Your search keyword '"Robert D. Groneberg"' showing total 13 results

1. Discovery of 7-Tetrahydropyran-2-yl Chromans: β-Site Amyloid Precursor Protein Cleaving Enzyme 1 (BACE1) Inhibitors That Reduce Amyloid β-Protein (Aβ) in the Central Nervous System

Author

Darin Smith, Guy Vigers, Sumeet Rana, Michael Burkard, April Cox, Robert D. Groneberg, Ryan J. Watts, Robert Kirk Delisle, Tony Pisal Tang, Andrew T. Metcalf, Kelly Regal, Susan P. Rhodes, Mary K. Geck Do, Karin D. Brown, Joseph P. Lyssikatos, Douglas Mccord Sammond, Matthew Volgraf, Albion D. Wright, Gunawardana Indrani W, Kimberly Scearce-Levie, Jennifer N. Otten, Allen A. Thomas, Michael Siu, Hans E. Purkey, Kevin W. Hunt, Xingrong Liu, and Darrin Dutcher

Subjects

Male, Models, Molecular, Stereochemistry, Guinea Pigs, Cathepsin D, Stereoisomerism, CHO Cells, Crystallography, X-Ray, Rats, Sprague-Dawley, Mice, Structure-Activity Relationship, chemistry.chemical_compound, Cricetulus, Cell Line, Tumor, Cricetinae, Drug Discovery, Amyloid precursor protein, Animals, Aspartic Acid Endopeptidases, Humans, Moiety, Structure–activity relationship, Spiro Compounds, Chromans, Guanidine, Pyrans, chemistry.chemical_classification, Amyloid beta-Peptides, biology, Brain, Rats, Macaca fascicularis, HEK293 Cells, Enzyme, chemistry, Biochemistry, biology.protein, Molecular Medicine, Efflux, Amyloid Precursor Protein Secretases

Abstract

In an attempt to increase selectivity vs Cathepsin D (CatD) in our BACE1 program, a series of 1,3,4,4a,10,10a-hexahydropyrano[4,3-b]chromene analogues was developed. Three different Asp-binding moieties were examined: spirocyclic acyl guanidines, aminooxazolines, and aminothiazolines in order to modulate potency, selectivity, efflux, and permeability. Using structure-based design, substitutions to improve binding to both the S3 and S2' sites of BACE1 were explored. An acyl guanidine moiety provided the most potent analogues. These compounds demonstrated 10-420 fold selectivity for BACE1 vs CatD, and were highly potent in a cell assay measuring Aβ1-40 production (5-99 nM). They also suffered from high efflux. Despite this undesirable property, two of the acyl guanidines achieved free brain concentrations (Cfree,brain) in a guinea pig PD model sufficient to cover their cell IC50s. Moreover, a significant reduction of Aβ1-40 in guinea pig, rat, and cyno CSF (58%, 53%, and 63%, respectively) was observed for compound 62.

Published

2014

2. Synthesis, structure–property relationships and pharmacokinetic evaluation of ethyl 6-aminonicotinate sulfonylureas as antagonists of the P2Y12 receptor

Author

Michael O'sullivan, Kay Brickmann, Peter Bach, Jonas Boström, Darren Martin Harvey, Robert D. Groneberg, J.J.J. van Giezen, and Fredrik Zetterberg

Subjects

Pharmacology, Sulfonyl, chemistry.chemical_classification, Stereochemistry, Organic Chemistry, General Medicine, Solvent, Piperazine, chemistry.chemical_compound, chemistry, Drug Discovery, Urea, Potency, Chemical stability, Solubility, IC50, Nuclear chemistry

Abstract

The present paper describes the development of a new series of P2Y12 receptor antagonists based on our previously reported piperazinyl urea series 1 (IC50 binding affinity = 0.33 μM, aq solubility

Published

2013

3. Tetrazole and ester substituted tetrahydoquinoxalines as potent cholesteryl ester transfer protein inhibitors

Author

Michael O'sullivan, Robert D. Groneberg, Mark D. Drew, Andrew Allen, C. Todd Eary, Vivienne Marsh, Devan Balachari, David A. Mareska, Ellen R. Laird, James F. Blake, Zachary Jones, and Laurence E. Burgess

Subjects

Stereochemistry, Chemistry, Pharmaceutical, Clinical Biochemistry, Molecular Conformation, Tetrazoles, Pharmaceutical Science, Biochemistry, Chemical synthesis, Inhibitory Concentration 50, Structure-Activity Relationship, chemistry.chemical_compound, High-density lipoprotein, In vivo, Quinoxalines, Drug Discovery, Cholesterylester transfer protein, Animals, Humans, Tetrazole, Molecular Biology, chemistry.chemical_classification, biology, Cholesterol, Cholesterol, HDL, Organic Chemistry, Esters, Stereoisomerism, Hydrogen-Ion Concentration, Cholesterol Ester Transfer Proteins, Rats, chemistry, Drug Design, biology.protein, Molecular Medicine, lipids (amino acids, peptides, and proteins), Glycoprotein, Lipoprotein

Abstract

Cholesteryl ester transfer protein is a plasma glycoprotein that transfers cholesterol ester between lipoprotein particles. Inhibition of this protein, in vitro and in vivo, produces an increase in plasma high density lipoprotein cholesterol (HDL-C). This communication will describe the SAR and synthesis of a series of substituted tetrahydroquinoxaline CETP inhibitors from early mu lead to advanced enantiomerically pure analogs.

Published

2007

4. Potent Nonpeptide Antagonists of the Bradykinin B1 Receptor: Structure−Activity Relationship Studies with Novel Diaminochroman Carboxamides

Author

Burgess Laurence E, Leyla Arik, Chester Chenguang Yuan, Nianhe Han, Randall W. Hungate, Derin C. D'amico, David A. Mareska, Feng-Yin Hsieh, Eileen Johnson, Hong Sun, Qingyian Liu, Barton H. Manning, Bobby Riahi, Christopher H. Fotsch, Gloria Biddlecome, Mark H. Norman, Augustus Kamassah, Ming Huang, Richard Loeloff, Gondi N. Kumar, Andras Toro, Jian J. Chen, Jason Brooks Human, Hideo Suzuki, Robert D. Groneberg, Benny C. Askew, Aiwen Li, Gordon Ng, James Zhan, Kaustav Biswas, Dianna Lester-Zeiner, Hong Dong, and David E. Clarke

Subjects

Male, medicine.drug_class, Pain, Bradykinin, Blood Pressure, Carboxamide, CHO Cells, In Vitro Techniques, Receptor, Bradykinin B1, Rats, Sprague-Dawley, Structure-Activity Relationship, chemistry.chemical_compound, Cricetulus, In vivo, Cricetinae, Microsomes, Drug Discovery, medicine, Animals, Humans, Moiety, Structure–activity relationship, Benzopyrans, Chromans, Receptor, Inflammation, Analgesics, Sulfonamides, Stereoisomerism, Amides, In vitro, Rats, Bradykinin B1 Receptor Antagonists, chemistry, Biochemistry, Hyperalgesia, Molecular Medicine, Calcium, Rabbits, medicine.symptom

Abstract

The bradykinin B1 receptor is induced following tissue injury and/or inflammation. Antagonists of this receptor have been studied as promising candidates for treatment of chronic pain. We have identified aryl sulfonamides containing a chiral chroman diamine moiety that are potent antagonists of the human B1 receptor. Our previously communicated lead, compound 2, served as a proof-of-concept molecule, but suffered from poor pharmacokinetic properties. With guidance from metabolic profiling, we performed structure-activity relationship studies and have identified potent analogs of 2. Variation of the sulfonamide moiety revealed a preference for 3- and 3,4-disubstituted aryl sulfonamides, while bulky secondary and tertiary amines were preferred at the benzylic amine position for potency at the B1 receptor. Modifying the beta-amino acid core of the molecule lead to the discovery of highly potent compounds with improved in vitro pharmacokinetic properties. The most potent analog at the human receptor, compound 38, was also active in a rabbit B1 receptor cellular assay. Furthermore, compound 38 displayed in vivo activity in two rabbit models, a pharmacodynamic model with a blood pressure readout and an efficacy model of inflammatory pain.

Published

2007

5. 8-Tetrahydropyran-2-yl chromans: highly selective beta-site amyloid precursor protein cleaving enzyme 1 (BACE1) inhibitors

Author

Jiangpeng Liao, Kelly Regal, Mary K. Geck Do, Kevin W. Hunt, Robert Kirk Delisle, Karin D. Brown, Susan P. Rhodes, Ryan J. Watts, Guy Vigers, Sumeet Rana, Darrin Dutcher, Brad Newhouse, Jennifer N. Otten, Michael Siu, Allen A. Thomas, Darin Smith, April Cox, Michael Burkard, Joseph P. Lyssikatos, Robert D. Groneberg, Xingrong Liu, Hans E. Purkey, Kimberly Scearce-Levie, and Albion D. Wright

Subjects

Male, Models, Molecular, Stereochemistry, Cathepsin D, chemistry.chemical_compound, Inhibitory Concentration 50, Mice, Structure-Activity Relationship, Drug Discovery, Amyloid precursor protein, Potency, Animals, Aspartic Acid Endopeptidases, Humans, Protease Inhibitors, Spiro Compounds, Chromans, chemistry.chemical_classification, biology, Brain, Stereoisomerism, Tetrahydropyran, Rats, Enzyme, HEK293 Cells, chemistry, biology.protein, Molecular Medicine, Efflux, Amyloid Precursor Protein Secretases, Selectivity, Methyl group

Abstract

A series of 2,3,4,4a,10,10a-hexahydropyrano[3,2-b]chromene analogs was developed that demonstrated high selectivity (>2000-fold) for BACE1 vs Cathepsin D (CatD). Three different Asp-binding moieties were examined: spirocyclic acyl guanidines, aminooxazolines, and aminothiazolines in order to modulate potency, selectivity, efflux, and permeability. Guided by structure based design, changes to P2′ and P3 moieties were explored. A conformationally restricted P2′ methyl group provided inhibitors with excellent cell potency (37–137 nM) and selectivity (435 to >2000-fold) for BACE1 vs CatD. These efforts lead to compound 59, which demonstrated a 69% reduction in rat CSF Aβ1–40 at 60 mg/kg (PO).

Published

2014

6. Spirocyclic β-site amyloid precursor protein cleaving enzyme 1 (BACE1) inhibitors: from hit to lowering of cerebrospinal fluid (CSF) amyloid β in a higher species

Author

Andrew T. Metcalf, Allison Marlow, Robert Kirk Delisle, Ryan J. Watts, April Cox, Christopher T. Clark, Kelly Regal, Douglas Mccord Sammond, Kevin W. Hunt, Mary K. Geck Do, Guy Vigers, Sumeet Rana, James P. Rizzi, Tony Pisal Tang, Allen A. Thomas, Nicholas C. Kallan, Xingrong Liu, Adam W. Cook, Michael Siu, Darin Smith, Hans E. Purkey, Gunawardana Indrani W, Darrin Dutcher, Joseph P. Lyssikatos, Michael Burkard, and Robert D. Groneberg

Subjects

Male, Amyloid beta, Guinea Pigs, Cathepsin D, Peptide, Structure-Activity Relationship, Cerebrospinal fluid, In vivo, mental disorders, Drug Discovery, medicine, Amyloid precursor protein, Animals, Aspartic Acid Endopeptidases, Humans, Protease Inhibitors, Spiro Compounds, Chromans, chemistry.chemical_classification, Amyloid beta-Peptides, biology, Chemistry, Hydantoins, Neurodegeneration, P3 peptide, medicine.disease, Rats, HEK293 Cells, Biochemistry, Blood-Brain Barrier, biology.protein, Molecular Medicine, Amyloid Precursor Protein Secretases

Abstract

A hallmark of Alzheimer's disease is the brain deposition of amyloid beta (Aβ), a peptide of 36-43 amino acids that is likely a primary driver of neurodegeneration. Aβ is produced by the sequential cleavage of APP by BACE1 and γ-secretase; therefore, inhibition of BACE1 represents an attractive therapeutic target to slow or prevent Alzheimer's disease. Herein we describe BACE1 inhibitors with limited molecular flexibility and molecular weight that decrease CSF Aβ in vivo, despite efflux. Starting with spirocycle 1a, we explore structure-activity relationships of core changes, P3 moieties, and Asp binding functional groups in order to optimize BACE1 affinity, cathepsin D selectivity, and blood-brain barrier (BBB) penetration. Using wild type guinea pig and rat, we demonstrate a PK/PD relationship between free drug concentrations in the brain and CSF Aβ lowering. Optimization of brain exposure led to the discovery of (R)-50 which reduced CSF Aβ in rodents and in monkey.

Published

2013

7. Synthesis, structure-property relationships and pharmacokinetic evaluation of ethyl 6-aminonicotinate sulfonylureas as antagonists of the P2Y₁₂ receptor

Author

Peter, Bach, Jonas, Boström, Kay, Brickmann, J J J, van Giezen, Robert D, Groneberg, Darren M, Harvey, Michael, O'Sullivan, and Fredrik, Zetterberg

Subjects

Structure-Activity Relationship, Molecular Structure, Nicotinic Acids, Purinergic P2Y Receptor Antagonists, Animals, Urea, Receptors, Purinergic P2Y12, Rats

Abstract

The present paper describes the development of a new series of P2Y12 receptor antagonists based on our previously reported piperazinyl urea series 1 (IC50 binding affinity = 0.33 μM, aq solubility0.1 μM, microsomal CLint (HLM) ≥300 μM/min/mg). By replacement of the urea functionality with a sulfonylurea group we observed increased affinity along with improved stability and solubility as exemplified by 47 (IC50 binding affinity = 0.042 μM, aq solubility = 90 μM, microsomal CLint (HLM) = 70 μM/min/mg). Further improvements in affinity and metabolic stability were achieved by replacing the central piperazine ring with a 3-aminoazetidine as exemplified by 3 (IC50 binding affinity = 0.0062 μM, aq solubility = 83 μM, microsomal CLint (HLM) = 28 μM/min/mg). The improved affinity observed in the in vitro binding assay also translated to the potency observed in the WPA aggregation assay (47: 19 nM and 3: 9.5 nM) and the observed in vitro ADME properties translates to the in vivo PK properties observed in rat. In addition, we found that the chemical stability of the sulfonylureas during prolonged storage in solution was related to the sulfonyl urea linker and depended on the type of solvent and the substitution pattern of the sulfonyl urea functionality.

Published

2012

8. Effects Of ARRY-797, A P38 Map Kinase Inhibitor, In Animal Models Of Pulmonary Inflammation Via Oral, Intratracheal Or Aerosol Delivery

Author

Albion D. Wright, Mark C. Munson, Thomas Pope, Stefan Gross, Pheneger Jed, Robert D. Groneberg, Laurence E. Burgess, Patrice Lee, and Corey Custer

Subjects

Aerosol delivery, biology, business.industry, p38 mitogen-activated protein kinases, Mitogen-activated protein kinase, Pulmonary inflammation, Immunology, biology.protein, Medicine, Pharmacology, business

Published

2011

9. Total synthesis of calicheamicin .gamma.1I. 1. Synthesis of the oligosaccharide fragment

Author

Robert D. Groneberg, Wilhelm Stahl, Adrian L. Smith, Erwin P. Schreiner, T. Miyazaki, N. A. Stylianides, Kyriacos C. Nicolaou, Yoshiharu Iwabuchi, Toshio Suzuki, and T. J. Schulze

Subjects

chemistry.chemical_classification, Allylic rearrangement, Natural product, Stereochemistry, Total synthesis, General Chemistry, Sigmatropic reaction, Oligosaccharide, Biochemistry, Combinatorial chemistry, Catalysis, chemistry.chemical_compound, Colloid and Surface Chemistry, chemistry, Calicheamicin, Stereoselectivity, Calicheamicin Gamma 1I

Abstract

The first total synthesis of the calicheamicin γ 1 I oligosaccharide fragment in the form of its methyl glycoside (62) has been achieved. The synthetic challenge of the B-ring was recognized and studied initially, resulting in a novel and unique solution to the stereochemical problems posed involving a [3,3]-sigmatropic rearrangement of an allylic thionoimidazolide (111). This chemistry was initially worked out on a model for the ABC-ring system (47) and then successfully applied to the real system. The success of this synthesis has enabled the completion of the first synthesis of the natural product itself, calicheamicin γ 1 I (I), as will be described in the following papers in this issue

Published

1993

10. Identification of a nonpeptidic and conformationally restricted bradykinin B1 receptor antagonist with anti-inflammatory activity

Author

David A. Mareska, Dianna Lester-Zeiner, Randall W. Hungate, Eileen Johnson, Toshi Aya, Leyla Arik, Bobby Riahi, Mark H. Norman, Augustus Kamassah, Jian J. Chen, Gloria Biddlecome, Judy Wang, Christopher H. Fotsch, Paul J. Reider, Jason Brooks Human, Benny C. Askew, Derin C. D'amico, Andras Toro, Burgess Laurence E, Carlo van Staden, Vellarkad N. Viswanadhan, Laird Ellen, Darren Martin Harvey, David E. Clarke, Gordon Ng, James Zhan, Kaustav Biswas, Christopher A. Willoughby, Hideo Suzuki, and Robert D. Groneberg

Subjects

Models, Molecular, Stereochemistry, medicine.drug_class, Entropy, Molecular Conformation, Bradykinin, Inflammation, CHO Cells, Pharmacology, In Vitro Techniques, Crystallography, X-Ray, Capillary Permeability, chemistry.chemical_compound, Structure-Activity Relationship, Cricetulus, Species Specificity, Cricetinae, Drug Discovery, Chlorocebus aethiops, medicine, Animals, Humans, Chromans, Pleurisy, Lagomorpha, biology, Anti-Inflammatory Agents, Non-Steroidal, Antagonist, Biological activity, Stereoisomerism, Receptor antagonist, biology.organism_classification, In vitro, Extravasation, Rats, Bradykinin B1 Receptor Antagonists, chemistry, Molecular Medicine, Rabbits, medicine.symptom

Abstract

We report the discovery of chroman 28, a potent and selective antagonist of human, nonhuman primate, rat, and rabbit bradykinin B1 receptors (0.4-17 nM). At 90 mg/kg s.c., 28 decreased plasma extravasation in two rodent models of inflammation. A novel method to calculate entropy is introduced and ascribed approximately 30% of the gained affinity between "flexible" 4 (Ki = 132 nM) and "rigid" 28 (Ki = 0.77 nM) to decreased conformational entropy.

Published

2007

11. A new class of bradykinin 1 receptor antagonists containing the piperidine acetic acid tetralin core

Author

David A. Mareska, Eileen Johnson, Christopher H. Fotsch, Dianna Lester-Zeiner, Qingyian Liu, Gloria Biddlecome, Gordon Ng, James Zhan, Kaustav Biswas, Nianhe Bruce Han, Yueh-Ju Judy Wang, Joe Zhu, Babak Riahi, Gondi N. Kumar, Kevin Yang, Robert D. Groneberg, Derin C. D'amico, Feng-Yin Hsieh, Jian Jeff Chen, Benny C. Askew, and Augustus Kamassah

Subjects

Tetrahydronaphthalenes, Stereochemistry, Clinical Biochemistry, Pharmaceutical Science, Bradykinin, Administration, Oral, Biological Availability, Inflammation, Pharmacology, Biochemistry, Chemical synthesis, chemistry.chemical_compound, Acetic acid, Inhibitory Concentration 50, Structure-Activity Relationship, Downregulation and upregulation, Piperidines, Drug Discovery, medicine, Animals, Receptor, Molecular Biology, Acetic Acid, Analgesics, Organic Chemistry, Anti-Inflammatory Agents, Non-Steroidal, Antagonist, Rats, Bradykinin B1 Receptor Antagonists, chemistry, Molecular Medicine, Piperidine, medicine.symptom

Abstract

The bradykinin 1 (B1) receptor is upregulated during times of inflammation and is important for maintaining inflamed and chronic pain states. Blocking this receptor has been shown to reverse and/or ameliorate pain and inflammation in animal models. In this report, we describe a new class of B1 receptor antagonists that contain the piperidine acetic acid tetralin core. A structure-activity relationship for these analogs is described in this paper. The most potent compounds from this class have IC50s20 nM in a B1 receptor functional assay. One of these compounds, 13g, shows modest oral bioavailability in rats.

Published

2005

12. Potent Nonpeptide Antagonists of the Bradykinin B1 Receptor:  Structure−Activity Relationship Studies with Novel Diaminochroman Carboxamides.

Author

Kaustav Biswas, Aiwen Li, Jian Jeffrey Chen, Derin C. D'Amico, Christopher Fotsch, Nianhe Han, Jason Human, Qingyian Liu, Mark H. Norman, Bobby Riahi, Chester Yuan, Hideo Suzuki, David A. Mareska, James Zhan, David E. Clarke, Andras Toro, Robert D. Groneberg, Laurence E. Burgess, Dianna Lester-Zeiner, and Gloria Biddlecome

Published

2007

13. Identification of a Nonpeptidic and Conformationally Restricted Bradykinin B1 Receptor Antagonist with Anti-Inflammatory Activity.

Author

Derin C. D'Amico, Toshi Aya, Jason Human, Christopher Fotsch, Jian Jeffrey Chen, Kaustav Biswas, Bobby Riahi, Mark H. Norman, Christopher A. Willoughby, Randall Hungate, Paul J. Reider, Gloria Biddlecome, Dianna Lester-Zeiner, Carlo Van Staden, Eileen Johnson, Augustus Kamassah, Leyla Arik, Judy Wang, Vellarkad N. Viswanadhan, and Robert D. Groneberg

Published

2007