Your search keyword '"small-molecule inhibitor"' showing total 466 results

451. Antiangiogenic therapies for glioblastoma.

Author

Arrillaga-Romany I and Norden AD

Subjects

Animals, Antibodies, Monoclonal, Humanized therapeutic use, Bevacizumab, Biomarkers metabolism, Brain Edema diagnosis, Brain Edema drug therapy, Brain Edema physiopathology, Brain Neoplasms diagnosis, Brain Neoplasms physiopathology, Drug Resistance, Neoplasm physiology, Glioblastoma diagnosis, Glioblastoma physiopathology, Humans, Randomized Controlled Trials as Topic, Angiogenesis Inhibitors therapeutic use, Brain Neoplasms drug therapy, Glioblastoma drug therapy

Abstract

Glioblastoma is the most prevalent malignant primary brain tumor in adults and to date effective durable treatments are lacking. Preclinical studies underscore the importance of neovascularization for tumor survival, making angiogenesis an important treatment target. Early clinical experience in recurrent glioblastoma suggested that antiangiogenic agents may provide clinical benefit by prolonging progression-free survival, improving quality of life and decreasing peritumoral edema. Two recent Phase III randomized trials of antiangiogenic therapy at initial diagnosis suggested improvement in progression-free survival, but failed to show an overall survival benefit. Ongoing preclinical research focuses on mechanisms of resistance and potential predictive biomarkers. Identification of targets to resistance pathways and of predictive biomarkers will hopefully improve efficacy of antiangiogenic therapies.

Published

2014

452. Small molecule inhibition of fibroblast growth factor receptors in cancer.

Author

Liang G, Chen G, Wei X, Zhao Y, and Li X

Subjects

Animals, Endometrial Neoplasms genetics, Endometrial Neoplasms metabolism, Female, Fibroblast Growth Factors genetics, Fibroblast Growth Factors metabolism, Gene Knockdown Techniques, Humans, Male, Neoplasm Proteins genetics, Neoplasm Proteins metabolism, Receptors, Fibroblast Growth Factor genetics, Receptors, Fibroblast Growth Factor metabolism, Signal Transduction drug effects, Signal Transduction genetics, Urinary Bladder Neoplasms genetics, Urinary Bladder Neoplasms metabolism, Urinary Bladder Neoplasms pathology, Antineoplastic Agents therapeutic use, Endometrial Neoplasms drug therapy, Neoplasm Proteins antagonists & inhibitors, Receptors, Fibroblast Growth Factor antagonists & inhibitors, Urinary Bladder Neoplasms drug therapy

Abstract

Fibroblast growth factors (FGFs) signal through FGF receptors (FGFRs), which are a sub-family of the superfamily of receptor tyrosine kinases, to regulate human development and metabolism. Uncontrolled FGF signaling is responsible for diverse array of developmental disorders, most notably skeletal syndromes due to FGFR gain-of-function mutations. Studies in the last few years have provided significant evidence for the importance of FGF signaling in the pathogenesis of diverse cancers, including endometrial and bladder cancers. FGFs are both potent mitogenic and angiogenic factors and can contribute to carcinogenesis by stimulating cell proliferation and tumor angiogenesis. Gene knockout and pharmacological inhibition of FGFRs in in vivo and in vitro models validate FGFRs as a target for cancer treatment. Considerable efforts are being expended to develop specific, small-molecule inhibitors for treating FGFR-driven cancers. Recent reviews on the FGF/FGFR system have focused primarily on signaling, pathophysiology, and functions in cancer. In this article, we review the key roles of FGFR in cancer, provide an update on the status of clinical trials with small-molecule FGFR inhibitors, and discuss how the current structural data on FGFR kinases guide the design and characterization of new FGFR inhibitors., (Copyright © 2013 Elsevier Ltd. All rights reserved.)

Published

2013

453. Sophoraflavanone G induces apoptosis of human cancer cells by targeting upstream signals of STATs.

Author

Kim BH, Won C, Lee YH, Choi JS, Noh KH, Han S, Lee H, Lee CS, Lee DS, Ye SK, and Kim MH

Subjects

Cell Line, Tumor, Cell Survival drug effects, Cytokines metabolism, Drug Screening Assays, Antitumor methods, Humans, NF-kappa B metabolism, Phosphorylation drug effects, STAT Transcription Factors genetics, Signal Transduction drug effects, Tyrosine metabolism, Antineoplastic Agents, Phytogenic pharmacology, Apoptosis drug effects, Flavanones pharmacology, STAT Transcription Factors metabolism

Abstract

Aberrantly activated signal transducer and activator of transcription (STAT) proteins are implicated with human cancers and represent essential roles for cancer cell survival and proliferation. Therefore, the development of small-molecule inhibitors of STAT signaling bearing pharmacological activity has therapeutic potential for the treatment of human cancers. In this study, we identified sophoraflavanone G as a novel small-molecule inhibitor of STAT signaling in human cancer cells. Sophoraflavanone G inhibited tyrosine phosphorylation of STAT proteins in Hodgkin's lymphoma and tyrosine phosphorylation of STAT3 in solid cancer cells by inhibiting phosphorylation of the Janus kinase (JAK) proteins, Src family tyrosine kinases, such as Lyn and Src, Akt, and ERK1/2. In addition, sophoraflavanone G inhibited STAT5 phosphorylation in murine-bone-marrow-derived pro-B cells transfected with translocated Ets Leukemia (TEL)-JAKs and cytokine-induced rat pre-T lymphoma cells, as well as STAT5b reporter activity in TEL-JAKs and STAT5b reporter systems. Sophoraflavanone G also inhibited nuclear factor-κB (NF-κB) signaling in multiple myeloma cells. Furthermore, sophoraflavanone G inhibited cancer cell proliferation and induced apoptosis by regulating the expression of apoptotic and anti-apoptotic proteins. Our data suggest that sophoraflavanone G is a novel small-molecule inhibitor of STAT signaling by targeting upstream signals of STATs that may have therapeutic potential for cancers caused by persistently activated STAT proteins., (Copyright © 2013 Elsevier Inc. All rights reserved.)

Published

2013

454. Validation of a cell-based ELISA as a screening tool identifying anti-alphavirus small-molecule inhibitors.

Author

Spurgers KB, Hurt CR, Cohen JW, Eccelston LT, Lind CM, Lingappa VR, and Glass PJ

Subjects

Animals, Antiviral Agents pharmacology, Chlorocebus aethiops, Enzyme-Linked Immunosorbent Assay methods, Vero Cells, Alphavirus drug effects, Antiviral Agents isolation & purification, Drug Evaluation, Preclinical methods

Abstract

Venezuelan (VEEV), eastern, and western equine encephalitis viruses, members of the genus Alphavirus, are causative agents of debilitative and sometimes fatal encephalitis. Although human cases are rare, these viruses pose a threat to military personnel, and to public health, due to their potential use as bioweapons. Currently, there are no licensed therapeutics for treating alphavirus infections. To address this need, small-molecules with potential anti-alphavirus activity, provided by collaborators, are tested routinely in live alphavirus assays utilizing time-consuming virus yield-reduction assays. To expedite the screening/hit-confirmation process, a cell-based enzyme-linked immunosorbent assay (ELISA) was developed and validated for the measurement of VEEV infection. A signal-to-background ratio of >900, and a z-factor of >0.8 indicated the robustness of this assay. For validation, the cell-based ELISA was compared directly to results from virus yield reduction assays in a single dose screen of 21 compounds. Using stringent criteria for anti-VEEV activity there was 90% agreement between the two assays (compounds displaying either antiviral activity, or no effect, in both assays). A concurrent compound-induced cell toxicity assay effectively filtered out false-positive hits. The cell-based ELISA also reproduced successfully compound dose-response virus inhibition data observed using the virus yield reduction assay. With available antibodies, this assay can be adapted readily to other viruses of interest to the biodefense community. Additionally, it is cost-effective, rapid, and amenable to automation and scale-up. Therefore, this assay could expedite greatly screening efforts and the identification of effective anti-alphavirus inhibitors., (Published by Elsevier B.V.)

Published

2013

455. Potent Targeting of the STAT3 Protein in Brain Cancer Stem Cells: A Promising Route for Treating Glioblastoma.

Author

Haftchenary S, Luchman HA, Jouk AO, Veloso AJ, Page BD, Cheng XR, Dawson SS, Grinshtein N, Shahani VM, Kerman K, Kaplan DR, Griffin C, Aman AM, Al-Awar R, Weiss S, and Gunning PT

Abstract

The STAT3 gene is abnormally active in glioblastoma (GBM) and is a critically important mediator of tumor growth and therapeutic resistance in GBM. Thus, for poorly treated brain cancers such as gliomas, astrocytomas, and glioblastomas, which harbor constitutively activated STAT3, a STAT3-targeting therapeutic will be of significant importance. Herein, we report a most potent, small molecule, nonphosphorylated STAT3 inhibitor, 31 (SH-4-54) that strongly binds to STAT3 protein (K D = 300 nM). Inhibitor 31 potently kills glioblastoma brain cancer stem cells (BTSCs) and effectively suppresses STAT3 phosphorylation and its downstream transcriptional targets at low nM concentrations. Moreover, in vivo, 31 exhibited blood-brain barrier permeability, potently controlled glioma tumor growth, and inhibited pSTAT3 in vivo. This work, for the first time, demonstrates the power of STAT3 inhibitors for the treatment of BTSCs and validates the therapeutic efficacy of a STAT3 inhibitor for GBM clinical application.

Published

2013

456. A thienopyrimidine derivative induces growth inhibition and apoptosis in human cancer cell lines via inhibiting Aurora B kinase activity.

Author

Li J, Hu H, Lang Q, Zhang H, Huang Q, Wu Y, and Yu L

Subjects

Antineoplastic Agents chemical synthesis, Antineoplastic Agents chemistry, Aurora Kinase B metabolism, Cell Line, Tumor, Cell Proliferation drug effects, Dose-Response Relationship, Drug, Drug Screening Assays, Antitumor, HCT116 Cells, HeLa Cells, Hep G2 Cells, Humans, MCF-7 Cells, Models, Molecular, Molecular Structure, Protein Kinase Inhibitors chemical synthesis, Protein Kinase Inhibitors chemistry, Pyrimidines chemical synthesis, Pyrimidines chemistry, Structure-Activity Relationship, Antineoplastic Agents pharmacology, Apoptosis drug effects, Aurora Kinase B antagonists & inhibitors, Protein Kinase Inhibitors pharmacology, Pyrimidines pharmacology

Abstract

Aurora kinases play a key role in the regulation of mitosis and have been regarded as promising targets of cancer therapy. In this paper we describe a thienopyrimidine derivative (S7), a novel potent ATP-competitive hit inhibitor of Aurora B kinase screened through a HTS system, with the IC50 141.12 nM in the biochemical kinase activity assay. Human tumor cells treated with S7 showed dose-dependent inhibition of auto-phosphorylation of Aurora B on Thr232 and another widely-used marker specific for Aurora B kinase, the phosphorylation of Histone H3 (Ser 10), demonstrating endogenous Aurora B kinase activity were inhibited at cellular level. Moreover, S7 treatment induced proliferation inhibition, colony formation inhibition and apoptosis of human tumor cell lines in a dose- and time-dependent manner., (Copyright © 2013 Elsevier Masson SAS. All rights reserved.)

Published

2013

457. In silico discovery of small-molecule Ras inhibitors that display antitumor activity by blocking the Ras-effector interaction.

Author

Shima F, Yoshikawa Y, Ye M, Araki M, Matsumoto S, Liao J, Hu L, Sugimoto T, Ijiri Y, Takeda A, Nishiyama Y, Sato C, Muraoka S, Tamura A, Osoda T, Tsuda K, Miyakawa T, Fukunishi H, Shimada J, Kumasaka T, Yamamoto M, and Kataoka T

Subjects

Animals, Cell Line, Transformed, Cell Line, Tumor, Computational Biology methods, Glutathione Transferase metabolism, Guanosine Triphosphate chemistry, Humans, Mice, Mice, Nude, Models, Molecular, Molecular Conformation, Mutation, NIH 3T3 Cells, Neoplasm Transplantation, Protein Binding, Protein Conformation, Signal Transduction, Antineoplastic Agents pharmacology, Drug Design, ras Proteins antagonists & inhibitors, ras Proteins metabolism

Abstract

Mutational activation of the Ras oncogene products (H-Ras, K-Ras, and N-Ras) is frequently observed in human cancers, making them promising anticancer drug targets. Nonetheless, no effective strategy has been available for the development of Ras inhibitors, partly owing to the absence of well-defined surface pockets suitable for drug binding. Only recently, such pockets have been found in the crystal structures of a unique conformation of Ras⋅GTP. Here we report the successful development of small-molecule Ras inhibitors by an in silico screen targeting a pocket found in the crystal structure of M-Ras⋅GTP carrying an H-Ras-type substitution P40D. The selected compound Kobe0065 and its analog Kobe2602 exhibit inhibitory activity toward H-Ras⋅GTP-c-Raf-1 binding both in vivo and in vitro. They effectively inhibit both anchorage-dependent and -independent growth and induce apoptosis of H-ras(G12V)-transformed NIH 3T3 cells, which is accompanied by down-regulation of downstream molecules such as MEK/ERK, Akt, and RalA as well as an upstream molecule, Son of sevenless. Moreover, they exhibit antitumor activity on a xenograft of human colon carcinoma SW480 cells carrying the K-ras(G12V) gene by oral administration. The NMR structure of a complex of the compound with H-Ras⋅GTP(T35S), exclusively adopting the unique conformation, confirms its insertion into one of the surface pockets and provides a molecular basis for binding inhibition toward multiple Ras⋅GTP-interacting molecules. This study proves the effectiveness of our strategy for structure-based drug design to target Ras⋅GTP, and the resulting Kobe0065-family compounds may serve as a scaffold for the development of Ras inhibitors with higher potency and specificity.

Published

2013

458. A High-Throughput Screening Method for Identification of Inhibitors of the Deubiquitinating Enzyme USP14.

Author

Lee BH, Finley D, and King RW

Abstract

Deubiquitinating enzymes (DUBs) reverse the process of ubiquitination, and number nearly 100 in humans. In principle, DUBs represent promising drug targets, as several of the enzymes have been implicated in human diseases. The isopeptidase activity of DUBs can be selectively inhibited by targeting the catalytic site with drug-like compounds. Notably, the mammalian 26S proteasome is associated with three major DUBs: RPN11, UCH37, and USP14. Because the ubiquitin 'chain-trimming' activity of USP14 can inhibit proteasome function, inhibitors of USP14 can stimulate proteasomal degradation. We recently established a high-throughput screening (HTS) method to identify small-molecule inhibitors specific for USP14. The protocols in this article cover the necessary procedures for preparing assay reagents, performing HTS for USP14 inhibitors, and carrying out post-HTS analysis. Curr. Protoc. Chem. Biol. 4:311-330 © 2012 by John Wiley & Sons, Inc.

Published

2012

459. Inhibitors of the cellular trafficking of ricin.

Author

Barbier J, Bouclier C, Johannes L, and Gillet D

Subjects

Animals, Benzamides pharmacology, Benzodiazepinones pharmacology, Drug Evaluation, Preclinical, High-Throughput Screening Assays, Humans, Protein Binding, Protein Transport drug effects, Thiophenes pharmacology, Ricin antagonists & inhibitors, Ricin pharmacokinetics

Abstract

Throughout the last decade, efforts to identify and develop effective inhibitors of the ricin toxin have focused on targeting its N-glycosidase activity. Alternatively, molecules disrupting intracellular trafficking have been shown to block ricin toxicity. Several research teams have recently developed high-throughput phenotypic screens for small molecules acting on the intracellular targets required for entry of ricin into cells. These screens have identified inhibitory compounds that can protect cells, and sometimes even animals against ricin. We review these newly discovered cellular inhibitors of ricin intoxication, discuss the advantages and drawbacks of chemical-genetics approaches, and address the issues to be resolved so that the therapeutic development of these small-molecule compounds can progress.

Published

2012

460. Targeted therapies in epithelial ovarian cancer: Molecular mechanisms of action.

Author

Itamochi H

Abstract

Ovarian cancer is the leading cause of death in women with gynecological cancer. Most patients are diagnosed at an advanced stage and have a poor prognosis. Currently, surgical tumor debulking, followed by platinum- and taxane-based chemotherapy is the standard treatment for advanced ovarian cancer. However, these patients are at great risk of recurrence and emerging drug resistance. Therefore, novel treatment strategies are required to improve outcomes for women with advanced ovarian cancer. A variety of molecular targeted agents, the majority of which are monoclonal antibodies and small-molecule protein-kinase inhibitors, have been explored in the management of ovarian cancer. The targets of these agents include angiogenesis, the human epidermal growth factor receptor family, ubiquitin-proteasome pathway, epigenetic modulators, poly(ADP-ribose) polymerase (PARP), and mammalian target of rapamycin (mTOR) signaling pathway, which are aberrant in tumor tissue. The antiangiogenic agent, bevacizumab, has been reported as the most effective targeted agent and should be included in the standard chemotherapeutic regimen for advanced ovarian cancer. PARP inhibitors, which are mainly used in breast and ovarian cancer susceptibility gene-mutated patients, and mTOR inhibitors are also attractive treatment strategies, either alone or combination with chemotherapy, for ovarian cancer. Understanding the tumor molecular biology and identification of predictive biomarkers are essential steps for selection of the best treatment strategies. This article reviews the molecular mechanisms of the most promising targeted agents that are under early phase clinical evaluation for ovarian cancer.

Published

2010

461. Mitochondrial dysfunction induced by a SH2 domain-targeting STAT3 inhibitor leads to metabolic synthetic lethality in cancer cells

Author

Genini, Davide, Brambilla, Lara, Laurini, Erik, Merulla, Jessica, Civenni, Gianluca, Pandit, Shusil, D’Antuono, Rocco, Perez, Laurent, Levy, David E., Pricl, Sabrina, Carbone, Giuseppina M., and Catapano, Carlo V.

Published

2017

462. CD4 T-cell cytokines synergize to induce proliferation of malignant and nonmalignant innate intraepithelial lymphocytes

Author

Kooy-Winkelaar, Yvonne M. C., Bouwer, Dagmar, Janssen, George M. C., Thompson, Allan, Brugman, Martijn H., Schmitz, Frederike, de Ru, Arnoud H., van Gils, Tom, Bouma, Gerd, van Rood, Jon J., van Veelen, Peter A., Mearin, M. Luisa, Mulder, Chris J., Koning, Frits, and van Bergen, Jeroen

Published

2017

463. Small molecule kinase inhibitor LRRK2-IN-1 demonstrates potent activity against colorectal and pancreatic cancer through inhibition of doublecortin-like kinase 1

Author

William L. Berry, Courtney W. Houchen, Randal May, Dongfeng Qu, Daniel Owen, Parthasarathy Chandrakesan, Ralf Janknecht, Sripathi M. Sureban, Nathaniel Weygant, and Naushad Ali

Subjects

Cancer Research, Cell Survival, Genetic Vectors, DCLK1, Gene Expression, P70-S6 Kinase 1, Antineoplastic Agents, Molecular Dynamics Simulation, Protein Serine-Threonine Kinases, Small-molecule inhibitor, Doublecortin-Like Kinases, Cell Movement, Cell Line, Tumor, Humans, Kinase activity, Protein Kinase Inhibitors, Cell Proliferation, Benzodiazepinones, Kinase inhibitor, Binding Sites, biology, Akt/PKB signaling pathway, Cyclin-dependent kinase 4, Kinase, Cell growth, Research, Cyclin-dependent kinase 2, Lentivirus, Intracellular Signaling Peptides and Proteins, Protein kinase R, Isoenzymes, Molecular Docking Simulation, Tumor stem cell, Drug Combinations, Pyrimidines, Oncology, biology.protein, Cancer research, Diffusion Chambers, Culture, Molecular Medicine, Proteoglycans, Collagen, Laminin, LRRK2-IN-1, Protein Binding

Abstract

Background Doublecortin-like kinase 1 (DCLK1) is emerging as a tumor specific stem cell marker in colorectal and pancreatic cancer. Previous in vitro and in vivo studies have demonstrated the therapeutic effects of inhibiting DCLK1 with small interfering RNA (siRNA) as well as genetically targeting the DCLK1+ cell for deletion. However, the effects of inhibiting DCLK1 kinase activity have not been studied directly. Therefore, we assessed the effects of inhibiting DCLK1 kinase activity using the novel small molecule kinase inhibitor, LRRK2-IN-1, which demonstrates significant affinity for DCLK1. Results Here we report that LRRK2-IN-1 demonstrates potent anti-cancer activity including inhibition of cancer cell proliferation, migration, and invasion as well as induction of apoptosis and cell cycle arrest. Additionally we found that it regulates stemness, epithelial-mesenchymal transition, and oncogenic targets on the molecular level. Moreover, we show that LRRK2-IN-1 suppresses DCLK1 kinase activity and downstream DCLK1 effector c-MYC, and demonstrate that DCLK1 kinase activity is a significant factor in resistance to LRRK2-IN-1. Conclusions Given DCLK1’s tumor stem cell marker status, a strong understanding of its biological role and interactions in gastrointestinal tumors may lead to discoveries that improve patient outcomes. The results of this study suggest that small molecule inhibitors of DCLK1 kinase should be further investigated as they may hold promise as anti-tumor stem cell drugs.

464. Temporal Activation of p53 by a Specific MDM2 Inhibitor Is Selectively Toxic to Tumors and Leads to Complete Tumor Growth Inhibition

Author

Shangary, Sanjeev, Qin, Dongguang, McEachern, Donna, Liu, Meilan, Miller, Rebecca S., Qiu, Su, Nikolovska-Coleska, Zaneta, Ding, Ke, Wang, Guoping, Chen, Jianyong, Bernard, Denzil, Zhang, Jian, Lu, Yipin, Gu, Qingyang, Shah, Rajal B., Pienta, Kenneth J., Ling, Xiaolan, Kang, Sanmao, Guo, Ming, Sun, Yi, Yang, Dajun, and Wang, Shaomeng

Published

2008

465. Three Classes of Glucocerebrosidase Inhibitors Identified by Quantitative High-Throughput Screening Are Chaperone Leads for Gaucher Disease

Author

Zheng, Wei, Padia, Janak, Urban, Daniel J., Jadhav, Ajit, Goker-Alpan, Ozlem, Simeonov, Anton, Goldin, Ehud, Auld, Douglas, LaMarca, Mary E., Inglese, James, Austin, Christopher P., and Sidransky, Ellen

Published

2007

466. Targeting AMAP1 and Cortactin Binding Bearing an Atypical src Homology 3/proline Interface for Prevention of Breast Cancer Invasion and Metastasis

Author

Hashimoto, Shigeru, Hirose, Mayumi, Hashimoto, Ari, Morishige, Masaki, Yamada, Atsuko, Hosaka, Harumi, Akagi, Ken-ichi, Ogawa, Eiji, Oneyama, Chitose, Agatsuma, Tsutomu, Okada, Masato, Kobayashi, Hidenori, Wada, Hiromi, Nakano, Hirofumi, Ikegami, Takahisa, Nakagawa, Atsushi, and Sabe, Hisataka

Published

2006