stewart EL, Stuart JD, and Ulrich JC

Subjects

ADP-ribosyl Cyclase 1 metabolism, Animals, Cell Line, Dogs, Drug Discovery, Humans, Liver drug effects, Liver metabolism, Mice, Inbred C57BL, Molecular Docking Simulation, Muscles drug effects, Muscles metabolism, NAD analysis, NAD blood, NAD metabolism, Obesity drug therapy, Obesity metabolism, Quinolones chemical synthesis, Quinolones pharmacokinetics, Thiazoles chemical synthesis, Thiazoles pharmacokinetics, ADP-ribosyl Cyclase 1 antagonists & inhibitors, Quinolones chemistry, Quinolones pharmacology, Thiazoles chemistry, Thiazoles pharmacology

Abstract

A series of thiazoloquin(az)olinones were synthesized and found to have potent inhibitory activity against CD38. Several of these compounds were also shown to have good pharmacokinetic properties and demonstrated the ability to elevate NAD levels in plasma, liver, and muscle tissue. In particular, compound 78c was given to diet induced obese (DIO) C57Bl6 mice, elevating NAD > 5-fold in liver and >1.2-fold in muscle versus control animals at a 2 h time point. The compounds described herein possess the most potent CD38 inhibitory activity of any small molecules described in the literature to date. The inhibitors should allow for a more detailed assessment of how NAD elevation via CD38 inhibition affects physiology in NAD deficient states.

Published

2015

14. Molecular basis for benzodiazepine agonist action at the type 1 cholecystokinin receptor.

Author

Harikumar KG, Cawston EE, Lam PCH, Patil A, Orry A, Henke BR, Abagyan R, Christopoulos A, Sexton PM, and Miller LJ

Subjects

Amino Acid Sequence, Animals, Benzodiazepines chemistry, CHO Cells, Cricetinae, Cricetulus, Models, Molecular, Molecular Sequence Data, Mutant Proteins agonists, Mutant Proteins chemistry, Mutant Proteins metabolism, ROC Curve, Receptor, Cholecystokinin A chemistry, Receptor, Cholecystokinin A metabolism, Receptor, Cholecystokinin B chemistry, Receptor, Cholecystokinin B metabolism, Recombinant Proteins agonists, Recombinant Proteins chemistry, Recombinant Proteins metabolism, Sequence Alignment, Benzodiazepines pharmacology, Receptor, Cholecystokinin A agonists

Abstract

Understanding the molecular basis of drug action can facilitate development of more potent and selective drugs. Here, we explore the molecular basis for action of a unique small molecule ligand that is a type 1 cholecystokinin (CCK) receptor agonist and type 2 CCK receptor antagonist, GI181771X. We characterize its binding utilizing structurally related radioiodinated ligands selective for CCK receptor subtypes that utilize the same allosteric ligand-binding pocket, using wild-type receptors and chimeric constructs exchanging the distinct residues lining this pocket. Intracellular calcium assays were performed to determine biological activity. Molecular models for docking small molecule agonists to the type 1 CCK receptor were developed using a ligand-guided refinement approach. The optimal model was distinct from the previous antagonist model for the same receptor and was mechanistically consistent with the current mutagenesis data. This study revealed a key role for Leu(7.39) that was predicted to interact with the isopropyl group in the N1 position of the benzodiazepine that acts as a "trigger" for biological activity. The molecular model was predictive of binding of other small molecule agonists, effectively distinguishing these from 1065 approved drug decoys with an area under curve value of 99%. The model also selectively enriched for agonist compounds, with 130 agonists identified by ROC analysis when seeded in 2175 non-agonist ligands of the type 1 CCK receptor (area under curve 78%). Benzodiazepine agonists in this series docked in consistent pose within this pocket, with a key role played by Leu(7.39), whereas the role of this residue was less clear for chemically distinct agonists.

Published

2013

15. PPAR modulators and PPAR pan agonists for metabolic diseases: the next generation of drugs targeting peroxisome proliferator-activated receptors?

Author

Feldman PL, Lambert MH, and Henke BR

Subjects

Drug Delivery Systems, Drug-Related Side Effects and Adverse Reactions, Humans, Peroxisome Proliferator-Activated Receptors agonists, Peroxisome Proliferator-Activated Receptors chemistry, Protein Binding, Metabolic Diseases drug therapy, Peroxisome Proliferator-Activated Receptors drug effects

Abstract

The Peroxisome Proliferator-Activated Receptors-PPAR alpha, PPAR gamma, and PPAR delta--are members of the nuclear receptor gene family that have emerged as therapeutic targets for the development of drugs to treat human metabolic diseases. The discovery of high affinity, subtype-selective agonists for each of the three PPAR subtypes has allowed elucidation of the pharmacology of these receptors and development of first-generation therapeutic agents for the treatment of diabetes and dyslipidemia. However, despite proven therapeutic benefits of selective PPAR agonists, safety concerns and dose-limiting side effects have been observed, and a number of late-stage development failures have been reported. Scientists have continued to explore ligand-based activation of PPARs in hopes of developing safer and more effective drugs. This review highlights recent efforts on two newer approaches, the simultaneous activation of all three PPAR receptors with a single ligand (PPAR pan agonists) and the selective modulation of a single PPAR receptor in a cell or tissue specific manner (selective PPAR modulator or SPPARM) in order to induce a subset of target genes and affect a restricted number of metabolic pathways.

Published

2008

16. Glycogen phosphorylase inhibitors.

Author

Henke BR and Sparks SM

Subjects

Diabetes Mellitus, Type 2 drug therapy, Enzyme Inhibitors therapeutic use, Glucose metabolism, Glycogen metabolism, Humans, Hyperglycemia drug therapy, Hyperglycemia enzymology, Hypoglycemic Agents therapeutic use, Liver metabolism, Diabetes Mellitus, Type 2 enzymology, Enzyme Inhibitors pharmacology, Glycogen Phosphorylase antagonists & inhibitors, Hypoglycemic Agents pharmacology, Liver drug effects

Abstract

Type 2 diabetes is a complex metabolic disease with hyperglycemia as its recognizable hallmark. Hepatic glucose output is elevated in Type 2 diabetic patients, and evidence suggests drugs which lower hepatic glucose production are effective antihyperglycemic agents. Glycogenolysis, which is the release of monomeric glucose from its polymeric storage form called glycogen, is a key contributor to hepatic glucose output. Glycogen phosphorylase is the enzyme that catalyzes this process. This review covers advances in the design of small molecule inhibitors of this enzyme, their biological activity, and their potential as effective antihyperglycemic agents for the treatment of Type 2 diabetes.

Published

2006

17. Synthesis and biodistribution of (11)C-GW7845, a positron-emitting agonist for peroxisome proliferator-activated receptor-{gamma}.

Author

Mathews WB, Foss CA, Stoermer D, Ravert HT, Dannals RF, Henke BR, and Pomper MG

Subjects

Animals, Carbon Radioisotopes chemistry, Carbon Radioisotopes pharmacokinetics, Female, Isotope Labeling methods, Male, Metabolic Clearance Rate, Mice, Mice, SCID, Organ Specificity, Oxazoles chemistry, Radiopharmaceuticals chemical synthesis, Radiopharmaceuticals pharmacokinetics, Tissue Distribution, Tyrosine chemistry, Tyrosine pharmacokinetics, Breast Neoplasms diagnostic imaging, Breast Neoplasms metabolism, Oxazoles pharmacokinetics, PPAR gamma agonists, PPAR gamma metabolism, Positron-Emission Tomography methods, Tyrosine analogs & derivatives

Abstract

Unlabelled: The goal of this study was to synthesize and evaluate in vivo the peroxisome proliferator-activated receptor-gamma (PPARgamma) agonist (11)C-GW7845 ((S)-2-(1-carboxy-2-{4-[2-(5-methyl-2-phenyloxazol-4-yl)ethoxy]phenyl}ethylamino)benzoic acid methyl ester) ((11)C-compound 1). PPARgamma is a member of a family of nuclear receptors that plays a central role in the control of lipid and glucose metabolism. Compound 1 is an analog of tyrosine (inhibitor constant, 3.7 nmol/L), which is an inhibitor of experimental mammary carcinogenesis., Methods: Protection of the carboxylic acid moiety of compound 1 was effected by treatment with N,N-dimethylformamide di-tert-butyl acetal to provide compound 2. Hydrolysis of the carbomethoxy group of compound 2 provided the benzoic acid (compound 3) that served as an immediate precursor to radiolabeling. Compound 3 underwent treatment with (11)C-methyl iodide followed by high-performance liquid chromatography to produce a radioactive peak sample that coeluted with a standard sample of compound 1. Analysis of biodistribution was undertaken by injecting male CD-1 mice via the tail vein with 6.03 MBq (163 microCi, 2.55 microg/kg) of (11)C-compound 1. To determine the tumor uptake of the radiotracer, 6 female SCID mice bearing MCF-7 xenografts were injected via the tail vein with 10.5 MBq (283 microCi, 0.235 microg/kg) of (11)C-compound 1., Results: (11)C-Compound 1 was synthesized at an 8% radiochemical yield in 29 min with an average specific radioactivity of 1,222 GBq/micromol (33,024 mCi/micromol; n = 6) at the end of synthesis. Spleen (target)-to-muscle uptake and tumor-to-muscle uptake ratios were 3.1 and 1.5, respectively, but this uptake could not be blocked with unlabeled compound 1 at 2 mg/kg., Conclusion: Further structural modification, perhaps to generate a less lipophilic tyrosine analog, will be necessary to enable receptor-mediated PPARgamma imaging by this class of agents.

Published

2005

18. Recent advances in estrogen receptor modulators.

Author

Henke BR and Heyer D

Subjects

Animals, Humans, Ligands, Receptors, Estrogen agonists, Receptors, Estrogen antagonists & inhibitors, Receptors, Estrogen drug effects, Selective Estrogen Receptor Modulators therapeutic use, Selective Estrogen Receptor Modulators pharmacology

Abstract

Modulation of estrogen action is an effective treatment for alleviating the symptoms associated with menopause, and also provides an alternative to ablative surgery for the treatment of breast cancer. The side effects associated with the currently used estrogen receptor-modulating drugs have resulted in the pursuit of agents with an improved therapeutic profile. Recent advances in understanding the molecular determinants of estrogen receptor signaling have contributed to the continued discovery and development of novel chemical compounds designed to exploit this knowledge. This review focuses on the recent clinical and preclinical development of novel classes of ligands that modulate the two estrogen receptor subtypes.

Published

2005

19. Peroxisome proliferator-activated receptor alpha/gamma dual agonists for the treatment of type 2 diabetes.

Author

Henke BR

Subjects

Animals, Diabetes Mellitus, Type 2 complications, Diabetes Mellitus, Type 2 metabolism, Humans, Hyperglycemia metabolism, Hypoglycemic Agents chemistry, Hypoglycemic Agents therapeutic use, Models, Molecular, Molecular Structure, Receptors, Cytoplasmic and Nuclear chemistry, Transcription Factors chemistry, Diabetes Mellitus, Type 2 drug therapy, Hypoglycemic Agents pharmacology, Receptors, Cytoplasmic and Nuclear agonists, Transcription Factors agonists

Published

2004

20. 1. Peroxisome proliferator-activated receptor gamma (PPARgamma) ligands and their therapeutic utility.

Author

Henke BR

Subjects

Alzheimer Disease drug therapy, Arteriosclerosis drug therapy, Diabetes Mellitus drug therapy, Humans, Hypertension drug therapy, Hypoglycemic Agents therapeutic use, Ligands, Neoplasms drug therapy, Peroxisome Proliferator-Activated Receptors therapeutic use, Protein Structure, Tertiary, Thiazolidinediones therapeutic use, PPAR gamma metabolism, Peroxisome Proliferator-Activated Receptors metabolism

Published

2004

21. A new series of estrogen receptor modulators that display selectivity for estrogen receptor beta.

Author

Henke BR, Consler TG, Go N, Hale RL, Hohman DR, Jones SA, Lu AT, Moore LB, Moore JT, Orband-Miller LA, Robinett RG, Shearin J, Spearing PK, Stewart EL, Turnbull PS, Weaver SL, Williams SP, Wisely GB, and Lambert MH

Subjects

Crystallography, X-Ray, Estrogen Receptor alpha, Estrogen Receptor beta, Genes, Reporter, Humans, Ligands, Models, Molecular, Radioligand Assay, Receptors, Estrogen agonists, Receptors, Estrogen antagonists & inhibitors, Receptors, Estrogen genetics, Stereoisomerism, Structure-Activity Relationship, Transcription, Genetic, Triazines chemistry, Triazines pharmacology, Tumor Cells, Cultured, Receptors, Estrogen drug effects, Triazines chemical synthesis

Abstract

A series of 1,3,5-triazine-based estrogen receptor (ER) modulators that are modestly selective for the ERbeta subtype are reported. Compound 1, which displayed modest potency and selectivity for ERbeta vs ERalpha, was identified via high-throughput screening utilizing an ERbeta SPA-based binding assay. Subsequent analogue preparation resulted in the identification of compounds such as 21 and 43 that display 25- to 30-fold selectivity for ERbeta with potencies in the 10-30 nM range. These compounds profile as full antagonists at ERbeta and weak partial agonists at ERalpha in a cell-based reporter gene assay. In addition, the X-ray crystal structure of compound 15 complexed with the ligand binding domain of ERbeta has been solved and was utilized in the design of more conformationally restrained analogues such as 31 in an attempt to increase selectivity for the ERbeta subtype.

Published

2002

22. Synthesis and biological activity of L-tyrosine-based PPARgamma agonists with reduced molecular weight.

Author

Liu KG, Lambert MH, Ayscue AH, Henke BR, Leesnitzer LM, Oliver WR Jr, Plunket KD, Xu HE, Sternbach DD, and Willson TM

Subjects

Animals, Diabetes Mellitus, Experimental drug therapy, Hypoglycemic Agents chemistry, Hypoglycemic Agents therapeutic use, Male, Molecular Weight, Rats, Rats, Zucker, Hypoglycemic Agents chemical synthesis, Hypoglycemic Agents pharmacology, Receptors, Cytoplasmic and Nuclear agonists, Transcription Factors agonists, Tyrosine chemical synthesis

Abstract

A series of PPARgamma agonists were synthesized from L-tyrosine that incorporated low molecular weight N-substituents. The most potent analogue, pyrrole (4e), demonstrated a K(i) of 6.9nM and an EC(50) of 4.7nM in PPARgamma binding and functional assays, respectively. Pyrrole (4e), which is readily synthesized from L-tyrosine methyl ester in four steps, also demonstrated in vivo activity in a rodent model of Type 2 diabetes.

Published

2001

23. Identification of a series of oxadiazole-substituted alpha-isopropoxy phenylpropanoic acids with activity on PPARalpha, PPARgamma, and PPARdelta.

Author

Liu KG, Smith JS, Ayscue AH, Henke BR, Lambert MH, Leesnitzer LM, Plunket KD, Willson TM, and Sternbach DD

Subjects

Chromatography, High Pressure Liquid, Drug Design, Drug Evaluation, Preclinical, Humans, Isomerism, Oxadiazoles chemistry, Structure-Activity Relationship, Receptors, Cytoplasmic and Nuclear agonists, Transcription Factors agonists

Abstract

A series of oxadiazole-substituted alpha-isopropoxy phenylpropanoic acids with dual agonist activity on PPARalpha and PPARgamma is described. Several of these compounds also showed partial agonist activity on PPARdelta. Resolution of one analogue showed that PPARalpha and PPARgamma activity resided in mainly one enantiomer, whereas PPARdelta activity was retained in both enantiomers.

Published

2001

24. 2-Amino-4,6-diarylpyridines as novel ligands for the estrogen receptor.

Author

Henke BR, Drewry DH, Jones SA, Stewart EL, Weaver SL, and Wiethe RW

Subjects

Bacteria genetics, Bacteria metabolism, Binding Sites physiology, Crystallography, X-Ray, Estrogen Receptor alpha, Estrogen Receptor beta, Humans, Ligands, Protein Binding physiology, Pyridines chemical synthesis, Pyridines metabolism, Raloxifene Hydrochloride metabolism, Sensitivity and Specificity, Receptors, Estrogen metabolism, Selective Estrogen Receptor Modulators chemical synthesis, Selective Estrogen Receptor Modulators pharmacology

Abstract

We have prepared a novel series of 2-amino-4,6-diarylpyridines that function as ligands of estrogen receptor alpha (ERalpha) and estrogen receptor beta (ERbeta). These compounds bind to both ERalpha and ERbeta with a modest selectivity for the alpha subtype. The most potent of these analogues, compound 19, has a K(i)=20nM at ERalpha. These molecules represent a novel template for designing potentially useful ligands for the estrogen receptor.

Published

2001

25. The PPARs: from orphan receptors to drug discovery.

Author

Willson TM, Brown PJ, Sternbach DD, and Henke BR

Subjects

Animals, Diabetes Mellitus drug therapy, Diabetes Mellitus metabolism, Humans, Hyperlipidemias drug therapy, Hyperlipidemias metabolism, Hypertension drug therapy, Hypertension metabolism, Inflammation drug therapy, Inflammation metabolism, Ligands, Models, Molecular, Neoplasms drug therapy, Neoplasms metabolism, Obesity drug therapy, Obesity metabolism, Receptors, Cytoplasmic and Nuclear chemistry, Receptors, Cytoplasmic and Nuclear metabolism, Transcription Factors chemistry, Transcription Factors metabolism, Drug Design, Nuclear Proteins physiology, Receptors, Cytoplasmic and Nuclear drug effects, Receptors, Cytoplasmic and Nuclear physiology, Transcription Factors drug effects, Transcription Factors physiology

Published

2000

26. Synthesis and biological activity of a novel series of indole-derived PPARgamma agonists.

Author

Henke BR, Adkison KK, Blanchard SG, Leesnitzer LM, Mook RA Jr, Plunket KD, Ray JA, Roberson C, Unwalla R, and Willson TM

Subjects

Animals, Biological Availability, Humans, Indoles pharmacokinetics, Rats, Structure-Activity Relationship, Indoles chemical synthesis, Indoles pharmacology, Receptors, Cytoplasmic and Nuclear agonists, Transcription Factors agonists

Abstract

The synthesis and structure-activity relationships of a novel series of indole 5-carboxylic acids that bind and activate peroxisome proliferator-activated receptor gamma (PPARgamma) are reported. These new analogs are selective for PPARgamma vs the other PPAR subtypes, and the most potent compounds in this series are comparable to in vitro potencies at PPARgamma reported for the thiazolidinedione-based antidiabetic drugs currently in clinical use.

Published

1999

27. A novel N-aryl tyrosine activator of peroxisome proliferator-activated receptor-gamma reverses the diabetic phenotype of the Zucker diabetic fatty rat.

Author

Brown KK, Henke BR, Blanchard SG, Cobb JE, Mook R, Kaldor I, Kliewer SA, Lehmann JM, Lenhard JM, Harrington WW, Novak PJ, Faison W, Binz JG, Hashim MA, Oliver WO, Brown HR, Parks DJ, Plunket KD, Tong WQ, Menius JA, Adkison K, Noble SA, and Willson TM

Subjects

Animals, Chromans therapeutic use, Clone Cells, Diabetes Mellitus, Experimental genetics, Glucose Clamp Technique, Humans, Hypoglycemic Agents therapeutic use, Immunohistochemistry, Logistic Models, Obesity genetics, Phenotype, Rats, Rats, Zucker, Receptors, Cytoplasmic and Nuclear agonists, Thiazoles therapeutic use, Transcription Factors agonists, Troglitazone, Tyrosine pharmacology, Benzophenones pharmacology, Diabetes Mellitus, Experimental physiopathology, Obesity physiopathology, Receptors, Cytoplasmic and Nuclear metabolism, Thiazolidinediones, Transcription Factors metabolism, Tyrosine analogs & derivatives

Abstract

The discovery that peroxisome proliferator-activated receptor (PPAR)-gamma was the molecular target of the thiazolidinedione class of antidiabetic agents suggested a key role for PPAR-gamma in the regulation of carbohydrate and lipid metabolism. Through the use of high-throughput biochemical assays, GW1929, a novel N-aryl tyrosine activator of human PPAR-gamma, was identified. Chronic oral administration of GW1929 or troglitazone to Zucker diabetic fatty (ZDF) rats resulted in dose-dependent decreases in daily glucose, free fatty acid, and triglyceride exposure compared with pretreatment values, as well as significant decreases in glycosylated hemoglobin. Whole body insulin sensitivity, as determined by the euglycemic-hyperinsulinemic clamp technique, was significantly increased in treated animals. Comparison of the magnitude of glucose lowering as a function of serum drug concentrations showed that GW1929 was 2 orders of magnitude more potent than troglitazone in vivo. These data were consistent with the relative in vitro potencies of GW1929 and troglitazone. Isolated perfused pancreas studies performed at the end of the study confirmed that pancreata from vehicle-treated rats showed no increase in insulin secretion in response to a step change in glucose from 3 to 10 mmol/l. In contrast, pancreata from animals treated with GW1929 showed a first- and second-phase insulin secretion pattern. Consistent with the functional data from the perfusion experiments, animals treated with the PPAR-gamma agonist had more normal islet architecture with preserved insulin staining compared with vehicle-treated ZDF rats. This is the first demonstration of in vivo efficacy of a novel nonthiazolidinedione identified as a high-affinity ligand for human PPAR-gamma. The increased potency of GW1929 compared with troglitazone both in vitro and in vivo may translate into improved clinical efficacy when used as monotherapy in type 2 diabetic patients. In addition, the significant improvement in daily meal tolerance may impact cardiovascular risk factor management in these patients.

Published

1999

28. N-(2-Benzoylphenyl)-L-tyrosine PPARgamma agonists. 2. Structure-activity relationship and optimization of the phenyl alkyl ether moiety.

Author

Collins JL, Blanchard SG, Boswell GE, Charifson PS, Cobb JE, Henke BR, Hull-Ryde EA, Kazmierski WM, Lake DH, Leesnitzer LM, Lehmann J, Lenhard JM, Orband-Miller LA, Gray-Nunez Y, Parks DJ, Plunkett KD, and Tong WQ

Subjects

Adipocytes cytology, Adipocytes drug effects, Animals, Cell Differentiation drug effects, Cell Line, Humans, Hypoglycemic Agents chemistry, Hypoglycemic Agents pharmacology, Hypolipidemic Agents chemistry, Hypolipidemic Agents pharmacology, Ligands, Lipids biosynthesis, Mice, Oxazoles chemistry, Oxazoles pharmacology, Propionates chemistry, Propionates pharmacology, Radioligand Assay, Receptors, Cytoplasmic and Nuclear metabolism, Recombinant Fusion Proteins agonists, Recombinant Fusion Proteins metabolism, Solubility, Structure-Activity Relationship, Thiazoles chemistry, Thiazoles pharmacology, Transcription Factors metabolism, Transfection, Tyrosine chemistry, Tyrosine pharmacology, DNA-Binding Proteins agonists, Hypoglycemic Agents chemical synthesis, Hypolipidemic Agents chemical synthesis, Oxazoles chemical synthesis, Propionates chemical synthesis, Receptors, Cytoplasmic and Nuclear agonists, Thiazoles chemical synthesis, Transcription Factors agonists, Tyrosine analogs & derivatives, Tyrosine chemical synthesis

Abstract

We previously reported the identification of (2S)-((2-benzoylphenyl)amino)-3-¿4-[2-(5-methyl-2-phenyloxazol-4-y l)e thoxy]phenyl¿propanoic acid (2) (PPARgamma pKi = 8.94, PPARgamma pEC50 = 9.47) as a potent and selective PPARgamma agonist. We now report the expanded structure-activity relationship around the phenyl alkyl ether moiety by pursuing both a classical medicinal chemistry approach and a solid-phase chemistry approach for analogue synthesis. The solution-phase strategy focused on evaluating the effects of oxazole and phenyl ring replacements of the 2-(5-methyl-2-phenyloxazol-4-yl)ethyl side chain of 2 with several replacements providing potent and selective PPARgamma agonists with improved aqueous solubility. Specifically, replacement of the phenyl ring of the phenyloxazole moiety with a 4-pyridyl group to give 2(S)-((2-benzoylphenyl)amino)-3-¿4-[2-(5-methyl-2-pyridin-4-yloxazol+ ++- 4-yl)ethoxy]phenyl¿propionic acid (16) (PPARgamma pKi = 8.85, PPARgamma pEC50 = 8.74) or a 4-methylpiperazine to give 2(S)-((2-benzoylphenyl)amino)-3-(4-¿2-[5-methyl-2-(4-methylpiperazin+ ++- 1-yl)thiazol-4-yl]ethoxy¿phenyl)propionic acid (24) (PPARgamma pKi = 8.66, PPARgamma pEC50 = 8.89) provided two potent and selective PPARgamma agonists with increased solubility in pH 7.4 phosphate buffer and simulated gastric fluid as compared to 2. The second strategy took advantage of the speed and ease of parallel solid-phase analogue synthesis to generate a more diverse set of phenyl alkyl ethers which led to the identification of a number of novel, high-affinity PPARgamma ligands (PPARgamma pKi's 6.98-8.03). The combined structure-activity data derived from the two strategies provide valuable insight on the requirements for PPARgamma binding, functional activity, selectivity, and aqueous solubility.

Published

1998

29. N-(2-Benzoylphenyl)-L-tyrosine PPARgamma agonists. 3. Structure-activity relationship and optimization of the N-aryl substituent.

Author

Cobb JE, Blanchard SG, Boswell EG, Brown KK, Charifson PS, Cooper JP, Collins JL, Dezube M, Henke BR, Hull-Ryde EA, Lake DH, Lenhard JM, Oliver W Jr, Oplinger J, Pentti M, Parks DJ, Plunket KD, and Tong WQ

Subjects

Administration, Oral, Animals, Benzoates chemistry, Benzoates pharmacology, Blood Glucose metabolism, Cell Line, Diabetes Mellitus, Experimental blood, Humans, Hypoglycemic Agents chemistry, Hypoglycemic Agents pharmacology, Hypolipidemic Agents chemistry, Hypolipidemic Agents pharmacology, Ligands, Lipids biosynthesis, Male, Mice, Oxazoles chemistry, Oxazoles pharmacology, Radioligand Assay, Rats, Receptors, Cytoplasmic and Nuclear metabolism, Solubility, Structure-Activity Relationship, Transcription Factors metabolism, Tyrosine chemistry, Tyrosine pharmacology, ortho-Aminobenzoates, Benzoates chemical synthesis, DNA-Binding Proteins agonists, Hypoglycemic Agents chemical synthesis, Hypolipidemic Agents chemical synthesis, Oxazoles chemical synthesis, Receptors, Cytoplasmic and Nuclear agonists, Transcription Factors agonists, Tyrosine analogs & derivatives, Tyrosine chemical synthesis

Abstract

3-¿4-[2-(Benzoxazol-2-ylmethylamino)ethoxy]phenyl¿-(2S)-((2- benzoylph enyl)amino)propionic acid (1) and (2S)-((2-benzoylphenyl)amino)-3-¿4-[2-(5-methyl-2-phenyloxazol-4-y l)e thoxy]phenyl¿propionic acid (2) are peroxisome proliferator-activated receptor gamma (PPARgamma) agonists and have antidiabetic activity in rodent models of type 2 diabetes. As part of an effort to develop the SAR of the N-2-benzoylphenyl moiety of 1 and 2, a series of novel carboxylic acid analogues, 23-66, modified only in the N-2-benzoylphenyl moiety were synthesized from L-tyrosine and evaluated as PPARgamma agonists. In general, only modest changes in the N-2-benzoylphenyl moiety of 1 and 2 are tolerated. More specifically, the best changes involve bioisosteric replacement of one of the two phenyl rings of this moiety. Addition of substituents to this moiety generally produced compounds that are less active in the cell-based functional assays of PPARgamma activity although binding affinity to PPARgamma may be maintained. A particularly promising set of analogues is the anthranilic acid esters 63-66 in which the phenyl ring in the 2-benzoyl group of 1 and 2 has been replaced by an alkoxy group. In particular, (S)-2-(1-carboxy-2-¿4-[2-(5-methyl-2-phenyloxazol-4-yl)ethoxy]phen yl¿ ethylamino)benzoic acid methyl ester (63) has a pKi of 8.43 in the binding assay using human PPARgamma ligand binding domain and a pEC50 of 9.21 in the in vitro murine lipogenesis functional assay of PPARgamma activity. Finally, 63 was found to normalize glycemia when dosed at 3 mg/kg bid po in the Zucker diabetic fatty rat model of type 2 diabetes.

Published

1998

30. N-(2-Benzoylphenyl)-L-tyrosine PPARgamma agonists. 1. Discovery of a novel series of potent antihyperglycemic and antihyperlipidemic agents.

Author

Henke BR, Blanchard SG, Brackeen MF, Brown KK, Cobb JE, Collins JL, Harrington WW Jr, Hashim MA, Hull-Ryde EA, Kaldor I, Kliewer SA, Lake DH, Leesnitzer LM, Lehmann JM, Lenhard JM, Orband-Miller LA, Miller JF, Mook RA Jr, Noble SA, Oliver W Jr, Parks DJ, Plunket KD, Szewczyk JR, and Willson TM

Subjects

Administration, Oral, Aminopyridines chemistry, Aminopyridines pharmacology, Animals, Blood Glucose metabolism, Cell Line, Diabetes Mellitus, Experimental blood, Humans, Hypoglycemic Agents chemistry, Hypoglycemic Agents pharmacology, Hypolipidemic Agents chemistry, Hypolipidemic Agents pharmacology, Ligands, Lipids biosynthesis, Male, Mice, Oxazoles chemistry, Oxazoles pharmacology, Propionates chemistry, Propionates pharmacology, Radioligand Assay, Rats, Receptors, Cytoplasmic and Nuclear metabolism, Recombinant Fusion Proteins agonists, Recombinant Fusion Proteins metabolism, Stereoisomerism, Structure-Activity Relationship, Transcription Factors metabolism, Transfection, Tyrosine chemistry, Tyrosine pharmacology, Aminopyridines chemical synthesis, DNA-Binding Proteins agonists, Hypoglycemic Agents chemical synthesis, Hypolipidemic Agents chemical synthesis, Oxazoles chemical synthesis, Propionates chemical synthesis, Receptors, Cytoplasmic and Nuclear agonists, Transcription Factors agonists, Tyrosine analogs & derivatives, Tyrosine chemical synthesis

Abstract

We have identified a novel series of antidiabetic N-(2-benzoylphenyl)-L-tyrosine derivatives which are potent, selective PPARgamma agonists. Through the use of in vitro PPARgamma binding and functional assays (2S)-3-(4-(benzyloxy)phenyl)-2-((1-methyl-3-oxo-3-phenylpropenyl)+ ++amin o)propionic acid (2) was identified as a structurally novel PPARgamma agonist. Structure-activity relationships identified the 2-aminobenzophenone moiety as a suitable isostere for the chemically labile enaminone moiety in compound 2, affording 2-((2-benzoylphenyl)amino)-3-(4-(benzyloxy)phenyl)propionic acid (9). Replacement of the benzyl group in 9 with substituents known to confer in vivo potency in the thiazolidinedione (TZD) class of antidiabetic agents provided a dramatic increase in the in vitro functional potency and affinity at PPARgamma, affording a series of potent and selective PPARgamma agonists exemplified by (2S)-((2-benzoylphenyl)amino)-3-¿4-[2-(methylpyridin-2-ylamino+ ++)ethoxy ]phenyl¿propionic acid (18), 3-¿4-[2-(benzoxazol-2-ylmethylamino)ethoxy]phenyl¿-(2S)-((2- benzoylph enyl)amino)propanoic acid (19), and (2S)-((2-benzoylphenyl)amino)-3-¿4-[2-(5-methyl-2-phenyloxazol-4-y l)e thoxy]phenyl¿propanoic acid (20). Compounds 18 and 20 show potent antihyperglycemic and antihyperlipidemic activity when given orally in two rodent models of type 2 diabetes. In addition, these analogues are readily prepared in chiral nonracemic fashion from L-tyrosine and do not show a propensity to undergo racemization in vitro. The increased potency of these PPARgamma agonists relative to troglitazone may translate into superior clinical efficacy for the treatment of type 2 diabetes.

Published

1998

31. Optimization of 3-(1H-indazol-3-ylmethyl)-1,5-benzodiazepines as potent, orally active CCK-A agonists.

Author

Henke BR, Aquino CJ, Birkemo LS, Croom DK, Dougherty RW Jr, Ervin GN, Grizzle MK, Hirst GC, James MK, Johnson MF, Queen KL, Sherrill RG, Sugg EE, Suh EM, Szewczyk JW, Unwalla RJ, Yingling J, and Willson TM

Subjects

Administration, Oral, Alkylation, Animals, Benzodiazepines administration & dosage, Benzodiazepines pharmacology, Benzodiazepinones pharmacology, CHO Cells, Cricetinae, Devazepide, Gallbladder drug effects, Gallbladder metabolism, Guinea Pigs, Hormone Antagonists pharmacology, Indazoles administration & dosage, Indazoles pharmacology, Mice, Models, Chemical, Rats, Receptor, Cholecystokinin A, Receptor, Cholecystokinin B, Receptors, Cholecystokinin metabolism, Benzodiazepines chemistry, Indazoles chemistry, Receptors, Cholecystokinin agonists

Abstract

We previously described a series of 3-(1H-indazol-3-ylmethyl)-1,5-benzodiazepine CCK-A agonists exemplified by compound 1 (GW 5823), which is the first reported binding selective CCK-A full agonist demonstrating oral efficacy in a rat feeding model. In this report we describe analogs of compound 1 designed to explore changes to the C3 and N1 pharmacophores and their effect on agonist activity and receptor selectivity. Agonist efficacy in this series was affected by stereoelectronic factors within the C3 moiety. Binding affinity for the CCK-A vs CCK-B receptor showed little dependence on the structure of the C3 moiety but was affected by the nature of the second substituent at C3. Structure-activity relationships at the N1-anilidoacetamide "trigger" moiety within the C3 indazole series were also investigated. Both agonist efficacy and binding affinity within this series were modulated by variation of substituents on the N1-anilidoacetamide moiety. Evaluation of several analogs in an vivo mouse gallbladder emptying assay revealed compound 1 to be the most potent and efficacious of all the analogs tested. The pharmacokinetic and pharmacodynamic profile of 1 in rats is also discussed.

Published

1997

32. 3-[2-(N-phenylacetamide)]-1,5-benzodiazepines: orally active, binding selective CCK-A agonists.

Author

Willson TM, Henke BR, Momtahen TM, Myers PL, Sugg EE, Unwalla RJ, Croom DK, Dougherty RW, Grizzle MK, Johnson MF, Queen KL, Rimele TJ, Yingling JD, and James MK

Subjects

Animals, Azepines metabolism, Azepines pharmacology, Gallbladder drug effects, Gallbladder physiology, Guinea Pigs, Mice, Molecular Structure, Muscle Contraction drug effects, Receptors, Cholecystokinin metabolism, Acetanilides, Azepines chemical synthesis, Cholecystokinin agonists

Abstract

A series of modifications were made to the C-3 substituent of the 1,5-benzodiazepine CCK-A agonist 1. Replacement of the inner urea NH and addition of a methyl group to generate a C-3 quaternary carbon resulted in acetamide 6, which showed CCK-A receptor binding selectivity and sub-micromolar agonist activity in vitro. Benzodiazepine 6 was active in an in vivo mouse gallbladder emptying assay and represents a novel orally active, binding selective CCK-A agonist.

Published

1996

33. 3-(1H-indazol-3-ylmethyl)-1,5-benzodiazepines: CCK-A agonists that demonstrate oral activity as satiety agents.

Author

Henke BR, Willson TM, Sugg EE, Croom DK, Dougherty RW Jr, Queen KL, Birkemo LS, Ervin GN, Grizzle MK, Johnson MF, and James MK

Subjects

Administration, Oral, Animals, Benzodiazepines chemistry, Binding Sites, CHO Cells, Cricetinae, Gallbladder drug effects, Guinea Pigs, Humans, Mice, Structure-Activity Relationship, Benzodiazepines pharmacology, Cholecystokinin agonists, Satiety Response drug effects

Published

1996

34. 3-[4-(1,2-Diphenylbut-1-enyl)phenyl]acrylic acid: a non-steroidal estrogen with functional selectivity for bone over uterus in rats.

Author

Willson TM, Henke BR, Momtahen TM, Charifson PS, Batchelor KW, Lubahn DB, Moore LB, Oliver BB, Sauls HR, and Triantafillou JA

Subjects

Acrylates chemistry, Alkaline Phosphatase biosynthesis, Animals, Bone Density drug effects, Cell Line, Enzyme Induction drug effects, Estrogen Antagonists pharmacology, Estrogens, Non-Steroidal chemistry, Female, Humans, Organ Size drug effects, Ovariectomy, Rats, Receptors, Estrogen chemistry, Receptors, Estrogen drug effects, Receptors, Estrogen physiology, Stilbenes chemistry, Structure-Activity Relationship, Uterus anatomy & histology, Uterus enzymology, Acrylates pharmacology, Bone and Bones drug effects, Cinnamates, Estrogens, Non-Steroidal pharmacology, Stilbenes pharmacology, Uterus drug effects

Published

1994