Your search keyword '"Nantermet PG"' showing total 28 results

1. Neutralization of Pathogenic Fungi with Small-Molecule Immunotherapeutics.

Author

Chirkin E, Muthusamy V, Mann P, Roemer T, Nantermet PG, and Spiegel DA

Subjects

Acetylglucosamine chemistry, Antibodies metabolism, B-Lymphocyte Subsets cytology, Candida albicans metabolism, Candida albicans pathogenicity, Chitin chemistry, Chitin metabolism, Dinitrobenzenes chemistry, Dinitrobenzenes immunology, Drug Design, Fungal Proteins chemistry, Fungal Proteins metabolism, HL-60 Cells, Host-Pathogen Interactions, Humans, Phagocytosis, Antibodies immunology, B-Lymphocyte Subsets immunology, Candida albicans immunology

Abstract

Systemic fungal infections represent an important public health concern, and new antifungal agents are highly desirable. Herein, we describe the design, synthesis, and biological evaluation of a novel class of antifungal compounds called antibody-recruiting molecules targeting fungi (ARM-Fs). Our approach relies on the use of non-peptidic small molecules, which selectively bind fungal cells and recruit endogenous antibodies to their surfaces, resulting in immune-mediated clearance. Using the opportunistic fungal pathogen Candida albicans as a model, we identified a highly specific bifunctional molecule able to mediate the engulfment and phagocytosis of C. albicans cells by human immune cells in biologically relevant functional assays. This work represents a novel therapeutic approach to treating fungal illness with significant potential to complement and/or combine with existing treatment strategies., (© 2017 Wiley-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2017

2. Synthesis of Complex Druglike Molecules by the Use of Highly Functionalized Bench-Stable Organozinc Reagents.

Author

Greshock TJ, Moore KP, McClain RT, Bellomo A, Chung CK, Dreher SD, Kutchukian PS, Peng Z, Davies IW, Vachal P, Ellwart M, Manolikakes SM, Knochel P, and Nantermet PG

Subjects

High-Throughput Screening Assays, Molecular Structure, Principal Component Analysis, Pyridines chemistry, Organometallic Compounds chemistry, Pyridines chemical synthesis, Zinc chemistry

Abstract

The reactivity of a representative set of 17 organozinc pivalates with 18 polyfunctional druglike electrophiles (informers) in Negishi cross-coupling reactions was evaluated by high-throughput experimentation protocols. The high-fidelity scaleup of successful reactions in parallel enabled the isolation of sufficient material for biological testing, thus demonstrating the high value of these new solid zinc reagents in a drug-discovery setting and potentially for many other applications in chemistry. Principal component analysis (PCA) clearly defined the independent roles of the zincates and the informers toward druggable-space coverage., (© 2016 Wiley-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2016

3. Discovery of MK-8718, an HIV Protease Inhibitor Containing a Novel Morpholine Aspartate Binding Group.

Author

Bungard CJ, Williams PD, Ballard JE, Bennett DJ, Beaulieu C, Bahnck-Teets C, Carroll SS, Chang RK, Dubost DC, Fay JF, Diamond TL, Greshock TJ, Hao L, Holloway MK, Felock PJ, Gesell JJ, Su HP, Manikowski JJ, McKay DJ, Miller M, Min X, Molinaro C, Moradei OM, Nantermet PG, Nadeau C, Sanchez RI, Satyanarayana T, Shipe WD, Singh SK, Truong VL, Vijayasaradhi S, Wiscount CM, Vacca JP, Crane SN, and McCauley JA

Abstract

A novel HIV protease inhibitor was designed using a morpholine core as the aspartate binding group. Analysis of the crystal structure of the initial lead bound to HIV protease enabled optimization of enzyme potency and antiviral activity. This afforded a series of potent orally bioavailable inhibitors of which MK-8718 was identified as a compound with a favorable overall profile.

Published

2016

4. Modeling a crowdsourced definition of molecular complexity.

Author

Sheridan RP, Zorn N, Sherer EC, Campeau LC, Chang CZ, Cumming J, Maddess ML, Nantermet PG, Sinz CJ, and O'Shea PD

Subjects

Databases, Chemical, Humans, Models, Chemical, Quantitative Structure-Activity Relationship, Stereoisomerism, Crowdsourcing, Molecular Structure

Abstract

This paper brings together the concepts of molecular complexity and crowdsourcing. An exercise was done at Merck where 386 chemists voted on the molecular complexity (on a scale of 1-5) of 2681 molecules taken from various sources: public, licensed, and in-house. The meanComplexity of a molecule is the average over all votes for that molecule. As long as enough votes are cast per molecule, we find meanComplexity is quite easy to model with QSAR methods using only a handful of physical descriptors (e.g., number of chiral centers, number of unique topological torsions, a Wiener index, etc.). The high level of self-consistency of the model (cross-validated R(2) ∼0.88) is remarkable given that our chemists do not agree with each other strongly about the complexity of any given molecule. Thus, the power of crowdsourcing is clearly demonstrated in this case. The meanComplexity appears to be correlated with at least one metric of synthetic complexity from the literature derived in a different way and is correlated with values of process mass intensity (PMI) from the literature and from in-house studies. Complexity can be used to differentiate between in-house programs and to follow a program over time.

Published

2014

5. Attenuation of scratch-induced reactive astrogliosis by novel EphA4 kinase inhibitors.

Author

Parmentier-Batteur S, Finger EN, Krishnan R, Rajapakse HA, Sanders JM, Kandpal G, Zhu H, Moore KP, Regan CP, Sharma S, Hess JF, Williams TM, Reynolds IJ, Vacca JP, Mark RJ, and Nantermet PG

Subjects

Animals, Astrocytes pathology, Blotting, Western, CHO Cells, Cell Movement drug effects, Cells, Cultured, Cricetinae, Cricetulus, Gliosis pathology, Humans, Immunohistochemistry, Ischemic Attack, Transient pathology, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Microscopy, Fluorescence, Rats, Rats, Sprague-Dawley, Small Molecule Libraries, Wound Healing drug effects, Gliosis drug therapy, Protein Kinase Inhibitors therapeutic use, Receptor, EphA4 antagonists & inhibitors, Wounds and Injuries pathology

Abstract

The EphA4 receptor and its ephrin ligands are involved in astrocytic gliosis following CNS injury. Therefore, a strategy aimed at the blockade of EphA4 signaling could have broad therapeutic interest in brain disorders. We have identified novel small molecule inhibitors of EphA4 kinase in specific enzymatic and cell-based assays. In addition, we have demonstrated in two in vitro models of scratch injury that EphA4 receptor kinase is activated through phosphorylation and is involved in the repopulation of the wound after the scratch. A potent EphA4 kinase inhibitor significantly inhibited wound closure and reduced the accumulation of the reactive astrocytes inside the scratch. We have also shown that after the transient focal cerebral ischemia in rats, a large glial scar is formed by the accumulation of astrocytes and chondroitin sulfate proteoglycan surrounding the infarcted tissue at 7 days and 14 days of reperfusion. EphA4 protein expression is highly up-regulated in the same areas at these time points, supporting its potential role in the glial scar formation and maintenance. Taken together, these results suggest that EphA4 kinase inhibitors might interfere with the astrogliosis reaction and thereby lead to improved neurological outcome after ischemic injury., (© 2011 Merck Sharp & Dohme Corp. Journal of Neurochemistry © 2011 International Society for Neurochemistry.)

Published

2011

6. Strategies towards improving the pharmacokinetic profile of ε-substituted lysinol-derived HIV protease inhibitors.

Author

Rajapakse HA, Walji AM, Moore KP, Zhu H, Mitra AW, Gregro AR, Tinney E, Burlein C, Touch S, Paton BL, Carroll SS, DiStefano DJ, Lai MT, Grobler JA, Sanchez RI, Williams TM, Vacca JP, and Nantermet PG

Subjects

Antiretroviral Therapy, Highly Active, HIV Infections drug therapy, HIV Protease Inhibitors chemistry, HIV Protease Inhibitors therapeutic use, Structure-Activity Relationship, HIV Protease Inhibitors pharmacokinetics, Lysine chemistry

Published

2011

7. SAR of tertiary carbinamine derived BACE1 inhibitors: role of aspartate ligand amine pKa in enzyme inhibition.

Author

Rajapakse HA, Nantermet PG, Selnick HG, Barrow JC, McGaughey GB, Munshi S, Lindsley SR, Young MB, Ngo PL, Holloway MK, Lai MT, Espeseth AS, Shi XP, Colussi D, Pietrak B, Crouthamel MC, Tugusheva K, Huang Q, Xu M, Simon AJ, Kuo L, Hazuda DJ, Graham S, and Vacca JP

Subjects

Catalysis, Humans, Models, Molecular, Structure-Activity Relationship, Amines metabolism, Amyloid Precursor Protein Secretases antagonists & inhibitors, Aspartic Acid metabolism, Aspartic Acid Endopeptidases antagonists & inhibitors, Enzyme Inhibitors pharmacology

Abstract

The optimization of tertiary carbinamine derived inhibitors of BACE1 from its discovery as an unstable lead to low nanomolar cell active compounds is described. Five-membered heterocycles are reported as stable and potency enhancing linkers. In the course of this work, we have discovered a clear trend where the activity of inhibitors at a given assay pH is dependent on pK(a) of the amino group that interacts directly with the catalytic aspartates. The potency of compounds as inhibitors of Alphabeta production in a cell culture assay correlated much better with BACE1 enzyme potency measured at pH 7.5 than at pH 4.5., (Copyright 2010 Elsevier Ltd. All rights reserved.)

Published

2010

8. Rapid P1 SAR of brain penetrant tertiary carbinamine derived BACE inhibitors.

Author

Zhu H, Young MB, Nantermet PG, Graham SL, Colussi D, Lai MT, Pietrak B, Price EA, Sankaranarayanan S, Shi XP, Tugusheva K, Holahan MA, Michener MS, Cook JJ, Simon A, Hazuda DJ, Vacca JP, and Rajapakse HA

Subjects

Amyloid Precursor Protein Secretases metabolism, Amyloid beta-Peptides metabolism, Animals, Aspartic Acid Endopeptidases metabolism, Brain metabolism, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors pharmacokinetics, Humans, Macaca mulatta, Oxadiazoles chemical synthesis, Oxadiazoles pharmacokinetics, Peptide Fragments metabolism, Structure-Activity Relationship, Sulfonamides chemical synthesis, Sulfonamides pharmacokinetics, Amyloid Precursor Protein Secretases antagonists & inhibitors, Aspartic Acid Endopeptidases antagonists & inhibitors, Brain enzymology, Enzyme Inhibitors chemistry, Oxadiazoles chemistry, Sulfonamides chemistry

Abstract

This Letter describes the one pot synthesis of tertiary carbinamine 3 and related analogs of brain penetrant BACE-1 inhibitors via the alkylation of the Schiff base intermediate 2. The methodology developed for this study provided a convenient and rapid means to explore the P1 region of these types of inhibitors, where the P1 group is installed in the final step using a one-pot two-step protocol. Further SAR studies led to the identification of 10 which is twofold more potent in vitro as compared to the lead compound. This inhibitor was characterized in a cisterna magna ported rhesus monkey model, where significant lowering of CSF Abeta40 was observed., (Copyright 2010 Elsevier Ltd. All rights reserved.)

Published

2010

9. Evolution of tertiary carbinamine BACE-1 inhibitors: Abeta reduction in rhesus CSF upon oral dosing.

Author

Nantermet PG, Rajapakse HA, Stanton MG, Stauffer SR, Barrow JC, Gregro AR, Moore KP, Steinbeiser MA, Swestock J, Selnick HG, Graham SL, McGaughey GB, Colussi D, Lai MT, Sankaranarayanan S, Simon AJ, Munshi S, Cook JJ, Holahan MA, Michener MS, and Vacca JP

Subjects

Administration, Oral, Amines administration & dosage, Amines pharmacology, Amyloid Precursor Protein Secretases chemistry, Amyloid Precursor Protein Secretases metabolism, Animals, Blood-Brain Barrier, Crystallography, X-Ray, Haplorhini, Inhibitory Concentration 50, Macaca mulatta, Molecular Conformation, Protease Inhibitors administration & dosage, Protease Inhibitors pharmacology, Structure-Activity Relationship, Amines chemistry, Amyloid Precursor Protein Secretases antagonists & inhibitors, Amyloid beta-Peptides cerebrospinal fluid, Peptide Fragments cerebrospinal fluid, Protease Inhibitors chemistry

Published

2009

10. Strategies toward improving the brain penetration of macrocyclic tertiary carbinamine BACE-1 inhibitors.

Author

Moore KP, Zhu H, Rajapakse HA, McGaughey GB, Colussi D, Price EA, Sankaranarayanan S, Simon AJ, Pudvah NT, Hochman JH, Allison T, Munshi SK, Graham SL, Vacca JP, and Nantermet PG

Subjects

Crystallography, X-Ray, Models, Molecular, Amines pharmacokinetics, Amyloid Precursor Protein Secretases antagonists & inhibitors, Aspartic Acid Endopeptidases antagonists & inhibitors, Brain metabolism, Enzyme Inhibitors pharmacokinetics

Abstract

This letter describes replacements for the P3 amide moiety present in previously reported tertiary carbinamine macrolactones. Although P-gp efflux issues associated with these amide-macrolactones were solved and full brain penetration was measured in one case, potency was compromised in the process.

Published

2007

11. Design, synthesis, and SAR of macrocyclic tertiary carbinamine BACE-1 inhibitors.

Author

Lindsley SR, Moore KP, Rajapakse HA, Selnick HG, Young MB, Zhu H, Munshi S, Kuo L, McGaughey GB, Colussi D, Crouthamel MC, Lai MT, Pietrak B, Price EA, Sankaranarayanan S, Simon AJ, Seabrook GR, Hazuda DJ, Pudvah NT, Hochman JH, Graham SL, Vacca JP, and Nantermet PG

Subjects

Amines chemical synthesis, Cyclization, Drug Design, Models, Molecular, Protease Inhibitors chemical synthesis, Structure-Activity Relationship, Amines chemistry, Amines pharmacology, Amyloid Precursor Protein Secretases antagonists & inhibitors, Aspartic Acid Endopeptidases antagonists & inhibitors, Protease Inhibitors chemistry, Protease Inhibitors pharmacology

Abstract

This Letter describes the design and synthesis of tertiary carbinamine macrocyclic inhibitors of the beta-secretase (BACE-1) enzyme. These macrocyclic inhibitors, some of which incorporate novel P2 substituents, display a 2- to 100-fold increase in potency relative to the previously described acyclic analogs while affording greater stability.

Published

2007

12. Discovery and SAR of isonicotinamide BACE-1 inhibitors that bind beta-secretase in a N-terminal 10s-loop down conformation.

Author

Stauffer SR, Stanton MG, Gregro AR, Steinbeiser MA, Shaffer JR, Nantermet PG, Barrow JC, Rittle KE, Collusi D, Espeseth AS, Lai MT, Pietrak BL, Holloway MK, McGaughey GB, Munshi SK, Hochman JH, Simon AJ, Selnick HG, Graham SL, and Vacca JP

Subjects

Animals, Baculoviridae drug effects, Baculoviridae enzymology, Biological Availability, Cells, Cultured, Magnetic Resonance Spectroscopy, Models, Molecular, Molecular Conformation, Molecular Weight, Niacinamide pharmacokinetics, Rats, Structure-Activity Relationship, Amyloid Precursor Protein Secretases antagonists & inhibitors, Aspartic Acid Endopeptidases antagonists & inhibitors, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors pharmacology, Niacinamide chemical synthesis, Niacinamide pharmacology

Abstract

A series of low-molecular weight 2,6-diamino-isonicotinamide BACE-1 inhibitors containing an amine transition-state isostere were synthesized and shown to be highly potent in both enzymatic and cell-based assays. These inhibitors contain a trans-S,S-methyl cyclopropane P(3) which bind BACE-1 in a 10s-loop down conformation giving rise to highly potent compounds with favorable molecular weight and moderate to high susceptibility to P-glycoprotein (P-gp) efflux.

Published

2007

13. Beta-secretase (BACE-1) inhibitors: accounting for 10s loop flexibility using rigid active sites.

Author

McGaughey GB, Colussi D, Graham SL, Lai MT, Munshi SK, Nantermet PG, Pietrak B, Rajapakse HA, Selnick HG, Stauffer SR, and Holloway MK

Subjects

Aspartic Acid analogs & derivatives, Aspartic Acid chemistry, Aspartic Acid pharmacology, Binding Sites, Catalysis, Chemical Phenomena, Chemistry, Physical, Crystallography, X-Ray, Enzyme Inhibitors chemistry, Ligands, Molecular Conformation, Structure-Activity Relationship, Thermodynamics, Amyloid Precursor Protein Secretases antagonists & inhibitors, Enzyme Inhibitors pharmacology

Abstract

BACE-1 is a flexible enzyme with experimentally determined motion in the flap region, the catalytic aspartates, and the 10s loop. Four in-house crystallographically determined complexes of tertiary carbinamine inhibitors revealed 10s loop motion in the S(3) pocket. These X-ray structures were used to correlate K(i) values, which span over five orders of magnitude, with the calculated interaction energy, using the Merck Molecular Force Field for a series of 19 tertiary carbinamine inhibitors.

Published

2007

14. Discovery of oxadiazoyl tertiary carbinamine inhibitors of beta-secretase (BACE-1).

Author

Rajapakse HA, Nantermet PG, Selnick HG, Munshi S, McGaughey GB, Lindsley SR, Young MB, Lai MT, Espeseth AS, Shi XP, Colussi D, Pietrak B, Crouthamel MC, Tugusheva K, Huang Q, Xu M, Simon AJ, Kuo L, Hazuda DJ, Graham S, and Vacca JP

Subjects

Aniline Compounds chemistry, Crystallography, X-Ray, Models, Molecular, Oxadiazoles chemistry, Amyloid Precursor Protein Secretases antagonists & inhibitors, Amyloid Precursor Protein Secretases chemistry, Aniline Compounds chemical synthesis, Oxadiazoles chemical synthesis

Abstract

We describe the discovery and optimization of tertiary carbinamine derived inhibitors of the enzyme beta-secretase (BACE-1). These novel non-transition-state-derived ligands incorporate a single primary amine to interact with the catalytic aspartates of the target enzyme. Optimization of this series provided inhibitors with intrinsic and functional potency comparable to evolved transition state isostere derived inhibitors of BACE-1.

Published

2006

15. P2 pyridine N-oxide thrombin inhibitors: a novel peptidomimetic scaffold.

Author

Nantermet PG, Burgey CS, Robinson KA, Pellicore JM, Newton CL, Deng JZ, Selnick HG, Lewis SD, Lucas BJ, Krueger JA, Miller-Stein C, White RB, Wong B, McMasters DR, Wallace AA, Lynch JJ Jr, Yan Y, Chen Z, Kuo L, Gardell SJ, Shafer JA, Vacca JP, and Lyle TA

Subjects

Hydrogen Bonding, Models, Molecular, Molecular Mimicry, Antithrombins chemistry, Pyrimidines chemistry

Abstract

In this study, we have demonstrated that the critical hydrogen bonding motif of the established 3-aminopyrazinone thrombin inhibitors can be effectively mimicked by a 2-aminopyridine N-oxide. As this peptidomimetic core is more resistant toward oxidative metabolism, it also overcomes the metabolic liability associated with the pyrazinones. An optimization study of the P(1) benzylamide delivered the potent thrombin inhibitor 21 (K(i) = 3.2 nM, 2xaPTT = 360 nM), which exhibited good plasma levels and half-life after oral dosing in the dog (C(max) = 2.6 microM, t(1/2) = 4.5 h).

Published

2005

16. 9-hydroxyazafluorenes and their use in thrombin inhibitors.

Author

Stauffer KJ, Williams PD, Selnick HG, Nantermet PG, Newton CL, Homnick CF, Zrada MM, Lewis SD, Lucas BJ, Krueger JA, Pietrak BL, Lyle EA, Singh R, Miller-Stein C, White RB, Wong B, Wallace AA, Sitko GR, Cook JJ, Holahan MA, Stranieri-Michener M, Leonard YM, Lynch JJ Jr, McMasters DR, and Yan Y

Subjects

Administration, Oral, Animals, Biological Availability, Blood Proteins metabolism, Crystallography, X-Ray, Dogs, Fluorenes chemistry, Fluorenes pharmacology, Half-Life, Humans, In Vitro Techniques, Macaca mulatta, Male, Microsomes, Liver metabolism, Models, Molecular, Proline chemistry, Proline pharmacology, Protein Binding, Rats, Rats, Sprague-Dawley, Stereoisomerism, Structure-Activity Relationship, Fluorenes chemical synthesis, Proline analogs & derivatives, Proline chemical synthesis, Thrombin antagonists & inhibitors

Abstract

Optimization of a previously reported thrombin inhibitor, 9-hydroxy-9-fluorenylcarbonyl-l-prolyl-trans-4-aminocyclohexylmethylamide (1), by replacing the aminocyclohexyl P1 group provided a new lead structure, 9-hydroxy-9-fluorenylcarbonyl-l-prolyl-2-aminomethyl-5-chlorobenzylamide (2), with improved potency (K(i) = 0.49 nM for human thrombin, 2x APTT = 0.37 microM in human plasma) and pharmacokinetic properties (F = 39%, iv T(1/2) = 13 h in dogs). An effective strategy for reducing plasma protein binding of 2 and improving efficacy in an in vivo thrombosis model in rats was to replace the lipophilic fluorenyl group in P3 with an azafluorenyl group. Systematic investigation of all possible azafluorenyl P3 isomers and azafluorenyl-N-oxide analogues of 2 led to the identification of an optimal compound, 3-aza-9-hydroxyfluoren-9(R)-ylcarbonyl-l-prolyl-2-aminomethyl-5-chlorobenzylamide (19b), with high potency (K(i) = 0.40 nM, 2x APTT = 0.18 microM), excellent pharmacokinetic properties (F = 55%, T(1/2) = 14 h in dogs), and complete efficacy in the in vivo thrombosis model in rats (inhibition of FeCl(3)-induced vessel occlusions in six of six rats receiving an intravenous infusion of 10 microg/kg/min of 19b). The stereochemistry of the azafluorenyl group in 19b was determined by X-ray crystallographic analysis of its N-oxide derivative (23b) bound in the active site of human thrombin.

Published

2005

17. Discovery and evaluation of potent P1 aryl heterocycle-based thrombin inhibitors.

Author

Young MB, Barrow JC, Glass KL, Lundell GF, Newton CL, Pellicore JM, Rittle KE, Selnick HG, Stauffer KJ, Vacca JP, Williams PD, Bohn D, Clayton FC, Cook JJ, Krueger JA, Kuo LC, Lewis SD, Lucas BJ, McMasters DR, Miller-Stein C, Pietrak BL, Wallace AA, White RB, Wong B, Yan Y, and Nantermet PG

Subjects

Benzylamines chemical synthesis, Benzylamines chemistry, Binding Sites, Heterocyclic Compounds chemistry, Models, Molecular, Pyrazines chemical synthesis, Pyrazines chemistry, Pyridines chemical synthesis, Pyridines chemistry, Structure-Activity Relationship, Tetrazoles chemical synthesis, Tetrazoles chemistry, Thiadiazoles chemical synthesis, Thiadiazoles chemistry, Thrombin chemistry, Triazoles chemical synthesis, Triazoles chemistry, Heterocyclic Compounds chemical synthesis, Thrombin antagonists & inhibitors

Abstract

In an effort to discover potent, clinically useful thrombin inhibitors, a rapid analogue synthetic approach was used to explore the P(1) region. Various benzylamines were coupled to a pyridine/pyrazinone P(2)-P(3) template. One compound with an o-thiadiazole benzylic substitution was found to have a thrombin K(i) of 0.84 nM. A study of ortho-substituted five-membered-ring heterocycles was undertaken and subsequently demonstrated that the o-triazole and tetrazole rings were optimal. Combination of these potent P(1) aryl heterocycles with a variety of P(2)-P(3) groups produced a compound with an extraordinary thrombin inhibitory activity of 1.4 pM. It is hoped that this potency enhancement in P(1) will allow for more diversification in the P(2)-P(3) region to ultimately address additional pharmacological concerns.

Published

2004

18. Imidazole acetic acid TAFIa inhibitors: SAR studies centered around the basic P(1)(') group.

Author

Nantermet PG, Barrow JC, Lindsley SR, Young M, Mao SS, Carroll S, Bailey C, Bosserman M, Colussi D, McMasters DR, Vacca JP, and Selnick HG

Subjects

Enzyme Inhibitors chemistry, Imidazoles chemistry, Models, Molecular, Structure-Activity Relationship, Carboxypeptidase B2 antagonists & inhibitors, Enzyme Inhibitors pharmacology, Imidazoles pharmacology

Abstract

Structural modifications of the aminopyridine P(1)(') group of imidazole acetic acid based TAFIa inhibitors led to the discovery of the aminocyclopentyl analog 28, a 1 nM TAFIa inhibitor with CLT(50) functional activity of 14 nM but without selectivity against CPB. While not as active, aminobutyl derivative 27 provided an improved 6.7-fold selectivity for TAFIa versus CPB.

Published

2004

19. Synthesis and evaluation of imidazole acetic acid inhibitors of activated thrombin-activatable fibrinolysis inhibitor as novel antithrombotics.

Author

Barrow JC, Nantermet PG, Stauffer SR, Ngo PL, Steinbeiser MA, Mao SS, Carroll SS, Bailey C, Colussi D, Bosserman M, Burlein C, Cook JJ, Sitko G, Tiller PR, Miller-Stein CM, Rose M, McMasters DR, Vacca JP, and Selnick HG

Subjects

Acetates pharmacokinetics, Acetates pharmacology, Aminopyridines pharmacokinetics, Aminopyridines pharmacology, Animals, Binding Sites, Carboxypeptidase B2 chemistry, Dogs, Fibrinolytic Agents pharmacokinetics, Fibrinolytic Agents pharmacology, Humans, Imidazoles pharmacokinetics, Imidazoles pharmacology, In Vitro Techniques, Microsomes metabolism, Models, Molecular, Propionates pharmacokinetics, Propionates pharmacology, Protease Inhibitors pharmacokinetics, Protease Inhibitors pharmacology, Rats, Structure-Activity Relationship, Acetates chemical synthesis, Aminopyridines chemical synthesis, Carboxypeptidase B2 antagonists & inhibitors, Fibrinolytic Agents chemical synthesis, Imidazoles chemical synthesis, Propionates chemical synthesis, Protease Inhibitors chemical synthesis

Abstract

Thrombin-activatable fibrinolysis inhibitor (TAFI) is an important regulator of fibrinolysis, and inhibitors of this enzyme have potential use in antithrombotic and thrombolytic therapy. Appropriately substituted imidazole acetic acids such as 10j were found to be potent inhibitors of activated TAFI and selective versus the related carboxypeptidases CPA, CPN, and CPM but not CPB. Further, 10j accelerated clot lysis in vitro and was shown to be efficacious in a primate model of thrombosis.

Published

2003

20. 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

21. Design and synthesis of potent and selective macrocyclic thrombin inhibitors.

Author

Nantermet PG, Barrow JC, Newton CL, Pellicore JM, Young M, Lewis SD, Lucas BJ, Krueger JA, McMasters DR, Yan Y, Kuo LC, Vacca JP, and Selnick HG

Subjects

Antithrombins pharmacology, Binding Sites, Crystallography, X-Ray, Drug Design, Models, Molecular, Proline chemistry, Pyrazines chemistry, Structure-Activity Relationship, Thrombin chemistry, Trypsin chemistry, Antithrombins chemical synthesis

Abstract

A series of potent and selective proline- and pyrazinone-based macrocyclic thrombin inhibitors is described. Detailed SAR studies led to the incorporation of specific functional groups in the tether that enhanced functional activity against thrombin and provided exquisite selectivity against trypsin and tPA. X-ray crystallography and molecular modeling studies revealed the inhibitor-enzyme interactions responsible for this selectivity.

Published

2003

22. Pharmacokinetic optimization of 3-amino-6-chloropyrazinone acetamide thrombin inhibitors. Implementation of P3 pyridine N-oxides to deliver an orally bioavailable series containing P1 N-benzylamides.

Author

Burgey CS, Robinson KA, Lyle TA, Nantermet PG, Selnick HG, Isaacs RC, Lewis SD, Lucas BJ, Krueger JA, Singh R, Miller-Stein C, White RB, Wong B, Lyle EA, Stranieri MT, Cook JJ, McMasters DR, Pellicore JM, Pal S, Wallace AA, Clayton FC, Bohn D, Welsh DC, Lynch JJ Jr, Yan Y, Chen Z, Kuo L, Gardell SJ, Shafer JA, and Vacca JP

Subjects

Animals, Biological Availability, Chemical Phenomena, Chemistry, Physical, Crystallography, X-Ray, Dogs, Half-Life, Humans, In Vitro Techniques, Injections, Intravenous, Macaca mulatta, Microsomes, Liver metabolism, Models, Molecular, Oxides chemistry, Rats, Solubility, Structure-Activity Relationship, Thrombosis chemically induced, Thrombosis drug therapy, Acetamides chemical synthesis, Acetamides pharmacology, Pyrazines chemical synthesis, Pyrazines pharmacology, Pyridines chemistry, Thrombin antagonists & inhibitors

Abstract

In this manuscript we demonstrate that a modification principally directed toward the improvement of the aqueous solubility (i.e., introduction a P3 pyridine N-oxide) of the previous lead compound afforded a new series of potent orally bioavailable P1 N-benzylamide thrombin inhibitors. An expedited investigation of the P1 SAR with respect to oral bioavailability, plasma half-life, and human liver microsome stability revealed 5 as the best candidate for advanced evaluation.

Published

2003

23. Non-peptidic small-molecule antagonists of the human platelet thrombin receptor PAR-1.

Author

Selnick HG, Barrow JC, Nantermet PG, and Connolly TM

Subjects

Blood Platelets drug effects, Humans, Inhibitory Concentration 50, Isoxazoles chemistry, Platelet Aggregation Inhibitors chemistry, Platelet Aggregation Inhibitors pharmacology, Structure-Activity Relationship, Urea chemistry, Isoxazoles pharmacology, Receptor, PAR-1 antagonists & inhibitors, Urea analogs & derivatives, Urea pharmacology

Abstract

The thrombin receptor on human platelets is the first member identified of a new family of G-protein coupled receptors referred to as protease activated receptors (PARs). These receptors are activated by a unique mechanism involving proteolytic cleavage of a portion of the extracellular domain to generate a new N-terminus which then acts as a tethered or intramolecular ligand (agonist) for the receptor. The hexapeptide SFLLRN-NH2 comprising the new N-terminus is referred to as the Thrombin Receptor Activating Peptide, or "TRAP" Thrombin is the most potent agonist for platelet aggregation and selective blockade of the intramolecular activation step without effecting the proteolytic activity of thrombin should result in moderation of platelet activation and aggregation without interfering with the other coagulation cascade effects of thrombin. Screening of combinatorial libraries identified a novel, non-peptide PAR-1 thrombin receptor antagonist. Examination of structure-activity relationships revealed that portions of the molecule could be replaced resulting in simpler molecules of lower molecular weight that were at the same time more potent. Molecules in this series were effective antagonists of TRAP-stimulated platelet activation, but had limited activity when thrombin was the agonist. Additional directed screening and subsequent lead refinement resulted in a second series of isoxazole based compounds. Some of the resultant molecules were potent PAR-1 antagonists that were effective against both TRAP- and thrombin-stimulated receptor activation. These compounds do not inhibit the proteolytic effects of thrombin but rather interfere with the intramolecular binding of the tethered ligand (SFLLRN) to the transmembrane portion of the thrombin receptor. They represent promising leads for future explorations of antithrombotic activity of thrombin receptor antagonists.

Published

2003

24. Discovery of a nonpeptidic small molecule antagonist of the human platelet thrombin receptor (PAR-1).

Author

Nantermet PG, Barrow JC, Lundell GF, Pellicore JM, Rittle KE, Young M, Freidinger RM, Connolly TM, Condra C, Karczewski J, Bednar RA, Gaul SL, Gould RJ, Prendergast K, and Selnick HG

Subjects

Blood Platelets drug effects, Drug Design, Humans, In Vitro Techniques, Indicators and Reagents, Peptide Fragments antagonists & inhibitors, Peptide Fragments pharmacology, Piperidines chemical synthesis, Piperidines chemistry, Platelet Activation drug effects, Platelet Aggregation drug effects, Platelet Aggregation Inhibitors chemical synthesis, Platelet Aggregation Inhibitors pharmacology, Receptor, PAR-1, Structure-Activity Relationship, Thrombin antagonists & inhibitors, Azepines chemical synthesis, Azepines pharmacology, Blood Platelets metabolism, Isoxazoles chemical synthesis, Isoxazoles pharmacology, Receptors, Thrombin antagonists & inhibitors

Abstract

The synthesis and biological evaluation of a series of nonpeptidic small molecule antagonists of the human platelet thrombin receptor (PAR-1) are described. Optimization of the 5-amino-3-arylisoxazole lead resulted in an approximate 100-fold increase in potency. The most potent of these compounds (54) inhibits platelet activation with IC(50)s of 90 nM against the thrombin receptor agonist peptide (TRAP) and 510 nM against thrombin as the agonist. Further, antagonist 54 fully blocks platelet aggregation stimulated by 1 nM thrombin for 10 min.

Published

2002

25. Discovery and initial structure-activity relationships of trisubstituted ureas as thrombin receptor (PAR-1) antagonists.

Author

Barrow JC, Nantermet PG, Selnick HG, Glass KL, Ngo PL, Young MB, Pellicore JM, Breslin MJ, Hutchinson JH, Freidinger RM, Condra C, Karczewski J, Bednar RA, Gaul SL, Stern A, Gould R, and Connolly TM

Subjects

Platelet Activation drug effects, Receptor, PAR-1, Structure-Activity Relationship, Urea chemistry, Receptors, Thrombin antagonists & inhibitors, Urea pharmacology

Abstract

Thrombin is the most potent agonist of platelet activation, and its effects are predominantly mediated by platelet thrombin receptors. Therefore, antagonists of the thrombin receptor have potential utility for the treatment of thrombotic disorders. Screening of combinatorial libraries revealed 2 to be a potent antagonist of the thrombin receptor. Modifications of this structure produced 11k, which inhibits thrombin receptor stimulated secretion and aggregation of platelets.

Published

2001

26. Selective alpha1a adrenergic receptor antagonists based on 4-aryl-3,4-dihydropyridine-2-ones.

Author

Nantermet PG, Barrow JC, Selnick HG, Homnick CF, Freidinger RM, Chang RS, O'Malley SS, Reiss DR, Broten TP, Ransom RW, Pettibone DJ, Olah T, and Forray C

Subjects

Adrenergic alpha-Antagonists chemistry, Animals, Dihydropyridines chemistry, Rats, Adrenergic alpha-1 Receptor Antagonists, Adrenergic alpha-Antagonists pharmacology, Dihydropyridines pharmacology

Abstract

A series of alpha1a receptor antagonists derived from a 4-aryl-3,4-dihydropyridine-2-one heterocycle is disclosed. Potency in the low nanomolar to picomolar range along with high selectivity was obtained. In vivo efficacy in a prostate contraction model in rats was observed with a few derivatives.

Published

2000

27. In vitro and in vivo evaluation of dihydropyrimidinone C-5 amides as potent and selective alpha(1A) receptor antagonists for the treatment of benign prostatic hyperplasia.

Author

Barrow JC, Nantermet PG, Selnick HG, Glass KL, Rittle KE, Gilbert KF, Steele TG, Homnick CF, Freidinger RM, Ransom RW, Kling P, Reiss D, Broten TP, Schorn TW, Chang RS, O'Malley SS, Olah TV, Ellis JD, Barrish A, Kassahun K, Leppert P, Nagarathnam D, and Forray C

Subjects

Adrenergic alpha-Antagonists chemistry, Adrenergic alpha-Antagonists pharmacokinetics, Adrenergic alpha-Antagonists pharmacology, Animals, Biological Availability, Caco-2 Cells, Crystallography, X-Ray, Dogs, Humans, Male, Prostatic Hyperplasia drug therapy, Pyrimidinones chemistry, Pyrimidinones metabolism, Pyrimidinones pharmacology, Radioligand Assay, Rats, Rats, Sprague-Dawley, Receptors, Adrenergic, alpha-1 metabolism, Structure-Activity Relationship, Adrenergic alpha-Antagonists chemical synthesis, Pyrimidinones chemical synthesis, Receptors, Adrenergic, alpha-1 drug effects

Abstract

alpha(1) Adrenergic receptors mediate both vascular and lower urinary tract tone, and alpha(1) receptor antagonists such as terazosin (1b) are used to treat both hypertension and benign prostatic hyperplasia (BPH). Recently, three different subtypes of this receptor have been identified, with the alpha(1A) receptor being most prevalent in lower urinary tract tissue. This paper explores 4-aryldihydropyrimidinones attached to an aminopropyl-4-arylpiperidine via a C-5 amide as selective alpha(1A) receptor subtype antagonists. In receptor binding assays, these types of compounds generally display K(i) values for the alpha(1a) receptor subtype <1 nM while being greater than 100-fold selective versus the alpha(1b) and alpha(1d) receptor subtypes. Many of these compounds were also evaluated in vivo and found to be more potent than terazosin in both a rat model of prostate tone and a dog model of intra-urethral pressure without significantly affecting blood pressure. While many of the compounds tested displayed poor pharmacokinetics, compound 48 was found to have adequate bioavailability (>20%) and half-life (>6 h) in both rats and dogs. Due to its selectivity for the alpha(1a) over the alpha(1b) and alpha(1d) receptors as well as its favorable pharmacokinetic profile, 48 has the potential to relieve the symptoms of BPH without eliciting effects on the cardiovascular system.

Published

2000

28. Total synthesis of taxol.

Author

Nicolaou KC, Yang Z, Liu JJ, Ueno H, Nantermet PG, Guy RK, Claiborne CF, Renaud J, Couladouros EA, and Paulvannan K

Subjects

Models, Molecular, Molecular Conformation, Paclitaxel chemistry, Stereoisomerism, Paclitaxel chemical synthesis

Abstract

Taxol, a substance originally isolated from the Pacific yew tree (Taxus brevifolia) more than two decades ago, has recently been approved for the clinical treatment of cancer patients. Hailed as having provided one of the most significant advances in cancer therapy, this molecule exerts its anticancer activity by inhibiting mitosis through enhancement of the polymerization of tubulin and consequent stabilization of microtubules. The scarcity of taxol and the ecological impact of harvesting it have prompted extension searches for alternative sources including semisynthesis, cellular culture production and chemical synthesis. The latter has been attempted for almost two decades, but these attempts have been thwarted by the magnitude of the synthetic challenge. Here we report the total synthesis of taxol by a convergent strategy, which opens a chemical pathway for the production of both the natural product itself and a variety of designed taxoids.

Published

1994