Your search keyword '"Kawano, Takeshi"' showing total 7 results

1. MUC1 oncoprotein blocks death receptor-mediated apoptosis by inhibiting recruitment of caspase-8.

Author

Agata N, Ahmad R, Kawano T, Raina D, Kharbanda S, and Kufe D

Subjects

Base Sequence, Cell Line, Tumor, Enzyme Activation, Humans, RNA, Small Interfering, Receptors, Death Domain physiology, Signal Transduction, Apoptosis physiology, Caspase 8 metabolism, Mucin-1 physiology, Receptors, Death Domain antagonists & inhibitors

Abstract

Stimulation of the death receptor superfamily induces the activation of caspase-8 and thereby the apoptotic response. The MUC1 oncoprotein is aberrantly overexpressed by diverse human malignancies and inhibits stress-induced apoptosis. The present results show that MUC1 blocks activation of caspase-8 and apoptosis in the response of malignant cells to tumor necrosis factor alpha, tumor necrosis factor-related apoptosis-inducing ligand, and Fas ligand. The results show that MUC1 associates constitutively with caspase-8. The MUC1 cytoplasmic domain (MUC1-CD) binds directly to the caspase-8 p18 fragment upstream to the catalytic Cys(360) site. The results also show that MUC1-CD binds to Fas-associated death domain (FADD) at the death effector domain. In nonmalignant epithelial cells, MUC1 interacts with caspase-8 and FADD as an induced response to death receptor stimulation. The functional significance of these interactions is supported by the demonstration that MUC1 competes with caspase-8 for binding to FADD and blocks recruitment of caspase-8 to the death-inducing signaling complex. These findings indicate that MUC1 is of importance to the physiologic regulation of caspase-8 activity and that overexpression of MUC1, as found in human malignancies, could contribute to constitutive inhibition of death receptor signaling pathways.

Published

2008

2. A novel isocoumarin derivative induces mitotic phase arrest and apoptosis of human multiple myeloma cells.

Author

Kawano T, Agata N, Kharbanda S, Avigan D, and Kufe D

Subjects

Cell Division drug effects, Cell Line, Tumor, Dose-Response Relationship, Drug, Drug Screening Assays, Antitumor, Flow Cytometry, Humans, Microtubules drug effects, Microtubules metabolism, Multiple Myeloma metabolism, Antimitotic Agents pharmacology, Apoptosis drug effects, Isocoumarins pharmacology, Mitosis drug effects, Multiple Myeloma pathology

Abstract

Purpose: The isocoumarin NM-3 reverses resistance of human multiple myeloma (MM) cells to dexamethasone and is in clinical trials. In the present work, the NM-3 analog, 185322, has been studied for activity against MM cells., Methods: Human U266, RPMI8226 and primary MM cells were analyzed for the effects of 185322 on cell cycle distribution, tubulin polymerization and induction of apoptosis., Results: We show that, in contrast to NM-3, treatment with 185322 is associated with a marked arrest of MM cells in M phase. The results also demonstrate that treatment with 185322 is associated with a rapid decrease in tubulin assembly and an increase in Bcl-2 phosphorylation, consistent with disruption of mitosis. Our results further demonstrate that mitotic failure induced by 185322 results in activation of an apoptotic response in MM cell lines and primary MM cells. By contrast, 185322 had little if any effect on growth and survival of human carcinoma cells., Conclusion: These findings identify a novel inhibitor of microtubule assembly that induces mitotic arrest and apoptosis of MM cells.

Published

2007

3. Depsipeptide enhances imatinib mesylate-induced apoptosis of Bcr-Abl-positive cells and ectopic expression of cyclin D1, c-Myc or active MEK abrogates this effect.

Author

Kawano T, Horiguchi-Yamada J, Iwase S, Akiyama M, Furukawa Y, Kan Y, and Yamada H

Subjects

Acetylation, Apoptosis physiology, Benzamides, Cyclin D1 genetics, Depsipeptides administration & dosage, Dose-Response Relationship, Drug, Drug Synergism, Histones metabolism, Humans, Hydroxamic Acids administration & dosage, Hydroxamic Acids pharmacology, Imatinib Mesylate, Immunoblotting, K562 Cells, MAP Kinase Kinase Kinases genetics, MAP Kinase Signaling System drug effects, Piperazines administration & dosage, Proto-Oncogene Proteins c-myc genetics, Pyrimidines administration & dosage, Antineoplastic Combined Chemotherapy Protocols pharmacology, Apoptosis drug effects, Cyclin D1 biosynthesis, Depsipeptides pharmacology, Fusion Proteins, bcr-abl biosynthesis, MAP Kinase Kinase Kinases biosynthesis, Piperazines pharmacology, Proto-Oncogene Proteins c-myc biosynthesis, Pyrimidines pharmacology

Abstract

Background: Imatinib mesylate (ST1571) is the first-line drugfor chronic myeloid leukemia (CML), but development of resistance to this drug is a clinical problem. To explore the effective use of ST1571, we studied the combination treatment with histone deacetylase inhibitor (depsipeptide, FK228)., Materials and Methods: FK228 and trichostatin A (TSA) were studied with respect to apoptosis of two Bcr-Abl-positive cell lines, K562 and TCC-S. Genetically-modified K562 cells by any of cyclin D1, c-Myc and active MEK genes were also studied. Apoptosis was examined by nuclear-morphology under a fluorescent microscope and by the expression of annexin V Changes of apoptosis-regulating genes and acetylated histone H4 were studied by immunoblot., Results: FK228 showed cytotoxicity at the nano-molar level. Combination treatment with STI571 and FK228 enhanced the induction of apoptosis significantly compared with each single treatment, although the histone acetylation level was not changed by the co-treatment. The combination treatment activated caspase-3 and cleaved PARP, but it did not induce any notable change in the expression of Bcl-XL, Bcl-2 and Bax compared with each single treatment. Enhanced apoptosis by the co-treatment was abrogated by ectopic expression of cyclin D1, c-Myc or active MEK CONCLUSION: The combination of FK228 with STI571 is a promising treatment for Bcr-Abl-positive CML, but the activation of the MEK/ERK pathway and its downstream target genes may bring resistance to the co-treatment in leukemic cells.

Published

2004

4. Telomerase overexpression in K562 leukemia cells protects against apoptosis by serum deprivation and double-stranded DNA break inducing agents, but not against DNA synthesis inhibitors.

Author

Akiyama M, Yamada O, Kanda N, Akita S, Kawano T, Ohno T, Mizoguchi H, Eto Y, Anderson KC, and Yamada H

Subjects

Antineoplastic Agents pharmacology, Apoptosis drug effects, Apoptosis radiation effects, Culture Media, Serum-Free, Cytarabine pharmacology, DNA Damage drug effects, DNA Damage genetics, DNA Damage radiation effects, DNA Replication drug effects, Etoposide pharmacology, Humans, Hydroxyurea pharmacology, K562 Cells drug effects, K562 Cells radiation effects, Nucleic Acid Synthesis Inhibitors pharmacology, Telomerase genetics, Telomere pathology, Transfection, Apoptosis genetics, K562 Cells enzymology, K562 Cells pathology, Telomerase biosynthesis

Abstract

Telomeres are specialized DNA/protein structures that act as protective caps to prevent end fusions. The maintenance of telomeres is essential for chromosomal stability. Telomerase is regulated by human telomerase reverse transcriptase (hTERT). c-Myc oncoprotein is also implicated in the positive regulation of hTERT expression. We show here that two clones of hTERT-transfected K562 erythroleukemia cells have elongated telomeres (22.5 and 24.0 kb), whereas telomere length of both c-Myc-transfected K562 cells and parental K562 cells is 6.5 kb. Telomerase activity and hTERT mRNA expression increased in hTERT-transfected K562 cells, while the expression levels of telomerase activity and hTERT in c-Myc-transfected K562 cells were similar to that in parental K562 cells, despite an overexpression of c-Myc. Importantly, we found that hTERT-transfected K562 cells are protected against apoptosis induced by serum deprivation and double-stranded DNA break inducing agents (ionizing irradiation, and etoposide (VP-16)), but not against DNA synthesis inhibitors (1-beta-D-arabinofuranosylcytosine and hydroxyurea). These findings suggest that overexpression of telomerase by transfecting hTERT confers telomere-elongation and resistance to double-stranded DNA break inducing agents.

Published

2002

5. Biological effects of a relatively low concentration of 1-b-D-arabinofuranosylcytosine in K562 cells: Alterations of the cell cycle, erythroid-differentiation, and apoptosis

Author

Yamada, Hisashi, Horiguchi-Yamada, Junko, Nagai, Makoto, Takahara, Shinobu, Sekikawa, Tetsuaki, Kawano, Takeshi, Itoh, Kiyoshi, Fukumi, Sachiko, and Iwase, Satsuki

Published

1998

6. Ectopic cyclin D1 expression blocks STI571-induced erythroid differentiation of K562 cells

Author

Kawano, Takeshi, Horiguchi-Yamada, Junko, Saito, Shinobu, Iwase, Satsuki, Furukawa, Yusuke, Kano, Yasuhiko, and Yamada, Hisashi

Subjects

*PROTEIN-tyrosine kinase inhibitors, *APOPTOSIS, *GENE expression, *CELL membranes

Abstract

Bcr-Abl tyrosine kinase inhibitor induces apoptosis and erythroid differentiation of K562 cells. During this erythroid differentiation, c-Myc and cyclin D1 transcripts are transiently downregulated. Accordingly, we studied the effect of cyclin D1 overexpression on erythroid differentiation. After treatment with 250 nM STI571, 90% of K562 and 25% of K562/D1 cells underwent erythroid differentiation. The basal expression of glycophorin A in K562/D1 cells was markedly diminished compared with that by parental cells. STI571 treatment failed to induce glycophorin A expression in K562/D1 cells. During STI571 treatment, ERK activity was downregulated in parental cells, while it was constantly activated in K562/D1 cells. These results suggest that ectopic expression of cyclin D1 causes the resistance of K562 cells to erythroid differentiation by modulating ERK regulation. [Copyright &y& Elsevier]

Published

2004

7. Antitumor activity of TMPyP4 interacting G-quadruplex in retinoblastoma cell lines

Author

Mikami-Terao, Yoko, Akiyama, Masaharu, Yuza, Yuki, Yanagisawa, Takaaki, Yamada, Osamu, Kawano, Takeshi, Agawa, Miyuki, Ida, Hiroyuki, and Yamada, Hisashi

Subjects

*ANTINEOPLASTIC agents, *PORPHYRINS, *QUADRUPLEX nucleic acids, *RETINOBLASTOMA, *CELL lines, *CANCER cell growth, *CELL cycle regulation, *APOPTOSIS, *THERAPEUTICS, *PREVENTION

Abstract

Abstract: To investigate the molecular mechanism of the antitumor activity of the cationic porphyrin 5, 10, 15, 20-tetra-(N-methyl-4-pyridyl)porphyrin (TMPyP4) in retinoblastoma cell lines, Y79 and WERI-Rb1 cells were treated with TMPyP4 for 0–72 h, after which growth inhibition, modulation of the cell cycle and the induction of apoptosis were examined. In addition, the effect of TMPyP4 on the susceptibility to irradiation was evaluated in Y79 and WERI-Rb1 cells. In vitro telomeric repeat amplification protocol assay showed TMPyP4 (10–100 μM) directly blocked telomerase elongation, suggesting that TMPyP4 can form stable guanine (G)-quadruplexes in extending telomere repeats in substrate oligonucleotides. The antiproliferative activities of TMPyP4 assessed with the MTS assay and expressed in terms of IC50: Y79 cells, 60 μM; WERI-Rb1 cells, 45 μM. Treatment with TMPyP4 at doses of 10, 20, 50 or 100 μM for 48 or 72 h significantly inhibited the growth of Y79 and WERI-Rb1 cells. Apoptosis, as assessed with CaspACE™ FITC-VAD-FMK, was induced by TMPyP4 in a dose-dependent manner. Induction of apoptosis by TMPyP4 was associated with increased expression of phosphorylated DNA damage response factor H2AX (Ser139), phosphorylated p53 (Ser46) protein and activation of mitogen-activated protein kinases in Y79 and WERI-Rb1 cells. Moreover, TMPyP4 significantly enhanced the susceptibility to irradiation in both cell lines. This study provides insight into the molecular mechanism of the antitumor effects of TMPyP4. G-quadruplex structure may be a potential therapeutic target in retinoblastoma. [Copyright &y& Elsevier]

Published

2009