Your search keyword '"F. Christopher Zusi"' showing total 6 results

1. BMS-933043, a Selective α7 nAChR Partial Agonist for the Treatment of Cognitive Deficits Associated with Schizophrenia

Author

Regina Miller, Nicholas J. Lodge, John E. Macor, Wendy Clarke, Lizbeth Gallagher, Linda J. Bristow, Daniel G. Morgan, Christiana I. Iwuagwu, Ryan Westphal, Haiquan Fang, Kimberley A. Lentz, Debra J. Post-Munson, Amy Easton, Matthew D. Hill, Bei Wang, Robert A. Mate, Ivar M. McDonald, James H. Cook, Yulia Benitex, Dalton King, Thaddeus F. Molski, Ronald J. Knox, F. Christopher Zusi, Richard E. Olson, Rex Denton, Jingsong Fan, Rulin Zhao, and Robert Zaczek

Subjects

0301 basic medicine, business.industry, Organic Chemistry, Cognition, Pharmacology, medicine.disease, Biochemistry, Partial agonist, 03 medical and health sciences, Nicotinic acetylcholine receptor, 030104 developmental biology, 0302 clinical medicine, Nicotinic agonist, In vivo, Schizophrenia, Drug Discovery, medicine, business, Receptor, 030217 neurology & neurosurgery, Acetylcholine, medicine.drug

Abstract

The therapeutic treatment of negative symptoms and cognitive dysfunction associated with schizophrenia is a significant unmet medical need. Preclinical literature indicates that α7 neuronal nicotinic acetylcholine (nACh) receptor agonists may provide an effective approach to treating cognitive dysfunction in schizophrenia. We report herein the discovery and evaluation of 1c (BMS-933043), a novel and potent α7 nACh receptor partial agonist with high selectivity against other nicotinic acetylcholine receptor subtypes (>100-fold) and the 5-HT3A receptor (>300-fold). In vivo activity was demonstrated in a preclinical model of cognitive impairment, mouse novel object recognition. BMS-933043 has completed Phase I clinical trials.

Published

2017

2. Development of 4-Heteroarylamino-1′-azaspiro[oxazole-5,3′-bicyclo[2.2.2]octanes] as α7 Nicotinic Receptor Agonists

Author

Daniel G. Morgan, Wendy Clarke, Nicholas J. Lodge, Yulia Benitex, John E. Macor, Debra J. Post-Munson, Ivar M. McDonald, Richard E. Olson, Dalton King, Rex Denton, Amy Easton, Ronald J. Knox, Kimberley A. Lentz, Christiana I. Iwuagwu, Matthew D. Hill, F. Christopher Zusi, Haiquan Fang, Robert Zaczek, Linda J. Bristow, Robert A. Mate, James H. Cook, and Regina Miller

Subjects

0301 basic medicine, Steric effects, Bicyclic molecule, Chemistry, Stereochemistry, Organic Chemistry, Biochemistry, Partial agonist, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, α7 nicotinic receptor, Drug Discovery, Receptor, α7 nachr, 030217 neurology & neurosurgery, Oxazole, Quinuclidine

Abstract

We describe the synthesis of quinuclidine-containing spiroimidates and their utility as α7 nicotinic acetylcholine receptor (nAChR) partial agonists. A convergent synthetic route allowed for rapid SAR investigation and provided a diverse set of fused 6,5-heteroaryl analogs. Two potent and selective α7 nAChR partial agonists, (1′S,3′R,4′S)-N-(7-bromopyrrolo[2,1-f][1,2,4]triazin-4-yl)-4H-1′-azaspiro[oxazole-5,3′-bicyclo[2.2.2]octan]-2-amine (20) and (1′S,3′R,4′S)-N-(7-chloropyrrolo[2,1-f][1,2,4]triazin-4-yl)-4H-1′-azaspiro[oxazole-5,3′-bicyclo[2.2.2]octan]-2-amine (21), were identified. Both agonists improved cognition in a preclinical rodent model of learning and memory. Additionally, 5-HT3A receptor SAR suggested the presence of a steric site that when engaged led to significant loss of affinity at that receptor.

Published

2016

3. A highly selective inhibitor of I?B kinase, BMS-345541, blocks both joint inflammation and destruction in collagen-induced arthritis in mice

Author

Kim W. McIntyre, James R. Burke, Kathleen M. Gillooly, Pin Lu, David J. Shuster, Donna M. Dambach, Qiu Yuping, Xiadi Zhou, Mark A. Pattoli, and F. Christopher Zusi

Subjects

Male, Immunology, Administration, Oral, Arthritis, Inflammation, IκB kinase, Protein Serine-Threonine Kinases, Mice, chemistry.chemical_compound, Rheumatology, In vivo, Quinoxalines, Animals, Immunology and Allergy, Medicine, Pharmacology (medical), BMS-345541, Enzyme Inhibitors, Autoimmune disease, business.industry, Imidazoles, I-Kappa-B Kinase, medicine.disease, Arthritis, Experimental, I-kappa B Kinase, chemistry, Mice, Inbred DBA, Rheumatoid arthritis, Chronic Disease, Joints, medicine.symptom, business

Abstract

Objective The transcription of several cytokines, cell adhesion molecules, and enzymes involved in the inflammatory and destructive mechanisms of rheumatoid arthritis is dependent on nuclear factor κB (NF-κB). Because IκB kinase (IKK) is critical in transducing the signal-inducible activation of NF-κB, we examined whether the highly selective and orally bioavailable IKK inhibitor BMS-345541 is efficacious against collagen-induced arthritis (CIA) in mice. Methods Arthritis in DBA/1LacJ male mice was induced by subcutaneous immunization with bovine type II collagen on day 0 and day 21. BMS-345541 was administered perorally daily, either prophylactically (before disease onset) or therapeutically (after disease onset). Clinical assessment of the incidence and severity of disease was conducted throughout the study, and histologic evaluation was performed at the time of study termination (day 42). Results When administered prophylactically, BMS-345541 (in a dose range of 10–100 mg/kg) was effective, in a dose-dependent manner, in reducing the incidence of disease and inhibiting clinical signs of disease. Histologic evaluation of the joints showed that both inflammation and joint destruction were blocked by the IKK inhibitor. Message levels of interleukin-1β in the joints were also dose-dependently inhibited in the mice that received BMS-345541. Dose-dependent efficacy in terms of both disease severity and histologic end points was observed with the therapeutic dosing regimen of BMS-345541, with use of the 100-mg/kg dose resulting in resolution of disease. Conclusion IKK plays a key role in CIA in mice, and inhibitors of this enzyme represent a promising target for the development of novel agents to treat rheumatoid arthritis and other inflammatory diseases. BMS-345541 represents the first example of an inhibitor of IKK that has antiinflammatory activity in vivo.

Published

2003

4. CONTRIBUTORS

Author

Jerry L. Adams, Shannon E. Beard, Jacqueline Benson, Jeffrey T. Billheimer, James R. Burke, Anuk Das, Sheng Ding, Kevin J. Duffy, Derek E. Eberhart, Michael J. Elliott, Connie L. Erickson-Miller, Francisco J. Esteva, John D. Haley, Kathleen H. Holt, Gabriel N. Hortobagyi, Kenneth K. Iwata, Robert E. Jordan, Laura L. Kirkpatrick, John C. Lee, William J. Pitts, Dietmar A. Seiffert, Kris Vaddi, D. Wade Walke, Tom Y-H. Wu, Li Yan, Brian P. Zambrowicz, Zhenping Zhu, and F. Christopher Zusi

Published

2007

5. BMS-345541 is a highly selective inhibitor of I kappa B kinase that binds at an allosteric site of the enzyme and blocks NF-kappa B-dependent transcription in mice

Author

Kim W. McIntyre, Mark A. Pattoli, James R. Burke, Violetta Iotzova, Joann Strnad, Qiu Yuping, Patrick J. Brassil, Kurt R. Gregor, F. Christopher Zusi, Wendy Clarke, Xiaoxia Yang, and John F. MacMaster

Subjects

Transcription, Genetic, Allosteric regulation, IκB kinase, Biology, Protein Serine-Threonine Kinases, environment and public health, Biochemistry, chemistry.chemical_compound, Mice, Catalytic Domain, Quinoxalines, Animals, BMS-345541, Enzyme Inhibitors, CHUK, Protein kinase A, Molecular Biology, Mice, Inbred BALB C, Kinase, Imidazoles, NF-kappa B, Cell Biology, Molecular biology, I-kappa B Kinase, enzymes and coenzymes (carbohydrates), IκBα, Kinetics, chemistry, Phosphorylation, Female, Allosteric Site

Abstract

The signal-inducible phosphorylation of serines 32 and 36 of I kappa B alpha is critical in regulating the subsequent ubiquitination and proteolysis of I kappa B alpha, which then releases NF-kappa B to promote gene transcription. The multisubunit I kappa B kinase responsible for this phosphorylation contains two catalytic subunits, termed I kappa B kinase (IKK)-1 and IKK-2. BMS-345541 (4(2'-aminoethyl)amino-1,8-dimethylimidazo(1,2-a)quinoxaline) was identified as a selective inhibitor of the catalytic subunits of IKK (IKK-2 IC(50) = 0.3 microm, IKK-1 IC(50) = 4 microm). The compound failed to inhibit a panel of 15 other kinases and selectively inhibited the stimulated phosphorylation of I kappa B alpha in cells (IC(50) = 4 microm) while failing to affect c-Jun and STAT3 phosphorylation, as well as mitogen-activated protein kinase-activated protein kinase 2 activation in cells. Consistent with the role of IKK/NF-kappa B in the regulation of cytokine transcription, BMS-345541 inhibited lipopolysaccharide-stimulated tumor necrosis factor alpha, interleukin-1 beta, interleukin-8, and interleukin-6 in THP-1 cells with IC(50) values in the 1- to 5-microm range. Although a Dixon plot of the inhibition of IKK-2 by BMS-345541 showed a non-linear relationship indicating non-Michaelis-Menten kinetic binding, the use of multiple inhibition analyses indicated that BMS-345541 binds in a mutually exclusive manner with respect to a peptide inhibitor corresponding to amino acids 26-42 of I kappa B alpha with Ser-32 and Ser-36 changed to aspartates and in a non-mutually exclusive manner with respect to ADP. The opposite results were obtained when studying the binding to IKK-1. A binding model is proposed in which BMS-345541 binds to similar allosteric sites on IKK-1 and IKK-2, which then affects the active sites of the subunits differently. BMS-345541 was also shown to have excellent pharmacokinetics in mice, and peroral administration showed the compound to dose-dependently inhibit the production of serum tumor necrosis factor alpha following intraperitoneal challenge with lipopolysaccharide. Thus, the compound is effective against NF-kappa B activation in mice and represents an important tool for investigating the role of IKK in disease models.

Published

2002

6. Competitive, reversible inhibition of cytosolic phospholipase A2 at the lipid-water interface by choline derivatives that partially partition into the phospholipid bilayer

Author

Mark R. Witmer, Kenneth M. Tramposch, James R. Burke, Lynda B. Davern, R. Thomas Swann, Radmila Micanovic, Daniel Smith, Kurt R. Gregor, Joseph J. Villafranca, F. Christopher Zusi, Ramesh Padmanabha, Jeffrey Tredup, and Susan P. Manly

Subjects

Stereochemistry, Lipid Bilayers, Phospholipid, Inositol 1,4,5-Trisphosphate, Phospholipase, Biochemistry, Phospholipases A, Choline, chemistry.chemical_compound, Phospholipase A2, Non-competitive inhibition, Humans, Scattering, Radiation, Lipid bilayer, Molecular Biology, Arachidonic Acid, biology, Calorimetry, Differential Scanning, Vesicle, Lasers, Substrate (chemistry), Water, Cell Biology, U937 Cells, Lipids, Dissociation constant, N-Formylmethionine Leucyl-Phenylalanine, Quaternary Ammonium Compounds, Kinetics, Phospholipases A2, Cholesterol, chemistry, biology.protein

Abstract

Cytosolic phospholipase A2 (cPLA2) catalyzes the selective release of arachidonic acid from the sn-2 position of phospholipids and is believed to play a key cellular role in the generation of arachidonic acid. When assaying the human recombinant cPLA2 using membranes isolated from [3H]arachidonate-labeled U937 cells as substrate, 2-(2'-benzyl-4-chlorophenoxy)ethyl-dimethyl-n-octadecyl-ammonium chloride (compound 1) was found to inhibit the enzyme in a dose-dependent manner (IC50 = 5 microM). It was over 70 times more selective for the cPLA2 as compared with the human nonpancreatic secreted phospholipase A2, and it did not inhibit other phospholipases. Additionally, it inhibited arachidonate production in N-formyl-methionyl-leucyl-phenylalanine-stimulated U937 cells. To further characterize the mechanism of inhibition, an assay in which the enzyme is bound to vesicles of 1,2-dimyristoyl-sn -glycero-3-phosphomethanol containing 6-10 mol % of 1-palmitoyl-2-[1-14C]arachidonoyl-sn-glycero-3-phosphocholine was employed. With this substrate system, the dose-dependent inhibition could be defined by kinetic equations describing competitive inhibition at the lipid-water interface. The apparent equilibrium dissociation constant for the inhibitor bound to the enzyme at the interface (KI*app) was determined to be 0.097 +/- 0.032 mol % versus an apparent dissociation constant for the arachidonate-containing phospholipid of 0.3 +/- 0.1 mol %. Thus, compound 1 represents a novel structural class of inhibitor of cPLA2 that partitions into the phospholipid bilayer and competes with the phospholipid substrate for the active site. Shorter n-alkyl-chained (C-4, C-6, C-8) derivatives of compound 1 were shown to have even smaller KI*app values. However, these short-chained analogs were less potent in terms of bulk inhibitor concentration needed for inhibition when using the [3H]arachidonate-labeled U937 membranes as substrate. This discrepancy was reconciled by showing that these shorter-chained analogs did not partition into the [3H]arachidonate-labeled U937 membranes as effectively as compound 1. The implications for in vivo efficacy that result from these findings are discussed.

Published

1999