Your search keyword '"Cutrona KJ"' showing total 21 results

1. Insights on JAK2 Modulation by Potent, Selective, and Cell-Permeable Pseudokinase-Domain Ligands.

Author

Liosi ME, Ippolito JA, Henry SP, Krimmer SG, Newton AS, Cutrona KJ, Olivarez RA, Mohanty J, Schlessinger J, and Jorgensen WL

Subjects

Humans, Janus Kinase 2 metabolism, Ligands, Mutation, STAT Transcription Factors genetics, STAT Transcription Factors metabolism, Signal Transduction, Janus Kinases metabolism, Myeloproliferative Disorders

Abstract

JAK2 is a non-receptor tyrosine kinase that regulates hematopoiesis through the JAK-STAT pathway. The pseudokinase domain (JH2) is an important regulator of the activity of the kinase domain (JH1). V617F mutation in JH2 has been associated with the pathogenesis of various myeloproliferative neoplasms, but JAK2 JH2 has been poorly explored as a pharmacological target. In light of this, we aimed to develop JAK2 JH2 binders that could selectively target JH2 over JH1 and test their capacity to modulate JAK2 activity in cells. Toward this goal, we optimized a diaminotriazole lead compound into potent, selective, and cell-permeable JH2 binders leveraging computational design, synthesis, binding affinity measurements for the JH1, JH2 WT, and JH2 V617F domains, permeability measurements, crystallography, and cell assays. Optimized diaminotriazoles are capable of inhibiting STAT5 phosphorylation in both WT and V617F JAK2 in cells.

Published

2022

2. Conversion of a False Virtual Screen Hit into Selective JAK2 JH2 Domain Binders Using Convergent Design Strategies.

Author

Henry SP, Liosi ME, Ippolito JA, Cutrona KJ, Krimmer SG, Newton AS, Schlessinger J, and Jorgensen WL

Abstract

The Janus kinase 2 (JAK2) pseudokinase domain (JH2) is an ATP-binding domain that regulates the activity of the catalytic tyrosine kinase domain (JH1). Dysregulation of JAK2 JH1 signaling caused by the V617F mutation in JH2 is implicated in various myeloproliferative neoplasms. To explore if JAK2 activity can be modulated by a small molecule binding to the ATP site in JH2, we have developed several ligand series aimed at selectively targeting the JAK2 JH2 domain. We report here the evolution of a false virtual screen hit into a new JAK2 JH2 series. Optimization guided by computational modeling has yielded analogues with nanomolar affinity for the JAK2 JH2 domain and >100-fold selectivity for the JH2 domain over the JH1 domain. A crystal structure for one of the potent compounds bound to JAK2 JH2 clarifies the origins of the strong binding and selectivity. The compounds expand the platform for seeking molecules to regulate JAK2 signaling, including V617F JAK2 hyperactivation., Competing Interests: The authors declare the following competing financial interest(s): Yale University has submitted a preliminary patent application on the compounds., (© 2022 American Chemical Society.)

Published

2022

3. Covalent Inhibition of Wild-Type HIV-1 Reverse Transcriptase Using a Fluorosulfate Warhead.

Author

Ippolito JA, Niu H, Bertoletti N, Carter ZJ, Jin S, Spasov KA, Cisneros JA, Valhondo M, Cutrona KJ, Anderson KS, and Jorgensen WL

Abstract

Covalent inhibitors of wild-type HIV-1 reverse transcriptase (CRTIs) are reported. Three compounds derived from catechol diether non-nucleoside inhibitors (NNRTIs) with addition of a fluorosulfate warhead are demonstrated to covalently modify Tyr181 of HIV-RT. X-ray crystal structures for complexes of the CRTIs with the enzyme are provided, which fully demonstrate the covalent attachment, and confirmation is provided by appropriate mass shifts in ESI-TOF mass spectra. The three CRTIs and six noncovalent analogues are found to be potent inhibitors with both IC 50 values for in vitro inhibition of WT RT and EC 50 values for cytopathic protection of HIV-1-infected human T-cells in the 5-320 nM range., Competing Interests: The authors declare no competing financial interest., (© 2021 American Chemical Society.)

Published

2021

4. Metadynamics as a Postprocessing Method for Virtual Screening with Application to the Pseudokinase Domain of JAK2.

Author

Cutrona KJ, Newton AS, Krimmer SG, Tirado-Rives J, and Jorgensen WL

Subjects

Binding Sites, Ligands, Protein Binding, Research Design

Abstract

With standard scoring methods, top-ranked compounds from virtual screening by docking often turn out to be inactive. For this reason, metadynamics, a method used to sample rare events, was studied to further evaluate docking poses with the aim of reducing false positives. Specifically, virtual screening was performed with Glide SP to seek potential molecules to bind to the ATP site in the pseudokinase domain of JAK2 kinase, and promising compounds were selected from the top-ranked 1000 based on visualization. Rescoring with Glide XP, GOLD, and MM/GBSA was unable to differentiate well between active and inactive compounds. Metadynamics was then used to gauge the relative binding affinity from the required time or the potential of mean force needed to dissociate the ligand from the bound complex. With consideration of previously known binders of varying affinities, metadynamics was able to differentiate between the most active compounds and inactive or weakly active ones, and it could identify correctly most of the selected virtual screening compounds as false positives. Thus, metadynamics has the potential to be a viable postprocessing method for virtual screening, minimizing the expense of buying or synthesizing inactive compounds.

Published

2020

5. Asymmetric Catalysis upon Helically Chiral Loratadine Analogues Unveils Enantiomer-Dependent Antihistamine Activity.

Author

Stone EA, Cutrona KJ, and Miller SJ

Subjects

Catalysis, Histamine Antagonists chemical synthesis, Histamine Antagonists chemistry, Humans, Loratadine analogs & derivatives, Loratadine chemistry, Molecular Conformation, Molecular Docking Simulation, Stereoisomerism, Aspartic Acid chemistry, Histamine Antagonists pharmacology, Loratadine pharmacology, Peptides chemistry, Receptors, Histamine metabolism

Abstract

Analogues of the conformationally dynamic Claritin (loratadine) and Clarinex (desloratadine) scaffolds have been enantio- and chemoselectively N -oxidized using an aspartic acid containing peptide catalyst to afford stable, helically chiral products in up to >99:1 er. The conformational dynamics and enantiomeric stability of the N -oxide products have been investigated experimentally and computationally with the aid of crystallographic data. Furthermore, biological assays show that rigidifying the core structure of loratadine and related analogues through N -oxidation affects antihistamine activity in an enantiomer-dependent fashion. Computational docking studies illustrate the observed activity differences.

Published

2020

6. Selective Janus Kinase 2 (JAK2) Pseudokinase Ligands with a Diaminotriazole Core.

Author

Liosi ME, Krimmer SG, Newton AS, Dawson TK, Puleo DE, Cutrona KJ, Suzuki Y, Schlessinger J, and Jorgensen WL

Subjects

Animals, HEK293 Cells, Humans, Ligands, Protein Binding physiology, Sf9 Cells, X-Ray Diffraction methods, Amitrole chemistry, Amitrole metabolism, Enzyme Activators chemistry, Enzyme Activators metabolism, Janus Kinase 2 chemistry, Janus Kinase 2 metabolism

Abstract

Janus kinases (JAKs) are non-receptor tyrosine kinases that are essential components of the JAK-STAT signaling pathway. Associated aberrant signaling is responsible for many forms of cancer and disorders of the immune system. The present focus is on the discovery of molecules that may regulate the activity of JAK2 by selective binding to the JAK2 pseudokinase domain, JH2. Specifically, the Val617Phe mutation in JH2 stimulates the activity of the adjacent kinase domain (JH1) resulting in myeloproliferative disorders. Starting from a non-selective screening hit, we have achieved the goal of discovering molecules that preferentially bind to the ATP binding site in JH2 instead of JH1. We report the design and synthesis of the compounds and binding results for the JH1, JH2, and JH2 V617F domains, as well as five crystal structures for JH2 complexes. Testing with a selective and non-selective JH2 binder on the autophosphorylation of wild-type and V617F JAK2 is also contrasted.

Published

2020

7. JAK2 JH2 Fluorescence Polarization Assay and Crystal Structures for Complexes with Three Small Molecules.

Author

Newton AS, Deiana L, Puleo DE, Cisneros JA, Cutrona KJ, Schlessinger J, and Jorgensen WL

Abstract

A competitive fluorescence polarization (FP) assay is reported for determining binding affinities of probe molecules with the pseudokinase JAK2 JH2 allosteric site. The syntheses of the fluorescent 5 and 6 used in the assay are reported as well as K d results for 10 compounds, including JNJ7706621, NVP-BSK805, and filgotinib (GLPG0634). X-ray crystal structures of JAK2 JH2 in complex with NVP-BSK805, filgotinib, and diaminopyrimidine 8 elucidate the binding poses.

Published

2017

8. Investigating the nucleic acid interactions of histone-derived antimicrobial peptides.

Author

Sim S, Wang P, Beyer BN, Cutrona KJ, Radhakrishnan ML, and Elmore DE

Subjects

Amino Acid Sequence, Amino Acid Substitution, Animals, Anti-Bacterial Agents chemical synthesis, Anti-Bacterial Agents isolation & purification, Anura physiology, Histones chemical synthesis, Histones isolation & purification, Kinetics, Molecular Dynamics Simulation, Molecular Mimicry, Protein Binding, Protein Structure, Secondary, Proteins chemical synthesis, Proteins isolation & purification, Structure-Activity Relationship, Thermodynamics, Anti-Bacterial Agents chemistry, Arginine chemistry, DNA, Bacterial chemistry, Histones chemistry, Lysine chemistry, Proteins chemistry

Abstract

While many antimicrobial peptides (AMPs) disrupt bacterial membranes, some translocate into bacteria and interfere with intracellular processes. Buforin II and DesHDAP1 are thought to kill bacteria by interacting with nucleic acids. Here, molecular modeling and experimental measurements are used to show that neither nucleic acid binding peptide selectively binds DNA sequences. Simulations and experiments also show that changing lysines to arginines enhances DNA binding, suggesting that including additional guanidinium groups is a potential strategy to engineer more potent AMPs. Moreover, the lack of binding specificity may make it more difficult for bacteria to evolve resistance to these and other similar AMPs., (© 2017 Federation of European Biochemical Societies.)

Published

2017

9. Role of arginine and lysine in the antimicrobial mechanism of histone-derived antimicrobial peptides.

Author

Cutrona KJ, Kaufman BA, Figueroa DM, and Elmore DE

Subjects

Amino Acid Sequence, Antimicrobial Cationic Peptides genetics, Antimicrobial Cationic Peptides metabolism, Cell Membrane drug effects, Cell Membrane metabolism, Molecular Sequence Data, Mutation, Protein Transport, Structure-Activity Relationship, Antimicrobial Cationic Peptides chemistry, Antimicrobial Cationic Peptides pharmacology, Arginine, Histones chemistry, Lysine

Abstract

Translocation of cell-penetrating peptides is often promoted by increased content of arginine or other guanidinium groups. However, relatively little research has considered the role of these functional groups on antimicrobial peptide activity. This study compared the activity of three histone-derived antimicrobial peptides-buforin II, DesHDAP1, and parasin-with variants that contain only lysine or arginine cationic residues. These peptides operate via different mechanisms as parasin causes membrane permeabilization while buforin II and DesHDAP1 translocate into bacteria. For all peptides, antibacterial activity increased with increased arginine content. Higher arginine content increased permeabilization for parasin while it improved translocation for buforin II and DesHDAP1. These observations provide insight into the relative importance of arginine and lysine in these antimicrobial peptides., (Copyright © 2015 Federation of European Biochemical Societies. Published by Elsevier B.V. All rights reserved.)

Published

2015

10. Evaluation of CM5 Charges for Nonaqueous Condensed-Phase Modeling.

Author

Dodda LS, Vilseck JZ, Cutrona KJ, and Jorgensen WL

Subjects

Models, Molecular, Thermodynamics, Quantum Theory

Abstract

Partial atomic charges for neutral molecules from quantum mechanical calculations are typically scaled for use in molecular modeling of liquid-phase systems. Optimal scale factors of 1.14 for CM1A and 1.27 for CM5 charges were previously determined for minimizing errors in free energies of hydration. The adequacy of the 1.14*CM1A and 1.27*CM5 models are evaluated here in pure liquid simulations in combination with the OPLS-AA force field. For 22 organic liquids, the 1.14*CM1A and 1.27*CM5 models yield mean unsigned errors (MUEs) of ca. 1.40 kcal/mol for heats of vaporization. Not surprisingly, this reflects overpolarization with the scale factors derived for aqueous media. Prediction of pure liquid properties using CM5 charges is optimized using a scale factor of 1.14, which reduces the MUE for heats of vaporization to 0.89 kcal/mol. However, due to the impracticality of using different scale factors in different explicit-solvent condensed-phase simulations, a universal scale factor of 1.20 emerged for CM5 charges. This provides a balance between errors in computed pure liquid properties and free energies of hydration. Computation of free energies of hydration by the GB/SA method further found that 1.20 is equally suited for use in explicit or implicit treatments of aqueous solvation. With 1.20*CM5 charges, a variety of condensed-phase simulations can be pursued while maintaining average errors of 1.0 kcal/mol in key thermodynamic properties.

Published

2015

11. Design, synthesis and SAR of a series of 1,3,5-trisubstituted benzenes as thrombin inhibitors.

Author

Isaacs RC, Newton CL, Cutrona KJ, Mercer SP, Payne LS, Stauffer KJ, Williams PD, Cook JJ, Krueger JA, Lewis SD, Lucas BJ, Lyle EA, Lynch JJ, McMasters DR, Naylor-Olsen AM, Michener MT, and Wallace AA

Subjects

Antithrombins chemistry, Antithrombins pharmacology, Benzene chemistry, Benzene pharmacology, Humans, Models, Molecular, Molecular Structure, Structure-Activity Relationship, Antithrombins chemical synthesis, Benzene chemical synthesis, Drug Design, Thrombin antagonists & inhibitors

Abstract

A novel 1,3,5-trisubstituted benzamide thrombin inhibitor template was designed via hybridization of a known aminopyridinoneacetamide and a known 1,3,5-trisubstituted phenyl ether. Optimization of this lead afforded a novel potent series of biaryl 1,3,5-trisubstituted benzenes with excellent functional anticoagulant potency., (Copyright © 2010 Elsevier Ltd. All rights reserved.)

Published

2011

12. P3 optimization of functional potency, in vivo efficacy and oral bioavailability in 3-aminopyrazinone thrombin inhibitors bearing non-charged groups at the P1 position.

Author

Isaacs RC, Newton CL, Cutrona KJ, Mercer SP, Dorsey BD, McDonough CM, Cook JJ, Krueger JA, Lewis SD, Lucas BJ, Lyle EA, Lynch JJ, Miller-Stein C, Michener MT, Wallace AA, White RB, and Wong BK

Subjects

Administration, Oral, Animals, Anticoagulants chemistry, Anticoagulants pharmacology, Binding Sites, Biological Availability, Dogs, Molecular Structure, Pyrazines chemistry, Pyrazines pharmacology, Rats, Structure-Activity Relationship, Anticoagulants chemical synthesis, Blood Coagulation Disorders drug therapy, Drug Design, Pyrazines chemical synthesis, Thrombin antagonists & inhibitors

Abstract

Although the S3 pocket of the thrombin active site is lined with lipophilic amino acid residues, the accommodation of polarity within the lipophilic P3 moiety of small molecule inhibitors is possible provided that the polar functionality is capable of pointing away from the binding pocket outwards toward solvent while simultaneously allowing the lipophilic portion of the P3 ligand to interact with the S3 amino acid residues. Manipulation of this motif provided the means to effect optimization of functional potency, in vivo antithrombotic efficacy and oral bioavailability in a series of 3-aminopyrazinone thrombin inhibitors which contained non-charged groups at the P1 position., (Copyright © 2010 Elsevier Ltd. All rights reserved.)

Published

2011

13. Structure-based design of novel groups for use in the P1 position of thrombin inhibitor scaffolds. Part 2: N-acetamidoimidazoles.

Author

Isaacs RC, Solinsky MG, Cutrona KJ, Newton CL, Naylor-Olsen AM, McMasters DR, Krueger JA, Lewis SD, Lucas BJ, Kuo LC, Yan Y, Lynch JJ, and Lyle EA

Subjects

Administration, Oral, Animals, Anticoagulants chemical synthesis, Anticoagulants chemistry, Anticoagulants pharmacokinetics, Antithrombins chemical synthesis, Antithrombins chemistry, Antithrombins pharmacokinetics, Biological Availability, Chlorides, Crystallography, X-Ray, Dogs, Ferric Compounds pharmacology, Imidazoles chemistry, Imidazoles pharmacokinetics, Macaca mulatta, Models, Molecular, Molecular Structure, Partial Thromboplastin Time, Rats, Structure-Activity Relationship, Thrombin chemistry, Thrombin metabolism, Trypsin metabolism, Anticoagulants pharmacology, Antithrombins pharmacology, Drug Design, Imidazoles chemical synthesis, Imidazoles pharmacology, Thrombin antagonists & inhibitors

Abstract

Guided by X-ray crystallography of thrombin-inhibitor complexes and molecular modeling, alkylation of the N1 nitrogen of the imidazole P1 ligand of the pyridinoneacetamide thrombin inhibitor 1 with various acetamide moieties furnished inhibitors with significantly improved thrombin potency, trypsin selectivity, functional in vitro anticoagulant potency and in vivo antithrombotic efficacy. In the pyrazinoneacetamide series, oral bioavailability was also improved.

Published

2008

14. Structure-based design of novel groups for use in the P1 position of thrombin inhibitor scaffolds. Part 1: Weakly basic azoles.

Author

Isaacs RC, Solinsky MG, Cutrona KJ, Newton CL, Naylor-Olsen AM, Krueger JA, Lewis SD, and Lucas BJ

Subjects

Azoles chemistry, Drug Design, Ligands, Molecular Structure, Structure-Activity Relationship, Trypsin drug effects, Azoles pharmacology, Enzyme Inhibitors pharmacology, Thrombin antagonists & inhibitors

Abstract

Despite their relatively weak basicity, simple azoles, specifically imidazoles and aminothiazoles, can function as potent surrogates for the more basic amines (e.g., alkyl amines, amidines, guanidines, etc.) which are most often employed as the P1 ligand in the design of noncovalent small molecule inhibitors of thrombin.

Published

2006

15. Unexpected enhancement of thrombin inhibitor potency with o-aminoalkylbenzylamides in the P1 position.

Author

Rittle KE, Barrow JC, Cutrona KJ, Glass KL, Krueger JA, Kuo LC, Lewis SD, Lucas BJ, McMasters DR, Morrissette MM, Nantermet PG, Newton CL, Sanders WM, Yan Y, Vacca JP, and Selnick HG

Subjects

Antithrombins chemistry, Crystallography, X-Ray, Molecular Structure, Amides chemistry, Antithrombins pharmacology

Abstract

Thrombin inhibitors incorporating o-aminoalkylbenzylamides in the P1 position were designed, synthesized and found to have enhanced potency and selectivity in several different structural classes. X-ray crystallographic analysis of compound 24 bound in the alpha-thrombin-hirugen complex provides an explanation for these unanticipated results.

Published

2003

16. 3-amino-4-sulfonylpyridinone acetamide and related pyridothiadiazine thrombin inhibitors.

Author

Sanderson PE, Cutrona KJ, Savage KL, Naylor-Olsen AM, Bickel DJ, Bohn DL, Clayton FC, Krueger JA, Lewis SD, Lucas BJ, Lyle EA, Wallace AA, Welsh DC, and Yan Y

Subjects

Acetamides pharmacokinetics, Administration, Oral, Animals, Disease Models, Animal, Dogs, Ferric Compounds toxicity, Humans, Models, Molecular, Pyridones pharmacokinetics, Rats, Structure-Activity Relationship, Sulfones chemistry, Sulfones pharmacokinetics, Sulfones pharmacology, Thiadiazines pharmacokinetics, Thrombosis chemically induced, Trypsin Inhibitors chemistry, Trypsin Inhibitors pharmacokinetics, Trypsin Inhibitors pharmacology, Acetamides chemistry, Acetamides pharmacology, Pyridones chemistry, Pyridones pharmacology, Thiadiazines chemistry, Thiadiazines pharmacology, Thrombin antagonists & inhibitors

Abstract

We describe a series of highly potent and efficacious thrombin inhibitors based on a 3-amino-4-sulfonylpyridinone acetamide template. The functionally dense sulfonyl group stabilizes the aminopyridinone, conformationally constrains the 4-substituent, and forms a hydrogen bond to the insertion loop tyrosine OH. We also describe a related series of fused bicyclic dihydrothiadiazinedioxide derivatives, of which one had improved pharmacokinetics in dogs after oral dosing.

Published

2003

17. Small, low nanomolar, noncovalent thrombin inhibitors lacking a group to fill the 'distal binding pocket'.

Author

Sanderson PE, Cutrona KJ, Dyer DL, Krueger JA, Kuo LC, Lewis SD, Lucas BJ, and Yan Y

Subjects

Binding Sites, Crystallization, Crystallography, X-Ray, Enzyme Inhibitors chemistry, Humans, Models, Molecular, Molecular Conformation, Thrombin chemistry, Acetamides chemical synthesis, Acetamides pharmacology, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors pharmacology, Pyridones chemical synthesis, Pyridones pharmacology, Thrombin antagonists & inhibitors

Abstract

Use of a chlorophenoxyacetamide P1 group with a pyridinone acetamide P2/P3 gave an exceptionally potent thrombin inhibitor (K(i)=40 pM). Truncation of the molecule at the N-terminus gave unique, low nanomolar, non-covalent thrombin inhibitors which do not have a group to fill thrombin's 'distal binding pocket'. A co-crystal structure indicates the importance of an intramolecular hydrogen bond between the P1 side chain and P1/P2 amide link in this series.

Published

2003

18. Efficacious, orally bioavailable thrombin inhibitors based on 3-aminopyridinone or 3-aminopyrazinone acetamide peptidomimetic templates.

Author

Sanderson PE, Lyle TA, Cutrona KJ, Dyer DL, Dorsey BD, McDonough CM, Naylor-Olsen AM, Chen IW, Chen Z, Cook JJ, Cooper CM, Gardell SJ, Hare TR, Krueger JA, Lewis SD, Lin JH, Lucas BJ Jr, Lyle EA, Lynch JJ Jr, Stranieri MT, Vastag K, Yan Y, Shafer JA, and Vacca JP

Subjects

Aminopyridines chemistry, Aminopyridines pharmacokinetics, Aminopyridines pharmacology, Animals, Biological Availability, Crystallography, X-Ray, Dogs, Macaca mulatta, Models, Molecular, Molecular Mimicry, Pyrazines chemistry, Pyrazines pharmacokinetics, Pyrazines pharmacology, Pyridones chemistry, Pyridones pharmacokinetics, Pyridones pharmacology, Rats, Structure-Activity Relationship, Aminopyridines chemical synthesis, Peptides chemistry, Pyrazines chemical synthesis, Pyridones chemical synthesis, Thrombin antagonists & inhibitors

Abstract

We have addressed the key deficiency of noncovalent pyridinone acetamide thrombin inhibitor L-374,087 (1), namely, its modest half-lives in animals, by making a chemically stable 3-alkylaminopyrazinone bioisostere for its 3-sulfonylaminopyridinone core. Compound 3 (L-375,378), the closest aminopyrazinone analogue of 1, has comparable selectivity and slightly decreased efficacy but significantly improved pharmacokinetics in rats, dogs, and monkeys to 1. We have developed an efficient and versatile synthesis of 3, and this compound has been chosen for further preclinical and clinical development.

Published

1998

19. C6 modification of the pyridinone core of thrombin inhibitor L-374,087 as a means of enhancing its oral absorption.

Author

Isaacs RC, Cutrona KJ, Newton CL, Sanderson PE, Solinsky MG, Baskin EP, Chen IW, Cooper CM, Cook JJ, Gardell SJ, Lewis SD, Lucas RJ Jr, Lyle EA, Lynch JJ Jr, Naylor-Olsen AM, Stranieri MT, Vastag K, and Vacca JP

Subjects

Administration, Oral, Animals, Antithrombins administration & dosage, Biological Availability, Dogs, Pyridines chemistry, Pyridines pharmacokinetics, Pyridines pharmacology, Pyridones pharmacology, Rats, Sulfanilamides chemistry, Sulfanilamides pharmacokinetics, Sulfanilamides pharmacology, Sulfonamides pharmacology, Antithrombins chemistry, Antithrombins pharmacokinetics, Pyridones chemistry, Pyridones pharmacokinetics, Sulfonamides chemistry, Sulfonamides pharmacokinetics

Abstract

1 (L-374,087) is a potent, selective, efficacious, and orally bioavailable thrombin inhibitor that contains a core 3-amino-2-pyridinone moiety. Replacement of the C6 pyridinone methyl group of 1 by a propyl group gave 5 (L-375,052), which retained all the excellent properties of 1, and also yielded higher plasma levels after oral dosing in dogs and rats.

Published

1998

20. L-374,087, an efficacious, orally bioavailable, pyridinone acetamide thrombin inhibitor.

Author

Sanderson PE, Cutrona KJ, Dorsey BD, Dyer DL, McDonough CM, Naylor-Olsen AM, Chen IW, Chen Z, Cook JJ, Gardell SJ, Krueger JA, Lewis SD, Lin JH, Lucas BJ Jr, Lyle EA, Lynch JJ Jr, Stranieri MT, Vastag K, Shafer JA, and Vacca JP

Subjects

Administration, Oral, Animals, Anticoagulants administration & dosage, Anticoagulants chemistry, Biological Availability, Chlorides, Crystallography, X-Ray, Dogs, Ferric Compounds, Kinetics, Macaca fascicularis, Models, Molecular, Molecular Structure, Pyridones administration & dosage, Pyridones chemistry, Rats, Structure-Activity Relationship, Sulfonamides administration & dosage, Sulfonamides chemistry, Thrombosis drug therapy, Trypsin metabolism, Anticoagulants pharmacology, Pyridones pharmacology, Sulfonamides pharmacology, Thrombin antagonists & inhibitors

Abstract

Replacement of the amidinopiperidine P1 group of 3-benzylsulfonylamino-6-methyl-2-pyridinone acetamide thrombin inhibitor L-373,890 (2) with a mildly basic 5-linked 2-amino-6-methylpyridine results in an equipotent compound L-374,087 (5, Ki = 0.5 nM). Compound 5 is highly selective for thrombin over trypsin, is efficacious in the rat ferric chloride model of arterial thrombosis and is orally bioavailable in dogs and cynomolgus monkeys. The structural basis for the critical importance of both methyl groups in 5 was confirmed by X-ray crystallography.

Published

1998

21. Characterization of the two-step pathway for inhibition of thrombin by alpha-ketoamide transition state analogs.

Author

Lewis SD, Lucas BJ, Brady SF, Sisko JT, Cutrona KJ, Sanderson PE, Freidinger RM, Mao SS, Gardell SJ, and Shafer JA

Subjects

Binding Sites, Binding, Competitive, Catalysis, Flow Injection Analysis, Fluorescent Dyes, Kinetics, Models, Chemical, Oligopeptides pharmacology, Serine Proteinase Inhibitors chemistry, Serine Proteinase Inhibitors pharmacology, Thrombin antagonists & inhibitors

Abstract

The interaction of thrombin with several potent and selective alpha-ketoamide transition state analogs was characterized. L-370, 518 (H-N-Me-D-Phe-Pro-t-4-aminocyclohexylglycyl N-methylcarboxamide) a potent (Ki = 90 pM) and selective (>10(4)-fold versus trypsin) ketoamide thrombin inhibitor was shown to bind thrombin via a two-step reaction wherein the initially formed thrombin-inhibitor complex (EI1) rearranges to a more stable, final complex (EI2). A novel sequential stopped-flow analysis showed that k-1, the rate constant for dissociation of EI1, was comparable to k2, the rate constant for conversion of EI1 to EI2 (0.049 and 0.035 s-1, respectively) indicating that formation of the initial complex EI1 is partially rate controlling. Replacement of the N-terminal methylamino group in L-370,518 with a hydrogen (L-372,051) resulted in a 44-fold loss in potency (Ki = 4 nM) largely due to an increase in k-1. Consequently in the reaction of L-372,051 with thrombin formation of EI1 was not rate controlling. Replacement of the P1' N-methylcarboxamide group of L-370,518 with an azetidylcarboxamido (L-372,228) produced a 58-fold increase in the value of the equilibrium constant (K-1) for dissociation of EI1. Nevertheless, L-372,228 was a 2-fold more potent thrombin inhibitor (Ki = 40 pM) than L-370,518 due to its 16-fold higher k2 and 10-fold lower k-2 values. The desketoamide analogs of L-370,518 and L-372,051, namely L-371,912 and L-372,011, inhibited thrombin via a one-step process. The Ki value for L-371,912 and the K-1 value for its alpha-ketoamide analog, L-370,518, were similar (5 and 14 nM, respectively). Likewise, the Ki value for L-372,011 and the K-1 value for its alpha-ketoamide analog, L-372,051, were similar (330 and 285 nM, respectively). These observations are consistent with the view that the alpha-ketoamides L-370,518 and L-372,051 form initial complexes with thrombin that are similar to the complexes formed by their desketoamide analogs, and in a second step the alpha-ketoamides react with the active site serine residue of thrombin to form a more stable hemiketal adduct.

Published

1998