Your search keyword '"Hung, Jan-Jong"' showing total 6 results

1. USP24-i-101 targeting of USP24 activates autophagy to inhibit drug resistance acquired during cancer therapy.

Author

Young MJ, Wang SA, Chen YC, Liu CY, Hsu KC, Tang SW, Tseng YL, Wang YC, Lin SM, and Hung JJ

Subjects

Animals, Humans, Mice, Cell Line, Tumor, Lung Neoplasms drug therapy, Lung Neoplasms pathology, Lung Neoplasms metabolism, Lung Neoplasms genetics, Autophagy drug effects, Drug Resistance, Neoplasm drug effects, Ubiquitin Thiolesterase metabolism, Ubiquitin Thiolesterase genetics, Ubiquitin Thiolesterase antagonists & inhibitors

Abstract

Drug resistance in cancer therapy is the major reason for poor prognosis. Addressing this clinically unmet issue is important and urgent. In this study, we found that targeting USP24 by the specific USP24 inhibitors, USP24-i and its analogues, dramatically activated autophagy in the interphase and mitotic periods of lung cancer cells by inhibiting E2F4 and TRAF6, respectively. USP24 functional knockout, USP24 C1695A , or targeting USP24 by USP24-i-101 inhibited drug resistance and activated autophagy in gefitinib-induced drug-resistant mice with doxycycline-induced EGFR L858R lung cancer, but this effect was abolished after inhibition of autophagy, indicating that targeting USP24-mediated induction of autophagy is required for inhibition of drug resistance. Genomic instability and PD-L1 levels were increased in drug resistant lung cancer cells and were inhibited by USP24-i-101 treatment or knockdown of USP24. In addition, inhibition of autophagy by bafilomycin-A1 significantly abolished the effect of USP24-i-101 on maintaining genomic integrity, decreasing PD-L1 and inhibiting drug resistance acquired in chemotherapy or targeted therapy. In summary, an increase in the expression of USP24 in cancer cells is beneficial for the induction of drug resistance and targeting USP24 by USP24-i-101 optimized from USP24-i inhibits drug resistance acquired during cancer therapy by increasing PD-L1 protein degradation and genomic stability in an autophagy induction-dependent manner., (© 2024. The Author(s).)

Published

2024

2. Tp53 haploinsufficiency is involved in hotspot mutations and cytoskeletal remodeling in gefitinib-induced drug-resistant EGFR L858R -lung cancer mice.

Author

Wang YS, Young MJ, Liu CY, Chen YC, and Hung JJ

Abstract

Tumor heterogeneity is the major factor for inducing drug resistance. p53 is the major defender to maintain genomic stability, which is a high proportion mutated in most of the cancer types. In this study, we established in vivo animal models of gefitinib-induced drug-resistant lung cancer containing EGFR L858R and EGFR L858R *Tp53 +/- mice to explore the molecular mechanisms of drug resistance by studying the genomic integrity and global gene expression. The cellular morphology of the lung tumors between gefitinib-induced drug-resistant mice and drug-sensitive mice were very different. In addition, in drug-resistant mice, the expression of many cytoskeleton-related genes were changed, accompanied by decreased amounts of actin filaments and increased amounts of microtubule, indicating that significant cytoskeletal remodeling is induced in gefitinib-induced drug-resistant EGFR L858R and EGFR L858R *Tp53 +/- lung cancer mice. The gene expression profiles and involved pathways were different in gefitinib-sensitive, gefitinib-resistant and Tp53 +/- -mice. Increases in drug resistance and nuclear size (N/C ratio) were found in EGFR L858R *Tp53 +/- drug-resistant mice. Mutational hotspot regions for drug resistance via Tp53 +/+ - and Tp53 +/- -mediated pathways are located on chromosome 1 and chromosome 11, respectively, and are related to prognosis of lung cancer cohorts. This study not only builds up a gefitinib-induced drug-resistant EGFR L858R lung cancer animal model, but also provides a novel mutation profile in a Tp53 +/+ - or Tp53 +/- -mediated manner and induced cytoskeleton remodeling during drug resistance, which could contribute to the prevention of drug resistance during cancer therapy., (© 2023. The Author(s).)

Published

2023

3. USP24 promotes drug resistance during cancer therapy.

Author

Wang SA, Young MJ, Wang YC, Chen SH, Liu CY, Lo YA, Jen HH, Hsu KC, and Hung JJ

Subjects

Animals, Drug Resistance, Neoplasm, Humans, Mice, Mice, SCID, Transfection, Drug Development methods, Neoplasms therapy, Ubiquitin Thiolesterase metabolism

Abstract

Drug resistance has remained an important issue in the treatment and prevention of various diseases, including cancer. Herein, we found that USP24 not only repressed DNA-damage repair (DDR) activity by decreasing Rad51 expression to cause the tumor genomic instability and cancer stemness, but also increased the levels of the ATP-binding cassette (ABC) transporters P-gp, ABCG2, and ezrin to enhance the pumping out of Taxol from cancer cells, thus resulted in drug resistance during cancer therapy. A novel USP24 inhibitor, NCI677397, was screened for specific inhibiting the catalytic activity of USP24. This inhibitor was identified to suppress drug resistance via decreasing genomic instability, cancer stemness, and the pumping out of drugs from cancer cells. Understanding the role and molecular mechanisms of USP24 in drug resistance will be beneficial for the future development of a novel USP24 inhibitor. Our studies provide a new insight of USP24 inhibitor for clinically implication of blocking drug resistance during chemotherapy., (© 2021. The Author(s).)

Published

2021

4. USP24 stabilizes bromodomain containing proteins to promote lung cancer malignancy.

Author

Wang SA, Young MJ, Jeng WY, Liu CY, and Hung JJ

Subjects

A549 Cells, Cell Line, Tumor, Cell Movement physiology, Cell Proliferation physiology, Disease Progression, Humans, Protein Stability, Transcription, Genetic physiology, Ubiquitin metabolism, Lung Neoplasms metabolism, Lung Neoplasms pathology, Ubiquitin Thiolesterase metabolism

Abstract

Bromodomain (BRD)-containing proteins are important for chromatin remodeling to regulate gene expression. In this study, we found that the deubiquitinase USP24 interacted with BRD through its C-terminus increased the levels of most BRD-containing proteins through increasing their protein stability by the removal of ubiquitin from Lys391/Lys400 of the BRD. In addition, we found that USP24 and BRG1 could regulate each other through regulating the protein stability and the transcriptional activity, respectively, of the other, suggesting that the levels of USP24 and BRG1 are regulated to form a positive feedback loop in cancer progression. Loss of the interaction motif of USP24 eliminated the ability of USP24 to stabilize BRD-containing proteins and abolished the effect of USP24 on cancer progression, including its inhibition of cancer cell proliferation and promotion of cancer cell migration, suggesting that the interaction between USP24 and the BRD is important for USP24-mediated effects on cancer progression. The targeting of BRD-containing proteins has been developed as a strategy for cancer therapy. Based on our study, targeting USP24 to inhibit the levels of BRD-containing proteins may inhibit cancer progression.

Published

2020

5. Nm23-H1-stabilized hnRNPA2/B1 promotes internal ribosomal entry site (IRES)-mediated translation of Sp1 in the lung cancer progression.

Author

Hung CY, Wang YC, Chuang JY, Young MJ, Liaw H, Chang WC, and Hung JJ

Subjects

5' Untranslated Regions, Aged, Animals, Cell Line, Tumor, Cell Proliferation, Disease Progression, Down-Regulation, Female, Gene Expression Regulation, Neoplastic, Gene Knockdown Techniques, Humans, Lung Neoplasms genetics, Lung Neoplasms metabolism, Male, Mice, Middle Aged, NM23 Nucleoside Diphosphate Kinases genetics, Neoplasm Staging, Neoplasm Transplantation, Prognosis, Protein Biosynthesis, Protein Stability, Sp1 Transcription Factor genetics, Survival Analysis, Heterogeneous-Nuclear Ribonucleoprotein Group A-B chemistry, Heterogeneous-Nuclear Ribonucleoprotein Group A-B metabolism, Internal Ribosome Entry Sites, Lung Neoplasms pathology, NM23 Nucleoside Diphosphate Kinases metabolism, Sp1 Transcription Factor metabolism

Abstract

Our recent studies have indicated that specificity protein-1 (Sp1) accumulates substantially in the early stage of lung cancer but is partially decreased in the late stages, which is an important factor in the progression of the cancer. In this study, we found that Nm23-H1 and hnRNPA2/B1 could be recruited to the 5'UTR of Sp1 mRNA. In investigating the clinical relevance of Nm23-H1/Sp1 levels, we found a positive correlation between lung cancer patients with poor prognosis and low levels of Sp1 and Nm23-H1, suggesting an association between Nm23-H1/Sp1 levels and survival rate. Knockdown of Nm23-H1 inhibits lung cancer growth but increases lung cancer cell malignancy, which could be rescued by overexpression of Sp1, indicating that Nm23-H1-induced Sp1 expression is critical for lung cancer progression. We also found that Nm23-H1 increases the protein stability of hnRNPA2/B1and is thereby co-recruited to the 5'UTR of Sp1 mRNA to regulate cap-independent translational activity. Since the Sp1 level is tightly regulated during lung cancer progression, understanding the molecular mechanisms underlying the regulation by Nm23-H1/hnRNPA2B1 of Sp1 expression in the various stages of lung cancer will be beneficial for lung cancer therapy in the future.

Published

2017

6. Chronic treatment with cisplatin induces chemoresistance through the TIP60-mediated Fanconi anemia and homologous recombination repair pathways.

Author

Su WP, Ho YC, Wu CK, Hsu SH, Shiu JL, Huang JC, Chang SB, Chiu WT, Hung JJ, Liu TL, Wu WS, Wu PY, Su WC, Chang JY, and Liaw H

Subjects

Acetylation, BRCA1 Protein genetics, Biomarkers, Cell Cycle drug effects, Cell Cycle genetics, Cell Line, Cisplatin pharmacology, DNA Breaks, Double-Stranded drug effects, Fanconi Anemia metabolism, Fanconi Anemia Complementation Group D2 Protein genetics, Gene Expression Regulation drug effects, Histones metabolism, Homologous Recombination, Humans, Lysine Acetyltransferase 5 metabolism, Promoter Regions, Genetic, Protein Binding, RNA Interference, RNA, Small Interfering genetics, Signal Transduction, Sister Chromatid Exchange, Transcription Initiation Site, Cisplatin therapeutic use, Drug Resistance genetics, Fanconi Anemia drug therapy, Fanconi Anemia genetics, Lysine Acetyltransferase 5 genetics, Recombinational DNA Repair

Abstract

The Fanconi anemia pathway in coordination with homologous recombination is essential to repair interstrand crosslinks (ICLs) caused by cisplatin. TIP60 belongs to the MYST family of acetyltransferases and is involved in DNA repair and regulation of gene transcription. Although the physical interaction between the TIP60 and FANCD2 proteins has been identified that is critical for ICL repair, it is still elusive whether TIP60 regulates the expression of FA and HR genes. In this study, we found that the chemoresistant nasopharyngeal carcinoma cells, derived from chronic treatment of cisplatin, show elevated expression of TIP60. Furthermore, TIP60 binds to the promoters of FANCD2 and BRCA1 by using the chromatin immunoprecipitation experiments and promote the expression of FANCD2 and BRCA1. Importantly, the depletion of TIP60 significantly reduces sister chromatid exchange, a measurement of HR efficiency. The similar results were also shown in the FNACD2-, and BRCA1-deficient cells. Additionally, these TIP60-deficient cells encounter more frequent stalled forks, as well as more DNA double-strand breaks resulting from the collapse of stalled forks. Taken together, our results suggest that TIP60 promotes the expression of FA and HR genes that are important for ICL repair and the chemoresistant phenotype under chronic treatment with cisplatin.

Published

2017