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1. Promoters of ASCL1‐ and NEUROD1‐dependent genes are specific targets of lurbinectedin in SCLC cells

Author

Federico Costanzo, Marta Martínez Diez, Gema Santamaría Nuñez, Juan Ignacio Díaz‐Hernandéz, Carlos Mario Genes Robles, Javier Díez Pérez, Emmanuel Compe, Romeo Ricci, Tsai‐Kun Li, Frédéric Coin, Juan Fernando Martínez Leal, Eva Maria Garrido‐Martin, and Jean Marc Egly

Subjects
ASCL1/NEUROD1, E‐boxes/CpG islands, lurbinectedin, transcription addiction, Medicine (General), R5-920, Genetics, QH426-470
Abstract

Abstract Small‐Cell Lung Cancer (SCLC) is an aggressive neuroendocrine malignancy with a poor prognosis. Here, we focus on the neuroendocrine SCLC subtypes, SCLC‐A and SCLC‐N, whose transcription addiction was driven by ASCL1 and NEUROD1 transcription factors which target E‐box motifs to activate up to 40% of total genes, the promoters of which are maintained in a steadily open chromatin environment according to ATAC and H3K27Ac signatures. This leverage is used by the marine agent lurbinectedin, which preferentially targets the CpG islands located downstream of the transcription start site, thus arresting elongating RNAPII and promoting its degradation. This abrogates the expression of ASCL1 and NEUROD1 and of their dependent genes, such as BCL2, INSM1, MYC, and AURKA, which are responsible for relevant SCLC tumorigenic properties such as inhibition of apoptosis and cell survival, as well as for a part of its neuroendocrine features. In summary, we show how the transcription addiction of these cells becomes their Achilles’s heel, and how this is effectively exploited by lurbinectedin as a novel SCLC therapeutic endeavor.

Published
2022
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2. Inflammatory interferon activates HIF-1α-mediated epithelial-to-mesenchymal transition via PI3K/AKT/mTOR pathway

Author

Yen-Hsiu Yeh, Ho-Fu Hsiao, Yen-Cheng Yeh, Tien-Wen Chen, and Tsai-Kun Li

Subjects
Tumor microenvironment, Inflammatory hypoxia, Interferon, HIF-1α, Epithelial-to-mesenchymal transition, Oncogenesis, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

Abstract Background Tumor microenvironments (TMEs) activate various axes/pathways, predominantly inflammatory and hypoxic responses, impact tumorigenesis, metastasis and therapeutic resistance significantly. Although molecular pathways of individual TME are extensively studied, evidence showing interaction and crosstalk between hypoxia and inflammation remain unclear. Thus, we examined whether interferon (IFN) could modulate both inflammatory and hypoxic responses under normoxia and its relation with cancer development. Methods IFN was used to induce inflammation response and HIF-1α expression in various cancer cell lines. Corresponding signaling pathways were then analyzed by a combination of pharmacological inhibitors, immunoblotting, GST-Raf pull-down assays, dominant-negative and short-hairpin RNA-mediated knockdown approaches. Specifically, roles of functional HIF-1α in the IFN-induced epithelial-mesenchymal transition (EMT) and other tumorigenic propensities were examined by knockdown, pharmacological inhibition, luciferase reporter, clonogenic, anchorage-independent growth, wound-healing, vasculogenic mimicry, invasion and sphere-formation assays as well as cellular morphology observation. Results We showed for the first time that IFN induced functional HIF-1α expression in a time- and dose- dependent manner in various cancer cell lines under both hypoxic and normoxic conditions, and then leading to an activated HIF-1α pathway in an IFN-mediated pro-inflammatory TME. IFN regulates anti-apoptosis activity, cellular metastasis, EMT and vasculogenic mimicry by a novel mechanism through mainly the activation of PI3K/AKT/mTOR axis. Subsequently, pharmacological and genetic modulations of HIF-1α, JAK, PI3K/AKT/mTOR or p38 pathways efficiently abrogate above IFN-induced tumorigenic propensities. Moreover, HIF-1α is required for the IFN-induced invasiveness, tumorigenesis and vasculogenic mimicry. Further supports for the HIF-1α-dependent tumorigenesis were obtained from results of xenograft mouse model and sphere-formation assay. Conclusions Our mechanistic study showed an induction of HIF-1α and EMT ability in an IFN-mediated inflammatory TME and thus demonstrating a novel interaction between inflammatory and hypoxic TMEs. Moreover, targeting HIF-1α may be a potential target for inhibiting tumor tumorigenesis and EMT by decreasing cancer cells wound healing and anchorage-independent colony growth. Our results also lead to rationale guidance for developing new therapeutic strategies to prevent relapse via targeting TME-providing IFN signaling and HIF-1α programming.

Published
2018
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4. Multiple Domains of the Tobacco mosaic virus p126 Protein Can Independently Suppress Local and Systemic RNA Silencing

Author

Li-Ya Wang, Shih-Shun Lin, Ting-Hsuan Hung, Tsai-Kun Li, Nai-Chun Lin, and Tang-Long Shen

Subjects
Microbiology, QR1-502, Botany, QK1-989
Abstract

Small RNA-mediated RNA silencing is a widespread antiviral mechanism in plants and other organisms. Many viruses encode suppressors of RNA silencing for counter-defense. The p126 protein encoded by Tobacco mosaic virus (TMV) has been reported to be a suppressor of RNA silencing but the mechanism of its function remains unclear. This protein is unique among the known plant viral silencing suppressors because of its large size and multiple domains. Here, we report that the methyltransferase, helicase, and nonconserved region II (NONII) of p126 each has silencing-suppressor function. The silencing-suppression activities of methyltransferase and helicase can be uncoupled from their enzyme activities. Specific amino acids in NONII previously shown to be crucial for viral accumulation and symptom development are also crucial for silencing suppression. These results suggest that some viral proteins have evolved to possess modular structural domains that can independently interfere with host silencing, and that this may be an effective mechanism of increasing the robustness of a virus.

Published
2012
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5. DNA topoisomerase II is involved in regulation of cyst wall protein genes and differentiation in Giardia lamblia.

Author

Bo-Chi Lin, Li-Hsin Su, Shih-Che Weng, Yu-Jiao Pan, Nei-Li Chan, Tsai-Kun Li, Hsin-Chih Wang, and Chin-Hung Sun

Subjects
Arctic medicine. Tropical medicine, RC955-962, Public aspects of medicine, RA1-1270
Abstract

The protozoan Giardia lamblia differentiates into infectious cysts within the human intestinal tract for disease transmission. Expression of the cyst wall protein (cwp) genes increases with similar kinetics during encystation. However, little is known how their gene regulation shares common mechanisms. DNA topoisomerases maintain normal topology of genomic DNA. They are necessary for cell proliferation and tissue development as they are involved in transcription, DNA replication, and chromosome condensation. A putative topoisomerase II (topo II) gene has been identified in the G. lamblia genome. We asked whether Topo II could regulate Giardia encystation. We found that Topo II was present in cell nuclei and its gene was up-regulated during encystation. Topo II has typical ATPase and DNA cleavage activity of type II topoisomerases. Mutation analysis revealed that the catalytic important Tyr residue and cleavage domain are important for Topo II function. We used etoposide-mediated topoisomerase immunoprecipitation assays to confirm the binding of Topo II to the cwp promoters in vivo. Interestingly, Topo II overexpression increased the levels of cwp gene expression and cyst formation. Microarray analysis identified up-regulation of cwp and specific vsp genes by Topo II. We also found that the type II topoisomerase inhibitor etoposide has growth inhibition effect on Giardia. Addition of etoposide significantly decreased the levels of cwp gene expression and cyst formation. Our results suggest that Topo II has been functionally conserved during evolution and that Topo II plays important roles in induction of the cwp genes, which is key to Giardia differentiation into cysts.

Published
2013
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12. Data from Mitoxantrone Inhibits HIF-1α Expression in a Topoisomerase II–Independent Pathway

Author

Tsai-Kun Li and Yng-Miin Toh

Abstract

Purpose: Solid tumors encounter a growth-limiting hypoxic microenvironment as they develop. Hypoxia-inducible factors (HIF) play important roles in hypoxia-associated tumor development and therapeutic resistance. Targeting the HIF pathway (especially HIF-1α) represents a promising cancer treatment strategy. Here, we report a novel class of HIF-1α inhibitors and the possible molecular basis of inhibition.Experimental Design: We analyzed the inhibitory effects of clinically used topoisomerase II (TOP2)–targeting drugs on HIF-1α expression with a primary focus on mitoxantrone. The potential role of TOP2 in mitoxantrone-inhibited HIF-1α expression was studied using pharmacologic inhibition, a knockdown approach, and TOP2 mutant cells. Moreover, involvement of mitoxantrone in proteasome-mediated degradation, transcription, and translation of HIF-1α was examined.Results: The TOP2-targeting mitoxantrone, but neither doxorubicin nor etoposide (VP-16), strongly inhibited HIF-1α expression under hypoxic conditions in a dose- and time-dependent manner. Surprisingly, the mitoxantrone-mediated inhibition of HIF-1α expression was largely independent of two TOP2 isozymes, proteasomal degradation, and transcription. Furthermore, mitoxantrone inhibited HIF-1α expression and function in a similar fashion as cycloheximide, suggesting that mitoxantrone might inhibit HIF-1α via a blockage at its translation step. In vitro translation experiments using HIF-1α mRNA further confirmed inhibition of HIF-1α translation by mitoxantrone. Interestingly, levels of the polysome-bound HIF-1α and VEGF-A mRNA were elevated and decreased after mitoxantrone treatment, respectively.Conclusions: We have identified the TOP2-targeting compound, mitoxantrone, as an HIF-1α inhibitor possibly through a translation inhibition mechanism, suggesting the possibility of an additional anticancer activity for mitoxantrone. Clin Cancer Res; 17(15); 5026–37. ©2011 AACR.

Published
2023

16. Data from DNA Topoisomerase III Alpha Regulates p53-Mediated Tumor Suppression

Author

Tsai-Kun Li, Yen-Hsiu Yeh, Shu-Chun Teng, Tang-Long Shen, Hsiang-Chin Chen, Han-Wen Chang, Jia-Rong Fan, and Mei-Yi Hsieh

Abstract

Purpose: Human DNA topoisomerase III alpha (hTOP3α) is involved in DNA repair surveillance and cell-cycle checkpoints possibly through formatting complex with tumor suppressors. However, its role in cancer development remained unsolved.Experimental Design: Coimmunoprecipitation, sucrose gradient, chromatin immunoprecipitation (ChIP), real time PCR, and immunoblotting analyses were performed to determine interactions of hTOP3α with p53. Paired cell lines with different hTOP3α levels were generated via ectopic expression and short hairpin RNA (shRNA)-mediated knockdown approaches. Cellular tumorigenic properties were analyzed using cell counting, colony formation, senescence, soft agar assays, and mouse xenograft models.Results: The hTOP3α isozyme binds to p53 and cofractionizes with p53 in gradients differing from fractions containing hTOP3α and BLM. Knockdown of hTOP3α expression (sh-hTOP3α) caused a higher anchorage-independent growth of nontumorigenic RHEK-1 cells. Similarly, sh-hTOP3α and ectopic expression of hTOP3α in cancer cell lines caused increased and reduced tumorigenic abilities, respectively. Genetic and mutation experiments revealed that functional hTOP3α, p53, and p21 are required for this tumor-suppressive activity. Mechanism-wise, ChIP data revealed that hTOP3α binds to the p53 and p21 promoters and positively regulates their expression. Two proteins affect promoter recruitments of each other and collaborate in p21 expression. Moreover, sh-hTOP3α and sh-p53 in AGS cells caused a similar reduction in senescence and hTOP3α mRNA levels were lower in gastric and renal tumor samples.Conclusion: We concluded that hTOP3α interacts with p53, regulates p53 and p21 expression, and contributes to the p53-mediated tumor suppression. Clin Cancer Res; 20(6); 1489–501. ©2014 AACR.

Published
2023

20. Activation of multiple proteolysis systems contributes to acute cadmium cytotoxicity

Author

Yen-Hsiu Yeh, Chia-Chih Tsai, Tien-Wen Chen, Chieh-Hua Lee, Wei-Jer Chang, Mei-Yi Hsieh, and Tsai-Kun Li

Subjects
A549 Cells, Cytotoxins, Proteolysis, Clinical Biochemistry, Humans, Cell Biology, General Medicine, Reactive Oxygen Species, Molecular Biology, DNA Topoisomerases, Cadmium, HeLa Cells
Abstract

Cadmium exhibits both toxic and carcinogenic effects, and its cytotoxicity is linked to various cellular pathways, such as oxidative stress, ubiquitin-proteasome, and p53-mediated response pathways. The molecular mechanism(s) underlying cadmium cytotoxicity appears to be complex, but remains largely unclear. Here, we examined the effects of cadmium on the protein catabolism using two surrogate markers, DNA topoisomerases I and II alpha and its contribution to cytotoxicity. We have found that cadmium exposure induced time- and concentration-dependent decreases in the protein level of surrogate markers and therefore suggest that cadmium may be involved in proteolysis system activation. A pharmacological study further revealed the novel role(s) of these proteolytic activities and reactive oxygen species (ROS) in the cadmium-induced acute toxicity: (i) Proteasome inhibition only partially relieved the cadmium-induced proteolysis of topoisomerases; (ii) Moreover, we report for the first time that the activation of metalloproteases, serine proteases, and cysteine proteases contributes to the acute cadmium cytotoxicity; (iii) Consistent with the notion that both ROS generation and proteolysis system activation contribute to the cadmium-induced proteolysis and cytotoxicity, the scavenger N-acetylcysteine and aforementioned protease inhibition not only reduced the cadmium-induced topoisomerase degradation but also alleviated the cadmium-induced cell killing. Taken together, acute cadmium exposure may activate multiple proteolytic systems and ROS formation, subsequently leading to intracellular damage and cytotoxicity. Thus, our results provide a novel insight into potential action mechanism(s) by which cadmium exerts its cytotoxic effect and suggest potential strategies to prevent cadmium-associated acute toxicity.

Published
2022

21. The role of extracellular vesicles in prostate cancer with clinical applications

Author

Chun-Jung Lin, Tang-Long Shen, Jer Tsong Hsieh, Yu Ling Tai, Benjamin P C Chen, and Tsai-Kun Li

Subjects
Male, 0301 basic medicine, Cancer Research, Stromal cell, Endosome, Endocrinology, Diabetes and Metabolism, Biology, Extracellular Vesicles, 03 medical and health sciences, Prostate cancer, Paracrine signalling, 0302 clinical medicine, Endocrinology, Biomarkers, Tumor, medicine, Humans, Tumor microenvironment, Prostatic Neoplasms, Prognosis, medicine.disease, Precision medicine, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, Intracellular
Abstract

In mammalian cells, extracellular vesicles (EVs) derived from the endosomal system carry many different kinds of bioactive molecule to deliver to recipient cells in a paracrine or endocrine manner. EVs can mediate local and systemic intercellular communications, including reeducating stromal cells, remodeling the architecture of the tumor microenvironment, modulating cancer metabolism and metastases, or even conferring drug resistance. Because the molecular and functional characteristics of prostate cancer (PCa) evolve over time, the bioactive molecule profiles/signatures of tumor-derived EVs (TDEs) reflect the real-time status of cancer cells. TDEs appear to be valuable diagnostic and prognostic biomarkers as well as potential therapeutic vehicles, suggesting their essential role in precision medicine of disease management. We summarized critical aspects of TDEs in PCa and discussed their potential clinical applications.

Published
2020

22. The paracrine induction of prostate cancer progression by caveolin-1

Author

Ping Mu, Andrew Dang, Debabrata Saha, Jer Tsong Hsieh, Yu-An Chen, Chih Ho Lai, Tang-Long Shen, U-Ging Lo, Yu-Ling Tai, Ho Lin, Eun-Jin Yun, Elizabeth Hernandez, Su Deng, Tsai-Kun Li, and Chun-Jung Lin

Subjects
Male, Cancer Research, Immunology, Population, Caveolin 1, Mice, SCID, Biology, Exosomes, Neuroendocrine differentiation, Article, Metastasis, Cellular and Molecular Neuroscience, Prostate cancer, Mice, Cancer stem cell, Cell Line, Tumor, Paracrine Communication, medicine, Animals, Humans, lcsh:QH573-671, education, education.field_of_study, Cancer stem cells, lcsh:Cytology, Cancer, Cell Biology, medicine.disease, Neoplasm Proteins, Prostatic Neoplasms, Castration-Resistant, Cancer cell, Cancer research, Stem cell, Signal Transduction
Abstract

A subpopulation of cancer stem cells (CSCs) plays a critical role of cancer progression, recurrence, and therapeutic resistance. Many studies have indicated that castration-resistant prostate cancer (CRPC) is associated with stem cell phenotypes, which could further promote neuroendocrine transdifferentiation. Although only a small subset of genetically pre-programmed cells in each organ has stem cell capability, CSCs appear to be inducible among a heterogeneous cancer cell population. However, the inductive mechanism(s) leading to the emergence of these CSCs are not fully understood in CRPC. Tumor cells actively produce, release, and utilize exosomes to promote cancer development and metastasis, cancer immune evasion as well as chemotherapeutic resistance; the impact of tumor-derived exosomes (TDE) and its cargo on prostate cancer (PCa) development is still unclear. In this study, we demonstrate that the presence of Cav-1 in TDE acts as a potent driver to induce CSC phenotypes and epithelial–mesenchymal transition in PCa undergoing neuroendocrine differentiation through NFκB signaling pathway. Furthermore, Cav-1 in mCRPC-derived exosomes is capable of inducing radio- and chemo-resistance in recipient cells. Collectively, these data support Cav-1 as a critical driver for mCRPC progression.

Published
2019

23. Selected ellipticine derivatives, known to target topoisomerase II, suppress the alternative lengthening of telomere (ALT) pathway in telomerase-negative cells

Author

Sevil, Zencir, Meng-Hsun, Hsieh, Joel-Sean, Hsu, Yavuz, Ergun, Guan-Ling, Chou, Tsai-Kun, Li, Shu-Chun, Teng, and Zeki, Topcu

Subjects
Fluorescent Antibody Technique, Humans, Telomere Homeostasis, Topoisomerase II Inhibitors, Antineoplastic Agents, Ellipticines, Telomerase, In Situ Hybridization, Fluorescence, Cell Line
Abstract

DNA topoisomerase and telomerase enzymes are popular targets of several anti-tumor drugs. Smooth proceeding of telomeric recombination requires Topoisomerase II (Top2), which is involved in telomere-telomere recombination through functioning in relaxation of positive supercoils among the cells adopting telomerase-independent Alternative lengthening of telomere (ALT) pathway. Most of the inhibitors reported so far have been designed to targetsolely telomerase-positive cells, which can potentially lead to therapeutic failure because tumor cells treated with telomerase inhibitors can activate the ALT pathway for telomere maintenance. Knowing that ALT cells are more sensitive against a Top2 inhibitor, ICRF-93 agent, compared to telomerase-positive cells, we analyzed two selected ellipticine derivatives that we recently reported as TopII-targeting compounds, to assess their effects on the formation of DNA breaks and suppression of ALT pathway.Cell viability, Comet, C-Circle assays, dot blot, immunofluorescence staining, and telomere fluorescence in situ hybridization (FISH) staining were used for determining the effect of the compounds on ALT status of tumor cells.Treatment of ALT cells with ellipticine derivatives resulted in the formation of DNA breaks and suppression of ALT-associated phenotypes in vitro. Our results will contribute to the development of therapeutic strategies combining telomerase and ALT pathway inhibitors.

Published
2020

24. Selected Ellipticine Derivatives, Known To Target Topoisomerase Ii, Suppress The Alternative Lengthening Of Telomere (Alt) Pathway In Telomerase-Negative Cells

Author

Joel-Sean Hsu, Yavuz Ergun, Sevil Zencir, Zeki Topcu, Guan-Ling Chou, Meng-Hsun Hsieh, Shu-Chun Teng, Tsai-Kun Li, and Ege Üniversitesi

Subjects
0301 basic medicine, Cancer Research, Telomerase, MTS assay, telomerase inhibitor, Fluorescent Antibody Technique, 0302 clinical medicine, ellipticine derivative, telomere length, Topoisomerase II Inhibitors, genetics, ALT cell line, Ellipticines, telomere homeostasis, antineoplastic agent, In Situ Hybridization, Fluorescence, gyrase inhibitor, chemistry.chemical_classification, Ellipticine derivatives, DNA strand breakage, SaOS-2 cell line, biology, medicine.diagnostic_test, drug effect, General Medicine, Alternative lengthening of telomere, unclassified drug, female, Oncology, priority journal, 030220 oncology & carcinogenesis, DNA supercoil, cytotoxicity, DNA topoisomerase II, phenotype, Antineoplastic Agents, telomerase, chemistry, Article, Cell Line, 03 medical and health sciences, comet assay, medicine, Humans, controlled study, Viability assay, human, DNA topoisomerase (ATP hydrolysing), drug selectivity, immunofluorescence, fluorescence in situ hybridization, cell viability, Topoisomerase, human cell, icrf 93, Anti-cancer therapeutics, In vitro, Telomere, 030104 developmental biology, Enzyme, Cancer research, biology.protein, ellipticine, Fluorescence in situ hybridization
Abstract

Background DNA topoisomerase and telomerase enzymes are popular targets of several anti-tumor drugs. Smooth proceeding of telomeric recombination requires Topoisomerase II (Top2), which is involved in telomere-telomere recombination through functioning in relaxation of positive supercoils among the cells adopting telomerase-independent Alternative lengthening of telomere (ALT) pathway. Most of the inhibitors reported so far have been designed to targetsolely telomerase-positive cells, which can potentially lead to therapeutic failure because tumor cells treated with telomerase inhibitors can activate the ALT pathway for telomere maintenance. Knowing that ALT cells are more sensitive against a Top2 inhibitor, ICRF-93 agent, compared to telomerase-positive cells, we analyzed two selected ellipticine derivatives that we recently reported as TopII-targeting compounds, to assess their effects on the formation of DNA breaks and suppression of ALT pathway. Methods Cell viability, Comet, C-Circle assays, dot blot, immunofluorescence staining, and telomere fluorescence in situ hybridization (FISH) staining were used for determining the effect of the compounds on ALT status of tumor cells. Results and conclusions Treatment of ALT cells with ellipticine derivatives resulted in the formation of DNA breaks and suppression of ALT-associated phenotypes in vitro. Our results will contribute to the development of therapeutic strategies combining telomerase and ALT pathway inhibitors., Turkish Scientific and Technical Research AssemblyTurkiye Bilimsel ve Teknolojik Arastirma Kurumu (TUBITAK) [115Z349], This research was supported by Grant 115Z349 (Z.T. and S.Z.) from the Turkish Scientific and Technical Research Assembly. the cell lines used in this study were provided by Drs. Shu-Chun Teng and Tsai-Kun Li (College of Medicine, National Taiwan University, Taipei, Taiwan).

Published
2020

25. Drug targeting of HIV-1 RNA.DNA hybrid structures: Thermodynamics of recognition and impact on reverse transcriptase-mediated ribonuclease H activity and viral replication

Author

Tsai-Kun Li, Barbieri, Christopher M., Hsin-Chin Lin, Rabson, Arnold B., Gengcheng Yang, Yupeng Fan, Gaffney, Barbara L., Pilch, Daniel S., and Jones, Roger A.

Subjects
Ribonuclease -- Structure, Reverse transcriptase -- Research, Thermodynamics -- Analysis, Biological sciences, Chemistry
Abstract

An approach for inhibiting the ribonuclease H (RNase H) activity of human immunodeficiency virus type I (HIV-I) reverse transcriptase (RT) is demonstrated by targeting RNase H RNA.DNA hybrid substrates. In this approach the binding of the 4,5-disubstituted 2-deoxystreptamine aminoglycosides, neomycin, paromomycin and ribostamycin, to two different chimeric RNA-DNA duplexes inhibits specific RT-mediated RNase cleavage in competitive manner.

Published
2004

27. Design, synthesis, and biological evaluation of heterotetracyclic quinolinone derivatives as anticancer agents targeting topoisomerases

Author

Tsung Chih Chen, Ting Yu Chang, Yi Song Chen, Mei Hsiang Lin, Jiann Fong Lee, Tsai-Kun Li, Yen Hsiu Yeh, Hao Syun Chou, Sung Bau Lee, Nian Zhe Lee, and Zheng Fang Liu

Subjects
Pharmacology, 0303 health sciences, biology, 010405 organic chemistry, Chemistry, DNA damage, Topoisomerase, Organic Chemistry, Cell, General Medicine, Cleavage (embryo), 01 natural sciences, Molecular biology, 0104 chemical sciences, 03 medical and health sciences, chemistry.chemical_compound, medicine.anatomical_structure, Apoptosis, Drug Discovery, Cancer cell, medicine, biology.protein, Gene, DNA, 030304 developmental biology
Abstract

A series of thiochromeno [2,3-c]quinolin-12-one derivatives with various substitutions were synthesized and evaluated as topoisomerase (Topo) inhibitors. Six (8, 10, 12, 14, 19, and 26) of 23 compounds showed strong inhibitory activities against Topo-mediated DNA relaxation and proliferation of five human cell lines including breast (MDA-MB-231, MDA-MB-468 and MCF7), colorectal (HCT116) and non-small cell lung (H1299) cancers. Among these, compounds 14 and 26 exhibited full inhibitory activities against Topo I at 3 μM and Topo IIα at 1 μM. Cancer cells treated with 26 accumulated DNA damage and were arrested at the G2/M phase. With time, cells proceeded to apoptosis, as revealed by increased amounts of cells with fragmented DNA and cleavage of caspase-8 and -9. In contrast, normal breast epithelial cells showed low sensitivity to 26. Taken together, our study identifies 26 as a potent Topo dual-inhibitor with low toxicity to normal cells, and elucidates that the terminal amino group of N-2-aminoethylamino or N-3-aminopropylamino at the 6th position and 8,10-di-halogen substituents on thiochromeno [2,3-c]quinolin-12-one are critical for the Topo-inhibiting and cancer-killing activities.

Published
2019

28. Retraction notice to 'Design, synthesis, and biological evaluation of heterotetracyclic quinolinone derivatives as anticancer agents targeting topoisomerases' [Eur. J. Med. Chem. 190 (2020) 112074]

Author

Ting Yu Chang, Hao Syun Chou, Sung Bau Lee, Yen Hsiu Yeh, Tsai-Kun Li, Tsung Chih Chen, Nian Zhe Lee, Yi Song Chen, Jiann Fong Lee, Zheng Fang Liu, and Mei Hsiang Lin

Subjects
Pharmacology, biology, Design synthesis, Notice, Chemistry, Topoisomerase, Organic Chemistry, Drug Discovery, biology.protein, General Medicine, Combinatorial chemistry, Biological evaluation
Abstract

This article has been retracted: please see Elsevier Policy on Article Withdrawal (https://www.elsevier.com/about/our-business/policies/article-withdrawal). This article has been retracted at the request of the authors. The authors regret to inform that they would like to withdraw this accepted article, due to serious errors in authorship, affiliations, material sources and supporting grant names/numbers. The authors sincerely apologize for these oversights and miscommunications the study caused.

Published
2020

29. Regioselective synthesis and biological evaluation of N-substituted 2-aminoquinazolin-4-ones

Author

Wen Hsiung Yeh, Pen Yuan Liao, Ming Hsuan Lu, Ming Chih Hsu, Chia Chi Lin, Tsai-Kun Li, Yi Hung Chen, Ying Cheng Chen, Yu Ting Liu, Tun Cheng Chien, Tsung Han Hsieh, Zhen Yuan Liao, and Yi Song Chen

Subjects
Aqueous solution, Molecular Structure, 010405 organic chemistry, Chemistry, Organic Chemistry, Regioselectivity, Antineoplastic Agents, 010402 general chemistry, 01 natural sciences, Biochemistry, Dimroth rearrangement, Medicinal chemistry, 0104 chemical sciences, chemistry.chemical_compound, Sodium hydroxide, Cyclization, Cell Line, Tumor, Nitriles, Structural isomer, Humans, ortho-Aminobenzoates, Physical and Theoretical Chemistry, Biological evaluation, Quinazolinones
Abstract

The reaction of methyl anthranilates with N-arylcyanamides in the presence of p-TsOH in t-BuOH under reflux afforded predominantly 3-arylquinazolin-4-ones. In contrast, the reaction of the same reactants with TMSCl in t-BuOH at 60 °C followed by the Dimroth rearrangement in aqueous ethanolic sodium hydroxide gave exclusively the regioisomers, 2-(N-arylamino)quinazolin-4-ones. The regioselective synthesis of N-aryl-substituted 2-aminoquinazolin-4-ones can be further applied to the synthesis of benzimidazo[2,1-b]quinazolin-12-ones.

Published
2018

30. Inflammatory interferon activates HIF-1α-mediated epithelial-to-mesenchymal transition via PI3K/AKT/mTOR pathway

Author

Tsai-Kun Li, Ho-Fu Hsiao, Yen-Cheng Yeh, Yen-Hsiu Yeh, and Tien-Wen Chen

Subjects
0301 basic medicine, Cancer Research, Epithelial-Mesenchymal Transition, MAP Kinase Signaling System, HIF-1α, Apoptosis, medicine.disease_cause, lcsh:RC254-282, Models, Biological, 03 medical and health sciences, Phosphatidylinositol 3-Kinases, Neoplasms, medicine, Tumor Microenvironment, Humans, Vasculogenic mimicry, Epithelial–mesenchymal transition, Hypoxia, Protein kinase B, Protein Kinase Inhibitors, PI3K/AKT/mTOR pathway, Oncogenesis, Janus Kinases, Tumor microenvironment, Chemistry, Research, TOR Serine-Threonine Kinases, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Hypoxia-Inducible Factor 1, alpha Subunit, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Oncology, Epithelial-to-mesenchymal transition, Inflammatory hypoxia, Cancer cell, Cancer research, ras Proteins, Interferon, Interferons, Signal transduction, Carcinogenesis, Proto-Oncogene Proteins c-akt, Biomarkers, Signal Transduction
Abstract

Background Tumor microenvironments (TMEs) activate various axes/pathways, predominantly inflammatory and hypoxic responses, impact tumorigenesis, metastasis and therapeutic resistance significantly. Although molecular pathways of individual TME are extensively studied, evidence showing interaction and crosstalk between hypoxia and inflammation remain unclear. Thus, we examined whether interferon (IFN) could modulate both inflammatory and hypoxic responses under normoxia and its relation with cancer development. Methods IFN was used to induce inflammation response and HIF-1α expression in various cancer cell lines. Corresponding signaling pathways were then analyzed by a combination of pharmacological inhibitors, immunoblotting, GST-Raf pull-down assays, dominant-negative and short-hairpin RNA-mediated knockdown approaches. Specifically, roles of functional HIF-1α in the IFN-induced epithelial-mesenchymal transition (EMT) and other tumorigenic propensities were examined by knockdown, pharmacological inhibition, luciferase reporter, clonogenic, anchorage-independent growth, wound-healing, vasculogenic mimicry, invasion and sphere-formation assays as well as cellular morphology observation. Results We showed for the first time that IFN induced functional HIF-1α expression in a time- and dose- dependent manner in various cancer cell lines under both hypoxic and normoxic conditions, and then leading to an activated HIF-1α pathway in an IFN-mediated pro-inflammatory TME. IFN regulates anti-apoptosis activity, cellular metastasis, EMT and vasculogenic mimicry by a novel mechanism through mainly the activation of PI3K/AKT/mTOR axis. Subsequently, pharmacological and genetic modulations of HIF-1α, JAK, PI3K/AKT/mTOR or p38 pathways efficiently abrogate above IFN-induced tumorigenic propensities. Moreover, HIF-1α is required for the IFN-induced invasiveness, tumorigenesis and vasculogenic mimicry. Further supports for the HIF-1α-dependent tumorigenesis were obtained from results of xenograft mouse model and sphere-formation assay. Conclusions Our mechanistic study showed an induction of HIF-1α and EMT ability in an IFN-mediated inflammatory TME and thus demonstrating a novel interaction between inflammatory and hypoxic TMEs. Moreover, targeting HIF-1α may be a potential target for inhibiting tumor tumorigenesis and EMT by decreasing cancer cells wound healing and anchorage-independent colony growth. Our results also lead to rationale guidance for developing new therapeutic strategies to prevent relapse via targeting TME-providing IFN signaling and HIF-1α programming. Electronic supplementary material The online version of this article (10.1186/s13046-018-0730-6) contains supplementary material, which is available to authorized users.

Published
2018

31. Additional file 5: of Inflammatory interferon activates HIF-1α-mediated epithelial-to-mesenchymal transition via PI3K/AKT/mTOR pathway

Author

Yen-Hsiu Yeh, Ho-Fu Hsiao, Yen-Cheng Yeh, Tien-Wen Chen, and Tsai-Kun Li

Abstract

Figure S5. The IFN-α not only attenuated MX-induced apoptosis, but also promote PI3K- and MAPK-P38-dependent invasion activity.(A) IFN-α co-treatment reduced the MX-induced apoptotic cleavage of PARP1.(B) LY294002 (LY) and SB203580 (SB) could both effectively inhibit the IFN-α-induced invasion abilities. (PPT 237 kb)

Published
2018
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32. Additional file 3: of Inflammatory interferon activates HIF-1α-mediated epithelial-to-mesenchymal transition via PI3K/AKT/mTOR pathway

Author

Yen-Hsiu Yeh, Ho-Fu Hsiao, Yen-Cheng Yeh, Tien-Wen Chen, and Tsai-Kun Li

Abstract

Figure S3. The JAK/PI-3 K, AKT/GSK3β and p38/ERK/JNK axes contributed to the IFN-α-induced HIF-1α expression. (A) Knockdown of STAT1 (si-STAT1) expression has no effect on the IFN-α-induced HIF-1α expression. (B) Ectopic expression of PTEN antagonized the IFN-α-activated AKT/GSK3β pathway. (C-D) β-catenin inhibition by FH535 treatment not only decreased the IFN-α-induced expression of HIF-1α (C), but also reduced the IFN-α-induced active β-catenin (D). (PPT 221 kb)

Published
2018
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33. Additional file 1: of Inflammatory interferon activates HIF-1α-mediated epithelial-to-mesenchymal transition via PI3K/AKT/mTOR pathway

Author

Yen-Hsiu Yeh, Ho-Fu Hsiao, Yen-Cheng Yeh, Tien-Wen Chen, and Tsai-Kun Li

Abstract

Figure S1. IFN-α-induced HIF-1α expression in transcription- and translation-dependent, but 26S proteasome-independent. (A) RNA transcription is required for IFN-α mediated HIF-1α induction. 769-P cells were pre-treated 30 min. With or without 100 μM DRB and subsequently exposed for 24 h with either IFN-α (1000 units/ml) or desferoxamine (DFX, 260 μM), and protein labels determined by immunoblotting analysis with indicated antibodies. (B-C) Interferon-α treatment promotes the de novo synthesis of HIF-1α expression (B) and does not impact on the stability of HIF-1α. (C) Cells were treated with IFN-α before addition of (DRB, 100 μM), cycloheximide (CHX, 100 μM) or MG-132 (10 μM) (D) IFN-α stimulated HIF-1α expression similarly in the VHL-deficient 769-P cells with or without ectopic expression of functional VHL. (PPT 251 kb)

Published
2018
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34. Additional file 4: of Inflammatory interferon activates HIF-1α-mediated epithelial-to-mesenchymal transition via PI3K/AKT/mTOR pathway

Author

Yen-Hsiu Yeh, Ho-Fu Hsiao, Yen-Cheng Yeh, Tien-Wen Chen, and Tsai-Kun Li

Subjects
enzymes and coenzymes (carbohydrates)
Abstract

Figure S4. NF-κB is minimally involved in the IFN-α mediated HIF-1α accumulation. (A) IFN-α slightly activated IKK as suggested by a minimal increase in IkBaS32 phosphorylation. (B-D) Targeting IKK/IkBα/NF-κB pathway by Sulfasalazine (Sulfa, B), IkBα-M mutant (C) and si-p65 (D) do not alter much of IFN-α-induced HIF-1α expression. (PPT 201 kb)

Published
2018
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35. Additional file 2: of Inflammatory interferon activates HIF-1α-mediated epithelial-to-mesenchymal transition via PI3K/AKT/mTOR pathway

Author

Yen-Hsiu Yeh, Ho-Fu Hsiao, Yen-Cheng Yeh, Tien-Wen Chen, and Tsai-Kun Li

Abstract

Figure S2. IFN-α could up-regulate HIF-1α expression in the presence of 1% O2 with a different induction kinetics. Cells were treated with or without IFN-α, exposed to hypoxia (1% O2) and then harvested at indicated time points (3, 6, 9 and 12 h) for immunoblotting. (PPT 162 kb)

Published
2018
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36. Additional file 6: of Inflammatory interferon activates HIF-1α-mediated epithelial-to-mesenchymal transition via PI3K/AKT/mTOR pathway

Author

Yen-Hsiu Yeh, Ho-Fu Hsiao, Yen-Cheng Yeh, Tien-Wen Chen, and Tsai-Kun Li

Abstract

Figure S6. Direct effects of IFN-α on the expression of EMT and stemness biomarkers. (A-B) Cells were treated with 0.5, 1, 2.5 and 5 mg of anti-IFN-α antibodies and their impacts on the expression of EMT marker vimentin (A) and stemness marker Bmi1 genes (B) were determined by immunoblotting analysis. (PPT 133 kb)

Published
2018
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37. Involvement of p38 MAPK in the Anticancer Activity of Cultivated Cordyceps militaris

Author

Wan-Jung Lai, Tang-Long Shen, Yen-Hsun Chen, Richard Chu, Shang-Min Chou, Tsai-Kun Li, Cheng-Hsiang Kao, Sheng-Hong Tsai, and Tzu-Wen Hong

Subjects
Programmed cell death, Poly ADP ribose polymerase, Gene Expression, HL-60 Cells, p38 Mitogen-Activated Protein Kinases, Histones, Cordyceps militaris, medicine, Humans, Cytotoxic T cell, Protein kinase B, Leukemia, biology, General Medicine, biology.organism_classification, medicine.disease, Antineoplastic Agents, Phytogenic, Up-Regulation, Cell biology, Complementary and alternative medicine, Apoptosis, Cordyceps, Cancer cell, Cancer research, Drug Screening Assays, Antitumor, DNA Damage, Drugs, Chinese Herbal, Signal Transduction
Abstract

Cordyceps militaris is a traditional Chinese medicine frequently used for tonic and therapeutic purposes. Reports from our laboratory and others have demonstrated that extracts of the cultivated fruiting bodies of C. militaris (CM) exhibit a potent cytotoxic effect against many cancer cell lines, especially human leukemia cells. Here, we further investigated the underlying mechanism through which CM is cytotoxic to cancer cells. The CM-mediated induction of PARP cleavage and its related DNA damage signal (γH2AX) was diminished by caspase inhibitor I. In contrast, a ROS scavenger failed to prevent CM-mediated leukemia cell death. Moreover, two signaling molecules, AKT and p38 MAPK, were activated during the course of apoptosis induction. Employing MTT analysis, we found that a p38 MAPK inhibitor but not an AKT inhibitor could rescue cells from CM-mediated cell death, as well as inhibit the cleavage of PARP, formation of apoptotic bodies and up-regulation of the γH2AX signal. These results suggest that CM-mediated leukemia cell death occurs through the activation of the p38 MAPK pathway, indicating its potential therapeutic effects against human leukemia.

Published
2015

38. Producing irreversible topoisomerase II-mediated DNA breaks by site-specific Pt(II)-methionine coordination chemistry

Author

Tsai-Kun Li, Shin Fu Chen, Ying Ren Wang, Yi Song Chen, Chyuan Chuan Wu, Yi Wen Liao, Tun Cheng Chien, Nei-Li Chan, Te-Sheng Lin, and Ko Ting Liu

Subjects
0301 basic medicine, Organoplatinum Compounds, Stereochemistry, Protein Conformation, Antineoplastic Agents, HL-60 Cells, Biology, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Protein structure, Methionine, Structural Biology, Antigens, Neoplasm, Cell Line, Tumor, medicine, Genetics, Moiety, Humans, Topoisomerase II Inhibitors, Poly-ADP-Ribose Binding Proteins, Etoposide, Podophyllotoxin, chemistry.chemical_classification, Topoisomerase, DNA Breaks, DNA, DNA-Binding Proteins, 030104 developmental biology, Enzyme, DNA Topoisomerases, Type II, Biochemistry, chemistry, 030220 oncology & carcinogenesis, biology.protein, Corrigendum, medicine.drug
Abstract

Human type II topoisomerase (Top2) isoforms, hTop2α and hTop2β, are targeted by some of the most successful anticancer drugs. These drugs induce Top2-mediated DNA cleavage to trigger cell-death pathways. The potency of these drugs correlates positively with their efficacy in stabilizing the enzyme-mediated DNA breaks. Structural analysis of hTop2α and hTop2β revealed the presence of methionine residues in the drug-binding pocket, we therefore tested whether a tighter Top2-drug association may be accomplished by introducing a methionine-reactive Pt2+ into a drug to further stabilize the DNA break. Herein, we synthesized an organoplatinum compound, etoplatin-N2β, by replacing the methionine-juxtaposing group of the drug etoposide with a cis-dichlorodiammineplatinum(II) moiety. Compared to etoposide, etoplatin-N2β more potently inhibits both human Top2s. While the DNA breaks arrested by etoposide can be rejoined, those captured by etoplatin-N2β are practically irreversible. Crystallographic analyses of hTop2β complexed with DNA and etoplatin-N2β demonstrate coordinate bond formation between Pt2+ and a flanking methionine. Notably, this stable coordinate tether can be loosened by disrupting the structural integrity of drug-binding pocket, suggesting that Pt2+ coordination chemistry may allow for the development of potent inhibitors with protein conformation-dependent reversibility. This approach may be exploited to achieve isoform-specific targeting of human Top2s.

Published
2017

39. Synergistic property of cordycepin in cultivated Cordyceps militaris-mediated apoptosis in human leukemia cells

Author

Shang-Min Chou, Tzu-Wen Hong, Wan-Jung Lai, Jui-Ya Lai, Sz Hsien Yu, Tang-Long Shen, Tsai-Kun Li, Richard Chu, Cheng-Hsiang Kao, Sheng-Hong Tsai, Shih-Torng Ding, and Yen-Hsun Chen

Subjects
Pharmaceutical Science, Antineoplastic Agents, Apoptosis, HL-60 Cells, DNA laddering, chemistry.chemical_compound, Drug Discovery, Cordyceps militaris, Humans, Cytotoxic T cell, Cell Proliferation, Pharmacology, Cordyceps, Deoxyadenosines, biology, Cordycepin, biology.organism_classification, Apoptotic body, Molecular biology, Complementary and alternative medicine, Biochemistry, chemistry, Cancer cell, Molecular Medicine
Abstract

Cordyceps militaris is a well-known Chinese traditional medicinal mushroom frequently used for tonics and recently of a potential interest for cancer intervention. Here, we explored the cancer cell killing activity of the hot water extracts of C. militaris cultured mycelia (CM(MY)) and cultivated fruiting bodies (CM(FB)). We found that CM(FB) exhibited a greater cytotoxic effect against various cancer cells over CM(MY). Apoptotic phenotypes including apoptotic body formation, DNA laddering, caspase 3 activation and cleavage of PARP proteins were induced by CM(FB) treatment but only slightly induced by same concentration of CM(MY) treatment in human HL-60 leukemia cells. Cordycepin in CM(FB) (10.47 mg/g) is significantly higher (∼ 15.2 times) than that of CM(MY) (0.69 mg/g). Using isobolographic analysis, the synergy of cytotoxicity was observed across different combined concentrations of CM(MY) and cordycepin. By complementing cordycepin into CM(MY) to the level comparable with CM(FB), we observed that CM(MY) (500 μg/ml) with cordycepin (4.8 μg/ml) induced apoptosis to a level similar to that induced by CM(FB) (500 μg/ml). Together, our results suggest that cordycepin possesses a synergistic cytotoxic effect with Cordyceps militaris-mediated apoptosis in human leukemia cells and therefore explaining a better anti-proliferating activity of CM(FB) over CM(MY).

Published
2014

40. DNA Topoisomerase III Alpha Regulates p53-Mediated Tumor Suppression

Author

Han-Wen Chang, Tsai-Kun Li, Jia-Rong Fan, Hsiang-Chin Chen, Tang-Long Shen, Mei Yi Hsieh, Yen-Hsiu Yeh, and Shu-Chun Teng

Subjects
Cyclin-Dependent Kinase Inhibitor p21, Chromatin Immunoprecipitation, Cancer Research, DNA repair, Immunoblotting, Mice, SCID, Biology, Real-Time Polymerase Chain Reaction, medicine.disease_cause, Small hairpin RNA, Mice, Mice, Inbred NOD, Cell Line, Tumor, medicine, Animals, Humans, Immunoprecipitation, Regulation of gene expression, Gene knockdown, Mutation, Molecular biology, Gene Expression Regulation, Neoplastic, Real-time polymerase chain reaction, DNA Topoisomerases, Type I, Oncology, Heterografts, Ectopic expression, Tumor Suppressor Protein p53, Chromatin immunoprecipitation
Abstract

Purpose: Human DNA topoisomerase III alpha (hTOP3α) is involved in DNA repair surveillance and cell-cycle checkpoints possibly through formatting complex with tumor suppressors. However, its role in cancer development remained unsolved. Experimental Design: Coimmunoprecipitation, sucrose gradient, chromatin immunoprecipitation (ChIP), real time PCR, and immunoblotting analyses were performed to determine interactions of hTOP3α with p53. Paired cell lines with different hTOP3α levels were generated via ectopic expression and short hairpin RNA (shRNA)-mediated knockdown approaches. Cellular tumorigenic properties were analyzed using cell counting, colony formation, senescence, soft agar assays, and mouse xenograft models. Results: The hTOP3α isozyme binds to p53 and cofractionizes with p53 in gradients differing from fractions containing hTOP3α and BLM. Knockdown of hTOP3α expression (sh-hTOP3α) caused a higher anchorage-independent growth of nontumorigenic RHEK-1 cells. Similarly, sh-hTOP3α and ectopic expression of hTOP3α in cancer cell lines caused increased and reduced tumorigenic abilities, respectively. Genetic and mutation experiments revealed that functional hTOP3α, p53, and p21 are required for this tumor-suppressive activity. Mechanism-wise, ChIP data revealed that hTOP3α binds to the p53 and p21 promoters and positively regulates their expression. Two proteins affect promoter recruitments of each other and collaborate in p21 expression. Moreover, sh-hTOP3α and sh-p53 in AGS cells caused a similar reduction in senescence and hTOP3α mRNA levels were lower in gastric and renal tumor samples. Conclusion: We concluded that hTOP3α interacts with p53, regulates p53 and p21 expression, and contributes to the p53-mediated tumor suppression. Clin Cancer Res; 20(6); 1489–501. ©2014 AACR.

Published
2014

41. A Negative Feedback of the HIF-1α Pathway via Interferon-Stimulated Gene 15 and ISGylation

Author

Tsai-Kun Li, Mei Yi Hsieh, Yen-Hsiu Yeh, Yu-Chen Yang, and Yen-Cheng Yeh

Subjects
Cancer Research, Biology, Response Elements, Cell Line, Tumor, Gene expression, Humans, Protein Interaction Domains and Motifs, Hypoxia, Ubiquitins, Transcription factor, Cell Proliferation, Regulation of gene expression, Gene knockdown, Interferon-stimulated gene, Hypoxia-Inducible Factor 1, alpha Subunit, ISG15, Molecular biology, Cell biology, Reverse transcription polymerase chain reaction, Cell Transformation, Neoplastic, Gene Expression Regulation, Oncology, Cytokines, Interferons, Signal transduction, Protein Binding, Signal Transduction
Abstract

Purpose: The IFN-stimulated gene 15 (ISG15)- and ubiquitin-conjugation pathways play roles in mediating hypoxic and inflammatory responses. To identify interaction(s) between these two tumor microenvironments, we investigated the effect of ISG15 on the activity of the master hypoxic transcription factor HIF-1α. Experimental Design: IFN and desferoxamine treatments were used to induce the expression of ISGs and HIF-1α, respectively. Interactions between HIF-1α and the ISG15 and ISGylation system were studied using knockdown of mRNA expression, immunoblotting, coimmunoprecipitation, and pull-down analyses. Effects of the ISG15 and ISGylation system on the HIF-1α–directed processes were examined using reporter, reverse transcription polymerase chain reaction (RT-PCR), and tumorigenic growth assays. Results: We found that the level of the free form of HIF-1α is differentially regulated by IFN treatment, and that the free ISG15 level is lower under hypoxia. Mechanism-directed studies have shown that HIF-1α not only interacts physically with ISG15, but is also ISGylated in multiple domains. ISG15 expression disrupts the functional dimerization of HIF-1α and -1β. Subsequently, expression of the ISG15 and/or ISGylation system attenuates HIF-1α–mediated gene expression and tumorigenic growth. Conclusion: In summary, our results revealed cross-talk between inflammatory and hypoxic pathways through the ISGylation of HIF-1α. On the basis of these results, we propose a novel negative feedback loop for the HIF-1α–mediated pathway involving the regulation of HIF-1α via IFN-induced ISGylation. Clin Cancer Res; 19(21); 5927–39. ©2013 AACR.

Published
2013

42. On the structural basis and design guidelines for type II topoisomerase-targeting anticancer drugs

Author

Nei-Li Chan, Yi-Ching Li, Ying-Ren Wang, Tsai-Kun Li, and C.-K. Wu

Subjects
Drug, Amsacrine, Models, Molecular, media_common.quotation_subject, Antineoplastic Agents, Guidelines as Topic, Drug action, Cleavage (embryo), chemistry.chemical_compound, Structure-Activity Relationship, Structural Biology, Antigens, Neoplasm, Genetics, Humans, Topoisomerase II Inhibitors, Poly-ADP-Ribose Binding Proteins, media_common, biology, Topoisomerase, DNA-Binding Proteins, DNA Topoisomerases, Type II, Biochemistry, chemistry, Drug Design, biology.protein, Biophysics, Topoisomerase-II Inhibitor, Mitoxantrone, Type II topoisomerase, DNA
Abstract

Type II topoisomerases (Top2s) alter DNA topology via the formation of an enzyme–DNA adduct termed cleavage complex, which harbors a transient double-strand break in one DNA to allow the passage of another. Agents targeting human Top2s are clinically active anticancer drugs whose trapping of Top2-mediated DNA breakage effectively induces genome fragmentation and cell death. To understand the structural basis of this drug action, we previously determined the structure of human Top2 β-isoform forming a cleavage complex with the drug etoposide and DNA, and described the insertion of drug into DNA cleavage site and drug-induced decoupling of catalytic groups. By developing a post-crystallization drug replacement procedure that simplifies structural characterization of drug-stabilized cleavage complexes, we have extended the analysis toward other structurally distinct drugs, m-AMSA and mitoxantrone. Besides the expected drug intercalation, a switch in ribose puckering in the 3′-nucleotide of the cleavage site was robustly observed in the new structures, representing a new mechanism for trapping the Top2 cleavage complex. Analysis of drug-binding modes and the conformational landscapes of the drug-binding pockets provide rationalization of the drugs’ structural-activity relationships and explain why Top2 mutants exhibit differential effects toward each drug. Drug design guidelines were proposed to facilitate the development of isoform-specific Top2-targeting anticancer agents.

Published
2013

43. Topoisomerase II-Mediated DNA Cleavage and Mutagenesis Activated by Nitric Oxide Underlie the Inflammation-Associated Tumorigenesis

Author

Han-Yi Elizabeth Chou, Yu-Chen Yang, Tsai-Kun Li, Wei-Jer Chang, Pei-Han Tai, and Tang-Long Shen

Subjects
Genome instability, Pyridines, Physiology, DNA damage, 9,10-Dimethyl-1,2-benzanthracene, Clinical Biochemistry, HL-60 Cells, Nitric Oxide, medicine.disease_cause, Biochemistry, Cell Line, Nitric oxide, S-Nitrosoglutathione, Mice, chemistry.chemical_compound, medicine, Animals, Humans, Nitric Oxide Donors, DNA Cleavage, Molecular Biology, Etoposide, General Environmental Science, Inflammation, Mice, Knockout, biology, Topoisomerase, Mutagenesis, Cell Biology, HCT116 Cells, Molecular biology, Coculture Techniques, Cell Transformation, Neoplastic, DNA Topoisomerases, Type II, chemistry, Cancer research, biology.protein, General Earth and Planetary Sciences, Carcinogenesis, medicine.drug
Abstract

Both cancer-suppressing and cancer-promoting properties of reactive nitrogen and oxygen species (RNOS) have been suggested to play a role in tumor pathology, particularly those activities associated with chronic inflammation. Here, we address the impact of nitric oxide (NO) on the induction of DNA damage and genome instability with a specific focus on the involvement of topoisomerase II (TOP2). We also investigate the contribution of NO to the formation of skin melanoma in mice.Similar to the TOP2-targeting drug, etoposide (VP-16), the NO-donor, S-nitrosoglutathione (GSNO), induces skin melanomas formation in 7,12-dimethyl- benz[a]anthracene (DMBA)-initiated mice. To explore the mechanism(s) underlying this NO-induced tumorigenesis, we use a co-culture model system to demonstrate that inflamed macrophages with inducible NO synthase (iNOS) expression cause γ-H2AX activation, p53 phosphorylation, and chromosome DNA breaks in the target cells. Inhibitor experiments revealed that NO and TOP2 isozymes are responsible for the above described cellular phenotypes. Notably, NO, unlike VP-16, preferentially induces the formation of TOP2β cleavable complexes (TOP2βcc) in cells. Moreover, GSNO induced TOP2-dependent DNA sequence rearrangements and cytotoxicity. Furthermore, the incidences of GSNO- and VP-16-induced skin melanomas were also observed to be lower in the skin-specific top2β-knockout mice. Our results suggest that TOP2 isozymes contribute to NO-induced mutagenesis and subsequent cancer development during chronic inflammation.We provide the first experimental evidence for the functional role of TOP2 in NO-caused DNA damage, mutagenesis, and carcinogenesis. Notably, these studies contribute to our molecular understanding of the cancer-promoting actions of RNOS during chronic inflammation.

Published
2013

44. microRNA-183 Mediates Protective Postconditioning of the Liver by Repressing Apaf-1

Author

Han-Chen Lin, Er-Yen Yen, I-Rue Lai, Tsai-Kun Li, and Shin-Yun Liu

Subjects
0301 basic medicine, Male, Programmed cell death, Physiology, Mrna expression, Clinical Biochemistry, Clone (cell biology), Gene Expression, Apoptosis, Biology, Pharmacology, Biochemistry, 03 medical and health sciences, Mice, 0302 clinical medicine, microRNA, Animals, Ischemic Postconditioning, Molecular Biology, General Environmental Science, Microarray analysis techniques, Cell Biology, Rats, Oxygen, MicroRNAs, Oxidative Stress, 030104 developmental biology, Apoptotic Protease-Activating Factor 1, Glucose, Gene Expression Regulation, Liver, 030220 oncology & carcinogenesis, Reperfusion Injury, General Earth and Planetary Sciences, RNA Interference, Injury model, In vivo experiment, Signal Transduction
Abstract

Ischemic postconditioning (iPoC) is known to mitigate ischemia-reperfusion (IR) injury of the liver, the mechanisms of which remain to be elucidated. This study explored the role of microRNA-183 (miR-183) in the protective mechanism of iPoC.Microarray analysis showed miR-183 was robustly expressed in rats' livers with iPoC. miR-183 repressed the mRNA expression of Apaf-1, which is an apoptosis promoting factor. Using an oxygen-glucose deprivation (OGD) injury model in Clone 9 cells, hypoxic postconditioning (HPoC) and an miR-183 mimetic significantly decreased cell death after OGD, but miR-183 inhibitors eliminated the protection of HPoC. The increased expression of Apaf-1 and the downstream activation of capsase-3/9 after OGD were mitigated by HPoC or the addition of miR-183 mimetics, whereas miR-183 inhibitor diminished the effect of HPoC on Apaf-1-caspase signaling. In the in vivo experiment, iPoC and agomiR-183 decreased the expression of serum ALT after liver IR in the mice, but antagomiR-183 mitigated the effect of iPoC. The results of hematoxylin and eosin and TUNEL staining were compatible with the biochemical assay. Moreover, iPoC and agomiR-183 decreased the expression of Apaf-1 and 4-HNE after IR injury in mouse livers, whereas the antagomiR-mediated prevention of miR-183 expression led to increased protein expression of Apaf-1 and 4-HNE in the postischemic livers.Our experiment showed the first time that miR-183 was induced in protective postconditioning and reduced reperfusion injury of the livers via the targeting of apoptotic signaling.miR-183 mediated the tolerance induced by iPoC in livers via Apaf-1 repressing. Antioxid. Redox Signal. 26, 583-597.

Published
2016

45. Trichodermin induces c-Jun N-terminal kinase-dependent apoptosis caused by mitotic arrest and DNA damage in human p53-mutated pancreatic cancer cells and xenografts

Author

Yung Wei Lin, Po Chuan Wang, Michael Hsiao, Yen Hsiu Yeh, Jih Jung Chen, Ming Hsien Chien, Tsai-Kun Li, Jyh Ming Chow, Tzong-Huei Lee, Wei Jiunn Lee, Shih-Wei Wang, and Kuo Tai Hua

Subjects
0301 basic medicine, Male, Cancer Research, DNA damage, Trichodermin, Mitosis, Apoptosis, Mice, SCID, Biology, 03 medical and health sciences, chemistry.chemical_compound, Mice, Pancreatic cancer, Cell Line, Tumor, medicine, Animals, Humans, Kinase, c-jun, Intrinsic apoptosis, JNK Mitogen-Activated Protein Kinases, Cancer, medicine.disease, Pancreatic Neoplasms, 030104 developmental biology, Oncology, chemistry, Cancer research, Tumor Suppressor Protein p53, DNA Damage, Signal Transduction
Abstract

Pancreatic cancer is an aggressive malignancy, which generally responds poorly to chemotherapy. In this study, trichodermin, an endophytic fungal metabolite from Nalanthamala psidii, was identified as a potent and selective antitumor agent in human pancreatic cancer. Trichodermin exhibited antiproliferative effects against pancreatic cancer cells, especially p53-mutated cells (MIA PaCa-2 and BxPC-3) rather than normal pancreatic epithelial cells. We found that trichodermin induced caspase-dependent and mitochondrial intrinsic apoptosis. Trichodermin also increased apoptosis through mitotic arrest by activating Cdc2/cyclin B1 complex activity. Moreover, trichodermin promoted the activation of c-Jun N-terminal kinase (JNK), and inhibition of JNK by its inhibitor, shRNA, or siRNA significantly reversed trichodermin-mediated caspase-dependent apoptosis. Trichodermin triggered DNA damage stress to activate p53 function for executing apoptosis in p53-mutated cells. Importantly, we demonstrated that trichodermin with efficacy similar to gemcitabine, profoundly suppressed tumor growth through inducing intratumoral DNA damage and JNK activation in orthotopic pancreatic cancer model. Based on these findings, trichodermin is a potential therapeutic agent worthy of further development into a clinical trial candidate for treating cancer, especially the mutant p53 pancreatic cancer.

Published
2016

46. Rottlerin potentiates camptothecin-induced cytotoxicity in human hormone refractory prostate cancers through increased formation and stabilization of topoisomerase I-DNA cleavage complexes in a PKCδ-independent pathway

Author

Ching-Shih Chen, Tsai-Kun Li, Yunn-Fang Ho, Lih-Ching Hsu, Jui-Ling Hsu, and Jih-Hwa Guh

Subjects
Male, Neoplasms, Hormone-Dependent, Cell Survival, DNA repair, DNA damage, Blotting, Western, Cell Culture Techniques, Apoptosis, Topoisomerase-I Inhibitor, Transfection, Biochemistry, Article, chemistry.chemical_compound, Cell Line, Tumor, Antineoplastic Combined Chemotherapy Protocols, In Situ Nick-End Labeling, medicine, Humans, Benzopyrans, heterocyclic compounds, DNA Cleavage, RNA, Small Interfering, Pharmacology, biology, Topoisomerase, Acetophenones, Prostatic Neoplasms, Drug Synergism, Flow Cytometry, Molecular biology, Protein Kinase C-delta, DNA Topoisomerases, Type I, chemistry, Cancer research, biology.protein, DNA fragmentation, Camptothecin, Topoisomerase I Inhibitors, Rottlerin, medicine.drug
Abstract

Combination therapy, which can optimize killing activity to cancers and minimize drug resistance, is a mainstream therapy against hormone-refractory prostate cancers (HRPCs). Rottlerin, a natural polyphenolic component, synergistically increased PC-3 (a HRPC cell line) apoptosis induced by camptothecin (a topoisomerase I inhibitor). Using siRNA technique to knockdown protein kinase C-δ (PKCδ), the data showed that rottlerin-mediated synergistic effect was PKCδ-independent, although rottlerin has been used as a PKCδ inhibitor. Rottlerin potentiated camptothecin-induced DNA fragmentation at S phase and ATM phosphorylation at Ser1981. The effect was correlated to apoptosis (r2 = 0.9). To detect upstream signals, the data showed that camptothecin acted on and stabilized topoisomerase I-DNA complex, leading to the formation of camptothecin-trapped cleavage complexes (TOP1cc). The effect was potentiated by rottlerin. To determine DNA repair capability, the time-related γH2A.X formation was examined after camptothecin removal. Consequently, rottlerin significantly inhibited camptothecin removal-mediated decline of γH2A.X formation at S phase, indicating the impairment of DNA repair activity in the presence of rottlerin. The combinatory treatment of camptothecin and rottlerin induced conformational change and activation of Bax and formation of truncated Bad, suggesting the contribution of mitochondria stress to apoptosis. In summary, the data suggest that rottlerin-mediated camptothecin sensitization is through the augmented stabilization of TOP1cc, leading to an increase of DNA damage stress and, possibly, an impairment of DNA repair capability. Subsequently, mitochondria-involved apoptosis is triggered through Bax activation and truncated Bad formation. The novel discovery may provide an anticancer approach of combinatory use between rottlerin and camptothecin for the treatment of HRPCs.

Published
2012

47. Multiple Domains of the Tobacco mosaic virus p126 Protein Can Independently Suppress Local and Systemic RNA Silencing

Author

Shih-Shun Lin, Ting-Hsuan Hung, Tang-Long Shen, Li-Ya Wang, Tsai-Kun Li, and Nai-Chun Lin

Subjects
RNA-induced transcriptional silencing, Physiology, RNA-induced silencing complex, DNA Mutational Analysis, Green Fluorescent Proteins, Trans-acting siRNA, Viral Proteins, Tobacco, Tobacco mosaic virus, Gene silencing, Plant Diseases, Genetics, biology, DNA Helicases, Helicase, Methyltransferases, General Medicine, Argonaute, Protein Structure, Tertiary, Plant Leaves, Tobacco Mosaic Virus, RNA silencing, Gene Expression Regulation, biology.protein, RNA Interference, Agronomy and Crop Science
Abstract

Small RNA-mediated RNA silencing is a widespread antiviral mechanism in plants and other organisms. Many viruses encode suppressors of RNA silencing for counter-defense. The p126 protein encoded by Tobacco mosaic virus (TMV) has been reported to be a suppressor of RNA silencing but the mechanism of its function remains unclear. This protein is unique among the known plant viral silencing suppressors because of its large size and multiple domains. Here, we report that the methyltransferase, helicase, and nonconserved region II (NONII) of p126 each has silencing-suppressor function. The silencing-suppression activities of methyltransferase and helicase can be uncoupled from their enzyme activities. Specific amino acids in NONII previously shown to be crucial for viral accumulation and symptom development are also crucial for silencing suppression. These results suggest that some viral proteins have evolved to possess modular structural domains that can independently interfere with host silencing, and that this may be an effective mechanism of increasing the robustness of a virus.

Published
2012

48. Mitoxantrone Inhibits HIF-1α Expression in a Topoisomerase II–Independent Pathway

Author

Yng-Miin Toh and Tsai-Kun Li

Subjects
Proteasome Endopeptidase Complex, Cancer Research, Antineoplastic Agents, Cycloheximide, Biology, Pharmacology, Gene Knockout Techniques, chemistry.chemical_compound, Cell Line, Tumor, medicine, Humans, Doxorubicin, RNA, Messenger, Etoposide, Gene knockdown, Mitoxantrone, Topoisomerase, Hypoxia-Inducible Factor 1, alpha Subunit, Kidney Neoplasms, DNA Topoisomerases, Type II, Oncology, chemistry, Cell culture, Protein Biosynthesis, Mutation, biology.protein, Signal transduction, Colorectal Neoplasms, Signal Transduction, medicine.drug
Abstract

Purpose: Solid tumors encounter a growth-limiting hypoxic microenvironment as they develop. Hypoxia-inducible factors (HIF) play important roles in hypoxia-associated tumor development and therapeutic resistance. Targeting the HIF pathway (especially HIF-1α) represents a promising cancer treatment strategy. Here, we report a novel class of HIF-1α inhibitors and the possible molecular basis of inhibition. Experimental Design: We analyzed the inhibitory effects of clinically used topoisomerase II (TOP2)–targeting drugs on HIF-1α expression with a primary focus on mitoxantrone. The potential role of TOP2 in mitoxantrone-inhibited HIF-1α expression was studied using pharmacologic inhibition, a knockdown approach, and TOP2 mutant cells. Moreover, involvement of mitoxantrone in proteasome-mediated degradation, transcription, and translation of HIF-1α was examined. Results: The TOP2-targeting mitoxantrone, but neither doxorubicin nor etoposide (VP-16), strongly inhibited HIF-1α expression under hypoxic conditions in a dose- and time-dependent manner. Surprisingly, the mitoxantrone-mediated inhibition of HIF-1α expression was largely independent of two TOP2 isozymes, proteasomal degradation, and transcription. Furthermore, mitoxantrone inhibited HIF-1α expression and function in a similar fashion as cycloheximide, suggesting that mitoxantrone might inhibit HIF-1α via a blockage at its translation step. In vitro translation experiments using HIF-1α mRNA further confirmed inhibition of HIF-1α translation by mitoxantrone. Interestingly, levels of the polysome-bound HIF-1α and VEGF-A mRNA were elevated and decreased after mitoxantrone treatment, respectively. Conclusions: We have identified the TOP2-targeting compound, mitoxantrone, as an HIF-1α inhibitor possibly through a translation inhibition mechanism, suggesting the possibility of an additional anticancer activity for mitoxantrone. Clin Cancer Res; 17(15); 5026–37. ©2011 AACR.

Published
2011

49. Structural Basis of Type II Topoisomerase Inhibition by the Anticancer Drug Etoposide

Author

Yu-Jen Yu, Tien-Jui Yen, Nei-Li Chan, Chia-Wang Chiang, Tsai-Kun Li, Li-Ying Lin, Te-Sheng Lin, Lynn Farh, and C.-K. Wu

Subjects
Models, Molecular, Base pair, Population, Crystallography, X-Ray, Cleavage (embryo), Structure-Activity Relationship, chemistry.chemical_compound, Catalytic Domain, medicine, Humans, Topoisomerase II Inhibitors, A-DNA, Protein Structure, Quaternary, education, Base Pairing, Etoposide, education.field_of_study, Multidisciplinary, biology, Topoisomerase, DNA, Protein Structure, Tertiary, DNA-Binding Proteins, DNA Topoisomerases, Type II, Biochemistry, chemistry, Drug Resistance, Neoplasm, Mutation, biology.protein, Mutant Proteins, Protein Multimerization, Type II topoisomerase, medicine.drug
Abstract

Type II topoisomerases (TOP2s) resolve the topological problems of DNA by transiently cleaving both strands of a DNA duplex to form a cleavage complex through which another DNA segment can be transported. Several widely prescribed anticancer drugs increase the population of TOP2 cleavage complex, which leads to TOP2-mediated chromosome DNA breakage and death of cancer cells. We present the crystal structure of a large fragment of human TOP2β complexed to DNA and to the anticancer drug etoposide to reveal structural details of drug-induced stabilization of a cleavage complex. The interplay between the protein, the DNA, and the drug explains the structure-activity relations of etoposide derivatives and the molecular basis of drug-resistant mutations. The analysis of protein-drug interactions provides information applicable for developing an isoform-specific TOP2-targeting strategy.

Published
2011

50. Sodium salicylate acts through direct inhibition of phosphoinositide 3-kinase-like kinases to modulate topoisomerase-mediated DNA damage responses

Author

Tsai-Kun Li, Tang-Long Shen, Ting-Hsiang Huang, Jia-Rong Fan, and Chen-Yu Wen

Subjects
DNA damage, Sodium Salicylate, Cell Cycle Proteins, Ataxia Telangiectasia Mutated Proteins, DNA-Activated Protein Kinase, Protein Serine-Threonine Kinases, Pharmacology, MAP2K7, chemistry.chemical_compound, Replication Protein A, Humans, Drug Interactions, ASK1, Phosphorylation, Kinase activity, Protein kinase A, Sodium salicylate, Cell Death, Cyclooxygenase 2 Inhibitors, biology, Tumor Suppressor Proteins, Anti-Inflammatory Agents, Non-Steroidal, Cyclin-dependent kinase 2, NF-kappa B, HCT116 Cells, DNA-Binding Proteins, chemistry, Biochemistry, biology.protein, Camptothecin, Cyclin-dependent kinase 9, Tumor Suppressor Protein p53, DNA Topoisomerases, DNA Damage, Signal Transduction
Abstract

Chemopreventive non-steroidal anti-inflammatory drugs (NSAIDs) exhibit diverse pharmacological and biological activities mainly through their inhibitory effect on cyclooxygenase (COX). However, COX-independent mechanisms involving kinase inhibition have been proposed to explain certain therapeutic effects of NSAIDs. Here, we explored the potential relationship between chemopreventive NSAIDs and DNA damage responses induced by treatment with topoisomerase-targeting drugs. (1) Sodium salicylate, a non-COX-selective NSAID, was shown to reduce DNA damage-induced RPA and p53 phosphorylation. (2) The formation of enzyme cleavable complexes by topoisomerase-targeting drugs was not affected in the presence of sodium salicylate. (3) The attenuating effect of NSAIDs on the DNA damage responses is COX-2-independent, since COX-2-selective inhibitors failed to inhibit DNA damage-induced phosphorylation of replication protein A (RPA) and p53. (4) This COX-2-independent attenuating effect was mediated through interference of neither nuclear factor kappa B nor extracellular signal-regulated kinase pathways. (5) The activation of ataxia telangiectasia mutated (ATM) kinase and DNA-dependent protein kinase (DNA-PK), two key signal transducers upstream of RPA and p53, was found to be significantly reduced with sodium salicylate treatment. (6) Most importantly, sodium salicylate and other NSAIDs directly inhibited kinase activity of ATM and DNA-PK. The extent of inhibition on the kinase activity also correlated with the degree of attenuation on the DNA damage responses. (7) Unexpectedly, sodium salicylate showed a p53-independent protection effect on topoisomerase-mediated cell killing. Together, our study provides evidence that NSAIDs exhibit a novel COX-independent modulating activity of NSAIDs on the DNA damage responses and it is through inhibition of phosphoinositide 3-kinase-like kinases.

Published
2010

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