Your search keyword '"DeMartino JA"' showing total 66 results

1. Urinary galectin-3 binding protein (G3BP) as a biomarker for disease activity and renal pathology characteristics in lupus nephritis.

Author

Ding H, Shen Y, Lin C, Qin L, He S, Dai M, Okitsu SL, DeMartino JA, Guo Q, and Shen N

Subjects

Biomarkers metabolism, Cross-Sectional Studies, Galectin 3, Humans, Antigens, Neoplasm urine, Biomarkers, Tumor urine, Kidney pathology, Lupus Nephritis pathology

Abstract

Objective: There is an urgent need to identify novel biomarkers of LN to reflect renal histological changes. This study aims to investigate urinary G3BP levels in LN patients and their association with renal disease activity both clinically and pathologically., Methods: This is a cross-sectional study. A total of 119 lupus nephritis patients were recruited. Thirty patients with chronic kidney diseases (CKD) and 27 healthy volunteers were also recruited as controls. Urinary G3BP was tested by ELISA. Renal histopathology was reviewed by an experienced renal pathologist. Other clinical variables were collected through chart review., Results: The levels of uG3BP were significantly increased in active LN patients compared to those in inactive LN (p<0.001), CKD patients (p=0.01), and healthy controls (p<0.001). ROC analysis indicated a good discrimination ability of uG3BP to differentiate active LN from CKD patients (AUC=0.7), inactive LN (AUC=0.76), or healthy controls (AUC=0.87). uG3BP was positively correlated with SLEDAI (ρ=0.352, p<0.001), rSLEDAI (ρ=0.302, p<0.001), and SLICC RAS (ρ=0.465, p<0.001), indicating a role as a biomarker of disease activity. It also correlated with clinical parameters, including 24-h urine protein, ESR, and serum C3 levels. In patients with 24-h urine protein > 3.0 g/24h, uG3BP levels were higher in proliferative LN than in membranous LN (p=0.04). They could discriminate the two pathogenic types of LN (AUC=0.72), and they also positively correlated with AI (ρ=0.389, p=0.008) and scores of hyaline deposits (ρ=0.418, p=0.006). While in patients with 24-h urine protein ≤ 3.0 g/24h, uG3BP levels were not significantly different between proliferative and membranous LN, and there was no apparent relationship between uG3BP levels with AI or with scores of hyaline deposits, but they correlated positively with scores of cellular/fibrocellular crescents (ρ=0.328, p=0.04)., Conclusion: uG3BP is a non-invasive biomarker for clinically and histologically reflecting disease activity. It is associated with active histological changes and can be used as a surrogate biomarker when the renal biopsy is impractical., (© 2022. The Author(s).)

Published

2022

2. Inhibition of IRF5 cellular activity with cell-penetrating peptides that target homodimerization.

Author

Banga J, Srinivasan D, Sun CC, Thompson CD, Milletti F, Huang KS, Hamilton S, Song S, Hoffman AF, Qin YG, Matta B, LaPan M, Guo Q, Lu G, Li D, Qian H, Bolin DR, Liang L, Wartchow C, Qiu J, Downing M, Narula S, Fotouhi N, DeMartino JA, Tan SL, Chen G, and Barnes BJ

Subjects

Dendritic Cells metabolism, Gene Expression Regulation, Interferon Regulatory Factors genetics, Interferon Regulatory Factors metabolism, Phosphorylation, Cell-Penetrating Peptides genetics, Cell-Penetrating Peptides metabolism, Cell-Penetrating Peptides pharmacology

Abstract

The transcription factor interferon regulatory factor 5 (IRF5) plays essential roles in pathogen-induced immunity downstream of Toll-, nucleotide-binding oligomerization domain-, and retinoic acid-inducible gene I-like receptors and is an autoimmune susceptibility gene. Normally, inactive in the cytoplasm, upon stimulation, IRF5 undergoes posttranslational modification(s), homodimerization, and nuclear translocation, where dimers mediate proinflammatory gene transcription. Here, we report the rational design of cell-penetrating peptides (CPPs) that disrupt IRF5 homodimerization. Biochemical and imaging analysis shows that IRF5-CPPs are cell permeable, noncytotoxic, and directly bind to endogenous IRF5. IRF5-CPPs were selective and afforded cell type- and species-specific inhibition. In plasmacytoid dendritic cells, inhibition of IRF5-mediated interferon-α production corresponded to a dose-dependent reduction in nuclear phosphorylated IRF5 [p(Ser 462 )IRF5], with no effect on pIRF5 levels. These data support that IRF5-CPPs function downstream of phosphorylation. Together, data support the utility of IRF5-CPPs as novel tools to probe IRF5 activation and function in disease., (Copyright © 2020 The Authors, some rights reserved; exclusive licensee American Association for the Advancement of Science. No claim to original U.S. Government Works. Distributed under a Creative Commons Attribution NonCommercial License 4.0 (CC BY-NC).)

Published

2020

3. Pharmacological Characterization of a Novel Beta 3 Adrenergic Agonist, Vibegron: Evaluation of Antimuscarinic Receptor Selectivity for Combination Therapy for Overactive Bladder.

Author

Di Salvo J, Nagabukuro H, Wickham LA, Abbadie C, DeMartino JA, Fitzmaurice A, Gichuru L, Kulick A, Donnelly MJ, Jochnowitz N, Hurley AL, Pereira A, Sanfiz A, Veronin G, Villa K, Woods J, Zamlynny B, Zycband E, Salituro GM, Frenkl T, Weber AE, Edmondson SD, and Struthers M

Subjects

Adrenergic beta-3 Receptor Agonists therapeutic use, Animals, Drug Interactions, Female, Humans, Macaca mulatta, Male, Muscarinic Antagonists therapeutic use, Muscle, Smooth drug effects, Muscle, Smooth physiopathology, Protein Transport drug effects, Pyrimidinones therapeutic use, Pyrrolidines therapeutic use, Rats, Species Specificity, Urinary Bladder drug effects, Urinary Bladder physiopathology, Urinary Bladder, Overactive metabolism, Urinary Bladder, Overactive physiopathology, Urodynamics drug effects, Adrenergic beta-3 Receptor Agonists pharmacology, Muscarinic Antagonists pharmacology, Pyrimidinones pharmacology, Pyrrolidines pharmacology, Receptors, Adrenergic, beta-3 metabolism, Urinary Bladder, Overactive drug therapy

Abstract

Although the physiologic role of muscarinic receptors in bladder function and the therapeutic efficacy of muscarinic antagonists for the treatment of overactive bladder are well established, the role of β 3 -adrenergic receptors (β 3 ARs) and their potential as therapeutics is just emerging. In this manuscript, we characterized the pharmacology of a novel β 3 AR agonist vibegron (MK-4618, KRP-114V) and explored mechanistic interactions of β 3 AR agonism and muscarinic antagonism in urinary bladder function. Vibegron is a potent, selective full β 3 AR agonist across species, and it dose dependently increased bladder capacity, decreased micturition pressure, and increased bladder compliance in rhesus monkeys. The relaxation effect of vibegron was enhanced when combined with muscarinic antagonists, but differentially influenced by muscarinic receptor subtype selectivity. The effect was greater when vibegron was co-administered with tolterodine, a nonselective antagonist, compared with coadministration with darifenacin, a selective M3 antagonist. Furthermore, a synergistic effect for bladder strip relaxation was observed with the combination of a β 3 AR agonist and tolterodine in contrast to simple additivity with darifenacin. To determine expression in rhesus bladder, we employed a novel β 3 AR agonist probe, [ 3 H]MRL-037, that selectively labels β 3 receptors in both urothelium and detrusor smooth muscle. Vibegron administration caused a dose-dependent increase in circulating glycerol and fatty acid levels in rhesus and rat in vivo, suggesting these circulating lipids can be surrogate biomarkers. The translation of our observation to the clinic has yet to be determined, but the combination of β 3 AR agonists with M2/M3 antimuscarinics has the potential to redefine the standard of care for the pharmacological treatment of overactive bladder., (Copyright © 2017 by The American Society for Pharmacology and Experimental Therapeutics.)

Published

2017

4. Discovery of N-[Bis(4-methoxyphenyl)methyl]-4-hydroxy-2-(pyridazin-3-yl)pyrimidine-5-carboxamide (MK-8617), an Orally Active Pan-Inhibitor of Hypoxia-Inducible Factor Prolyl Hydroxylase 1-3 (HIF PHD1-3) for the Treatment of Anemia.

Author

Debenham JS, Madsen-Duggan C, Clements MJ, Walsh TF, Kuethe JT, Reibarkh M, Salowe SP, Sonatore LM, Hajdu R, Milligan JA, Visco DM, Zhou D, Lingham RB, Stickens D, DeMartino JA, Tong X, Wolff M, Pang J, Miller RR, Sherer EC, and Hale JJ

Subjects

Administration, Oral, Anemia enzymology, Animals, Dose-Response Relationship, Drug, Enzyme Inhibitors administration & dosage, Enzyme Inhibitors chemistry, Humans, Hypoxia-Inducible Factor-Proline Dioxygenases metabolism, Mice, Mice, Inbred C57BL, Models, Molecular, Molecular Structure, Pyridazines administration & dosage, Pyridazines chemistry, Pyrimidines administration & dosage, Pyrimidines chemistry, Rats, Rats, Sprague-Dawley, Structure-Activity Relationship, Anemia drug therapy, Drug Discovery, Enzyme Inhibitors pharmacology, Hypoxia-Inducible Factor-Proline Dioxygenases antagonists & inhibitors, Pyridazines pharmacology, Pyrimidines pharmacology

Abstract

The discovery of novel 4-hydroxy-2-(heterocyclic)pyrimidine-5-carboxamide inhibitors of hypoxia-inducible factor (HIF) prolyl hydroxylases (PHD) is described. These are potent, selective, orally bioavailable across several species, and active in stimulating erythropoiesis. Mouse and rat studies showed hematological changes with elevations of plasma EPO and circulating reticulocytes following single oral dose administration, while 4-week q.d. po administration in rat elevated hemoglobin levels. A major focus of the optimization process was to decrease the long half-life observed in higher species with early compounds. These efforts led to the identification of 28 (MK-8617), which has advanced to human clinical trials for anemia.

Published

2016

5. Development of a pharmacodynamic assay based on PLCγ2 phosphorylation for quantifying spleen tyrosine kinase (SYK)-Bruton's tyrosine kinase (BTK) signaling.

Author

Hsu J, Zhang J, Kitson C, Tan SL, Narula S, DeMartino JA, and Liao C

Subjects

Agammaglobulinaemia Tyrosine Kinase, Antigens, CD analysis, Antigens, Differentiation, T-Lymphocyte analysis, Arthritis, Rheumatoid blood, Arthritis, Rheumatoid metabolism, Blood Platelets cytology, Blood Platelets metabolism, Hematologic Neoplasms metabolism, Humans, Inflammation metabolism, Intracellular Signaling Peptides and Proteins metabolism, Lectins, C-Type analysis, Phosphorylation, Protein-Tyrosine Kinases metabolism, Signal Transduction, Syk Kinase, Enzyme Assays methods, Immunoassay methods, Intracellular Signaling Peptides and Proteins antagonists & inhibitors, Phospholipase C gamma metabolism, Protein-Tyrosine Kinases antagonists & inhibitors

Abstract

Spleen tyrosine kinase (SYK) and Bruton's tyrosine kinase (BTK) are key mediators in coupling cell surface receptors, such as the B-cell receptor (BCR), to downstream signaling events affecting diverse biological functions. There is therefore tremendous interest in the development of pharmacological inhibitors targeting the SYK-BTK axis for the treatment of inflammatory disorders and hematological malignancies. A good pharmacodynamic (PD) assay, ideally a blood-based assay that measures proximal events, is warranted for evaluation of such inhibitors. In platelets, collagen-induced activation of membrane glycoprotein GPVI is dependent on the SYK-BTK axis. Here, we report the development of a novel immunoassay that uses the dissociation-enhanced lanthanide fluorescent immunoassay (DELFIA) to measure GPVI-mediated phosphorylation of phospholipase C γ2 (PLCγ2), a direct substrate of SYK and BTK, in platelets. The assay was validated using SYK or BTK inhibitors and generated IC50 correlated with those from the BCR-induced B-cell activation assay. Furthermore, this assay showed good stability and uniformity over a period of 24 h in different donors. Interestingly, compound IC50 values using blood from patients with rheumatoid arthritis were slightly higher compared with those produced using samples from healthy donors. This novel platelet PLCγ2 phosphorylation-based immunoassay should serve as a promising PD assay for preclinical and clinical development of inhibitors targeting the SYK-BTK axis.

Published

2013

6. Assessment of Brd4 inhibition in idiopathic pulmonary fibrosis lung fibroblasts and in vivo models of lung fibrosis.

Author

Tang X, Peng R, Phillips JE, Deguzman J, Ren Y, Apparsundaram S, Luo Q, Bauer CM, Fuentes ME, DeMartino JA, Tyagi G, Garrido R, Hogaboam CM, Denton CP, Holmes AM, Kitson C, Stevenson CS, and Budd DC

Subjects

Acetylation, Animals, Anti-Inflammatory Agents pharmacology, Antibiotics, Antineoplastic toxicity, Azepines pharmacology, Bleomycin toxicity, Cell Cycle Proteins, Cell Movement physiology, Cell Proliferation, Cells, Cultured, Connective Tissue Growth Factor metabolism, Cytokines metabolism, Disease Models, Animal, Fibroblasts metabolism, Growth Substances metabolism, Histones metabolism, Humans, Idiopathic Pulmonary Fibrosis chemically induced, Interleukin-6 genetics, Interleukin-6 metabolism, Male, Mice, Mice, Inbred C57BL, Skin cytology, Triazoles pharmacology, Fibroblasts pathology, Idiopathic Pulmonary Fibrosis pathology, Nuclear Proteins antagonists & inhibitors, Transcription Factors antagonists & inhibitors

Abstract

Idiopathic pulmonary fibrosis (IPF) is a chronic lung disease of high unmet medical need. Although bromodomain (Brd) and extra terminal domain isoforms have recently been implicated in mediating inflammatory and oncologic indications, their roles in lung fibrosis have not been comprehensively assessed. We investigated the role of Brd on the profibrotic responses of lung fibroblasts (LFs) in patients with rapidly progressing IPF and a mouse bleomycin model of lung fibrosis. The enhanced migration, proliferation, and IL-6 release observed in LFs from patients with rapidly progressing IPF are attenuated by pharmacologic inhibition of Brd4. These changes are accompanied by enhanced histone H4 lysine5 acetylation and association of Brd4 with genes involved in the profibrotic responses in IPF LFs as demonstrated using chromatin immunoprecipitation and quantitative PCR. Oral administration of 200 mg/kg per day Brd4 inhibitor JQ1 in a therapeutic dosing regimen substantially attenuated lung fibrosis induced by bleomycin in C57BL/6 mice. In conclusion, this study shows that the Brd4 inhibitor JQ1, administered in a therapeutic dosage, is capable of inhibiting the profibrotic effects of IPF LFs and attenuates bleomycin-induced lung fibrosis in mice. These results suggest that Brd4 inhibitors may represent a novel therapy for the treatment of rapidly progressing IPF., (Copyright © 2013 American Society for Investigative Pathology. Published by Elsevier Inc. All rights reserved.)

Published

2013

7. Characterization of a novel CRAC inhibitor that potently blocks human T cell activation and effector functions.

Author

Chen G, Panicker S, Lau KY, Apparsundaram S, Patel VA, Chen SL, Soto R, Jung JK, Ravindran P, Okuhara D, Bohnert G, Che Q, Rao PE, Allard JD, Badi L, Bitter HM, Nunn PA, Narula SK, and DeMartino JA

Subjects

Anilides pharmacology, Animals, CD4-Positive T-Lymphocytes immunology, CD4-Positive T-Lymphocytes metabolism, CHO Cells, Calcineurin metabolism, Calcineurin Inhibitors, Calcium metabolism, Calcium Channels genetics, Cell Line, Cell Proliferation drug effects, Cricetinae, Cyclosporine pharmacology, Cytokines genetics, Cytokines metabolism, Gene Expression drug effects, Gene Expression genetics, Humans, Lymphocyte Activation drug effects, Lymphocyte Culture Test, Mixed methods, Membrane Proteins genetics, Membrane Proteins metabolism, Neoplasm Proteins genetics, Neoplasm Proteins metabolism, ORAI1 Protein, Rats, Receptors, Antigen, T-Cell genetics, Receptors, Antigen, T-Cell metabolism, Stromal Interaction Molecule 1, Tacrolimus pharmacology, Thiadiazoles pharmacology, CD4-Positive T-Lymphocytes drug effects, Calcium Channel Blockers pharmacology, Calcium Channels metabolism

Abstract

Store operated calcium entry (SOCE) downstream of T cell receptor (TCR) activation in T lymphocytes has been shown to be mediated mainly through the Calcium Release Activated Calcium (CRAC) channel. Here, we compared the effects of a novel, potent and selective CRAC current inhibitor, 2,6-Difluoro-N-{5-[4-methyl-1-(5-methyl-thiazol-2-yl)-1,2,5,6-tetrahydro-pyridin-3-yl]-pyrazin-2-yl}-benzamide (RO2959), on T cell effector functions with that of a previously reported CRAC channel inhibitor, YM-58483, and a calcineurin inhibitor Cyclosporin A (CsA). Using both electrophysiological and calcium-based fluorescence measurements, we showed that RO2959 is a potent SOCE inhibitor that blocked an IP3-dependent current in CRAC-expressing RBL-2H3 cells and CHO cells stably expressing human Orai1 and Stim1, as well as SOCE in human primary CD4(+) T cells triggered by either TCR stimulation or thapsigargin treatment. Furthermore, we demonstrated that RO2959 completely inhibited cytokine production as well as T cell proliferation mediated by TCR stimulation or MLR (mixed lymphocyte reaction). Lastly, we showed by gene expression array analysis that RO2959 potently blocked TCR triggered gene expression and T cell functional pathways similar to CsA and another calcineurin inhibitor FK506. Thus, both from a functional and transcriptional level, our data provide evidence that RO2959 is a novel and selective CRAC current inhibitor that potently inhibits human T cell functions., (Copyright © 2012 Elsevier Ltd. All rights reserved.)

Published

2013

8. Targeting the SYK-BTK axis for the treatment of immunological and hematological disorders: recent progress and therapeutic perspectives.

Author

Tan SL, Liao C, Lucas MC, Stevenson C, and DeMartino JA

Subjects

Adaptive Immunity drug effects, Adjuvants, Immunologic administration & dosage, Adjuvants, Immunologic chemistry, Agammaglobulinaemia Tyrosine Kinase, Animals, Clinical Trials as Topic, Drug Evaluation, Preclinical, Hematologic Diseases enzymology, Hematologic Diseases immunology, Humans, Immune System Diseases enzymology, Immune System Diseases immunology, Immunity, Innate drug effects, Molecular Structure, Molecular Targeted Therapy, Protein Kinase Inhibitors administration & dosage, Protein Kinase Inhibitors chemistry, Syk Kinase, Adjuvants, Immunologic therapeutic use, Hematologic Diseases drug therapy, Immune System Diseases drug therapy, Intracellular Signaling Peptides and Proteins antagonists & inhibitors, Protein Kinase Inhibitors therapeutic use, Protein-Tyrosine Kinases antagonists & inhibitors

Abstract

Spleen Tyrosine Kinase (SYK) and Bruton's Tyrosine Kinase (BTK) are non-receptor cytoplasmic tyrosine kinases that are primarily expressed in cells of hematopoietic lineage. Both are key mediators in coupling activated immunoreceptors to downstream signaling events that affect diverse biological functions, from cellular proliferation, differentiation and adhesion to innate and adaptive immune responses. As such, pharmacological inhibitors of SYK or BTK are being actively pursued as potential immunomodulatory agents for the treatment of autoimmune and inflammatory disorders. Deregulation of SYK or BTK activity has also been implicated in certain hematological malignancies. To date, from a clinical perspective, pharmacological inhibition of SYK activity has demonstrated encouraging efficacy in patients with rheumatoid arthritis (RA), while patients with relapsed or refractory chronic lymphocytic leukemia (CLL)/small lymphocytic lymphoma (SLL) have benefited from covalent inhibitors of BTK in early clinical studies. Here, we review and discuss recent insights into the emerging role of the SYK-BTK axis in innate immune cell function as well as in the maintenance of survival and homing signals for tumor cell progression. The current progress on the clinical development of SYK and BTK inhibitors is also highlighted., (Copyright © 2013 Elsevier Inc. All rights reserved.)

Published

2013

9. Bruton's Tyrosine Kinase mediates platelet receptor-induced generation of microparticles: a potential mechanism for amplification of inflammatory responses in rheumatoid arthritis synovial joints.

Author

Hsu J, Gu Y, Tan SL, Narula S, DeMartino JA, and Liao C

Subjects

Agammaglobulinaemia Tyrosine Kinase, Arthritis, Rheumatoid metabolism, B-Lymphocytes immunology, Catalysis, Coculture Techniques, Humans, Interleukin-6 biosynthesis, Interleukin-8 biosynthesis, Lectins, C-Type metabolism, Lymphocyte Activation immunology, Phospholipase C gamma metabolism, Phosphorylation, Platelet Activation, Platelet Aggregation drug effects, Platelet Membrane Glycoproteins antagonists & inhibitors, Protein Kinase Inhibitors pharmacology, Receptors, Antigen, B-Cell metabolism, Blood Platelets metabolism, Cell-Derived Microparticles metabolism, Platelet Membrane Glycoproteins metabolism, Protein-Tyrosine Kinases metabolism, Synovitis metabolism

Abstract

Platelet microparticles (pMPs) are small membrane-coated vesicles that are released from the plasma membrane upon platelet activation. In the joint fluid of patients with rheumatoid arthritis, pMP can interact with and activate fibroblast-like synoviocytes (FLS), which are important effector cells that mediate both immune activation and joint destruction. The signaling process by which engagement of glycoprotein VI (GPVI), a surface glycoprotein receptor for collagen which is expressed on platelets, triggers pMP generation is poorly understood, but has been suggested to involve Spleen Tyrosine Kinase (SYK), best known as an upstream activator of Bruton's Tyrosine Kinase (BTK) in B cells. In this study, we showed that activation of human platelets triggered by convulxin or collagen, specific ligands for GPVI receptor, or alternatively by antibody-mediated cross-linking of another platelet receptor, C type lectin-like receptor 2 (CLEC2), resulted in phosphorylation of BTK and downstream effector, phospholipase Cγ2 (PLCγ2). A potent and selective BTK inhibitor, RN486, inhibited GPVI- or CLEC2-mediated PLCγ2 phosphorylation and pMP production in a dose-dependent manner. BTK is also an essential effector of B cell receptor (BCR)-induced B cell signaling. Consistent with the biology, the IC50s of BTK inhibitors with varying potencies in a BCR-dependent B cell activation marker assay correlated with those in the GPVI-mediated PLCγ2 phosphorylation. In a co-culture system consisting of human primary synovial FLS and activated human platelets, convulxin stimulation resulted in elevated production of pro-inflammatory cytokines, IL-6 and IL-8, an effect which was dose-dependently blocked by RN486. The effects are specific as RN486 abrogated platelet aggregation induced by GPVI ligands but not by other platelet surface receptor agonists. Taken together, our data further support the potential therapeutic utility of BTK inhibitors in RA therapy, by inhibiting GPVI-mediated platelet activation and thus subsequent amplification of inflammation driven by pMP-induced FLS cytokines production., (Copyright © 2012 Elsevier B.V. All rights reserved.)

Published

2013

10. BET bromodomain proteins mediate downstream signaling events following growth factor stimulation in human lung fibroblasts and are involved in bleomycin-induced pulmonary fibrosis.

Author

Tang X, Peng R, Ren Y, Apparsundaram S, Deguzman J, Bauer CM, Hoffman AF, Hamilton S, Liang Z, Zeng H, Fuentes ME, Demartino JA, Kitson C, Stevenson CS, and Budd DC

Subjects

Actins biosynthesis, Administration, Oral, Animals, Becaplermin, Bleomycin, Cell Cycle Proteins, Cell Movement, Cell Proliferation, Cytokines metabolism, Epigenesis, Genetic, Extracellular Matrix Proteins biosynthesis, Fibroblasts drug effects, Humans, Lung drug effects, Lung pathology, Male, Mice, Mice, Inbred C57BL, Nuclear Proteins antagonists & inhibitors, Nuclear Proteins genetics, Protein Serine-Threonine Kinases antagonists & inhibitors, Protein Serine-Threonine Kinases genetics, Proto-Oncogene Proteins c-sis metabolism, Pulmonary Fibrosis chemically induced, Pulmonary Fibrosis prevention & control, RNA, Small Interfering genetics, Transcription Factors antagonists & inhibitors, Transcription Factors genetics, Transcription, Genetic, Transforming Growth Factor beta1 metabolism, Fibroblasts physiology, Lung metabolism, Nuclear Proteins metabolism, Protein Serine-Threonine Kinases metabolism, Proto-Oncogene Proteins c-sis pharmacology, Pulmonary Fibrosis metabolism, Transcription Factors metabolism, Transforming Growth Factor beta1 pharmacology

Abstract

Epigenetic alterations, such as histone acetylation, regulate the signaling outcomes and phenotypic responses of fibroblasts after growth factor stimulation. The bromodomain and extra-terminal domain-containing proteins (Brd) bind to acetylated histone residues, resulting in recruitment of components of the transcriptional machinery and subsequent gene transcription. Given the central importance of fibroblasts in tissue fibrosis, this study sought to determine the role of Brd proteins in human lung fibroblasts (LFs) after growth factor stimulation and in the murine bleomycin model of lung fibrosis. Using small interfering RNA against human Brd2 and Brd4 and pharmacologic Brd inhibitors, this study found that Brd2 and Brd4 are essential in mediating the phenotypic responses of LFs downstream of multiple growth factor pathways. Growth factor stimulation of LFs causes increased histone acetylation, association of Brd4 with growth factor-responsive genes, and enhanced transcription of these genes that could be attenuated with pharmacologic Brd inhibitors. Of note, lung fibrosis induced after intratracheal bleomycin challenge in mice could be prevented by pretreatment of animals with pharmacologic inhibitors of Brd proteins. This study is the first demonstration of a role for Brd2 and Brd4 proteins in mediating the responses of LFs after growth factor stimulation and in driving the induction of lung fibrosis in mice in response to bleomycin challenge.

Published

2013

11. Evidence for cyclic diguanylate as a vaccine adjuvant with novel immunostimulatory activities.

Author

Gray PM, Forrest G, Wisniewski T, Porter G, Freed DC, DeMartino JA, Zaller DM, Guo Z, Leone J, Fu TM, and Vora KA

Subjects

Alum Compounds administration & dosage, Animals, Antibodies, Bacterial immunology, Cyclic GMP administration & dosage, Cyclic GMP immunology, Female, Germinal Center immunology, Hepatitis B Surface Antigens administration & dosage, Humans, Immunity, Cellular, Immunity, Humoral, Immunization, Immunoglobulin G immunology, Immunologic Memory, Interferon-gamma biosynthesis, Interferon-gamma immunology, Interleukin-10 biosynthesis, Interleukin-10 immunology, Leukocytes, Mononuclear drug effects, Leukocytes, Mononuclear immunology, Leukocytes, Mononuclear metabolism, Lipopolysaccharides administration & dosage, Lipopolysaccharides immunology, Macaca mulatta, Mice, Oligodeoxyribonucleotides administration & dosage, Oligodeoxyribonucleotides immunology, Th1 Cells drug effects, Th1 Cells immunology, Th1 Cells metabolism, Tumor Necrosis Factor-alpha biosynthesis, Tumor Necrosis Factor-alpha immunology, Adjuvants, Immunologic administration & dosage, Antibodies, Bacterial biosynthesis, Cyclic GMP analogs & derivatives, Immunoglobulin G biosynthesis

Abstract

Cyclic diguanylate (c-di-GMP), a bacterial signaling molecule, possesses protective immunostimulatory activity in bacterial challenge models. This study explored the potential of c-di-GMP as a vaccine adjuvant comparing it with LPS, CpG oligonucleotides, and a conventional aluminum salt based adjuvant. In this evaluation, c-di-GMP was a more potent activator of both humoral and Th1-like immune responses as evidenced by the robust IgG2a antibody response it induced in mice and the strong IFN-γ, TNF-α and IP-10 responses, it elicited in mice and in vitro in non-human primate peripheral blood mononuclear cells. Further, compared to LPS or CpG, c-di-GMP demonstrated a more pronounced ability to induce germinal center formation, a hallmark of long-term memory, in immunized mice. Together, these data add to the growing body of evidence supporting the utility of c-di-GMP as an adjuvant in vaccination for sustained and robust immune responses and provide a rationale for further evaluation in appropriate models of immunization., (Copyright © 2012 Elsevier Inc. All rights reserved.)

Published

2012

12. 1,3,8-Triazaspiro[4.5]decane-2,4-diones as efficacious pan-inhibitors of hypoxia-inducible factor prolyl hydroxylase 1-3 (HIF PHD1-3) for the treatment of anemia.

Author

Vachal P, Miao S, Pierce JM, Guiadeen D, Colandrea VJ, Wyvratt MJ, Salowe SP, Sonatore LM, Milligan JA, Hajdu R, Gollapudi A, Keohane CA, Lingham RB, Mandala SM, DeMartino JA, Tong X, Wolff M, Steinhuebel D, Kieczykowski GR, Fleitz FJ, Chapman K, Athanasopoulos J, Adam G, Akyuz CD, Jena DK, Lusen JW, Meng J, Stein BD, Xia L, Sherer EC, and Hale JJ

Subjects

Animals, Aza Compounds pharmacokinetics, Aza Compounds pharmacology, Dogs, ERG1 Potassium Channel, Erythropoietin biosynthesis, Ether-A-Go-Go Potassium Channels metabolism, High-Throughput Screening Assays, Humans, Hydantoins pharmacokinetics, Hydantoins pharmacology, Hypoxia-Inducible Factor-Proline Dioxygenases, Indoles chemical synthesis, Indoles pharmacokinetics, Indoles pharmacology, Liver drug effects, Liver enzymology, Macaca mulatta, Mass Spectrometry, Mice, Mice, Inbred C57BL, Protein Binding, Rats, Spiro Compounds pharmacokinetics, Spiro Compounds pharmacology, Structure-Activity Relationship, Up-Regulation, Anemia drug therapy, Aza Compounds chemical synthesis, Hydantoins chemical synthesis, Hypoxia-Inducible Factor 1 metabolism, Procollagen-Proline Dioxygenase antagonists & inhibitors, Spiro Compounds chemical synthesis

Abstract

The discovery of 1,3,8-triazaspiro[4.5]decane-2,4-diones (spirohydantoins) as a structural class of pan-inhibitors of the prolyl hydroxylase (PHD) family of enzymes for the treatment of anemia is described. The initial hit class, spirooxindoles, was identified through affinity selection mass spectrometry (AS-MS) and optimized for PHD2 inhibition and optimal PK/PD profile (short-acting PHDi inhibitors). 1,3,8-Triazaspiro[4.5]decane-2,4-diones (spirohydantoins) were optimized as an advanced lead class derived from the original spiroindole hit. A new set of general conditions for C-N coupling, developed using a high-throughput experimentation (HTE) technique, enabled a full SAR analysis of the spirohydantoins. This rapid and directed SAR exploration has resulted in the first reported examples of hydantoin derivatives with good PK in preclinical species. Potassium channel off-target activity (hERG) was successfully eliminated through the systematic introduction of acidic functionality to the molecular structure. Undesired upregulation of alanine aminotransferese (ALT) liver enzymes was mitigated and a robust on-/off-target margin was achieved. Spirohydantoins represent a class of highly efficacious, short-acting PHD1-3 inhibitors causing a robust erythropoietin (EPO) upregulation in vivo in multiple preclinical species. This profile deems spirohydantoins as attractive short-acting PHDi inhibitors with the potential for treatment of anemia., (© 2012 American Chemical Society)

Published

2012

13. Dual targeting of CCR2 and CX3CR1 in an arterial injury model of vascular inflammation.

Author

Jerath MR, Liu P, Struthers M, Demartino JA, Peng R, Peterson LB, Cumiskey AM, Yang L, Rojas M, Patel DD, and Fong AM

Abstract

Objectives: The chemokine receptors CCR2 and CX3CR1 are important in the development of coronary artery disease. The purpose of this study is to analyze the effect of a novel CCR2 inhibitor in conjunction with CX3CR1 deletion on vascular inflammation., Methods: The novel CCR2 antagonist MRL-677 was characterized using an in vivo model of monocyte migration. To determine the relative roles of CCR2 and CX3CR1 in vascular remodeling, normal or CX3CR1 deficient mice were treated with MRL-677. After 14 days, the level of intimal hyperplasia in the artery was visualized by paraffin sectioning and histology of the hind limbs., Results: MRL-677 is a CCR2 antagonist that is effective in blocking macrophage trafficking in a peritoneal thioglycollate model. Intimal hyperplasia resulting from vascular injury was also assessed in mice. Based on the whole-blood potency of MRL-677, sufficient drug levels were maintained for the entire 14 day experimental period to afford good coverage of mCCR2 with MRL-677. Blocking CCR2 with MRL-677 resulted in a 56% decrease in the vascular injury response (n = 9, p < 0.05) in normal animals. Mice in which both CCR2 and CX3CR1 pathways were targeted (CX3CR1 KO mice given MRL-677) had an 88% decrease in the injury response (n = 6, p = 0.009)., Conclusion: In this study we have shown that blocking CCR2 with a low molecular weight antagonist ameliorates the inflammatory response to vascular injury. The protective effect of CCR2 blockade is increased in the presence of CX3CR1 deficiency suggesting that CX3CR1 and CCR2 have non-redundant functions in the progression of vascular inflammation.

Published

2010

14. Assessment of chemokine receptor function on monocytes in whole blood: In vitro and ex vivo evaluations of a CCR2 antagonist.

Author

Wisniewski T, Bayne E, Flanagan J, Shao Q, Wnek R, Matheravidathu S, Fischer P, Forrest MJ, Peterson L, Song X, Yang L, Demartino JA, and Struthers M

Subjects

Animals, Cell Movement drug effects, Cell Movement immunology, Cell Shape drug effects, Cell Shape immunology, High-Throughput Screening Assays, Humans, Injections, Intravenous, Macaca mulatta, Monocytes pathology, Pharmaceutical Preparations administration & dosage, Receptors, CCR2 metabolism, Sensitivity and Specificity, Skin pathology, Small Molecule Libraries, Cell Migration Assays, Leukocyte, Monocytes drug effects, Pharmaceutical Preparations metabolism, Receptors, CCR2 antagonists & inhibitors, Skin drug effects

Abstract

Inhibition of monocyte and macrophage function by targeting chemokine receptors represents an attractive strategy for therapeutic intervention in inflammatory diseases. We describe an assay to assess chemokine receptor function on whole blood monocytes by measuring chemokine stimulated change in cell shape as measured by flow cytometry. The relative potential of the chemokine receptors CCR1, CCR2, CCR5, CX(3)CR1, and CXCR4 to activate monocytes in whole blood was evaluated and compared. Analysis of MCP-1 response for monocytes in blood from numerous donors revealed that the assay method had excellent intra-donor reproducibility and sensitivity. Further, the utility of this assay to determine target engagement by chemokine receptor antagonists was demonstrated using a CCR2 antagonist in rhesus monkeys. Blockade of CCR2 on whole blood monocytes was demonstrated ex vivo on blood samples collected from rhesus monkeys administered a small molecule CCR2 antagonist (MK-0812). Using a delayed-type hypersensitivity reaction to elicit monocyte recruitment to the skin of rhesus monkeys, we also evaluated the ability of MK-0812 to block monocyte migration in vivo. Blockade of CCR2 stimulation of whole blood monocytes was correlated with the inhibition of monocyte recruitment to the skin, validating the potential to use this approach in the evaluation of dose selection for chemokine receptor antagonists clinically., (Copyright 2009 Elsevier B.V. All rights reserved.)

Published

2010

15. Design, synthesis, and structure-activity relationship of novel CCR2 antagonists.

Author

Kothandaraman S, Donnely KL, Butora G, Jiao R, Pasternak A, Morriello GJ, Goble SD, Zhou C, Mills SG, Maccoss M, Vicario PP, Ayala JM, Demartino JA, Struthers M, Cascieri MA, and Yang L

Subjects

Administration, Oral, Animals, Chemotaxis, Dogs, Drug Design, Humans, Inhibitory Concentration 50, Macaca mulatta, Models, Chemical, Molecular Structure, Rats, Rats, Sprague-Dawley, Structure-Activity Relationship, Chemistry, Pharmaceutical methods, Receptors, CCR2 antagonists & inhibitors, Receptors, CCR2 chemistry

Abstract

A series of novel 1-aminocyclopentyl-3-carboxyamides incorporating substituted tetrahydropyran moieties have been synthesized and subsequently evaluated for their antagonistic activity against the human CCR2 receptor. Among them analog 59 was found to posses potent antagonistic activity.

Published

2009

16. Conformational studies of 3-amino-1-alkyl-cyclopentane carboxamide CCR2 antagonists leading to new spirocyclic antagonists.

Author

Pasternak A, Goble SD, Doss GA, Tsou NN, Butora G, Vicario PP, Ayala JM, Struthers M, Demartino JA, Mills SG, and Yang L

Subjects

Acetals chemistry, Acetals pharmacology, Crystallography, X-Ray, Cyclopentanes pharmacology, Humans, Kinetics, Molecular Conformation, Monocytes drug effects, Monocytes metabolism, Receptors, CCR2 metabolism, Spiro Compounds pharmacology, Structure-Activity Relationship, Cyclopentanes chemistry, Receptors, CCR2 antagonists & inhibitors, Spiro Compounds chemistry

Abstract

In an effort to shed light on the active binding conformation of our 3-amino-1-alkyl-cyclopentane carboxamide CCR2 antagonists, we prepared several conformationally constrained analogs resulting from backbone cyclization. Evaluation of CCR2 binding affinities for these analogs gave insight into the optimal relative positions of the piperidine and benzylamide moieties while simultaneously leading to the discovery of a new, potent lead type based upon a spirocyclic acetal scaffold.

Published

2008

17. Potent heteroarylpiperidine and carboxyphenylpiperidine 1-alkyl-cyclopentane carboxamide CCR2 antagonists.

Author

Pasternak A, Goble SD, Vicario PP, Di Salvo J, Ayala JM, Struthers M, DeMartino JA, Mills SG, and Yang L

Subjects

Animals, Humans, Molecular Structure, Piperidines chemistry, Potassium Channel Blockers pharmacology, Rats, Structure-Activity Relationship, Piperidines chemical synthesis, Piperidines pharmacology, Receptors, CCR2 antagonists & inhibitors

Abstract

This report describes replacement of the 4-(4-fluorophenyl)piperidine moiety in our CCR2 antagonists with 4-heteroaryl piperidine and 4-(carboxyphenyl)-piperidine subunits. Some of the resulting analogs retained potency in our CCR2 binding assay and had improved selectivity versus the I(Kr) channel; poor selectivity against I(Kr) had been a liability of earlier analogs in this series.

Published

2008

18. Mice overexpressing chemokine ligand 2 (CCL2) in astrocytes display enhanced nociceptive responses.

Author

Menetski J, Mistry S, Lu M, Mudgett JS, Ransohoff RM, Demartino JA, Macintyre DE, and Abbadie C

Subjects

Animals, Astrocytes metabolism, Chemokines biosynthesis, Enzyme-Linked Immunosorbent Assay, Formaldehyde, Freund's Adjuvant, Ganglia, Spinal metabolism, Hot Temperature, Inflammation chemically induced, Inflammation complications, Inflammation physiopathology, Male, Mice, Pain Measurement, Peripheral Nerve Injuries, Peripheral Nervous System Diseases complications, Peripheral Nervous System Diseases physiopathology, Phenotype, Physical Stimulation, Reaction Time physiology, Reverse Transcriptase Polymerase Chain Reaction, Schwann Cells physiology, Spinal Cord physiology, Astrocytes physiology, Chemokine CCL2 biosynthesis, Chemokine CCL2 physiology, Pain physiopathology

Abstract

Recent findings demonstrate that chemokines, and more specifically CC chemokine ligand 2 (CCL2 or monocyte chemoattractant protein-1), play a major role in pain processing. In the present study, we assess nociceptive responses of mice that overexpressed CCL2 under control of glial fibrillary acidic protein promoter (CCL2 tg). In models of acute nociception CCL2 tg mice demonstrated significantly enhanced nociceptive behavior relative to wild-type controls in responses to both thermal (hot plate) and chemical (formalin test) stimulus modalities. There were no differences in mechanical allodynia in the partial sciatic nerve ligation model, in terms of either magnitude or duration of the allodynic response; however, both groups responded to the maximal extent measurable. In a model of inflammatory pain, elicited by intraplantar administration of complete Freund's adjuvant (CFA), CCL2 tg mice displayed both greater edema and thermal hyperalgesia compared with control mice. In control mice, edema and hyperalgesia returned to baseline values 5-7 days post CFA. However, in CCL2 tg mice, thermal hyperalgesia was significantly different from baseline up to 3 weeks post CFA. Parallel to these enhanced behavioral responses CCL2 serum levels were significantly greater in CCL2 overexpressing mice and remained elevated 7 days post CFA. Consequently, proinflammatory cytokine mRNA expression (IL-1beta, IL-6, and TNFalpha) levels were greater in skin, dorsal root ganglia (DRG), and spinal cord, whereas the anti-inflammatory cytokine (IL-10) level was lower in skin and DRG in CCL2 overexpressing mice than in control mice. Taken together with data from CCR2-deficient mice, these present data confirm a key role of CCL2/CCR2 axis in pain pathways and suggest that inhibiting this axis may result in novel pain therapies.

Published

2007

19. CCR5 blockade modulates inflammation and alloimmunity in primates.

Author

Schröder C, Pierson RN 3rd, Nguyen BN, Kawka DW, Peterson LB, Wu G, Zhang T, Springer MS, Siciliano SJ, Iliff S, Ayala JM, Lu M, Mudgett JS, Lyons K, Mills SG, Miller GG, Singer II, Azimzadeh AM, and DeMartino JA

Subjects

Animals, Antibody Formation drug effects, Antibody Formation immunology, Autoimmunity drug effects, Autoimmunity immunology, Cyclosporine administration & dosage, Disease Models, Animal, Graft Survival immunology, HIV Infections drug therapy, HIV Infections immunology, HIV Infections pathology, Heart Transplantation pathology, Humans, Immunosuppressive Agents administration & dosage, Inflammation drug therapy, Inflammation immunology, Inflammation pathology, Isoantibodies immunology, Kidney Transplantation immunology, Macaca fascicularis, Macrophages pathology, Male, Stress, Physiological drug therapy, Stress, Physiological immunology, Stress, Physiological pathology, T-Lymphocytes pathology, Transplantation Tolerance immunology, Transplantation, Homologous, Valine administration & dosage, Vascular Diseases drug therapy, Vascular Diseases immunology, Vascular Diseases pathology, CCR5 Receptor Antagonists, Graft Survival drug effects, Heart Transplantation immunology, Macrophages immunology, Pyrazoles administration & dosage, T-Lymphocytes immunology, Transplantation Tolerance drug effects, Valine analogs & derivatives

Abstract

Pharmacologic antagonism of CCR5, a chemokine receptor expressed on macrophages and activated T cells, is an effective antiviral therapy in patients with macrophage-tropic HIV infection, but its efficacy in modulating inflammation and immunity is only just beginning to be investigated. In this regard, the recruitment of CCR5-bearing cells into clinical allografts is a hallmark of acute rejection and may anticipate chronic rejection, whereas conventionally immunosuppressed renal transplant patients homozygous for a nonfunctional Delta32 CCR5 receptor rarely exhibit late graft loss. Therefore, we explored the effects of a potent, highly selective CCR5 antagonist, Merck's compound 167 (CMPD 167), in an established cynomolgus monkey cardiac allograft model. Although perioperative stress responses (fever, diminished activity) and the recruitment of CCR5-bearing leukocytes into the graft were markedly attenuated, anti-CCR5 monotherapy only marginally prolonged allograft survival. In contrast, relative to cyclosporine A monotherapy, CMPD 167 with cyclosporine A delayed alloantibody production, suppressed cardiac allograft vasculopathy, and tended to further prolong graft survival. CCR5 therefore represents an attractive therapeutic target for attenuating postsurgical stress responses and favorably modulating pathogenic alloimmunity in primates, including man.

Published

2007

20. Diaryl substituted pyrazoles as potent CCR2 receptor antagonists.

Author

Pinkerton AB, Huang D, Cube RV, Hutchinson JH, Struthers M, Ayala JM, Vicario PP, Patel SR, Wisniewski T, DeMartino JA, and Vernier JM

Subjects

Chemotaxis drug effects, Humans, In Vitro Techniques, Indicators and Reagents, Monocytes drug effects, Oxidation-Reduction, Receptors, CCR2, Receptors, Chemokine drug effects, Structure-Activity Relationship, Pyrazoles chemical synthesis, Pyrazoles pharmacology, Receptors, Chemokine antagonists & inhibitors

Abstract

We have identified and synthesized a series of diaryl substituted pyrazoles as potent antagonists of the chemokine receptor subtype 2. Structure-activity relationship studies directed toward improving the potency led to the discovery of 23 (IC50 = 6 nM).

Published

2007

21. Methylxanthine drugs are chitinase inhibitors: investigation of inhibition and binding modes.

Author

Rao FV, Andersen OA, Vora KA, Demartino JA, and van Aalten DM

Subjects

Chitinases metabolism, Enzyme Inhibitors chemistry, Enzyme Inhibitors metabolism, Models, Molecular, Molecular Structure, Protein Binding, Xanthines chemistry, Xanthines metabolism, Chitinases antagonists & inhibitors, Enzyme Inhibitors pharmacology, Xanthines pharmacology

Abstract

Family 18 chitinases play key roles in a range of pathogenic organisms and are overexpressed in the asthmatic lung. By screening a library of marketed drug molecules, we have identified methylxanthine derivatives as possible inhibitor leads. These derivatives, theophylline, caffeine, and pentoxifylline, are used therapeutically as antiinflammatory agents, with pleiotropic mechanisms of action. Here it is shown that they are also competitive inhibitors against a fungal family 18 chitinase, with pentoxifylline being the most potent (K(i) of 37 microM). Crystallographic analysis of chitinase-inhibitor complexes revealed specific interactions with the active site, mimicking the reaction intermediate analog, allosamidin. Mutagenesis identified the key active site residues, conserved in mammalian chitinases, which contribute to inhibitor affinity. Enzyme assays also revealed that these methylxanthines are active against human chitinases.

Published

2005

22. Potent 1,3,4-trisubstituted pyrrolidine CCR5 receptor antagonists: effects of fused heterocycles on antiviral activity and pharmacokinetic properties.

Author

Kim D, Wang L, Hale JJ, Lynch CL, Budhu RJ, Maccoss M, Mills SG, Malkowitz L, Gould SL, DeMartino JA, Springer MS, Hazuda D, Miller M, Kessler J, Hrin RC, Carver G, Carella A, Henry K, Lineberger J, Schleif WA, and Emini EA

Subjects

Administration, Oral, Animals, Anti-HIV Agents pharmacokinetics, HeLa Cells, Heterocyclic Compounds pharmacokinetics, Humans, Pyrrolidines pharmacokinetics, Rats, Receptors, CCR5 metabolism, Anti-HIV Agents chemistry, CCR5 Receptor Antagonists, Heterocyclic Compounds chemistry, Pyrrolidines chemistry

Abstract

A series of 1,3,4-trisubstituted pyrrolidine CCR5 receptor antagonists containing a variety of fused heterocycles at the 4-position of the piperidine side chain has been discovered, which are orally bioavailable with potent anti-HIV activity.

Published

2005

23. Synthesis and evaluation of CCR5 antagonists containing modified 4-piperidinyl-2-phenyl-1-(phenylsulfonylamino)-butane.

Author

Shah SK, Chen N, Guthikonda RN, Mills SG, Malkowitz L, Springer MS, Gould SL, Demartino JA, Carella A, Carver G, Holmes K, Schleif WA, Danzeisen R, Hazuda D, Kessler J, Lineberger J, Miller M, Emini EA, and MacCoss M

Subjects

Anti-HIV Agents pharmacology, Butanes chemical synthesis, Butanes pharmacology, Dose-Response Relationship, Drug, Inhibitory Concentration 50, Piperidines chemical synthesis, Piperidines pharmacology, Structure-Activity Relationship, Sulfones pharmacology, Viruses drug effects, Anti-HIV Agents chemical synthesis, CCR5 Receptor Antagonists, Sulfones chemical synthesis

Abstract

Synthesis of analogs containing more rigid bicyclic piperidine replacements for the 4-benzyloxycarbonyl-(ethyl)amino-piperidine moiety of the CCR5 antagonist structure, 1, is described. Although similar binding affinity to the lead was achieved with some analogs they were overall less potent anti-HIV agents suggesting that other features besides CCR5 binding are required for good anti-viral activity.

Published

2005

24. A unique pattern of up- and down-regulation of chemokine receptor CXCR3 on inflammation-inducing Th1 cells.

Author

Chen J, Vistica BP, Takase H, Ham DI, Fariss RN, Wawrousek EF, Chan CC, DeMartino JA, Farber JM, and Gery I

Subjects

Adoptive Transfer, Animals, Cell Movement immunology, Cells, Cultured, Disease Models, Animal, Down-Regulation, Eye Diseases pathology, Mice, Mice, Transgenic, RNA, Messenger analysis, Receptors, CXCR3, Receptors, Chemokine immunology, Reverse Transcriptase Polymerase Chain Reaction, Spleen immunology, Up-Regulation, Eye Diseases immunology, Inflammation immunology, Lymphocyte Activation immunology, Receptors, Chemokine biosynthesis, Th1 Cells immunology

Abstract

Chemokine receptor CXCR3 and its CXC ligands play major roles in Th1 cell-induced inflammatory processes. Here, we examined the expression of CXCR3 by TCR-transgenic Th1 lymphocytes that induce ocular inflammation in mice expressing the target antigen in their lenses. The essential role of CXCR3 in this model was indicated by the observation that the ocular inflammation was significantly blocked by an antibody against this receptor. CXCR3 expression by Th1 cells was elevated during their initial activation in culture and further increased during the consecutive incubation with IL-2. However, CXCR3 expression declined dramatically during the ensuing antigenic reactivation, in parallel with down-regulation of its mRNA. Yet, reactivated Th1 cells exhibited the highest degree of pathogenicity when adoptively transferred into recipients. Transferred reactivated Th1 cells proliferated vigorously and re-expressed CXCR3 while residing in the spleen of recipient mice, reaching approximately 85% positivity 4 days post cell transfer when their massive migration to the target eyes began. Importantly, infiltrating Th1 cells underwent profound phenotypic changes in the eye that closely resembled those seen during reactivation of Th1 cells in vitro and included down-regulation of CXCR3. These observations thus show that expression of CXCR3, a major participant in Th1-induced inflammation, fluctuates profoundly during cell activation and migration and is down-regulated upon re-exposure of these cells to the antigen, in vitro or in the target organ.

Published

2004

25. Syntheses and biological evaluation of 5-(piperidin-1-yl)-3-phenyl-pentylsulfones as CCR5 antagonists.

Author

Shankaran K, Donnelly KL, Shah SK, Caldwell CG, Chen P, Finke PE, Oates B, MacCoss M, Mills SG, DeMartino JA, Gould SL, Malkowitz L, Siciliano SJ, Springer MS, Kwei G, Carella A, Carver G, Danzeisen R, Hazuda D, Holmes K, Kessler J, Lineberger J, Miller MD, Emini EA, and Schleif WA

Subjects

Anti-HIV Agents pharmacology, Binding Sites, CD4 Antigens metabolism, Cell Line, Drug Design, Humans, Inhibitory Concentration 50, Piperidines chemistry, Receptors, CCR5 metabolism, Stereoisomerism, Structure-Activity Relationship, Sulfones pharmacology, Anti-HIV Agents chemical synthesis, CCR5 Receptor Antagonists, Sulfones chemical synthesis

Abstract

Cellular proliferation of HIV-1 requires the cooperative assistance of both the CCR5 and CD4 receptors. Our medicinal chemistry efforts in this area have resulted in the identification of N-alkyl piperidine sulfones as CCR5 antagonists. These compounds display potent binding and show antiviral properties in HIV-1 spread cell-based assays.

Published

2004

26. Antagonists of human CCR5 receptor containing 4-(pyrazolyl)piperidine side chains. Part 3: SAR studies on the benzylpyrazole segment.

Author

Shu M, Loebach JL, Parker KA, Mills SG, Chapman KT, Shen DM, Malkowitz L, Springer MS, Gould SL, DeMartino JA, Siciliano SJ, Salvo JD, Lyons K, Pivnichny JV, Kwei GY, Carella A, Carver G, Holmes K, Schleif WA, Danzeisen R, Hazuda D, Kessler J, Lineberger J, Miller MD, and Emini EA

Subjects

Animals, Anti-HIV Agents chemical synthesis, Biological Availability, Dogs, HeLa Cells, Humans, Molecular Structure, Monocytes drug effects, Piperidines chemical synthesis, Pyrazoles pharmacokinetics, Rats, Structure-Activity Relationship, Anti-HIV Agents chemistry, Anti-HIV Agents pharmacokinetics, CCR5 Receptor Antagonists, Piperidines chemistry, Piperidines pharmacokinetics, Pyrazoles chemistry

Abstract

Extensive SAR studies in our benzylpyrazole series of CCR5 antagonists have shown that both lipophilic and hydrophilic substituents on the phenyl of the benzyl group increase antiviral potency. However, improvements in pharmacokinetic profiles were generally only observed with more lipophilic substitutions. 4-Biphenyl (51) performed the best in this regard. Highly lipophilic substituents impart undesirable ion channel activity to these CCR5 antagonists. Alkoxy substituents provide a good balance of antiviral activity, pharmacokinetic parameters, and selectivity. Compounds 42b and 42d, containing a 3,4-dimethoxy substituent, are considered the most promising improvements over parent compounds 9. They demonstrate improved antiviral activity while retaining good pharmacokinetic profile and selectivity.

Published

2004

27. Antagonists of human CCR5 receptor containing 4-(pyrazolyl)piperidine side chains. Part 2: Discovery of potent, selective, and orally bioavailable compounds.

Author

Shen DM, Shu M, Willoughby CA, Shah S, Lynch CL, Hale JJ, Mills SG, Chapman KT, Malkowitz L, Springer MS, Gould SL, DeMartino JA, Siciliano SJ, Lyons K, Pivnichny JV, Kwei GY, Carella A, Carver G, Holmes K, Schleif WA, Danzeisen R, Hazuda D, Kessler J, Lineberger J, Miller MD, and Emini EA

Subjects

Acetates chemistry, Acetates pharmacokinetics, Administration, Oral, Animals, Anti-HIV Agents chemistry, Biological Availability, Dogs, HeLa Cells, Humans, Macaca mulatta, Molecular Structure, Monocytes drug effects, Piperidines chemistry, Pyrazoles chemistry, Pyrazoles pharmacokinetics, Rats, Structure-Activity Relationship, Anti-HIV Agents chemical synthesis, Anti-HIV Agents pharmacokinetics, CCR5 Receptor Antagonists, Piperidines chemical synthesis, Piperidines pharmacokinetics

Abstract

Modifications of the alkyl acetic acid portion and the phenyl on pyrrolidine in our lead pyrazole compound 1 afforded the isopropyl compound 9. This compound is a potent CCR5 antagonist showing good in vitro antiviral activity against HIV-1, an excellent selectivity profile, and good oral bioavailability in three animal species. During this investigation, a new method for the preparation of alpha-(pyrrolidin-1-yl)-alpha,alpha-dialkyl acetic acid from a pyrrolidine and alpha-bromo-alpha,alpha-dialkyl acetic acid using silver triflate was discovered. This allowed us to prepare compounds such as 24 and 25 for the first time. A novel Pd-mediated N-dealkylation of alpha-(pyrrolidin-1-yl)acetic acid was also uncovered.

Published

2004

28. Antagonists of human CCR5 receptor containing 4-(pyrazolyl)piperidine side chains. Part 1: Discovery and SAR study of 4-pyrazolylpiperidine side chains.

Author

Shen DM, Shu M, Mills SG, Chapman KT, Malkowitz L, Springer MS, Gould SL, DeMartino JA, Siciliano SJ, Kwei GY, Carella A, Carver G, Holmes K, Schleif WA, Danzeisen R, Hazuda D, Kessler J, Lineberger J, Miller MD, and Emini EA

Subjects

Animals, Anti-HIV Agents chemistry, Cell Division drug effects, HeLa Cells, Humans, Molecular Structure, Piperidines chemistry, Pyrazoles chemistry, Pyrazoles pharmacokinetics, Rats, Structure-Activity Relationship, Anti-HIV Agents chemical synthesis, Anti-HIV Agents pharmacokinetics, CCR5 Receptor Antagonists, Piperidines chemical synthesis, Piperidines pharmacokinetics

Abstract

Replacement of the flexible connecting chains between the piperidine moiety and an aromatic group in previous CCR5 antagonists with heterocycles, such as pyrazole and isoxazole, provided potent CCR5 antagonists with excellent anti-HIV-1 activity in vitro. SAR studies revealed optimal placement of an unsubstituted nitrogen atom in the heterocycle to be meta to the bond connected to the 4-position of piperidine. Truncation of a benzyl group to a phenyl group afforded compounds with dramatically improved oral bioavailability, albeit with reduced activity.

Published

2004

29. Chemokine receptor-directed agents as novel anti-HIV-1 therapies.

Author

Mills SG and DeMartino JA

Subjects

Anti-HIV Agents chemistry, Anti-HIV Agents therapeutic use, Antibodies immunology, Antibodies pharmacology, Antibodies therapeutic use, CCR5 Receptor Antagonists, Chemokine CCL5 analogs & derivatives, Chemokines chemistry, Heterocyclic Compounds, 4 or More Rings chemistry, Heterocyclic Compounds, 4 or More Rings pharmacology, Heterocyclic Compounds, 4 or More Rings therapeutic use, Humans, Molecular Structure, Oligopeptides chemistry, Oligopeptides pharmacology, Oligopeptides therapeutic use, Receptors, CCR5 immunology, Receptors, CCR5 physiology, Receptors, CXCR4 antagonists & inhibitors, Receptors, CXCR4 immunology, Receptors, CXCR4 physiology, Anti-HIV Agents pharmacology, HIV Infections drug therapy, HIV-1 drug effects, Receptors, Chemokine antagonists & inhibitors

Abstract

Historically, therapeutic benefit in the treatment of human immunodeficiency virus infection (HIV-1) infection has been best achieved by targeting viral proteins like HIV protease involved in viral replication rather than host cell proteins, like CD4, which facilitate the process of viral infection. Two discoveries in 1996 presented a novel opportunity to redress this issue: 1) the understanding that heptahelical G-protein coupled chemokine receptors on the surface of T cells and macrophages functioned together with CD4 to mediate viral entry, and 2) the observation that CD4 positive T cells from individuals homozygous for the CCR5 delta 32 null allele were resistant to infection by macrophage-tropic strains of the virus in vitro and in vivo. Since that time, data demonstrating that selective blockade of two chemokine receptors, CCR5 and CXCR4, by small molecule chemokine receptor antagonists or receptor-directed biologics could robustly inhibit the infection of human peripheral blood mononuclear cells (PBMCs) by macrophage-tropic and T-cell line tropic strains respectively in vitro has validated this potential approach to therapy. Early clinical trial data now also confirms that these types of agents will have anti-viral activity in some HIV-1 infected individuals; however to date, dose limiting off-target activities have prohibited a full test of their potential clinical value. It also remains to be seen how these types of agents will fare in synergy with existing HIV-1 targeted antivirals, or those currently in development.

Published

2004

30. Use of a small molecule CCR5 inhibitor in macaques to treat simian immunodeficiency virus infection or prevent simian-human immunodeficiency virus infection.

Author

Veazey RS, Klasse PJ, Ketas TJ, Reeves JD, Piatak M Jr, Kunstman K, Kuhmann SE, Marx PA, Lifson JD, Dufour J, Mefford M, Pandrea I, Wolinsky SM, Doms RW, DeMartino JA, Siciliano SJ, Lyons K, Springer MS, and Moore JP

Subjects

Animals, CD4-Positive T-Lymphocytes drug effects, Simian Acquired Immunodeficiency Syndrome therapy, Simian Acquired Immunodeficiency Syndrome transmission, Valine analogs & derivatives, Anti-Retroviral Agents pharmacology, CCR5 Receptor Antagonists, Macaca mulatta virology, Pyrazoles pharmacology, Simian Acquired Immunodeficiency Syndrome drug therapy, Simian Immunodeficiency Virus drug effects, Valine pharmacology

Abstract

Human immunodeficiency virus type 1 (HIV-1) fuses with cells after sequential interactions between its envelope glycoproteins, CD4 and a coreceptor, usually CC chemokine receptor 5 (CCR5) or CXC receptor 4 (CXCR4). CMPD 167 is a CCR5-specific small molecule with potent antiviral activity in vitro. We show that CMPD 167 caused a rapid and substantial (4-200-fold) decrease in plasma viremia in six rhesus macaques chronically infected with simian immunodeficiency virus (SIV) strains SIVmac251 or SIVB670, but not in an animal infected with the X4 simian-human immunodeficiency virus (SHIV), SHIV-89.6P. In three of the SIV-infected animals, viremia reduction was sustained. In one, there was a rapid, but partial, rebound and in another, there was a rapid and complete rebound. There was a substantial delay (>21 d) between the end of therapy and the onset of full viremia rebound in two animals. We also evaluated whether vaginal administration of gel-formulated CMPD 167 could prevent vaginal transmission of the R5 virus, SHIV-162P4. Complete protection occurred in only 2 of 11 animals, but early viral replication was significantly less in the 11 CMPD 167-recipients than in 9 controls receiving carrier gel. These findings support the development of small molecule CCR5 inhibitors as antiviral therapies, and possibly as components of a topical microbicide to prevent HIV-1 sexual transmission.

Published

2003

31. Expression and characterization of the chemokine receptor CCR2B from rhesus monkey.

Author

Jin H, Vicario PP, Zweerink H, Goyal S, Hanlon WA, Dorn CP, Mills SG, DeMartino JA, Cascieri MA, and Struthers M

Subjects

Amino Acid Sequence, Animals, CHO Cells, Calcium metabolism, Cloning, Molecular, Cricetinae, Female, Flow Cytometry, Humans, Macaca mulatta, Molecular Sequence Data, Radioligand Assay, Receptors, CCR2, Receptors, Chemokine metabolism, Sequence Homology, Amino Acid, Transfection, Chemokine CCL2 metabolism, Receptors, Chemokine genetics

Abstract

Species selectivity of chemokine receptor antagonists is a potential deterrent to making preclinical assessments in vivo. To determine if rhesus monkey disease models could support these assessments, we pharmacologically and functionally characterized recombinant rhesus CCR2B receptor. For these studies we obtained the CCR2B coding region by PCR from genomic rhesus DNA and expressed the receptor as stable transfectants in Chinese Hamster Ovary cells. The surface expression of recombinant rhesus CCR2B was detected by flow cytometry using a commercially available monoclonal anti-hCCR2B antibody. This antibody was used to detect rhCCR2B on monocytes in peripheral blood mononuclear cell preparations from rhesus whole blood. The recombinantly expressed CCR2B exhibited similar high affinity binding to the CCR2 chemokine ligands from rhesus and human 125I-rhMCP-1 (K(d)=433+/-14 pM) and 125I-hMCP-1 (K(d)=550+/-256 pM). In competition binding, the receptor exhibited selective high affinity binding to the monocyte chemoattractant protein (MCP) family chemokines with little affinity for most other members of the CC family of chemokines. One exception was eotaxin, a high affinity ligand for CCR3, which bound to rhesus CCR2B receptor (K(i)=1467+/-205 pM). Chemokines which exhibited binding affinity for the receptor were tested for their ability to induce intracellular calcium release. In these experiments the relative potencies of the MCP family of chemokines for rhCCR2B were similar to the observed binding affinities. In contrast, eotaxin was functionally inactive as an antagonist or agonist to this receptor. TAK-799 (N,N-dimethyl-N-[4-[[[2-(4-methylphenyl)-6,7-dihydro-5H-benzocyclohepten-8-yl]carbonyl]amino]benzyl]tetrahydro-2H-pyran-4-aminium chloride), a dual CCR2/CCR5 antagonist, demonstrated high affinity for the rhesus CCR2B in competition with 125I-hMCP-1 binding to the receptor (K(i)=0.5 nM) and also potently blocked the MCP-1 induced calcium mobilization mediated through the receptor.

Published

2003

32. CCR5 antagonists: 3-(pyrrolidin-1-yl)propionic acid analogues with potent anti-HIV activity.

Author

Lynch CL, Hale JJ, Budhu RJ, Gentry AL, Finke PE, Caldwell CG, Mills SG, MacCoss M, Shen DM, Chapman KT, Malkowitz L, Springer MS, Gould SL, DeMartino JA, Siciliano SJ, Cascieri MA, Carella A, Carver G, Holmes K, Schleif WA, Danzeisen R, Hazuda D, Kessler J, Lineberger J, Miller M, and Emini E

Subjects

Anti-HIV Agents pharmacokinetics, Biological Availability, Propionates pharmacokinetics, Pyrrolidines pharmacokinetics, Anti-HIV Agents pharmacology, CCR5 Receptor Antagonists, Propionates pharmacology, Pyrrolidines pharmacology

Abstract

[reaction: see text] A novel approach to alpha,alpha-disubstituted-beta-amino acids (beta(2,2)-amino acids) was employed in the synthesis of a series of 3-(pyrrolidin-1-yl)propionic acids possessing high affinity for the CCR5 receptor and potent anti-HIV activity. The rat pharmacokinetics for these new analogues featured higher bioavailabilities and lower rates of clearance as compared to cyclopentane 1.

Published

2003

33. Impaired neuropathic pain responses in mice lacking the chemokine receptor CCR2.

Author

Abbadie C, Lindia JA, Cumiskey AM, Peterson LB, Mudgett JS, Bayne EK, DeMartino JA, MacIntyre DE, and Forrest MJ

Subjects

Animals, Behavior, Animal, Freund's Adjuvant pharmacology, Ganglia, Spinal metabolism, Hot Temperature, Immunohistochemistry, Macrophages metabolism, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Mice, Transgenic, Monocytes metabolism, RNA, Messenger metabolism, Receptors, CCR2, Reverse Transcriptase Polymerase Chain Reaction, Sciatic Nerve metabolism, Spinal Cord metabolism, Temperature, Time Factors, Up-Regulation, Neurons metabolism, Pain, Receptors, Chemokine genetics, Receptors, Chemokine physiology

Abstract

Mice lacking the chemokine receptor chemotactic cytokine receptor 2 (CCR2) have a marked attenuation of monocyte recruitment in response to various inflammatory stimuli and a reduction of inflammatory lesions in models of demyelinating disease. In the present study, we compared nociceptive responses in inflammatory and neuropathic models of pain in CCR2 knockout and wild-type mice. In acute pain tests, responses were equivalent in CCR2 knockout and wild-type mice. In models of inflammatory pain, CCR2 knockout mice showed a 70% reduction in phase 2 of the intraplantar formalin-evoked pain response but only a modest (20-30%) and nonsignificant reduction of mechanical allodynia after intraplantar Freund's adjuvant (CFA). In a model of neuropathic pain, the development of mechanical allodynia was totally abrogated in CCR2 knockout mice. CFA administration induced marked up-regulation of CCR2 mRNA in the skin and a moderate increase in the sciatic nerve and dorsal root ganglia (DRG). In response to nerve ligation, persistent and marked up-regulation of CCR2 mRNA was evident in the nerve and DRG. Disruption of Schwann cells in response to nerve lesion resulted in infiltration of CCR2-positive monocytes/macrophages not only to the neuroma but also to the DRG. Chronic pain also resulted in the appearance of activated CCR2-positive microglia in the spinal cord. Collectively, these data suggest that the recruitment and activation of macrophages and microglia peripherally and in neural tissue may contribute to both inflammatory and neuropathic pain states. Accordingly, blockade of the CCR2 receptor may provide a novel therapeutic modality for the treatment of chronic pain.

Published

2003

34. Antibody-mediated blockade of the CXCR3 chemokine receptor results in diminished recruitment of T helper 1 cells into sites of inflammation.

Author

Xie JH, Nomura N, Lu M, Chen SL, Koch GE, Weng Y, Rosa R, Di Salvo J, Mudgett J, Peterson LB, Wicker LS, and DeMartino JA

Subjects

Adoptive Transfer, Animals, Antibodies pharmacology, Antigens immunology, Cells, Cultured, Freund's Adjuvant, Genes, T-Cell Receptor, Hypersensitivity, Delayed immunology, Ligands, Mice, Mice, Inbred C57BL, Mice, Transgenic, Peritoneum cytology, Peritoneum drug effects, Peritoneum immunology, Peritonitis chemically induced, Peritonitis immunology, Receptors, CXCR3, Receptors, Chemokine agonists, Receptors, Chemokine immunology, Th1 Cells transplantation, Th2 Cells immunology, Chemotaxis, Leukocyte, Inflammation immunology, Receptors, Chemokine antagonists & inhibitors, Th1 Cells immunology

Abstract

Naïve T cells, when activated by specific antigen and cytokines, up-regulate adhesion molecules as well as chemokine receptors on their surface, which allows them to migrate to inflamed tissues. Human studies have shown that CXCR3 is one of the chemokine receptors that is induced during T cell activation. Moreover, CXCR3-positive T cells are enriched at inflammatory sites in patients with autoimmune diseases such as rheumatoid arthritis and multiple sclerosis. In this study, we use a mouse model of inflammation to demonstrate that CXCR3 is required for activated T cell transmigration to inflamed tissue. Using an anti- mCXCR3 antibody, we have shown that in vitro-differentiated T helper (Th) 1 and Th2 cells up-regulated CXCR3 upon stimulation with specific antigen/major histocompatibility complex. However, only Th1 cells, when adoptively transferred to syngeneic recipients, are efficiently recruited to the peritoneum in an adjuvant-induced peritonitis model. Furthermore, the neutralizing anti-mCXCR3 antibody profoundly inhibits the recruitment of Th1 cells to the inflamed peritoneum. Real-time, quantitative reverse transcriptase-polymerase chain reaction analysis demonstrates that the CXCR3 ligands, interferon (IFN)-inducible protein 10 (CXCL10) and IFN-inducible T cell alpha chemoattractant (CXCL11), are among the many chemokines induced in the adjuvant-treated peritoneum. The anti-mCXCR3 antibody is also effective in inhibiting a delayed-type hypersensitivity response, which is largely mediated by enhanced trafficking of activated T cells to peripheral inflammatory sites. Collectively, our results suggest that CXCR3 has a critical role in T cell transmigration to sites of inflammation and thus, may serve as a molecular target for anti-inflammatory therapies.

Published

2003

35. Binding of 2-aryl-4-(piperidin-1-yl)butanamines and 1,3,4-trisubstituted pyrrolidines to human CCR5: a molecular modeling-guided mutagenesis study of the binding pocket.

Author

Castonguay LA, Weng Y, Adolfsen W, Di Salvo J, Kilburn R, Caldwell CG, Daugherty BL, Finke PE, Hale JJ, Lynch CL, Mills SG, MacCoss M, Springer MS, and DeMartino JA

Subjects

Alanine genetics, Amides chemistry, Amino Acid Sequence, Amino Acid Substitution genetics, Animals, Binding Sites genetics, Binding, Competitive genetics, CHO Cells, Cattle, Cricetinae, Humans, Molecular Sequence Data, Protein Structure, Secondary genetics, Quaternary Ammonium Compounds chemistry, Receptors, CCR5 biosynthesis, Receptors, CCR5 genetics, Rhodopsin chemistry, Sequence Homology, Amino Acid, Structure-Activity Relationship, Butanes chemistry, CCR5 Receptor Antagonists, Models, Molecular, Mutagenesis, Site-Directed, Piperidines chemistry, Pyrrolidines chemistry, Receptors, CCR5 chemistry

Abstract

The results of investigations in these laboratories of 2-aryl-4-(piperidin-1-yl)butanamines and 1,3,4-trisubstituted pyrrolidines as human CCR5 antagonists have recently been disclosed. To facilitate further development of these antagonists, we have developed a pharmacophore model based on the structure-activity relationships (SAR) and a human CCR5 receptor docking model using the crystal structure of rhodopsin as a template [Palczewski, K., et al. (2000) Science 289, 739-745]. Guided by the receptor docking model, we have mapped the compounds' site of interaction with CCR5 using site-directed mutagenesis experiments. Our results are consistent with a binding site for the two series that is located within a cavity near the extracellular surface formed by transmembrane helices 2, 3, 6, and 7. This site is overlapping yet distinct from that reported for another antiviral agent which binds to CCR5 [Dragic, T., et al. (2000) Proc. Natl. Acad. Sci. U.S.A. 97, 5639-5644].

Published

2003

36. 1,3,4 Trisubstituted pyrrolidine CCR5 receptor antagonists bearing 4-aminoheterocycle substituted piperidine side chains.

Author

Willoughby CA, Rosauer KG, Hale JJ, Budhu RJ, Mills SG, Chapman KT, MacCoss M, Malkowitz L, Springer MS, Gould SL, DeMartino JA, Siciliano SJ, Cascieri MA, Carella A, Carver G, Holmes K, Schleif WA, Danzeisen R, Hazuda D, Kessler J, Lineberger J, Miller M, and Emini EA

Subjects

Animals, Anti-HIV Agents chemical synthesis, CHO Cells, Chemokine CCL4, Cricetinae, Half-Life, HeLa Cells, Humans, Hydrogen Bonding, Macrophage Inflammatory Proteins metabolism, Piperidines pharmacokinetics, Pyrrolidines pharmacokinetics, Rats, CCR5 Receptor Antagonists, Piperidines chemical synthesis, Piperidines pharmacology, Pyrrolidines chemical synthesis, Pyrrolidines pharmacology

Abstract

A new class of 4-(aminoheterocycle)piperidine derived 1,3,4 trisubstituted pyrrolidine CCR5 antagonists is reported. Compound 4a is shown to have good binding affinity (1.8 nM) and antiviral activity in PBMC's (IC(95)=50 nM). Compound 4a also has improved PK properties relative to 1.

Published

2003

37. 1,3,4-Trisubstituted pyrrolidine CCR5 receptor antagonists: modifications of the arylpropylpiperidine side chains.

Author

Lynch CL, Willoughby CA, Hale JJ, Holson EJ, Budhu RJ, Gentry AL, Rosauer KG, Caldwell CG, Chen P, Mills SG, MacCoss M, Berk S, Chen L, Chapman KT, Malkowitz L, Springer MS, Gould SL, DeMartino JA, Siciliano SJ, Cascieri MA, Carella A, Carver G, Holmes K, Schleif WA, Danzeisen R, Hazuda D, Kessler J, Lineberger J, Miller M, and Emini EA

Subjects

Animals, Anti-HIV Agents pharmacokinetics, Anti-HIV Agents pharmacology, Dogs, Half-Life, Humans, Leukocytes, Mononuclear, Macaca mulatta, Metabolic Clearance Rate, Piperidines chemistry, Pyrrolidines chemical synthesis, Pyrrolidines pharmacology, Radioligand Assay, Rats, Structure-Activity Relationship, Tumor Cells, Cultured, Anti-HIV Agents chemical synthesis, CCR5 Receptor Antagonists, Pyrrolidines pharmacokinetics

Abstract

The 4-(3-phenylprop-1-yl)piperidine moiety of the 1,3,4-trisubstituted pyrrolidine CCR5 antagonist 1 was modified with electron deficient aromatics as well as replacement of the benzylic methylene with sulfones, gem-difluoromethylenes and alcohols in an effort to balance the antiviral potency with reasonable pharmacokinetics.

Published

2003

38. 1,3,4-Trisubstituted pyrrolidine CCR5 receptor antagonists. Part 4: synthesis of N-1 acidic functionality affording analogues with enhanced antiviral activity against HIV.

Author

Lynch CL, Hale JJ, Budhu RJ, Gentry AL, Mills SG, Chapman KT, MacCoss M, Malkowitz L, Springer MS, Gould SL, DeMartino JA, Siciliano SJ, Cascieri MA, Carella A, Carver G, Holmes K, Schleif WA, Danzeisen R, Hazuda D, Kessler J, Lineberger J, Miller M, and Emini EA

Subjects

Animals, Anti-HIV Agents pharmacokinetics, CHO Cells, Cell Membrane Permeability, Chemical Phenomena, Chemistry, Physical, Chemokine CCL4, Cricetinae, HeLa Cells, Humans, Indicators and Reagents, Macrophage Inflammatory Proteins antagonists & inhibitors, Pyrrolidines pharmacokinetics, Rats, Structure-Activity Relationship, Anti-HIV Agents chemical synthesis, Anti-HIV Agents pharmacology, CCR5 Receptor Antagonists, HIV-1 drug effects, Pyrrolidines chemical synthesis, Pyrrolidines pharmacology

Abstract

A series of alpha-(pyrrolidin-1-yl)acetic acids is presented as selective and potent antivirals against HIV. Several of the pyrrolidine zwitterions demonstrated reasonable in vitro properties, enhanced antiviral activities and improved pharmacokinetic profiles over pyrrolidine 1.

Published

2002

39. 1,3,4-Trisubstituted pyrrolidine CCR5 receptor antagonists. Part 3: polar functionality and its effect on anti-HIV-1 activity.

Author

Hale JJ, Budhu RJ, Mills SG, MacCoss M, Gould SL, DeMartino JA, Springer MS, Siciliano SJ, Malkowitz L, Schleif WA, Hazuda D, Miller M, Kessler J, Danzeisen R, Holmes K, Lineberger J, Carella A, Carver G, and Emini EA

Subjects

Animals, Anti-HIV Agents pharmacokinetics, CHO Cells, Calcium Channels, L-Type drug effects, Chemical Phenomena, Chemistry, Physical, Chemokine CCL4, Cricetinae, Half-Life, HeLa Cells, Humans, Macrophage Inflammatory Proteins antagonists & inhibitors, Rats, Receptors, CCR5 chemistry, Structure-Activity Relationship, Anti-HIV Agents chemical synthesis, Anti-HIV Agents pharmacology, CCR5 Receptor Antagonists, HIV-1 drug effects

Abstract

Incorporation of acidic functional groups into a lead CCR5 antagonist identified from a targeted combinatorial library resulted in compounds with enhanced anti-HIV-1 activity and attenuated L-type calcium channel affinity.

Published

2002

40. The CXC chemokine murine monokine induced by IFN-gamma (CXC chemokine ligand 9) is made by APCs, targets lymphocytes including activated B cells, and supports antibody responses to a bacterial pathogen in vivo.

Author

Park MK, Amichay D, Love P, Wick E, Liao F, Grinberg A, Rabin RL, Zhang HH, Gebeyehu S, Wright TM, Iwasaki A, Weng Y, DeMartino JA, Elkins KL, and Farber JM

Subjects

Animals, Cell Movement, Chemokine CXCL9, Chemotaxis, Leukocyte, Mice, Mice, Inbred C57BL, RNA, Messenger analysis, Receptors, CXCR3, Receptors, Chemokine physiology, Antibodies, Bacterial biosynthesis, Antigen-Presenting Cells metabolism, B-Lymphocytes immunology, Chemokines, CXC physiology, Intercellular Signaling Peptides and Proteins, Lymphocyte Activation, T-Lymphocytes physiology

Abstract

Monokine induced by IFN-gamma (Mig; CXC chemokine ligand 9) is an IFN-gamma-inducible CXC chemokine that signals through the receptor CXCR3 and is known to function as a chemotactic factor for human T cells, particularly following T cell activation. The mig gene can be induced in multiple cell types and organs, and Mig has been shown to contribute to T cell infiltration into immune/inflammatory reactions in peripheral tissues in mice. We have investigated the expression and activities of Mig and CXCR3 in mouse cells and the role of Mig in models of host defense in mice. Murine (Mu)Mig functioned as a chemotactic factor for resting memory and activated T cells, both CD4(+) and CD8(+), and responsiveness to MuMig correlated with surface expression of MuCXCR3. Using mig(-/-) mice, we found that MuMig was not necessary for survival after infections with a number of intracellular pathogens. Surprisingly, however, we found that mig(-/-) mice showed reductions of 50-75% in Abs produced against the intracellular bacterium Francisella tularensis live vaccine strain. Furthermore, we found that MuMig induced both calcium signals and chemotaxis in activated B cells, and that B cell activation induced expression of MuCXCR3. In addition, IFN-gamma induced the expression of mumig in APCs, including CD8 alpha(+) and CD8 alpha(-) dendritic cells. Together, our data suggest that Mig and CXCR3 may be important not only to recruit T cells to peripheral inflammatory sites, but also in some cases to maximize interactions among activated T cells, B cells, and dendritic cells within lymphoid organs to provide optimal humoral responses to pathogens.

Published

2002

41. Photochemical preparation of a pyridone containing tetracycle: a Jak protein kinase inhibitor.

Author

Thompson JE, Cubbon RM, Cummings RT, Wicker LS, Frankshun R, Cunningham BR, Cameron PM, Meinke PT, Liverton N, Weng Y, and DeMartino JA

Subjects

Animals, Cell Division drug effects, DNA-Binding Proteins metabolism, Interleukin-2 antagonists & inhibitors, Interleukin-2 pharmacology, Interleukin-4 antagonists & inhibitors, Interleukin-4 pharmacology, Janus Kinase 3, Mice, Phosphorylation, Photochemistry, STAT5 Transcription Factor, Trans-Activators metabolism, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Milk Proteins, Protein-Tyrosine Kinases antagonists & inhibitors, Pyridones chemistry

Abstract

Jak3 is a protein tyrosine kinase that is associated with the shared gamma chain of receptors for cytokines IL2, IL4, IL7, IL9, and IL13. We have discovered that a pyridone-containing tetracycle (6) may be prepared from trisubstituted imidazole (5) in high yield by irradiation with >350 nm light. Compound 6 inhibits Jak3 with K(I)=5 nM; it also inhibits Jak family members Tyk2 and Jak2 with IC(50)=1 nM and murine Jak1with IC(50)=15 nM. Compound 6 was tested as an inhibitor of 21 other protein kinases; it inhibited these kinases with IC(50)s ranging from 130 nM to >10 microM. Compound 6 also blocks IL2 and IL4 dependent proliferation of CTLL cells and inhibits the phosphorylation of STAT5 (an in vivo substrate of the Jak family) as measured by Western blotting.

Published

2002

42. CCR5 antagonists: bicyclic isoxazolidines as conformationally constrained N-1-substituted pyrrolidines.

Author

Lynch CL, Gentry AL, Hale JJ, Mills SG, MacCoss M, Malkowitz L, Springer MS, Gould SL, DeMartino JA, Siciliano SJ, Cascieri MA, Doss G, Carella A, Carver G, Holmes K, Schleif WA, Danzeisen R, Hazuda D, Kessler J, Lineberger J, Miller M, and Emini EA

Subjects

Anti-HIV Agents pharmacology, Bridged Bicyclo Compounds, Heterocyclic chemical synthesis, Bridged Bicyclo Compounds, Heterocyclic chemistry, Bridged Bicyclo Compounds, Heterocyclic pharmacology, HIV-1 drug effects, Humans, Isoxazoles chemistry, Isoxazoles pharmacology, Microbial Sensitivity Tests, Molecular Conformation, Protein Binding, Pyrrolidines chemical synthesis, Pyrrolidines chemistry, Pyrrolidines pharmacology, Structure-Activity Relationship, Anti-HIV Agents chemical synthesis, CCR5 Receptor Antagonists, Isoxazoles chemical synthesis

Abstract

A series of CCR5 antagonists containing bicyclic isoxazolidines was generated through a nitrone mediated cycloaddition with olefins bearing the preferred pharmacophores previously described. Potent antagonists (3 and 16) were generated with enhanced affinity for the CCR5 receptor while maintaining antiviral activity against HIV.

Published

2002

43. Design, synthesis, and SAR of heterocycle-containing antagonists of the human CCR5 receptor for the treatment of HIV-1 infection.

Author

Kim D, Wang L, Caldwell CG, Chen P, Finke PE, Oates B, MacCoss M, Mills SG, Malkowitz L, Gould SL, DeMartino JA, Springer MS, Hazuda D, Miller M, Kessler J, Danzeisen R, Carver G, Carella A, Holmes K, Lineberger J, Schleif WA, and Emini EA

Subjects

Anti-HIV Agents chemical synthesis, Anti-HIV Agents chemistry, Anti-HIV Agents pharmacology, HIV-1 isolation & purification, HeLa Cells, Heterocyclic Compounds chemical synthesis, Heterocyclic Compounds chemistry, Heterocyclic Compounds pharmacology, Humans, Structure-Activity Relationship, Anti-HIV Agents therapeutic use, CCR5 Receptor Antagonists, HIV Infections drug therapy, Heterocyclic Compounds therapeutic use

Abstract

Replacement of the large hydantoin-indole moiety from our previous work with a variety of smaller heterocyclic analogues gave rise to potent CCR5 antagonists having binding affinity comparable to the hydantoin analogues. The synthesis, SAR, and biological profiles of this class of antagonists are described.

Published

2001

44. Discovery of human CCR5 antagonists containing hydantoins for the treatment of HIV-1 infection.

Author

Kim D, Wang L, Caldwell CG, Chen P, Finke PE, Oates B, MacCoss M, Mills SG, Malkowitz L, Gould SL, DeMartino JA, Springer MS, Hazuda D, Miller M, Kessler J, Danzeisen R, Carver G, Carella A, Holmes K, Lineberger J, Schleif WA, and Emini EA

Subjects

Anti-HIV Agents chemistry, Anti-HIV Agents pharmacology, HIV-1 isolation & purification, Humans, Hydantoins chemistry, Hydantoins pharmacology, Anti-HIV Agents therapeutic use, CCR5 Receptor Antagonists, HIV Infections drug therapy, Hydantoins therapeutic use

Abstract

A series of hydantoin derivatives has been discovered as highly potent nonpeptide antagonists for the human CCR5 receptor. The synthesis, SAR, and biological profiles of this class of antagonists are described.

Published

2001

45. 1,3,4-Trisubstituted pyrrolidine CCR5 receptor antagonists. Part 2: lead optimization affording selective, orally bioavailable compounds with potent anti-HIV activity.

Author

Hale JJ, Budhu RJ, Holson EB, Finke PE, Oates B, Mills SG, MacCoss M, Gould SL, DeMartino JA, Springer MS, Siciliano S, Malkowitz L, Schleif WA, Hazuda D, Miller M, Kessler J, Danzeisen R, Holmes K, Lineberger J, Carella A, Carver G, and Emini E

Subjects

Administration, Oral, Animals, Anti-HIV Agents chemical synthesis, Anti-HIV Agents chemistry, Anti-HIV Agents pharmacokinetics, Biological Availability, CHO Cells, Cricetinae, HeLa Cells, Humans, Microbial Sensitivity Tests, Pyrrolidines chemical synthesis, Pyrrolidines chemistry, Pyrrolidines pharmacokinetics, Structure-Activity Relationship, Anti-HIV Agents pharmacology, CCR5 Receptor Antagonists, HIV drug effects, Pyrrolidines pharmacology

Abstract

Investigations of the structure-activity relationships of 1,3,4-trisubstituted pyrrolidine human CCR5 receptor antagonists afforded orally bioavailable compounds with the ability to inhibit HIV replication in vitro.

Published

2001

46. Antagonists of the human CCR5 receptor as anti-HIV-1 agents. Part 3: a proposed pharmacophore model for 1-[N-(methyl)-N-(phenylsulfonyl)amino]-2-(phenyl)-4-[4-(substituted)piperidin-1-yl]butanes.

Author

Finke PE, Meurer LC, Oates B, Shah SK, Loebach JL, Mills SG, MacCoss M, Castonguay L, Malkowitz L, Springer MS, Gould SL, and DeMartino JA

Subjects

Animals, Anti-HIV Agents metabolism, Butanes metabolism, Cells, Cultured, Chemokine CCL4, Cricetinae, Humans, Inhibitory Concentration 50, Models, Biological, Models, Molecular, Neutrophils drug effects, Neutrophils virology, Piperidines chemistry, Structure-Activity Relationship, Anti-HIV Agents chemistry, Anti-HIV Agents pharmacology, Butanes chemistry, Butanes pharmacology, CCR5 Receptor Antagonists, Macrophage Inflammatory Proteins metabolism

Abstract

Structure-activity relationship studies directed toward the optimization of (2S)-2-(3-chlorophenyl)-1-[N-(methyl)-N-(phenylsulfonyl)amino]-4-[4-(substituted)piperidin-1-yl]butanes as CCR5 antagonists resulted in the synthesis of the spiro-indanone derivative 8c (IC50=5 nM). These and previous results are summarized in a proposed pharmacophore model for this class of CCR5 antagonist.

Published

2001

47. Antagonists of the human CCR5 receptor as anti-HIV-1 agents. Part 4: synthesis and structure-activity relationships for 1-[N-(methyl)-N-(phenylsulfonyl)amino]-2-(phenyl)-4-(4-(N-(alkyl)-N-(benzyloxycarbonyl)amino)piperidin-1-yl)butanes.

Author

Finke PE, Oates B, Mills SG, MacCoss M, Malkowitz L, Springer MS, Gould SL, DeMartino JA, Carella A, Carver G, Holmes K, Danzeisen R, Hazuda D, Kessler J, Lineberger J, Miller M, Schleif WA, and Emini EA

Subjects

Animals, Cells, Cultured, Cricetinae, Drug Design, Drug Evaluation, Preclinical, HIV-1 drug effects, Humans, Inhibitory Concentration 50, Neutrophils drug effects, Neutrophils virology, Structure-Activity Relationship, Anti-HIV Agents chemistry, Anti-HIV Agents pharmacology, Butanes chemical synthesis, Butanes chemistry, Butanes pharmacology, CCR5 Receptor Antagonists, Piperidines chemistry, Piperidines pharmacology

Abstract

(2S)-2-(3-Chlorophenyl)-1-[N-(methyl)-N-(phenylsulfonyl)amino]-4-[spiro(2,3-dihydrobenzthiophene-3,4'-piperidin-1'-yl)]butane S-oxide (1b) has been identified as a potent CCR5 antagonist having an IC50=10 nM. Herein, structure-activity relationship studies of non-spiro piperidines are described, which led to the discovery of 4-(N-(alkyl)-N-(benzyloxycarbonyl)amino)piperidine derivatives (3-5) as potent CCR5 antagonists.

Published

2001

48. 1,3,4-Trisubstituted pyrrolidine CCR5 receptor antagonists. Part 1: discovery of the pyrrolidine scaffold and determination of its stereochemical requirements.

Author

Hale JJ, Budhu RJ, Mills SG, MacCoss M, Malkowitz L, Siciliano S, Gould SL, DeMartino JA, and Springer MS

Subjects

Animals, Binding, Competitive, CHO Cells, Chemokine CCL4, Cricetinae, Iodine Radioisotopes, Macrophage Inflammatory Proteins chemistry, Macrophage Inflammatory Proteins pharmacology, Molecular Conformation, Pyrrolidines chemistry, Receptors, CCR5 genetics, Transfection, CCR5 Receptor Antagonists, Pyrrolidines pharmacology

Abstract

A series of 1,3,4-trisubstituted pyrrolidines was discovered to have the ability to displace [(125)I]-MIP-1alpha from the CCR5 receptor expressed on Chinese hamster ovary (CHO) cell membranes. CCR5 activity was found to be dependent on the regiochemistry and the absolute stereochemistry of the pyrrolidine.

Published

2001

49. CCR5, CXCR4, and CD4 are clustered and closely apposed on microvilli of human macrophages and T cells.

Author

Singer II, Scott S, Kawka DW, Chin J, Daugherty BL, DeMartino JA, DiSalvo J, Gould SL, Lineberger JE, Malkowitz L, Miller MD, Mitnaul L, Siciliano SJ, Staruch MJ, Williams HR, Zweerink HJ, and Springer MS

Subjects

Animals, CD4 Antigens genetics, Cell Line, Cells, Cultured, Fluorescent Antibody Technique, Golgi Apparatus metabolism, HIV Antibodies immunology, HIV Envelope Protein gp120 metabolism, HIV-1 physiology, Humans, Macrophages cytology, Macrophages ultrastructure, Macrophages virology, Membrane Microdomains metabolism, Membrane Microdomains ultrastructure, Microscopy, Electron, Scanning, Microscopy, Immunoelectron, Microvilli ultrastructure, Rabbits, Receptors, CCR2, Receptors, CCR5 genetics, Receptors, CXCR4 genetics, Receptors, Chemokine metabolism, Secretory Vesicles metabolism, T-Lymphocytes cytology, T-Lymphocytes ultrastructure, T-Lymphocytes virology, Thermodynamics, CD4 Antigens metabolism, HIV-1 metabolism, Macrophages metabolism, Microvilli metabolism, Receptors, CCR5 metabolism, Receptors, CXCR4 metabolism, T-Lymphocytes metabolism

Abstract

The chemokine receptors CCR5 and CXCR4 act synergistically with CD4 in an ordered multistep mechanism to allow the binding and entry of human immunodeficiency virus type 1 (HIV-1). The efficiency of such a coordinated mechanism depends on the spatial distribution of the participating molecules on the cell surface. Immunoelectron microscopy was performed to address the subcellular localization of the chemokine receptors and CD4 at high resolution. Cells were fixed, cryoprocessed, and frozen; 80-nm cryosections were double labeled with combinations of CCR5, CXCR4, and CD4 antibodies and then stained with immunogold. Surprisingly, CCR5, CXCR4, and CD4 were found predominantly on microvilli and appeared to form homogeneous microclusters in all cell types examined, including macrophages and T cells. Further, while mixed microclusters were not observed, homogeneous microclusters of CD4 and the chemokine receptors were frequently separated by distances less than the diameter of an HIV-1 virion. Such distributions are likely to facilitate cooperative interactions with HIV-1 during virus adsorption to and penetration of human leukocytes and have significant implications for development of therapeutically useful inhibitors of the entry process. Although the mechanism underlying clustering is not understood, clusters were observed in small trans-Golgi vesicles, implying that they were organized shortly after synthesis and well before insertion into the cellular membrane. Chemokine receptors normally act as sensors, detecting concentration gradients of their ligands and thus providing directional information for cellular migration during both normal homeostasis and inflammatory responses. Localization of these sensors on the microvilli should enable more precise monitoring of their environment, improving efficiency of the chemotactic process. Moreover, since selectins, some integrins, and actin are also located on or in the microvillus, this organelle has many of the major elements required for chemotaxis.

Published

2001

50. Antagonists of the human CCR5 receptor as anti-HIV-1 agents. Part 2: structure-activity relationships for substituted 2-Aryl-1-[N-(methyl)-N-(phenylsulfonyl)amino]-4-(piperidin-1-yl)butanes.

Author

Finke PE, Meurer LC, Oates B, Mills SG, MacCoss M, Malkowitz L, Springer MS, Daugherty BL, Gould SL, DeMartino JA, Siciliano SJ, Carella A, Carver G, Holmes K, Danzeisen R, Hazuda D, Kessler J, Lineberger J, Miller M, Schleif WA, and Emini EA

Subjects

Animals, Anti-HIV Agents chemistry, Anti-HIV Agents metabolism, Butanes chemical synthesis, Butanes chemistry, Butanes metabolism, Butylamines chemical synthesis, Butylamines chemistry, Butylamines metabolism, CHO Cells, Chemokine CCL4, Combinatorial Chemistry Techniques, Cricetinae, Humans, Inhibitory Concentration 50, Macrophage Inflammatory Proteins metabolism, Piperidines chemical synthesis, Piperidines chemistry, Piperidines metabolism, Protein Binding, Receptors, CCR5 genetics, Receptors, CCR5 metabolism, Structure-Activity Relationship, Sulfonamides chemical synthesis, Sulfonamides chemistry, Sulfonamides metabolism, Transfection, Anti-HIV Agents chemical synthesis, CCR5 Receptor Antagonists

Abstract

(2S)-2-(3,4-Dichlorophenyl)-1-[N-(methyl)-N-(phenylsulfonyl)amino]-4-[spiro(2,3-dihydrobenzthiophene-3,4'-piperidin-1'-yl)]butane S-oxide (3) has been identified as a potent CCR5 antagonist lead structure having an IC50 = 35 nM. Herein, we describe the structure-activity relationship studies directed toward the requirement for and optimization of the C-2 phenyl fragment. The phenyl was found to be important for CCR5 antagonism and substitution was limited to small moieties at the 3-position (13 and 16: X= H, 3-F, 3-Cl, 3-Me).

Published

2001