Your search keyword '"Elliott PJ"' showing total 104 results

1. Treating metastatic solid tumors with bortezomib and a tumor necrosis factor-related apoptosis-inducing ligand receptor agonist antibody.

Author

Shanker A, Brooks AD, Tristan CA, Wine JW, Elliott PJ, Yagita H, Takeda K, Smyth MJ, Murphy WJ, Sayers TJ, Shanker, Anil, Brooks, Alan David, Tristan, Carlos Alberto, Wine, John William, Elliott, Peter John, Yagita, Hideo, Takeda, Kazuyoshi, Smyth, Mark John, Murphy, William Joseph, and Sayers, Thomas Joseph

Abstract

Background: Resistance of tumors to cell death signals poses a complex clinical problem. We explored the therapeutic potential and in vivo toxicity of a combination of bortezomib, a proteasome inhibitor, and MD5-1, a tumor necrosis factor-related apoptosis-inducing ligand (TRAIL) receptor (DR5) agonist monoclonal antibody, in mouse carcinomas. METHODS; Mice bearing Renca-FLAG (renal) or 4T1 (mammary) tumors were treated with bortezomib and/or MD5-1 and examined for lung metastases (Renca-FLAG: n = 93; 4T1: n = 40) or monitored for survival (Renca-FLAG: n = 143). Toxicity was assessed by histopathology and hematology. Viability and apoptotic signaling in Renca-FLAG and 4T1 cells treated with bortezomib alone or in combination with TRAIL were analyzed using 3-[4,5-dimethyiazol-2-yl-5]-[3-carboxymethyloxyphenyl]-2-[4-sulfophenyl]-2H tetrazolium assay and by measuring mitochondrial membrane depolarization and caspase-8 and caspase-3 activation. All statistical tests were two-sided.Results: Bortezomib (20 nM) sensitized Renca-FLAG and 4T1 cells to TRAIL-mediated apoptosis (mean percent decrease in numbers of viable cells, bortezomib + TRAIL vs TRAIL: Renca-FLAG, 95% vs 34%, difference = 61%, 95% confidence interval [CI] = 52% to 69%, P < .001; 4T1, 85% vs 20%, difference = 65%, 95% CI = 62% to 69%, P < .001). Sensitization involved activation of caspase-8 and caspase-3 but not mitochondrial membrane depolarization, suggesting an amplified signaling of the extrinsic cell death pathway. Treatment with bortezomib and MD5-1 reduced lung metastases in mice carrying Renca and 4T1 tumors (mean number of metastases, bortezomib + MD5-1 vs MD5-1: Renca-FLAG, 1 vs 8, difference = 7, 95% CI = 5 to 9, P < .001; 4T1, 1 vs 12, difference = 11, 95% CI = 9 to 12, P < .001) and increased median survival of mice bearing Renca-FLAG tumors (bortezomib + MD5-1 vs bortezomib + control isotype antibody: 22 of 30 [73%] were still alive at day 180 vs median survival of 42 days [95% CI = 41 to 44 days, P < .001]) in the absence of obvious toxicity.Conclusion: Bortezomib combined with DR5 agonist monoclonal antibody may be a useful treatment for metastatic solid tumors. [ABSTRACT FROM AUTHOR]

Published

2008

2. The risk to the United Kingdom population of zinc cadmium sulfide dispersion by the Ministry of Defence during the "cold war".

Author

Elliott PJ, Phillips CJC, Clayton B, Lachmann PJ, Elliott, P J, Phillips, C J C, Clayton, B, and Lachmann, P J

Abstract

Objectives: To estimate exposures to cadmium (Cd) received by the United Kingdom population as a result of the dispersion of zinc Cd sulfide (ZnCdS) by the Ministry of Defence between 1953 and 1964, as a simulator of biological warfare agents.Methods: A retrospective risk assessment study was carried out on the United Kingdom population during the period 1953-64. This determined land and air dispersion of ZnCdS over most of the United Kingdom, inhalation exposure of the United Kingdom population, soil contamination, and risks to personnel operating equipment that dispersed ZnCdS.Results: About 4600 kg ZnCdS were dispersed from aircraft and ships, at times when the prevailing winds would allow large areas of the country to be covered. Cadmium released from 44 long range trials for which data are available, and extrapolated to a total of 76 trials to allow for trials with incomplete information, is about 1.2% of the estimated total release of Cd into the atmosphere over the same period. "Worst case" estimates are 10 microg Cd inhaled over 8 years, equivalent to Cd inhaled in an urban environment in 12100 days, or from smoking 100 cigarettes. A further 250 kg ZnCdS was dispersed from the land based sites, but significant soil contamination occurred only in limited areas, which were and have remained uninhabited. Of the four personnel involved in the dispersion procedures (who were probably exposed to much higher concentrations of Cd than people on the ground), none are suspected of having related illnesses.Conclusion: Exposure to Cd from dissemination of ZnCdS during the "cold war" should not have resulted in adverse health effects in the United Kingdom population. [ABSTRACT FROM AUTHOR]

Published

2002

3. Nicotinamide Improves Aspects of Healthspan, but Not Lifespan, in Mice.

Author

Mitchell SJ, Bernier M, Aon MA, Cortassa S, Kim EY, Fang EF, Palacios HH, Ali A, Navas-Enamorado I, Di Francesco A, Kaiser TA, Waltz TB, Zhang N, Ellis JL, Elliott PJ, Frederick DW, Bohr VA, Schmidt MS, Brenner C, Sinclair DA, Sauve AA, Baur JA, and de Cabo R

Subjects

Animals, Diet, High-Fat, Disease Models, Animal, Fatty Liver drug therapy, Inflammation drug therapy, Longevity, Mice, Inbred C57BL, Niacinamide administration & dosage, Oxidative Stress drug effects, Sirtuin 1 metabolism, Dietary Supplements, Healthy Aging metabolism, Liver drug effects, Liver metabolism, NAD metabolism, Niacinamide pharmacology

Abstract

The role in longevity and healthspan of nicotinamide (NAM), the physiological precursor of NAD + , is elusive. Here, we report that chronic NAM supplementation improves healthspan measures in mice without extending lifespan. Untargeted metabolite profiling of the liver and metabolic flux analysis of liver-derived cells revealed NAM-mediated improvement in glucose homeostasis in mice on a high-fat diet (HFD) that was associated with reduced hepatic steatosis and inflammation concomitant with increased glycogen deposition and flux through the pentose phosphate and glycolytic pathways. Targeted NAD metabolome analysis in liver revealed depressed expression of NAM salvage in NAM-treated mice, an effect counteracted by higher expression of de novo NAD biosynthetic enzymes. Although neither hepatic NAD + nor NADP + was boosted by NAM, acetylation of some SIRT1 targets was enhanced by NAM supplementation in a diet- and NAM dose-dependent manner. Collectively, our results show health improvement in NAM-supplemented HFD-fed mice in the absence of survival effects., (Published by Elsevier Inc.)

Published

2018

4. Phase I randomized, double-blind pilot study of micronized resveratrol (SRT501) in patients with hepatic metastases--safety, pharmacokinetics, and pharmacodynamics.

Author

Howells LM, Berry DP, Elliott PJ, Jacobson EW, Hoffmann E, Hegarty B, Brown K, Steward WP, and Gescher AJ

Subjects

Aged, Antineoplastic Agents, Phytogenic administration & dosage, Caspase 3 metabolism, Combined Modality Therapy methods, Double-Blind Method, Female, Hepatectomy methods, Humans, Male, Middle Aged, Neoplasm Metastasis, Pilot Projects, Placebos, Postoperative Complications, Resveratrol, Stilbenes administration & dosage, Titanium pharmacology, Antineoplastic Agents, Phytogenic pharmacokinetics, Antineoplastic Agents, Phytogenic pharmacology, Liver Neoplasms drug therapy, Stilbenes pharmacokinetics, Stilbenes pharmacology

Abstract

The phytochemical resveratrol has undergone extensive preclinical investigation for its putative cancer chemopreventive properties. Low systemic availability of the parent compound due to rapid and extensive metabolism may confound its usefulness as a potential agent to prevent malignancies in organs remote from the site of absorption. Micronization allows increased drug absorption, thus increasing availability. Here we describe a pilot study of SRT501, micronized resveratrol, given as 5.0 g daily for 14 days, to patients with colorectal cancer and hepatic metastases scheduled to undergo hepatectomy. The purpose of the study was to assess the safety, pharmacokinetics, and pharmacodynamics of the formulation. SRT501 was found to be well tolerated. Mean plasma resveratrol levels following a single dose of SRT501 administration were 1,942 ± 1,422 ng/mL, exceeding those published for equivalent doses of nonmicronized resveratrol by 3.6-fold. Resveratrol was detectable in hepatic tissue following SRT501 administration (up to 2,287 ng/g). Cleaved caspase-3, a marker of apoptosis, significantly increased by 39% in malignant hepatic tissue following SRT501 treatment compared with tissue from the placebo-treated patients. SRT501 warrants further clinical exploration to assess its potential clinical utility., (©2011 AACR.)

Published

2011

5. Sirt1 inhibition promotes in vivo arterial thrombosis and tissue factor expression in stimulated cells.

Author

Breitenstein A, Stein S, Holy EW, Camici GG, Lohmann C, Akhmedov A, Spescha R, Elliott PJ, Westphal CH, Matter CM, Lüscher TF, and Tanner FC

Subjects

Animals, Benzamides pharmacology, Binding Sites, Cells, Cultured, Disease Models, Animal, Dose-Response Relationship, Drug, Endothelial Cells enzymology, Enzyme Activators, Genes, Reporter, Humans, Mice, Mice, Inbred C57BL, Mice, Knockout, Mitogen-Activated Protein Kinases metabolism, Naphthalenes pharmacology, Naphthols pharmacology, Promoter Regions, Genetic, Pyrones pharmacology, RNA Interference, RNA, Messenger metabolism, Resveratrol, Sirtuin 1 deficiency, Sirtuin 1 genetics, Stilbenes pharmacology, Thromboplastin genetics, Thrombosis blood, Thrombosis enzymology, Thrombosis genetics, Transcription Factor RelA deficiency, Transcription Factor RelA genetics, Transcription Factor RelA metabolism, Transfection, Endothelial Cells drug effects, Histone Deacetylase Inhibitors pharmacology, Sirtuin 1 antagonists & inhibitors, Sirtuin 1 metabolism, Thromboplastin metabolism, Thrombosis etiology

Abstract

Aims: The mammalian silent information regulator-two 1 (Sirt1) blunts the noxious effects of cardiovascular risk factors such as type 2 diabetes mellitus and obesity. Nevertheless, the role of Sirt1 in regulating the expression of tissue factor (TF), the key trigger of coagulation, and arterial thrombus formation remains unknown., Methods and Results: Human as well as mouse cell lines were used for in vitro experiments, and C57Bl/6 mice for in vivo procedures. Sirt1 inhibition by splitomicin or sirtinol enhanced cytokine-induced endothelial TF protein expression as well as surface activity, while TF pathway inhibitor protein expression did not change. Sirt1 inhibition further enhanced TF mRNA expression, TF promoter activity, and nuclear translocation as well as DNA binding of the p65 subunit of nuclear factor-kappa B (NFκB/p65). Sirt1 siRNA enhanced TF protein and mRNA expression, and this effect was reduced in NFκB/p65(-/-) mouse embryonic fibroblasts reconstituted with non-acetylatable Lys(310)-mutant NFκB/p65. Activation of the mitogen-activated protein kinases p38, c-Jun NH(2)-terminal kinase, and p44/42 (ERK) remained unaffected. In vivo, mice treated with the Sirt1 inhibitor splitomicin exhibited enhanced TF activity in the arterial vessel wall and accelerated carotid artery thrombus formation in a photochemical injury model., Conclusion: We provide pharmacological and genetic evidence that Sirt1 inhibition enhances TF expression and activity by increasing NFκB/p65 activation in human endothelial cells. Furthermore, Sirt1 inhibition induces arterial thrombus formation in vivo. Hence, modulation of Sirt1 may offer novel therapeutic options for targeting thrombosis.

Published

2011

6. SRT1720 improves survival and healthspan of obese mice.

Author

Minor RK, Baur JA, Gomes AP, Ward TM, Csiszar A, Mercken EM, Abdelmohsen K, Shin YK, Canto C, Scheibye-Knudsen M, Krawczyk M, Irusta PM, Martín-Montalvo A, Hubbard BP, Zhang Y, Lehrmann E, White AA, Price NL, Swindell WR, Pearson KJ, Becker KG, Bohr VA, Gorospe M, Egan JM, Talan MI, Auwerx J, Westphal CH, Ellis JL, Ungvari Z, Vlasuk GP, Elliott PJ, Sinclair DA, and de Cabo R

Subjects

Animals, Apoptosis drug effects, Body Composition drug effects, Dietary Fats administration & dosage, Gene Expression drug effects, Glucose metabolism, Homeostasis drug effects, Liver drug effects, Liver pathology, Male, Mice, Mice, Inbred C57BL, Pancreas drug effects, Heterocyclic Compounds, 4 or More Rings pharmacology, Longevity drug effects, Obesity physiopathology

Abstract

Sirt1 is an NAD(+)-dependent deacetylase that extends lifespan in lower organisms and improves metabolism and delays the onset of age-related diseases in mammals. Here we show that SRT1720, a synthetic compound that was identified for its ability to activate Sirt1 in vitro, extends both mean and maximum lifespan of adult mice fed a high-fat diet. This lifespan extension is accompanied by health benefits including reduced liver steatosis, increased insulin sensitivity, enhanced locomotor activity and normalization of gene expression profiles and markers of inflammation and apoptosis, all in the absence of any observable toxicity. Using a conditional SIRT1 knockout mouse and specific gene knockdowns we show SRT1720 affects mitochondrial respiration in a Sirt1- and PGC-1α-dependent manner. These findings indicate that SRT1720 has long-term benefits and demonstrate for the first time the feasibility of designing novel molecules that are safe and effective in promoting longevity and preventing multiple age-related diseases in mammals.

Published

2011

7. AMPK regulates energy expenditure by modulating NAD+ metabolism and SIRT1 activity.

Author

Cantó C, Gerhart-Hines Z, Feige JN, Lagouge M, Noriega L, Milne JC, Elliott PJ, Puigserver P, and Auwerx J

Subjects

Acetylation, Aminoimidazole Carboxamide analogs & derivatives, Animals, Cell Line, Enzyme Activation, Forkhead Box Protein O1, Forkhead Box Protein O3, Forkhead Transcription Factors genetics, Gene Expression Regulation, Genes, Mitochondrial genetics, Male, Mice, Muscle, Skeletal cytology, Muscle, Skeletal enzymology, Muscle, Skeletal metabolism, Mutation, Oxygen Consumption, Peroxisome Proliferator-Activated Receptor Gamma Coactivator 1-alpha, Phosphorylation, Ribonucleotides, Sirtuin 1, Trans-Activators genetics, Trans-Activators metabolism, Transcription Factors, Transcription, Genetic, AMP-Activated Protein Kinases metabolism, Energy Metabolism genetics, NAD metabolism, Sirtuins metabolism

Abstract

AMP-activated protein kinase (AMPK) is a metabolic fuel gauge conserved along the evolutionary scale in eukaryotes that senses changes in the intracellular AMP/ATP ratio. Recent evidence indicated an important role for AMPK in the therapeutic benefits of metformin, thiazolidinediones and exercise, which form the cornerstones of the clinical management of type 2 diabetes and associated metabolic disorders. In general, activation of AMPK acts to maintain cellular energy stores, switching on catabolic pathways that produce ATP, mostly by enhancing oxidative metabolism and mitochondrial biogenesis, while switching off anabolic pathways that consume ATP. This regulation can take place acutely, through the regulation of fast post-translational events, but also by transcriptionally reprogramming the cell to meet energetic needs. Here we demonstrate that AMPK controls the expression of genes involved in energy metabolism in mouse skeletal muscle by acting in coordination with another metabolic sensor, the NAD+-dependent type III deacetylase SIRT1. AMPK enhances SIRT1 activity by increasing cellular NAD+ levels, resulting in the deacetylation and modulation of the activity of downstream SIRT1 targets that include the peroxisome proliferator-activated receptor-gamma coactivator 1alpha and the forkhead box O1 (FOXO1) and O3 (FOXO3a) transcription factors. The AMPK-induced SIRT1-mediated deacetylation of these targets explains many of the convergent biological effects of AMPK and SIRT1 on energy metabolism.

Published

2009

8. Small molecule activators of SIRT1 replicate signaling pathways triggered by calorie restriction in vivo.

Author

Smith JJ, Kenney RD, Gagne DJ, Frushour BP, Ladd W, Galonek HL, Israelian K, Song J, Razvadauskaite G, Lynch AV, Carney DP, Johnson RJ, Lavu S, Iffland A, Elliott PJ, Lambert PD, Elliston KO, Jirousek MR, Milne JC, and Boss O

Subjects

Animals, Enzyme Activation drug effects, Gene Expression Profiling, Heterocyclic Compounds, 4 or More Rings chemistry, Heterocyclic Compounds, 4 or More Rings pharmacology, Mice, Microarray Analysis, Molecular Structure, Resveratrol, Signal Transduction drug effects, Sirtuin 1, Stilbenes chemistry, Stilbenes pharmacology, Caloric Restriction, Enzyme Activation genetics, Models, Genetic, Signal Transduction genetics, Sirtuins metabolism

Abstract

Background: Calorie restriction (CR) produces a number of health benefits and ameliorates diseases of aging such as type 2 diabetes. The components of the pathways downstream of CR may provide intervention points for developing therapeutics for treating diseases of aging. The NAD+-dependent protein deacetylase SIRT1 has been implicated as one of the key downstream regulators of CR in yeast, rodents, and humans. Small molecule activators of SIRT1 have been identified that exhibit efficacy in animal models of diseases typically associated with aging including type 2 diabetes. To identify molecular processes induced in the liver of mice treated with two structurally distinct SIRT1 activators, SIRT501 (formulated resveratrol) and SRT1720, for three days, we utilized a systems biology approach and applied Causal Network Modeling (CNM) on gene expression data to elucidate downstream effects of SIRT1 activation., Results: Here we demonstrate that SIRT1 activators recapitulate many of the molecular events downstream of CR in vivo, such as enhancing mitochondrial biogenesis, improving metabolic signaling pathways, and blunting pro-inflammatory pathways in mice fed a high fat, high calorie diet., Conclusion: CNM of gene expression data from mice treated with SRT501 or SRT1720 in combination with supporting in vitro and in vivo data demonstrates that SRT501 and SRT1720 produce a signaling profile that mirrors CR, improves glucose and insulin homeostasis, and acts via SIRT1 activation in vivo. Taken together these results are encouraging regarding the use of small molecule activators of SIRT1 for therapeutic intervention into type 2 diabetes, a strategy which is currently being investigated in multiple clinical trials.

Published

2009

9. Specific SIRT1 activation mimics low energy levels and protects against diet-induced metabolic disorders by enhancing fat oxidation.

Author

Feige JN, Lagouge M, Canto C, Strehle A, Houten SM, Milne JC, Lambert PD, Mataki C, Elliott PJ, and Auwerx J

Subjects

Acetylation, Animals, Diet, Dietary Fats administration & dosage, Energy Metabolism, Heterocyclic Compounds, 4 or More Rings therapeutic use, Insulin Resistance physiology, Male, Metabolic Diseases drug therapy, Mice, Mice, Inbred C57BL, Motor Activity drug effects, Obesity drug therapy, Oxidation-Reduction, Physical Conditioning, Animal, Sirtuin 1, Sirtuins agonists, Sirtuins genetics, Heterocyclic Compounds, 4 or More Rings pharmacology, Lipid Metabolism drug effects, Metabolic Diseases metabolism, Obesity metabolism, Sirtuins metabolism

Abstract

The NAD(+)-dependent deacetylase SIRT1 controls metabolic processes in response to low nutrient availability. We report the metabolic phenotype of mice treated with SRT1720, a specific and potent synthetic activator of SIRT1 that is devoid of direct action on AMPK. SRT1720 administration robustly enhances endurance running performance and strongly protects from diet-induced obesity and insulin resistance by enhancing oxidative metabolism in skeletal muscle, liver, and brown adipose tissue. These metabolic effects of SRT1720 are mediated by the induction of a genetic network controlling fatty acid oxidation through a multifaceted mechanism that involves the direct deacetylation of PGC-1alpha, FOXO1, and p53 and the indirect stimulation of AMPK signaling through a global metabolic adaptation mimicking low energy levels. Combined with our previous work on resveratrol, the current study further validates SIRT1 as a target for the treatment of metabolic disorders and characterizes the mechanisms underlying the therapeutic potential of SIRT1 activation.

Published

2008

10. Sirtuins--novel therapeutic targets to treat age-associated diseases.

Author

Lavu S, Boss O, Elliott PJ, and Lambert PD

Subjects

Aging drug effects, Animals, Caloric Restriction methods, Cardiovascular Diseases enzymology, Diabetes Mellitus, Type 2 enzymology, Drug Delivery Systems methods, Humans, Neoplasms enzymology, Sirtuins agonists, Aging metabolism, Cardiovascular Diseases drug therapy, Diabetes Mellitus, Type 2 drug therapy, Drug Delivery Systems trends, Neoplasms drug therapy, Sirtuins metabolism

Abstract

Sirtuins post-translationally modulate the function of many cellular proteins that undergo reversible acetylation-deacetylation cycles, affecting physiological responses that have implications for treating diseases of ageing. Potent small-molecule modulators of sirtuins have shown efficacy in preclinical models of metabolic, neurodegenerative and inflammatory diseases, and so hold promise for drug discovery efforts in multiple therapeutic areas. Here, we discuss current knowledge and data that strengthens sirtuins as a druggable set of enzymes for the treatment of age-associated diseases, including activation of SIRT1 in type 2 diabetes.

Published

2008

11. Resveratrol delays age-related deterioration and mimics transcriptional aspects of dietary restriction without extending life span.

Author

Pearson KJ, Baur JA, Lewis KN, Peshkin L, Price NL, Labinskyy N, Swindell WR, Kamara D, Minor RK, Perez E, Jamieson HA, Zhang Y, Dunn SR, Sharma K, Pleshko N, Woollett LA, Csiszar A, Ikeno Y, Le Couteur D, Elliott PJ, Becker KG, Navas P, Ingram DK, Wolf NS, Ungvari Z, Sinclair DA, and de Cabo R

Subjects

Age Factors, Aging genetics, Aging metabolism, Animals, Antioxidants pharmacology, Antioxidants therapeutic use, Apoptosis drug effects, Apoptosis physiology, Cardiovascular System drug effects, Cardiovascular System physiopathology, Food Deprivation physiology, Food, Formulated, Gene Expression Regulation drug effects, Gene Expression Regulation genetics, Inflammation drug therapy, Inflammation prevention & control, Longevity genetics, Male, Mice, Mice, Inbred C57BL, Osteoporosis drug therapy, Osteoporosis prevention & control, Resveratrol, Stilbenes therapeutic use, Transcription, Genetic genetics, Treatment Outcome, Aging drug effects, Caloric Restriction, Energy Intake genetics, Longevity drug effects, Stilbenes pharmacology, Transcription, Genetic drug effects

Abstract

A small molecule that safely mimics the ability of dietary restriction (DR) to delay age-related diseases in laboratory animals is greatly sought after. We and others have shown that resveratrol mimics effects of DR in lower organisms. In mice, we find that resveratrol induces gene expression patterns in multiple tissues that parallel those induced by DR and every-other-day feeding. Moreover, resveratrol-fed elderly mice show a marked reduction in signs of aging, including reduced albuminuria, decreased inflammation, and apoptosis in the vascular endothelium, increased aortic elasticity, greater motor coordination, reduced cataract formation, and preserved bone mineral density. However, mice fed a standard diet did not live longer when treated with resveratrol beginning at 12 months of age. Our findings indicate that resveratrol treatment has a range of beneficial effects in mice but does not increase the longevity of ad libitum-fed animals when started midlife.

Published

2008

12. Sirtuins: novel targets for metabolic disease.

Author

Elliott PJ and Jirousek M

Subjects

Base Sequence, Diabetes Mellitus, Type 2 drug therapy, Diabetes Mellitus, Type 2 enzymology, Energy Metabolism drug effects, Enzyme Activators chemistry, Enzyme Activators pharmacology, Enzyme Inhibitors pharmacology, Humans, Metabolic Diseases enzymology, Molecular Sequence Data, Molecular Structure, Obesity drug therapy, Obesity enzymology, Resveratrol, Sirtuin 1, Sirtuins genetics, Sirtuins metabolism, Stilbenes chemistry, Stilbenes pharmacology, Enzyme Activators therapeutic use, Metabolic Diseases drug therapy, Sirtuins agonists, Stilbenes therapeutic use

Abstract

Sirtuins represent a novel family of enzymes that are collectively well situated to help regulate nutrient sensing and utilization, metabolic rate and ultimately metabolic disease. Activation of one of these enzymes, SIRT1, leads to enhanced activity of multiple proteins, including peroxisome-proliferator activated receptor coactivator-1alpha (PGC-1alpha), which helps to mediate some of the in vitro and in vivo effects of sirtuins. As such, enhanced SIRT1 activity decreases glucose levels, improves insulin sensitivity, increases mitochondrial number and function, decreases adiposity, improves exercise tolerance and potentially lowers body weight. SRT-501 is a proprietary formulation of resveratrol with improved bioavailability. As such, SRT-501 represents the first in a novel class of SIRT1 activators that has proven to be safe and well-tolerated in humans. Clinical trials in type 2 diabetic patients are currently underway.

Published

2008

13. Effects of prednisolone on the systemic release of mediators of cell-mediated cytotoxicity during human endotoxemia.

Author

de Kruif MD, Lemaire LC, Giebelen IA, Groot AP, Pater JM, van den Pangaart PS, Elliott PJ, and van der Poll T

Subjects

Administration, Oral, Adult, Chemokine CXCL10 blood, Chemokine CXCL9 blood, Cytotoxicity, Immunologic immunology, Dose-Response Relationship, Drug, Endotoxemia blood, Granzymes blood, Humans, Injections, Intravenous, Killer Cells, Natural cytology, Killer Cells, Natural immunology, Lipopolysaccharides administration & dosage, Lipopolysaccharides pharmacology, Male, Prednisolone administration & dosage, T-Lymphocytes cytology, T-Lymphocytes, Cytotoxic cytology, T-Lymphocytes, Cytotoxic immunology, Cytotoxicity, Immunologic drug effects, Endotoxemia immunology, Prednisolone pharmacology, T-Lymphocytes immunology

Abstract

Corticosteroids are widely used for the suppression of cell-mediated cytoxicity. This process is mediated by natural killer cells and cytotoxic T lymphocytes, and their activation can be monitored by levels of the chemokines CXCL9 and CXCL10, the degranulation product granzymes A and B, and by levels of secretory phospholipase A2. The current study aimed to determine the effects of increasing doses of prednisolone on the release of these mediators in healthy humans exposed to LPS. Therefore, 32 healthy men received prednisolone orally at doses of 0, 3, 10, or 30 mg (n = 8 per group) at 2 h before intravenous injection of Escherichia coil LPS (4 ng/kg). Prednisolone dose-dependently attenuated the LPS-induced rises in the plasma concentrations of the chemokines CXCL9 and CXCL10, as well as of granzymes A and B levels. CXCL10 and granzyme B release were most sensitive to prednisolone, with a significant inhibition already achieved at the lowest prednisolone dose (3 mg). The levels of secretory phospholipase A2 were increased after LPS administration but were not significantly affected by prednisolone. This study demonstrates that prednisolone differentially inhibits the systemic release of mediators involved in cell-mediated cytotoxicity in humans in vivo.

Published

2008

14. The influence of corticosteroids on the release of novel biomarkers in human endotoxemia.

Author

de Kruif MD, Lemaire LC, Giebelen IA, Struck J, Morgenthaler NG, Papassotiriou J, Elliott PJ, and van der Poll T

Subjects

Administration, Oral, Adrenomedullin blood, Adult, Arginine Vasopressin blood, Atrial Natriuretic Factor blood, Biomarkers blood, Calcitonin blood, Calcitonin Gene-Related Peptide, Dose-Response Relationship, Drug, Endotoxemia chemically induced, Humans, Inflammation Mediators blood, Injections, Intravenous, Lipopolysaccharides pharmacology, Male, Prednisolone blood, Prednisolone pharmacokinetics, Prospective Studies, Sepsis blood, Sepsis drug therapy, Severity of Illness Index, Endotoxemia blood, Endotoxemia drug therapy, Peptide Hormones blood, Prednisolone pharmacology, Protein Precursors blood

Abstract

Objective: Sepsis intervention studies need better patient stratification methods, and one way to realize this is the introduction of stable biomarkers. A set of recently developed novel biomarkers, based upon precursor-fragments of short-lived hormones, was previously shown to be increased during sepsis. However, it is not known whether these biomarkers are influenced by sepsis intervention strategies. Therefore we investigated the markers in a model of human endotoxemia intervened by increasing doses of prednisolone., Design and Setting: Prospective, open-label study in a specialized clinical research unit of a university hospital., Subjects: Thirty-two healthy male volunteers., Interventions: Subjects received prednisolone orally at doses of 0, 3, 10 or 30 mg (n=8 per group) at 2 h before intravenous injection of Escherichia coli lipopolysaccharide (LPS) (4 ng/kg). Blood samples were drawn during 24 h after LPS injection., Measurements and Results: LPS injection caused an increase in levels of midregional pro-adrenomedullin (MR-proADM), midregional pro-atrial natriuretic peptide (MR-proANP), C-terminal pro-arginine-vasopressin (CT-proAVP) and procalcitonin (PCT). Prednisolone caused a dose dependent inhibition of MR-proADM, MR-proANP and CT-proAVP levels., Conclusions: These results show that a set of novel, highly stable sepsis biomarkers was increased during human endotoxemia and was dose-dependently inhibited by corticosteroid pre-treatment.

Published

2008

15. Small molecule activators of SIRT1 as therapeutics for the treatment of type 2 diabetes.

Author

Milne JC, Lambert PD, Schenk S, Carney DP, Smith JJ, Gagne DJ, Jin L, Boss O, Perni RB, Vu CB, Bemis JE, Xie R, Disch JS, Ng PY, Nunes JJ, Lynch AV, Yang H, Galonek H, Israelian K, Choy W, Iffland A, Lavu S, Medvedik O, Sinclair DA, Olefsky JM, Jirousek MR, Elliott PJ, and Westphal CH

Subjects

Acetylation, Allosteric Site, Animals, Blood Glucose metabolism, Catalytic Domain, Cell Line, Dietary Fats administration & dosage, Dietary Fats pharmacology, Disease Models, Animal, Drosophila melanogaster, Heterocyclic Compounds, 4 or More Rings pharmacology, Heterocyclic Compounds, 4 or More Rings therapeutic use, Humans, Insulin metabolism, Insulin pharmacology, Male, Mice, Mitochondria drug effects, Mitochondria metabolism, Rats, Rats, Sprague-Dawley, Rats, Zucker, Resveratrol, Sirtuin 1, Sirtuins metabolism, Stilbenes chemistry, Stilbenes pharmacology, Caloric Restriction, Diabetes Mellitus, Type 2 drug therapy, Sirtuins agonists

Abstract

Calorie restriction extends lifespan and produces a metabolic profile desirable for treating diseases of ageing such as type 2 diabetes. SIRT1, an NAD+-dependent deacetylase, is a principal modulator of pathways downstream of calorie restriction that produce beneficial effects on glucose homeostasis and insulin sensitivity. Resveratrol, a polyphenolic SIRT1 activator, mimics the anti-ageing effects of calorie restriction in lower organisms and in mice fed a high-fat diet ameliorates insulin resistance, increases mitochondrial content, and prolongs survival. Here we describe the identification and characterization of small molecule activators of SIRT1 that are structurally unrelated to, and 1,000-fold more potent than, resveratrol. These compounds bind to the SIRT1 enzyme-peptide substrate complex at an allosteric site amino-terminal to the catalytic domain and lower the Michaelis constant for acetylated substrates. In diet-induced obese and genetically obese mice, these compounds improve insulin sensitivity, lower plasma glucose, and increase mitochondrial capacity. In Zucker fa/fa rats, hyperinsulinaemic-euglycaemic clamp studies demonstrate that SIRT1 activators improve whole-body glucose homeostasis and insulin sensitivity in adipose tissue, skeletal muscle and liver. Thus, SIRT1 activation is a promising new therapeutic approach for treating diseases of ageing such as type 2 diabetes.

Published

2007

16. Prednisolone dose-dependently influences inflammation and coagulation during human endotoxemia.

Author

de Kruif MD, Lemaire LC, Giebelen IA, van Zoelen MA, Pater JM, van den Pangaart PS, Groot AP, de Vos AF, Elliott PJ, Meijers JC, Levi M, and van der Poll T

Subjects

Adult, Biomarkers blood, Chemokines blood, Cytokines blood, Cytokines drug effects, Dose-Response Relationship, Drug, Endothelial Cells drug effects, Escherichia coli, Fibrinolysis drug effects, Humans, Lipopolysaccharides administration & dosage, Male, Neutrophil Activation drug effects, Prednisolone pharmacology, Blood Coagulation drug effects, Endotoxemia drug therapy, Endotoxemia pathology, Inflammation drug therapy, Prednisolone administration & dosage

Abstract

The effects of steroids on the outcome of sepsis are dose dependent. Low doses appear to be beneficial, but high doses do not improve outcome for reasons that are insufficiently understood. The effects of steroids on systemic inflammation as a function of dose have not previously been studied in humans. To determine the effects of increasing doses of prednisolone on inflammation and coagulation in humans exposed to LPS, 32 healthy males received prednisolone orally at doses of 0, 3, 10, or 30 mg (n = 8 per group) at 2 h before i.v. injection of Escherichia coli LPS (4 ng/kg). Prednisolone dose-dependently inhibited the LPS-induced release of cytokines (TNF-alpha and IL-6) and chemokines (IL-8 and MCP-1), while enhancing the release of the anti-inflammatory cytokine IL-10. Prednisolone attenuated neutrophil activation (plasma elastase levels) and endothelial cell activation (von Willebrand factor). Most remarkably, prednisolone did not inhibit LPS-induced coagulation activation, measured by plasma concentrations of thrombin-antithrombin complexes, prothrombin fragment F1+2, and soluble tissue factor. In addition, activation of the fibrinolytic pathway (tissue-type plasminogen activator and plasmin-alpha(2)-antiplasmin complexes) was dose-dependently enhanced by prednisolone. These data indicate that prednisolone dose-dependently and differentially influences the systemic activation of different host response pathways during human endotoxemia.

Published

2007

17. The proteasome inhibitor bortezomib (Velcade) sensitizes some human tumor cells to Apo2L/TRAIL-mediated apoptosis.

Author

Brooks AD, Ramirez T, Toh U, Onksen J, Elliott PJ, Murphy WJ, and Sayers TJ

Subjects

Bortezomib, Cell Line, Tumor, Dose-Response Relationship, Drug, Humans, Ligands, TNF-Related Apoptosis-Inducing Ligand, Tumor Suppressor Protein p53 metabolism, bcl-2-Associated X Protein metabolism, Antineoplastic Agents pharmacology, Apoptosis, Apoptosis Regulatory Proteins metabolism, Boronic Acids pharmacology, Membrane Glycoproteins metabolism, Neoplasms metabolism, Proteasome Inhibitors, Pyrazines pharmacology, Tumor Necrosis Factor-alpha metabolism

Abstract

On testing a panel of different human cancer cell lines, we observed that the proteasome inhibitor bortezomib could dramatically sensitize some lines to the apoptotic effects of Apo2L/TRAIL. Certain renal, colon, or breast tumor cell lines were dramatically sensitized, whereas other tumor lines from the same tissue of origin remained resistant. This sensitization did not correlate with either the p53 status of the individual tumor cell lines or their intrinsic sensitivity to Apo2L/TRAIL. Colon cancer cell lines lacking p53 or Bax were sensitized by bortezomib, suggesting that neither p53 nor Bax levels were crucial for sensitization. Although the molecular basis of bortezomib sensitization of tumor cells to Apo2L/TRAIL remains to be determined, this combination can have an enhanced apoptotic effect over either agent alone for certain human cancer cells.

Published

2005

18. The proteasome inhibitor PS-341 sensitizes neoplastic cells to TRAIL-mediated apoptosis by reducing levels of c-FLIP.

Author

Sayers TJ, Brooks AD, Koh CY, Ma W, Seki N, Raziuddin A, Blazar BR, Zhang X, Elliott PJ, and Murphy WJ

Subjects

Animals, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Apoptosis Regulatory Proteins, Bone Marrow Purging, Boronic Acids therapeutic use, Bortezomib, CASP8 and FADD-Like Apoptosis Regulating Protein, Carrier Proteins analysis, Disease-Free Survival, Drug Synergism, Membrane Glycoproteins therapeutic use, Mice, Neoplasms, Experimental drug therapy, Neoplasms, Experimental pathology, Protease Inhibitors pharmacology, Protease Inhibitors therapeutic use, Pyrazines therapeutic use, TNF-Related Apoptosis-Inducing Ligand, Transplantation, Isogeneic, Treatment Outcome, Tumor Cells, Cultured, Tumor Necrosis Factor-alpha therapeutic use, Antineoplastic Combined Chemotherapy Protocols pharmacology, Apoptosis drug effects, Boronic Acids pharmacology, Carrier Proteins drug effects, Intracellular Signaling Peptides and Proteins, Membrane Glycoproteins pharmacology, Pyrazines pharmacology, Tumor Necrosis Factor-alpha pharmacology

Abstract

Because of the pivotal role the proteasome plays in apoptosis, inhibitors of this enzyme, such as PS-341, provide a great opportunity for exploring synergy between proteasome inhibition and other apoptosis-inducing agents. Tumor necrosis factor-related apoptosis-inducing ligand (TRAIL) can selectively induce apoptosis in tumor cells. In overnight assays, combinations of PS-341 and TRAIL were much more effective than either agent alone in promoting apoptosis of a murine myeloid leukemia, C1498, and a murine renal cancer, Renca. For C1498 cells, apoptosis sensitization by PS-341 affected neither the activity of nuclear factor kappaB (NF-kappaB) nor the levels of most antiapoptotic proteins. However, reductions in the antiapoptotic protein c-FLIP in response to PS-341 were observed in both C1498 and Renca cells. Treatment of normal bone marrow mixed with C1498 tumor cells for 18 hours with a combination of PS-341 and TRAIL resulted in a specific depletion of the tumor cells. Upon transfer to irradiated syngeneic recipient mice, mixtures treated with the PS-341 plus TRAIL combination resulted in enhanced long-term tumor-free survival of mice. These data therefore support the targeting of apoptotic pathways in tumor cells, using combinations of agents such as PS-341 and TRAIL that interact synergistically to preferentially promote tumor cell apoptosis.

Published

2003

19. Systematic discovery of multicomponent therapeutics.

Author

Borisy AA, Elliott PJ, Hurst NW, Lee MS, Lehar J, Price ER, Serbedzija G, Zimmermann GR, Foley MA, Stockwell BR, and Keith CT

Subjects

Animals, Automation, Candida albicans metabolism, Cell Division, Colony-Forming Units Assay, Cytokines metabolism, DNA, Complementary metabolism, Dose-Response Relationship, Drug, Drug Design, Drug Resistance, Microbial, Enzyme-Linked Immunosorbent Assay, Fluconazole pharmacology, Humans, Interferon-gamma metabolism, Mice, Neoplasm Transplantation, Neoplasms drug therapy, RNA metabolism, Tumor Cells, Cultured, Tumor Necrosis Factor-alpha metabolism, Antifungal Agents pharmacology, Drug Evaluation, Preclinical methods, Drug Screening Assays, Antitumor methods

Abstract

Multicomponent therapies, originating through deliberate mixing of drugs in a clinical setting, through happenstance, and through rational design, have a successful history in a number of areas of medicine, including cancer, infectious diseases, and CNS disorders. We have developed a high-throughput screening method for identifying effective combinations of therapeutic compounds. We report here that systematic screening of combinations of small molecules reveals unexpected interactions between compounds, presumably due to interactions between the pathways on which they act. Through systematic screening of approximately 120,000 different two-component combinations of reference-listed drugs, we identified potential multicomponent therapeutics, including (i) fungistatic and analgesic agents that together generate fungicidal activity in drug-resistant Candida albicans, yet do not significantly affect human cells, (ii) glucocorticoid and antiplatelet agents that together suppress the production of tumor necrosis factor-alpha in human primary peripheral blood mononu-clear cells, and (iii) antipsychotic and antiprotozoal agents that do not exhibit significant antitumor activity alone, yet together prevent the growth of tumors in mice. Systematic combination screening may ultimately be useful for exploring the connectivity of biological pathways and, when performed with reference-listed drugs, may result in the discovery of new combination drug regimens.

Published

2003

20. Proteasome inhibition: a new anti-inflammatory strategy.

Author

Elliott PJ, Zollner TM, and Boehncke WH

Subjects

Acetylcysteine therapeutic use, Animals, Antineoplastic Agents therapeutic use, Arthritis, Rheumatoid drug therapy, Asthma drug therapy, Boronic Acids therapeutic use, Bortezomib, Clinical Trials as Topic, Cysteine Endopeptidases, Disease Models, Animal, Humans, Inflammation drug therapy, Lysine chemistry, Models, Biological, Models, Chemical, Multiple Sclerosis drug therapy, NF-kappa B metabolism, Neoplasms drug therapy, Peptides chemistry, Protease Inhibitors therapeutic use, Proteasome Endopeptidase Complex, Psoriasis drug therapy, Pyrazines therapeutic use, Reperfusion Injury, Acetylcysteine analogs & derivatives, Anti-Inflammatory Agents therapeutic use, Multienzyme Complexes antagonists & inhibitors

Abstract

The ubiquitin-proteasome pathway has a central role in the selective degradation of intracellular proteins. Among the key proteins modulated by the proteasome are those involved in the control of inflammatory processes, cell cycle regulation, and gene expression. Consequently proteasome inhibition is a potential treatment option for cancer and inflammatory conditions. Thus far, proof of principle has been obtained from studies in numerous animal models for a variety of human diseases including cancer, reperfusion injury, and inflammatory conditions such as rheumatoid arthritis, asthma, multiple sclerosis, and psoriasis. Two proteasome inhibitors, each representing a unique chemical class, are currently under clinical evaluation. Velcade (PS-341) is currently being evaluated in multiple phase II clinical trials for several solid tumor indications and has just entered a phase III trial for multiple myeloma. PS-519, representing another class of inhibitors, focuses on the inflammatory events following ischemia and reperfusion injury. Since proteasome inhibitors exhibit anti-inflammatory and antiproliferative effects, diseases characterized by both of these processes simultaneously, as is the case in rheumatoid arthritis or psoriasis, might also represent clinical opportunities for such drugs.

Published

2003

21. Proteasome inhibition ablates activation of NF-kappa B in myocardial reperfusion and reduces reperfusion injury.

Author

Pye J, Ardeshirpour F, McCain A, Bellinger DA, Merricks E, Adams J, Elliott PJ, Pien C, Fischer TH, Baldwin AS Jr, and Nichols TC

Subjects

Animals, Creatine Kinase blood, Creatine Kinase, MB Form, Cysteine Endopeptidases, Disease Models, Animal, Enzyme Inhibitors pharmacology, Female, Isoenzymes blood, Male, Myocardial Ischemia drug therapy, Myocardial Ischemia physiopathology, Myocardial Reperfusion, NF-kappa B antagonists & inhibitors, Proteasome Endopeptidase Complex, Swine, Troponin I blood, Acetylcysteine analogs & derivatives, Acetylcysteine pharmacology, Multienzyme Complexes antagonists & inhibitors, Myocardial Reperfusion Injury prevention & control, Myocardium metabolism, NF-kappa B metabolism

Abstract

Both acute coronary occlusion and reperfusion of an infarct-related artery lead to significant myocardial cell death. Recent evidence has been presented that activation of the transcription factor nuclear factor-kappaB (NF-kappaB) plays a critical role in reperfusion injury. NF-kappaB is usually bound to its inhibitor, IkappaB, and classic activation of NF-kappaB occurs when the 20S proteasome degrades IkappaB that has been phosphorylated and ubiquitinated. In this study, activation of NF-kappaB was inhibited by systemic administration of a 20S proteasome inhibitor (PS-519) in a porcine model of myocardial reperfusion injury. The experimental protocol induced myocardial ischemia in the distribution of the left anterior descending coronary artery for 1 h with subsequent reperfusion for 3 h. A single systemic treatment with PS-519 reduced 20S proteasome activity; blocked activation of NF-kappaB induced by reperfusion; reduced creatine kinase, creatine kinase-muscle-brain fraction, and troponin I release from the myocardium; preserved regional myocardial function measured by segmental shortening; significantly reduced the size of myocardial infarction; and exhibited no acute toxicity. These data show that myocardial reperfusion injury can be inhibited by using proteasome inhibitors, which likely function through the inhibition of NF-kappaB activation.

Published

2003

22. Mechanisms of proteasome inhibitor PS-341-induced G(2)-M-phase arrest and apoptosis in human non-small cell lung cancer cell lines.

Author

Ling YH, Liebes L, Jiang JD, Holland JF, Elliott PJ, Adams J, Muggia FM, and Perez-Soler R

Subjects

Blotting, Western, Bortezomib, Cell Cycle, Cell Division, Cyclin-Dependent Kinase Inhibitor p21, Cyclins metabolism, Cysteine Endopeptidases, Dose-Response Relationship, Drug, G2 Phase, Humans, Immunohistochemistry, Microtubules metabolism, Mitosis, Mutation, Precipitin Tests, Protease Inhibitors pharmacology, Proteasome Endopeptidase Complex, Time Factors, Tumor Cells, Cultured, Tumor Suppressor Protein p53 metabolism, Up-Regulation, Apoptosis, Boronic Acids pharmacology, Carcinoma, Non-Small-Cell Lung pathology, Lung Neoplasms pathology, Multienzyme Complexes antagonists & inhibitors, Pyrazines pharmacology

Abstract

Purpose: PS-341 is a novel dipeptide boronic acid proteasome inhibitor with in vitro and in vivo antitumor activity that induces mechanisms of apoptosis by unknown mechanisms., Experimental Design: Human non-small cell lung cancer cell lines were used to investigate effects PS-341 on cell proliferation, cell cycle progression, and the induction of apoptosis., Results: PS-341 was 38-360-fold more cytotoxic against H460 cells when compared with the proteasome inhibitors MG-132 and PSI. Differential PS-341 cytotoxic effects were found with respect to P53 function: H322 cells (p53 mutant) were 6-fold less sensitive as compared with H460 cells (p53 wild type); and H358 cells (p53 null) were 1.6-fold more sensitive as compared with H460 cells (p53 wild type). A concentration- and time-dependent cell cycle blockade at G(2)-M phase was seen for H460 cells without any direct effects on microtubule polymerization or depolymerization. PS-341 exposure in H460 cells led to stabilization of p53, induction of p21(cip/waf-1) and MDM2 expression, an increase in cyclin B and cyclin A, and the activation of cyclin B and cyclin A kinases. MDM2 induction was found only in H460 cells, whereas in H322 and H358 cells, G(2)-M-phase arrest, p21(cip/waf-1) induction, and an increase in cyclin B1 were found. The commitment of G(2)-M-phase cells to apoptosis was verified by the activation of caspase-3 and cleavage of poly(ADP-ribose) polymerase in drug-free medium., Conclusions: Our data suggest that the PS-341-induced G(2)-M-phase arrest may be associated with the inhibition of degradation of cell cycle regulators and that the up-regulation of p21(cip/waf-1) expression may be via p53-dependent and/or -independent pathways. The resulting disturbance of cell cycle progression leads either to growth inhibition or to the initiation of apoptotic pathways.

Published

2003

23. Delayed treatment with MLN519 reduces infarction and associated neurologic deficit caused by focal ischemic brain injury in rats via antiinflammatory mechanisms involving nuclear factor-kappaB activation, gliosis, and leukocyte infiltration.

Author

Williams AJ, Hale SL, Moffett JR, Dave JR, Elliott PJ, Adams J, and Tortella FC

Subjects

Animals, Astrocytes pathology, Brain Ischemia metabolism, Cell Movement physiology, Cysteine Endopeptidases metabolism, Gliosis pathology, Inflammation Mediators metabolism, Leukocytes physiology, Male, Multienzyme Complexes metabolism, NF-kappa B physiology, Nerve Degeneration etiology, Proteasome Endopeptidase Complex, Rats, Rats, Sprague-Dawley, Recovery of Function, Acetylcysteine analogs & derivatives, Acetylcysteine pharmacology, Brain Ischemia complications, Infarction, Middle Cerebral Artery etiology, Infarction, Middle Cerebral Artery pathology, Nervous System Diseases etiology, Nervous System Diseases physiopathology

Abstract

Secondary brain injury due to ischemia includes the infiltration of leukocytes into the brain parenchyma mediated by activation of nuclear factor-kappaB (NF-kappaB), which is activated by proteasome degradation. Neuroprotection with the proteasome inhibitor MLN519 has previously been reported to decrease ischemic brain injury in rats. The authors used higher doses of MLN519 to evaluate the neuroprotection therapeutic window after 24 hours of brain injury in rats as correlated to proteasome levels, activated NF-kappaB immunoreactivity, and leukocyte infiltration. Male Sprague-Dawley rats were subjected to 2-hour middle cerebral artery occlusion (MCAO) and recovery. MLN519 or vehicle was administered after injury with a single injection given in delayed increments of 2 hours (i.e., 4, 6, or 8 hours after MCAO). Treatment with MLN519 up to 6 hours after MCAO (4 hours after reperfusion) effectively reduced neuronal and astrocytic degeneration, decreased cortical infarct volume, and increased neurologic recovery. These effects were related to >80% reductions in blood proteasome levels, reduced neutrophil infiltration, and a decrease in activated NF-kappaB immunoreactivity. This improved neuroprotection profile and antiinflammatory effect of MLN519 provides an exciting avenue for potential treatment of focal ischemic brain injury in humans.

Published

2003

24. Assays for proteasome inhibition.

Author

Elliott PJ, Soucy TA, Pien CS, Adams J, and Lightcap ES

Subjects

Antineoplastic Agents blood, Clinical Trials as Topic, Cysteine Endopeptidases blood, Drug Screening Assays, Antitumor, Fluorometry, Humans, Leukocytes drug effects, Leukocytes enzymology, Multienzyme Complexes blood, Neoplasm Proteins metabolism, Protease Inhibitors blood, Proteasome Endopeptidase Complex, Reproducibility of Results, Antineoplastic Agents pharmacology, Multienzyme Complexes antagonists & inhibitors, Protease Inhibitors pharmacology

Published

2003

25. Effect of the proteasome inhibitor MLN519 on the expression of inflammatory molecules following middle cerebral artery occlusion and reperfusion in the rat.

Author

Berti R, Williams AJ, Velarde LC, Moffett JR, Elliott PJ, Adams J, Yao C, Dave JR, and Tortella FC

Subjects

Animals, Cell Adhesion Molecules metabolism, Cytokines biosynthesis, DNA chemistry, DNA genetics, DNA isolation & purification, Gene Expression Regulation drug effects, Immunohistochemistry, Infarction, Middle Cerebral Artery drug therapy, Inflammation genetics, Kinetics, Male, NF-kappa B metabolism, Proteasome Endopeptidase Complex, RNA, Messenger biosynthesis, RNA, Messenger isolation & purification, Rats, Rats, Sprague-Dawley, Reverse Transcriptase Polymerase Chain Reaction, Acetylcysteine analogs & derivatives, Acetylcysteine pharmacology, Cysteine Endopeptidases drug effects, Infarction, Middle Cerebral Artery pathology, Inflammation metabolism, Middle Cerebral Artery physiology, Multienzyme Complexes drug effects, Neuroprotective Agents pharmacology, Reperfusion Injury drug therapy, Reperfusion Injury metabolism

Abstract

Anti-inflammatory treatment with the proteasome inhibitor MLN519 has been previously reported to be neuroprotective against ischemic brain injury in rats. These effects have been related to inhibition of the transcription factor NF-kappaB, which is activated through ubiquitin-proteasomal degradation. The aim of this study was to evaluate the effects of MLN519 to alter the expression of several inflammatory genes under the control of NF-kappaB. Male Sprague-Dawley rats underwent middle cerebral artery occlusion (MCAo) followed by vehicle or MLN519 (1.0 g/kg, i.v.) treatment immediately after reperfusion of blood to the brain at 2h. Gene expression was evaluated 3-72 h post-MCAo. The most striking effects of intravenous treatment with MLN519 were associated with reductions in ICAM-1 expression at 3 h followed by reductions in E-selectin (12-72 h). Less dramatic reductions were observed in IL-1Beta (3-24 h) and TNF-Alpha (24 h) with no apparent effects on IL-6 and VCAM-1 mRNA levels. Immunohistochemical analysis revealed that the genes most dramatically affected by MLN519 had highest expression in endothelial cells and leukocytes (E-selectin, ICAM-1),indicating that these cell types may be the primary targets of intravenously delivered MLN519 treatment.

Published

2003

26. Phase I trial of the proteasome inhibitor PS-341 in patients with refractory hematologic malignancies.

Author

Orlowski RZ, Stinchcombe TE, Mitchell BS, Shea TC, Baldwin AS, Stahl S, Adams J, Esseltine DL, Elliott PJ, Pien CS, Guerciolini R, Anderson JK, Depcik-Smith ND, Bhagat R, Lehman MJ, Novick SC, O'Connor OA, and Soignet SL

Subjects

Adult, Aged, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Boronic Acids chemistry, Boronic Acids pharmacology, Bortezomib, Cysteine Endopeptidases, Drug Administration Schedule, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Female, Hematologic Neoplasms pathology, Humans, Male, Middle Aged, Proteasome Endopeptidase Complex, Pyrazines chemistry, Pyrazines pharmacology, Treatment Outcome, United States, Antineoplastic Agents administration & dosage, Antineoplastic Agents adverse effects, Boronic Acids administration & dosage, Boronic Acids adverse effects, Enzyme Inhibitors administration & dosage, Enzyme Inhibitors adverse effects, Hematologic Neoplasms drug therapy, Multienzyme Complexes antagonists & inhibitors, Pyrazines administration & dosage, Pyrazines adverse effects

Abstract

Purpose: To determine the maximum-tolerated dose (MTD), dose-limiting toxicity (DLT), and pharmacodynamics (PD) of the proteasome inhibitor bortezomib (previously known as PS-341) in patients with refractory hematologic malignancies., Patients and Methods: Patients received PS-341 twice weekly for 4 weeks at either 0.40, 1.04, 1.20, or 1.38 mg/m(2), followed by a 2-week rest. The PD of PS-341 was evaluated by measurement of whole blood 20S proteasome activity., Results: Twenty-seven patients received 293 doses of PS-341, including 24 complete cycles. DLTs at doses above the 1.04-mg/m(2) MTD attributed to PS-341 included thrombocytopenia, hyponatremia, hypokalemia, fatigue, and malaise. In three of 10 patients receiving additional therapy, serious reversible adverse events appeared during cycle 2, including one episode of postural hypotension, one systemic hypersensitivity reaction, and grade 4 transaminitis in a patient with hepatitis C and a substantial acetaminophen ingestion. PD studies revealed PS-341 induced 20S proteasome inhibition in a time-dependent manner, and this inhibition was also related to both the dose in milligrams per meter squared, and the absolute dose of PS-341. Among nine fully assessable patients with heavily pretreated plasma cell dyscrasias completing one cycle of therapy, there was one complete response and a reduction in paraprotein levels and/or marrow plasmacytosis in eight others. In addition, one patient with mantle cell lymphoma and another with follicular lymphoma had shrinkage of nodal disease., Conclusion: PS-341 was well tolerated at 1.04 mg/m(2) on this dose-intensive schedule, although patients need to be monitored for electrolyte abnormalities and late toxicities. Additional studies are indicated to determine whether incorporation of dose/body surface area yields a superior PD model to dosing without normalization. PS-341 showed activity against refractory multiple myeloma and possibly non-Hodgkin's lymphoma in this study, and merits further investigation in these populations.

Published

2002

27. Early clinical experience with the novel proteasome inhibitor PS-519.

Author

Shah IM, Lees KR, Pien CP, and Elliott PJ

Subjects

Acetylcysteine pharmacokinetics, Bilirubin metabolism, Blood Pressure drug effects, Cysteine Endopeptidases, Double-Blind Method, Electrocardiography drug effects, Heart Rate drug effects, Humans, Leukocyte Count, Male, Neutrophils drug effects, Proteasome Endopeptidase Complex, Acetylcysteine adverse effects, Acetylcysteine analogs & derivatives, Multienzyme Complexes antagonists & inhibitors

Abstract

Aims: The main objective of this study was to investigate the safety, tolerability and pharmacodynamics of the novel proteasome inhibitor PS-519 in young male volunteers. Many pro-inflammatory mediators such as cytokines and cell adhesion molecules that are responsible for the development of the cerebral infarct are under the control of the transcription factor Nuclear Factor kappa-B (NF-kappaB). The activity of NF-kappaB is itself tightly regulated through the multicatalytic enzyme known as the proteasome. PS-519 is a novel and highly selective small molecule that inhibits the proteasome. An ex vivo assay of 20S proteasome activity allows monitoring of the drug effect in blood. PS-519 is protective in multiple animal models of cerebral ischaemia over a range of doses that achieve 20S inhibition of 40%-80%., Methods: PS-519 has been administered to healthy male volunteers as single and repeated doses up to 1.6 mg m(-2). It was given as an intravenous bolus over 20-30 s in a double blind, randomized, placebo-controlled phase I study, examining vital signs, safety, tolerability and blood 20S proteasome inhibition., Results: Thirty-nine subjects received single doses of 0.012 mg m-2-1.6 mg m(-2) and 28 subjects received doses of 0.5 mg m(-2)-1.6 mg m(-2) on three consecutive days. The drug was well tolerated. There was no clear treatment-emergent symptom or abnormality of laboratory tests. Proteasome inhibition in blood samples as measured by 20S assay achieved the intended maximum target level of 70-80% with 1.6 mg m(-2), and was reproducible with repeated dosing., Conclusions: This study has demonstrated that proteasome inhibition is well tolerated by healthy subjects at levels that are maximally neuroprotective in experimental conditions. Further clinical evaluation appears justified.

Published

2002

28. Quantitative real-time RT-PCR analysis of inflammatory gene expression associated with ischemia-reperfusion brain injury.

Author

Berti R, Williams AJ, Moffett JR, Hale SL, Velarde LC, Elliott PJ, Yao C, Dave JR, and Tortella FC

Subjects

Animals, Base Sequence, Corpus Striatum immunology, Corpus Striatum pathology, DNA Primers, E-Selectin genetics, Ischemic Attack, Transient physiopathology, Male, Middle Cerebral Artery, RNA, Messenger genetics, Rats, Rats, Sprague-Dawley, Reperfusion Injury physiopathology, Reverse Transcriptase Polymerase Chain Reaction, Gene Expression Regulation, Inflammation genetics, Intercellular Adhesion Molecule-1 genetics, Interleukin-6 genetics, Ischemic Attack, Transient genetics, Reperfusion Injury genetics, Tumor Necrosis Factor-alpha genetics, Vascular Cell Adhesion Molecule-1 genetics

Abstract

Ischemia-reperfusion brain injury initiates an inflammatory response involving the expression of adhesion molecules and cytokines, some of which are regulated by the nuclear transcription factor NF-kappaB. In this study the authors examined mRNA expression levels for several important genes associated with inflammation at five time points (3, 6, 12, 24, and 72 hours) after transient middle cerebral artery occlusion (MCAO) in Sprague-Dawley rats. A sensitive and quantitative technique (TaqMan real-time QRT-PCR) was used to simultaneously measure mRNA levels for key cell adhesion molecules and inflammatory cytokines. Gene expression increased significantly in the injured hemisphere for interleukin (IL)-1beta (12-fold increase at 24 hours), IL-6 (25-fold increase at 6 hours) and ICAM-1 (4-fold increase at 24 hours), and the interhemispheric differences for these genes were significant for every time point examined (P < 0.05 for all values). Tumor necrosis factor-alpha mRNA was upregulated in the injured versus uninjured hemisphere from 3 to 24 hours (5-fold increase at 6 hours), while E-selectin showed a significant increase in mRNA levels from 6 to 24 hours after MCAO (10-fold increase at 6 hours) (P < 0.05 for all values). VCAM-1 mRNA levels did not respond differentially to injury at any time point between the two brain hemispheres. At all time points examined, activated NF-kappaB immunoreactivity was observed in cells throughout the infarct-damaged tissue. These results are consistent with the proinflammatory properties of the induced molecules, which are involved in the initiation of the inflammatory cascade, and may thus contribute to secondary cellular responses that lead to further brain damage.

Published

2002

29. A phase I trial of the novel proteasome inhibitor PS341 in advanced solid tumor malignancies.

Author

Aghajanian C, Soignet S, Dizon DS, Pien CS, Adams J, Elliott PJ, Sabbatini P, Miller V, Hensley ML, Pezzulli S, Canales C, Daud A, and Spriggs DR

Subjects

Adult, Aged, Antineoplastic Agents toxicity, Boronic Acids toxicity, Bortezomib, Cysteine Endopeptidases metabolism, Dose-Response Relationship, Drug, Female, Follow-Up Studies, Humans, Male, Middle Aged, Multienzyme Complexes metabolism, Proteasome Endopeptidase Complex, Pyrazines toxicity, Signal Transduction, Time Factors, Antineoplastic Agents pharmacokinetics, Antineoplastic Agents therapeutic use, Boronic Acids pharmacokinetics, Boronic Acids therapeutic use, Multienzyme Complexes antagonists & inhibitors, Neoplasms drug therapy, Pyrazines pharmacokinetics, Pyrazines therapeutic use

Abstract

Purpose: The purpose of this study was to evaluate the toxicity and pharmacodynamic behavior of the novel proteasome inhibitor PS341 administered as a twice weekly i.v. bolus for 2 weeks, followed by a 1-week recovery period in patients with advanced solid tumor malignancies., Experimental Design: In this Phase I trial, 43 patients were treated with PS341 in doses ranging from 0.13 to 1.56 mg/m2/dose. A standard Phase I design was used. Pharmacodynamic studies were performed to access 20S proteasome activity., Results: Forty-three patients were treated with 89 cycles of PS341. Patients were heavily pretreated. Dose-limiting toxicities on this schedule were diarrhea and sensory neurotoxicity. Other side effects seen were fatigue, fever, anorexia, nausea, vomiting, rash, pruritus, and headache. There was no dose-limiting hematological toxicity. A dose-related inhibition of 20S proteasome activity with increasing dose of PS341 was seen. There was one major response in a patient with refractory non-small cell lung carcinoma., Conclusions: Given the results of this trial, it is safe and reasonable to recommend treatment with PS341 on the schedule used in this trial at 1.56 mg/m2/dose in Phase II trials. Particular care should be taken with patients with preexisting neuropathy. Further testing in Phase II trials is warranted.

Published

2002

30. PS-341, a novel proteasome inhibitor, induces Bcl-2 phosphorylation and cleavage in association with G2-M phase arrest and apoptosis.

Author

Ling YH, Liebes L, Ng B, Buckley M, Elliott PJ, Adams J, Jiang JD, Muggia FM, and Perez-Soler R

Subjects

Amino Acid Chloromethyl Ketones pharmacology, Blotting, Western, Bortezomib, Cell Line, Cysteine Endopeptidases, DNA Fragmentation, Flow Cytometry, G2 Phase, Humans, Mitosis, Models, Biological, Phosphorylation, Proteasome Endopeptidase Complex, Subcellular Fractions metabolism, Time Factors, Tosylphenylalanyl Chloromethyl Ketone pharmacology, Tumor Cells, Cultured, Antineoplastic Agents pharmacology, Apoptosis, Boronic Acids pharmacology, Multienzyme Complexes antagonists & inhibitors, Protease Inhibitors pharmacology, Proto-Oncogene Proteins c-bcl-2 metabolism, Pyrazines pharmacology, Tosylphenylalanyl Chloromethyl Ketone analogs & derivatives

Abstract

Treatment with the proteasome inhibitor, PS-341 resulted in concentration- and time-dependent effects on Bcl-2 phosphorylation and cleavage in H460 cells that coincided with the PS-341-induced G2-M phase arrest. The observed Bcl-2 cleavage paralleled the degree of PS-341-induced apoptosis but was detected to a similar extent with comparable concentrations of two other proteasome inhibitors (MG-132 and PSI). Calpain inhibitors, ALLM and ALLN, and the caspase inhibitors, Z-VAD and AC-YVAD did not induce BcI-2 phosphorylation and cleavage. Exposure to PS-341 resulted in an additional Mr 25,000 cleavage fragment of Bcl-2, whereas only a Mr 23,000 fragment was observed with other anticancer agents. The formation of the Mr 25,000 fragment was not prevented by caspase inhibitors unlike the Mr 23,000 fragment, which suggests mediation by a caspase-independent pathway. Cell fractionation studies revealed that the Bcl-2 cleaved fragments localize within membrane structures and was an early event (at approximately 12 h, posttreatment), and before the observed cleavage of poly(ADP-ribose) polymerase (PARP), beta-catenin, and DNA fragmentation (at approximately 36 h posttreatment). The Mr 23,000 Bcl-2 cleavage product was inhibited by the pan-caspase inhibitor and the inhibitors of capase-3, -8, -9; but the PARP cleavage was prevented only by the pan-caspase and caspase-3 inhibitors, which suggests that the Mr 23,000 Bcl-2 cleavage occurred at both the initiation and execution stages of apoptosis. The inhibition of the ubiquitin/proteasome pathway by PS-341 leads, at an early stage of apoptosis, to Bcl-2 phosphorylation and a unique proteolytic cleavage product, which are associated with G2-M phase arrest and the induction of apoptosis.

Published

2002

31. Proteasome inhibition reduces superantigen-mediated T cell activation and the severity of psoriasis in a SCID-hu model.

Author

Zollner TM, Podda M, Pien C, Elliott PJ, Kaufmann R, and Boehncke WH

Subjects

Acetylcysteine pharmacology, Animals, Antigens, CD metabolism, Antigens, Differentiation, T-Lymphocyte metabolism, Cysteine Endopeptidases, Cysteine Proteinase Inhibitors pharmacology, DNA drug effects, DNA metabolism, Disease Models, Animal, Enterotoxins immunology, HLA-DR Antigens metabolism, Humans, Lectins, C-Type, Lymphocyte Activation drug effects, Mice, Mice, SCID, NF-kappa B metabolism, Proteasome Endopeptidase Complex, Psoriasis drug therapy, Psoriasis enzymology, Psoriasis pathology, Receptors, Interleukin-2 metabolism, Skin Transplantation immunology, T-Lymphocytes drug effects, Transplantation, Heterologous, Acetylcysteine analogs & derivatives, Bacterial Toxins, Multienzyme Complexes antagonists & inhibitors, Psoriasis immunology, Superantigens metabolism, T-Lymphocytes immunology

Abstract

There is increasing evidence that bacterial superantigens contribute to inflammation and T cell responses in psoriasis. Psoriatic inflammation entails a complex series of inductive and effector processes that require the regulated expression of various proinflammatory genes, many of which require NF-kappa B for maximal trans-activation. PS-519 is a potent and selective proteasome inhibitor based upon the naturally occurring compound lactacystin, which inhibits NF-kappa B activation by blocking the degradation of its inhibitory protein I kappa B. We report that proteasome inhibition by PS-519 reduces superantigen-mediated T cell-activation in vitro and in vivo. Proliferation was inhibited along with the expression of very early (CD69), early (CD25), and late T cell (HLA-DR) activation molecules. Moreover, expression of E-selectin ligands relevant to dermal T cell homing was reduced, as was E-selectin binding in vitro. Finally, PS-519 proved to be therapeutically effective in a SCID-hu xenogeneic psoriasis transplantation model. We conclude that inhibition of the proteasome, e.g., by PS-519, is a promising means to treat T cell-mediated disorders such as psoriasis.

Published

2002

32. Postischemic (6-Hour) treatment with recombinant human tissue plasminogen activator and proteasome inhibitor PS-519 reduces infarction in a rat model of embolic focal cerebral ischemia.

Author

Zhang L, Zhang ZG, Zhang RL, Lu M, Adams J, Elliott PJ, and Chopp M

Subjects

Animals, Behavior, Animal drug effects, Blood Pressure drug effects, Body Weight drug effects, Brain Ischemia complications, Brain Ischemia metabolism, Brain Ischemia pathology, Cell Count, Cerebral Hemorrhage etiology, Cerebral Hemorrhage pathology, Cerebral Hemorrhage prevention & control, Cerebral Infarction etiology, Cerebral Infarction pathology, Cysteine Endopeptidases, Cysteine Proteinase Inhibitors administration & dosage, Disease Models, Animal, Drug Administration Schedule, Drug Therapy, Combination, Fibrinolytic Agents administration & dosage, Fibrinolytic Agents adverse effects, Humans, Intracranial Embolism complications, Intracranial Embolism pathology, Male, Multienzyme Complexes antagonists & inhibitors, Neurologic Examination, Peroxidase metabolism, Proteasome Endopeptidase Complex, Rats, Rats, Wistar, Recombinant Proteins administration & dosage, Recombinant Proteins adverse effects, Time Factors, Tissue Plasminogen Activator adverse effects, Acetylcysteine administration & dosage, Acetylcysteine analogs & derivatives, Brain Ischemia drug therapy, Cerebral Infarction prevention & control, Intracranial Embolism drug therapy, Tissue Plasminogen Activator administration & dosage

Abstract

Background and Purpose: The proteasome inhibitor PS-519 blocks activation of nuclear factor-kappaB, a major mediator of inflammation. We tested the hypothesis that combination treatment of recombinant human tissue plasminogen activator (rhtPA) and PS-519 extends the therapeutic window for treatment of stroke with rhtPA without increasing incidence of hemorrhagic transformation., Methods: The middle cerebral artery (MCA) of male Wistar rats (n=56) was occluded by an embolus. After embolization, animals were randomly divided into the following groups: PS-519 treatment groups: PS-519 was given at 2, 4, or 6 hours after MCA occlusion; rhtPA treatment groups: rhtPA was given at 2 or 4 hours after MCA occlusion; combination treatment groups: PS-519 and rhtPA were given at 2, 4, or 6 hours after MCA occlusion; control group: the same volume of saline was given at 2 hours after MCA occlusion., Results: Administration of PS-519 alone at 2 or 4 hours, but not 6 hours, significantly (P<0.05) reduced infarct volume and improved neurological recovery compared with the control group. Administration of rhtPA alone at 2 hours, but not 4 hours, significantly (P<0.05) reduced infarct volume and improved neurological recovery compared with the control group. Furthermore, combination treatment with rhtPA and PS-519 even at 6 hours significantly (P<0.05) reduced infarct volume, improved neurological recovery, and did not increase the incidence of hemorrhagic transformation compared with the control group or the group treated with PS-519 alone., Conclusions: Our data suggest that combination treatment with PS-519 and rhtPA extends the neuroprotective effect to at least 6 hours after embolization.

Published

2001

33. The proteasome: a new target for novel drug therapies.

Author

Elliott PJ and Ross JS

Subjects

Acetylcysteine pharmacokinetics, Animals, Antineoplastic Agents pharmacokinetics, Boronic Acids pharmacokinetics, Bortezomib, Carcinoma, Lewis Lung drug therapy, Carcinoma, Lewis Lung enzymology, Clinical Trials, Phase I as Topic, Cysteine Endopeptidases, Cysteine Proteinase Inhibitors pharmacokinetics, Disease Models, Animal, Humans, Neoplasms enzymology, Proteasome Endopeptidase Complex, Pyrazines pharmacokinetics, Acetylcysteine analogs & derivatives, Acetylcysteine therapeutic use, Antineoplastic Agents therapeutic use, Boronic Acids therapeutic use, Cysteine Proteinase Inhibitors therapeutic use, Multienzyme Complexes antagonists & inhibitors, Neoplasms drug therapy, Pyrazines therapeutic use

Abstract

The proteasome is an enzyme present in all cells, from yeast to human, and has a central role in the proteolytic degradation of the vast majority of intracellular proteins. Among the key proteins modulated by the proteasome are those involved in controlling inflammatory processes, cell cycle regulation, and gene expression. As such, agents that inhibit the proteasome have been shown to be active in numerous animal models of inflammation and cancer Two proteasome inhibitors are under clinical evaluation. PS-519 is being studied for the treatment of reperfusion injury that occurs following cerebral ischemia and myocardial infarction. The other, PS-341, has recently entered multiple phase 2 clinical trials for the treatment of multiple myeloma, chronic lymphocytic leukemia, and a variety of solid tumors. The proteasome may have an important role in the evolution of HIV-related disorders including AIDS and inflammatory disorders. Therapeutic strategies using proteasome inhibitors for the treatment of these conditions have now entered preclinical development.

Published

2001

34. Enhanced chemosensitivity to CPT-11 with proteasome inhibitor PS-341: implications for systemic nuclear factor-kappaB inhibition.

Author

Cusack JC Jr, Liu R, Houston M, Abendroth K, Elliott PJ, Adams J, and Baldwin AS Jr

Subjects

Animals, Apoptosis drug effects, Boronic Acids administration & dosage, Bortezomib, Camptothecin administration & dosage, Colorectal Neoplasms drug therapy, Colorectal Neoplasms pathology, Cysteine Endopeptidases, Dose-Response Relationship, Drug, Drug Synergism, Enzyme Inhibitors administration & dosage, Female, Humans, Irinotecan, Mice, Mice, Nude, Multienzyme Complexes antagonists & inhibitors, Proteasome Endopeptidase Complex, Pyrazines administration & dosage, Tumor Cells, Cultured, Xenograft Model Antitumor Assays, Antineoplastic Combined Chemotherapy Protocols pharmacology, Boronic Acids pharmacology, Camptothecin analogs & derivatives, Camptothecin pharmacology, Enzyme Inhibitors pharmacology, NF-kappa B antagonists & inhibitors, Pyrazines pharmacology

Abstract

Inducible activation of nuclear factor-kappaB (NF-kappaB) inhibits the apoptotic response to chemotherapy and irradiation. Activation of NF-kappaB via phosphorylation of an inhibitor protein IkappaB leads to degradation of IkappaB through the ubiquitin-proteasome pathway. We hypothesized that inactivation of proteasome function will inhibit inducible NF-kappaB activation, thereby increasing levels of apoptosis in response to chemotherapy and enhancing antitumor effects. To assess the effects of proteasome inhibition on chemotherapy response, human colorectal cancer cells were pretreated with the dipeptide boronic acid analogue PS-341 (1 microM) prior to exposure to SN-38, the active metabolite of the topoisomerase I inhibitor, CPT-11. Inducible activation of NF-kappaB and growth response were evaluated in vitro and in vivo. Effects on p53, p21, p27 and apoptosis were determined. Pretreatment with PS-341 inhibited activation of NF-kappaB induced by SN-38 and resulted in a significantly higher level of growth inhibition (64-75%) compared with treatment with PS-341 alone (20-30%) or SN-38 alone (24-47%; P < 0.002). Combination therapy resulted in a 94% decrease in tumor size compared with the control group and significantly improved tumoricidal response to treatment compared with all treatment groups (P = 0.02). The level of apoptosis was 80-90% in the treatment group that received combination treatment compared with treatment with single agent alone (10%). Proteasome inhibition blocks chemotherapy-induced NF-kappaB activation, leading to a dramatic augmentation of chemosensitivity and enhanced apoptosis. Combining proteasome inhibition with chemotherapy has significant potential to overcome the high incidence of chemotherapy resistance. Clinical studies are currently in development to evaluate the role of proteasome inhibition as an important adjuvant to systemic chemotherapy.

Published

2001

35. 26S proteasome inhibition induces apoptosis and limits growth of human pancreatic cancer.

Author

Shah SA, Potter MW, McDade TP, Ricciardi R, Perugini RA, Elliott PJ, Adams J, and Callery MP

Subjects

Adenocarcinoma drug therapy, Adenocarcinoma pathology, Adenocarcinoma physiopathology, Animals, Antineoplastic Combined Chemotherapy Protocols pharmacology, Apoptosis physiology, Boronic Acids metabolism, Bortezomib, Camptothecin analogs & derivatives, Camptothecin pharmacology, Cell Cycle drug effects, Cell Division drug effects, Cyclin-Dependent Kinase Inhibitor p21, Cyclins metabolism, Dipeptides metabolism, Dipeptides pharmacology, Drug Resistance, Neoplasm, Humans, Irinotecan, Mice, Mice, Nude, Mitogens administration & dosage, Pancreatic Neoplasms physiopathology, Peptide Hydrolases metabolism, Protease Inhibitors pharmacology, Pyrazines metabolism, Tumor Cells, Cultured, Xenograft Model Antitumor Assays methods, Antineoplastic Agents pharmacology, Apoptosis drug effects, Boronic Acids pharmacology, Cyclins drug effects, NF-kappa B antagonists & inhibitors, Pancreatic Neoplasms drug therapy, Pancreatic Neoplasms pathology, Peptide Hydrolases drug effects, Proteasome Endopeptidase Complex, Pyrazines pharmacology

Abstract

The 26S proteasome degrades proteins that regulate transcription factor activation, cell cycle progression, and apoptosis. In cancer, this may allow for uncontrolled cell division, promoting tumor growth, and spread. We examined whether selective inhibition of the 26S proteasome with PS-341, a dipeptide boronic acid analogue, would block proliferation and induce apoptosis in human pancreatic cancer. Proteasome inhibition significantly blocked mitogen (FCS) induced proliferation of BxPC3 human pancreatic cancer cells in vitro, while arresting cell cycle progression and inducing apoptosis by 24 h. Accumulation of p21(Cip1-Waf-1), a cyclin dependent kinase (CDK) inhibitor normally degraded by the 26S proteasome, occurred by 3 h and correlated with cell cycle arrest. When BxPC3 pancreatic cancer xenografts were established in athymic nu/nu mice, weekly administration of 1 mg/kg PS-341 significantly inhibited tumor growth. Both cellular apoptosis and p21(Cip1-Waf-1) protein levels were increased in PS-341 treated xenografts. Inhibition of tumor xenograft growth was greatest (89%) when PS-341 was combined with the tumoricidal agent CPT-11. Combined CPT-11/PS-341 therapy, but not single agent therapy, yielded highly apoptotic tumors, significantly inhibited tumor cell proliferation, and blocked NF-kappaB activation indicating this systemic therapy was effective at the cancer cell level. 26S proteasome inhibition may represent a new therapeutic approach against this highly resistant and lethal malignancy., (Copyright 2001 Wiley-Liss, Inc.)

Published

2001

36. The proteasome inhibitor PS-341 inhibits growth, induces apoptosis, and overcomes drug resistance in human multiple myeloma cells.

Author

Hideshima T, Richardson P, Chauhan D, Palombella VJ, Elliott PJ, Adams J, and Anderson KC

Subjects

Bone Marrow Cells cytology, Bortezomib, Cell Adhesion physiology, Cell Division drug effects, DNA-Binding Proteins metabolism, Drug Resistance, Neoplasm, Enzyme Activation drug effects, Growth Inhibitors pharmacology, Humans, MAP Kinase Signaling System drug effects, Mitogen-Activated Protein Kinase 3, Mitogen-Activated Protein Kinases antagonists & inhibitors, Mitogen-Activated Protein Kinases metabolism, Multiple Myeloma enzymology, Multiple Myeloma pathology, NF-KappaB Inhibitor alpha, Stromal Cells cytology, Tumor Cells, Cultured, Antineoplastic Agents pharmacology, Apoptosis drug effects, Boronic Acids pharmacology, I-kappa B Proteins, Multiple Myeloma drug therapy, Protease Inhibitors pharmacology, Pyrazines pharmacology

Abstract

Human multiple myeloma (MM) is a presently incurable hematological malignancy, and novel biologically based therapies are urgently needed. Proteasome inhibitors represent a novel potential anticancer therapy. In this study, we demonstrate that the proteasome inhibitor PS-341 directly inhibits proliferation and induces apoptosis of human MM cell lines and freshly isolated patient MM cells; inhibits mitogen-activated protein kinase growth signaling in MM cells; induces apoptosis despite induction of p21 and p27 in both p53 wild-type and p53 mutant MM cells; overcomes drug resistance; adds to the anti-MM activity of dexamethasone; and overcomes the resistance to apoptosis in MM cells conferred by interleukin-6. PS-341 also inhibits the paracrine growth of human MM cells by decreasing their adherence to bone marrow stromal cells (BMSCs) and related nuclear factor kappaB-dependent induction of interleukin-6 secretion in BMSCs, as well as inhibiting proliferation and growth signaling of residual adherent MM cells. These data, therefore, demonstrate that PS-341 both acts directly on MM cells and alters cellular interactions and cytokine secretion in the BM millieu to inhibit tumor cell growth, induce apoptosis, and overcome drug resistance. Given the acceptable animal and human toxicity profile of PS-341, these studies provide the framework for clinical evaluation of PS-341 to improve outcome for patients with this universally fatal hematological malignancy.

Published

2001

37. New agents in cancer clinical trials.

Author

Adams J and Elliott PJ

Subjects

Benzamides, Benzoquinones, Boronic Acids therapeutic use, Bortezomib, Clinical Trials as Topic, Dioxoles therapeutic use, Enzyme Inhibitors therapeutic use, Humans, Hydroxamic Acids therapeutic use, Imatinib Mesylate, Isoquinolines therapeutic use, Lactams, Macrocyclic, Piperazines therapeutic use, Pyrazines therapeutic use, Pyrimidines therapeutic use, Rifabutin analogs & derivatives, Rifabutin therapeutic use, Stilbenes therapeutic use, Tetrahydrofolates therapeutic use, Tetrahydroisoquinolines, Trabectedin, Vorinostat, Antineoplastic Agents therapeutic use, Neoplasms drug therapy

Published

2000

38. Proteasome inhibitor PS519 reduces infarction and attenuates leukocyte infiltration in a rat model of focal cerebral ischemia.

Author

Phillips JB, Williams AJ, Adams J, Elliott PJ, and Tortella FC

Subjects

Acetylcysteine pharmacology, Animals, Cell Movement immunology, Corpus Striatum blood supply, Corpus Striatum physiology, Disease Models, Animal, Electroencephalography, Infarction, Middle Cerebral Artery immunology, Infarction, Middle Cerebral Artery metabolism, Ischemic Attack, Transient immunology, Ischemic Attack, Transient metabolism, Macrophages cytology, Male, Neuroprotective Agents pharmacology, Neutrophils cytology, Proteasome Endopeptidase Complex, Rats, Rats, Sprague-Dawley, Recovery of Function, Acetylcysteine analogs & derivatives, Cysteine Endopeptidases metabolism, Infarction, Middle Cerebral Artery drug therapy, Ischemic Attack, Transient drug therapy, Macrophages immunology, Multienzyme Complexes metabolism, Neutrophils immunology

Abstract

Background and Purpose: Reperfusion brain injury after cerebral ischemia is associated with a developing inflammatory response at the site of infarction. Proteasome inhibitors block nuclear factor-kappaB activation and provide anti-inflammatory effects in several animal models of peripheral inflammation. We tested the novel proteasome inhibitor PS519 in a rat model of transient focal ischemia to establish its pharmacodynamics as a neuroprotection treatment and related effects on leukocyte infiltration., Methods: Rats were subjected to 2 hours of focal cerebral ischemia by means of the filament method of middle cerebral artery occlusion (MCAo). After either 22 or 70 hours of reperfusion, infarct size was measured and neurological function, electroencephalographic (EEG) activity, and/or neutrophil and macrophage infiltration was quantified. PS519 was administered in a single intravenous bolus at 2 hours after MCAo. In addition, the therapeutic window for PS519 was estimated by delaying treatment for 4 or 6 hours after MCAo., Results: Dose-response analysis of infarct volume at 24 hours revealed that PS519 neuroprotection approached 60%, and clinical evaluations showed significant improvements in neurological function and EEG activity. Neutrophil infiltration at 24 hours was also significantly decreased in cortical and striatal infarcted tissue of PS519-treated rats. Delaying the PS519 treatment up to 4 hours continued to result in significant neuroprotection. In the 72-hour injury model, infarction was reduced 40% by PS519, and significant improvements in neurological function and EEG recovery were again measured. Considerable reductions in both neutrophil and macrophage infiltration were evident., Conclusions: PS519 mitigates infarction and improves neurological recovery in brain-injured rats, an effect in part caused by a reduction in the leukocyte inflammatory response.

Published

2000

39. Treatment of established relapsing experimental autoimmune encephalomyelitis with the proteasome inhibitor PS-519.

Author

Vanderlugt CL, Rahbe SM, Elliott PJ, Dal Canto MC, and Miller SD

Subjects

Animals, Cysteine Proteinase Inhibitors therapeutic use, Encephalomyelitis, Autoimmune, Experimental drug therapy, Epitopes, T-Lymphocyte immunology, Female, Mice, Myelin Proteolipid Protein immunology, Peptide Fragments immunology, Proteasome Endopeptidase Complex, Recurrence, Spinal Cord immunology, T-Lymphocytes immunology, Cysteine Endopeptidases immunology, Cysteine Proteinase Inhibitors immunology, Encephalomyelitis, Autoimmune, Experimental immunology, Multienzyme Complexes immunology

Abstract

PLP139-151-induced relapsing experimental autoimmune encephalomyelitis (R-EAE) in SJL mice is a Th1-mediated autoimmune demyelinating disease model for multiple sclerosis (MS) in which the primary disease relapse is mediated by T cells specific for the endogenous PLP178-191 epitope. This complex inflammatory process requires the co-ordinated expression of a wide variety of immune-related genes active at a variety of stages of the autoimmune process which are regulated, in part, by the transcription factor nuclear factor (NF)-kappaB which is activated via the ubiquitin-proteasome pathway. We asked if in vivo administration of a selective inhibitor of the ubiquitin-proteasome pathway, PS-519, which downregulates activation of NF-kappaB, could downregulate ongoing R-EAE. Administration of PS-519 during the remission phase, following acute clinical disease was effective in significantly reducing the incidence of clinical relapses, CNS histopathology, and T cell responses to both the initiating and relapse-associated PLP epitopes. The inhibition of clinical disease was dependent upon continuous administration of PS-519 in that recovery of T cell function and onset of disease relapses developed within 10-14 days of drug withdrawal. The data suggest that targeting the ubiquitin proteasome pathway, in particular NF-kappaB, may offer a novel and efficacious approach for the treatment of progressive autoimmune diseases, including MS., (Copyright 2000 Academic Press.)

Published

2000

40. Proteasome inhibition measurements: clinical application.

Author

Lightcap ES, McCormack TA, Pien CS, Chau V, Adams J, and Elliott PJ

Subjects

Acetylcysteine analogs & derivatives, Acetylcysteine pharmacology, Animals, Antineoplastic Agents pharmacology, Boronic Acids pharmacology, Bortezomib, Cysteine Endopeptidases blood, Humans, In Vitro Techniques, Kinetics, Male, Multienzyme Complexes blood, Protease Inhibitors pharmacology, Proteasome Endopeptidase Complex, Pyrazines pharmacology, Rats, Rats, Sprague-Dawley, Reproducibility of Results, Sensitivity and Specificity, Spectrometry, Fluorescence, Cysteine Endopeptidases metabolism, Multienzyme Complexes metabolism

Abstract

Background: PS-341, a selective inhibitor of the proteasome, currently is under evaluation as an anticancer agent in multiple phase I clinical trials. In animal-model studies, PS-341 was rapidly removed from the vascular compartment and distributed widely, quickly approaching the limits of detection. An accurate pharmacodynamic assay has been developed as an alternative or complement to pharmacokinetic measurements., Methods: Fluorogenic kinetic assays for both the chymotryptic and tryptic activities of the proteasome have been optimized for both whole blood and blood cells. Using the ratio of these activities and the catalytic mechanism of the proteasome, we developed a novel method of calculating percentage of inhibition, using two structurally unrelated inhibitors (PS-341 and lactacystin)., Results: This ratio method was demonstrated to be sensitive (detection limit of 13% inhibition with 10 microgram of cell lysate), specific to the proteasome (PS-341 provides >98% inhibition), accurate (112% analyte recovery), and precise (0% +/- 5% inhibition at 0 nmol/L PS-341 and 74.5% +/- 1.7% inhibition at 200 nmol/L PS-341). Using these assays, we found that both erythrocytes and leukocytes contain proteasome at 3 micromol/L. Pharmacodynamic results for PS-341 obtained from the whole-blood ratio method were comparable to those using leukocytes determined by another method., Conclusions: The described assay provides a reliable method for studying the pharmacodynamics of proteasome inhibitors and is now in use in concurrent phase I clinical trials with PS-341.

Published

2000

41. Proteasome inhibition: a new strategy in cancer treatment.

Author

Adams J, Palombella VJ, and Elliott PJ

Subjects

Animals, Humans, Mice, Neoplasms pathology, Neoplasms, Experimental drug therapy, Proteasome Endopeptidase Complex, Antineoplastic Agents pharmacology, Cysteine Endopeptidases drug effects, Multienzyme Complexes drug effects, Neoplasms drug therapy

Abstract

The ubiquitin proteasome pathway is a highly conserved intracellular pathway for the degradation of proteins. Many of the short-lived regulatory proteins which govern cell division, growth, activation, signaling and transcription are substrates that are temporally degraded by the proteasome. In recent years, new and selective inhibitors of the proteasome have been employed in cell culture systems to examine the anti-tumor potential of these agents. This review covers the chemistry of selected proteasome inhibitors, possible mechanisms of action in cell culture and the in vivo examination of proteasome inhibitors in murine and human xenograft tumor models in mice. One inhibitor, PS-341, has recently entered Phase I clinical trials in cancer patients with advanced disease to further test the potential of this approach.

Published

2000

42. A new model of cancer cachexia: contribution of the ubiquitin-proteasome pathway.

Author

Lazarus DD, Destree AT, Mazzola LM, McCormack TA, Dick LR, Xu B, Huang JQ, Pierce JW, Read MA, Coggins MB, Solomon V, Goldberg AL, Brand SJ, and Elliott PJ

Subjects

Animals, Cachexia drug therapy, Dexamethasone therapeutic use, Disease Models, Animal, Glucocorticoids therapeutic use, Indomethacin therapeutic use, Male, Mice, Mice, Inbred BALB C, Mice, Inbred DBA, Muscle Proteins metabolism, Muscles metabolism, Proteasome Endopeptidase Complex, Cachexia etiology, Cachexia metabolism, Cysteine Endopeptidases metabolism, Multienzyme Complexes metabolism, Neoplasms, Experimental complications, Ubiquitins metabolism

Abstract

A new model of cachexia is described in which muscle protein metabolism related to the ubiquitin-proteasome pathway was investigated. Cloning of the colon-26 tumor produced a cell line, termed R-1, which induced cytokine (noninterleukin-1beta, interleukin-6 and tumor necrosis factor-alpha)-independent cachexia. Implantation of R-1 cells in mice elicited significant (20-30%) weight loss and decreased blood glucose by 70%, and adipose tissue levels declined by 95% and muscle weights decreased by 20-25%. Food intake was unaffected. The decrease in muscle weight reflected a decline in insoluble, but not soluble, muscle protein that was associated with a significant increase in net protein degradation. The rate of ubiquitin conjugation of proteins was significantly elevated in muscles of cachectic mice. Furthermore, the proteasome inhibitor lactacystin blocked the increase in protein breakdown but had no significant effect on proteolysis. Several markers of the ubiquitin-proteasome pathway, E2(14k) mRNA and E2(14k) protein and ubiquitin-protein conjugates, were not elevated. Future investigations with this new model should gain further insights into the mechanisms of cachexia and provide a background to evaluate novel and more efficacious therapies.

Published

1999

43. Proteasome inhibition: A novel mechanism to combat asthma.

Author

Elliott PJ, Pien CS, McCormack TA, Chapman ID, and Adams J

Subjects

Animals, Asthma physiopathology, Asthma prevention & control, Dexamethasone adverse effects, Hypersensitivity, Delayed chemically induced, Lactones chemistry, Lactones pharmacology, Male, Mice, Mice, Inbred BALB C, Proteasome Endopeptidase Complex, Pulmonary Eosinophilia immunology, Pulmonary Eosinophilia physiopathology, Pulmonary Eosinophilia prevention & control, Rats, Rats, Inbred BN, Structure-Activity Relationship, Cysteine Endopeptidases drug effects, Cysteine Proteinase Inhibitors physiology, Multienzyme Complexes drug effects

Abstract

Background: Nuclear factor-kappaB (NF-kappaB) is a critical transcription factor required for the regulation of many genes involved in inflammatory responses to noxious stimuli. On activation, NF-kappaB induces the transcription of numerous proinflammatory cytokines, enzymes, and cellular adhesion molecules. Blockade of the proteasome with selective inhibitors attenuates the effects of NF-kappaB, leading to suppression of the inflammatory response., Objective: We sought to determine whether proteasome inhibitors would be active in a model of asthma., Methods: The mouse delayed-type hypersensitivity model was used to screen a panel of compounds for in vivo activity. The proteasome inhibitor, PS-519, was shown to be the most active in this model and was selected for further development. Allergen-induced pulmonary eosinophilia in Brown Norway rats was used subsequently to determine anti-inflammatory activity in an animal model., Results: Direct administration of PS-519 into the lungs significantly reduced leukocyte numbers, particularly the selective increase in eosinophils. Because steroids are the mainstay anti-inflammatory therapy in asthma, and data is available to suggest their possible interaction to suppress the activation of NF-kappaB, rats were also treated by inhalation with combinations of a steroid and the proteasome inhibitor. In both the delayed-type hypersensitivity and the animal eosinophil model, low doses of proteasome inhibitors were shown to be effective when given with low doses of steroids., Conclusion: Taken together, the present data suggest that proteasome inhibition may represent a novel strategy for the treatment of inflammatory lung diseases such as asthma.

Published

1999

44. Proteasome inhibitors: a novel class of potent and effective antitumor agents.

Author

Adams J, Palombella VJ, Sausville EA, Johnson J, Destree A, Lazarus DD, Maas J, Pien CS, Prakash S, and Elliott PJ

Subjects

Algorithms, Animals, Antineoplastic Agents pharmacokinetics, Boronic Acids pharmacokinetics, Computer Simulation, Drug Screening Assays, Antitumor, Humans, Male, Mice, Mice, Nude, Models, Chemical, Protease Inhibitors pharmacokinetics, Tumor Cells, Cultured drug effects, Antineoplastic Agents pharmacology, Boronic Acids pharmacology, Protease Inhibitors pharmacology

Abstract

The ubiquitin-proteasome pathway plays a critical role in the regulated degradation of proteins involved in cell cycle control and tumor growth. Dysregulating the degradation of such proteins should have profound effects on tumor growth and cause cells to undergo apoptosis. To test this hypothesis, we developed a novel series of proteasome inhibitors, exemplified by PS-341, which we describe here. As determined by the National Cancer Institute in vitro screen, PS-341 has substantial cytotoxicity against a broad range of human tumor cells, including prostate cancer cell lines. The PC-3 prostate cell line was, therefore, chosen to further examine the antitumor activity of PS-341. In vitro, PS-341 elicits proteasome inhibition, leading to an increase in the intracellular levels of specific proteins, including the cyclin-dependent kinase inhibitor, p21. Moreover, exposure of such cells to PS-341 caused them to accumulate in the G2-M phase of the cell cycle and subsequently undergo apoptosis, as indicated by nuclear condensation and poly(ADP-ribose) polymerase cleavage. Following weekly i.v. treatment of PS-341 to mice bearing the PC-3 tumor, a significant decrease (60%) in tumor burden was observed in vivo. Direct injection of PS-341 into the tumor also caused a substantial (70%) decrease in tumor volume with 40% of the drug-treated mice having no detectable tumors at the end of the study. Studies also revealed that i.v. administration of PS-341 resulted in a rapid and widespread distribution of PS-341, with highest levels identified in the liver and gastrointestinal tract and lowest levels in the skin and muscle. Modest levels were found in the prostate, whereas there was no apparent penetration of the central nervous system. An assay to follow the biological activity of the PS-341 was established and used to determine temporal drug activity as well as its ability to penetrate tissues. As such, PS-341 was shown to penetrate PC-3 tumors and inhibit intracellular proteasome activity 1.0 h after i.v. dosing. These data illustrate that PS-341 not only reaches its biological target but has a direct effect on its biochemical target, the proteasome. Importantly, the data show that inhibition of this target site by PS-341 results in reduced tumor growth in murine tumor models. Together, the results highlight that the proteasome is a novel biochemical target and that inhibitors such as PS-341 represent a unique class of antitumor agents. PS-341 is currently under clinical evaluation for advanced cancers.

Published

1999

45. Inhibition of NF-kappa B activation in vitro and in vivo: role of 26S proteasome.

Author

Grisham MB, Palombella VJ, Elliott PJ, Conner EM, Brand S, Wong HL, Pien C, Mazzola LM, Destree A, Parent L, and Adams J

Subjects

Acetylcysteine analogs & derivatives, Acetylcysteine pharmacology, Animals, Arthritis drug therapy, Boronic Acids pharmacology, Cell Adhesion Molecules biosynthesis, Cytokines biosynthesis, Dipeptides pharmacology, Endothelium, Vascular drug effects, Endothelium, Vascular metabolism, Female, HeLa Cells, Humans, Hypersensitivity, Delayed drug therapy, Jurkat Cells, Leupeptins pharmacology, Rats, Rats, Inbred Lew, T-Lymphocytes drug effects, NF-kappa B metabolism, Peptide Hydrolases drug effects, Protease Inhibitors pharmacology, Proteasome Endopeptidase Complex

Abstract

It is becoming increasingly apparent that NF-kappa B plays a critical role in regulating the inflammatory response. Data obtained from studies in our laboratories demonstrate that the proteasome plays an important role in the inflammatory cascade by regulating the activation of NF-kappa B. Indeed, the availability of selective and orally active proteasome inhibitors should prove useful in delineating the roles of the proteasome and NF-kappa B in other pathophysiological conditions such as cancer and heart disease.

Published

1999

46. Role of the proteasome and NF-kappaB in streptococcal cell wall-induced polyarthritis.

Author

Palombella VJ, Conner EM, Fuseler JW, Destree A, Davis JM, Laroux FS, Wolf RE, Huang J, Brand S, Elliott PJ, Lazarus D, McCormack T, Parent L, Stein R, Adams J, and Grisham MB

Subjects

Animals, Arthritis, Experimental immunology, Arthritis, Experimental pathology, Cell Adhesion Molecules biosynthesis, Cell Wall immunology, Cells, Cultured, Cysteine Proteinase Inhibitors pharmacology, Cytokines biosynthesis, Endothelium, Vascular cytology, Endothelium, Vascular drug effects, Female, Gene Expression Regulation, Humans, Joints pathology, Joints physiopathology, Nitric Oxide metabolism, Proteasome Endopeptidase Complex, Rats, Rats, Inbred Lew, Tumor Necrosis Factor-alpha pharmacology, Ubiquitins metabolism, Umbilical Veins, Arthritis, Experimental physiopathology, Cell Adhesion Molecules genetics, Cysteine Endopeptidases metabolism, Cytokines genetics, Endothelium, Vascular physiology, Multienzyme Complexes metabolism, NF-kappa B metabolism, Streptococcus immunology

Abstract

The transcription factor NF-kappaB activates a number of genes whose protein products are proinflammatory. In quiescent cells, NF-kappaB exists in a latent form and is activated via a signal-dependent proteolytic mechanism in which the inhibitory protein IkappaB is degraded by the ubiquitin-proteasome pathway. Consequently, inhibition of the proteasome suppresses activation of NF-kappaB. This suppression should therefore decrease transcription of many genes encoding proinflammatory proteins and should ultimately have an anti-inflammatory effect. To this end, a series of peptide boronic acid inhibitors of the proteasome, exemplified herein by PS-341, were developed. The proteasome is the large multimeric protease that catalyzes the final proteolytic step of the ubiquitin-proteasome pathway. PS-341, a potent, competitive inhibitor of the proteasome, readily entered cells and inhibited the activation of NF-kappaB and the subsequent transcription of genes that are regulated by NF-kappaB. Significantly, PS-341 displayed similar effects in vivo. Oral administration of PS-341 had anti-inflammatory effects in a model of Streptococcal cell wall-induced polyarthritis and liver inflammation in rats. The attenuation of inflammation in this model was associated with an inhibition of IkappaBalpha degradation and NF-kappaB-dependent gene expression. These experiments clearly demonstrate that the ubiquitin-proteasome pathway and NF-kappaB play important roles in regulating chronic inflammation and that, as predicted, proteasome inhibition has an anti-inflammatory effect.

Published

1998

47. Cerebrovascular effects of the bradykinin analog RMP-7 in normal and irradiated dog brain.

Author

Fike JR, Gobbel GT, Mesiwala AH, Shin HJ, Nakagawa M, Lamborn KR, Seilhan TM, and Elliott PJ

Subjects

Animals, Blood Pressure drug effects, Blood Pressure radiation effects, Bradykinin pharmacology, Brain diagnostic imaging, Brain Edema diagnostic imaging, Brain Edema etiology, Dogs, Male, Radiation Injuries, Experimental, Reference Values, Tomography, X-Ray Computed, Bradykinin analogs & derivatives, Brain drug effects, Brain radiation effects, Cerebrovascular Circulation drug effects, Cerebrovascular Circulation radiation effects

Abstract

The effects of an intravenous (i.v.) injection of the bradykinin analog RMP-7 (100 ng/kg) were assessed in normal dogs and dogs with focal, radiation-induced brain lesions. A dose of 20 Gy was delivered to a point 0.75 cm from a removable interstitial 125I source; parameters relating to blood flow and permeability were quantified using computed tomography 2-8 weeks after irradiation. Blood flow-related endpoints included regional cerebral blood flow (rCBF), mean transit time of blood and vascular volume, while endpoints related to permeability included blood-to-brain transfer constant (Ki), brain-to-blood transfer constant and plasma volume. In unirradiated brain, an i.v. bolus of RMP-7 administered through the left cephalic vein induced a rapid and transient hypotension and a statistically significant increase in vascular volume; no alterations in any parameter related to permeability were observed. After irradiation, changes in rCBF after RMP-7 depended upon time after exposure, effects presumably due to changing morphology in the irradiated tissues. In the radiation lesions, significant increases in Ki were observed 5 minutes after injection of RMP-7, but those increases were not related to time after irradiation or alteration in blood flow-related parameters. Our results showed that RMP-7 selectively increased permeability in already damaged vasculature without affecting the extent or volume of radiation-induced vasogenic edema. These data suggest that RMP-7 may provide an effective means to enhance the delivery of compounds to an already compromised brain while not exacerbating the potential adverse effects of pre-existing vasogenic edema.

Published

1998

48. Telomere length in myelodysplastic syndromes.

Author

Boultwood J, Fidler C, Kusec R, Rack K, Elliott PJ, Atoyebi O, Chapman R, Oscier DG, and Wainscoat JS

Subjects

Adult, Aged, Aged, 80 and over, Blotting, Southern, Bone Marrow Cells pathology, DNA Probes chemistry, Granulocytes pathology, Humans, Karyotyping, Lymphocytes pathology, Middle Aged, Myelodysplastic Syndromes blood, Myelodysplastic Syndromes pathology, Reference Values, Repetitive Sequences, Nucleic Acid, Telomere ultrastructure, Myelodysplastic Syndromes genetics, Telomere genetics

Abstract

We have studied telomere length in the bone marrow cells or the granulocyte and lymphocyte cell fractions of 54 patients with myelodysplastic syndromes (MDS) by Southern blot hybridization using the (TTAGGG)4 probe. The average telomere length expressed as the peak telomere repeat array (TRA) in the peripheral blood, or bone marrow samples obtained from a group of 21 healthy age-matched controls (26-89 years old, mean age 55), ranged between 7.5 and 9.5 kb (mean peak TRA 8.6 kb). Twenty-four patients with refractory anemia (RA) were studied; 10/24 (42%) had telomere reduction (<7.5 kb) relative to age-matched controls and the mean peak TRA was 7.5 kb (range 4.0-9.0 kb). Eleven patients with RA with excess blasts (RAEB) were studied; 5/11 (45%) had reduced telomeres relative to age-matched controls and the mean peak TRA was 7.1 kb (range 5.0-9.0 kb). Eighteen patients with MDS in transformation to AML, comprising 15 with RAEB in transformation (RAEBt) and 3 with CMML in transformation (CMMLt), were also studied. Thirteen of eighteen patients (72%) had telomere reduction relative to age-matched controls and the mean peak TRA was 6.1 kb (range 3.5-9.0 kb). Thirty-six patients included in the study had either a normal karyotype or a simple karyotype (1 karyotypic change) and 20/36 (55%) of these had telomere reduction and the mean peak TRA was 7.1 kb (range 4.3-9.0 kb); 8 patients had a complex karyotype (3 or more karyotypic changes) and 5/8 (62%) of these had telomere reduction and the mean peak TRA was 6.1 kb (range 3.5-9.0 kb). We conclude, firstly that there is heterogeneity of telomere length in MDS and that this is observed throughout the spectrum of FAB-subtypes. Secondly, these data show that a marked reduction in telomere length in MDS if often associated with leukemic transformation and with the presence of complex karyotypic abnormalities.

Published

1997

49. Controlled modulation of BBB permeability using the bradykinin agonist, RMP-7.

Author

Bartus RT, Elliott PJ, Dean RL, Hayward NJ, Nagle TL, Huff MR, Snodgrass PA, and Blunt DG

Subjects

Animals, Autoradiography, Biomarkers, Bradykinin agonists, Bradykinin pharmacology, Brain Neoplasms, Capillaries drug effects, Capillaries metabolism, Carbon Radioisotopes pharmacokinetics, Endothelium, Vascular drug effects, Endothelium, Vascular metabolism, Female, Male, Neoplasm Transplantation, Rats, Rats, Inbred F344, Rats, Wistar, Tumor Cells, Cultured drug effects, Tumor Cells, Cultured metabolism, Blood-Brain Barrier drug effects, Bradykinin analogs & derivatives, Carboplatin pharmacokinetics, Carcinogens pharmacokinetics, Carmustine pharmacokinetics, Dextrans pharmacokinetics, Plasma Substitutes pharmacokinetics

Abstract

Previous studies have shown that the bradykinin agonist, RMP-7, can safely permeabilize the blood brain barrier (BBB) by activation of constitutive B2 receptors on endothelial cells. The paper describes a series of studies using quantitative autoradiography and intracarotid infusions of RMP-7 to further elucidate the effect on BBB permeability. Because earlier studies also demonstrated that even greater effects of RMP-7 were observed in the BBB associated with brain tumors, animal models were employed so that comparisons could be made between the effects of RMP-7 within tumor, brain tissue proximal to tumor, and brain tissue distal from tumor. In the first study, the effect of RMP-7 on enhancing the BBB permeation of three compounds of different physical characteristics was directly compared ([14C]carboplatin, small, hydrophilic; [14C]dextran, large, hydrophilic; [14C]BCNU, small, lipophilic). RMP-7 increased permeability of the vascular barriers to both hydrophilic compounds, carboplatin and dextran. While the effects of RMP-7 were observed on nontumor BBB, the greatest and most consistent effects were observed on the blood brain tumor barrier. This was true for both carboplatin and dextran, with progressively less effect seen as the distance from tumor boundary increased. This topographic effect was more pronounced with the larger molecular weight compound, dextran. No effect of RMP-7 was seen in permeabilizing the BBB or the blood brain tumor barrier for the lipophilic drug, BCNU. In a second study, the generality of RMP-7's effects was established by demonstrating similar increases in permeability to carboplatin in both inbred (Fischer 344) and outbred (Wistar) rat strains, implanted with varying tumor cell lines. Finally, several additional studies were performed to gain greater insight into the dynamics involved with eventual restoration of the BBB following RMP-7 administration. In one series, it was demonstrated that the BBB begins to close nearly immediately upon withdrawal of RMP-7, with complete restoration occurring within minutes. In another series, tachyphylaxis or desensitization resulting from continuous RMP-7 infusion was studied. These studies demonstrated that 60 min of continuous RMP-7 infusion resulted in complete, spontaneous restoration of the barrier to both carboplatin and dextran. Moreover, the desensitization appears to be linked to the initial activation of the receptors in a way which suggests that obligatory desensitization may exist as part of a more complete response. These data are discussed as they relate to practical issues to enhance delivery of drugs across the BBB, as well as more fundamental issues involving the function of the BBB and its interaction with the brain.

Published

1996

50. Unlocking the blood-brain barrier: a role for RMP-7 in brain tumor therapy.

Author

Elliott PJ, Hayward NJ, Huff MR, Nagle TL, Black KL, and Bartus RT

Subjects

Animals, Bradykinin pharmacology, Brain Neoplasms drug therapy, Dose-Response Relationship, Drug, Female, Glioma drug therapy, Kinetics, Rats, Rats, Wistar, Tumor Cells, Cultured drug effects, Tumor Cells, Cultured metabolism, Blood-Brain Barrier drug effects, Bradykinin analogs & derivatives, Brain Neoplasms metabolism, Carboplatin metabolism, Glioma metabolism

Abstract

The effect and mechanism of the blood-brain barrier-permeabilizing agent, RMP-7, was investigated in a series of studies employing a rat RG2 glioma model. Changes in uptake of carboplatin into brain tumor and various nontumor brain tissue regions was determined using a sophisticated image analysis system. This system permitted quantitative autoradiography to be analyzed simultaneously with overlayed histological images from the same coronal brain section. A wide range of intracarotid doses of RMP-7 (0.01 to 9.0 micrograms/kg) was shown to significantly increase the permeability of carboplatin into tumor tissue and surrounding brain tissue (up to twofold) in a dose-dependent manner. Additionally, substantially greater permeability effects were seen in the tumor compared to healthy brain. Moreover, a clear topographic profile was observed in nontumor brain tissue, with progressively less uptake observed with increasing distance from the tumor. The fact that RMP-7 increased the uptake of carboplatin into ipsilateral brain tissue outside the tumor mass has potential implications for treating human glioma patients, for it is commonly recognized that tumor cells typically migrate from the tumor mass into surrounding brain tissue thereby escaping conventional attempts to destroy the malignant cells. To help elucidate the mechanism of RMP-7's permeability effects, the uptake of carboplatin was also determined under conditions where either the bradykinin B2 receptor antagonist, HOE140, or the B1 antagonist, [desArg10]HOE140, was coadministered with RMP-7. Results indicate that RMP-7's effects are mediated specifically through bradykinin B2 receptors. Furthermore, neither bradykinin antagonist alone affected the uptake of carboplatin into the leaky tumor region, suggesting that abnormal elevations in endogenous bradykinin activity are not likely responsible for the characteristic leaky nature of the tumor vascular barrier. The combined results from these studies therefore offer new insight into the characteristics of the vascular barriers in normal and tumor brain tissue and further elucidate the novel permeability effects of RMP-7. Together, they support its potential use as an adjunctive therapy for the selective delivery of chemotherapeutic drugs to brain tumors and possibly other neurodegenerative conditions.

Published

1996