Your search keyword '"Newton, Robert C."' showing total 294 results

251. Surgical management of renal hypertension

Author

Smithwick, Reginald H., primary, Newton, Robert C., additional, Crocker, Diane H., additional, and Harrison, J.Hartwell, additional

Published

1964

252. Some equilibrium reactions in the join CaAl2Si2O8-H2O

Author

Newton, Robert C., primary and Kennedy, G. C., additional

Published

1963

253. Thermodynamic Properties of Minerals and Related Substances at 298.15° K (25,0° C) and One Atmosphere (1.013 Bars) Pressure and at Higher Temperatures.Richard A. Robie , David R. Waldbaum

Author

Newton, Robert C., primary

Published

1971

254. BeO in pegmatitic cordierite

Author

Newton, Robert C., primary

Published

1966

255. Kyanite-Andalusite Equilibrium from 700° to 800°C

Author

Newton, Robert C., primary

Published

1966

256. Plasma Biomarker Association with Response in Acute GVHD Subjects Treated with the Combination of Itacitinib and Corticosteroids in a Phase 1 Clinical Trial

Author

Pratta, Michael A., Liu, Hao, Arbushites, Michael C., Newton, Robert C, and Howell, Michael D.

Abstract

Pratta: Incyte Research Institute: Employment, Equity Ownership. Liu:Incyte Research Institute: Employment, Equity Ownership. Arbushites:Incyte Corporation: Employment, Equity Ownership. Newton:Incyte Research Institute: Employment, Equity Ownership. Howell:Incyte Research Institute: Employment, Equity Ownership.

Published

2018

257. Janus Kinase (Jak) 1 Inhibition Affects Both Megakaryopoiesis and Thrombopoiesis

Author

Jarocha, Danuta Jadwiga, Gadue, Paul, Tong, Wei, Newton, Robert C, and Poncz, Mortimer

Abstract

Jarocha: Incyte Corporation: Consultancy, Research Funding. Gadue:Incyte Corporation: Consultancy, Research Funding. Tong:Incyte Corporation: Consultancy, Research Funding. Newton:Incyte Research Institute: Employment, Equity Ownership. Poncz:Incyte Corporation: Consultancy, Research Funding.

Published

2018

258. Cell-of-Origin Subtype Prediction of Diffuse Large B-Cell Lymphoma Using Gene Expression and Proteomic Data

Author

Liu, Huiqing, Lu, Jin, Dong, Zhiwan, Liu, Hao, Salinas, Edward, Owens, Sherry, Pratta, Michael A., Smith, Michael F., Tada, Hiroomi, Newton, Robert C, and Burn, Timothy

Abstract

Liu: Incyte Research Institute: Employment, Equity Ownership. Lu:Incyte Research Institute: Employment, Equity Ownership. Dong:Incyte Research Institute: Employment, Equity Ownership. Liu:Incyte Research Institute: Employment, Equity Ownership. Salinas:Incyte Research Institute: Employment, Equity Ownership. Owens:Incyte Research Institute: Employment, Equity Ownership. Pratta:Incyte Research Institute: Employment, Equity Ownership. Smith:Incyte Research Institute: Employment, Equity Ownership. Tada:Incyte Research Institute: Employment, Equity Ownership. Newton:Incyte Research Institute: Employment, Equity Ownership. Burn:Incyte Research Institute: Employment, Equity Ownership.

Published

2018

259. Acceptance of the Roebling Medal for 2010 of the Mineralogical Society of America.

Author

NEWTON, ROBERT C.

Subjects

*GEOPHYSICS, *MINERALOGICAL research, *ROEBLING Medal

Abstract

The article presents the text of a speech by Robert C. Newton, awardee of the Roebling Medal for 2010, delivered at the Mineralogical Society of America awarding ceremony held at the University of California-Los Angeles (UCLA) in Los Angeles, California. Newton spoke about his lucky breaks since he started studying geology at the University of Kansas and his first job at the Department of Geophysical Sciences in Chicago. He also highlighted his work as co-editor of the "Journal of Geology" with Fred Anderson from 1983 to 1997.

Published

2011

260. An Ongoing Open-Label Phase 1/2 Study of INCB050465, a Selective PI3Kδ Inhibitor, in Patients with Previously Treated B-Cell Malignancies

Author

Phillips, Tycel, Ramchandren, Rod, Wertheim, Michael S, Gutierrez, Martin E, Edenfield, William J, Dawkins, Fitzroy, DeMarini, Doug J, Zhou, Li, Yeleswaram, Swamy, Newton, Robert C, Chen, Xuejun, and Forero-Torres, Andres

Abstract

Gutierrez: Bayer Health Care Pharmaceuticals, Inc.: Other: Traveling and Lodging- Food and Beverage; Pfizer Inc: Consultancy; Merck Sharp & Dohme Corporation: Consultancy, Other: Travel and Lodging; Pharmacyclics LLC, An AbbVie Company: Other: Food and Beverage; Incyte Corporation: Consultancy; E.R. Squibb & Sons, LLC (Bristol Myers Squibb): Consultancy, Other: Travel and Lodging. Edenfield:Astellas/Medivation: Speakers Bureau; Novartis: Speakers Bureau; Greenville Health System Cancer Institute: Employment. Dawkins:Incyte Corporation: Employment, Other: Stocks. DeMarini:Incyte Corporation: Employment, Other: Stocks. Zhou:Incyte Corporation: Employment, Other: Stocks. Yeleswaram:Incyte Corporation: Employment, Other: Stocks. Newton:Incyte Corporation: Employment, Other: Stocks. Chen:Incyte Corporation: Employment, Other: Stocks. Forero-Torres:Seattle Genetics: Research Funding; Genentech/Roche: Research Funding; Juno: Research Funding; Incyte: Research Funding; Abbvie: Research Funding; Novartis: Research Funding; Pfizer: Research Funding.

Published

2016

261. Solubility of andradite, Ca3Fe2Si3O12, in a 10 mol% NaCl solution at 800 °C and 10 kbar: Implications for the metasomatic origin of grandite garnet in calc-silicate granulites.

Author

Wykes, Jeremy L., Newton, Robert C., and Manning, Craig E.

Subjects

*MINERALS

Abstract

An abstract of the article "Solubility of andradite, Ca3Fe2Si3O12, in a 10 mol% NaCl solution at 800 °C and 10 kbar: Implications for the metasomatic origin of grandite garnet in calc-silicate granulites," by Jeremy L. Wykes, Robert C. Newton, and Craig E. Manning is presented.

Published

2008

262. Reviews

Author

Newton, Robert C.

Published

1985

263. Reviews

Author

Newton, Robert C.

Published

1975

264. V. S. Sobolev and D. A. Brown. The Facies of Regional Metamorphism at High Pressures.

Author

Newton, Robert C.

Published

1978

265. Reviews

Author

Newton, Robert C.

Published

1978

266. Surendra K. Saxena. Thermodynamics of Rock-Forming Crystalline Solutions.

Author

Newton, Robert C.

Published

1975

267. Reviews

Author

Newton, Robert C.

Published

1971

268. Richard A. Robie and David R. Waldbaum. Thermodynamic Properties of Minerals and Related Substances at 298.15° K (25,0° C) and One Atmosphere (1.013 Bars) Pressure and at Higher Temperatures.

Author

Newton, Robert C.

Published

1971

269. ChemInform Abstract: Therapeutic Potential and Strategies for Inhibiting Tumor Necrosis Factor-α.

Author

Newton, Robert C. and Decicco, Carl P.

Published

1999

270. The Nature of the Orthopyroxene Isograd in Precambrian High-Grade Terrains

Author

Newton, Robert C.

Published

1990

271. Reviews

Author

Newton, Robert C.

Published

1984

272. Reviews

Author

Newton, Robert C.

Published

1987

273. Alfred Kröner and Reinhard Greiling. Precambrian Tectonics Illustrated.

Author

Newton, Robert C.

Published

1987

274. Akiho Miyashiro, Keiiti Aki, and A. M. Celâl Şengör. Orogeny.

Author

Newton, Robert C.

Published

1984

275. P. J. Hart. The Earth's Crust and Upper Mantle.

Author

Newton, Robert C.

Published

1971

276. Book reviews.

Author

Newton, Robert C.

Subjects

GRANULITES & Crustal Evolution (Book)

Abstract

Reviews the book `Granulites and Crustal Evolution,' edited by D. Vielzeuf and Ph. Vidal.

Published

1995

277. Geology and Evolution of the Indian Plate: From Hadean to Holocene, 4 Ga to 4 Ka.

Author

Newton, Robert C.

Subjects

GEOLOGY, NONFICTION

Abstract

The article reviews the book "Geology and Evolution of the Indian Plate: From Hadean to Holocene, 4 Ga to 4 Ka," by S. M. Naqvi.

Published

2006

278. Reviews.

Author

Newton, Robert C.

Subjects

THERMODYNAMICS in Geochemistry (Book)

Abstract

Reviews the book `Thermodynamics in Geochemistry,' by Greg M. Anderson and David A. Crerar.

Published

1995

279. A randomised, open-label, phase 2 study of the IDO1 inhibitor epacadostat (INCB024360) versus tamoxifen as therapy for biochemically recurrent (CA-125 relapse)–only epithelial ovarian cancer, primary peritoneal carcinoma, or fallopian tube cancer.

Author

Kristeleit, Rebecca, Davidenko, Irina, Shirinkin, Vadim, El-Khouly, Fatima, Bondarenko, Igor, Goodheart, Michael J., Gorbunova, Vera, Penning, Carol A., Shi, Jack G., Liu, Xiangdong, Newton, Robert C., Zhao, Yufan, Maleski, Janet, Leopold, Lance, and Schilder, Russell J.

Subjects

*OVARIAN epithelial cancer, *TAMOXIFEN, *CANCER relapse, *IMMUNOLOGICAL tolerance, *CANCER chemotherapy, *CANCER treatment

Abstract

Objective Indoleamine 2,3-dioxygenase-1 (IDO1) is a key regulator of immune tolerance in ovarian cancer. This study investigated efficacy and safety of the IDO1 enzyme inhibitor epacadostat versus tamoxifen in patients with biochemical-only recurrence (CA-125 elevation) following complete remission after first-line chemotherapy for advanced epithelial ovarian, primary peritoneal, or fallopian tube cancer. Methods In this open-label, phase 2 study (NCT01685255), patients were randomised 1:1 to epacadostat 600 mg or tamoxifen 20 mg twice daily for successive 28-day cycles and stratified by time since completion of first-line chemotherapy to first CA-125 elevation (3 to < 12 or ≥ 12 months). The primary endpoint was investigator-assessed progression-free survival (PFS; RECIST v1.1). Secondary endpoints included CA-125 response (Gynecologic Cancer InterGroup criteria), overall survival, safety, and tolerability. Results The study was terminated primarily due to slow accrual and lack of evidence of superiority. Median PFS was 3.75 months for epacadostat ( n = 22) versus 5.56 months for tamoxifen ( n = 20; HR, 1.34 [95% CI, 0.58–3.14]; P = 0.54). Of evaluable patients, 1 (5.0%) epacadostat and 3 (15.8%) tamoxifen patients had confirmed CA-125 responses. The most common treatment-emergent adverse event was fatigue (epacadostat, 36.4%; tamoxifen, 40.0%). Immune-related adverse events, observed with epacadostat only, were primarily rash (18.2%) and pruritus (9.1%). Epacadostat pharmacokinetics/pharmacodynamics were consistent with its known mechanism of action. IDO1 expression was observed in 94% of archival tumour samples. Conclusions This first report of immunotherapy evaluation in biochemical-only relapse ovarian cancer and of IDO1 inhibitor monotherapy in ovarian cancer found no significant difference in efficacy between epacadostat and tamoxifen. Epacadostat was generally well tolerated. [ABSTRACT FROM AUTHOR]

Published

2017

280. Phase 2 study of the JAK kinase inhibitor ruxolitinib in patients with refractory leukemias, including postmyeloproliferative neoplasm acute myeloid leukemia.

Author

Eghtedar, Alireza, Verstovsek, Srdan, Estrov, Zeev, Burger, Jan, Cortes, Jorge, Bivins, Carol, Faderl, Stefan, Ferrajoli, Alessandra, Borthakur, Gautam, George, Solly, Scherle, Peggy A., Newton, Robert C., Kantarjian, Hagop M., and Ravandi, Farhad

Subjects

*ACUTE myeloid leukemia treatment, *CLINICAL trials, *KINASES, *CELL cycle, *DRUG dosage, *MEDICAL statistics, *GENETIC mutation

Abstract

We conducted a phase 2 study of ruxolitinib in patients with relapsed/refractory leukemias. Patients with acceptable performance status (0-2), adequate organ function, and no active infection, received ruxolitinib 25 mg orally twice a day for 4 weeks (1 cycle). Response was assessed after every 2 cycles of treatment, and patients who completed 2 cycles were allowed to continue treatment until disease progression. Dose escalation to 50 mg twice daily was permitted in pa tients demonstrating a benefit. Thirty-eight patients, with a median age of 69 years (range, 45-88), were treated. The median number of prior therapies was 2 (range, 1-6). Twelve patients had JAK2V617F mutation. Patients received a median of 2 cycles of therapy (range, 1-22). Three of 18 patients with postmyeloproliferative neoplasm (MPN) acute myeloid leukemia (AML) showed a significant response; 2 achieved complete remission (CR) and one achieved a CR with insufficient recovery of blood counts (CRi). The responding patients with palpable spleens also had significant reductions in spleen size. Overall, ruxolitinib was very well tolerated with only 4 patients having grade 3 or higher toxicity. Ruxolitinib has modest antileukemic activity as a single agent, particularly in patients with post-MPN AML. [ABSTRACT FROM AUTHOR]

Published

2012

281. Design and synthesis of novel CCR2 antagonists: Investigation of non-aryl/heteroaryl binding motifs

Author

Trujillo, John I., Huang, Wei, Hughes, Robert O., Joseph Rogier, D., Turner, Steven R., Devraj, Rajesh, Morton, Philip A., Xue, Chu-Biao, Chao, Ganfeng, Covington, Maryanne B., Newton, Robert C., and Metcalf, Brian

Subjects

*DRUG design, *BIOSYNTHESIS, *DRUG synergism, *PYRAN, *HEPTANE, *INFLAMMATION, *DOFETILIDE

Abstract

Abstract: This report describes the design and synthesis of a series of CCR2 antagonists incorporating novel non-aryl/heteroaryl RHS (right hand side) motifs. Previous SAR in the area has suggested an aryl/heteroaryl substituent as a necessary structural feature for binding to the CCR2 receptor. Herein we describe the SAR with regards to potency (binding to hCCR2), dofetilide activity and metabolic stability (in vitro HLM) for this series. The resulting outcome was the identification of compounds with excellent properties for the investigation of the role of CCR2 in disease. [Copyright &y& Elsevier]

Published

2011

282. Targeting ADAM-mediated ligand cleavage to inhibit HER3 and EGFR pathways in non-small cell lung cancer

Author

Zhou, Bin-Bing S., Peyton, Michael, He, Biao, Liu, Changnian, Girard, Luc, Caudler, Eian, Lo, Yvonne, Baribaud, Frederic, Mikami, Iwao, Reguart, Noemi, Yang, Gengjie, Li, Yanlong, Yao, Wenqing, Vaddi, Kris, Gazdar, Adi F., Friedman, Steven M., Jablons, David M., Newton, Robert C., Fridman, Jordan S., and Minna, John D.

Subjects

*AUTOCRINE mechanisms, *LUNG cancer, *PROTEINS, *LIGANDS (Biochemistry), *DRUGS

Abstract

Summary: We describe here the existence of a heregulin-HER3 autocrine loop, and the contribution of heregulin-dependent, HER2-mediated HER3 activation to gefitinib insensitivity in non-small cell lung cancer (NSCLC). ADAM17 protein, a major ErbB ligand sheddase, is upregulated in NSCLC and is required not only for heregulin-dependent HER3 signaling, but also for EGFR ligand-dependent signaling in NSCLC cell lines. A selective ADAM inhibitor, INCB3619, prevents the processing and activation of multiple ErbB ligands, including heregulin. In addition, INCB3619 inhibits gefitinib-resistant HER3 signaling and enhances gefitinib inhibition of EGFR signaling in NSCLC. These results show that ADAM inhibition affects multiple ErbB pathways in NSCLC and thus offers an excellent opportunity for pharmacological intervention, either alone or in combination with other drugs. [Copyright &y& Elsevier]

Published

2006

283. Estudo experimental de magmatismo granítico potássico

Author

Soares, Marcos Roberto Farias, Hartmann, Leo Afraneo, and Newton, Robert C.

Subjects

Petrologia, Geologia do petróleo, Petrologia experimental, Geoquímica

Abstract

Esta tese de Petrologia Experimental aborda simultaneamente os aspectos petroquímicos e experimentais da geração de magmas graníticos potássicos, a partir do estudo da fusão por desidratação de uma rocha tonalítica em condições equivalentes aquelas de uma crosta espessa (0.8, 1.0, 1.3, 1.5 e 1.9 GPa), sujeita a um gradiente geotérmico elevado (800_

Published

1998

284. Clinicogenomic Analysis of FGFR2 -Rearranged Cholangiocarcinoma Identifies Correlates of Response and Mechanisms of Resistance to Pemigatinib.

Author

Silverman IM, Hollebecque A, Friboulet L, Owens S, Newton RC, Zhen H, Féliz L, Zecchetto C, Melisi D, and Burn TC

Subjects

Adult, Bile Duct Neoplasms genetics, Cholangiocarcinoma genetics, Cohort Studies, Drug Resistance, Neoplasm, Female, Gene Rearrangement, Humans, Male, Bile Duct Neoplasms drug therapy, Cholangiocarcinoma drug therapy, Morpholines therapeutic use, Pyrimidines therapeutic use, Pyrroles therapeutic use, Receptor, Fibroblast Growth Factor, Type 2 genetics

Abstract

Pemigatinib, a selective FGFR1-3 inhibitor, has demonstrated antitumor activity in FIGHT-202, a phase II study in patients with cholangiocarcinoma harboring FGFR2 fusions/rearrangements, and has gained regulatory approval in the United States. Eligibility for FIGHT-202 was assessed using genomic profiling; here, these data were utilized to characterize the genomic landscape of cholangiocarcinoma and to uncover unique molecular features of patients harboring FGFR2 rearrangements. The results highlight the high percentage of patients with cholangiocarcinoma harboring potentially actionable genomic alterations and the diversity in gene partners that rearrange with FGFR2 . Clinicogenomic analysis of pemigatinib-treated patients identified mechanisms of primary and acquired resistance. Genomic subsets of patients with other potentially actionable FGF/FGFR alterations were also identified. Our study provides a framework for molecularly guided clinical trials and underscores the importance of genomic profiling to enable a deeper understanding of the molecular basis for response and nonresponse to targeted therapy. SIGNIFICANCE: We utilized genomic profiling data from FIGHT-202 to gain insights into the genomic landscape of cholangiocarcinoma, to understand the molecular diversity of patients with FGFR2 fusions or rearrangements, and to interrogate the clinicogenomics of patients treated with pemigatinib. Our study highlights the utility of genomic profiling in clinical trials. This article is highlighted in the In This Issue feature, p. 211 ., (©2020 American Association for Cancer Research.)

Published

2021

285. First-in-Human Phase I Study of the Oral Inhibitor of Indoleamine 2,3-Dioxygenase-1 Epacadostat (INCB024360) in Patients with Advanced Solid Malignancies.

Author

Beatty GL, O'Dwyer PJ, Clark J, Shi JG, Bowman KJ, Scherle PA, Newton RC, Schaub R, Maleski J, Leopold L, and Gajewski TF

Subjects

Administration, Oral, Adult, Aged, Dose-Response Relationship, Drug, Drug Administration Schedule, Drug-Related Side Effects and Adverse Reactions classification, Female, Humans, Indoleamine-Pyrrole 2,3,-Dioxygenase antagonists & inhibitors, Male, Middle Aged, Neoplasm Staging, Neoplasms genetics, Neoplasms pathology, Drug-Related Side Effects and Adverse Reactions pathology, Indoleamine-Pyrrole 2,3,-Dioxygenase genetics, Neoplasms drug therapy, Oximes administration & dosage, Sulfonamides administration & dosage

Abstract

Purpose: Indoleamine 2,3-dioxygenase-1 (IDO1) catalyzes the degradation of tryptophan to N-formyl-kynurenine. Overexpressed in many solid malignancies, IDO1 can promote tumor escape from host immunosurveillance. This first-in-human phase I study investigated the maximum tolerated dose, safety, pharmacokinetics, pharmacodynamics, and antitumor activity of epacadostat (INCB024360), a potent and selective inhibitor of IDO1. Experimental Design: Fifty-two patients with advanced solid malignancies were treated with epacadostat [50 mg once daily or 50, 100, 300, 400, 500, 600, or 700 mg twice daily (BID)] in a dose-escalation 3 + 3 design and evaluated in 28-day cycles. Treatment was continued until disease progression or unacceptable toxicity. Results: One dose-limiting toxicity (DLT) occurred at the dose of 300 mg BID (grade 3, radiation pneumonitis); another DLT occurred at 400 mg BID (grade 3, fatigue). The most common adverse events in >20% of patients overall were fatigue, nausea, decreased appetite, vomiting, constipation, abdominal pain, diarrhea, dyspnea, back pain, and cough. Treatment produced significant dose-dependent reductions in plasma kynurenine levels and in the plasma kynurenine/tryptophan ratio at all doses and in all patients. Near maximal changes were observed at doses of ≥100 mg BID with >80% to 90% inhibition of IDO1 achieved throughout the dosing period. Although no objective responses were detected, stable disease lasting ≥16 weeks was observed in 7 of 52 patients. Conclusions: Epacadostat was generally well tolerated, effectively normalized kynurenine levels, and produced maximal inhibition of IDO1 activity at doses of ≥100 mg BID. Studies investigating epacadostat in combination with other immunomodulatory drugs are ongoing. Clin Cancer Res; 23(13); 3269-76. ©2017 AACR ., (©2017 American Association for Cancer Research.)

Published

2017

286. Selective inhibition of IDO1 effectively regulates mediators of antitumor immunity.

Author

Liu X, Shin N, Koblish HK, Yang G, Wang Q, Wang K, Leffet L, Hansbury MJ, Thomas B, Rupar M, Waeltz P, Bowman KJ, Polam P, Sparks RB, Yue EW, Li Y, Wynn R, Fridman JS, Burn TC, Combs AP, Newton RC, and Scherle PA

Subjects

Animals, Apoptosis drug effects, Apoptosis immunology, B7-2 Antigen immunology, B7-2 Antigen metabolism, Coculture Techniques, Dendritic Cells enzymology, Dose-Response Relationship, Drug, HeLa Cells, Humans, Immunity, Cellular drug effects, Immunity, Cellular immunology, Indoleamine-Pyrrole 2,3,-Dioxygenase metabolism, Mice, Mice, Inbred BALB C, Mice, Nude, Neoplasms drug therapy, Neoplasms enzymology, T-Lymphocytes enzymology, Tryptophan Oxygenase immunology, Tryptophan Oxygenase metabolism, Dendritic Cells immunology, Enzyme Inhibitors pharmacology, Indoleamine-Pyrrole 2,3,-Dioxygenase antagonists & inhibitors, Indoleamine-Pyrrole 2,3,-Dioxygenase immunology, Neoplasms immunology, T-Lymphocytes immunology

Abstract

Indoleamine 2,3-dioxygenase-1 (IDO1; IDO) mediates oxidative cleavage of tryptophan, an amino acid essential for cell proliferation and survival. IDO1 inhibition is proposed to have therapeutic potential in immunodeficiency-associated abnormalities, including cancer. Here, we describe INCB024360, a novel IDO1 inhibitor, and investigate its roles in regulating various immune cells and therapeutic potential as an anticancer agent. In cellular assays, INCB024360 selectively inhibits human IDO1 with IC(50) values of approximately 10nM, demonstrating little activity against other related enzymes such as IDO2 or tryptophan 2,3-dioxygenase (TDO). In coculture systems of human allogeneic lymphocytes with dendritic cells (DCs) or tumor cells, INCB024360 inhibition of IDO1 promotes T and natural killer (NK)-cell growth, increases IFN-gamma production, and reduces conversion to regulatory T (T(reg))-like cells. IDO1 induction triggers DC apoptosis, whereas INCB024360 reverses this and increases the number of CD86(high) DCs, potentially representing a novel mechanism by which IDO1 inhibition activates T cells. Furthermore, IDO1 regulation differs in DCs versus tumor cells. Consistent with its effects in vitro, administration of INCB024360 to tumor-bearing mice significantly inhibits tumor growth in a lymphocyte-dependent manner. Analysis of plasma kynurenine/tryptophan levels in patients with cancer affirms that the IDO pathway is activated in multiple tumor types. Collectively, the data suggest that selective inhibition of IDO1 may represent an attractive cancer therapeutic strategy via up-regulation of cellular immunity.

Published

2010

287. Developing c-MET pathway inhibitors for cancer therapy: progress and challenges.

Author

Liu X, Newton RC, and Scherle PA

Subjects

Animals, Humans, Neoplasms genetics, Neoplasms metabolism, Proto-Oncogene Proteins c-met genetics, Neoplasms drug therapy, Protein Kinase Inhibitors therapeutic use, Proto-Oncogene Proteins c-met antagonists & inhibitors, Proto-Oncogene Proteins c-met metabolism, Signal Transduction

Abstract

Successfully developed target-based therapies have significantly changed cancer treatment. Among many targets, the c-MET receptor tyrosine kinase and its ligand hepatocyte growth factor have recently gained considerable attention. The c-MET pathway is dysregulated in most human malignancies, and regulates tumor formation, progression and dissemination, and numerous c-MET pathway inhibitors are currently being evaluated in the clinic. Although some studies have shown impressive evidence of antitumor activity, the data should be interpreted with caution because of the distinct properties of these agents and diverse patient populations studied. Furthermore, in tumor types where patients might benefit from c-MET inhibition, rational combination treatments might ultimately provide maximal clinical benefit. Here, we review the evidence linking c-MET activation to cancer, and discuss the latest progress, opportunities and challenges in the clinical development of c-MET pathway inhibitors.

Published

2010

288. Alpha,Beta-cyclic-beta-benzamido hydroxamic acids: Novel oxaspiro[4.4]nonane templates for the discovery of potent, selective, orally bioavailable inhibitors of tumor necrosis factor-alpha converting enzyme (TACE).

Author

Ott GR, Asakawa N, Liu RQ, Covington MB, Qian M, Vaddi K, Newton RC, Trzaskos JM, Christ DD, Galya L, Scholz T, Marshall W, and Duan JJ

Subjects

ADAM17 Protein, Administration, Oral, Alkanes chemical synthesis, Alkanes pharmacokinetics, Alkanes pharmacology, Animals, Biological Availability, Caco-2 Cells, Humans, Hydroxamic Acids chemical synthesis, Hydroxamic Acids pharmacokinetics, Matrix Metalloproteinase Inhibitors, Matrix Metalloproteinases metabolism, Models, Molecular, Protease Inhibitors chemical synthesis, Protease Inhibitors pharmacokinetics, Rats, Rats, Sprague-Dawley, Spiro Compounds chemical synthesis, Spiro Compounds pharmacokinetics, Spiro Compounds pharmacology, ADAM Proteins antagonists & inhibitors, Alkanes chemistry, Hydroxamic Acids chemistry, Hydroxamic Acids pharmacology, Protease Inhibitors chemistry, Protease Inhibitors pharmacology, Spiro Compounds chemistry

Abstract

Two novel oxaspiro[4.4]nonane beta-benzamido hydroxamic scaffolds have been synthesized in enantio- and diasteriomerically pure form. These templates proved to be exceptional platforms that have led to the discovery of potent inhibitors of TACE that are active in a cellular assay measuring suppression of LPS-induced TNF-alpha. Furthermore, these inhibitors are selective against related MMPs, demonstrate permeability in a Caco-2 assay, and display good oral bioavailability.

Published

2008

289. Alpha,beta-cyclic-beta-benzamido hydroxamic acids: novel templates for the design, synthesis, and evaluation of selective inhibitors of TNF-alpha converting enzyme (TACE).

Author

Ott GR, Asakawa N, Lu Z, Liu RQ, Covington MB, Vaddi K, Qian M, Newton RC, Christ DD, Traskos JM, Decicco CP, and Duan JJ

Subjects

ADAM17 Protein, Administration, Oral, Animals, Biological Availability, Chromatography, High Pressure Liquid, Enzyme Inhibitors chemical synthesis, Humans, Hydroxamic Acids administration & dosage, Hydroxamic Acids chemical synthesis, Hydroxamic Acids pharmacokinetics, Rats, Stereoisomerism, ADAM Proteins antagonists & inhibitors, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Hydroxamic Acids chemistry, Hydroxamic Acids pharmacology

Abstract

Selective inhibitors of TNF-alpha Converting Enzyme (TACE) based on (1R,2S)-cyclopentyl, (3S,4S)-pyrrolidinyl, and (3R,4S)-tetrahydrofuranyl beta-benzamido hydroxamic acids have been synthesized and evaluated. This study has led to the discovery of novel inhibitors whose profiles include activity against TACE in an enzyme assay, potency in the suppression of LPS-stimulated TNF-alpha in human whole blood, selectivity against a panel of MMPs and oral bioavailability.

Published

2008

290. Pharmacokinetics and pharmacodynamics of DPC 333 ((2R)-2-((3R)-3-amino-3{4-[2-methyl-4-quinolinyl) methoxy] phenyl}-2-oxopyrrolidinyl)-N-hydroxy-4-methylpentanamide)), a potent and selective inhibitor of tumor necrosis factor alpha-converting enzyme in rodents, dogs, chimpanzees, and humans.

Author

Qian M, Bai SA, Brogdon B, Wu JT, Liu RQ, Covington MB, Vaddi K, Newton RC, Fossler MJ, Garner CE, Deng Y, Maduskuie T, Trzaskos J, Duan JJ, Decicco CP, and Christ DD

Subjects

ADAM17 Protein, Adult, Animals, Anti-Inflammatory Agents blood, Arthritis, Experimental blood, Arthritis, Experimental pathology, Dogs, Double-Blind Method, Endotoxemia blood, Endotoxemia chemically induced, Female, Humans, Lipopolysaccharides, Male, Mice, Mice, Inbred BALB C, Pan troglodytes, Quinolines blood, Rats, Rats, Inbred Strains, Synovial Fluid chemistry, Tumor Necrosis Factor-alpha antagonists & inhibitors, Tumor Necrosis Factor-alpha blood, ADAM Proteins antagonists & inhibitors, Anti-Inflammatory Agents pharmacokinetics, Anti-Inflammatory Agents therapeutic use, Arthritis, Experimental drug therapy, Endotoxemia drug therapy, Quinolines pharmacokinetics, Quinolines therapeutic use

Abstract

DPC 333 ((2R)-2-((3R)-3-amino-3{4-[2-methyl-4-quinolinyl) methoxy] phenyl}-2-oxopyrrolidinyl)-N-hydroxy-4-methylpentanamide)) is a potent and selective inhibitor of tumor necrosis factor (TNF)-alpha-converting enzyme (TACE). It significantly inhibits lipopolysaccharide-induced soluble TNF-alpha production in blood from rodents, chimpanzee, and human, with IC(50) values ranging from 17 to 100 nM. In rodent models of endotoxemia, DPC 333 inhibited the production of TNF-alpha in a dose-dependent manner, with an oral ED(50) ranging from 1.1 to 6.1 mg/kg. Oral dosing of DPC 333 at 5.5 mg/kg daily for 2 weeks in a rat collagen antibody-induced arthritis model suppressed the maximal response by approximately 50%. DPC 333 was distributed widely to tissues including the synovium, the site of action for antiarthritic drugs. Pharmacokinetic and pharmacodynamic studies in chimpanzee revealed a systemic clearance of 0.4 l/h/kg, a V(ss) of 0.6 l/kg, an oral bioavailability of 17%, and an ex vivo IC(50) for the suppression of TNF-alpha production of 55 nM (n = 1). In a phase I clinical trial with male volunteers after single escalating doses of oral DPC 333, the terminal half-life was between 3 and 6 h and the ex vivo IC(50) for suppressing TNF-alpha production was 113 nM. Measurement of the suppression of TNF-alpha production ex vivo may serve as a good biomarker in evaluating the therapeutic efficacy of TACE inhibitors. Overall, the pharmacological profiles of DPC 333 support the notion that suppression of TNF-alpha with TACE inhibitors like DPC 333 may provide a novel approach in the treatment of various inflammatory diseases including rheumatoid arthritis, via control of excessive TNF-alpha production.

Published

2007

291. Design, synthesis, and evaluation of benzothiadiazepine hydroxamates as selective tumor necrosis factor-alpha converting enzyme inhibitors.

Author

Cherney RJ, Duan JJ, Voss ME, Chen L, Wang L, Meyer DT, Wasserman ZR, Hardman KD, Liu RQ, Covington MB, Qian M, Mandlekar S, Christ DD, Trzaskos JM, Newton RC, Magolda RL, Wexler RR, and Decicco CP

Subjects

ADAM Proteins, ADAM17 Protein, Animals, Benzodiazepinones chemistry, Benzodiazepinones pharmacology, Blood Proteins metabolism, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Humans, Hydroxamic Acids chemistry, Hydroxamic Acids pharmacology, Leukocytes, Mononuclear drug effects, Matrix Metalloproteinase Inhibitors, Models, Molecular, Protein Binding, Structure-Activity Relationship, Swine, Thiazepines chemistry, Thiazepines pharmacology, Tumor Necrosis Factor-alpha biosynthesis, Benzodiazepinones chemical synthesis, Enzyme Inhibitors chemical synthesis, Hydroxamic Acids chemical synthesis, Metalloendopeptidases antagonists & inhibitors, Thiazepines chemical synthesis, Tumor Necrosis Factor-alpha antagonists & inhibitors

Abstract

Elevated levels of tumor necrosis factor-alpha (TNF-alpha) have been associated with several inflammatory diseases, and therefore, strategies for its suppression have become important targets in drug discovery. Our efforts to suppress TNF-alpha have centered on the inhibition of TNF-alpha converting enzyme (TACE) through the use of hydroxamate inhibitors. Starting from broad-spectrum matrix metalloproteinase (MMP) inhibitors, we have designed and synthesized novel benzothiadiazepines as potent and selective TACE inhibitors. The benzothiadiazepines were synthesized with variation in P1 and P1' in order to effect potency and selectivity. The inhibitors were evaluated versus porcine TACE (pTACE), and the initial selectivity was assessed with counterscreens of MMP-1, -2, and -9. Several potent and selective inhibitors were discovered with compound 41 being the most active against pTACE (K(i) = 5 nM) while still maintaining good selectivity versus the MMP's (at least 75-fold). Most compounds were assessed in the human peripheral blood mononuclear cell assay (PBMC) and the human whole blood assay (WBA) to determine their ability to suppress TNF-alpha. Compound 32 was the most potent compound in the PBMC assay (IC(50) = 0.35 microM), while compound 62 was the most active in the WBA (IC(50) = 1.4 microM).

Published

2003

292. Induction of aggrecanase 1 (ADAM-TS4) by interleukin-1 occurs through activation of constitutively produced protein.

Author

Pratta MA, Scherle PA, Yang G, Liu RQ, and Newton RC

Subjects

ADAM Proteins, ADAMTS4 Protein, Animals, Blotting, Western, Cartilage, Articular cytology, Cartilage, Articular enzymology, Cattle, Cells, Cultured, Chondrocytes cytology, Enzyme Activation drug effects, Fibroblasts cytology, Fibroblasts enzymology, Fluorescent Antibody Technique, Metalloendopeptidases analysis, Peptides metabolism, Procollagen N-Endopeptidase, Substrate Specificity, Chondrocytes enzymology, Interleukin-1 pharmacology, Metalloendopeptidases metabolism

Abstract

Objective: To study the production of aggrecanase 1 (ADAM-TS4) in monolayer chondrocytes, capsular fibroblasts, and cartilage., Methods: Bovine nasal and articular cartilage, monolayer chondrocytes, and capsular fibroblasts were incubated in the absence and presence of interleukin-1 (IL-1). ADAM-TS4 production was evaluated by immunofluorescence or by Western blot analysis. Aggrecanase activity was measured in cells grown on an immobilized peptide substrate, and peptide cleavage was monitored by enzyme-linked immunosorbent assay., Results: There was constitutive production of ADAM-TS4 in both cells and tissue. The protein was associated with the extracellular matrix based on the observation that the staining could be reduced following treatment of chondrocytes with heparin or exposure to chondroitinase ABC. Interestingly, there was no detectable change in the abundance of ADAM-TS4 in response to IL-1. Western blot analysis of cell lysates from IL-1-stimulated chondrocytes showed no evidence of increased ADAM-TS4 production, but resulted in activation of ADAM-TS4. The activation was associated with an increased generation in the aggrecanase neoepitope NITEGE in nasal cartilage in response to IL-1. These data suggest that induction of aggrecanase activity both in cells and in cartilage by IL-1 may involve the stimulation of an activator of ADAM-TS4. Consistent with this observation, culture of chondrocytes on a solid support containing a peptide substrate resulted in the generation of aggrecanase-mediated cleavage that could be blocked by selective inhibitors of ADAM-TS4., Conclusion: These data support the hypothesis that ADAM-TS4 is constitutively produced in these cells and tissue, and that stimulation by IL-1 results in aggrecanase activation. Thus, the activator could be a potential target by which to control aggrecanase-mediated degradation in arthritic diseases.

Published

2003

293. Discovery of gamma-lactam hydroxamic acids as selective inhibitors of tumor necrosis factor alpha converting enzyme: design, synthesis, and structure-activity relationships.

Author

Duan JJ, Chen L, Wasserman ZR, Lu Z, Liu RQ, Covington MB, Qian M, Hardman KD, Magolda RL, Newton RC, Christ DD, Wexler RR, and Decicco CP

Subjects

ADAM Proteins, ADAM17 Protein, Administration, Oral, Animals, Biological Availability, Dogs, Hydroxamic Acids chemistry, Hydroxamic Acids pharmacology, Lactams chemistry, Lactams pharmacology, Matrix Metalloproteinase 3 chemistry, Models, Molecular, Protease Inhibitors chemistry, Protease Inhibitors pharmacology, Rats, Rats, Sprague-Dawley, Structure-Activity Relationship, Swine, Hydroxamic Acids chemical synthesis, Lactams chemical synthesis, Metalloendopeptidases antagonists & inhibitors, Protease Inhibitors chemical synthesis

Abstract

New gamma-lactam TACE inhibitors were designed from known MMP inhibitors. A homology model of TACE was built and examined to identify the S1' site as the key area for TACE selectivity over MMPs. Rational exploration of the P1'-S1' interactions resulted in the discovery of the 3,5-disubstituted benzyl ether as a TACE-selective P1' group. Further optimization led to the discovery of IK682 as a selective and orally bioavailable TACE inhibitor.

Published

2002

294. Discovery and structure-activity relationship of N-(ureidoalkyl)-benzyl-piperidines as potent small molecule CC chemokine receptor-3 (CCR3) antagonists.

Author

De Lucca GV, Kim UT, Johnson C, Vargo BJ, Welch PK, Covington M, Davies P, Solomon KA, Newton RC, Trainor GL, Decicco CP, and Ko SS

Subjects

Animals, Anti-Allergic Agents chemistry, Anti-Allergic Agents pharmacology, CHO Cells, Calcium metabolism, Chemokine CCL11, Chemokines, CC pharmacology, Chemotaxis, Leukocyte drug effects, Cricetinae, Eosinophils cytology, Eosinophils drug effects, Eosinophils metabolism, Humans, In Vitro Techniques, Piperidines chemistry, Piperidines pharmacology, Receptors, CCR3, Receptors, Chemokine metabolism, Structure-Activity Relationship, Urea chemistry, Urea pharmacology, Anti-Allergic Agents chemical synthesis, Piperidines chemical synthesis, Receptors, Chemokine antagonists & inhibitors, Urea analogs & derivatives, Urea chemical synthesis

Abstract

Structure-activity relationship (SAR) studies of initial screening hits from our corporate library of compounds and a structurally related series of CCR1 receptor antagonists were used to determine that an N-(alkyl)benzylpiperidine is an essential pharmacophore for selective CCR3 antagonists. Further SAR studies that introduced N-(ureidoalkyl) substituents improved the binding potency of these compounds from the micromolar to the low nanomolar range. This new series of compounds also displays highly potent, in vitro functional CCR3-mediated antagonism of eotaxin-induced Ca(2+) mobilization and chemotaxis of human eosinophils.

Published

2002