Your search keyword '"Platt, James T."' showing total 6 results

1. The broad-spectrum receptor tyrosine kinase inhibitor dovitinib suppresses growth of BRAF-mutant melanoma cells in combination with other signaling pathway inhibitors.

Author

Langdon CG, Held MA, Platt JT, Meeth K, Iyidogan P, Mamillapalli R, Koo AB, Klein M, Liu Z, Bosenberg MW, and Stern DF

Subjects

Animals, Cell Line, Tumor, Cell Proliferation drug effects, Drug Resistance, Neoplasm drug effects, Drug Synergism, Humans, Indoles pharmacology, Male, Melanoma enzymology, Mice, Nude, Neoplasm Proteins metabolism, Skin Neoplasms, Small Molecule Libraries pharmacology, Sulfonamides pharmacology, Vemurafenib, Melanoma, Cutaneous Malignant, Benzimidazoles pharmacology, Melanoma genetics, Melanoma pathology, Mutation genetics, Protein Kinase Inhibitors pharmacology, Quinolones pharmacology, Signal Transduction drug effects

Abstract

BRAF inhibitors have revolutionized treatment of mutant BRAF metastatic melanomas. However, resistance develops rapidly following BRAF inhibitor treatment. We have found that BRAF-mutant melanoma cell lines are more sensitive than wild-type BRAF cells to the small molecule tyrosine kinase inhibitor dovitinib. Sensitivity is associated with inhibition of a series of known dovitinib targets. Dovitinib in combination with several agents inhibits growth more effectively than either agent alone. These combinations inhibit BRAF-mutant melanoma and colorectal carcinoma cell lines, including cell lines with intrinsic or selected BRAF inhibitor resistance. Hence, combinations of dovitinib with second agents are potentially effective therapies for BRAF-mutant melanomas, regardless of their sensitivity to BRAF inhibitors., (© 2015 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2015

2. PDK1 and SGK3 Contribute to the Growth of BRAF-Mutant Melanomas and Are Potential Therapeutic Targets.

Author

Scortegagna M, Lau E, Zhang T, Feng Y, Sereduk C, Yin H, De SK, Meeth K, Platt JT, Langdon CG, Halaban R, Pellecchia M, Davies MA, Brown K, Stern DF, Bosenberg M, and Ronai ZA

Subjects

Animals, Benzoates pharmacology, Bridged Bicyclo Compounds, Heterocyclic pharmacology, Cell Line, Tumor, Drug Screening Assays, Antitumor, G1 Phase Cell Cycle Checkpoints, Humans, Immediate-Early Proteins metabolism, Indazoles pharmacology, Lymphatic Metastasis, Melanoma drug therapy, Melanoma secondary, Mice, Knockout, Molecular Targeted Therapy, Protein Kinase Inhibitors pharmacology, Protein Serine-Threonine Kinases metabolism, Pyrimidines pharmacology, Pyruvate Dehydrogenase Acetyl-Transferring Kinase, Skin enzymology, Skin pathology, Skin Neoplasms drug therapy, Skin Neoplasms pathology, Melanoma enzymology, Protein Serine-Threonine Kinases physiology, Proto-Oncogene Proteins B-raf genetics, Skin Neoplasms enzymology

Abstract

Melanoma development involves members of the AGC kinase family, including AKT, PKC, and, most recently, PDK1, as elucidated recently in studies of Braf::Pten mutant melanomas. Here, we report that PDK1 contributes functionally to skin pigmentation and to the development of melanomas harboring a wild-type PTEN genotype, which occurs in about 70% of human melanomas. The PDK1 substrate SGK3 was determined to be an important mediator of PDK1 activities in melanoma cells. Genetic or pharmacologic inhibition of PDK1 and SGK3 attenuated melanoma growth by inducing G1 phase cell-cycle arrest. In a synthetic lethal screen, pan-PI3K inhibition synergized with PDK1 inhibition to suppress melanoma growth, suggesting that focused blockade of PDK1/PI3K signaling might offer a new therapeutic modality for wild-type PTEN tumors. We also noted that responsiveness to PDK1 inhibition associated with decreased expression of pigmentation genes and increased expression of cytokines and inflammatory genes, suggesting a method to stratify patients with melanoma for PDK1-based therapies. Overall, our work highlights the potential significance of PDK1 as a therapeutic target to improve melanoma treatment., (©2015 American Association for Cancer Research.)

Published

2015

3. MERTK controls melanoma cell migration and survival and differentially regulates cell behavior relative to AXL.

Author

Tworkoski KA, Platt JT, Bacchiocchi A, Bosenberg M, Boggon TJ, and Stern DF

Subjects

Cell Line, Tumor, Cell Movement, Cell Proliferation, Cell Survival, Cytophotometry, Gene Expression Profiling, HEK293 Cells, Humans, Neoplasm Metastasis, Oligonucleotide Array Sequence Analysis, Phosphorylation, Proto-Oncogene Proteins genetics, Receptor Protein-Tyrosine Kinases genetics, Signal Transduction, Skin Neoplasms metabolism, c-Mer Tyrosine Kinase, cdc42 GTP-Binding Protein metabolism, Axl Receptor Tyrosine Kinase, Gene Expression Regulation, Neoplastic, Melanoma metabolism, Proto-Oncogene Proteins metabolism, Proto-Oncogene Proteins physiology, Receptor Protein-Tyrosine Kinases metabolism, Receptor Protein-Tyrosine Kinases physiology

Abstract

The receptor tyrosine kinase AXL regulates melanoma cell proliferation and migration. We now demonstrate that AXL and the related kinase MERTK are alternately expressed in melanoma and are associated with different transcriptional signatures. MERTK-positive melanoma cells are more proliferative and less migratory than AXL-positive melanoma cells and overexpression of AXL increases cell motility relative to MERTK. MERTK is expressed in up to 50% of melanoma cells and shRNA-mediated knockdown of MERTK reduces colony formation and cell migration in a CDC42-dependent fashion. Targeting MERTK also decreases cell survival and proliferation in an AKT-dependent manner. Finally, we identify a novel mutation in the kinase domain of MERTK, MERTK(P) (802S) , that increases the motility of melanoma cells relative to wild-type MERTK. Together, these data demonstrate that MERTK is a possible therapeutic target in melanoma, that AXL and MERTK are associated with differential cell behaviors, and that mutations in MERTK may contribute to melanoma pathogenesis., (© 2013 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2013

4. Genotype-selective combination therapies for melanoma identified by high-throughput drug screening.

Author

Held MA, Langdon CG, Platt JT, Graham-Steed T, Liu Z, Chakraborty A, Bacchiocchi A, Koo A, Haskins JW, Bosenberg MW, and Stern DF

Subjects

Animals, Cell Line, Tumor, Drug Interactions, Drug Resistance, Neoplasm, Drug Therapy, Combination, Genes, ras genetics, High-Throughput Screening Assays, Humans, Melanoma genetics, Mice, Mice, Nude, Xenograft Model Antitumor Assays, Antineoplastic Agents administration & dosage, Melanoma drug therapy, Proto-Oncogene Proteins B-raf genetics, ras Proteins genetics

Abstract

Unlabelled: Resistance and partial responses to targeted monotherapy are major obstacles in cancer treatment. Systematic approaches to identify efficacious drug combinations for cancer are not well established, especially in the context of genotype. To address this, we have tested pairwise combinations of an array of small-molecule inhibitors on early-passage melanoma cultures using combinatorial drug screening. Results reveal several inhibitor combinations effective for melanomas with activating RAS or BRAF mutations, including mutant BRAF melanomas with intrinsic or acquired resistance to vemurafenib. Inhibition of both EGF receptor and AKT sensitized treatment-resistant BRAF mutant melanoma cultures to vemurafenib. Melanomas with RAS mutations were more resistant to combination therapies relative to BRAF mutants, but were sensitive to combinations of statins and cyclin-dependent kinase inhibitors in vitro and in vivo. These results show the use of combinatorial drug screening for discovering unique treatment regimens that overcome resistance phenotypes of mutant BRAF- and RAS-driven melanomas., Significance: We have used drug combinatorial screening to identify effective combinations for mutant BRAF melanomas, including those resistant to vemurafenib, and mutant RAS melanomas that are resistant to many therapies. Mechanisms governing the interactions of the drug combinations are proposed, and in vivo xenografts show the enhanced benefit and tolerability of a mutant RAS -selective combination, which is currently lacking in the clinic.

Published

2013

5. Polymerization of 5,6-dihydroxyindole-2-carboxylic acid to melanin by the pmel 17/silver locus protein.

Author

Chakraborty, Ashok K., Platt, James T., Kim, Kack K., Byoung Se Kwon, Bennett, Dorothy C., and Pawelek, John M.

Subjects

*MELANOGENESIS, *CARBOXYLIC acids, *PHYSIOLOGICAL oxidation, *MELANOMA, *SUPEROXIDES, *BIOCHEMISTRY

Abstract

Recent advances in melanogenesis have focused on the role of dihydroxyindole-2-carboxylic acid [(HO)2IndCOOH]. For example, it has been shown that formation of (HO)2IndCOOH from depachrome is catalyzed by dopachrome tautomerase, that the melanogenic protein tyrosinase-related protein (TRP)-1 can oxidize (HO)2IndCOOH to its indole quinone, that (HO)2IndCOOH-melanins can be synthesized chemically, that mammalian melanins are naturally rich in (HO)2IndCOOH subunits, and that (HO)2IndCOOH is incorporated into melanins are naturally rich in (HO)2IndCOOH subunits, and that (HO)2IndCOOH is incorporated into melanins of melanomas in mice. The question thus emerges as to the mechanims(s) by which (HO)2IndCOOH and other precursors become incorporated into melanins in vivo. Accordingly, an activity was partially purified that catalyzed melanin formation with (HO)2IndCOOH as a substrate. Analyses of the (HO)2IndCOOH polymerization factor from Cloudman melanoma cells revealed the following: it was proteinaceous in that it was heat labile and destroyed by proteinase K; it was a glycoprotein in that it adhered to wheat germ agglutinin and was eluted with N-acetyl glucosamine; it was located predominantly in the melanosomal fraction of cell homogenates; the activity was reduced by exposure to the metal chelators EDTA and EGTA, but not by phenylthiourea, a tyrosinase inhibitor; activity was found with the mouse pmel 17/silver locus protein immunopurified from human melanoma cells, and was significantly reduced in extracts of mouse melanocytes cultured from silver (si/si) mice compare to extracts from Si/Si melanocytes. In summary, an activity has been identified in human to mouse melanoma cells that catalyzes the superoxide-dependent polymerization of (HO)2IndCOOH to melanin in vitro, and appears to be a function of the pmel 17/silver protein of the human pmel 17 gene and the mouse silver locus. [ABSTRACT FROM AUTHOR]

Published

1996

6. β-Catenin Signaling Controls Metastasis in Braf-Activated Pten-Deficient Melanomas

Author

Damsky, William E., Curley, David P., Santhanakrishnan, Manjula, Rosenbaum, Lara E., Platt, James T., Gould Rothberg, Bonnie E., Taketo, Makoto M., Dankort, David, Rimm, David L., McMahon, Martin, and Bosenberg, Marcus

Subjects

*CELLULAR signal transduction, *MELANOMA, *METASTASIS, *GENETIC mutation, *CELL differentiation, *LABORATORY mice

Abstract

Summary: Malignant melanoma is characterized by frequent metastasis, however, specific changes that regulate this process have not been clearly delineated. Although it is well known that Wnt signaling is frequently dysregulated in melanoma, the functional implications of this observation are unclear. By modulating β-catenin levels in a mouse model of melanoma that is based on melanocyte-specific Pten loss and BrafV600E mutation, we demonstrate that β-catenin is a central mediator of melanoma metastasis to the lymph nodes and lungs. In addition to altering metastasis, β-catenin levels control tumor differentiation and regulate both MAPK/Erk and PI3K/Akt signaling. Highly metastatic tumors with β-catenin stabilization are very similar to a subset of human melanomas. Together these findings establish Wnt signaling as a metastasis regulator in melanoma. [ABSTRACT FROM AUTHOR]

Published

2011