Your search keyword '"Chang, Hyo Won"' showing total 59 results

51. Tristetraprolin regulates phagocytosis through interaction with CD47 in head and neck cancer.

Author

Lee, Won Hyeok, Kim, Song Hee, An, Jae Hee, Kim, Tae-Koon, Cha, Hee Jeong, Chang, Hyo Won, Kim, Sang Yoon, Kim, Seong Who, and Han, Myung Woul

Subjects

HEAD & neck cancer, CD47 antigen, PHAGOCYTIC function tests, PHAGOCYTOSIS, REVERSE transcriptase polymerase chain reaction

Abstract

CD47 is expressed in all human cancer cells, including head and neck cancer, and initiates a signaling cascade to inhibit macrophage phagocytosis. However, the mechanism underlying CD47 overexpression has not been elucidated in radioresistant head and neck cancer. The present study demonstrated that decreased Tristetraprolin (TTP) expression induced a sustained overexpression of CD47 using reverse transcription-quantitative PCR and western blotting, and that CD47 overexpression prevented phagocytosis using a phagocytosis assay in a radioresistant HN31R cell line. Subsequently, using TTP transfection, RNA interference, duel-luciferase assay and EMSA, it was revealed that TTP transfection enhanced phagocytosis through degradation of CD47 mRNA by directly binding to CD47 AREs within the CD47 3'UTR. Based on our previous study, methylation-specific PCR and western blotting revealed that DNMT1 was overexpressed in radioresistant HN31R cell line and TTP expression was decreased epigenetically by DMNT1 associated DNA methylation. Overall, these findings provided novel insight into the role of TTP as a biomarker of CD47-positive head and neck cancer patients. [ABSTRACT FROM AUTHOR]

Published

2022

52. Putative progenitor/stem cells isolated from human oral mucosa are resistant to ionizing radiation

Author

Jeong, Eun-Jeong, primary, Choi, Seung-Ho, additional, Chang, Sung-eun, additional, Chang, Hyo Won, additional, Roh, Jong-Lyel, additional, Lee, Sang-wook, additional, Chung, Yoo-Sam, additional, and Kim, Sang Yoon, additional

Published

2008

53. Wnt signaling controls radiosensitivity via cyclooxygenase‐2‐mediated Ku expression in head and neck cancer

Author

Chang, Hyo Won, primary, Roh, Jong‐Lyel, additional, Jeong, Eun‐Jeong, additional, Lee, Sang‐wook, additional, Kim, Seung‐Whan, additional, Choi, Seung‐Ho, additional, Park, Sung‐Kyung, additional, and Kim, Sang Yoon, additional

Published

2007

54. Biological removal of explosive 2,4,6-trinitrotoluene by Stenotrophomonas sp. OK-5 in bench-scale bioreactors.

Author

Lee, Myung-Seok, Chang, Hyo-Won, Kahng, Hyung-Yeel, So, Jae-Seong, and Oh, Kye-Heon

Published

2002

55. Biological removal of explosive 2,4,6-trinitrotoluene byStenotrophomonassp. OK-5 in bench-scale bioreactors

Author

Lee, Myung-Seok, Chang, Hyo-Won, Kahng, Hyung-Yeel, So, Jae-Seong, and Oh, Kye-Heon

Abstract

The biological removal of 2,4,6-trinitrotoluene (TNT) was studied in a bench-scale bioreactor using a bacterial culture of strain OK-5 originally isolated from soil samples contaminated with TNT. The TNT was completely removed within 4 days of incubation in a 2.5 L benchscale bioreactor containing a newly developed medium. The TNT was catabolized in the presence of different supplemented carbons. Only minimal growth was observed in the killed controls and cultures that only received TNT during the incubation period. This catabolism was affected by the concentration ratio of the substrate to the biomass. The addition of various nitrogen sources produced a delayed effect for the TNT degradation. Tween 80 enhanced the degradation of TNT under these conditions. Two metabolic intermediates were detected and identified as 2-amino-4,6-dinitrotoluene and 4-amino-2,6-dinitrotoluene based on HPLC and GC-MS analyses, respectively. Strain OK-5 was characterized using the BIOLOG system and fatty acid profile produced by a microbial identification system equipped with a Hewlett packard HP 5890 II gas chromatograph. As such, the bacterium was identified as aStenotrophomonasspecies and designated asStenotrophomonassp. OK-5.

Published

2002

56. Metronomic oral doxorubicin in combination of Chk1 inhibitor MK-8776 for p53-deficient breast cancer treatment.

Author

Lee, Hanul, Choi, Jeong Uk, Chung, Seung Woo, Kim, Gui Chul, Kim, Sang Yoon, Byun, Youngro, Chang, Hyo Won, Kim, Ji Won, Kweon, Seho, Mahmud, Foyez, and Son, Woo-Chan

Subjects

*DOXORUBICIN, *CANCER chemotherapy, *KINASE inhibitors, *P53 protein, *BREAST cancer treatment

Abstract

Abstract Metronomic chemotherapy, which is defined as a low-dose and frequent administration of cytotoxic drugs without drug-free breaks, has been recently emerged as an alternative to traditional MTD therapy and has shown therapeutic benefit in breast cancer patients in numbers of clinical studies. Unlike MTD, metronomic chemotherapy acts by multiple mechanisms including antiangiogenic effect and immunomodulation, but the direct cytotoxic effect only playing a minor role due to the lowered dose. In this light, within the limits of p53-deficient breast cancer, we demonstrate the enhanced anticancer effect of metronomic chemotherapy using doxorubicin when combined with Chk1 inhibitor MK-8776 by specifically augmenting the direct cytotoxic effect on cancer cells. Since the oral drug is greatly favored in metronomic chemotherapy due to the frequent and potential long-term administration, we prepared an oral doxorubicin by producing an ionic complex with deoxycholic acid, which showed sufficient bioavailability and anticancer effect when administered orally. MK-8776 selectively enhanced the cytotoxic effect of low-concentration doxorubicin in p53-deficient breast cancer cells by abrogating the Chk1-dependent cell cycle arrest in vitro. Consistently, combining MK-8776 significantly improved the anticancer effect of the daily administered oral doxorubicin in p53-deficient breast cancer xenografts especially in a lower dose of doxorubicin without evident systemic toxicities. Combination therapy of MK-8776 and metronomic oral doxorubicin would be thus promising in the treatment of p53-deficient breast cancer benefited from the augmented direct cytotoxic effect and low risk of toxicities. [ABSTRACT FROM AUTHOR]

Published

2018

57. Exosome-guided direct reprogramming of tumor-associated macrophages from protumorigenic to antitumorigenic to fight cancer.

Author

Kim H, Park HJ, Chang HW, Back JH, Lee SJ, Park YE, Kim EH, Hong Y, Kwak G, Kwon IC, Lee JE, Lee YS, Kim SY, Yang Y, and Kim SH

Abstract

Highly immunosuppressive tumor microenvironment containing various protumoral immune cells accelerates malignant transformation and treatment resistance. In particular, tumor-associated macrophages (TAMs), as the predominant infiltrated immune cells in a tumor, play a pivotal role in regulating the immunosuppressive tumor microenvironment. As a potential therapeutic strategy to counteract TAMs, here we explore an exosome-guided in situ direct reprogramming of tumor-supportive M2-polarized TAMs into tumor-attacking M1-type macrophages. Exosomes derived from M1-type macrophages (M1-Exo) promote a phenotypic switch from anti-inflammatory M2-like TAMs toward pro-inflammatory M1-type macrophages with high conversion efficiency. Reprogrammed M1 macrophages possessing protein-expression profiles similar to those of classically activated M1 macrophages display significantly increased phagocytic function and robust cross-presentation ability, potentiating antitumor immunity surrounding the tumor. Strikingly, these M1-Exo also lead to the conversion of human patient-derived TAMs into M1-like macrophages that highly express MHC class II, offering the clinical potential of autologous and allogeneic exosome-guided direct TAM reprogramming for arming macrophages to join the fight against cancer., Competing Interests: The authors declare no conflicts of interest., (© 2022 The Authors.)

Published

2022

58. Autophagy inhibition can overcome radioresistance in breast cancer cells through suppression of TAK1 activation.

Author

Han MW, Lee JC, Choi JY, Kim GC, Chang HW, Nam HY, Kim SW, and Kim SY

Subjects

Antifungal Agents pharmacology, Antimalarials pharmacology, Autophagy radiation effects, Blotting, Western, Breast Neoplasms drug therapy, Breast Neoplasms radiotherapy, Cell Proliferation drug effects, Cell Proliferation radiation effects, Chloroquine pharmacology, Female, Gamma Rays, Gene Expression Regulation, Neoplastic radiation effects, Humans, Macrolides pharmacology, Phosphorylation drug effects, Signal Transduction radiation effects, Tumor Cells, Cultured, Autophagy drug effects, Breast Neoplasms metabolism, Breast Neoplasms pathology, Gene Expression Regulation, Neoplastic drug effects, MAP Kinase Kinase Kinases metabolism, Radiation Tolerance drug effects, Signal Transduction drug effects

Abstract

Background/aim: Autophagy is frequently activated in radioresistant cancer cells. In the present study, we evaluated the role of autophagy and transforming growth factor-activated kinase 1 (TAK1) in radioresistance., Materials and Methods: TAK1 phosphorylation in MDA-MB231 breast cancer cells was evaluated by western blotting. The regulatory effects of the TAK1 inhibitor and autophagy inhibitor were assessed by cell morphology, cell survival and induction of apoptosis., Results: Radiation induced the phosphorylation of TAK1, whereas the inhibition of TAK1 activity enhanced the cytotoxicity of radiation in MDA-MB231 cells. Autophagy inhibitors significantly enhanced radiation-induced apoptosis of MDA-MB231 cells. This augmentation in radiosensitivity seemed to result from the suppression of TAK1 activation., Conclusion: Inhibition of autophagy enhanced radiosensitivity through suppression of radiation-induced TAK1 activation, suggesting that the modulation of TAK1-induced autophagy may be a good therapeutic strategy to treat radioresistant breast cancer.

Published

2014

59. Proteomic analysis of two head and neck cancer cell lines presenting different radiation sensitivity.

Author

Lee YS, Chang HW, Jeong JE, Lee SW, and Kim SY

Subjects

Antioxidants metabolism, Blotting, Western, Cell Line, Tumor, Electrophoresis, Gel, Two-Dimensional, HSP27 Heat-Shock Proteins, Humans, Molecular Chaperones, Reactive Oxygen Species metabolism, Cell Survival radiation effects, Glutathione S-Transferase pi analysis, Heat-Shock Proteins analysis, Neoplasm Proteins analysis, Otorhinolaryngologic Neoplasms pathology, Otorhinolaryngologic Neoplasms radiotherapy, Peroxiredoxins analysis, Proteomics, Radiation Tolerance radiation effects

Abstract

Conclusion: We found four proteins in the AMC-HN-9 cells that might perform important functions in radio-resistance. These results also suggest that this cell line may provide us with important information about cancer cells regarding the roles of reactive oxygen species (ROS and antioxidants) in irradiation., Objective: Radiation susceptibility can be determined by the expression of some proteins. To identify such proteins involved in radiation susceptibility, we analyzed two cell lines with different radiation sensitivity., Materials and Methods: The AMC-HN-3 and -9 cell lines established from head and neck cancer patients were employed. They were irradiated with 4 Gy and two-dimensional polyacrylamide gel electrophoresis (2-D PAGE) was carried out. Then matrix-assisted laser desorption/ionization time-of-flight (MALDI-TOF) mass spectrometry (MS) was performed to identify 20 proteins. Western blotting was used to confirm the significantly expressed proteins., Results: After 2-D PAGE, five spots were differentially expressed in the AMC-HN-9. Heat shock protein 27 kDa (HSP27), peroxiredoxin (Prx) II, glutathione S-transferase pi (GSTP), and an unknown protein were detected through MALDI-TOF MS. By using Western blotting, remarkable increments of the band intensity of HSP27, GSTP, Prx II, and Prx IV were confirmed in the AMC-HN-9 cell line.

Published

2008