Your search keyword '"John A. Lupisella"' showing total 9 results

1. Discovery of BMS-986235/LAR-1219: A Potent Formyl Peptide Receptor 2 (FPR2) Selective Agonist for the Prevention of Heart Failure

Author

John A. Lupisella, Kiyoshi Fujii, David A. Gordon, Mei-Yin Hsu, Toshikazu Yamaoka, Yasuchi Kohno, Kohei Ohata, Kosuke Tsuda, Kazuto Arakawa, Nancy L. Carson, Kazunori Fukuchi, Ruth R. Wexler, Francisco Villarreal, Ellen K. Kick, Junichi Ishiyama, Jacek Ostrowski, Shingo Matsushima, Hitomi Yamada, Yoshifumi Saito, Bruce R. Ito, Yoshikazu Asahina, Ricardo Garcia, and Nicholas R. Wurtz

Subjects

Agonist, medicine.drug_class, Neutrophils, Drug Evaluation, Preclinical, Inflammation, Pharmacology, 01 natural sciences, Formyl peptide receptor 2, Macrophage phagocytosis, 03 medical and health sciences, chemistry.chemical_compound, Mice, Structure-Activity Relationship, Phagocytosis, Drug Discovery, medicine, Animals, Humans, Cardiac structure, Receptors, Lipoxin, 030304 developmental biology, Heart Failure, 0303 health sciences, Chemistry, Chemotaxis, Macrophages, medicine.disease, Receptors, Formyl Peptide, Pyrrolidinones, 0104 chemical sciences, Neutrophil chemotaxis, 010404 medicinal & biomolecular chemistry, Disease Models, Animal, HEK293 Cells, Heart failure, Lactam, Microsomes, Liver, Molecular Medicine, medicine.symptom

Abstract

Formyl peptide receptor 2 (FPR2) agonists can stimulate resolution of inflammation and may have utility for treatment of diseases caused by chronic inflammation, including heart failure. We report the discovery of a potent and selective FPR2 agonist and its evaluation in a mouse heart failure model. A simple linear urea with moderate agonist activity served as the starting point for optimization. Introduction of a pyrrolidinone core accessed a rigid conformation that produced potent FPR2 and FPR1 agonists. Optimization of lactam substituents led to the discovery of the FPR2 selective agonist 13c, BMS-986235/LAR-1219. In cellular assays 13c inhibited neutrophil chemotaxis and stimulated macrophage phagocytosis, key end points to promote resolution of inflammation. Cardiac structure and functional improvements were observed in a mouse heart failure model following treatment with BMS-986235/LAR-1219.

Published

2020

2. Beneficial and Adverse Effects of an LXR Agonist on Human Lipid and Lipoprotein Metabolism and Circulating Neutrophils

Author

Lisa Salvador, Richard Martin, Raju Mohan, Philip Wastall, Zhaoqing Wang, John A. Lupisella, Kamelia Behnia, Paul G. Sleph, Todd G. Kirchgessner, Petia Shipkova, Gayani Fernando, Jane Zhang, Carol S. Ryan, Rongan Zhang, Shuyan Du, Tong Li, Harold Malone, Ellen K. Kick, Glenn H. Cantor, Jun Zhu, Yu Chen Barrett, Jacek Ostrowski, Long Yuan, Denise Grimm, Aiqing He, John S. Lee, Robert J.A. Frost, Mohit D. Gandhi, Ricardo Garcia, Robert J. Garmise, and Xiaoqin Liu

Subjects

Male, 0301 basic medicine, Apolipoprotein E, Apolipoprotein B, Neutrophils, Physiology, Leukocyte Count, chemistry.chemical_compound, 0302 clinical medicine, Cell Movement, Mononuclear Phagocyte System, ATP Binding Cassette Transporter, Subfamily G, Member 1, Liver X Receptors, biology, Reverse cholesterol transport, Imidazoles, Healthy Volunteers, 3. Good health, Cholesterol, Adipose Tissue, lipids (amino acids, peptides, and proteins), ATP Binding Cassette Transporter 1, Adult, Agonist, medicine.medical_specialty, Adolescent, medicine.drug_class, Lipoproteins, Hypercholesterolemia, Young Adult, 03 medical and health sciences, Therapeutic index, Internal medicine, medicine, Animals, Humans, RNA, Messenger, Liver X receptor, Molecular Biology, Triglycerides, Macrophages, Lipid metabolism, Cell Biology, Lipid Metabolism, Rats, Mice, Inbred C57BL, Macaca fascicularis, 030104 developmental biology, Endocrinology, chemistry, biology.protein, Hydroxymethylglutaryl-CoA Reductase Inhibitors, 030217 neurology & neurosurgery

Abstract

The development of LXR agonists for the treatment of coronary artery disease has been challenged by undesirable properties in animal models. Here we show the effects of an LXR agonist on lipid and lipoprotein metabolism and neutrophils in human subjects. BMS-852927, a novel LXRβ-selective compound, had favorable profiles in animal models with a wide therapeutic index in cynomolgus monkeys and mice. In healthy subjects and hypercholesterolemic patients, reverse cholesterol transport pathways were induced similarly to that in animal models. However, increased plasma and hepatic TG, plasma LDL-C, apoB, apoE, and CETP and decreased circulating neutrophils were also evident. Furthermore, similar increases in LDL-C were observed in normocholesterolemic subjects and statin-treated patients. The primate model markedly underestimated human lipogenic responses and did not predict human neutrophil effects. These studies demonstrate both beneficial and adverse LXR agonist clinical responses and emphasize the importance of further translational research in this area.

Published

2016

3. Discovery of Highly Potent Liver X Receptor β Agonists

Author

William C. Stevens, John A. Lupisella, Venkataiah Bollu, Richard Martin, Denise Grimm, Rangaraj Narayanan, Max H. Nanao, Ruth R. Wexler, Raju Mohan, Xiaoping Hou, Meriah Neissel Valente, Brant Clayton Boren, Grace Yan, James Smalley, Brett B. Busch, Jacek Ostrowski, Paul G. Sleph, Yinong Xie, Barry Brock, Ira G. Schulman, A. David Rodrigues, Artur Plonowski, Glenn H. Cantor, Michael Charles Nyman, Huiping Zhang, Lam Nguyen, Ellen K. Kick, Todd G. Kirchgessner, and Kamelia Behnia

Subjects

0301 basic medicine, Agonist, biology, medicine.drug_class, Organic Chemistry, Liver X receptor alpha, Pharmacology, Biochemistry, Blood proteins, Sulfone, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, ABCG1, chemistry, ABCA1, Drug Discovery, biology.protein, medicine, lipids (amino acids, peptides, and proteins), Liver X receptor, Whole blood

Abstract

Introducing a uniquely substituted phenyl sulfone into a series of biphenyl imidazole liver X receptor (LXR) agonists afforded a dramatic potency improvement for induction of ATP binding cassette transporters, ABCA1 and ABCG1, in human whole blood. The agonist series demonstrated robust LXRβ activity (>70%) with low partial LXRα agonist activity (

Published

2016

4. N-Aryl-oxazolidin-2-imine Muscle Selective Androgen Receptor Modulators Enhance Potency through Pharmacophore Reorientation

Author

Stanley R. Krystek, Donald Egan, John S. Sack, Joyce E. Kuhns, Alexandra A. Nirschl, Gary J. Grover, Rajasree Golla, John A. Lupisella, James A. Bryson, John D. Dimarco, Jack Z. Gougoutas, Ligaya M. Simpkins, Aberra Fura, Jacek Ostrowski, Yan Zou, Yi-Xin Li, Robert Zahler, Yongmi An, James C. Sutton, Kevin Kish, Viral Vyas, Lawrence G. Hamann, Ramakrishna Seethala, Paul G. Sleph, and Blake C. Beehler

Subjects

Male, Models, Molecular, Stereochemistry, Imine, Molecular Conformation, Crystallography, X-Ray, Substrate Specificity, chemistry.chemical_compound, Drug Discovery, Animals, Humans, Potency, Oxazoles, Chemistry, Muscles, Aryl, Prostate, Hydrogen-Ion Concentration, In vitro, Rats, Bioavailability, Androgen receptor, Selective androgen receptor modulator, Androgens, Molecular Medicine, Pharmacophore

Abstract

A novel selective androgen receptor modulator (SARM) scaffold was discovered as a byproduct obtained during synthesis of our earlier series of imidazolidin-2-ones. The resulting oxazolidin-2-imines are among the most potent SARMs known, with many analogues exhibiting sub-nM in vitro potency in binding and functional assays. Despite the potential for hydrolytic instability at gut pH, compounds of the present class showed good oral bioavailability and were highly active in a standard rodent pharmacological model.

Published

2009

5. 11β-hydroxysteroid dehydrogenase type 1 gene knockout attenuates atherosclerosis and in vivo foam cell formation in hyperlipidemic apoE⁻/⁻ mice

Author

Robert Langish, David A. Gordon, Wen-Pin Yang, Thomas Harrity, Carol S. Ryan, Mujing Yan, Jeffrey A. Robl, Bo Guan, Linda Watson, Nancy L. Carson, Aiqing He, George C. Psaltis, Joseph R. Taylor, Richard Yang, Rongan Zhang, Jian Chen, Petia Shipkova, Amy Truong, Peter S. Gargalovic, Samuel Hellings, Jacek Ostrowski, Debra Search, Ricardo Garcia, and John A. Lupisella

Subjects

Male, Anatomy and Physiology, Mouse, lcsh:Medicine, Blood Pressure, Dehydrogenase, Cardiovascular, Biochemistry, Mice, chemistry.chemical_compound, Endocrinology, 11β-hydroxysteroid dehydrogenase type 1, Molecular Cell Biology, Drug Discovery, 11-beta-Hydroxysteroid Dehydrogenase Type 1, Membrane Receptor Signaling, lcsh:Science, Ketocholesterols, Lipoprotein Receptors, Bone Marrow Transplantation, Oligonucleotide Array Sequence Analysis, Foam cell, Mice, Knockout, Hormone Synthesis, Multidisciplinary, biology, Reverse Transcriptase Polymerase Chain Reaction, Toll-Like Receptors, Animal Models, Hormone Receptor Signaling, Lipids, Cholesterol, Medicine, lipids (amino acids, peptides, and proteins), hormones, hormone substitutes, and hormone antagonists, Glucocorticoid, Research Article, Signal Transduction, medicine.drug, Drugs and Devices, medicine.medical_specialty, Drug Research and Development, Lipoproteins, Endocrine System, Cardiovascular Pharmacology, Model Organisms, Apolipoproteins E, Vascular Biology, In vivo, Internal medicine, medicine, Animals, Biology, Glucocorticoids, Gene knockout, Diabetic Endocrinology, Analysis of Variance, Endocrine Physiology, lcsh:R, Proteins, Diabetes Mellitus Type 2, Atherosclerosis, Hormones, chemistry, biology.protein, Diet, Atherogenic, lcsh:Q, Nuclear Receptor Signaling, Cortisone, Foam Cells

Abstract

BACKGROUND: Chronic glucocorticoid excess has been linked to increased atherosclerosis and general cardiovascular risk in humans. The enzyme 11β-hydroxysteroid dehydrogenase type 1 (11βHSD1) increases active glucocorticoid levels within tissues by catalyzing the conversion of cortisone to cortisol. Pharmacological inhibition of 11βHSD1 has been shown to reduce atherosclerosis in murine models. However, the cellular and molecular details for this effect have not been elucidated. METHODOLOGY/PRINCIPAL FINDINGS: To examine the role of 11βHSD1 in atherogenesis, 11βHSD1 knockout mice were created on the pro-atherogenic apoE⁻/⁻ background. Following 14 weeks of Western diet, aortic cholesterol levels were reduced 50% in 11βHSD1⁻/⁻/apoE⁻/⁻ mice vs. 11βHSD1⁺/⁺/apoE⁻/⁻ mice without changes in plasma cholesterol. Aortic 7-ketocholesterol content was reduced 40% in 11βHSD1⁻/⁻/apoE⁻/⁻ mice vs. control. In the aortic root, plaque size, necrotic core area and macrophage content were reduced ∼30% in 11βHSD1⁻/⁻/apoE⁻/⁻mice. Bone marrow transplantation from 11βHSD1⁻/⁻/apoE⁻/⁻ mice into apoE⁻/⁻ recipients reduced plaque area 39-46% in the thoracic aorta. In vivo foam cell formation was evaluated in thioglycollate-elicited peritoneal macrophages from 11βHSD1⁺/⁺/apoE⁻/⁻ and 11βHSD1⁻/⁻/apoE⁻/⁻ mice fed a Western diet for ∼5 weeks. Foam cell cholesterol levels were reduced 48% in 11βHSD1⁻/⁻/apoE⁻/⁻ mice vs. control. Microarray profiling of peritoneal macrophages revealed differential expression of genes involved in inflammation, stress response and energy metabolism. Several toll-like receptors (TLRs) were downregulated in 11βHSD1⁻/⁻/apoE⁻/⁻ mice including TLR 1, 3 and 4. Cytokine release from 11βHSD1⁻/⁻/apoE⁻/⁻-derived peritoneal foam cells was attenuated following challenge with oxidized LDL. CONCLUSIONS: These findings suggest that 11βHSD1 inhibition may have the potential to limit plaque development at the vessel wall and regulate foam cell formation independent of changes in plasma lipids. The diminished cytokine response to oxidized LDL stimulation is consistent with the reduction in TLR expression and suggests involvement of 11βHSD1 in modulating binding of pro-atherogenic TLR ligands.

Published

2013

6. Ligand-induced Conformational Changes in the Human Retinoic Acid Receptor γ Detected Using Monoclonal Antibodies

Author

Peter R. Reczek, Richard P. Darveau, Joyce Driscoll, John A. Lupisella, and Carrie Seachord

Subjects

Models, Molecular, Protein Conformation, Receptors, Retinoic Acid, Molecular Sequence Data, Retinoic acid, Tretinoin, Retinoic acid receptor beta, Biology, Ligands, Biochemistry, Epitopes, chemistry.chemical_compound, Antibody Specificity, Humans, Amino Acid Sequence, Molecular Biology, Antibodies, Monoclonal, Cell Biology, Retinoic acid receptor gamma, Ligand (biochemistry), Retinoid X receptor gamma, Molecular biology, Peptide Fragments, Recombinant Proteins, Retinoic acid receptor, Epitope mapping, chemistry, Retinoic acid receptor alpha, Epitope Mapping, Protein Binding

Abstract

The mechanism by which the naturally occurring ligand for a nuclear hormone receptor regulates transcription remains largely unknown. One approach combines the specificity of monoclonal antibodies, which recognize a three-dimensional epitope, with ligand binding. Using purified retinoic acid receptor gamma D and E domains, a panel of six unique monoclonal antibodies were isolated and characterized using solid-state receptor binding and retinoic acid receptor (RAR)-RXR heterodimer supershift formation. Three antibodies are specific for RARgamma (mAbI, mAbII, and mAbV) and four recognize a three-dimensional epitope (mAbI, mAbIV, mAbV, and mAbVI). Three antibodies (mAbIII, mAbV, and mAbVI) dissociate from the receptor in electrophoretic mobility shift assays upon the addition of retinoic acid. In particular, the binding characteristics of mAbIII, whose epitope was mapped to a region identified as an omega-loop (amino acids 207-222), suggest a model for ligand binding to the receptor. In this model, ligand binding causes a positioning of helix 12 into a favorable conformation for interaction with the transcriptional machinery. The Omega-loop then closes in order to stabilize this "active" position. The results reported here also suggest that a region of the hinge or D domain of the receptor (amino acids 156-188), an area that can play a role in protein-protein interactions, may also be important in ligand-induced functional changes.

Published

1996

7. The Ligand Binding Domain of the Human Retinoic Acid Receptor γ Is Predominantly α-Helical with a Trp Residue in the Ligand Binding Site

Author

Joyce Driscoll, John A. Lupisella, Peter R. Reczek, and William J. Metzler

Subjects

Alanine, Binding Sites, Base Sequence, Receptors, Retinoic Acid, Stereochemistry, Ligand binding assay, Molecular Sequence Data, Tryptophan, Retinoic acid, Cell Biology, Ligands, Ligand (biochemistry), Biochemistry, Fluorescence, Protein Structure, Secondary, chemistry.chemical_compound, Retinoic acid receptor, chemistry, Humans, Binding site, Molecular Biology, Peptide sequence

Abstract

Retinoic acid exerts its many biological effects by interaction with a nuclear protein, the retinoic acid receptor (RAR). The details of this interaction are unknown due mainly to the lack of sufficient quantities of pure functional receptor protein for biochemical and structural studies. We have recently subcloned the D and E domains of human RAR gamma for expression in Escherichia coli. Using nickel-chelation affinity chromatography with a polyhistidine amino-terminal tail, purification of the DE peptide with a pI of 5.18 was accomplished to greater than 98% purity. Scatchard analysis and fluorescence quenching techniques using the purified protein indicate a very high percentage of functional molecules ( > 95%) with a Kd for retinoic acid (t-RA) of 0.6 +/- 0.1 nM. Circular dichroism spectra of the purified domains predict a predominantly alpha-helical structure (approximately 56%) with little beta sheet present. No significant changes in these structural characteristics were observed upon binding of t-RA. Inspection of the amino acid sequence within these domains identified a single tryptophan residue at position 227. Modeling the amino acid sequence in this region as an alpha-helical structure indicates that this tryptophan is adjacent to alanine 234, which corresponds to alanine 225 in RAR beta that has previously been linked to the ligand binding site. Fluorescence of this tryptophan was quenched in a dose-dependent manner on the addition of t-RA, confirming that Trp-227 is within the ligand binding site. Tryptophan fluorescence quenching analysis also demonstrates that a single retinoic acid molecule is bound per receptor and suggests that receptor-ligand interactions occur within the amino-terminal portion of the predominantly alpha-helical ligand binding domain.

Published

1995

8. Discovery of potent, orally-active, and muscle-selective androgen receptor modulators based on an N-aryl-hydroxybicyclohydantoin scaffold

Author

Blake C. Beehler, Paul G. Sleph, Aberra Fura, Rajasree Golla, Mark E. Salvati, Joyce E. Kuhns, Lawrence G. Hamann, Ramakrishna Seethala, Yongmi An, Jacek Ostrowski, Mary F. Malley, Tammy C. Wang, Chongqing Sun, Jeffrey A. Robl, Yanting Huang, John S. Sack, Stanley R. Krystek, Gary J. Grover, and John A. Lupisella

Subjects

Agonist, Bridged-Ring Compounds, Male, Transcriptional Activation, medicine.medical_specialty, medicine.drug_class, Administration, Oral, Breast Neoplasms, Myoblasts, Mice, In vivo, Prostate, Internal medicine, Drug Discovery, medicine, Animals, Humans, Androgen Receptor Antagonists, Receptor, Luciferases, Muscle, Skeletal, Cells, Cultured, Chemistry, Hydantoins, Biological activity, Dihydrotestosterone, Rats, Androgen receptor, Muscular Atrophy, medicine.anatomical_structure, Endocrinology, Selective androgen receptor modulator, Receptors, Androgen, Molecular Medicine

Abstract

A novel, N-aryl-bicyclohydantoin selective androgen receptor modulator scaffold was discovered through structure-guided modifications of androgen receptor antagonists. A prototype compound (7R,7aS)-10b from this series is a potent and highly tissue-selective agonist of the androgen receptor. After oral dosing in a rat atrophied levator ani muscle model, (7R,7aS)-10b demonstrated efficacy at restoring levator ani muscle mass to that of intact controls and exhibited >50-fold selectivity for muscle over prostate.

Published

2006

9. Tandem optimization of target activity and elimination of mutagenic potential in a potent series of N-aryl bicyclic hydantoin-based selective androgen receptor modulators

Author

James M. Johnson, David A. Betebenner, Chongqing Sun, Yan Zou, Mark C. Manfredi, Yanting Huang, Tammy C. Wang, Scott A. Biller, Laura Custer, Robert Zahler, Jacek Ostrowski, Jennifer Price, Celia D’Arienzo, Lawrence G. Hamann, Stanley R. Krystek, John A. Lupisella, Rajasree Golla, Ramakrishna Seethala, Joyce E. Kuhns, David J. Augeri, Yingzhi Bi, and Aberra Fura

Subjects

endocrine system, Stereochemistry, Chemistry, Pharmaceutical, Clinical Biochemistry, Molecular Conformation, Pharmaceutical Science, Hydantoin, Mutagen, medicine.disease_cause, Biochemistry, Ames test, chemistry.chemical_compound, Structure-Activity Relationship, Genes, Reporter, Drug Discovery, medicine, Escherichia coli, Animals, Molecular Biology, chemistry.chemical_classification, Bicyclic molecule, Hydantoins, fungi, Organic Chemistry, food and beverages, Aromatic amine, Biological activity, Androgen Antagonists, Androgen receptor, Kinetics, Macaca fascicularis, Selective androgen receptor modulator, chemistry, Models, Chemical, Mutagenesis, Receptors, Androgen, Drug Design, Molecular Medicine, Mutagens

Abstract

Pharmacokinetic studies in cynomolgus monkeys with a novel prototype selective androgen receptor modulator revealed trace amounts of an aniline fragment released through hydrolytic metabolism. This aniline fragment was determined to be mutagenic in an Ames assay. Subsequent concurrent optimization for target activity and avoidance of mutagenicity led to the identification of a pharmacologically superior clinical candidate without mutagenic potential.

Published

2006