Your search keyword '"Percy H. Carter"' showing total 113 results

1. BMS-813160: A Potent CCR2 and CCR5 Dual Antagonist Selected as a Clinical Candidate

Author

Anne Rose, Qihong Zhao, Kumaravel Selvakumar, Percy H. Carter, Prakash Anjanappa, Jing Chen, Sandhya Mandlekar, Mary Ellen Cvijic, Andrew J. Tebben, Songmei Xu, Gregory D. Brown, Venkatram Reddy Paidi, Arvind Mathur, Douglas G. Batt, Jian Pang, Joel C. Barrish, Robert J. Cherney, Melissa Yarde, and Ragini Vuppugalla

Subjects

CCR2, Human liver, Chemistry, education, Organic Chemistry, Antagonist, Peritonitis, Pharmacology, medicine.disease, Biochemistry, Bioavailability, Pharmacokinetics, Permeability (electromagnetism), Drug Discovery, medicine, Microsome

Abstract

[Image: see text] BMS-813160 (compound 3) was identified as a potent and selective CCR2/5 dual antagonist. Compound 3 displayed good permeability at pH = 7.4 in PAMPA experiments and demonstrated excellent human liver microsome stability. Pharmacokinetic studies established that 3 had excellent oral bioavailability and exhibited low clearance in dog and cyno. Compound 3 was also studied in the mouse thioglycollate-induced peritonitis model, which confirmed its ability to inhibit the migration of inflammatory monocytes and macrophages. As a result of this profile, compound 3 was selected as a clinical candidate.

Published

2021

2. Discovery of BMS-753426: A Potent Orally Bioavailable Antagonist of CC Chemokine Receptor 2

Author

Andrew J. Tebben, Sandhya Mandlekar, Michael A. Gallela, Songmei Xu, Robert J. Cherney, Mary Ellen Cvijic, Anne Rose, John V. Duncia, Mary F. Malley, Yang Michael G, Arvind Mathur, Percy H. Carter, Amy A. Sarjeant, Jian Pang, Bei Wang, Zili Xiao, Ragini Vuppugalla, Purnima Khandelwal, Qihong Zhao, Gardner Daniel S, Joseph B. Santella, Douglas G. Batt, Gregory D. Brown, and Rulin Zhao

Subjects

CCR2, 010405 organic chemistry, Chemistry, Monocyte, Organic Chemistry, Antagonist, Cyclohexylamine, Pharmacology, 01 natural sciences, Biochemistry, Reductive amination, 0104 chemical sciences, Bioavailability, 010404 medicinal & biomolecular chemistry, chemistry.chemical_compound, medicine.anatomical_structure, Pharmacokinetics, Drug Discovery, medicine, CC chemokine receptors

Abstract

[Image: see text] To improve the metabolic stability profile of BMS-741672 (1a), we undertook a structure–activity relationship study in our trisubstituted cyclohexylamine series. This ultimately led to the identification of 2d (BMS-753426) as a potent and orally bioavailable antagonist of CCR2. Compared to previous clinical candidate 1a, the tert-butyl amine 2d showed significant improvements in pharmacokinetic properties, with lower clearance and higher oral bioavailability. Furthermore, compound 2d exhibited improved affinity for CCR5 and good activity in models of both monocyte migration and multiple sclerosis in the hCCR2 knock-in mouse. The synthesis of 2d was facilitated by the development of a simplified approach to key intermediate (4R)-9b that deployed a stereoselective reductive amination which may prove to be of general interest.

Published

2021

3. Bicyclic Ligand-Biased Agonists of S1P1: Exploring Side Chain Modifications to Modulate the PK, PD, and Safety Profiles

Author

Alaric J. Dyckman, Lois D. Lehman-McKeeman, Huadong Sun, Hong Shi, Mary Ellen Cvijic, Ding Ren Shen, Xiaoxia Yang, Michael Yang, Tracy L. Taylor, Hai-Yun Xiao, Zili Xiao, Luisa Salter-Cid, Jian Pang, Percy H. Carter, Paul Levesque, Arvind Mathur, John L. Gilmore, Jenny Xie, T. G. Murali Dhar, Georgia Cornelius, Anthony M. Marino, Kim W. McIntyre, and Bethanne M. Warrack

Subjects

Chemistry, Metabolite, Arthritis, Pharmacology, medicine.disease, Ligand (biochemistry), chemistry.chemical_compound, Immune system, Pharmacokinetics, In vivo, Drug Discovery, medicine, Molecular Medicine, Receptor, PK/PD models

Abstract

Sphingosine-1-phosphate (S1P) binds to a family of sphingosine-1-phosphate G-protein-coupled receptors (S1P1-5). The interaction of S1P with these S1P receptors has a fundamental role in many physiological processes in the vascular and immune systems. Agonist-induced functional antagonism of S1P1 has been shown to result in lymphopenia. As a result, agonists of this type hold promise as therapeutics for autoimmune disorders. The previously disclosed differentiated S1P1 modulator BMS-986104 (1) exhibited improved preclinical cardiovascular and pulmonary safety profiles as compared to earlier full agonists of S1P1; however, it demonstrated a long pharmacokinetic half-life (T1/2 18 days) in the clinic and limited formation of the desired active phosphate metabolite. Optimization of this series through incorporation of olefins, ethers, thioethers, and glycols into the alkyl side chain afforded an opportunity to reduce the projected human T1/2 and improve the formation of the active phosphate metabolite while maintaining efficacy as well as the improved safety profile. These efforts led to the discovery of 12 and 24, each of which are highly potent, biased agonists of S1P1. These compounds not only exhibited shorter in vivo T1/2 in multiple species but are also projected to have significantly shorter T1/2 values in humans when compared to our first clinical candidate. In models of arthritis, treatment with 12 and 24 demonstrated robust efficacy.

Published

2021

4. Discovery of BMS-986202: A Clinical Tyk2 Inhibitor that Binds to Tyk2 JH2

Author

Jianqing Li, Daniel Smith, John S. Tokarski, Lihong Cheng, John E. Macor, Javed Khan, Adriana Zupa-Fernandez, Anil Thankappan, Chunjian Liu, Charu Chaudhry, David S. Weinstein, Percy H. Carter, Kathleen M. Gillooly, Kim W. McIntyre, Yifan Zhang, Anjaneya Chimalakonda, Joann Strnad, James Lin, James R. Burke, David J. Shuster, Manoj Chiney, Paul A. Elzinga, Max Ruzanov, Louis J. Lombardo, and Charles M. Langevine

Subjects

Cyclopropanes, TYK2 Kinase, Chemistry, Hydrogen bond, Drug discovery, Ligand, Stereochemistry, Plasma protein binding, Crystallography, X-Ray, Catalysis, Pyridazine, Mice, Structure-Activity Relationship, chemistry.chemical_compound, Amide, Drug Discovery, Animals, Humans, Psoriasis, Molecular Medicine, Structure–activity relationship, Moiety, Oxazoles, Protein Kinase Inhibitors, Protein Binding

Abstract

A search for structurally diversified Tyk2 JH2 ligands from 6 (BMS-986165), a pyridazine carboxamide-derived Tyk2 JH2 ligand as a clinical Tyk2 inhibitor currently in late development for the treatment of psoriasis, began with a survey of six-membered heteroaryl groups in place of the N-methyl triazolyl moiety in 6. The X-ray co-crystal structure of an early lead (12) revealed a potential new binding pocket. Exploration of the new pocket resulted in two frontrunners for a clinical candidate. The potential hydrogen bonding interaction with Thr599 in the pocket was achieved with a tertiary amide moiety, confirmed by the X-ray co-crystal structure of 29. When the diversity search was extended to nicotinamides, a single fluorine atom addition was found to significantly enhance the permeability, which directly led to the discovery of 7 (BMS-986202) as a clinical Tyk2 inhibitor that binds to Tyk2 JH2. The preclinical studies of 7, including efficacy studies in mouse models of IL-23-driven acanthosis, anti-CD40-induced colitis, and spontaneous lupus, will also be presented.

Published

2020

5. Aryl Ether-Derived Sphingosine-1-Phosphate Receptor (S1P1) Modulators: Optimization of the PK, PD, and Safety Profiles

Author

John L. Gilmore, Kim W. McIntyre, Lois D. Lehman-McKeeman, David Marcoux, Hai-Yun Xiao, Georgia Cornelius, Alaric J. Dyckman, Mary Ellen Cvijic, Jenny Xie, Yang Michael G, T. G. Murali Dhar, Zili Xiao, Tracy L. Taylor, Anthony M. Marino, Ding Ren Shen, Percy H. Carter, Paul Levesque, Arvind Mathur, Huadong Sun, and Hong Shi

Subjects

Bicyclic molecule, 010405 organic chemistry, Stereochemistry, Aryl, Sphingosine-1-phosphate receptor, Organic Chemistry, Ether, 01 natural sciences, Biochemistry, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, chemistry.chemical_compound, chemistry, In vivo, Drug Discovery, Potency, PK/PD models, ED50

Abstract

[Image: see text] Efforts aimed at increasing the in vivo potency and reducing the elimination half-life of 1 and 2 led to the identification of aryl ether and thioether-derived bicyclic S1P(1) differentiated modulators 3–6. The effects of analogs 3–6 on lymphocyte reduction in the rat (desired pharmacology) along with pulmonary- and cardiovascular-related effects (undesired pharmacology) are described. Optimization of the overall properties in the aryl ether series yielded 3d, and the predicted margin of safety against the cardiovascular effects of 3d would be large enough for human studies. Importantly, compared to 1 and 2, compound 3d had a better profile in both potency (ED(50) < 0.05 mg/kg) and predicted human half-life (t(1/2) ∼ 5 days).

Published

2020

6. Optimization of Nicotinamides as Potent and Selective IRAK4 Inhibitors with Efficacy in a Murine Model of Psoriasis

Author

Joel C. Barrish, John Hynes, Ajay Saxena, Natesan Murugesan, Dianlin Xie, Anjaneya Chimalakonda, Stefan Ruepp, Mitalee Das, Richard Rampulla, Durgarao Kantheti, Chunhong Yan, Julie Carman, Jignesh Nagar, Siva Subramani, Qian Ruan, William J. Pitts, Rajeev S. Bhide, Paul A. Elzinga, Venkatram Reddy Paidi, John S. Sack, Mark Fereshteh, Thangavel Soodamani, Amrita Jha Mukherjee, T. Thanga Mariappan, Ramesh Kumar Sistla, Kaushik Ghosh, Debarati Mazumder, Kamalavenkatesh Palanisamy, Deborah A. Holloway, Susan E. Kiefer, John A. Newitt, Satheesh Kesavan Nair, Polimera Subba Rao, Shailesh Dudhgoankar, Percy H. Carter, Xin Li, Srinivas Maddi, S. Pon Saravanakumar, Sreekantha Ratna Kumar, and Sucharita Bose

Subjects

Nicotinamide, Organic Chemistry, TLR7, Pharmacology, IRAK4, medicine.disease, Biochemistry, chemistry.chemical_compound, chemistry, Pharmacokinetics, Pharmacodynamics, Psoriasis, Drug Discovery, medicine, Potency, Kinome

Abstract

[Image: see text] IRAK4 is an attractive therapeutic target for the treatment of inflammatory conditions. Structure guided optimization of a nicotinamide series of inhibitors has been expanded to explore the IRAK4 front pocket. This has resulted in the identification of compounds such as 12 with improved potency and selectivity. Additionally 12 demonstrated activity in a pharmacokinetics/pharmacodynamics (PK/PD) model. Further optimization efforts led to the identification of the highly kinome selective 21, which demonstrated a robust PD effect and efficacy in a TLR7 driven model of murine psoriasis.

Published

2020

7. Rationally Designed, Conformationally Constrained Inverse Agonists of RORγt—Identification of a Potent, Selective Series with Biologic-Like in Vivo Efficacy

Author

Carolyn A. Weigelt, Sha Li, David Marcoux, Georgia Cornelius, Qihong Zhao, Mary Ellen Cvijic, John E. Macor, Jingwu Duan, Melissa Yarde, Muthalagu Vetrichelvan, David J. Shuster, Qingjie Liu, Richard Rampulla, Kim W. McIntyre, Mary T. Obermeier, Shiuhang Yip, Purnima Khandelwal, Sureshbabu Vishwakrishnan, Anuradha Gupta, Virna Borowski, Peng Li, Kevin Stefanski, Sridharan Ramlingam, Myra Beaudoin-Bertrand, Nageswara Maddala, Sridhar Vanteru, Percy H. Carter, Arvind Mathur, Aberra Fura, Max Ruzanov, John Hynes, Dauh-Rurng Wu, Jinhong Wang, Luisa Salter-Cid, John S. Sack, Cornelius Lyndon A M, Anurag S. Srivastava, Robert J. Cherney, Kumaravel Selvakumar, Mushkin Basha, Arun Kumar Gupta, Douglas G. Batt, Rex Denton, Sukhen Karmakar, Qing Shi, Ananta Karmakar, Naveen Manjunath, Javed Khan, Jenny Xie, Joseph A. Tino, and T. G. Murali Dhar

Subjects

Models, Molecular, Pyrrolidines, Drug Inverse Agonism, Protein Conformation, Pharmacology, 01 natural sciences, Jurkat Cells, Mice, Structure-Activity Relationship, 03 medical and health sciences, Psoriatic arthritis, RAR-related orphan receptor gamma, In vivo, Drug Discovery, medicine, Animals, Humans, Inverse agonist, Structure–activity relationship, Tissue Distribution, 030304 developmental biology, 0303 health sciences, Chemistry, Nuclear Receptor Subfamily 1, Group F, Member 3, medicine.disease, In vitro, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Nuclear receptor, Drug Design, Molecular Medicine

Abstract

RORγt is an important nuclear receptor that regulates the production of several pro-inflammatory cytokines such as IL-17 and IL-22. As a result, RORγt has been identified as a potential target for the treatment of various immunological disorders such as psoriasis, psoriatic arthritis, and inflammatory bowel diseases. Structure and computer-assisted drug design led to the identification of a novel series of tricyclic RORγt inverse agonists with significantly improved in vitro activity in the reporter (Gal4) and human whole blood assays compared to our previous chemotype. Through careful structure activity relationship, several potent and selective RORγt inverse agonists have been identified. Pharmacokinetic studies allowed the identification of the lead molecule 32 with a low peak-to-trough ratio. This molecule showed excellent activity in an IL-2/IL-23-induced mouse pharmacodynamic study and demonstrated biologic-like efficacy in an IL-23-induced preclinical model of psoriasis.

Published

2019

8. Identification of potent, selective and orally bioavailable phenyl ((R)-3-phenylpyrrolidin-3-yl)sulfone analogues as RORγt inverse agonists

Author

Zhonghui Lu, James J.-W. Duan, Haiyun Xiao, James Neels, Dauh-Rurng Wu, Carolyn A. Weigelt, John S. Sack, Javed Khan, Max Ruzanov, Yongmi An, Melissa Yarde, Ananta Karmakar, Sureshbabu Vishwakrishnan, Venkata Baratam, Harisha Shankarappa, Sridhar Vanteru, Venkatesh Babu, Mushkin Basha, Arun Kumar Gupta, Selvakumar Kumaravel, Arvind Mathur, Qihong Zhao, Luisa M. Salter-Cid, Percy H. Carter, and T.G. Murali Dhar

Subjects

Models, Molecular, Pyrrolidines, Dose-Response Relationship, Drug, Drug Inverse Agonism, Molecular Structure, Organic Chemistry, Clinical Biochemistry, Administration, Oral, Biological Availability, Pharmaceutical Science, Nuclear Receptor Subfamily 1, Group F, Member 3, Crystallography, X-Ray, Biochemistry, Mice, Structure-Activity Relationship, Drug Discovery, Animals, Humans, Molecular Medicine, Sulfones, Molecular Biology

Abstract

An X-ray crystal structure of one of our previously discovered RORγt inverse agonists bound to the RORγt ligand binding domain revealed that the cyclohexane carboxylic acid group of compound 2 plays a significant role in RORγt binding, forming four hydrogen bonding and ionic interactions with RORγt. SAR studies centered around the cyclohexane carboxylic acid group led to identification of several structurally diverse and more potent compounds, including new carboxylic acid analogues 7 and 20, and cyclic sulfone analogues 34 and 37. Notably, compounds 7 and 20 were found to maintain the desirable pharmacokinetic profile of 2.

Published

2019

9. Identification of N-Methyl Nicotinamide and N-Methyl Pyridazine-3-Carboxamide Pseudokinase Domain Ligands as Highly Selective Allosteric Inhibitors of Tyrosine Kinase 2 (TYK2)

Author

Yanlei Zhang, Jeffrey Tredup, Mertzman Michael E, Nelly Aranibar, Kim W. McIntyre, Kathleen M. Gillooly, Jodi K. Muckelbauer, James R. Burke, Lihong Cheng, Joann Strnad, Celia D’Arienzo, Dawn Mulligan, Stephen T. Wrobleski, Charu Chaudhry, Adriana Zupa-Fernandez, Percy H. Carter, Dianlin Xie, Manoj Chiney, Elizabeth M. Heimrich, Moslin Ryan M, Christine Huang, Xiaoxia Yang, Shuqun Lin, David S. Weinstein, Tokarski John S, Chiehying Chang, Louis J. Lombardo, Huadong Sun, and Steven H. Spergel

Subjects

Nicotinamide, medicine.drug_class, Allosteric regulation, Carboxamide, Pyridazine, chemistry.chemical_compound, chemistry, Biochemistry, Tyrosine kinase 2, Drug Discovery, medicine, Molecular Medicine, Structure–activity relationship, Transferase, Tyrosine kinase

Abstract

As a member of the Janus (JAK) family of nonreceptor tyrosine kinases, TYK2 plays an important role in mediating the signaling of pro-inflammatory cytokines including IL-12, IL-23, and type 1 interferons. The nicotinamide 4, identified by a SPA-based high-throughput screen targeting the TYK2 pseudokinase domain, potently inhibits IL-23 and IFNα signaling in cellular assays. The described work details the optimization of this poorly selective hit (4) to potent and selective molecules such as 47 and 48. The discoveries described herein were critical to the eventual identification of the clinical TYK2 JH2 inhibitor (see following report in this issue). Compound 48 provided robust inhibition in a mouse IL-12-induced IFNγ pharmacodynamic model as well as efficacy in an IL-23 and IL-12-dependent mouse colitis model. These results demonstrate the ability of TYK2 JH2 domain binders to provide a highly selective alternative to conventional TYK2 orthosteric inhibitors.

Published

2019

10. Development of a Scalable Synthesis for the Potent Kinase Inhibitor BMS-986236; 1-(5-(4-(3-Hydroxy-3-methylbutyl)-1H-1,2,3-triazol-1-yl)-4-(isopropylamino)pyridin-2-yl)-1H-pyrazolo[3,4-b]pyridine-5-carbonitrile

Author

Lokesh Babu Jarugu, Suresh Krishnamoorthy, Anuradha Gupta, Muniyappa Shankar, Prakasam Kuppusamy, Satheesh Kesavan Nair, Joseph B. Santella, Muthalagu Vetrichelvan, Pirama Nayagam Arunachalam, Roshan Y. Nimje, Sridhar Vanteru, Arvind Mathur, Percy H. Carter, China Anki Reddy, Prakash Anjanappa, Nanjundaswamy Kanikahalli Chikkananjaiah, Sivakumar Ganesan, Richard Rampulla, Arun Kumar Gupta, Nageswararao Maddala, Murali Botlagunta, and John Hynes

Subjects

010405 organic chemistry, Kinase, Organic Chemistry, Triazole, 010402 general chemistry, 01 natural sciences, Combinatorial chemistry, 0104 chemical sciences, chemistry.chemical_compound, Column chromatography, chemistry, Pyridine, Azide, Physical and Theoretical Chemistry

Abstract

A scalable route to 1-(5-(4-(3-hydroxy-3-methylbutyl)-1H-1,2,3-triazol-1-yl)-4-(isopropylamino)pyridin-2-yl)-1H-pyrazolo[3,4-b]pyridine-5-carbonitrile (1, BMS-986236) was developed by incorporating an alternate azide intermediate following safety-driven processes. The newly developed process involved mitigating safety hazards and eliminating the column chromatography purification. The issue of trace metal contamination in the final API observed in the first-generation synthesis has been overcome.

Published

2019

11. Identification of Imidazo[1,2-b]pyridazine Derivatives as Potent, Selective, and Orally Active Tyk2 JH2 Inhibitors

Author

Charu Chaudhry, Percy H. Carter, Moslin Ryan M, Celia D’Arienzo, James Lin, Jodi K. Muckelbauer, Luisa Salter-Cid, Tracy L. Taylor, Kim W. McIntyre, Chunjian Liu, James R. Burke, Paul A. Elzinga, Hyunsoo Park, Kathleen M. Gillooly, Chiehying Chang, Dianlin Xie, Jing Chen, Lihong Cheng, David S. Weinstein, Cliff Chen, Jeffrey Tredup, Huadong Sun, Peng Li, Louis J. Lombardo, Adriana Zupa-Fernandez, Joann Strnad, John S. Tokarski, Dauh-Rurng Wu, and Nelly Aranibar

Subjects

chemistry.chemical_classification, 010405 organic chemistry, Hydrogen bond, Stereochemistry, Aryl, Organic Chemistry, Ring (chemistry), 01 natural sciences, Biochemistry, 0104 chemical sciences, Pyridazine, 010404 medicinal & biomolecular chemistry, chemistry.chemical_compound, chemistry, Tyrosine kinase 2, Pharmacodynamics, Intramolecular force, Drug Discovery, Alkyl

Abstract

In sharp contrast to a previously reported series of 6-anilino imidazopyridazine based Tyk2 JH2 ligands, 6-((2-oxo-N1-substituted-1,2-dihydropyridin-3-yl)amino)imidazo[1,2-b]pyridazine analogs were found to display dramatically improved metabolic stability. The N1-substituent on 2-oxo-1,2-dihydropyridine ring can be a variety of alkyl, aryl, and heteroaryl groups, but among them, 2-pyridyl provided much enhanced Caco-2 permeability, attributed to its ability to form intramolecular hydrogen bonds. Further structure-activity relationship studies at the C3 position led to the identification of highly potent and selective Tyk2 JH2 inhibitor 6, which proved to be highly effective in inhibiting IFNγ production in a rat pharmacodynamics model and fully efficacious in a rat adjuvant arthritis model.

Published

2019

12. Identification and Preclinical Pharmacology of ((1R,3S)-1-Amino-3-((S)-6-(2-methoxyphenethyl)-5,6,7,8-tetrahydronaphthalen-2-yl)cyclopentyl)methanol (BMS-986166): A Differentiated Sphingosine-1-phosphate Receptor 1 (S1P1) Modulator Advanced into Clinical Trials

Author

Lloyd Lecureux, Elizabeth M. Heimrich, Rochelle Thomas, Lois D. Lehman-McKeeman, Hai-Yun Xiao, Georgia Cornelius, Zheng Yang, Alaric J. Dyckman, Anuradha Gupta, Percy H. Carter, Yu-Wen Li, Paul Levesque, Tracy L. Taylor, Zili Xiao, Mary Ellen Cvijic, Arvind Mathur, John L. Gilmore, Lei Gong, Jenny Xie, Marta Dabros, Ding Ren Shen, Xiaoxia Yang, T. G. Murali Dhar, Xia D. Zhou, Yang Michael G, Bala Pragalathan, Huadong Sun, Anthony M. Marino, Hong Shi, Dauh-Rurng Wu, Richard Rampulla, Kim W. McIntyre, Cliff Chen, Luisa Salter-Cid, Bethanne M. Warrack, Celia D’Arienzo, and Virna Borowski

Subjects

Agonist, 0303 health sciences, medicine.drug_class, Sphingosine-1-phosphate receptor, Metabolite, Pharmacology, 01 natural sciences, Fingolimod, Partial agonist, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, 03 medical and health sciences, chemistry.chemical_compound, chemistry, Pharmacokinetics, In vivo, Pharmacodynamics, Drug Discovery, medicine, Molecular Medicine, 030304 developmental biology, medicine.drug

Abstract

Recently, our research group reported the identification of BMS-986104 (2) as a differentiated S1P1 receptor modulator. In comparison to fingolimod (1), a full agonist of S1P1 currently marketed for the treatment of relapse remitting multiple sclerosis (RRMS), 2 offers several potential advantages having demonstrated improved safety multiples in preclinical evaluations against undesired pulmonary and cardiovascular effects. In clinical trials, 2 was found to exhibit a pharmacokinetic half-life (T1/2) longer than that of 1, as well as a reduced formation of the phosphate metabolite that is required for activity against S1P1. Herein, we describe our efforts to discover highly potent, partial agonists of S1P1 with a shorter T1/2 and increased in vivo phosphate metabolite formation. These efforts culminated in the discovery of BMS-986166 (14a), which was advanced to human clinical evaluation. The pharmacokinetic/pharmacodynamic (PK/PD) relationship as well as pulmonary and cardiovascular safety assessments ar...

Published

2019

13. Bicyclic Ligand-Biased Agonists of S1P

Author

John L, Gilmore, Hai-Yun, Xiao, T G Murali, Dhar, Michael, Yang, Zili, Xiao, Xiaoxia, Yang, Tracy L, Taylor, Kim W, McIntyre, Bethanne M, Warrack, Hong, Shi, Paul C, Levesque, Anthony M, Marino, Georgia, Cornelius, Arvind, Mathur, Ding Ren, Shen, Jian, Pang, Mary Ellen, Cvijic, Lois D, Lehman-McKeeman, Huadong, Sun, Jenny, Xie, Luisa, Salter-Cid, Percy H, Carter, and Alaric J, Dyckman

Subjects

Lung Diseases, Male, Serine Endopeptidases, Drug Evaluation, Preclinical, Arthritis, Experimental, Autoimmune Diseases, Rats, Bridged Bicyclo Compounds, Chemotaxis, Leukocyte, Structure-Activity Relationship, Rats, Inbred Lew, Animals, Humans, Myocytes, Cardiac, Proprotein Convertases, Phosphorylation, Bronchoalveolar Lavage Fluid, Biotransformation, Half-Life

Abstract

Sphingosine-1-phosphate (S1P) binds to a family of sphingosine-1-phosphate G-protein-coupled receptors (S1P

Published

2021

14. Driving Potency with Rotationally Stable Atropisomers: Discovery of Pyridopyrimidinedione-Carbazole Inhibitors of BTK

Author

Soo S. Ko, James Kempson, Yingru Zhang, Tracy L. Taylor, Kim W. McIntyre, James R. Burke, Luisa Salter-Cid, Shiuhang Yip, Celia D’Arienzo, Aberra Fura, Stacey Skala, Joseph A. Tino, Jun Dai, Chunlei Wang, Joel C. Barrish, Michael Galella, Kathleen M. Gillooly, Bei Wang, Dauh-Rurng Wu, Lorell Discenza, Xiaoping Hou, Arvind Mathur, Richard Rampulla, Dawn Sun, Scott H. Watterson, Mary T. Obermeier, Percy H. Carter, Mark A. Pattoli, Anurag S. Srivastava, Lihong Cheng, Rulin Zhao, Peng Li, Claudine Pulicicchio, Joseph Pawluczyk, and Rodney Vickery

Subjects

Autoimmune disease, Atropisomer, biology, Stereochemistry, Carbazole, Organic Chemistry, medicine.disease, Biochemistry, Small molecule, chemistry.chemical_compound, chemistry, Drug Discovery, medicine, biology.protein, Bruton's tyrosine kinase, Kinase activity, Chirality (chemistry), Tyrosine kinase

Abstract

[Image: see text] Bruton’s tyrosine kinase (BTK) has been shown to play a key role in the pathogenesis of autoimmunity. Therefore, the inhibition of the kinase activity of BTK with a small molecule inhibitor could offer a breakthrough in the clinical treatment of many autoimmune diseases. This Letter describes the discovery of BMS-986143 through systematic structure–activity relationship (SAR) development. This compound benefits from defined chirality derived from two rotationally stable atropisomeric axes, providing a potent and selective single atropisomer with desirable efficacy and tolerability profiles.

Published

2020

15. Discovery of Potent and Orally Bioavailable Small Molecule Antagonists of Toll-like Receptors 7/8/9 (TLR7/8/9)

Author

Shana L. Posy, David A Critton, Stefan Ruepp, Ratna Kumar Sreekantha, Laxman Pasunoori, Dharmpal S. Dodd, Murali Subramanian, Andrew Watson, Percy H. Carter, Honghe Wan, Debarati Mazumder Tagore, Paul Davies, Shailesh Dudhgaonkar, Gary L. Schieven, Ratika Srivastava, Luisa Salter-Cid, Michael A. Poss, Alaric J. Dyckman, and Mussari Christopher P

Subjects

Autoimmune disease, Toll-like receptor, Innate immune system, 010405 organic chemistry, Organic Chemistry, virus diseases, Context (language use), TLR7, Pharmacology, TLR8, Biology, medicine.disease_cause, medicine.disease, 01 natural sciences, Biochemistry, 0104 chemical sciences, Autoimmunity, 010404 medicinal & biomolecular chemistry, Drug Discovery, medicine, Receptor

Abstract

[Image: see text] The toll-like receptor (TLR) family is an evolutionarily conserved component of the innate immune system, responsible for the early detection of foreign or endogenous threat signals. In the context of autoimmunity, the unintended recognition of self-motifs as foreign promotes initiation or propagation of disease. Overactivation of TLR7 and TLR9 have been implicated as factors contributing to autoimmune disorders such as psoriasis, arthritis, and lupus. In our search for small molecule antagonists of TLR7/9, 7f was identified as possessing excellent on-target potency for human TLR7/9 as well as for TLR8, with selectivity against other representative TLR family members. Good pharmacokinetic properties and a relatively balanced potency against TLR7 and TLR9 in mouse systems (systems which lack functional TLR8) made this an excellent in vivo tool compound, and efficacy from oral dosing in preclinical models of autoimmune disease was demonstrated.

Published

2020

16. Discovery of 2,6-difluorobenzyl ether series of phenyl ((R)-3-phenylpyrrolidin-3-yl)sulfones as surprisingly potent, selective and orally bioavailable RORγt inverse agonists

Author

Bin Jiang, Sylwia Stachura, T. G. Murali Dhar, Carolyn A. Weigelt, Dauh Rurng Wu, Jingwu Duan, Luisa M. Salter–Cid, Javed Khan, Ding Ren Shen, Melissa Yarde, Qihong Zhao, Zhonghui Lu, Percy H. Carter, John S. Sack, and Max Ruzanov

Subjects

Pyrrolidines, Drug Inverse Agonism, Stereochemistry, Clinical Biochemistry, Pharmaceutical Science, Ether, Alcohol, Crystallography, X-Ray, 01 natural sciences, Biochemistry, Sulfone, chemistry.chemical_compound, Mice, Structure-Activity Relationship, Drug Stability, In vivo, Drug Discovery, Moiety, Inverse agonist, Animals, Humans, Sulfones, Binding site, Molecular Biology, Pregnane X receptor, Molecular Structure, 010405 organic chemistry, Chemistry, Organic Chemistry, Hep G2 Cells, Nuclear Receptor Subfamily 1, Group F, Member 3, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Microsomes, Liver, Molecular Medicine

Abstract

In an effort to discover oral inverse agonists of RORγt to treat inflammatory diseases, a new 2,6–difluorobenzyl ether series of cyclopentyl sulfones were found to be surprisingly more potent than the corresponding alcohol derivatives. When combined with a more optimized phenyl ((R)–3–phenylpyrrolidin–3–yl)sulfone template, the 2,6–difluorobenzyl ethers yielded a set of very potent RORγt inverse agonists (e.g., compound 26, RORγt Gal4 EC50 11 nM) that are highly selective against PXR, LXRα and LXRβ. After optimizing for stability in human and mouse liver microsomes, compounds 29 and 38 were evaluated in vivo and found to have good oral bioavailability (56% and 101%, respectively) in mice. X–ray co–crystal structure of compound 27 in RORγt revealed that the bulky benzyl ether group causes helix 11 of the protein to partially uncoil to create a new, enlarged binding site, which nicely accommodates the benzyl ether moiety, leading to net potency gain.

Published

2020

17. Use of a Conformational-Switching Mechanism to Modulate Exposed Polarity: Discovery of CCR2 Antagonist BMS-741672

Author

Mary Ellen Cvijic, Andrew J. Tebben, Jian Pang, Mary F. Malley, Ruowei Mo, Joseph B. Santella, Songmei Xu, Qihong Zhao, Douglas G. Batt, Jing Chen, Anne Rose, Bei Wang, Hong Shi, Marta Dabros, Anurag S. Srivastava, Percy H. Carter, Purnima Khandelwal, Yang Michael G, Gardner Daniel S, Gregory D. Brown, Sandhya Mandlekar, Michael Galella, Rulin Zhao, Zili Xiao, John V. Duncia, Sarah C. Traeger, Joel C. Barrish, Robert J. Cherney, and Soo S. Ko

Subjects

education.field_of_study, Membrane permeability, 010405 organic chemistry, Chemistry, Organic Chemistry, Population, 01 natural sciences, Biochemistry, 0104 chemical sciences, Polar surface area, Bioavailability, 010404 medicinal & biomolecular chemistry, Drug Discovery, Side chain, Biophysics, Selectivity, education, Conformational isomerism, Ion channel

Abstract

[Image: see text] We encountered a dilemma in the course of studying a series of antagonists of the G-protein coupled receptor CC chemokine receptor-2 (CCR2): compounds with polar C3 side chains exhibited good ion channel selectivity but poor oral bioavailability, whereas compounds with lipophilic C3 side chains exhibited good oral bioavailability in preclinical species but poor ion channel selectivity. Attempts to solve this through the direct modulation of physicochemical properties failed. However, the installation of a protonation-dependent conformational switching mechanism resolved the problem because it enabled a highly selective and relatively polar molecule to access a small population of a conformer with lower polar surface area and higher membrane permeability. Optimization of the overall properties in this series yielded the CCR2 antagonist BMS-741672 (7), which embodied properties suitable for study in human clinical trials.

Published

2019

18. Discovery of BMS-986251: A Clinically Viable, Potent, and Selective RORγt Inverse Agonist

Author

Qingjie Liu, Mary T. Obermeier, John S. Sack, Carolyn A. Weigelt, Georgia Cornelius, Percy H. Carter, David J. Shuster, Luisa Salter-Cid, Aberra Fura, Virna Borowski, Jingwu Duan, Purnima Khandelwal, Qing Shi, Robert J. Cherney, Cornelius Lyndon A M, Jinhong Wang, Jenny Xie, Max Ruzanov, Kevin Stefanski, Rex Denton, T. G. Murali Dhar, David Marcoux, Shiuhang Yip, Melissa Yarde, Douglas G. Batt, Javed Khan, Joseph A. Tino, Qihong Zhao, Anurag S. Srivastava, Arvind Mathur, Mary Ellen Cvijic, John E. Macor, Sha Li, and Dauh-Rurng Wu

Subjects

chemistry.chemical_classification, 010405 organic chemistry, Chemistry, Organic Chemistry, Inflammation, Acanthosis, Pharmacology, medicine.disease, 01 natural sciences, Biochemistry, 0104 chemical sciences, Bioavailability, 010404 medicinal & biomolecular chemistry, Pharmacokinetics, Pharmacodynamics, Drug Discovery, medicine, Inverse agonist, medicine.symptom, Whole blood, Tricyclic

Abstract

[Image: see text] Novel tricyclic analogues were designed, synthesized, and evaluated as RORγt inverse agonists. Several of these compounds were potent in an IL-17 human whole blood assay and exhibited excellent oral bioavailability in mouse pharmacokinetic studies. This led to the identification of compound 5, which displayed dose-dependent inhibition of IL-17F production in a mouse IL-2/IL-23 stimulated pharmacodynamic model. In addition, compound 5 was studied in mouse acanthosis and imiquimod-induced models of skin inflammation, where it demonstrated robust efficacy comparable to a positive control. As a result of this excellent overall profile, compound 5 (BMS-986251) was selected as a clinically viable developmental candidate.

Published

2020

19. Identification of bicyclic hexafluoroisopropyl alcohol sulfonamides as retinoic acid receptor-related orphan receptor gamma (RORγ/RORc) inverse agonists. Employing structure-based drug design to improve pregnane X receptor (PXR) selectivity

Author

Celia D’Arienzo, Ananta Karmakar, Marta Dabros, Michael Galella, Jingwu Duan, John S. Sack, Dhanya Kumar Raut, David S. Weinstein, Andrew T. Pudzianowski, Ding-Ren Shen, Sylwia Stachura, Joel C. Barrish, Arun Kumar Gupta, Huadong Sun, William R. Foster, Javed Khan, Melissa Yarde, Dan Camac, Lauren Haque, Qihong Zhao, Dauh-Rurng Wu, Carolyn A. Weigelt, Faye Wang, Percy H. Carter, Luisa Salter-Cid, Hemalatha Hemagiri, Jenny Xie, T. G. Murali Dhar, Zhonghui Lu, Virna Borowski, Hua Gong, and John E. Somerville

Subjects

Male, Models, Molecular, 0301 basic medicine, Receptors, Steroid, Propanols, Receptors, Retinoic Acid, Clinical Biochemistry, Pharmaceutical Science, Benzothiazine, Pharmacology, Crystallography, X-Ray, 01 natural sciences, Biochemistry, Bridged Bicyclo Compounds, Mice, Structure-Activity Relationship, 03 medical and health sciences, chemistry.chemical_compound, RAR-related orphan receptor gamma, Drug Discovery, Animals, Humans, Inverse agonist, Liver X receptor, Receptor, Molecular Biology, Liver X Receptors, Orphan receptor, Mice, Inbred BALB C, Sulfonamides, Pregnane X receptor, Dose-Response Relationship, Drug, Molecular Structure, Organic Chemistry, Pregnane X Receptor, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Retinoic acid receptor, 030104 developmental biology, chemistry, Drug Design, Molecular Medicine

Abstract

We disclose the optimization of a high throughput screening hit to yield benzothiazine and tetrahydroquinoline sulfonamides as potent RORγt inverse agonists. However, a majority of these compounds showed potent activity against pregnane X receptor (PXR) and modest activity against liver X receptor α (LXRα). Structure-based drug design (SBDD) led to the identification of benzothiazine and tetrahydroquinoline sulfonamide analogs which completely dialed out LXRα activity and were less potent at PXR. Pharmacodynamic (PD) data for compound 35 in an IL-23 induced IL-17 mouse model is discussed along with the implications of a high Ymax in the PXR assay for long term preclinical pharmacokinetic (PK) studies.

Published

2018

20. Highly Selective Inhibition of Tyrosine Kinase 2 (TYK2) for the Treatment of Autoimmune Diseases: Discovery of the Allosteric Inhibitor BMS-986165

Author

Max Ruzanov, David J. Shuster, Manoj Chiney, Kim W. McIntyre, James R. Burke, Celia D’Arienzo, Nelly Aranibar, Elizabeth M. Heimrich, Louis J. Lombardo, Dianlin Xie, Moslin Ryan M, Joann Strnad, Anjaneya Chimalakonda, Lihong Cheng, James Kempson, Adriana Zupa-Fernandez, Javed Khan, Charu Chaudhry, Huadong Sun, Shuqun Lin, Percy H. Carter, Steven H. Spergel, Christine Huang, Dawn Mulligan, Stephen T. Wrobleski, Kathleen M. Gillooly, Yanlei Zhang, Jeffrey Tredup, David S. Weinstein, Tokarski John S, William J. Pitts, and Xiaoxia Yang

Subjects

Gene isoform, Allosteric regulation, Crystallography, X-Ray, 01 natural sciences, Autoimmune Diseases, 03 medical and health sciences, Mice, Allosteric Regulation, Heterocyclic Compounds, Drug Discovery, medicine, Animals, Humans, Kinome, Protein Kinase Inhibitors, 030304 developmental biology, Autoimmune disease, TYK2 Kinase, 0303 health sciences, Kinase Family, Chemistry, medicine.disease, Highly selective, Small molecule, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Tyrosine kinase 2, Cancer research, Molecular Medicine

Abstract

Small molecule JAK inhibitors have emerged as a major therapeutic advancement in treating autoimmune diseases. The discovery of isoform selective JAK inhibitors that traditionally target the catalytically active site of this kinase family has been a formidable challenge. Our strategy to achieve high selectivity for TYK2 relies on targeting the TYK2 pseudokinase (JH2) domain. Herein we report the late stage optimization efforts including a structure-guided design and water displacement strategy that led to the discovery of BMS-986165 (11) as a high affinity JH2 ligand and potent allosteric inhibitor of TYK2. In addition to unprecedented JAK isoform and kinome selectivity, 11 shows excellent pharmacokinetic properties with minimal profiling liabilities and is efficacious in several murine models of autoimmune disease. On the basis of these findings, 11 appears differentiated from all other reported JAK inhibitors and has been advanced as the first pseudokinase-directed therapeutic in clinical development as an oral treatment for autoimmune diseases.

Published

2019

21. Identification of

Author

Ryan, Moslin, Yanlei, Zhang, Stephen T, Wrobleski, Shuqun, Lin, Michael, Mertzman, Steven, Spergel, John S, Tokarski, Joann, Strnad, Kathleen, Gillooly, Kim W, McIntyre, Adriana, Zupa-Fernandez, Lihong, Cheng, Huadong, Sun, Charu, Chaudhry, Christine, Huang, Celia, D'Arienzo, Elizabeth, Heimrich, Xiaoxia, Yang, Jodi K, Muckelbauer, ChiehYing, Chang, Jeffrey, Tredup, Dawn, Mulligan, Dianlin, Xie, Nelly, Aranibar, Manoj, Chiney, James R, Burke, Louis, Lombardo, Percy H, Carter, and David S, Weinstein

Subjects

Niacinamide, TYK2 Kinase, Mice, Structure-Activity Relationship, Allosteric Regulation, Nicotinic Acids, Animals, Humans, Ligands, Protein Kinase Inhibitors

Abstract

As a member of the Janus (JAK) family of nonreceptor tyrosine kinases, TYK2 plays an important role in mediating the signaling of pro-inflammatory cytokines including IL-12, IL-23, and type 1 interferons. The nicotinamide

Published

2019

22. Discovery of Branebrutinib (BMS-986195): A Strategy for Identifying a Highly Potent and Selective Covalent Inhibitor Providing Rapid in Vivo Inactivation of Bruton's Tyrosine Kinase (BTK)

Author

Richard Rampulla, Stacey Skala, Charu Chaudhry, Percy H. Carter, Alban Allentoff, Tracy L. Taylor, Ling Li, Andrew J. Tebben, Luisa Salter-Cid, Aberra Fura, Rulin Zhao, Ian M. Catlett, Richard A. Westhouse, Myra Beaudoin Bertrand, John E. Macor, Robin Moore, Celia D’Arienzo, Matt Pokross, Douglas G. Batt, Scott H. Watterson, Mary T. Obermeier, Qingjie Liu, Daniel Smith, Lorell Discenza, Michael Galella, Jun Dai, Arvind Mathur, Kathleen M. Gillooly, Elizabeth M. Heimrich, Jianqing Li, Zheng Yang, Michael Wallace, Kim W. McIntyre, James R. Burke, Mark A. Pattoli, Joseph A. Tino, Lihong Cheng, Naiyu Zheng, Rodney Vickery, Claudine Pulicicchio, Yifan Zhang, Qian Ruan, and Paul A. Elzinga

Subjects

Indoles, B-cell receptor, 01 natural sciences, Arthritis, Rheumatoid, 03 medical and health sciences, Inhibitory Concentration 50, Mice, Piperidines, immune system diseases, In vivo, hemic and lymphatic diseases, Drug Discovery, Agammaglobulinaemia Tyrosine Kinase, Bruton's tyrosine kinase, Animals, Humans, Lupus Erythematosus, Systemic, Receptor, Protein Kinase Inhibitors, 030304 developmental biology, 0303 health sciences, biology, Dose-Response Relationship, Drug, Kinase, Drug discovery, Chemistry, breakpoint cluster region, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Macaca fascicularis, Cancer research, biology.protein, Molecular Medicine, Tyrosine kinase

Abstract

Bruton’s tyrosine kinase (BTK), a non-receptor tyrosine kinase, is a member of the Tec family of kinases and is essential for B cell receptor (BCR) mediated signaling. BTK also plays a critical role in the downstream signaling pathways for the Fcγ receptor in monocytes, the Fce receptor in granulocytes, and the RANK receptor in osteoclasts. As a result, pharmacological inhibition of BTK is anticipated to provide an effective strategy for the clinical treatment of autoimmune diseases such as rheumatoid arthritis and lupus. This article will outline the evolution of our strategy to identify a covalent, irreversible inhibitor of BTK that has the intrinsic potency, selectivity, and pharmacokinetic properties necessary to provide a rapid rate of inactivation systemically following a very low dose. With excellent in vivo efficacy and a very desirable tolerability profile, 5a (branebrutinib, BMS-986195) has advanced into clinical studies.

Published

2019

23. Structure-based Discovery of Phenyl (3-Phenylpyrrolidin-3-yl)sulfones as Selective, Orally Active RORγt Inverse Agonists

Author

John S. Sack, Sylwia Stachura, Bin Jiang, Sridhar Vanteru, Percy H. Carter, Lisa Zhang, Max Ruzanov, Javed Khan, Zhonghui Lu, Jenny Xie, Jingwu Duan, Qihong Zhao, Ding-Ren Shen, Luisa Salter-Cid, T. G. Murali Dhar, Dauh-Rurng Wu, Arvind Mathur, David J. Shuster, Virna Borowski, Arun Kumar Gupta, Carolyn A. Weigelt, Michael Galella, William R. Foster, and Melissa Yarde

Subjects

chemistry.chemical_classification, Sulfonyl, Bicyclic molecule, 010405 organic chemistry, Stereochemistry, Organic Chemistry, 01 natural sciences, Biochemistry, Pyrrolidine, 0104 chemical sciences, Sulfonamide, Sulfone, 010404 medicinal & biomolecular chemistry, chemistry.chemical_compound, chemistry, Oral administration, Drug Discovery, Inverse agonist, Selectivity

Abstract

[Image: see text] A new phenyl (3-phenylpyrrolidin-3-yl)sulfone series of RORγt inverse agonists was discovered utilizing the binding conformation of previously reported bicyclic sulfonamide 1. Through a combination of structure-based design and structure–activity relationship studies, a polar set of amides at N1-position of the pyrrolidine ring and perfluoroisopropyl group at para-position of the 3-phenyl group were identified as critical structural elements to achieve high selectivity against PXR, LXRα, and LXRβ. Further optimization led to the discovery of (1R,4r)-4-((R)-3-((4-fluorophenyl)sulfonyl)-3-(4-(perfluoropropan-2-yl)phenyl)pyrrolidine-1-carbonyl)cyclohexane-1-carboxylic acid (26), which displayed excellent selectivity, desirable liability and pharmacokinetic properties in vitro, and a good pharmacokinetic profile in mouse. Oral administration of 26 demonstrated dose-dependent inhibition of IL-17 production in a mouse IL-2/IL-23-induced pharmacodynamic model and biologic-like efficacy in an IL-23-induced mouse acanthosis model.

Published

2019

24. Identification and Preclinical Pharmacology of ((1 R,3 S)-1-Amino-3-(( S)-6-(2-methoxyphenethyl)-5,6,7,8-tetrahydronaphthalen-2-yl)cyclopentyl)methanol (BMS-986166): A Differentiated Sphingosine-1-phosphate Receptor 1 (S1P

Author

John L, Gilmore, Hai-Yun, Xiao, T G Murali, Dhar, Michael G, Yang, Zili, Xiao, Jenny, Xie, Lois D, Lehman-McKeeman, Lei, Gong, Huadong, Sun, Lloyd, Lecureux, Cliff, Chen, Dauh-Rurng, Wu, Marta, Dabros, Xiaoxia, Yang, Tracy L, Taylor, Xia D, Zhou, Elizabeth M, Heimrich, Rochelle, Thomas, Kim W, McIntyre, Virna, Borowski, Bethanne M, Warrack, Yuwen, Li, Hong, Shi, Paul C, Levesque, Zheng, Yang, Anthony M, Marino, Georgia, Cornelius, Celia J, D'Arienzo, Arvind, Mathur, Richard, Rampulla, Anuradha, Gupta, Bala, Pragalathan, Ding Ren, Shen, Mary Ellen, Cvijic, Luisa M, Salter-Cid, Percy H, Carter, and Alaric J, Dyckman

Subjects

Clinical Trials as Topic, Dose-Response Relationship, Drug, Tetrahydronaphthalenes, Rats, Inbred Lew, Animals, Humans, Naphthalenes, Bronchoalveolar Lavage Fluid, Sphingosine-1-Phosphate Receptors, Half-Life, Rats

Abstract

Recently, our research group reported the identification of BMS-986104 (2) as a differentiated S1P

Published

2019

25. Discovery of a JAK1/3 Inhibitor and Use of a Prodrug To Demonstrate Efficacy in a Model of Rheumatoid Arthritis

Author

Sidney Pitt, John S. Sack, Vicky Tang, William J. Pitts, Steven H. Spergel, Jonathan Lippy, Junqing Guo, Michael Galella, Mertzman Michael E, Sylwia Stachura, Steven G. Nadler, Aberra Fura, Percy H. Carter, Gary L. Schieven, Luisa Salter-Cid, Kim W. McIntyre, James Kempson, Javed Khan, Lauren Haque, Rosemary Zhang, John S. Tokarski, Guoxiang Shen, Kathleen M. Gillooly, Stephen T. Wrobleski, and Joel C. Barrish

Subjects

Tofacitinib, Kinase, business.industry, Organic Chemistry, Prodrug, Pharmacology, medicine.disease, Biochemistry, Immune system, Tyrosine kinase 2, Rheumatoid arthritis, Drug Discovery, Functional selectivity, Medicine, business, Tyrosine kinase

Abstract

[Image: see text] The four members of the Janus family of nonreceptor tyrosine kinases play a significant role in immune function. The JAK family kinase inhibitor, tofacitinib 1, has been approved in the United States for use in rheumatoid arthritis (RA) patients. A number of JAK inhibitors with a variety of JAK family selectivity profiles are currently in clinical trials. Our goal was to identify inhibitors that were functionally selective for JAK1 and JAK3. Compound 22 was prepared with the desired functional selectivity profile, but it suffered from poor absorption related to physical properties. Use of the phosphate prodrug 32 enabled progression to a murine collagen induced arthritis (CIA) model. The demonstration of a robust efficacy in the CIA model suggests that use of phosphate prodrugs may resolve issues with progressing this chemotype for the treatment of autoimmune diseases such as RA.

Published

2019

26. Regioselective Epoxide Ring Opening for the Stereospecific Scale-Up Synthesis of BMS-960, A Potent and Selective Isoxazole-Containing S1P1 Receptor Agonist

Author

Alaric J. Dyckman, Bang-Chi Chen, Percy H. Carter, Zhiwei Guo, Amarjit Singh, John L. Gilmore, James E. Sheppeck, Animesh Goswami, Huiping Zhang, Xiaoping Hou, and Arvind Mathur

Subjects

Agonist, Trifluoromethyl, 010405 organic chemistry, medicine.drug_class, Stereochemistry, Organic Chemistry, Epoxide, Regioselectivity, Alcohol, 010402 general chemistry, 01 natural sciences, 0104 chemical sciences, Benzonitrile, chemistry.chemical_compound, Stereospecificity, chemistry, medicine, Physical and Theoretical Chemistry, Isoxazole

Abstract

This article presents a stereospecific scale-up synthesis of (S)-1-((S)-2-hydroxy-2-(4-(5-(3-phenyl-4-(trifluoromethyl)isoxazol-5-yl)-1,2,4-oxadiazol-3-yl)phenyl)ethyl)piperidine-3-carboxylic acid (BMS-960), a potent and selective isoxazole-containing S1P1 receptor agonist. The process highlights an enzymatic reduction of α-bromoketone toward the preparation of (S)-bromo alcohol, a key precursor of (S)-4-(oxiran-2-yl)benzonitrile. A regioselective and stereospecific epoxide ring-opening reaction was also optimized along with improvements to 1,2,4-oxadiazole formation, hydrolysis, and crystallization. The improved process was utilized to synthesize batches of BMS-960 for Ames testing and other toxicological studies.

Published

2017

27. Identification of imidazo[1,2-b]pyridazine TYK2 pseudokinase ligands as potent and selective allosteric inhibitors of TYK2 signalling

Author

Dianlin Xie, Jing Chen, Celia D’Arienzo, Jodi K. Muckelbauer, Nelly Aranibar, John S. Sack, Jeffrey Tredup, Christine Huang, Charu Chaudhry, Joann Strnad, Percy H. Carter, John S. Tokarski, Adriana Zupa-Fernandez, Joseph B. Santella, Yuval Blat, Gardner Daniel S, James R. Burke, James Lin, David S. Weinstein, Moslin Ryan M, Yifan Zhang, Lihong Cheng, Chong-Hwan Chang, Donna L. Pedicord, Chunjian Liu, J. V. Duncia, and Huadong Sun

Subjects

0301 basic medicine, Pharmacology, chemistry.chemical_classification, Stereochemistry, Organic Chemistry, Allosteric regulation, Pharmaceutical Science, Biochemistry, Pyridazine, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, Signalling, Enzyme, chemistry, Tyrosine kinase 2, Drug Discovery, Molecular Medicine, Transferase, Selectivity, Tyrosine kinase

Abstract

As a member of the Janus (JAK) family of non-receptor tyrosine kinases, TYK2 mediates the signaling of pro-inflammatory cytokines including IL-12, IL-23 and type 1 interferon (IFN), and therefore represents an attractive potential target for treating the various immuno-inflammatory diseases in which these cytokines have been shown to play a role. Following up on our previous report that ligands to the pseudokinase domain (JH2) of TYK2 suppress cytokine-mediated receptor activation of the catalytic (JH1) domain, the imidazo[1,2-b]pyridazine (IZP) 7 was identified as a promising hit compound. Through iterative modification of each of the substituents of the IZP scaffold, the cellular potency was improved while maintaining selectivity over the JH1 domain. These studies led to the discovery of the JH2-selective TYK2 inhibitor 29, which provided encouraging systemic exposures after oral dosing in mice. Phosphodiesterase 4 (PDE4) was identified as an off-target and potential liability of the IZP ligands, and selectivity for TYK2 JH2 over this enzyme was obtained by elaborating along selectivity vectors determined from analyses of X-ray co-crystal structures of representative ligands of the IZP class bound to both proteins.

Published

2017

28. Identification of potent tricyclic prodrug S1P1 receptor modulators

Author

Marta Dabros, Paul Levesque, Elizabeth M. Heimrich, Arvind Mathur, Percy H. Carter, Richard Rampulla, Anuradha Gupta, Lois D. Lehman-McKeeman, Huadong Sun, David Marcoux, Ding Ren Shen, Xiaoxia Yang, Xia D. Zhou, Hai-Yun Xiao, Dauh-Rurng Wu, Louis J. Lombardo, Hong Shi, Zheng Yang, Mary Ellen Cvijic, Alaric J. Dyckman, Kim W. McIntyre, Luisa Salter-Cid, Celia D’Arienzo, Anthony M. Marino, Bala Pragalathan, Georgia Cornelius, Jenny Xie, T. G. Murali Dhar, Tracy L. Taylor, and Rochelle Thomas

Subjects

0301 basic medicine, Drug, Agonist, medicine.drug_class, Metabolite, media_common.quotation_subject, Pharmaceutical Science, Pharmacology, Biochemistry, Partial agonist, 03 medical and health sciences, chemistry.chemical_compound, Drug Discovery, medicine, media_common, chemistry.chemical_classification, S1p1 receptor, Organic Chemistry, Prodrug, Fingolimod, 030104 developmental biology, chemistry, Molecular Medicine, medicine.drug, Tricyclic

Abstract

Recently, our research group reported the identification of prodrug amino-alcohol 2 as a potent and efficacious S1P1 receptor modulator. This molecule is differentiated preclinically over the marketed drug fingolimod (Gilenya 1), whose active phosphate metabolite is an S1P1 full agonist, in terms of pulmonary and cardiovascular safety. S1P1 partial agonist 2, however, has a long half-life in rodents and was projected to have a long half-life in humans. The purpose of this communication is to disclose highly potent partial agonists of S1P1 with shorter half-lives relative to the clinical compound 2. PK/PD relationships as well as their preclinical pulmonary and cardiovascular safety assessment are discussed.

Published

2017

29. Asymmetric Hydroboration Approach to the Scalable Synthesis of ((1R,3S)-1-Amino-3-((R)-6-hexyl-5,6,7,8-tetrahydronaphthalen-2-yl)cyclopentyl)methanol (BMS-986104) as a Potent S1P1 Receptor Modulator

Author

Ding Ren Shen, Mary Ellen Cvijic, Hai-Yun Xiao, Alaric J. Dyckman, Yu-Wen Li, Bala Pragalathan, Joel C. Barrish, Georgia Cornelius, Peng Li, Tracy L. Taylor, Zili Xiao, Lois D. Lehman-McKeeman, Jianlin Feng, Dauh-Rurng Wu, John L. Gilmore, Percy H. Carter, David Marcoux, Zheng Yang, Arvind Mathur, Elizabeth M. Heimrich, Kim W. McIntyre, Bethanne M. Warrack, Anuradha Gupta, Yang Michael G, Luisa Salter-Cid, Praveen Balimane, Virna Borowski, Jenny Xie, T. G. Murali Dhar, Alda Fernandes, and Anthony M. Marino

Subjects

0301 basic medicine, chemistry.chemical_classification, Alkene, S1p1 receptor, Stereochemistry, Combinatorial chemistry, Brain Cell, 03 medical and health sciences, chemistry.chemical_compound, Hydroboration, 030104 developmental biology, 0302 clinical medicine, Lysophosphatidylcholine, chemistry, Drug Discovery, Molecular Medicine, Methanol, 030217 neurology & neurosurgery

Abstract

We describe a highly efficient route for the synthesis of 4a (BMS-986104). A key step in the synthesis is the asymmetric hydroboration of trisubstituted alkene 6. Particularly given the known difficulties involved in this type of transformation (6 → 7), the current methodology provides an efficient approach to prepare this class of compounds. In addition, we disclose the efficacy of 4a in a mouse EAE model, which is comparable to 4c (FTY720). Mechanistically, 4a exhibited excellent remyelinating effects on lysophosphatidylcholine (LPC) induced demyelination in a three-dimensional brain cell culture assay.

Published

2016

30. Discovery of 6-Fluoro-5-(R)-(3-(S)-(8-fluoro-1-methyl-2,4-dioxo-1,2-dihydroquinazolin-3(4H)-yl)-2-methylphenyl)-2-(S)-(2-hydroxypropan-2-yl)-2,3,4,9-tetrahydro-1H-carbazole-8-carboxamide (BMS-986142): A Reversible Inhibitor of Bruton’s Tyrosine Kinase (BTK) Conformationally Constrained by Two Locked Atropisomers

Author

Jun Dai, Arvind Mathur, Lihong Cheng, Kim W. McIntyre, Dawn Sun, Joseph A. Tino, Shiuhang Yip, Douglas G. Batt, Jodi K. Muckelbauer, James R. Burke, Joel C. Barrish, Rodney Vickery, Celia D’Arienzo, Luisa Salter-Cid, Qingjie Liu, Tracy L. Taylor, Hua Gong, Mark A. Pattoli, Elizabeth M. Heimrich, Yingru Zhang, Andy J. Tebben, Myra Beaudoin Bertrand, Kathleen M. Gillooly, Chiehying Chang, Percy H. Carter, Scott H. Watterson, Mary T. Obermeier, Claudine Pulicicchio, Aberra Fura, Chunlei Wang, Michael Galella, Charles M. Langevine, Sarah C. Traeger, Lorell Discenza, Peng Li, Yifan Zhang, Qing Shi, Stacey Skala, Dauh-Rurng Wu, Richard Rampulla, and George V. De Lucca

Subjects

0301 basic medicine, Atropisomer, biology, 010405 organic chemistry, medicine.drug_class, Kinase, Chemistry, Stereochemistry, B-cell receptor, Carboxamide, 01 natural sciences, 0104 chemical sciences, 03 medical and health sciences, 030104 developmental biology, immune system diseases, hemic and lymphatic diseases, Drug Discovery, medicine, biology.protein, Molecular Medicine, Structure–activity relationship, Bruton's tyrosine kinase, Transferase, Tyrosine kinase

Abstract

Bruton's tyrosine kinase (BTK), a nonreceptor tyrosine kinase, is a member of the Tec family of kinases. BTK plays an essential role in B cell receptor (BCR)-mediated signaling as well as Fcγ receptor signaling in monocytes and Fce receptor signaling in mast cells and basophils, all of which have been implicated in the pathophysiology of autoimmune disease. As a result, inhibition of BTK is anticipated to provide an effective strategy for the clinical treatment of autoimmune diseases such as lupus and rheumatoid arthritis. This article details the structure–activity relationships (SAR) leading to a novel series of highly potent and selective carbazole and tetrahydrocarbazole based, reversible inhibitors of BTK. Of particular interest is that two atropisomeric centers were rotationally locked to provide a single, stable atropisomer, resulting in enhanced potency and selectivity as well as a reduction in safety liabilities. With significantly enhanced potency and selectivity, excellent in vivo properties an...

Published

2016

31. Discovery and SAR of pyrrolo[2,1-f][1,2,4]triazin-4-amines as potent and selective PI3Kδ inhibitors

Author

Carolyn A. Weigelt, Xiaomei Gu, Lan-Ying Qin, Christine B. Goldstine, Sylwia Stachura, Jenny Xie, Zheming Ruan, T. G. Murali Dhar, Donna L. Pedicord, Michael A. Poss, Luisa Salter-Cid, Rajeev S. Bhide, Percy H. Carter, James Neels, John S. Sack, Stefan Ruepp, Kevin Stefanski, Paul Davies, and Stacey Skala

Subjects

0301 basic medicine, Gene isoform, Clinical Biochemistry, Drug Evaluation, Preclinical, Pharmaceutical Science, chemical and pharmacologic phenomena, Phosphatidylinositol 3-Kinases, Biochemistry, PI3K signaling, Inhibitory Concentration 50, Mice, Structure-Activity Relationship, 03 medical and health sciences, 0302 clinical medicine, Drug Discovery, Animals, Protein Isoforms, Structure–activity relationship, Amines, Protein Kinase Inhibitors, Molecular Biology, Phosphoinositide-3 Kinase Inhibitors, Binding Sites, biology, Triazines, Chemistry, Arthritis, Organic Chemistry, Protein Structure, Tertiary, Molecular Docking Simulation, Disease Models, Animal, 030104 developmental biology, 030220 oncology & carcinogenesis, biology.protein, Molecular Medicine, Keyhole limpet hemocyanin, Protein Binding, Collagen-induced arthritis

Abstract

Aberrant Class I PI3K signaling is a key factor contributing to many immunological disorders and cancers. We have identified 4-amino pyrrolotriazine as a novel chemotype that selectively inhibits PI3Kδ signaling despite not binding to the specificity pocket of PI3Kδ isoform. Structure activity relationship (SAR) led to the identification of compound 30 that demonstrated efficacy in mouse Keyhole Limpet Hemocyanin (KLH) and collagen induced arthritis (CIA) models.

Published

2016

32. Discovery and Structure–Activity Relationship (SAR) of a Series of Ethanolamine-Based Direct-Acting Agonists of Sphingosine-1-phosphate (S1P1)

Author

John L. Gilmore, Georgia Cornelius, Mary Ellen Cvijic, Jenny Xie, Lauren Haque, Andrew J. Tebben, Luisa Salter-Cid, Alaric J. Dyckman, Praveen Balimane, Paul Levesque, Anthony M. Marino, Percy H. Carter, Julia P. Li, Michael Galella, Kathleen M. Gillooly, Kim W. McIntyre, Virna Borowski, Joel C. Barrish, Bethanne M. Warrack, Celia D’Arienzo, William J. Pitts, Parag Mukhopadhyay, Scott H. Watterson, Ding Ren Shen, Melissa Yarde, James E. Sheppeck, and Tracy L. Taylor

Subjects

Male, 0301 basic medicine, Encephalomyelitis, Autoimmune, Experimental, Lymphocyte, Metabolite, Carboxylic acid, Inflammation, Pharmacology, 01 natural sciences, Mice, Structure-Activity Relationship, 03 medical and health sciences, chemistry.chemical_compound, Dogs, Ethanolamine, Drug Discovery, medicine, Animals, Humans, Structure–activity relationship, Lymphocyte Count, Lymphocytes, Sphingosine-1-phosphate, chemistry.chemical_classification, 010405 organic chemistry, Chemistry, Arthritis, Haplorhini, Sphingolipid, Rats, 0104 chemical sciences, Mice, Inbred C57BL, Receptors, Lysosphingolipid, 030104 developmental biology, medicine.anatomical_structure, Rats, Inbred Lew, Molecular Medicine, Female, medicine.symptom

Abstract

Sphingosine-1-phosphate (S1P) is a bioactive sphingolipid metabolite that regulates a multitude of physiological processes such as lymphocyte trafficking, cardiac function, vascular development, and inflammation. Because of the ability of S1P1 receptor agonists to suppress lymphocyte egress, they have great potential as therapeutic agents in a variety of autoimmune diseases. In this article, the discovery of selective, direct acting S1P1 agonists utilizing an ethanolamine scaffold containing a terminal carboxylic acid is described. Potent S1P1 agonists such as compounds 18a and 19a which have greater than 1000-fold selectivity over S1P3 are described. These compounds efficiently reduce blood lymphocyte counts in rats through 24 h after single doses of 1 and 0.3 mpk, respectively. Pharmacodynamic properties of both compounds are discussed. Compound 19a was further studied in two preclinical models of disease, exhibiting good efficacy in both the rat adjuvant arthritis model (AA) and the mouse experimental autoimmune encephalomyelitis model (EAE).

Published

2016

33. An Efficient Scale-Up Synthesis of BMS-520, a Potent and Selective Isoxazole-Containing S1P1 Receptor Agonist

Author

Bang-Chi Chen, Percy H. Carter, Alaric J. Dyckman, William J. Pitts, Juliang Zhu, Huiping Zhang, Arvind Mathur, Scott H. Watterson, and Xiaoping Hou

Subjects

Agonist, Trifluoromethyl, 010405 organic chemistry, S1p1 receptor, medicine.drug_class, Stereochemistry, Organic Chemistry, Regioselectivity, 010402 general chemistry, 01 natural sciences, Cycloaddition, 0104 chemical sciences, Hydrolysis, chemistry.chemical_compound, chemistry, Structural isomer, medicine, Physical and Theoretical Chemistry, Isoxazole

Abstract

This article reports an efficient scale-up synthesis of 1-(4-(5-(3-phenyl-4-(trifluoromethyl)isoxazol-5-yl)-1,2,4-oxadiazol-3-yl)benzyl)azetidine-3-carboxylic acid (BMS-520), a potent and selective isoxazole-containing S1P1 receptor agonist. This process features a highly regioselective cycloaddition leading to a key intermediate, ethyl 3-phenyl-4-(trifluoromethyl)isoxazole-5-carboxylate, a chemo-selective hydrolysis of its regioisomers, as well as an improved method for 1,2,4-oxadiazole formation, relative to the original synthesis. The improved process was applied to the preparation of multiple batches of BMS-520 for preclinical toxicological studies.

Published

2016

34. Discovery of (3S,4S)-3-methyl-3-(4-fluorophenyl)-4-(4-(1,1,1,3,3,3-hexafluoro-2-hydroxyprop-2-yl)phenyl)pyrrolidines as novel RORγt inverse agonists

Author

Javed Khan, Dhanya Kumar Raut, Sylwia Stachura, Qihong Zhao, Jingwu Duan, Melissa Yarde, Bin Jiang, Hemalatha Hemagiri, Arvind Mathur, Ananta Karmakar, Michael Galella, T. G. Murali Dhar, John S. Sack, Percy H. Carter, Luisa Salter-Cid, Arun Kumar Gupta, Carolyn A. Weigelt, Dauh-Rurng Wu, and Ding-Ren Shen

Subjects

Pyrrolidines, Drug Inverse Agonism, Stereochemistry, medicine.drug_class, Clinical Biochemistry, Pharmaceutical Science, Carboxamide, Molecular Dynamics Simulation, Crystallography, X-Ray, 01 natural sciences, Biochemistry, Pyrrolidine, Mice, Structure-Activity Relationship, chemistry.chemical_compound, RAR-related orphan receptor gamma, Drug Discovery, medicine, Animals, Humans, Inverse agonist, Molecular Biology, chemistry.chemical_classification, Pregnane X receptor, Binding Sites, Bicyclic molecule, 010405 organic chemistry, Organic Chemistry, Pregnane X Receptor, Nuclear Receptor Subfamily 1, Group F, Member 3, 0104 chemical sciences, Sulfonamide, 010404 medicinal & biomolecular chemistry, Binding conformation, chemistry, Drug Design, Microsomes, Liver, Molecular Medicine

Abstract

A novel series of cis-3,4-diphenylpyrrolidines were designed as RORγt inverse agonists based on the binding conformation of previously reported bicyclic sulfonamide 1. Preliminary synthesis and structure–activity relationship (SAR) study established (3S,4S)-3-methyl-3-(4-fluorophenyl)-4-(4-(1,1,1,3,3,3-hexafluoro-2-hydroxyprop-2-yl)phenyl)pyrrolidine as the most effective scaffold. Subsequent SAR optimization led to identification of a piperidinyl carboxamide 31, which was potent against RORγt (EC50 of 61 nM in an inverse agonist assay), selective relative to RORα, RORβ, LXRα and LXRβ, and stable in human and mouse liver microsomes. Furthermore, compound 31 exhibited considerably lower PXR Ymax (46%) and emerged as a promising lead. The binding mode of the diphenylpyrrolidine series was established with an X-ray co-crystal structure of 10A/RORγt.

Published

2020

35. Identification of Imidazo[1,2

Author

Chunjian, Liu, James, Lin, Ryan, Moslin, John S, Tokarski, Jodi, Muckelbauer, ChiehYing, Chang, Jeffrey, Tredup, Dianlin, Xie, Hyunsoo, Park, Peng, Li, Dauh-Rurng, Wu, Joann, Strnad, Adriana, Zupa-Fernandez, Lihong, Cheng, Charu, Chaudhry, Jing, Chen, Cliff, Chen, Huadong, Sun, Paul, Elzinga, Celia, D'arienzo, Kathleen, Gillooly, Tracy L, Taylor, Kim W, McIntyre, Luisa, Salter-Cid, Louis J, Lombardo, Percy H, Carter, Nelly, Aranibar, James R, Burke, and David S, Weinstein

Abstract

[Image: see text] In sharp contrast to a previously reported series of 6-anilino imidazopyridazine based Tyk2 JH2 ligands, 6-((2-oxo-N1-substituted-1,2-dihydropyridin-3-yl)amino)imidazo[1,2-b]pyridazine analogs were found to display dramatically improved metabolic stability. The N1-substituent on 2-oxo-1,2-dihydropyridine ring can be a variety of alkyl, aryl, and heteroaryl groups, but among them, 2-pyridyl provided much enhanced Caco-2 permeability, attributed to its ability to form intramolecular hydrogen bonds. Further structure–activity relationship studies at the C3 position led to the identification of highly potent and selective Tyk2 JH2 inhibitor 6, which proved to be highly effective in inhibiting IFNγ production in a rat pharmacodynamics model and fully efficacious in a rat adjuvant arthritis model.

Published

2019

36. Conversion of carbazole carboxamide based reversible inhibitors of Bruton's tyrosine kinase (BTK) into potent, selective irreversible inhibitors in the carbazole, tetrahydrocarbazole, and a new 2,3-dimethylindole series

Author

Jonathan Lippy, Joseph A. Tino, Qingjie Liu, Mark A. Pattoli, Songmei Xu, James R. Burke, Charu Chaudhry, Percy H. Carter, Douglas G. Batt, and Neha Surti

Subjects

Models, Molecular, Indoles, medicine.drug_class, Clinical Biochemistry, Carbazoles, Pharmaceutical Science, Carboxamide, Crystallography, X-Ray, 01 natural sciences, Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, Structure-Activity Relationship, 0302 clinical medicine, Drug Discovery, medicine, Agammaglobulinaemia Tyrosine Kinase, Bruton's tyrosine kinase, Humans, Molecular Biology, Protein Kinase Inhibitors, biology, Dose-Response Relationship, Drug, Molecular Structure, 010405 organic chemistry, Carbazole, Btk inhibitors, Organic Chemistry, Combinatorial chemistry, 0104 chemical sciences, chemistry, 030220 oncology & carcinogenesis, Lipophilicity, Electrophile, biology.protein, Molecular Medicine, Selectivity

Abstract

Incorporation of a suitably-placed electrophilic group transformed a series of reversible BTK inhibitors based on carbazole-1-carboxamide and tetrahydrocarbazole-1-carboxamide into potent, irreversible inhibitors. Removal of one ring from the core of these compounds provided a potent irreversible series of 2,3-dimethylindole-7-carboxamides having excellent potency and improved selectivity, with the additional advantages of reduced lipophilicity and molecular weight.

Published

2018

37. Leveraging a 'Catch-Release' Logic Gate Process for the Synthesis and Nonchromatographic Purification of Thioether- or Amine-Bridged Macrocyclic Peptides

Author

Mahboubeh Kheirabadi, Martin D. Eastgate, Kenneth M. Boy, David K. Leahy, Percy H. Carter, Gardner S. Creech, Jennifer X. Qiao, and David S. Nirschl

Subjects

chemistry.chemical_classification, 010405 organic chemistry, Organic Chemistry, Leaving group, 010402 general chemistry, 01 natural sciences, Combinatorial chemistry, 0104 chemical sciences, Amino acid, chemistry.chemical_compound, chemistry, Thioether, Nucleophile, Logic gate, Peptide synthesis, Side chain, Amine gas treating

Abstract

Macrocyclic peptides containing N-alkylated amino acids have emerged as a promising therapeutic modality, capable of modulating protein-protein interactions and an intracellular delivery of hydrophilic payloads. While multichannel automated solid-phase peptide synthesis (SPPS) is a practical approach for peptide synthesis, the requirement for slow and inefficient chromatographic purification of the product peptides is a significant limitation to exploring these novel compounds. Herein, we invent a "catch-release" strategy for the nonchromatographic purification of macrocyclic peptides. A traceless catch process is enabled by the invention of a dual-functionalized N-terminal acetate analogue, which serves as a handle for capture onto a purification resin and as a leaving group for macrocyclization. Displacement by a C-terminal nucleophilic side chain thus releases the desired macrocycle from the purification resin. By design, this catch/release process is a logic test for the presence of the key components required for cyclization, thus removing impurities which lack the required functionality, such as common classes of peptide impurities, including hydrolysis fragments and truncated sequences. The method was shown to be highly effective with three libraries of macrocyclic peptides, containing macrocycles of 5-20 amino acids, with either thioether- or amine-based macrocyclic linkages; in this latter class, the reported method represents an enabling technology. In all cases, the catch-release protocol afforded significant enrichment of the target peptides purity, in many cases completely obviating the need for chromatography. Importantly, we have adapted this process for automation on a standard multichannel peptide synthesizer, achieving an efficient and completely integrated synthesis and purification platform for the preparation of these important molecules.

Published

2018

38. Identification and Preclinical Pharmacology of BMS-986104: A Differentiated S1P1 Receptor Modulator in Clinical Trials

Author

Kim W. McIntyre, Luisa Salter-Cid, Bethanne M. Warrack, Celia D’Arienzo, Lois D. Lehman-McKeeman, Rochelle Thomas, Praveen Balimane, Anthony M. Marino, Joel C. Barrish, Elizabeth M. Heimrich, Ding Ren Shen, Xiaoxia Yang, Xia D. Zhou, Jenny Xie, Hong Shi, T. G. Murali Dhar, James Hennan, Jia L. Zhu, Dauh-Rurng Wu, Marta Dabros, Paul Levesque, Percy H. Carter, Arvind Mathur, Mary Ellen Cvijic, Alaric J. Dyckman, Georgia Cornelius, Zheng Yang, Hai-Yun Xiao, and Tracy L. Taylor

Subjects

0301 basic medicine, Bradycardia, business.industry, S1p1 receptor, Sphingosine-1-phosphate receptor, Multiple sclerosis, Organic Chemistry, Pharmacology, medicine.disease, Biochemistry, Fingolimod, Clinical trial, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Drug Discovery, Heart rate, medicine, medicine.symptom, Colitis, business, 030217 neurology & neurosurgery, medicine.drug

Abstract

Clinical validation of S1P receptor modulation therapy was achieved with the approval of fingolimod (Gilenya, 1) as the first oral therapy for relapsing remitting multiple sclerosis. However, 1 causes a dose-dependent reduction in the heart rate (bradycardia), which occurs within hours after first dose. We disclose the identification of clinical compound BMS-986104 (3d), a novel S1P1 receptor modulator, which demonstrates ligand-biased signaling and differentiates from 1 in terms of cardiovascular and pulmonary safety based on preclinical pharmacology while showing equivalent efficacy in a T-cell transfer colitis model.

Published

2016

39. Discovery and synthesis of cyclohexenyl derivatives as modulators of CC chemokine receptor 2 activity

Author

Mary-Ellen Cvijic, Percy H. Carter, Douglas G. Batt, Qing Shi, George V. Delucca, Rui-Qin Liu, Qihong Zhao, Gregory D. Brown, Feng Qiu, Joel C. Barrish, and Michael Galella

Subjects

Models, Molecular, 0301 basic medicine, CCR2, Receptors, CCR2, Stereochemistry, animal diseases, Clinical Biochemistry, Cyclohexene, Pharmaceutical Science, Ring (chemistry), 01 natural sciences, Biochemistry, Structure-Activity Relationship, 03 medical and health sciences, chemistry.chemical_compound, Cyclohexenes, parasitic diseases, Drug Discovery, Humans, Structure–activity relationship, Molecular Biology, IC50, G protein-coupled receptor, Drug discovery, Chemistry, Organic Chemistry, hemic and immune systems, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, 030104 developmental biology, Molecular Medicine, CC chemokine receptors

Abstract

A novel cyclohexenyl series of CCR2 antagonists has been discovered. This series of small, rigid compounds exhibits submicromolar binding affinity for CCR2. Modification of the substituents on the cyclohexene ring led to the identification of potent CCR2 antagonists. Progress from initial lead 5 (IC50=700nM) to (-)-38 (IC50=9.0nM) is discussed.

Published

2016

40. Design and synthesis of carbazole carboxamides as promising inhibitors of Bruton’s tyrosine kinase (BTK) and Janus kinase 2 (JAK2)

Author

Matt Pokross, Jonathan Lippy, Qingjie Liu, Yongmi An, Chiehying Chang, Joseph A. Tino, James R. Burke, Andrew J. Tebben, Zheng Yang, Lin Chen, Douglas G. Batt, Jodi K. Muckelbauer, Percy H. Carter, Neha Surti, and Haiqing Wang

Subjects

Clinical Biochemistry, Carbazoles, Pharmaceutical Science, Biochemistry, Structure-Activity Relationship, chemistry.chemical_compound, Drug Discovery, Protein-Tyrosine Kinases, Humans, Structure–activity relationship, Bruton's tyrosine kinase, Protein Kinase Inhibitors, Molecular Biology, Janus kinase 2, Dose-Response Relationship, Drug, Molecular Structure, biology, Carbazole, Organic Chemistry, Janus Kinase 2, Amides, chemistry, Drug Design, biology.protein, Molecular Medicine, Tyrosine kinase

Abstract

Four series of disubstituted carbazole-1-carboxamides were designed and synthesised as inhibitors of Bruton's tyrosine kinase (BTK). 4,7- and 4,6-disubstituted carbazole-1-carboxamides were potent and selective inhibitors of BTK, while 3,7- and 3,6-disubstituted carbazole-1-carboxamides were potent and selective inhibitors of Janus kinase 2 (JAK2).

Published

2015

41. The Discovery of Macrocyclic XIAP Antagonists from a DNA-Programmed Chemistry Library, and Their Optimization To Give Lead Compounds with in Vivo Antitumor Activity

Author

Yong Zhang, Ming Lei, Shana L. Posy, Kyoung S. Kim, Benjamin A. Seigal, Joseph Fargnoli, Stuart Emanuel, Percy H. Carter, Nicholas K. Terrett, Neha Surti, Robert M. Borzilleri, Henry Shen, Joseph G. Naglich, Matthew Pokross, Randy Talbott, Andrew Fraley, and William H. Connors

Subjects

Models, Molecular, Macrocyclic Compounds, Stereochemistry, Antineoplastic Agents, Breast Neoplasms, X-Linked Inhibitor of Apoptosis Protein, Crystallography, X-Ray, Cocrystal, Mice, In vivo, Cell Line, Tumor, Drug Discovery, Animals, Humans, Genomic library, Breast, Caspase, Gene Library, biology, Caspase 3, Chemistry, Drug discovery, Combinatorial chemistry, XIAP, Cell culture, Apoptosis, biology.protein, Molecular Medicine, Female

Abstract

Affinity selection screening of macrocycle libraries derived from DNA-programmed chemistry identified XIAP BIR2 and BIR3 domain inhibitors that displace bound pro-apoptotic caspases. X-ray cocrystal structures of key compounds with XIAP BIR2 suggested potency-enhancing structural modifications. Optimization of dimeric macrocycles with similar affinity for both domains were potent pro-apoptotic agents in cancer cell lines and efficacious in shrinking tumors in a mouse xenograft model.

Published

2015

42. Discovery of a Potent and Orally Bioavailable Dual Antagonist of CC Chemokine Receptors 2 and 5

Author

Jian Pang, Ruowei Mo, Joseph B. Santella, Mary Ellen Cvijic, Gregory D. Brown, Anne Rose, John V. Duncia, Jing Chen, Douglas G. Batt, Songmei Xu, Sarah C. Traeger, Sandhya Mandlekar, Soo S. Ko, David J. Nelson, Percy H. Carter, Andrew J. Tebben, Qihong Zhao, Joel C. Barrish, Robert J. Cherney, and Cheryl M. Clark

Subjects

CCR2, Chemokine, biology, Chemistry, Organic Chemistry, Antagonist, Pharmacology, Biochemistry, Bioavailability, chemistry.chemical_compound, Drug Discovery, Quinazoline, biology.protein, Benzamide, CC chemokine receptors, G protein-coupled receptor

Abstract

We describe the hybridization of our previously reported acyclic and cyclic CC chemokine receptor 2 (CCR2) antagonists to lead to a new series of dual antagonists of CCR2 and CCR5. Installation of a γ-lactam as the spacer group and a quinazoline as a benzamide mimetic improved oral bioavailability markedly. These efforts led to the identification of 13d, a potent and orally bioavailable dual antagonist suitable for use in both murine and monkey models of inflammation.

Published

2015

43. Identification of a Potent, Selective, and Efficacious Phosphatidylinositol 3-Kinase δ (PI3Kδ) Inhibitor for the Treatment of Immunological Disorders

Author

Dezhi Xing, Carolyn A. Weigelt, Luisa Salter-Cid, Pirama Nayagam Arunachalam, Rodney B.W. Smith, Ling Li, Melissa Yarde, Jodi K. Muckelbauer, Jonathan Lippy, Mary Ellen Cvijic, Sidney Pitt, John S. Sack, Thatipamula Rp, Michael A. Poss, Paul Levesque, Robert J. Cherney, Ipsit Kundu, David Marcoux, Gary L. Schieven, Arvind Mathur, Qingjie Liu, Zheming Ruan, Rosemary Zhang, R M Fancher, Shweta Padmanabhan, Scott H. Watterson, Qing Shi, Mary T. Obermeier, Anurag S. Srivastava, Anuradha Gupta, Douglas G. Batt, James Neels, Joseph A. Tino, Kevin Stefanski, Percy H. Carter, Macor John E, John Hynes, Myra Beaudoin-Bertrand, Hao Lu, Kim W. McIntyre, Stacey Skala, Aberra Fura, Lan-Ying Qin, Cornelius Lyndon A M, James Hennan, Richard Rampulla, Bogdan Sleczka, Jenny Xie, Kallem Rajareddy, Jie Pan, Christine B. Goldstine, Hua Gong, Qian Ruan, Kathleen M. Gillooly, Donna L. Pedicord, Jingsong Fan, Rajeev S. Bhide, and Stefan Ruepp

Subjects

0301 basic medicine, Antigens, Differentiation, T-Lymphocyte, Male, ERG1 Potassium Channel, hERG, Drug Evaluation, Preclinical, Phosphatidylinositol 3-Kinases, Pharmacology, Pyrazole, 03 medical and health sciences, chemistry.chemical_compound, Structure-Activity Relationship, Dogs, Antigens, CD, Drug Discovery, Structure–activity relationship, Potency, Animals, Humans, Lectins, C-Type, Phosphatidylinositol, Enzyme Inhibitors, Phosphoinositide-3 Kinase Inhibitors, Mice, Inbred BALB C, biology, Kinase, Arthritis, Experimental, Isoenzymes, 030104 developmental biology, chemistry, Immune System Diseases, biology.protein, Molecular Medicine, Pyrazoles, Female, Efflux, Rabbits, Caco-2 Cells

Abstract

PI3Kδ plays an important role controlling immune cell function and has therefore been identified as a potential target for the treatment of immunological disorders. This article highlights our work toward the identification of a potent, selective, and efficacious PI3Kδ inhibitor. Through careful SAR, the successful replacement of a polar pyrazole group by a simple chloro or trifluoromethyl group led to improved Caco-2 permeability, reduced Caco-2 efflux, reduced hERG PC activity, and increased selectivity profile while maintaining potency in the CD69 hWB assay. The optimization of the aryl substitution then identified a 4′-CN group that improved the human/rodent correlation in microsomal metabolic stability. Our lead molecule is very potent in PK/PD assays and highly efficacious in a mouse collagen-induced arthritis model.

Published

2017

44. Discovery of highly potent, selective, covalent inhibitors of JAK3

Author

Jingwu Duan, Stephen T. Wrobleski, Joel C. Barrish, Jagabandhu Das, Gary L. Schieven, Steven H. Spergel, Charu Chaudhry, Percy H. Carter, John S. Tokarski, Damaso Ovalle, John S. Sack, Aberra Fura, Zhonghui Lu, James Kempson, Luisa Salter-Cid, William J. Pitts, Junqing Guo, Yuval Blatt, John Hynes, Shuqun Lin, Hong Wu, Bin Jiang, Bingwei V. Yang, and Javed Khan

Subjects

0301 basic medicine, Stereochemistry, Cell Survival, Clinical Biochemistry, Drug Evaluation, Preclinical, Pharmaceutical Science, Crystal structure, Biochemistry, Active site cysteine, Cell Line, 03 medical and health sciences, Residue (chemistry), Inhibitory Concentration 50, Structure-Activity Relationship, Catalytic Domain, Drug Discovery, Molecule, Humans, Molecular Biology, Protein Kinase Inhibitors, Binding Sites, Chemistry, Organic Chemistry, Janus Kinase 3, Janus Kinase 1, Janus Kinase 2, Combinatorial chemistry, Molecular Docking Simulation, 030104 developmental biology, Covalent bond, Electrophile, Molecular Medicine

Abstract

A useful and novel set of tool molecules have been identified which bind irreversibly to the JAK3 active site cysteine residue. The design was based on crystal structure information and a comparative study of several electrophilic warheads.

Published

2017

45. Discovery of potent and efficacious pyrrolopyridazines as dual JAK1/3 inhibitors

Author

Sidney Pitt, Sylwia Stachura, Rosemary Zhang, Steven G. Nadler, Kim W. McIntyre, Hong Wu, James Kempson, Jonathan Lippy, John Hynes, Joel C. Barrish, Zhonghui Lu, Percy H. Carter, Gary L. Schieven, Bin Jiang, Kate Gillooly, William J. Pitts, Javed Khan, Stephen T. Wrobleski, Jingwu Duan, Aberra Fura, Guoxiang Shen, John S. Tokarski, John S. Sack, and Luisa Salter-Cid

Subjects

0301 basic medicine, Clinical Biochemistry, Drug Evaluation, Preclinical, Molecular Conformation, Pharmaceutical Science, Pharmacology, Crystallography, X-Ray, 01 natural sciences, Biochemistry, Rats, Sprague-Dawley, chemistry.chemical_compound, Mice, Catalytic Domain, Drug Discovery, Mice, Inbred BALB C, biology, Chemistry, Translation (biology), Pyridazines, Tyrosine kinase 2, Molecular Medicine, Half-Life, hERG, Molecular Dynamics Simulation, Pyrrolopyridazine, Cell Line, 03 medical and health sciences, Inhibitory Concentration 50, Structure-Activity Relationship, In vivo, Potency, Animals, Humans, Pyrroles, Molecular Biology, Protein Kinase Inhibitors, Inflammation, TYK2 Kinase, Binding Sites, 010405 organic chemistry, Aryl, Organic Chemistry, Janus Kinase 3, Janus Kinase 1, Janus Kinase 2, 0104 chemical sciences, Rats, Disease Models, Animal, 030104 developmental biology, Murine model, biology.protein

Abstract

A series of potent dual JAK1/3 inhibitors have been developed from a moderately selective JAK3 inhibitor. Substitution at the C6 position of the pyrrolopyridazine core with aryl groups provided exceptional biochemical potency against JAK1 and JAK3 while maintaining good selectivity against JAK2 and Tyk2. Translation to in vivo efficacy was observed in a murine model of chronic inflammation. X-ray co-crystal structure determination confirmed the presumed inhibitor binding orientation in JAK3. Efforts to reduce hERG channel inhibition will be described.

Published

2017

46. Discovery of pyrrolo[1,2-b]pyridazine-3-carboxamides as Janus kinase (JAK) inhibitors

Author

Joel C. Barrish, Aberra Fura, Guoxiang Shen, Jingwu Duan, David S. Nirschl, Jonathan Lippy, Stephen T. Wrobleski, Rosemary Zhang, Lidia M. Doweyko, Bingwei V. Yang, Lauren Haque, Murray McKinnon, Shuqun Lin, Luisa Salter-Cid, Sidney Pitt, William J. Pitts, Percy H. Carter, John S. Sack, Gary L. Schieven, Bin Jiang, John Hynes, Gregory D. Brown, John S. Tokarski, Zhonghui Lu, Javed Khan, and Steven G. Nadler

Subjects

Models, Molecular, Protein Conformation, Stereochemistry, Clinical Biochemistry, Substituent, Administration, Oral, Pharmaceutical Science, Enzyme-Linked Immunosorbent Assay, Biochemistry, Pyrrolopyridazine, Pyridazine, Interferon-gamma, Mice, Structure-Activity Relationship, chemistry.chemical_compound, Drug Discovery, Functional selectivity, Animals, Humans, Pyrroles, Tissue Distribution, Protein Kinase Inhibitors, Molecular Biology, Whole blood, Mice, Inbred BALB C, Molecular Structure, Organic Chemistry, Janus Kinase 3, Janus Kinase 1, Janus Kinase 2, Pyridazines, chemistry, Tyrosine kinase 2, Molecular Medicine, Amine gas treating, Janus kinase

Abstract

A new class of Janus kinase (JAK) inhibitors was discovered using a rationally designed pyrrolo[1,2-b]pyridazine-3-carboxamide scaffold. Preliminary studies identified (R)-(2,2-dimethylcyclopentyl)amine as a preferred C4 substituent on the pyrrolopyridazine core (3b). Incorporation of amino group to 3-position of the cyclopentane ring resulted in a series of JAK3 inhibitors (4g-4j) that potently inhibited IFNγ production in an IL2-induced whole blood assay and displayed high functional selectivity for JAK3-JAK1 pathway relative to JAK2. Further modifications led to the discovery of an orally bioavailable (2-fluoro-2-methylcyclopentyl)amino analogue 5g which is a nanomolar inhibitor of both JAK3 and TYK2, functionally selective for the JAK3-JAK1 pathway versus JAK2, and active in a human whole blood assay.

Published

2014

47. Purine derivatives as potent Bruton’s tyrosine kinase (BTK) inhibitors for autoimmune diseases

Author

Alaric J. Dyckman, Joann Strnad, Jodi K. Muckelbauer, Yongmi An, Chiehying Chang, Lin Cheng, Hedy Li, James Lin, Joseph A. Tino, George V. De Lucca, Kim W. McIntyre, Qing Shi, Katerina Leftheris, James R. Burke, Chunjian Liu, Gilbert C. Olini, Andrew J. Tebben, Percy H. Carter, Qian Ruan, S. H. Spergel, and Neha Surti

Subjects

Models, Molecular, Purine, Clinical Biochemistry, Cell, Pharmaceutical Science, Crystallography, X-Ray, Biochemistry, Autoimmune Diseases, Mice, chemistry.chemical_compound, In vivo, Drug Discovery, Agammaglobulinaemia Tyrosine Kinase, medicine, Animals, Humans, Bruton's tyrosine kinase, Protein Kinase Inhibitors, Molecular Biology, ADME, CD86, B-Lymphocytes, biology, Chemistry, Kinase, Passive Cutaneous Anaphylaxis, Organic Chemistry, Protein-Tyrosine Kinases, Rats, medicine.anatomical_structure, Purines, biology.protein, Molecular Medicine, Function (biology)

Abstract

Investigation of various heterocyclic core isosteres of imidazopyrazines 1 & 2 yielded purine derivatives 3 & 8 as potent and selective BTK inhibitors. Subsequent SAR studies of the purine series led to the discovery of 20 as a leading compound. Compound 20 is very selective when screened against a panel of 400 kinases and is a potent inhibitor in cellular assays of human B cell function including B-Cell proliferation and CD86 cell surface expression and exhibited in vivo efficacy in a mouse PCA model. Its X-ray co-crystal structure with BTK shows that the high selectivity is gained from filling a BTK specific lipophilic pocket. However, physical and ADME properties leading to low oral exposure hindered further development.

Published

2014

48. Asymmetric Hydroboration Approach to the Scalable Synthesis of ((1R,3S)-1-Amino-3-((R)-6-hexyl-5,6,7,8-tetrahydronaphthalen-2-yl)cyclopentyl)methanol (BMS-986104) as a Potent S1P

Author

Michael G, Yang, Zili, Xiao, T G Murali, Dhar, Hai-Yun, Xiao, John L, Gilmore, David, Marcoux, Jenny H, Xie, Kim W, McIntyre, Tracy L, Taylor, Virna, Borowski, Elizabeth, Heimrich, Yu-Wen, Li, Jianlin, Feng, Alda, Fernandes, Zheng, Yang, Praveen, Balimane, Anthony M, Marino, Georgia, Cornelius, Bethanne M, Warrack, Arvind, Mathur, Dauh-Rurng, Wu, Peng, Li, Anuradha, Gupta, Bala, Pragalathan, Ding Ren, Shen, Mary Ellen, Cvijic, Lois D, Lehman-McKeeman, Luisa, Salter-Cid, Joel C, Barrish, Percy H, Carter, and Alaric J, Dyckman

Subjects

Mice, Inbred BALB C, Encephalomyelitis, Autoimmune, Experimental, Dose-Response Relationship, Drug, Molecular Structure, Naphthalenes, Mice, Inbred C57BL, Disease Models, Animal, Mice, Receptors, Lysosphingolipid, Structure-Activity Relationship, HEK293 Cells, Animals, Humans, Female, Lymphocytes, Cells, Cultured

Abstract

We describe a highly efficient route for the synthesis of 4a (BMS-986104). A key step in the synthesis is the asymmetric hydroboration of trisubstituted alkene 6. Particularly given the known difficulties involved in this type of transformation (6 → 7), the current methodology provides an efficient approach to prepare this class of compounds. In addition, we disclose the efficacy of 4a in a mouse EAE model, which is comparable to 4c (FTY720). Mechanistically, 4a exhibited excellent remyelinating effects on lysophosphatidylcholine (LPC) induced demyelination in a three-dimensional brain cell culture assay.

Published

2016

49. Structure of CC chemokine receptor 2 with orthosteric and allosteric antagonists

Author

Marta Dabros, Gye Won Han, Ruben Abagyan, Vadim Cherezov, Andrew J. Tebben, Natalia V. Ortiz Zacarías, Robert J. Cherney, Ling Qin, Laura H. Heitman, Raymond C. Stevens, Adriaan P. IJzerman, Dean Stamos, Percy H. Carter, Chunxia Zhao, Martin Gustavsson, Irina Kufareva, Henk de Vries, Tracy M. Handel, and Yi Zheng

Subjects

0301 basic medicine, CCR1, CCR2, Chemokine, General Science & Technology, animal diseases, Allosteric regulation, Biology, Pharmacology, Ligands, 03 medical and health sciences, Chemokine receptor, Models, parasitic diseases, Receptors, Humans, Receptor, Multidisciplinary, Crystallography, Binding Sites, Molecular, CC, Heterotrimeric GTP-Binding Proteins, Pyrrolidinones, 3. Good health, Cell biology, 030104 developmental biology, Chemokine binding, Drug Design, biology.protein, Quinazolines, X-Ray, Chemokines, CC chemokine receptors, Allosteric Site

Abstract

Structure of CC chemokine receptor 2 with orthosteric and allosteric antagonistsYi Zheng, Ling Qin, Natalia V. Ortiz Zacarías, Henk de Vries, Gye Won Han, Martin Gustavsson, Marta Dabros, Chunxia Zhao, Robert J. Cherney, Percy Carter, Dean Stamos, Ruben Abagyan, Vadim Cherezov, Raymond C. Stevens, Adriaan P. IJzerman, Laura H. Heitman, Andrew Tebben, Irina Kufareva & Tracy M. HandelCC chemokine receptor 2 (CCR2) is one of 19 members of the chemokine receptor subfamily of human class A G-protein-coupled receptors. CCR2 is expressed on monocytes, immature dendritic cells, and T-cell subpopulations, and mediates their migration towards endogenous CC chemokine ligands such as CCL2 (ref. 1). CCR2 and its ligands are implicated in numerous inflammatory and neurodegenerative diseases2 including atherosclerosis, multiple sclerosis, asthma, neuropathic pain, and diabetic nephropathy, as well as cancer3. These disease associations have motivated numerous preclinical studies and clinical trials4 (see http://www.clinicaltrials.gov) in search of therapies that target the CCR2–chemokine axis. To aid drug discovery efforts5, here we solve a structure of CCR2 in a ternary complex with an orthosteric (BMS-681 (ref. 6)) and allosteric (CCR2-RA-[R]7) antagonist. BMS-681 inhibits chemokine binding by occupying the orthosteric pocket of the receptor in a previously unseen binding mode. CCR2-RA-[R] binds in a novel, highly druggable pocket that is the most intracellular allosteric site observed in class A G-protein-coupled receptors so far; this site spatially overlaps the G-protein-binding site in homologous receptors. CCR2-RA-[R] inhibits CCR2 non-competitively by blocking activation-associated conformational changes and formation of the G-protein-binding interface. The conformational signature of the conserved microswitch residues observed in double-antagonist-bound CCR2 resembles the most inactive G-protein-coupled receptor structures solved so far. Like other protein–protein interactions, receptor–chemokine complexes are considered challenging therapeutic targets for small molecules, and the present structure suggests diverse pocket epitopes that can be exploited to overcome obstacles in drug design.

Published

2016

50. Identification of Tricyclic Agonists of Sphingosine-1-phosphate Receptor 1 (S1P

Author

Hai-Yun, Xiao, Scott H, Watterson, Charles M, Langevine, Anurag S, Srivastava, Soo S, Ko, Yanlei, Zhang, Robert J, Cherney, Wei-Wei, Guo, John L, Gilmore, James E, Sheppeck, Dauh-Rurng, Wu, Peng, Li, Duraisamy, Ramasamy, Piramanayagam, Arunachalam, Arvind, Mathur, Tracy L, Taylor, David J, Shuster, Kim W, McIntyre, Ding-Ren, Shen, Melissa, Yarde, Mary Ellen, Cvijic, Anthony M, Marino, Praveen V, Balimane, Zheng, Yang, Dana M, Banas, Georgia, Cornelius, Celia J, D'Arienzo, Bethanne M, Warrack, Lois, Lehman-McKeeman, Luisa M, Salter-Cid, Jenny, Xie, Joel C, Barrish, Percy H, Carter, Alaric J, Dyckman, and T G Murali, Dhar

Subjects

Male, Dose-Response Relationship, Drug, Molecular Structure, Fingolimod Hydrochloride, Freund's Adjuvant, Ligands, Arthritis, Experimental, Mycobacterium, Rats, Macaca fascicularis, Mice, Receptors, Lysosphingolipid, Structure-Activity Relationship, Dogs, Rats, Inbred Lew, Drug Design, Animals, Tissue Distribution, Lymphocytes, Heterocyclic Compounds, 3-Ring

Abstract

Fingolimod (1) is the first approved oral therapy for the treatment of relapsing remitting multiple sclerosis. While the phosphorylated metabolite of fingolimod was found to be a nonselective S1P receptor agonist, agonism specifically of S1P

Published

2016