Your search keyword '"Wexler RR"' showing total 184 results

1. Discovery and Optimization of Aryl Piperidinone Ureas as Selective Formyl Peptide Receptor 2 Agonists.

Author

Wurtz NR, Shirude PS, Cheney DL, Lupisella JA, Chattopadhyay AK, Baligar V, Seshadri B, Anjanappa P, Viet A, Valente MN, Hsu MY, Abousleiman M, Sarodaya S, Tagore DM, Dudhgaonkar S, Putlur S, Dierks EA, Ostrowski J, Wexler RR, Garcia R, and Kick EK

Abstract

We report the discovery and optimization of aryl piperidinone urea formyl peptide receptor 2 (FPR2) agonists from a weakly active high-throughput screening (HTS) hit to potent and selective agonists with favorable efficacy in acute in vivo models. A basis for the selectivity for FPR2 over FPR1 is proposed based on docking molecules into recently reported FPR2 and FPR1 cryoEM structures. Compounds from the new scaffold reported in this study exhibited superior potency and selectivity and favorable ADME profiles. Furthermore, select compounds were evaluated in an acute rat lipopolysaccharide (LPS) inflammation model and demonstrated robust dose-dependent induction of IL10, a marker for inflammation resolution, providing a valuable proof of concept for this class of FPR2 agonists., Competing Interests: The authors declare no competing financial interest., (© 2024 American Chemical Society.)

Published

2024

2. Discovery of BMS-986308: A Renal Outer Medullary Potassium Channel Inhibitor for the Treatment of Heart Failure.

Author

Richter JM, Gunaga P, Yadav N, Bora RO, Bhide R, Rajugowda N, Govindrajulu K, Godesi S, Akuthota N, Rao P, Sivaraman A, Panda M, Kaspady M, Gupta A, Mathur A, Levesque PC, Gulia J, Dokania M, Ramarao M, Kole P, Chacko S, Lentz KA, Sivaprasad Lvj S, Thatipamula RP, Sridhar S, Kamble S, Govindrajan A, Soleman SI, Gordon DA, Wexler RR, and Priestley ES

Subjects

Animals, Humans, Rats, Structure-Activity Relationship, Potassium Channels, Inwardly Rectifying antagonists & inhibitors, Potassium Channels, Inwardly Rectifying metabolism, Drug Discovery, Diuresis drug effects, Piperazines pharmacology, Piperazines chemistry, Piperazines therapeutic use, Piperazines chemical synthesis, Piperazines pharmacokinetics, Male, Rats, Sprague-Dawley, Heart Failure drug therapy, Potassium Channel Blockers therapeutic use, Potassium Channel Blockers pharmacology, Potassium Channel Blockers chemistry, Potassium Channel Blockers pharmacokinetics, Potassium Channel Blockers chemical synthesis

Abstract

Recent literature reports highlight the importance of the renal outer medullary potassium (ROMK) channel in renal sodium and potassium homeostasis and emphasize the potential impact that ROMK inhibitors could have as a novel mechanism diuretic in heart failure patients. A series of piperazine-based ROMK inhibitors were designed and optimized to achieve excellent ROMK potency, hERG selectivity, and ADME properties, which led to the identification of compound 28 (BMS-986308). BMS-986308 demonstrated efficacy in the volume-loaded rat diuresis model as well as promising in vitro and in vivo profiles and was therefore advanced to clinical development.

Published

2024

3. Empowering Voices: Inspiring Women in Medicinal Chemistry.

Author

Blanco MJ, Bronson JJ, DiMauro EF, Dzierba C, Eggen M, Garner AL, Georg G, Giarolla J, Goodwin NC, Grenier-Davies MC, Haskell-Luevano C, Holzgrabe U, Huang R, Lagiakos HR, Leftheris K, Martin Y, Matos MJ, May-Dracka TL, Müller CE, Newman AH, Parmee E, Petter JC, Tamayo NA, Wexler RR, Bolognesi ML, Ripka A, and Young W

Subjects

Humans, Female, Chemistry, Pharmaceutical, Power, Psychological

Abstract

As we celebrate International Women's Day 2024 with the theme "Inspire Inclusion", the women of the ACS Medicinal Chemistry Division (MEDI) want to foster a sense of belonging, relevance, and empowerment by sharing uplifting stories of what inspired them to become medicinal chemists. In this editorial, we are featuring female medicinal chemistry scientists to provide role models, encouragement, and inspiration to others. We asked women medicinal chemists to contribute a brief paragraph about what inspired them to become medicinal chemists or what inspires them today as medicinal chemists. The responses and contributions highlight their passions and motivations, such as their love of the sciences and their drive to improve human health by contributing to basic research and creating lifesaving drugs.

Published

2024

4. Discovery of Potent and Selective Quinoxaline-Based Protease-Activated Receptor 4 (PAR4) Antagonists for the Prevention of Arterial Thrombosis.

Author

Zhang X, Jiang W, Richter JM, Bates JA, Reznik SK, Stachura S, Rampulla R, Doddalingappa D, Ulaganathan S, Hua J, Bostwick JS, Sum C, Posy S, Malmstrom S, Dickey J, Harden D, Lawrence RM, Guarino VR, Schumacher WA, Wong P, Yang J, Gordon DA, Wexler RR, and Priestley ES

Subjects

Animals, Macaca fascicularis, Quinoxalines pharmacology, Quinoxalines therapeutic use, Receptors, Thrombin, Thrombin, Hemorrhage, Receptor, PAR-1, Blood Platelets, Platelet Aggregation, Fibrinolytic Agents pharmacology, Fibrinolytic Agents therapeutic use, Thrombosis drug therapy, Thrombosis prevention & control

Abstract

PAR4 is a promising antithrombotic target with potential for separation of efficacy from bleeding risk relative to current antiplatelet therapies. In an effort to discover a novel PAR4 antagonist chemotype, a quinoxaline-based HTS hit 3 with low μM potency was identified. Optimization of the HTS hit through the use of positional SAR scanning and the design of conformationally constrained cores led to the discovery of a quinoxaline-benzothiazole series as potent and selective PAR4 antagonists. The lead compound 48 , possessing a 2 nM IC 50 against PAR4 activation by γ-thrombin in platelet-rich plasma (PRP) and greater than 2500-fold selectivity versus PAR1, demonstrated robust antithrombotic efficacy and minimal bleeding in the cynomolgus monkey models.

Published

2024

5. Empowering Voices: Inspiring Women in Medicinal Chemistry.

Author

Blanco MJ, Bronson JJ, DiMauro EF, Dzierba C, Eggen M, Garner AL, Georg G, Giarolla J, Goodwin NC, Grenier-Davies MC, Haskell-Luevano C, Holzgrabe U, Huang R, Lagiakos HR, Leftheris K, Martin Y, Matos MJ, May-Dracka TL, Müller CE, Newman AH, Parmee E, Petter JC, Tamayo NA, Wexler RR, Bolognesi ML, Ripka A, and Young W

Abstract

As we celebrate International Women's Day 2024 with the theme "Inspire Inclusion", the women of the ACS Medicinal Chemistry Division (MEDI) want to foster a sense of belonging, relevance, and empowerment by sharing uplifting stories of what inspired them to become medicinal chemists. In this editorial, we are featuring female medicinal chemistry scientists to provide role models, encouragement, and inspiration to others. We asked women medicinal chemists to contribute a brief paragraph about what inspired them to become medicinal chemists or what inspires them today as medicinal chemists. The responses and contributions highlight their passions and motivations, such as their love of the sciences and their drive to improve human health by contributing to basic research and creating lifesaving drugs., (Published 2024 by American Chemical Society.)

Published

2024

6. Phthalazinone-based lactams and cyclic ureas as ROCK2 selective inhibitors.

Author

Hu Z, Sitkoff D, Glunz PW, Zou Y, Wang C, Muckelbauer JK, Adam LP, Wexler RR, and Quan ML

Subjects

Protein Isoforms, Amides, Lactams pharmacology, rho-Associated Kinases antagonists & inhibitors

Abstract

Derivatives of lactam, cyclic urea and carbamate were explored as aniline amide replacements in a series of phthalazinone-based ROCK inhibitors. Potent ROCK2 inhibitors such as 22 were identified with excellent overall kinase selectivity as well as good isoform selectivity over ROCK1., 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 © 2023 Elsevier Ltd. All rights reserved.)

Published

2023

7. Design and preparation of N-linked hydroxypyridine-based APJ agonists.

Author

Richter JM, Alex Bates J, Gargalovic P, Onorato JM, Generaux C, Wang T, Gordon DA, Wexler RR, and Finlay HJ

Subjects

Animals, Apelin, Apelin Receptors agonists, Rats, Pyridines, Receptors, G-Protein-Coupled agonists

Abstract

Agonism of the apelin receptor (APJ) has demonstrated beneficial effects in models of heart failure. We have previously disclosed compounds such as 4, which showed good APJ agonist activity but were metabolized to the mono-demethylated, non-interconverting atropisomer metabolites. Herein, we detail the design and optimization of a novel series of N-linked APJ agonists with good potency, metabolic stability, and rat pharmacokinetic profile, which are unable to undergo the same metabolic mono-demethylation cleavage., (Copyright © 2022 Elsevier Ltd. All rights reserved.)

Published

2022

8. Discovery of Two Novel Antiplatelet Clinical Candidates (BMS-986120 and BMS-986141) That Antagonize Protease-Activated Receptor 4.

Author

Priestley ES, Banville J, Deon D, Dubé L, Gagnon M, Guy J, Lapointe P, Lavallée JF, Martel A, Plamondon S, Rémillard R, Ruediger E, Tremblay F, Posy SL, Guarino VR, Richter JM, Li J, Gupta A, Vetrichelvan M, Balapragalathan TJ, Mathur A, Hua J, Callejo M, Guay J, Sum CS, Cvijic ME, Watson C, Wong P, Yang J, Bouvier M, Gordon DA, Wexler RR, and Marinier A

Subjects

Benzofurans, Blood Platelets, Humans, Imidazoles, Morpholines, Receptor, PAR-1, Receptors, Thrombin, Thiazoles, Thrombin, Platelet Aggregation, Thrombosis drug therapy

Abstract

Protease-activated receptor 4 (PAR4) is a G-protein coupled receptor that is expressed on human platelets and activated by the coagulation enzyme thrombin. PAR4 plays a key role in blood coagulation, and its importance in pathological thrombosis has been increasingly recognized in recent years. Herein, we describe the optimization of a series of imidazothiadiazole PAR4 antagonists to a first-in-class clinical candidate, BMS-986120 ( 43 ), and a backup clinical candidate, BMS-986141 ( 49 ). Both compounds demonstrated excellent antithrombotic efficacy and minimal bleeding time prolongation in monkey models relative to the clinically important antiplatelet agent clopidogrel and provide a potential opportunity to improve the standard of care in the treatment of arterial thrombosis.

Published

2022

9. Discovery of Heteroaryl Urea Isosteres for Formyl Peptide Receptor 2 Agonists.

Author

Wurtz NR, Johnson JA, Viet A, Shirude PS, Baligar V, Madduri S, Cheney DL, Park H, Lupisella JA, Hsu MY, Abousleiman M, Galella MA, Aulakh D, Dierks EA, Garcia RA, Ostrowski J, Kick EK, and Wexler RR

Abstract

Formyl peptide receptor 2 (FPR2) agonists have shown efficacy in inflammatory-driven animal disease models and have the potential to treat a range of diseases. Many reported synthetic agonists contain a phenylurea, which appears to be necessary for activity in the reported chemotypes. We set out to find isosteres for the phenylurea and focused our efforts on heteroaryl rings. The wide range of potencies with heterocyclic isosteres demonstrates how electronic effects of the heteroatom placement impact molecular recognition. Herein, we report our discovery of benzimidazole and aminophenyloxadiazole FPR2 agonists with low nanomolar activity., Competing Interests: The authors declare no competing financial interest., (© 2022 American Chemical Society.)

Published

2022

10. Discovery of Milvexian, a High-Affinity, Orally Bioavailable Inhibitor of Factor XIa in Clinical Studies for Antithrombotic Therapy.

Author

Dilger AK, Pabbisetty KB, Corte JR, De Lucca I, Fang T, Yang W, Pinto DJP, Wang Y, Zhu Y, Mathur A, Li J, Hou X, Smith D, Sun D, Zhang H, Krishnananthan S, Wu DR, Myers JE Jr, Sheriff S, Rossi KA, Chacko S, Zheng JJ, Galella MA, Ziemba T, Dierks EA, Bozarth JM, Wu Y, Crain E, Wong PC, Luettgen JM, Wexler RR, and Ewing WR

Subjects

Animals, Mice, Rabbits, Administration, Oral, Macaca fascicularis, Molecular Structure, Pyrazoles administration & dosage, Pyrazoles chemical synthesis, Pyrazoles pharmacokinetics, Pyrazoles therapeutic use, Rats, Sprague-Dawley, Structure-Activity Relationship, Rats, Carotid Artery Thrombosis drug therapy, Factor XIa antagonists & inhibitors, Fibrinolytic Agents administration & dosage, Fibrinolytic Agents chemical synthesis, Fibrinolytic Agents pharmacokinetics, Fibrinolytic Agents therapeutic use, Pyrimidines administration & dosage, Pyrimidines chemical synthesis, Pyrimidines pharmacokinetics, Pyrimidines therapeutic use, Triazoles administration & dosage, Triazoles chemical synthesis, Triazoles pharmacokinetics, Triazoles therapeutic use

Abstract

Factor XIa (FXIa) is an enzyme in the coagulation cascade thought to amplify thrombin generation but has a limited role in hemostasis. From preclinical models and human genetics, an inhibitor of FXIa has the potential to be an antithrombotic agent with superior efficacy and safety. Reversible and irreversible inhibitors of FXIa have demonstrated excellent antithrombotic efficacy without increased bleeding time in animal models (Weitz, J. I., Chan, N. C. Arterioscler. Thromb. Vasc. Biol. 2019, 39 (1), 7-12). Herein, we report the discovery of a novel series of macrocyclic FXIa inhibitors containing a pyrazole P2' moiety. Optimization of the series for (pharmacokinetic) PK properties, free fraction, and solubility resulted in the identification of milvexian ( BMS-986177/JNJ-70033093 , 17 , FXIa K i = 0.11 nM) as a clinical candidate for the prevention and treatment of thromboembolic disorders, suitable for oral administration.

Published

2022

11. Milvexian, an orally bioavailable, small-molecule, reversible, direct inhibitor of factor XIa: In vitro studies and in vivo evaluation in experimental thrombosis in rabbits.

Author

Wong PC, Crain EJ, Bozarth JM, Wu Y, Dilger AK, Wexler RR, Ewing WR, Gordon D, and Luettgen JM

Subjects

Animals, Factor XIa, Fibrinolytic Agents therapeutic use, Partial Thromboplastin Time, Rabbits, Carotid Artery Thrombosis drug therapy, Thrombosis drug therapy

Abstract

Background: Milvexian (BMS-986177/JNJ-70033093) is an orally bioavailable factor XIa (FXIa) inhibitor currently in phase 2 clinical trials., Objectives: To evaluate in vitro properties and in vivo characteristics of milvexian., Methods: In vitro properties of milvexian were evaluated with coagulation and enzyme assays, and in vivo profiles were characterized with rabbit models of electrolytic-induced carotid arterial thrombosis and cuticle bleeding time (BT)., Results: Milvexian is an active-site, reversible inhibitor of human and rabbit FXIa (K i 0.11 and 0.38 nM, respectively). Milvexian increased activated partial thromboplastin time (APTT) without changing prothrombin time and potently prolonged plasma APTT in humans and rabbits. Milvexian did not alter platelet aggregation to ADP, arachidonic acid, or collagen. Milvexian was evaluated for in vivo prevention and treatment of thrombosis. For prevention, milvexian 0.063 + 0.04, 0.25 + 0.17, and 1 + 0.67 mg/kg+mg/kg/h preserved 32 ± 6*, 54 ± 10*, and 76 ± 5%* of carotid blood flow (CBF) and reduced thrombus weight by 15 ± 10*, 45 ± 2*, and 70 ± 4%*, respectively (*p < .05; n = 6/dose). For treatment, thrombosis was initiated for 15 min and CBF decreased to 40% of control. Seventy-five minutes after milvexian administration, CBF averaged 1 ± 0.3, 39 ± 10, and 66 ± 2%* in groups treated with vehicle and milvexian 0.25 + 0.17 and 1 + 0.67 mg/kg+mg/kg/h, respectively (*p < .05 vs. vehicle; n = 6/group). The combination of milvexian 1 + 0.67 mg/kg+mg/kg/h and aspirin 4 mg/kg/h intravenous did not increase BT versus aspirin monotherapy., Conclusions: Milvexian is an effective antithrombotic agent with limited impact on hemostasis, even when combined with aspirin in rabbits. This study supports inhibition of FXIa with milvexian as a promising antithrombotic therapy with a wide therapeutic window., (© 2021 Bristol Myers Squibb. Journal of Thrombosis and Haemostasis published by Wiley Periodicals LLC on behalf of International Society on Thrombosis and Haemostasis.)

Published

2022

12. Identification of a Hydroxypyrimidinone Compound ( 21 ) as a Potent APJ Receptor Agonist for the Potential Treatment of Heart Failure.

Author

Meng W, Pi Z, Brigance R, Rossi KA, Schumacher WA, Bostwick JS, Gargalovic PS, Onorato JM, Luk CE, Generaux CN, Wang T, Wexler RR, and Finlay HJ

Subjects

Animals, Dogs, Drug Discovery, Humans, Pyrimidinones chemistry, Pyrimidinones pharmacokinetics, Pyrimidinones therapeutic use, Rats, Structure-Activity Relationship, Apelin Receptors agonists, Heart Failure drug therapy, Pyrimidinones pharmacology

Abstract

This paper describes our continued efforts in the area of small-molecule apelin receptor agonists. Recently disclosed compound 2 showed an acceptable metabolic stability but demonstrated monodemethylation of the dimethoxyphenyl group to generate atropisomer metabolites in vitro . In this article, we extended the structure-activity relationship at the C2 position that led to the identification of potent pyrazole analogues with excellent metabolic stability. Due to the increased polarity at C2, the permeability for these compounds decreased. Further adjustment of the polarity by replacing the N1 2,6-dimethoxyphenyl group with a 2,6-diethylphenyl group and reoptimization for the potency of the C5 pyrroloamides resulted in potent compounds with improved permeability. Compound 21 displayed excellent pharmacokinetic profiles in rat, monkey, and dog models and robust pharmacodynamic efficacy in the rodent heart failure model. Compound 21 also showed an acceptable safety profile in preclinical toxicology studies and was selected as a backup development candidate for the program.

Published

2021

13. Identification of 6-Hydroxypyrimidin-4(1 H )-one-3-carboxamides as Potent and Orally Active APJ Receptor Agonists.

Author

Pi Z, Johnson JA, Meng W, Phillips M, Schumacher WA, Bostwick JS, Gargalovic PS, Onorato JM, Generaux CN, Wang T, He Y, Gordon DA, Wexler RR, and Finlay HJ

Abstract

The apelin receptor (APJ) is a significant regulator of cardiovascular function and is involved in heart failure and other cardiovascular diseases. (Pyr 1 )apelin-13 is one of the endogenous agonists of the APJ receptor. Administration of (Pyr 1 )apelin-13 increases cardiac output in preclinical models and humans. Recently we disclosed clinical lead BMS-986224 ( 1 ), a C3 oxadiazole pyridinone APJ receptor agonist with robust pharmacodynamic effects similar to (Pyr 1 )apelin-13 in an acute rat pressure-volume loop model. Herein we describe the structure-activity relationship of the carboxamides as oxadiazole bioisosteres at C3 of the pyridinone core and C5 of the respective pyrimidinone core. This study led to the identification of structurally differentiated 6-hydroxypyrimidin-4(1 H )-one-3-carboxamide 14a with pharmacodynamic effects comparable to those of compound 1 ., Competing Interests: The authors declare the following competing financial interest(s): The authors of this Letter were employees of Bristol Myers Squibb at the time of this research., (© 2021 American Chemical Society.)

Published

2021

14. Identification of 6-hydroxy-5-phenyl sulfonylpyrimidin-4(1H)-one APJ receptor agonists.

Author

Tora G, Jiang J, Bostwick JS, Gargalovic PS, Onorato JM, Luk CE, Generaux C, Xu C, Galella MA, Wang T, He Y, Wexler RR, and Finlay HJ

Subjects

Animals, Area Under Curve, Cardiovascular Agents chemical synthesis, Drug Design, Half-Life, Humans, Intercellular Signaling Peptides and Proteins chemistry, Macaca fascicularis, Molecular Structure, Pyrimidinones chemistry, Pyrimidinones pharmacology, Rats, Structure-Activity Relationship, Apelin Receptors agonists, Cardiovascular Agents pharmacokinetics, Cardiovascular Agents pharmacology, Intercellular Signaling Peptides and Proteins pharmacology

Abstract

Heart failure (HF) treatment remains a critical unmet medical need. Studies in normal healthy volunteers and HF patients have shown that [Pyr 1 ]apelin-13, the endogenous ligand for the APJ receptor, improves cardiac function. However, the short half-life of [Pyr 1 ]apelin-13 and the need for intravenous administration have limited the therapeutic potential for chronic use. We sought to identify potent, small-molecule APJ agonists with improved pharmaceutical properties to enable oral dosing in clinical studies. In this manuscript, we describe the identification of a series of pyrimidinone sulfones as a structurally differentiated series to the clinical lead (compound 1). Optimization of the sulfone series for potency, metabolic stability and oral bioavailability led to the identification of compound 22, which showed comparable APJ potency to [Pyr 1 ]apelin-13 and exhibited an acceptable pharmacokinetic profile to advance to the acute hemodynamic rat model., (Copyright © 2021 Elsevier Ltd. All rights reserved.)

Published

2021

15. Selective FPR2 Agonism Promotes a Proresolution Macrophage Phenotype and Improves Cardiac Structure-Function Post Myocardial Infarction.

Author

García RA, Lupisella JA, Ito BR, Hsu MY, Fernando G, Carson NL, Allocco JJ, Ryan CS, Zhang R, Wang Z, Heroux M, Carrier M, St-Onge S, Bouvier M, Dudhgaonkar S, Nagar J, Bustamante-Pozo MM, Garate-Carrillo A, Chen J, Ma X, Search DJ, Dierks EA, Kick EK, Wexler RR, Gordon DA, Ostrowski J, Wurtz NR, and Villarreal F

Abstract

Dysregulated inflammation following myocardial infarction (MI) leads to maladaptive healing and remodeling. The study characterized and evaluated a selective formyl peptide receptor 2 (FPR2) agonist BMS-986235 in cellular assays and in rodents undergoing MI. BMS-986235 activated G proteins and promoted β-arrestin recruitment, enhanced phagocytosis and neutrophil apoptosis, regulated chemotaxis, and stimulated interleukin-10 and monocyte chemoattractant protein-1 gene expression. Treatment with BMS-986235 improved mouse survival, reduced left ventricular area, reduced scar area, and preserved wall thickness. Treatment increased macrophage arginase-1 messenger RNA and CD206 receptor levels indicating a proresolution phenotype. In rats following MI, BMS-986235 preserved viable myocardium, attenuated left ventricular remodeling, and increased ejection fraction relative to control animals. Therefore, FPR2 agonism improves post-MI healing, limits remodeling and preserves function, and may offer an innovative therapeutic option to improve outcomes., Competing Interests: This work was supported by Bristol Myers Squibb (Princeton, New Jersey, USA). All authors are employees of Bristol Myers Squibb or affiliates via collaboration or contract research., (© 2021 The Authors.)

Published

2021

16. From basic science to life-saving therapy: the rationale, and drug discovery efforts that led to the direct factor Xa inhibitor eliquis.

Author

Knabb RM and Wexler RR

Subjects

Factor Xa Inhibitors therapeutic use, Humans, Pyrazoles, Pyridones, Drug Discovery

Abstract

Over the past few decades, drug discovery directed at the treatment and prevention of thromboembolic diseases has been challenged by the need to balance robust efficacy with improved safety relative to the standard of care. To this end, the most impactful advance to date has been the discovery and development of oral factor Xa inhibitors. In this essay, a brief account of the program that culminated in the discovery of Eliquis (apixaban) and the commitment to identify a compound with an optimal profile are described., (© 2021. The Author(s), under exclusive licence to Springer Science+Business Media, LLC, part of Springer Nature.)

Published

2021

17. Discussion of talks from the symposium: Factor X: From thrombokinase to oral anti-coagulants and beyond.

Author

Milstone LM, Jackson C, Becker RC, Camire R, Knabb R, Mann K, Ruf W, Wexler RR, and Wood J

Subjects

Blood Coagulation Tests, Factor Xa, Humans, Thromboplastin, Factor X metabolism

Published

2021

18. Small molecule and macrocyclic pyrazole derived inhibitors of myeloperoxidase (MPO).

Author

Hu CH, Neissel Valente MW, Halpern OS, Jusuf S, Khan JA, Locke GA, Duke GJ, Liu X, Duclos FJ, Wexler RR, Kick EK, and Smallheer JM

Subjects

Dose-Response Relationship, Drug, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors chemistry, Humans, Macrocyclic Compounds chemical synthesis, Macrocyclic Compounds chemistry, Molecular Structure, Peroxidase metabolism, Pyrazoles chemical synthesis, Pyrazoles chemistry, Small Molecule Libraries chemical synthesis, Small Molecule Libraries chemistry, Structure-Activity Relationship, Enzyme Inhibitors pharmacology, Macrocyclic Compounds pharmacology, Peroxidase antagonists & inhibitors, Pyrazoles pharmacology, Small Molecule Libraries pharmacology

Abstract

Myeloperoxidase (MPO), a critical enzyme in antimicrobial host-defense, has been implicated in chronic inflammatory diseases such as coronary artery disease. The design and evaluation of MPO inhibitors for the treatment of cardiovascular disease are reported herein. Starting with the MPO and triazolopyridine 3 crystal structure, novel inhibitors were designed incorporating a substituted pyrazole, which allowed for substituents to interact with hydrophobic and hydrophilic patches in the active site. SAR exploration of the substituted pyrazoles led to piperidine 17, which inhibited HOCl production from activated neutrophils with an IC 50 value of 2.4 μM and had selectivity against thyroid peroxidase (TPO). Optimization of alkylation chemistry on the pyrazole nitrogen facilitated the preparation of many analogs, including macrocycles designed to bridge two hydrophobic regions of the active site. Multiple macrocyclization strategies were pursued to prepare analogs that optimally bound to the active site, leading to potent macrocyclic MPO inhibitors with TPO selectivity, such as compound 30., (Copyright © 2021 Elsevier Ltd. All rights reserved.)

Published

2021

19. Discovery of a Hydroxypyridinone APJ Receptor Agonist as a Clinical Candidate.

Author

Johnson JA, Kim SH, Jiang J, Phillips M, Schumacher WA, Bostwick JS, Gargalovic PS, Onorato JM, Luk CE, Generaux C, He Y, Chen XQ, Xu C, Galella MA, Wang T, Gordon DA, Wexler RR, and Finlay HJ

Subjects

Animals, Apelin Receptors metabolism, Dogs, Drug Discovery, Haplorhini, Humans, Intercellular Signaling Peptides and Proteins metabolism, Male, Models, Molecular, Pyridones pharmacokinetics, Rats, Rats, Sprague-Dawley, Apelin Receptors agonists, Pyridones chemistry, Pyridones pharmacology

Abstract

Apelin-13 is an endogenous peptidic agonist of the apelin receptor (APJ) receptor with the potential for improving cardiac function in heart failure patients. However, the low plasma stability of apelin-13 necessitates continuous intravenous infusion for therapeutic use. There are several approaches to increase the stability of apelin-13 including attachment of pharmacokinetic enhancing groups, stabilized peptides, and Fc-fusion approaches. We sought a small-molecule APJ receptor agonist approach to target a compound with a pharmacokinetic profile amenable for chronic oral administration. This manuscript describes sequential optimization of the pyrimidinone series, leading to pyridinone 14 , with in vitro potency equivalent to the endogenous ligand apelin-13 and with an excellent oral bioavailability and PK profile in multiple preclinical species. Compound 14 exhibited robust pharmacodynamic effects similar to apelin-13 in an acute rat pressure-volume loop model and was advanced as a clinical candidate.

Published

2021

20. Discovery and structure activity relationships of 7-benzyl triazolopyridines as stable, selective, and reversible inhibitors of myeloperoxidase.

Author

Shaw SA, Vokits BP, Dilger AK, Viet A, Clark CG, Abell LM, Locke GA, Duke G, Kopcho LM, Dongre A, Gao J, Krishnakumar A, Jusuf S, Khan J, Spronk SA, Basso MD, Zhao L, Cantor GH, Onorato JM, Wexler RR, Duclos F, and Kick EK

Subjects

Dose-Response Relationship, Drug, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors chemistry, Humans, Molecular Docking Simulation, Molecular Structure, Peroxidase metabolism, Pyridines chemical synthesis, Pyridines chemistry, Structure-Activity Relationship, Triazoles chemical synthesis, Triazoles chemistry, Drug Discovery, Enzyme Inhibitors pharmacology, Peroxidase antagonists & inhibitors, Pyridines pharmacology, Triazoles pharmacology

Abstract

Myeloperoxidase (MPO) is a heme peroxidase found in neutrophils, monocytes and macrophages that efficiently catalyzes the oxidation of endogenous chloride into hypochlorous acid for antimicrobial activity. Chronic MPO activation can lead to indiscriminate protein modification causing tissue damage, and has been associated with chronic inflammatory diseases, atherosclerosis, and acute cardiovascular events. Triazolopyrimidine 5 is a reversible MPO inhibitor; however it suffers from poor stability in acid, and is an irreversible inhibitor of the DNA repair protein methyl guanine methyl transferase (MGMT). Structure-based drug design was employed to discover benzyl triazolopyridines with improved MPO potency, as well as acid stability, no reactivity with MGMT, and selectivity against thyroid peroxidase (TPO). Structure-activity relationships, a crystal structure of the MPO-inhibitor complex, and acute in vivo pharmacodynamic data are described herein., (Copyright © 2020 Elsevier Ltd. All rights reserved.)

Published

2020

21. Discovery of a phenylpyrazole amide ROCK inhibitor as a tool molecule for in vivo studies.

Author

Hu Z, Wang C, Glunz PW, Li J, Cheadle NL, Chen AY, Chen XQ, Myers JE, Guarino VR, Rose A, Sack JS, Sitkoff D, Taylor DS, Xu S, Yan C, Zhang H, Zhang L, Hennan J, Adam LP, Wexler RR, and Quan ML

Subjects

Amides chemical synthesis, Amides chemistry, Animals, Blood Pressure drug effects, Crystallography, X-Ray, Dose-Response Relationship, Drug, Humans, Mice, Models, Molecular, Molecular Structure, Protein Kinase Inhibitors chemical synthesis, Protein Kinase Inhibitors chemistry, Pyrazoles chemical synthesis, Pyrazoles chemistry, Structure-Activity Relationship, rho-Associated Kinases metabolism, Amides pharmacology, Drug Discovery, Protein Kinase Inhibitors pharmacology, Pyrazoles pharmacology, rho-Associated Kinases antagonists & inhibitors

Abstract

Structure-activity relationship optimization on a series of phenylpyrazole amides led to the identification of a dual ROCK1 and ROCK2 inhibitor (25) which demonstrated good potency, kinome selectivity and favorable pharmacokinetic profiles. Compound 25 was selected as a tool molecule for in vivo studies including evaluating hemodynamic effects in telemeterized mice, from which moderate decreases in blood pressure were observed., 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 Ltd. All rights reserved.)

Published

2020

22. Identification of 5H-chromeno[3,4-c]pyridine and 6H-isochromeno[3,4-c]pyridine derivatives as potent and selective dual ROCK inhibitors.

Author

Hu Z, Wang C, Sitkoff D, Cheadle NL, Xu S, Muckelbauer JK, Adam LP, Wexler RR, and Quan ML

Subjects

Crystallography, X-Ray, Dose-Response Relationship, Drug, Humans, Models, Molecular, Molecular Structure, Protein Kinase Inhibitors chemistry, Pyridines chemistry, Structure-Activity Relationship, rho-Associated Kinases metabolism, Protein Kinase Inhibitors pharmacology, Pyridines pharmacology, rho-Associated Kinases antagonists & inhibitors

Abstract

A novel series of 5H-chromeno[3,4-c]pyridine, 6H-isochromeno[3,4-c]pyridine and 6H-isochromeno[4,3-d]pyrimidine derivatives as dual ROCK1 and ROCK2 inhibitors is described. Optimization led to compounds with sub-nanomolar inhibitory affinity for both kinases and excellent kinome selectivity. Compound 19 exhibited ROCK1 and ROCK2 IC 50 of 0.67 nM and 0.18 nM respectively., 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 Ltd. All rights reserved.)

Published

2020

23. Discovery of a High Affinity, Orally Bioavailable Macrocyclic FXIa Inhibitor with Antithrombotic Activity in Preclinical Species.

Author

Yang W, Wang Y, Lai A, Clark CG, Corte JR, Fang T, Gilligan PJ, Jeon Y, Pabbisetty KB, Rampulla RA, Mathur A, Kaspady M, Neithnadka PR, Arumugam A, Raju S, Rossi KA, Myers JE Jr, Sheriff S, Lou Z, Zheng JJ, Chacko SA, Bozarth JM, Wu Y, Crain EJ, Wong PC, Seiffert DA, Luettgen JM, Lam PYS, Wexler RR, and Ewing WR

Subjects

Administration, Oral, Animals, Biological Availability, Crystallography, X-Ray, Dogs, Drug Evaluation, Preclinical, Factor XIa chemistry, Factor XIa metabolism, Fibrinolytic Agents chemistry, Fibrinolytic Agents pharmacokinetics, Humans, Hydrophobic and Hydrophilic Interactions, Macrocyclic Compounds administration & dosage, Macrocyclic Compounds chemistry, Macrocyclic Compounds pharmacokinetics, Macrocyclic Compounds pharmacology, Models, Molecular, Rabbits, Structure-Activity Relationship, Factor XIa antagonists & inhibitors, Fibrinolytic Agents administration & dosage, Fibrinolytic Agents pharmacology

Abstract

Oral factor XIa (FXIa) inhibitors may provide a promising new antithrombotic therapy with an improved benefit to bleeding risk profile over existing antithrombotic agents. Herein, we report application of a previously disclosed cyclic carbamate P1 linker which provided improved oral bioavailability in the imidazole-based 13-membered macrocycle to the 12-membered macrocycle. This resulted in identification of compound 4 with desired FXIa inhibitory potency and good oral bioavailability but high in vivo clearance. Further structure-activity relationship (SAR) studies of heterocyclic core modifications to replace the imidazole core as well as various linkers to the P1 group led to the discovery of compound 6f , a potent FXIa inhibitor with selectivity against most of the relevant serine proteases. Compound 6f also demonstrated excellent pharmacokinetics (PK) profile (high oral bioavailability and low clearance) in multiple preclinical species. Compound 6f achieved robust antithrombotic efficacy in a rabbit efficacy model at doses which preserved hemostasis.

Published

2020

24. Discovery and SAR of aryl hydroxy pyrimidinones as potent small molecule agonists of the GPCR APJ.

Author

Myers MC, Bilder DM, Cavallaro CL, Chao HJ, Su S, Burford NT, Nayeem A, Wang T, Yan M, Langish RA, Dabros M, Li YX, Rose AV, Behnia K, Onorato JM, Gargalovic PS, Wexler RR, and Lawrence RM

Subjects

Drug Discovery, HEK293 Cells, High-Throughput Screening Assays, Humans, Molecular Structure, Pyrimidinones chemical synthesis, Structure-Activity Relationship, Apelin Receptors agonists, Pyrimidinones pharmacology

Abstract

This article describes the discovery of aryl hydroxy pyrimidinones and the medicinal chemistry efforts to optimize this chemotype for potent APJ agonism. APJ is a G-protein coupled receptor whose natural agonist peptide, apelin, displays hemodynamic improvement in the cardiac function of heart failure patients. A high throughput screen was undertaken to identify small molecule hits that could be optimized to mimic the apelin in vitro response. A potent and low molecular weight aryl hydroxy pyrimidinone analog 30 was identified through optimization of an HTS hit and medicinal chemistry efforts to improve its properties., 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 Ltd. All rights reserved.)

Published

2020

25. Identification of Reversible Small Molecule Inhibitors of Endothelial Lipase (EL) That Demonstrate HDL-C Increase In Vivo.

Author

Tora G, Kim SH, Pi Z, Johnson JA, Jiang J, Phillips M, Lloyd J, Abell LM, Lu H, Locke G, Adam LP, Taylor DS, Yin X, Behnia K, Zhao L, Yang R, Basso M, Caporuscio C, Chen AY, Liu E, Kirshgessner T, Onorato JM, Ryan C, Traeger SC, Gordon D, Wexler RR, and Finlay HJ

Subjects

Animals, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors pharmacokinetics, Ketones chemical synthesis, Ketones pharmacokinetics, Male, Mice, Inbred C57BL, Molecular Structure, Oxadiazoles chemical synthesis, Oxadiazoles pharmacokinetics, Structure-Activity Relationship, Cholesterol, HDL metabolism, Enzyme Inhibitors pharmacology, Ketones pharmacology, Lipase antagonists & inhibitors, Oxadiazoles pharmacology

Abstract

Endothelial lipase (EL) hydrolyzes phospholipids in high-density lipoprotein (HDL) resulting in reduction in plasma HDL levels. Studies with murine transgenic, KO, or loss-of-function variants strongly suggest that inhibition of EL will lead to sustained plasma high-density lipoprotein cholesterol (HDL-C) increase and, potentially, a reduced cardiovascular disease (CVD) risk. Herein, we describe the discovery of a series of oxadiazole ketones, which upon optimization, led to the identification of compound 12 . Compound 12 was evaluated in a mouse pharmacodynamics (PD) model and demonstrated a 56% increase in plasma HDL-C. In a mouse reverse cholesterol transport study, compound 12 stimulated cholesterol efflux by 53% demonstrating HDL-C functionality.

Published

2020

26. Orally bioavailable amine-linked macrocyclic inhibitors of factor XIa.

Author

Fang T, Corte JR, Gilligan PJ, Jeon Y, Osuna H, Rossi KA, Myers JE Jr, Sheriff S, Lou Z, Zheng JJ, Harper TW, Bozarth JM, Wu Y, Luettgen JM, Seiffert DA, Wexler RR, and Lam PYS

Subjects

Administration, Oral, Animals, Binding Sites, Drug Design, Factor XIa metabolism, Half-Life, Macrocyclic Compounds metabolism, Macrocyclic Compounds pharmacokinetics, Molecular Dynamics Simulation, Protein Structure, Tertiary, Pyridines chemistry, Rats, Serine Proteinase Inhibitors metabolism, Serine Proteinase Inhibitors pharmacokinetics, Structure-Activity Relationship, Amines chemistry, Factor XIa antagonists & inhibitors, Macrocyclic Compounds chemistry, Serine Proteinase Inhibitors chemical synthesis

Abstract

The discovery of orally bioavailable FXIa inhibitors has been a challenge. Herein, we describe our efforts to address this challenge by optimization of our imidazole-based macrocyclic series. Our optimization strategy focused on modifications to the P2 prime, macrocyclic amide linker, and the imidazole scaffold. Replacing the amide of the macrocyclic linker with amide isosteres led to the discovery of substituted amine linkers which not only maintained FXIa binding affinity but also improved oral exposure in rats. Combining the optimized macrocyclic amine linker with a pyridine scaffold afforded compounds 23 and 24 that were orally bioavailable, single-digit nanomolar FXIa inhibitors with excellent selectivity against relevant blood coagulation enzymes., (Copyright © 2020 Elsevier Ltd. All rights reserved.)

Published

2020

27. Potent, Orally Bioavailable, and Efficacious Macrocyclic Inhibitors of Factor XIa. Discovery of Pyridine-Based Macrocycles Possessing Phenylazole Carboxamide P1 Groups.

Author

Corte JR, Pinto DJP, Fang T, Osuna H, Yang W, Wang Y, Lai A, Clark CG, Sun JH, Rampulla R, Mathur A, Kaspady M, Neithnadka PR, Li YC, Rossi KA, Myers JE Jr, Sheriff S, Lou Z, Harper TW, Huang C, Zheng JJ, Bozarth JM, Wu Y, Wong PC, Crain EJ, Seiffert DA, Luettgen JM, Lam PYS, Wexler RR, and Ewing WR

Subjects

Animals, Biological Availability, Blood Coagulation drug effects, Crystallography, X-Ray, Drug Design, Drug Discovery, Fibrinolytic Agents pharmacokinetics, Humans, Imidazoles chemical synthesis, Imidazoles pharmacology, Macrocyclic Compounds chemical synthesis, Macrocyclic Compounds pharmacology, Models, Molecular, Partial Thromboplastin Time, Rabbits, Serine Proteinase Inhibitors chemical synthesis, Serine Proteinase Inhibitors pharmacology, Structure-Activity Relationship, Thrombosis drug therapy, Factor XIa antagonists & inhibitors, Fibrinolytic Agents chemical synthesis, Fibrinolytic Agents pharmacology, Pyridines chemical synthesis, Pyridines pharmacology

Abstract

Factor XIa (FXIa) inhibitors are promising novel anticoagulants, which show excellent efficacy in preclinical thrombosis models with minimal effects on hemostasis. The discovery of potent and selective FXIa inhibitors which are also orally bioavailable has been a challenge. Here, we describe optimization of the imidazole-based macrocyclic series and our initial progress toward meeting this challenge. A two-pronged strategy, which focused on replacement of the imidazole scaffold and the design of new P1 groups, led to the discovery of potent, orally bioavailable pyridine-based macrocyclic FXIa inhibitors. Moreover, pyridine-based macrocycle 19 , possessing the phenylimidazole carboxamide P1, exhibited excellent selectivity against relevant blood coagulation enzymes and displayed antithrombotic efficacy in a rabbit thrombosis model.

Published

2020

28. Benzothiazole-based compounds as potent endothelial lipase inhibitors.

Author

Meng W, Adam LP, Behnia K, Zhao L, Yang R, Kopcho LM, Locke GA, Taylor DS, Yin X, Wexler RR, and Finlay H

Subjects

Animals, Benzothiazoles pharmacology, Drug Evaluation, Preclinical, Enzyme Inhibitors pharmacology, Gene Expression Regulation drug effects, Humans, Lipase genetics, Lipoproteins, HDL metabolism, Lipoproteins, LDL metabolism, Mice, Mice, Inbred C57BL, Mice, Knockout, Models, Molecular, Molecular Structure, Structure-Activity Relationship, Benzothiazoles chemistry, Cardiovascular Diseases drug therapy, Enzyme Inhibitors chemistry, Lipase antagonists & inhibitors

Abstract

A series of benzothiazoles with a cyano group was synthesized and evaluated as endothelial lipase (EL) inhibitors for the potential treatment of cardiovascular diseases. Efforts to reduce molecular weight and polarity in the series led to improved physicochemical properties of these compounds, as well as selectivity for EL over hepatic lipase (HL). As a benchmark compound, 8i demonstrated potent EL activity, an acceptable absorption, distribution, metabolism and elimination (ADME) profile and pharmacokinetic (PK) exposure which allowed further evaluation in preclinical animal efficacy studies., (Copyright © 2019. Published by Elsevier Ltd.)

Published

2019

29. Structure based design of macrocyclic factor XIa inhibitors: Discovery of cyclic P1 linker moieties with improved oral bioavailability.

Author

Clark CG, Rossi KA, Corte JR, Fang T, Smallheer JM, De Lucca I, Nirschl DS, Orwat MJ, Pinto DJP, Hu Z, Wang Y, Yang W, Jeon Y, Ewing WR, Myers JE Jr, Sheriff S, Lou Z, Bozarth JM, Wu Y, Rendina A, Harper T, Zheng J, Xin B, Xiang Q, Luettgen JM, Seiffert DA, Wexler RR, and Lam PYS

Subjects

Administration, Oral, Biological Availability, Humans, Ligands, Macrocyclic Compounds pharmacology, Models, Molecular, Molecular Structure, Serine Proteinase Inhibitors pharmacology, Structure-Activity Relationship, Drug Design, Drug Discovery, Factor XIa antagonists & inhibitors, Macrocyclic Compounds administration & dosage, Macrocyclic Compounds chemistry, Serine Proteinase Inhibitors administration & dosage, Serine Proteinase Inhibitors chemistry

Abstract

This manuscript describes the discovery of a series of macrocyclic inhibitors of FXIa with oral bioavailability. Assisted by structure based drug design and ligand bound X-ray crystal structures, the group linking the P1 moiety to the macrocyclic core was modified with the goal of reducing H-bond donors to improve pharmacokinetic performance versus 9. This effort resulted in the discovery of several cyclic P1 linkers, exemplified by 10, that are constrained mimics of the bioactive conformation displayed by the acrylamide linker of 9. These cyclic P1 linkers demonstrated enhanced bioavailability and improved potency., (Copyright © 2019 Elsevier Ltd. All rights reserved.)

Published

2019

30. Corrigendum to "Identification of substituted benzothiazole sulfones as potent and selective inhibitors of endothelial lipase" [Bioorg. Med. Chem. Lett. 29 (2019) 1918-1921].

Author

Kim SH, Johnson JA, Jiang J, Parkhurst B, Phillips M, Pi Z, Qiao JX, Tora G, Ye Chen A, Liu E, Yin X, Yang R, Zhao L, Taylor DS, Basso M, Behnia K, Onorato J, Chen XQ, Abell LM, Lu H, Locke G, Caporuscio C, Adam LP, Gordon D, Wexler RR, and Finlay HJ

Published

2019

31. Discovery of Potent Protease-Activated Receptor 4 Antagonists with in Vivo Antithrombotic Efficacy.

Author

Miller MM, Banville J, Friends TJ, Gagnon M, Hangeland JJ, Lavallée JF, Martel A, O'Grady H, Rémillard R, Ruediger E, Tremblay F, Posy SL, Allegretto NJ, Guarino VR, Harden DG, Harper TW, Hartl K, Josephs J, Malmstrom S, Watson C, Yang Y, Zhang G, Wong P, Yang J, Bouvier M, Seiffert DA, Wexler RR, Lawrence RM, Priestley ES, and Marinier A

Subjects

Animals, Benzofurans chemistry, Benzofurans pharmacokinetics, Biological Availability, Disease Models, Animal, Fibrinolytic Agents chemistry, Fibrinolytic Agents pharmacokinetics, HEK293 Cells, Hemorrhage metabolism, Humans, Macaca fascicularis, Models, Chemical, Molecular Structure, Platelet Aggregation drug effects, Receptors, Thrombin genetics, Receptors, Thrombin metabolism, Structure-Activity Relationship, Thrombosis metabolism, Benzofurans pharmacology, Fibrinolytic Agents pharmacology, Hemorrhage prevention & control, Receptors, Thrombin antagonists & inhibitors, Thrombosis prevention & control

Abstract

In an effort to identify novel antithrombotics, we have investigated protease-activated receptor 4 (PAR4) antagonism by developing and evaluating a tool compound, UDM-001651 , in a monkey thrombosis model. Beginning with a high-throughput screening hit, we identified an imidazothiadiazole-based PAR4 antagonist chemotype. Detailed structure-activity relationship studies enabled optimization to a potent, selective, and orally bioavailable PAR4 antagonist, UDM-001651 . UDM-001651 was evaluated in a monkey thrombosis model and shown to have robust antithrombotic efficacy and no prolongation of kidney bleeding time. This combination of excellent efficacy and safety margin strongly validates PAR4 antagonism as a promising antithrombotic mechanism.

Published

2019

32. Identification of substituted benzothiazole sulfones as potent and selective inhibitors of endothelial lipase.

Author

Kim SH, Johnson JA, Jiang J, Parkhurst B, Phillips M, Pi Z, Qiao JX, Tora G, Ye Chen A, Liu E, Yin X, Yang R, Zhao L, Taylor DS, Basso M, Behnia K, Onorato J, Chen XQ, Abell LM, Lu H, Locke G, Caporuscio C, Adam LP, Gordon D, Wexler RR, and Finlay HJ

Abstract

A low level of high density lipoprotein (HDL) is an independent risk factor for cardiovascular disease. HDL reduces inflammation and plays a central role in reverse cholesterol transport, where cholesterol is removed from peripheral tissues and atherosclerotic plaque. One approach to increase plasma HDL is through inhibition of endothelial lipase (EL). EL hydrolyzes phospholipids in HDL resulting in reduction of plasma HDL. A series of benzothiazole sulfone amides was optimized for EL inhibition potency, lipase selectivity and improved pharmacokinetic profile leading to the identification of Compound 32. Compound 32 was evaluated in a mouse pharmacodynamic model and found to show no effect on HDL cholesterol level despite achieving targeted plasma exposure (C trough  > 15 fold over mouse plasma EL IC 50 over 4 days)., (Copyright © 2019 Elsevier Ltd. All rights reserved.)

Published

2019

33. Discovery of a Lead Triphenylethanamine Cholesterol Ester Transfer Protein (CETP) Inhibitor.

Author

Finlay HJ, Jiang J, Rampulla R, Salvati ME, Qiao JX, Wang TC, Lawrence RM, Harikrishnan LS, Kamau MG, Taylor DS, Chen AYA, Yin X, Huang CS, Chang M, Chen XQ, Sleph PG, Xu C, Li J, Levesque P, Adam LP, and Wexler RR

Abstract

Lead optimization of the diphenylpyridylethanamine (DPPE) and triphenylethanamine (TPE) series of CETP inhibitors to improve their pharmaceutical profile is described. Polar groups at the N -terminus position in the DPPE series resulted in further improvement in potency and pharmaceutical properties concomitant with retaining the safety, efficacy, and pharmacokinetic (PK) profile. A structure-activity relationship observed in the DPPE series was extended to the corresponding analogs in the more potent TPE series, and further optimization resulted in the identification of 2-amino- N -(( R )-1-(3-cyclopropoxy-4-fluorophenyl)-1-(3-fluoro-5-(1,1,2,2-tetrafluoroethoxy)phenyl)-2-phenylethyl)-4,4,4-trifluoro-3-hydroxy-3-(trifluoromethyl)butanamide ( 13 ). Compound 13 demonstrated no significant changes in either mean arterial blood pressure or heart rate in telemetry rats, had an excellent PK profile, and demonstrated robust efficacy in human CETP/apo-B-100 dual transgenic mice and in hamsters., Competing Interests: The authors declare no competing financial interest.

Published

2019

34. Discovery and synthesis of tetrahydropyrimidinedione-4-carboxamides as endothelial lipase inhibitors.

Author

Hu CH, Wang TC, Qiao JX, Haque L, Chen AYA, Taylor DS, Ying X, Onorato JM, Galella M, Shen H, Huang CS, Toussaint N, Li YX, Abell L, Adam LP, Gordon D, Wexler RR, and Finlay HJ

Subjects

Animals, Cholesterol, HDL blood, Cholesterol, HDL metabolism, Enzyme Inhibitors blood, Enzyme Inhibitors chemical synthesis, Humans, Lipase blood, Lipase metabolism, Mice, Models, Molecular, Pyrimidinones blood, Pyrimidinones chemical synthesis, Structure-Activity Relationship, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Lipase antagonists & inhibitors, Pyrimidinones chemistry, Pyrimidinones pharmacology

Abstract

Endothelial lipase (EL) inhibitors have been shown to elevate HDL-C levels in pre-clinical murine models and have potential benefit in prevention and treatment of cardiovascular diseases. Modification of the 1-ethyl-3-hydroxy-1,5-dihydro-2H-pyrrol-2-one (DHP) lead, 1, led to the discovery of a series of potent tetrahydropyrimidinedione (THP) EL inhibitors. Synthesis and SAR studies including modification of the amide group, together with changes on the pyrimidinone core led to a series of arylcycloalkyl, indanyl, and tetralinyl substituted 5-amino or 5-hydroxypyrimidinedione-4-carboxamides. Several compounds were advanced to PK evaluation. Among them, compound 4a was one of the most potent with measurable EL HDL hSerum potency and compound 3g demonstrated the best overall pharmacokinetic parameters., (Copyright © 2018 Elsevier Ltd. All rights reserved.)

Published

2018

35. Sulfonylated Benzothiazoles as Inhibitors of Endothelial Lipase.

Author

Johnson JA, Tora G, Pi Z, Phillips M, Yin X, Yang R, Zhao L, Chen AY, Taylor DS, Basso M, Rose A, Behnia K, Onorato J, Chen XQ, Abell LM, Lu H, Locke G, Caporuscio C, Galella M, Adam LP, Gordon D, Wexler RR, and Finlay HJ

Abstract

Endothelial lipase (EL) selectively metabolizes high density lipoprotein (HDL) particles. Inhibition of EL has been shown to increase HDL concentration in preclinical animal models and was targeted as a potential treatment of atherosclerosis. We describe the introduction of an α-sulfone moiety to a benzothiazole series of EL inhibitors resulting in increased potency versus EL. Optimization for selectivity versus hepatic lipase and pharmacokinetic properties resulted in the discovery of 24 , which showed good in vitro potency and bioavailability but, unexpectedly, did not increase HDL in the mouse pharmacodynamic model at the target plasma exposure., Competing Interests: The authors declare no competing financial interest.

Published

2018

36. Potent Triazolopyridine Myeloperoxidase Inhibitors.

Author

Wurtz NR, Viet A, Shaw SA, Dilger A, Valente MN, Khan JA, Jusuf S, Narayanan R, Fernando G, Lo F, Liu X, Locke GA, Kopcho L, Abell LM, Sleph P, Basso M, Zhao L, Wexler RR, Duclos F, and Kick EK

Abstract

Myeloperoxidase (MPO) generates reactive oxygen species that potentially contribute to many chronic inflammatory diseases. A recently reported triazolopyrimidine MPO inhibitor was optimized to improve acid stability and remove methyl guanine methyl transferase (MGMT) activity. Multiple synthetic routes were explored that allowed rapid optimization of a key benzyl ether side chain. Crystal structures of inhibitors bound to the MPO active site demonstrated alternate binding modes and guided rational design of MPO inhibitors. Thioether 36 showed significant inhibition of MPO activity in an acute mouse inflammation model after oral dosing., Competing Interests: The authors declare no competing financial interest.

Published

2018

37. Factor XIa Inhibitors as New Anticoagulants.

Author

Quan ML, Pinto DJP, Smallheer JM, Ewing WR, Rossi KA, Luettgen JM, Seiffert DA, and Wexler RR

Subjects

Antibodies, Monoclonal chemistry, Antibodies, Monoclonal pharmacology, Aptamers, Nucleotide chemistry, Aptamers, Nucleotide pharmacology, Catalytic Domain, Clinical Trials as Topic, Factor XIa chemistry, Factor XIa metabolism, Humans, Small Molecule Libraries chemistry, Small Molecule Libraries pharmacology, Anticoagulants chemistry, Anticoagulants pharmacology, Factor XIa antagonists & inhibitors

Abstract

With the introduction of thrombin and factor Xa inhibitors to the oral anticoagulant market, significant improvements in both efficacy and safety have been achieved. Early clinical and preclinical data suggest that inhibitors of factor XIa can provide a still safer alternative, with expanded efficacy for arterial indications. This Perspective provides an overview of target rationale and details of the discovery and development of inhibitors of factor XIa as next generation antithrombotic agents.

Published

2018

38. PK/PD Disconnect Observed with a Reversible Endothelial Lipase Inhibitor.

Author

Hangeland JJ, Abell LM, Adam LP, Jiang J, Friends TJ, Haque LE, Neels J, Onorato JM, Chen AYA, Taylor DS, Yin X, Harrity TW, Basso MD, Yang R, Sleph PG, Gordon DA, Huang CS, Wexler RR, Finlay HJ, and Lawrence RM

Abstract

Screening of a small set of nonselective lipase inhibitors against endothelial lipase (EL) identified a potent and reversible inhibitor, N -(3-(3,4-dichlorophenyl)propyl)-3-hydroxy-1-methyl-2-oxo-1,2-dihydropyridine-4-carboxamide ( 5 ; EL IC 50 = 61 nM, EL HDL IC 50 = 454 nM). Deck mining identified a related hit, N -(3-(3,4-dichlorophenyl)propyl)-4-hydroxy-1-methyl-5-oxo-2,5-dihydro-1 H -pyrrole-3-carboxamide ( 6a ; EL IC 50 = 41 nM, EL HDL IC 50 = 1760 nM). Both compounds were selective against lipoprotein lipase (LPL) but nonselective versus hepatic lipase (HL). Optimization of compound 6a for EL inhibition using HDL as substrate led to N -(4-(3,4 - dichlorophenyl)butan-2-yl)-1-ethyl-4-hydroxy-5-oxo-2,5-dihydro-1 H -pyrrole-3-carboxamide ( 7c ; EL IC 50 = 148 nM, EL HDL IC 50 = 218 nM) having improved PK over compound 6a , providing a tool molecule to test for the ability to increase HDL-cholesterol (HDL-C) levels in vivo using a reversible EL inhibitor. Compound 7c did not increase HDL-C in vivo despite achieving plasma exposures targeted on the basis of enzyme activity and protein binding demonstrating the need to develop more physiologically relevant in vitro assays to guide compound progression for in vivo evaluation., Competing Interests: The authors declare no competing financial interest.

Published

2018

39. Correction to "Atropisomer Control in Macrocyclic Factor VIIa Inhibitors".

Author

Glunz PW, Mueller L, Cheney DL, Ladziata V, Zou Y, Wurtz NR, Wei A, Wong PC, Wexler RR, and Priestley ES

Published

2018

40. Pyridazine and pyridazinone derivatives as potent and selective factor XIa inhibitors.

Author

Hu Z, Wang C, Han W, Rossi KA, Bozarth JM, Wu Y, Sheriff S, Myers JE Jr, Luettgen JM, Seiffert DA, Wexler RR, and Quan ML

Subjects

Crystallography, X-Ray, Dose-Response Relationship, Drug, Factor XIa metabolism, Humans, Microsomes, Liver drug effects, Microsomes, Liver metabolism, Models, Molecular, Molecular Structure, Pyridazines chemical synthesis, Pyridazines chemistry, Serine Proteinase Inhibitors chemical synthesis, Serine Proteinase Inhibitors chemistry, Structure-Activity Relationship, Factor XIa antagonists & inhibitors, Pyridazines pharmacology, Serine Proteinase Inhibitors pharmacology

Abstract

Pyridazine and pyridazinone derivatives were designed and synthesized as coagulation factor XIa inhibitors. Potent and selective inhibitors with single digit nanomolar affinity for factor XIa were discovered. Selected inhibitors demonstrated moderate oral bioavailability., (Copyright © 2018 Elsevier Ltd. All rights reserved.)

Published

2018

41. Discovery of a Parenteral Small Molecule Coagulation Factor XIa Inhibitor Clinical Candidate (BMS-962212).

Author

Pinto DJP, Orwat MJ, Smith LM 2nd, Quan ML, Lam PYS, Rossi KA, Apedo A, Bozarth JM, Wu Y, Zheng JJ, Xin B, Toussaint N, Stetsko P, Gudmundsson O, Maxwell B, Crain EJ, Wong PC, Lou Z, Harper TW, Chacko SA, Myers JE Jr, Sheriff S, Zhang H, Hou X, Mathur A, Seiffert DA, Wexler RR, Luettgen JM, and Ewing WR

Subjects

Animals, Anticoagulants pharmacokinetics, Anticoagulants pharmacology, Blood Coagulation drug effects, Crystallography, X-Ray, Dogs, Drug Discovery, Factor XIa chemistry, Factor XIa metabolism, Humans, Isoquinolines pharmacokinetics, Isoquinolines pharmacology, Male, Molecular Docking Simulation, Rabbits, Rats, Small Molecule Libraries chemistry, Small Molecule Libraries pharmacokinetics, Small Molecule Libraries pharmacology, Small Molecule Libraries therapeutic use, Thrombosis blood, para-Aminobenzoates pharmacokinetics, para-Aminobenzoates pharmacology, Anticoagulants chemistry, Anticoagulants therapeutic use, Factor XIa antagonists & inhibitors, Isoquinolines chemistry, Isoquinolines therapeutic use, Thrombosis drug therapy, para-Aminobenzoates chemistry, para-Aminobenzoates therapeutic use

Abstract

Factor XIa (FXIa) is a blood coagulation enzyme that is involved in the amplification of thrombin generation. Mounting evidence suggests that direct inhibition of FXIa can block pathologic thrombus formation while preserving normal hemostasis. Preclinical studies using a variety of approaches to reduce FXIa activity, including direct inhibitors of FXIa, have demonstrated good antithrombotic efficacy without increasing bleeding. On the basis of this potential, we targeted our efforts at identifying potent inhibitors of FXIa with a focus on discovering an acute antithrombotic agent for use in a hospital setting. Herein we describe the discovery of a potent FXIa clinical candidate, 55 (FXIa K i = 0.7 nM), with excellent preclinical efficacy in thrombosis models and aqueous solubility suitable for intravenous administration. BMS-962212 is a reversible, direct, and highly selective small molecule inhibitor of FXIa.

Published

2017

42. Triazolopyrimidines identified as reversible myeloperoxidase inhibitors.

Author

Duclos F, Abell LM, Harden DG, Pike K, Nowak K, Locke GA, Duke GJ, Liu X, Fernando G, Shaw SA, Vokits BP, Wurtz NR, Viet A, Valente MN, Stachura S, Sleph P, Khan JA, Gao J, Dongre AR, Zhao L, Wexler RR, Gordon DA, and Kick EK

Abstract

Myeloperoxidase, a mammalian peroxidase involved in the immune system as an anti-microbial first responder, can produce hypochlorous acid in response to invading pathogens. Myeloperoxidase has been implicated in several chronic pathological diseases due to the chronic production of hypochlorous acid, as well as other reactive radical species. A high throughput screen and triaging protocol was developed to identify a reversible inhibitor of myeloperoxidase toward the potential treatment of chronic diseases such as atherosclerosis. The identification and characterization of a reversible myeloperoxidase inhibitor, 7-(benzyloxy)-3 H -[1,2,3]triazolo[4,5- d ]pyrimidin-5-amine is described.

Published

2017

43. Macrocyclic factor XIa inhibitors.

Author

Wang C, Corte JR, Rossi KA, Bozarth JM, Wu Y, Sheriff S, Myers JE Jr, Luettgen JM, Seiffert DA, Wexler RR, and Quan ML

Subjects

Dose-Response Relationship, Drug, Factor XIa metabolism, Humans, Imidazoles chemical synthesis, Imidazoles chemistry, Macrocyclic Compounds chemical synthesis, Macrocyclic Compounds chemistry, Molecular Structure, Serine Proteinase Inhibitors chemical synthesis, Serine Proteinase Inhibitors chemistry, Structure-Activity Relationship, Factor XIa antagonists & inhibitors, Imidazoles pharmacology, Macrocyclic Compounds pharmacology, Serine Proteinase Inhibitors pharmacology

Abstract

A series of macrocyclic factor XIa (FXIa) inhibitors was designed based on an analysis of the crystal structures of the acyclic phenylimidazole compounds. Further optimization using structure-based design led to inhibitors with pM affinity for FXIa, excellent selectivity against a panel of relevant serine proteases, and good potency in the activated partial thromboplastin time (aPTT) clotting assay., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published

2017

44. Macrocyclic inhibitors of Factor XIa: Discovery of alkyl-substituted macrocyclic amide linkers with improved potency.

Author

Corte JR, Yang W, Fang T, Wang Y, Osuna H, Lai A, Ewing WR, Rossi KA, Myers JE Jr, Sheriff S, Lou Z, Zheng JJ, Harper TW, Bozarth JM, Wu Y, Luettgen JM, Seiffert DA, Quan ML, Wexler RR, and Lam PYS

Subjects

Amides chemical synthesis, Amides chemistry, Crystallography, X-Ray, Dose-Response Relationship, Drug, Factor XIa metabolism, Humans, Macrocyclic Compounds chemical synthesis, Macrocyclic Compounds chemistry, Models, Molecular, Molecular Structure, Serine Proteinase Inhibitors chemical synthesis, Serine Proteinase Inhibitors chemistry, Structure-Activity Relationship, Amides pharmacology, Drug Discovery, Factor XIa antagonists & inhibitors, Macrocyclic Compounds pharmacology, Serine Proteinase Inhibitors pharmacology

Abstract

Optimization of macrocyclic inhibitors of FXIa is described which focused on modifications to both the macrocyclic linker and the P1 group. Increases in potency were discovered through interactions with a key hydrophobic region near the S1 prime pocket by substitution of the macrocyclic linker with small alkyl groups. Both the position of substitution and the absolute stereochemistry of the alkyl groups on the macrocyclic linker which led to improved potency varied depending on the ring size of the macrocycle. Replacement of the chlorophenyltetrazole cinnamide P1 in these optimized macrocycles reduced the polar surface area and improved the oral bioavailability for the series, albeit at the cost of a decrease in potency., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published

2017

45. Neutral macrocyclic factor VIIa inhibitors.

Author

Wurtz NR, Parkhurst BL, DeLucca I, Glunz PW, Jiang W, Zhang X, Cheney DL, Bozarth JM, Rendina AR, Wei A, Harper T, Luettgen JM, Wu Y, Wong PC, Seiffert DA, Wexler RR, and Priestley ES

Subjects

Dose-Response Relationship, Drug, Humans, Macrocyclic Compounds chemical synthesis, Macrocyclic Compounds chemistry, Molecular Structure, Serine Proteinase Inhibitors chemical synthesis, Serine Proteinase Inhibitors chemistry, Structure-Activity Relationship, Factor VIIa antagonists & inhibitors, Macrocyclic Compounds pharmacology, Serine Proteinase Inhibitors pharmacology

Abstract

Factor VIIa (FVIIa) inhibitors have shown strong antithrombotic efficacy in preclinical thrombosis models with limited bleeding liabilities. Discovery of potent, orally active FVIIa inhibitors has been largely unsuccessful due to the requirement of a basic P1 group to interact with Asp189 in the S1 binding pocket, limiting their membrane permeability. We have combined recently reported neutral P1 binding substituents with a highly optimized macrocyclic chemotype to produce FVIIa inhibitors with low nanomolar potency and enhanced permeability., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published

2017

46. Selective I Kur Inhibitors for the Potential Treatment of Atrial Fibrillation: Optimization of the Phenyl Quinazoline Series Leading to Clinical Candidate 5-[5-Phenyl-4-(pyridin-2-ylmethylamino)quinazolin-2-yl]pyridine-3-sulfonamide.

Author

Gunaga P, Lloyd J, Mummadi S, Banerjee A, Dhondi NK, Hennan J, Subray V, Jayaram R, Rajugowda N, Umamaheshwar Reddy K, Kumaraguru D, Mandal U, Beldona D, Adisechen AK, Yadav N, Warrier J, Johnson JA, Sale H, Putlur SP, Saxena A, Chimalakonda A, Mandlekar S, Conder M, Xing D, Gupta AK, Gupta A, Rampulla R, Mathur A, Levesque P, Wexler RR, and Finlay HJ

Subjects

Animals, Carbon-13 Magnetic Resonance Spectroscopy, Dogs, Mass Spectrometry, Potassium Channel Blockers pharmacology, Proton Magnetic Resonance Spectroscopy, Quinazolines chemistry, Quinazolines pharmacology, Rabbits, Sodium Channel Blockers pharmacology, Structure-Activity Relationship, Sulfonamides chemistry, Sulfonamides pharmacology, Atrial Fibrillation drug therapy, Potassium Channel Blockers therapeutic use, Quinazolines therapeutic use, Sodium Channel Blockers therapeutic use, Sulfonamides therapeutic use

Abstract

We have recently disclosed 5-phenyl-N-(pyridin-2-ylmethyl)-2-(pyrimidin-5-yl)quinazolin-4-amine 1 as a potent I Kur current blocker with selectivity versus hERG, Na and Ca channels, and an acceptable preclinical PK profile. Upon further characterization in vivo, compound 1 demonstrated an unacceptable level of brain penetration. In an effort to reduce the level of brain penetration while maintaining the overall profile, SAR was developed at the C2' position for a series of close analogues by employing hydrogen bond donors. As a result, 5-[5-phenyl-4-(pyridin-2-ylmethylamino)quinazolin-2-yl]pyridine-3-sulfonamide (25) was identified as the lead compound in this series. Compound 25 showed robust effects in rabbit and canine pharmacodynamic models and an acceptable cross-species pharmacokinetic profile and was advanced as the clinical candidate. Further optimization of 25 to mitigate pH-dependent absorption resulted in identification of the corresponding phosphoramide prodrug (29) with an improved solubility and pharmacokinetic profile.

Published

2017

47. Structure-Based Design of Macrocyclic Factor XIa Inhibitors: Discovery of the Macrocyclic Amide Linker.

Author

Corte JR, Fang T, Osuna H, Pinto DJ, Rossi KA, Myers JE Jr, Sheriff S, Lou Z, Zheng JJ, Harper TW, Bozarth JM, Wu Y, Luettgen JM, Seiffert DA, Decicco CP, Wexler RR, and Quan ML

Subjects

Drug Discovery, Hydrogen Bonding, Ligands, Macrocyclic Compounds chemistry, Macrocyclic Compounds pharmacokinetics, Molecular Structure, Serine Proteinase Inhibitors pharmacokinetics, Amides chemistry, Factor XIa antagonists & inhibitors, Macrocyclic Compounds pharmacology, Serine Proteinase Inhibitors chemistry, Serine Proteinase Inhibitors pharmacology

Abstract

A novel series of macrocyclic FXIa inhibitors was designed based on our lead acyclic phenyl imidazole chemotype. Our initial macrocycles, which were double-digit nanomolar FXIa inhibitors, were further optimized with assistance from utilization of structure-based drug design and ligand bound X-ray crystal structures. This effort resulted in the discovery of a macrocyclic amide linker which was found to form a key hydrogen bond with the carbonyl of Leu41 in the FXIa active site, resulting in potent FXIa inhibitors. The macrocyclic FXIa series, exemplified by compound 16, had a FXIa K i = 0.16 nM with potent anticoagulant activity in an in vitro clotting assay (aPTT EC 1.5x = 0.27 μM) and excellent selectivity against the relevant blood coagulation enzymes.

Published

2017

48. Blockade of protease-activated receptor-4 (PAR4) provides robust antithrombotic activity with low bleeding.

Author

Wong PC, Seiffert D, Bird JE, Watson CA, Bostwick JS, Giancarli M, Allegretto N, Hua J, Harden D, Guay J, Callejo M, Miller MM, Lawrence RM, Banville J, Guy J, Maxwell BD, Priestley ES, Marinier A, Wexler RR, Bouvier M, Gordon DA, Schumacher WA, and Yang J

Subjects

Administration, Oral, Animals, Blood Platelets metabolism, Guinea Pigs, HEK293 Cells, Humans, Inhibitory Concentration 50, Macaca fascicularis, Male, Protein Domains, Receptor, PAR-1 metabolism, Stroke drug therapy, Thrombin chemistry, Thrombosis, Treatment Outcome, Antibodies therapeutic use, Fibrinolytic Agents therapeutic use, Hemorrhage drug therapy, Platelet Aggregation Inhibitors therapeutic use, Receptors, Thrombin antagonists & inhibitors

Abstract

Antiplatelet agents are proven efficacious treatments for cardiovascular and cerebrovascular diseases. However, the existing drugs are compromised by unwanted and sometimes life-threatening bleeding that limits drug usage or dosage. There is a substantial unmet medical need for an antiplatelet drug with strong efficacy and low bleeding risk. Thrombin is a potent platelet agonist that directly induces platelet activation via the G protein (heterotrimeric guanine nucleotide-binding protein)-coupled protease-activated receptors PAR1 and PAR4. A PAR1 antagonist is approved for clinical use, but its use is limited by a substantial bleeding risk. Conversely, the potential of PAR4 as an antiplatelet target has not been well characterized. Using anti-PAR4 antibodies, we demonstrated a low bleeding risk and an effective antithrombotic profile with PAR4 inhibition in guinea pigs. Subsequently, high-throughput screening and an extensive medicinal chemistry effort resulted in the discovery of BMS-986120, an orally active, selective, and reversible PAR4 antagonist. In a cynomolgus monkey arterial thrombosis model, BMS-986120 demonstrated potent and highly efficacious antithrombotic activity. BMS-986120 also exhibited a low bleeding liability and a markedly wider therapeutic window compared to the standard antiplatelet agent clopidogrel tested in the same nonhuman primate model. These preclinical findings define the biological role of PAR4 in mediating platelet aggregation. In addition, they indicate that targeting PAR4 is an attractive antiplatelet strategy with the potential to treat patients at a high risk of atherothrombosis with superior safety compared with the current standard of care., (Copyright © 2017, American Association for the Advancement of Science.)

Published

2017

49. Design and Synthesis of Novel Meta-Linked Phenylglycine Macrocyclic FVIIa Inhibitors.

Author

Richter JM, Cheney DL, Bates JA, Wei A, Luettgen JM, Rendina AR, Harper TM, Narayanan R, Wong PC, Seiffert D, Wexler RR, and Priestley ES

Abstract

Two novel series of meta-linked phenylglycine-based macrocyclic FVIIa inhibitors have been designed to improve the rodent metabolic stability and PK observed with the precursor para-linked phenylglycine macrocycles. Through iterative structure-based design and optimization, the TF/FVIIa K i was improved to subnanomolar levels with good clotting activity, metabolic stability, and permeability.

Published

2016

50. Discovery of Highly Potent Liver X Receptor β Agonists.

Author

Kick EK, Busch BB, Martin R, Stevens WC, Bollu V, Xie Y, Boren BC, Nyman MC, Nanao MH, Nguyen L, Plonowski A, Schulman IG, Yan G, Zhang H, Hou X, Valente MN, Narayanan R, Behnia K, Rodrigues AD, Brock B, Smalley J, Cantor GH, Lupisella J, Sleph P, Grimm D, Ostrowski J, Wexler RR, Kirchgessner T, and Mohan R

Abstract

Introducing a uniquely substituted phenyl sulfone into a series of biphenyl imidazole liver X receptor (LXR) agonists afforded a dramatic potency improvement for induction of ATP binding cassette transporters, ABCA1 and ABCG1, in human whole blood. The agonist series demonstrated robust LXRβ activity (>70%) with low partial LXRα agonist activity (<25%) in cell assays, providing a window between desired blood cell ABCG1 gene induction in cynomolgus monkeys and modest elevation of plasma triglycerides for agonist 15 . The addition of polarity to the phenyl sulfone also reduced binding to the plasma protein, human α-1-acid glycoprotein. Agonist 15 was selected for clinical development based on the favorable combination of in vitro properties, excellent pharmacokinetic parameters, and a favorable lipid profile.

Published

2016