Your search keyword '"Plicamycin"' showing total 1,052 results

1. Chemotherapy for pain: reversing inflammatory and neuropathic pain with the anticancer agent mithramycin A.

Author

Xu, Zheyun, Lee, Man-Cheung, Sheehan, Kayla, Fujii, Keisuke, Rabl, Katalin, Rader, Gabriella, Varney, Scarlett, Sharma, Manohar, Eilers, Helge, Levine, Jon, Schumacher, Mark, Miaskowski, Christine, and Kober, Kord

Subjects

Humans, Plicamycin, Oxaliplatin, Antineoplastic Agents, Neuralgia, Hyperalgesia, Ganglia, Spinal

Abstract

The persistence of inflammatory and neuropathic pain is poorly understood. We investigated a novel therapeutic paradigm by targeting gene networks that sustain or reverse persistent pain states. Our prior observations found that Sp1-like transcription factors drive the expression of TRPV1, a pain receptor, that is blocked in vitro by mithramycin A (MTM), an inhibitor of Sp1-like factors. Here, we investigate the ability of MTM to reverse in vivo models of inflammatory and chemotherapy-induced peripheral neuropathy (CIPN) pain and explore MTMs underlying mechanisms. Mithramycin reversed inflammatory heat hyperalgesia induced by complete Freund adjuvant and cisplatin-induced heat and mechanical hypersensitivity. In addition, MTM reversed both short-term and long-term (1 month) oxaliplatin-induced mechanical and cold hypersensitivity, without the rescue of intraepidermal nerve fiber loss. Mithramycin reversed oxaliplatin-induced cold hypersensitivity and oxaliplatin-induced TRPM8 overexpression in dorsal root ganglion (DRG). Evidence across multiple transcriptomic profiling approaches suggest that MTM reverses inflammatory and neuropathic pain through broad transcriptional and alternative splicing regulatory actions. Mithramycin-dependent changes in gene expression following oxaliplatin treatment were largely opposite to and rarely overlapped with changes in gene expression induced by oxaliplatin alone. Notably, RNAseq analysis revealed MTM rescue of oxaliplatin-induced dysregulation of mitochondrial electron transport chain genes that correlated with in vivo reversal of excess reactive oxygen species in DRG neurons. This finding suggests that the mechanism(s) driving persistent pain states such as CIPN are not fixed but are sustained by ongoing modifiable transcription-dependent processes.

Published

2024

2. Continuous 24h Intravenous Infusion of Mithramycin, an Inhibitor of Cancer Stem Cell Signaling, in People With Primary Thoracic Malignancies or Carcinomas, Sarcomas or Germ Cell Neoplasms With Pleuropulmonary Metastases

Author

David Schrump, M.D., Principal Investigator

Published

2022

3. Identification of plicamycin, TG02, panobinostat, lestaurtinib, and GDC-0084 as promising compounds for the treatment of central nervous system infections caused by the free-living amebae Naegleria, Acanthamoeba and Balamuthia.

Author

Kangussu-Marcolino, Monica, Ehrenkaufer, Gretchen, Chen, Emily, Debnath, Anjan, and Singh, Upinder

Subjects

Acanthamoeba, Balamuthia, CNS infection, Drug screening, Naegleria, ReFRAME library, Acanthamoeba, Amebiasis, Amoebozoa, Antiprotozoal Agents, Carbazoles, Cell Culture Techniques, Central Nervous System Protozoal Infections, Culture Media, Dose-Response Relationship, Drug, Drug Evaluation, Preclinical, Enzyme Inhibitors, Furans, Heterocyclic Compounds, 4 or More Rings, Inhibitory Concentration 50, Naegleria, Oxazines, Panobinostat, Plicamycin, Pyrimidines

Abstract

The free-living amebae Naegleria, Acanthamoeba, and Balamuthia cause rare but life-threatening infections. All three parasites can cause meningoencephalitis. Acanthamoeba can also cause chronic keratitis and both Balamuthia and Acanthamoeba can cause skin and systemic infections. There are minimal drug development pipelines for these pathogens despite a lack of available treatment regimens and high fatality rates. To identify anti-amebic drugs, we screened 159 compounds from a high-value repurposed library against trophozoites of the three amebae. Our efforts identified 38 compounds with activity against at least one ameba. Multiple drugs that bind the ATP-binding pocket of mTOR and PI3K are active, highlighting these compounds as important inhibitors of these parasites. Importantly, 24 active compounds have progressed at least to phase II clinical studies and overall 15 compounds were active against all three amebae. Based on central nervous system (CNS) penetration or exceptional potency against one amebic species, we identified sixteen priority compounds for the treatment of meningoencephalitis caused by these pathogens. The top five compounds are (i) plicamycin, active against all three free-living amebae and previously U.S. Food and Drug Administration (FDA) approved, (ii) TG02, active against all three amebae, (iii and iv) FDA-approved panobinostat and FDA orphan drug lestaurtinib, both highly potent against Naegleria, and (v) GDC-0084, a CNS penetrant mTOR inhibitor, active against at least two of the three amebae. These results set the stage for further investigation of these clinically advanced compounds for treatment of infections caused by the free-living amebae, including treatment of the highly fatal meningoencephalitis.

Published

2019

4. Chromomycin A2 potently inhibits glucose-stimulated insulin secretion from pancreatic β cells

Author

Kalwat, Michael A, Hwang, In Hyun, Macho, Jocelyn, Grzemska, Magdalena G, Yang, Jonathan Z, McGlynn, Kathleen, MacMillan, John B, and Cobb, Melanie H

Subjects

Biochemistry and Cell Biology, Medical Physiology, Biomedical and Clinical Sciences, Biological Sciences, Diabetes, Genetics, 1.1 Normal biological development and functioning, 5.1 Pharmaceuticals, 2.1 Biological and endogenous factors, Metabolic and endocrine, Animals, Cell Line, Gene Expression, Humans, Insulin Secretion, Insulin-Secreting Cells, Mice, Plicamycin, Primary Cell Culture, Signal Transduction, Streptomyces, Physiology, Biochemistry and cell biology, Zoology, Medical physiology

Abstract

Modulators of insulin secretion could be used to treat diabetes and as tools to investigate β cell regulatory pathways in order to increase our understanding of pancreatic islet function. Toward this goal, we previously used an insulin-linked luciferase that is cosecreted with insulin in MIN6 β cells to perform a high-throughput screen of natural products for chronic effects on glucose-stimulated insulin secretion. In this study, using multiple phenotypic analyses, we found that one of the top natural product hits, chromomycin A2 (CMA2), potently inhibited insulin secretion by at least three potential mechanisms: disruption of Wnt signaling, interference of β cell gene expression, and partial suppression of Ca2+ influx. Chronic treatment with CMA2 largely ablated glucose-stimulated insulin secretion even after washout, but it did not inhibit glucose-stimulated generation of ATP or Ca2+ influx. However, by using the KATP channel opener diazoxide, we uncovered defects in depolarization-induced Ca2+ influx that may contribute to the suppressed secretory response. Glucose-responsive ERK1/2 and S6 phosphorylation were also disrupted by chronic CMA2 treatment. By querying the FUSION bioinformatic database, we revealed that the phenotypic effects of CMA2 cluster with a number of Wnt-GSK3 pathway-related genes. Furthermore, CMA2 consistently decreased GSK3β phosphorylation and suppressed activation of a β-catenin activity reporter. CMA2 and a related compound, mithramycin, are known to have DNA interaction properties, possibly abrogating transcription factor binding to critical β cell gene promoters. We observed that CMA2 but not mithramycin suppressed expression of PDX1 and UCN3. However, neither expression of INSI/II nor insulin content was affected by chronic CMA2. The mechanisms of CMA2-induced insulin secretion defects may involve components both proximal and distal to Ca2+ influx. Therefore, CMA2 is an example of a chemical that can simultaneously disrupt β cell function through both noncytotoxic and cytotoxic mechanisms. Future therapeutic applications of CMA2 and similar aureolic acid analogues should consider their potential effects on pancreatic islet function.

Published

2018

5. Mithramycin for Lung, Esophagus, and Other Chest Cancers

Author

David Schrump, M.D., Principal Investigator

Published

2019

6. Mithramycin for Children and Adults With Solid Tumors or Ewing Sarcoma

Author

Brigitte Widemann, M.D., Principal Investigator

Published

2018

7. Mithramycin Is a Gene-Selective Sp1 Inhibitor That Identifies a Biological Intersection between Cancer and Neurodegeneration

Author

Sleiman, Sama F, Langley, Brett C, Basso, Manuela, Berlin, Jill, Xia, Li, Payappilly, Jimmy B, Kharel, Madan K, Guo, Hengchang, Marsh, J Lawrence, Thompson, Leslie Michels, Mahishi, Lata, Ahuja, Preeti, MacLellan, W Robb, Geschwind, Daniel H, Coppola, Giovanni, Rohr, Jürgen, and Ratan, Rajiv R

Subjects

Biomedical and Clinical Sciences, Neurosciences, Prevention, Cancer, Genetics, Rare Diseases, Neurodegenerative, 2.1 Biological and endogenous factors, 5.1 Pharmaceuticals, Analysis of Variance, Animals, Animals, Genetically Modified, Antibiotics, Antineoplastic, Blotting, Western, Cell Survival, Cells, Cultured, Cerebral Cortex, Chromatin Immunoprecipitation, Drosophila, Neurons, Plicamycin, Rats, Rats, Sprague-Dawley, Sp1 Transcription Factor, Structure-Activity Relationship, Medical and Health Sciences, Psychology and Cognitive Sciences, Neurology & Neurosurgery

Abstract

Oncogenic transformation of postmitotic neurons triggers cell death, but the identity of genes critical for degeneration remain unclear. The antitumor antibiotic mithramycin prolongs survival of mouse models of Huntington's disease in vivo and inhibits oxidative stress-induced death in cortical neurons in vitro. We had correlated protection by mithramycin with its ability to bind to GC-rich DNA and globally displace Sp1 family transcription factors. To understand how antitumor drugs prevent neurodegeneration, here we use structure-activity relationships of mithramycin analogs to discover that selective DNA-binding inhibition of the drug is necessary for its neuroprotective effect. We identify several genes (Myc, c-Src, Hif1α, and p21(waf1/cip1)) involved in neoplastic transformation, whose altered expression correlates with protective doses of mithramycin or its analogs. Most interestingly, inhibition of one these genes, Myc, is neuroprotective, whereas forced expression of Myc induces Rattus norvegicus neuronal cell death. These results support a model in which cancer cell transformation shares key genetic components with neurodegeneration.

Published

2011

8. Combination of cabazitaxel and plicamycin induces cell death in drug resistant B-cell acute lymphoblastic leukemia.

Author

Nair, Rajesh R., Gibson, Laura F., Piktel, Debbie, and Geldenhuys, Werner J.

Subjects

*LYMPHOBLASTIC leukemia treatment, *B cells, *CELL death, *DRUG resistance in cancer cells, *CABAZITAXEL, *BONE marrow, *THERAPEUTICS

Abstract

Highlights • High-throughput screening identified cabazitaxel and plicamycin for use in ALL. • Cabazitaxel and plicamycin show synergism in inducing death in ALL cells. • Nanoparticle formulation of cabazitaxel and plicamycin retains their activity. Abstract Bone marrow microenvironment mediated downregulation of BCL6 is critical for maintaining cell quiescence and modulating therapeutic response in B-cell acute lymphoblastic leukemia (ALL). In the present study, we have performed a high throughput cell death assay using BCL6 knockdown REH ALL cell line to screen a library of FDA-approved oncology drugs. In the process, we have identified a microtubule inhibitor, cabazitaxel (CAB), and a RNA synthesis inhibitor, plicamycin (PLI) as potential anti-leukemic agents. CAB and PLI inhibited cell proliferation in not only the BCL6 knockdown REH cell line, but also six other ALL cell lines. Furthermore, combination of CAB and PLI had a synergistic effect in inhibiting proliferation in a cytarabine-resistant (REH/Ara-C) ALL cell line. Use of nanoparticles for delivery of CAB and PLI demonstrated that the combination was very effective when tested in a co-culture model that mimics the in vivo bone marrow microenvironment that typically supports ALL cell survival and migration into protective niches. Furthermore, exposure to PLI inhibited SOX2 transcription and exposure to CAB inhibited not only Mcl-1 expression but also chemotaxis in ALL cells. Taken together, our study demonstrates the utility of concomitantly targeting different critical regulatory pathways to induce cell death in drug resistant ALL cells. [ABSTRACT FROM AUTHOR]

Published

2018

9. MYB mediates downregulation of the colorectal cancer metastasis suppressor heterogeneous nuclear ribonucleoprotein L‐like during epithelial‐mesenchymal transition

Author

Waki Hosoda, Koji Komori, Yasuhiro Shimizu, Yasushi Yatabe, Keiichiro Sakuma, Masahiro Aoki, and Eiichi Sasaki

Subjects

Cancer Research, Epithelial-Mesenchymal Transition, Heterogeneous nuclear ribonucleoprotein, Transcription, Genetic, Sp1 Transcription Factor, Down-Regulation, colorectal cancer, MYB, Transfection, Heterogeneous-Nuclear Ribonucleoproteins, Gene Knockout Techniques, Proto-Oncogene Proteins c-myb, Cell, Molecular, and Stem Cell Biology, Downregulation and upregulation, Humans, Metastasis suppressor, Epithelial–mesenchymal transition, Neoplasm Metastasis, Promoter Regions, Genetic, Cell Proliferation, Gene knockdown, epithelial‐mesenchymal transition, Binding Sites, General transcription factor, Chemistry, Original Articles, Plicamycin, General Medicine, HNRNP, SP1, Gene Expression Regulation, Neoplastic, Oncology, Gene Knockdown Techniques, Cancer cell, Disease Progression, Cancer research, Original Article, Colorectal Neoplasms, HT29 Cells

Abstract

Heterogeneous nuclear ribonucleoprotein L‐like (HNRNPLL), a suppressor of colorectal cancer (CRC) metastasis, is transcriptionally downregulated when CRC cells undergo epithelial‐mesenchymal transition (EMT). Here we show that decrease of MYB mediates the downregulation of HNRNPLL during EMT. The promoter activity was attributed to a region from −273 to −10 base pairs upstream of the transcription start site identified by 5'‐RACE analysis, and the region contained potential binding sites for MYB and SP1. Luciferase reporter gene assays and knockdown or knockout experiments for genes encoding the MYB family proteins, MYB, MYBL1, and MYBL2, revealed that MYB was responsible for approximately half of the promoter activity. On the other hand, treatment with mithramycin A, an inhibitor for SP1 and SP3, suppressed the promoter activity and their additive contribution was confirmed by knockout experiments. The expression level of MYB was reduced on EMT while that of SP1 and SP3 was unchanged, suggesting that the downregulation of HNRNPLL during EMT was mediated by the decrease of MYB expression while SP1 and SP3 determine the basal transcription level of HNRNPLL. Histopathological analysis confirmed the accumulation of MYB‐downregulated cancer cells at the invasion front of clinical CRC tissues. These results provide an insight into the molecular mechanism underlying CRC progression., Heterogeneous nuclear ribonucleoprotein L‐like (HNRNPLL), a suppressor of colorectal cancer (CRC) metastasis, is transcriptionally downregulated when CRC cells undergo epithelial‐mesenchymal transition (EMT). Here we show that decrease of MYB mediates the downregulation of HNRNPLL during EMT.

Published

2021

10. Gastric cancer-derived exosomal miR-135b-5p impairs the function of Vγ9Vδ2 T cells by targeting specificity protein 1

Author

Mingyuan Wang, Linqing Sun, Guangbo Zhang, Weichang Chen, Yanzheng Gu, Tongguo Shi, Yanjun Chen, Jiayu Wang, Jinghan Zhu, Jin Shen, and Juntao Li

Subjects

Cancer Research, Plicamycin, Chemistry, T cell, medicine.medical_treatment, Immunology, Immunotherapy, Exosome, Microvesicles, 03 medical and health sciences, 0302 clinical medicine, medicine.anatomical_structure, Oncology, Apoptosis, medicine, Cancer research, Immunology and Allergy, Cytotoxic T cell, Viability assay, 030215 immunology, medicine.drug

Abstract

Recent studies have shown that tumor-derived exosomes participate in the communication between tumor cells and their microenvironment and mediate malignant biological behaviors including immune escape. In this study, we found that gastric cancer (GC) cell-derived exosomes could be effectively uptaken by Vγ9Vδ2 T cells, decrease the cell viability of Vγ9Vδ2 T cells, induce apoptosis, and reduce the production of cytotoxic cytokines IFN-γ and TNF-α. Furthermore, we demonstrated that exosomal miR-135b-5p was delivered into Vγ9Vδ2 T cells. Exosomal miR-135b-5p impaired the function of Vγ9Vδ2 T cells by targeting specificity protein 1 (SP1). More importantly, blocking the SP1 function by Plicamycin, an SP1 inhibitor, abolished the effect of stable miR-135b-5p knockdown GC cell-derived exosomes on Vγ9Vδ2 T cell function. Collectively, our results suggest that GC cell-derived exosomes impair the function of Vγ9Vδ2 T cells via miR-135b-5p/SP1 pathway, and targeting exosomal miR-135b-5p/SP1 axis may improve the efficiency of GC immunotherapy based on Vγ9Vδ2 T cells.

Published

2021

11. Interleukin-10 suppression enhances T-cell antitumor immunity and responses to checkpoint blockade in chronic lymphocytic leukemia

Author

Jon S. Thorson, Sara S. Alhakeem, Gerhard C. Hildebrandt, Subbarao Bondada, Yinan Zhang, Natarajan Muthusamy, Khaled A. Shaaban, Yang Liu, Li Chen, Francesc Marti, James P. Collard, Markos Leggas, Jacqueline R. Rivas, Roger A. Fleischman, and Joseph M. Eckenrode

Subjects

0301 basic medicine, Cancer Research, T cell, Chronic lymphocytic leukemia, antitumor immunity, Apoptosis, Mice, SCID, CD8-Positive T-Lymphocytes, Lymphocyte Activation, Article, B7-H1 Antigen, 03 medical and health sciences, Mice, 0302 clinical medicine, Mice, Inbred NOD, hemic and lymphatic diseases, Tumor Cells, Cultured, Medicine, Cytotoxic T cell, Animals, Humans, Immune Checkpoint Inhibitors, Cell Proliferation, Antibiotics, Antineoplastic, business.industry, Effector, Hematology, Plicamycin, immune checkpoint blockade, medicine.disease, Leukemia, Lymphocytic, Chronic, B-Cell, Xenograft Model Antitumor Assays, Immune checkpoint, Blockade, Interleukin-10, Gene Expression Regulation, Neoplastic, Interleukin 10, Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Case-Control Studies, IL-10, Cancer research, business, CD8, CLL

Abstract

T-cell dysfunction is a hallmark of B-cell Chronic Lymphocytic Leukemia (CLL), where CLL cells downregulate T-cell responses through regulatory molecules including programmed death ligand-1 (PD-L1) and Interleukin-10 (IL-10). Immune checkpoint blockade (ICB) aims to restore T-cell function by preventing the ligation of inhibitory receptors like PD-1. However, most CLL patients do not respond well to this therapy. Thus, we investigated whether IL-10 suppression could enhance antitumor T-cell activity and responses to ICB. Since CLL IL-10 expression depends on Sp1, we utilized a novel, better tolerated analogue of the Sp1 inhibitor mithramycin (MTMox32E) to suppress CLL IL-10. MTMox32Etreatment inhibited mouse and human CLL IL-10 production and maintained T-cell effector functionin vitro. In the Eμ-Tcl1 mouse model, treatment reduced plasma IL-10 and CLL burden and increased CD8+T-cell proliferation, effector and memory cell prevalence, and interferon-γ production. When combined with ICB, suppression of IL-10 improved responses to anti-PD-L1 as shown by a 4.5-fold decrease in CLL cell burden compared to anti-PD-L1 alone. Combination therapy also produced more interferon-γ+, cytotoxic effector KLRG1+, and memory CD8+T-cells, and fewer exhausted T-cells. Since current therapies for CLL do not target IL-10, this provides a novel strategy to improve immunotherapies.

Published

2021

12. Specific protein 1 inhibitor mithramycin A protects cardiomyocytes from myocardial infarction via interacting with PARP

Author

Xiaofei Li, Hai-Hua Geng, Ya-Min Su, Rong Huang, Xiaochen Lu, Hongzhuan Sheng, and Mengkang Fan

Subjects

Male, 0301 basic medicine, Cardiotonic Agents, Transcription, Genetic, Cell Survival, Sp1 Transcription Factor, Poly ADP ribose polymerase, Myocardial Infarction, Apoptosis, Mitochondrial Proteins, 03 medical and health sciences, 0302 clinical medicine, Transcription (biology), In vivo, Animals, Myocytes, Cardiac, Viability assay, Gene knockdown, Chemistry, Membrane Proteins, Plicamycin, Cell Biology, General Medicine, Cell Hypoxia, Mice, Inbred C57BL, 030104 developmental biology, Cell culture, 030220 oncology & carcinogenesis, Cancer research, Poly(ADP-ribose) Polymerases, Stem cell, Protein Binding, Developmental Biology

Abstract

Specific protein 1 (SP1) might act as a critical transcription regulator in myocardial infarction (MI), but little evidence about its function in regulating cardiac apoptosis, a major cause of MI development, has been revealed. This study tried to investigate the role of SP1 in MI and its interaction with poly-ADP-ribose polymerase (PARP)-1 by using SP1 inhibitor, mithramycin A (mithA). Primary mouse cardiomyocytes and commercial mouse cardiomyocytes were subjected to mithA treatment under hypoxia conditions, while cell viability, Nix promoter activity, and its expression were detected correspondingly. PARP overexpression and knockdown were conducted, respectively, in mithA-treated and SP1-overexpressing cells. Co-immunoprecipitation was used to verify the interaction between PARP and SP1. For in vivo experiments, mithA administration was performed after the injections of adenovirus for PARP overexpression, and then, MI introduction was carried out. Infarct size and lactate dehydrogenase level were measured to assess MI injury. SP1 inhibitor mithA attenuated hypoxia-induced decrease of cell viability and Nix transcriptional activation, which could be inhibited by PARP overexpression. Knockdown of PARP prevented SP1-induced transcription of Nix and cell viability change, and PARP showed direct interaction with SP1. Furthermore, mithA administration reduced MI injuries, while PARP overexpression could suppress the improvement. The cardioprotective role of SP1 inhibitor mithA was demonstrated here expanding the role of SP1 in MI development involving hypoxia-induced cardiac apoptosis. Moreover, PARP acted as a transcriptional coactivator in Nix transcription involving its interaction with SP1.

Published

2021

13. The antitumor antibiotic mithramycin: new advanced approaches in modification and production

Author

Renata Novakova, Dagmar Homerova, Beatrica Sevcikova, Jan Kormanec, Bronislava Rezuchova, Dominika Csolleiova, and Lubomira Feckova

Subjects

0303 health sciences, Antibiotics, Antineoplastic, biology, 030306 microbiology, Heterologous, Promoter, Plicamycin, Sarcoma, Ewing, General Medicine, Computational biology, biology.organism_classification, Applied Microbiology and Biotechnology, Streptomyces, Anti-Bacterial Agents, 03 medical and health sciences, Polyketide, Transcription (biology), Polyketides, Gene cluster, Humans, Heterologous expression, Transcription factor, 030304 developmental biology, Biotechnology

Abstract

The aureolic acid-type polyketide mithramycin (MTM) has a remarkable cytotoxicity against a variety of human tumors and has been used for the treatment of several types of cancer, including chronic and acute myeloid leukemia, testicular carcinoma, hypercalcemia, and Paget's disease. However, its clinical use is quite limited due to its toxicity. Recently, interest in MTM has been renewed after its identification as a top candidate for the inhibition of the aberrant fusion transcription factor EWS-FLI1, associated with malignant transformation and progression of Ewing sarcoma tumor family. The mechanism of MTM inhibition involves its reversible non-intercalative interaction with GC-rich DNA regions. As a result of this binding, MTM blocks binding of transcription factors (such as Sp1) to their GC-rich promoters and inhibits transcription of several proto-oncogenes and thus suppresses various types of cancer. Knowledge of the biosynthesis of MTM and its gene cluster has enabled genetic modifications of the gene cluster and combinatorial biosynthesis to produce new modified MTM molecules ("mithralogues") with improved efficacy and lower toxicity, which has also renewed interest in the clinical development of MTM. However, production yields of MTM and its analogues are low in the natural production strains. Recent developments in genetic engineering approaches have made it possible to increase MTM production through more rational strategies based on genetic manipulations and heterologous expression in optimized chassis. Recent construction of various genetically modified strains of Streptomyces lividans has shown their use for efficient heterologous production of various biologically active secondary metabolites including MTM. KEY POINTS: • Discovery a novel bifunctional glycosyl hydrolase from uncultured microorganism. • Heterologous production of MTM in engineered S. lividans strains is efficient.

Published

2020

14. Mithramycin selectively attenuates DNA-damage-induced neuronal cell death

Author

Bogdan A. Stoica, Ethan P. Glaser, Alan I. Faden, Brian M. Polster, Taryn G. Aubrecht, Boris Sabirzhanov, Rebecca J. Henry, and Oleg Makarevich

Subjects

Male, Cancer Research, Programmed cell death, Transcription, Genetic, DNA damage, Proto-Oncogene Proteins c-jun, Transcriptional regulatory elements, Immunology, Cell death in the nervous system, Apoptosis, Molecular neuroscience, Neuroprotection, Models, Biological, Article, Rats, Sprague-Dawley, Cellular and Molecular Neuroscience, Transactivation, Downregulation and upregulation, Brain Injuries, Traumatic, Animals, lcsh:QH573-671, Caspase, Etoposide, Neurons, biology, Cell Death, Chemistry, lcsh:Cytology, Intrinsic apoptosis, Cell Biology, Plicamycin, Cell biology, Mitochondria, Mice, Inbred C57BL, Neuroprotective Agents, biology.protein, Tumor Suppressor Protein p53, Chromatin immunoprecipitation, Biomarkers, DNA Damage, Signal Transduction

Abstract

DNA damage triggers cell death mechanisms contributing to neuronal loss and cognitive decline in neurological disorders, including traumatic brain injury (TBI), and as a side effect of chemotherapy. Mithramycin, which competitively targets chromatin-binding sites of specificity protein 1 (Sp1), was used to examine previously unexplored neuronal cell death regulatory mechanisms via rat primary neurons in vitro and after TBI in mice (males). In primary neurons exposed to DNA-damage-inducing chemotherapy drugs in vitro we showed that DNA breaks sequentially initiate DNA-damage responses, including phosphorylation of ATM, H2AX and tumor protein 53 (p53), transcriptional activation of pro-apoptotic BH3-only proteins, and mitochondrial outer membrane permeabilization (MOMP), activating caspase-dependent and caspase-independent intrinsic apoptosis. Mithramycin was highly neuroprotective in DNA-damage-dependent neuronal cell death, inhibiting chemotherapeutic-induced cell death cascades downstream of ATM and p53 phosphorylation/activation but upstream of p53-induced expression of pro-apoptotic molecules. Mithramycin reduced neuronal upregulation of BH3-only proteins and mitochondrial dysfunction, attenuated caspase-3/7 activation and caspase substrates’ cleavage, and limited c-Jun activation. Chromatin immunoprecipitation indicated that mithramycin attenuates Sp1 binding to pro-apoptotic gene promoters without altering p53 binding suggesting it acts by removing cofactors required for p53 transactivation. In contrast, the DNA-damage-independent neuronal death models displayed caspase initiation in the absence of p53/BH3 activation and were not protected even when mithramycin reduced caspase activation. Interestingly, experimental TBI triggers a multiplicity of neuronal death mechanisms. Although markers of DNA-damage/p53-dependent intrinsic apoptosis are detected acutely in the injured cortex and are attenuated by mithramycin, these processes may play a reduced role in early neuronal death after TBI, as caspase-dependent mechanisms are repressed in mature neurons while other, mithramycin-resistant mechanisms are active. Our data suggest that Sp1 is required for p53-mediated transactivation of neuronal pro-apoptotic molecules and that mithramycin may attenuate neuronal cell death in conditions predominantly involving DNA-damage-induced p53-dependent intrinsic apoptosis.

Published

2020

15. CDK9 Blockade Exploits Context-dependent Transcriptional Changes to Improve Activity and Limit Toxicity of Mithramycin for Ewing Sarcoma

Author

Joel H. Everett, Carleen Klumpp-Thomas, Elissa Boguslawski, Natasha J. Caplen, Scott E. Martin, Ian Beddows, Lee J. Helman, Sergey Dikalov, Brandon Oswald, Susan M. Kitchen-Goosen, Marie Adams, Zachary Madaj, Guillermo Flores, and Patrick J. Grohar

Subjects

0301 basic medicine, Cancer Research, Drug-Related Side Effects and Adverse Reactions, Mice, Nude, Apoptosis, Bone Neoplasms, RNA polymerase II, Sarcoma, Ewing, Article, Mice, 03 medical and health sciences, 0302 clinical medicine, Transcription (biology), Tumor Cells, Cultured, medicine, Animals, Humans, Cytotoxicity, Cell Proliferation, Antibiotics, Antineoplastic, BTG2, biology, Chemistry, Kinase, Plicamycin, medicine.disease, Cyclin-Dependent Kinase 9, Xenograft Model Antitumor Assays, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Toxicity, Cancer research, biology.protein, Female, Cyclin-dependent kinase 9, Sarcoma

Abstract

There is a need to develop novel approaches to improve the balance between efficacy and toxicity for transcription factor–targeted therapies. In this study, we exploit context-dependent differences in RNA polymerase II processivity as an approach to improve the activity and limit the toxicity of the EWS-FLI1–targeted small molecule, mithramycin, for Ewing sarcoma. The clinical activity of mithramycin for Ewing sarcoma is limited by off-target liver toxicity that restricts the serum concentration to levels insufficient to inhibit EWS-FLI1. In this study, we perform an siRNA screen of the druggable genome followed by a matrix drug screen to identify mithramycin potentiators and a synergistic “class” effect with cyclin-dependent kinase 9 (CDK9) inhibitors. These CDK9 inhibitors enhanced the mithramycin-mediated suppression of the EWS-FLI1 transcriptional program leading to a shift in the IC50 and striking regressions of Ewing sarcoma xenografts. To determine whether these compounds may also be liver protective, we performed a qPCR screen of all known liver toxicity genes in HepG2 cells to identify mithramycin-driven transcriptional changes that contribute to the liver toxicity. Mithramycin induces expression of the BTG2 gene in HepG2 but not Ewing sarcoma cells, which leads to a liver-specific accumulation of reactive oxygen species (ROS). siRNA silencing of BTG2 rescues the induction of ROS and the cytotoxicity of mithramycin in these cells. Furthermore, CDK9 inhibition blocked the induction of BTG2 to limit cytotoxicity in HepG2, but not Ewing sarcoma cells. These studies provide the basis for a synergistic and less toxic EWS-FLI1–targeted combination therapy for Ewing sarcoma.

Published

2020

16. Insight into mithramycin disruption of ETS transcription leads to improved understanding of more selective analogs

Author

Girma M. Woldemichael and Barry R. O'Keefe

Subjects

0303 health sciences, genetic structures, Base Sequence, Chemistry, fungi, 030302 biochemistry & molecular biology, Allosteric regulation, DNA, Plicamycin, Article, Cell biology, 03 medical and health sciences, Structural Biology, Transcription (biology), A-DNA, Enhancer, Molecular Biology, Transcription factor, Transcription Factors, 030304 developmental biology

Abstract

ETS family transcription factors of ERG and FLI1 play a key role in oncogenesis of prostate cancer and Ewing sarcoma by binding regulatory DNA sites and interfering with function of other factors. Mithramycin (MTM) is an anti-cancer, DNA binding natural product that functions as a potent antagonist of ERG and FLI1 by an unknown mechanism. We present a series of crystal structures of the DNA binding domain (DBD) of ERG/FLI1 culminating in a structure of a high-order complex of the ERG/FLI1 DBD, transcription factor Runx2, core binding factor beta (Cbfβ) and MTM on a DNA enhancer site, along with supporting DNA binding studies using MTM and its analogues. Taken together, these data provide insight into allosteric mechanisms underlying ERG and FLI1 transactions and their disruption by MTM analogues.

Published

2021

17. Everolimus and plicamycin specifically target chemoresistant colorectal cancer cells of the CMS4 subtype

Author

Deng, Jiayin, Tian, Ai-Ling, Pan, Hui, Sauvat, Allan, Leduc, Marion, Liu, Peng, Zhao, Liwei, Zhang, Shuai, Chen, Hui, Taly, Valérie, Laurent-Puig, Pierre, Senovilla, Laura, Li, Yingqiu, Kroemer, Guido, Kepp, Oliver, Sun Yat-Sen University [Guangzhou] (SYSU), Centre de Recherche des Cordeliers (CRC (UMR_S_1138 / U1138)), École pratique des hautes études (EPHE), Université Paris sciences et lettres (PSL)-Université Paris sciences et lettres (PSL)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Sorbonne Université (SU)-Université de Paris (UP), Université Paris-Sud - Paris 11 (UP11), Institut Gustave Roussy (IGR), Institut Universitaire de France (IUF), Ministère de l'Education nationale, de l’Enseignement supérieur et de la Recherche (M.E.N.E.S.R.), Universidad de Valladolid [Valladolid] (UVa), Cancer Research and Personalized Medicine - CARPEM [Paris], Institut National de la Santé et de la Recherche Médicale (INSERM)-Université Paris Descartes - Paris 5 (UPD5)-Hôpital Cochin [AP-HP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Hôpital Européen Georges Pompidou [APHP] (HEGP), Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Hôpitaux Universitaires Paris Ouest - Hôpitaux Universitaires Île de France Ouest (HUPO)-Hôpitaux Universitaires Paris Ouest - Hôpitaux Universitaires Île de France Ouest (HUPO)-CHU Necker - Enfants Malades [AP-HP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP), Chinese Academy of Medical Sciences [Jiangsu, P.R. China], Karolinska University Hospital [Stockholm], Shanghai Key Laboratory of Atmospheric Particle Pollution and Prevention (LAP3), Fudan University [Shanghai], China Scholarship Council, Institut National du Cancer (France), Ligue Nationale contre le Cancer (France), Agence Nationale de la Recherche (France), Fondation pour la Recherche Médicale, European Commission, Institut Universitaire de France, Fondation Leducq, TALY, Valerie, Université Paris sciences et lettres (PSL)-Université Paris sciences et lettres (PSL)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Sorbonne Université (SU)-Université Paris Cité (UPCité), Hôpital Européen Georges Pompidou [APHP] (HEGP), Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Hôpitaux Universitaires Paris Ouest - Hôpitaux Universitaires Île de France Ouest (HUPO)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Hôpitaux Universitaires Paris Ouest - Hôpitaux Universitaires Île de France Ouest (HUPO)-Hôpital Cochin [AP-HP], and Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Université Paris Descartes - Paris 5 (UPD5)-Institut National de la Santé et de la Recherche Médicale (INSERM)-CHU Necker - Enfants Malades [AP-HP]

Subjects

QH573-671, Cancer therapy, [SDV]Life Sciences [q-bio], Apoptosis, [SDV.CAN]Life Sciences [q-bio]/Cancer, Plicamycin, Article, [SDV] Life Sciences [q-bio], Cytoskeletal Proteins, Mice, Antineoplastic Combined Chemotherapy Protocols, Animals, Humans, Everolimus, Colorectal Neoplasms, Cytology, Adaptor Proteins, Signal Transducing, Cell Proliferation

Abstract

© The Author(s) 2021., Colorectal cancers (CRC) can be classified into four consensus molecular subtypes (CMS), among which CMS1 has the best prognosis, contrasting with CMS4 that has the worst outcome. CMS4 CRC is notoriously resistant against therapeutic interventions, as demonstrated by preclinical studies and retrospective clinical observations. Here, we report the finding that two clinically employed agents, everolimus (EVE) and plicamycin (PLI), efficiently target the prototypic CMS4 cell line MDST8. As compared to the prototypic CMS1 cell line LoVo, MDST8 cells treated with EVE or PLI demonstrated stronger cytostatic and cytotoxic effects, increased signs of apoptosis and autophagy, as well as a more pronounced inhibition of DNA-to-RNA transcription and RNA-to-protein translation. Moreover, nontoxic doses of EVE and PLI induced the shrinkage of MDST8 tumors in mice, yet had only minor tumor growth-reducing effects on LoVo tumors. Altogether, these results suggest that EVE and PLI should be evaluated for their clinical activity against CMS4 CRC., JD, A-LT, HP, SZ, and HC are supported by the China Scholarship Council. OK receives funding by the DIM ELICIT initiative of the Ile de France and Institut National du Cancer (INCa); GK, VT, and PLP are supported by the Ligue contre le Cancer (équipes labellisées, Program “Equipe labelisée LIGUE”; no. EL2016.LNCC (VT/PLP)); Agence National de la Recherche (ANR)—Projets blancs; ANR under the frame of E-Rare-2, the ERA-Net for Research on Rare Diseases; AMMICa US23/CNRS UMS3655; Association pour la recherche sur le cancer (ARC); Association “Le Cancer du Sein, Parlons-en!”; Cancéropôle Ile-de-France; Chancelerie des universités de Paris (Legs Poix), Fondation pour la Recherche Médicale (FRM); a donation by Elior; European Research Area Network on Cardiovascular Diseases (ERA-CVD, MINOTAUR); Gustave Roussy Odyssea, the European Union Horizon 2020 Project Oncobiome; Fondation Carrefour; INCa; Inserm (HTE); Institut Universitaire de France; LeDucq Foundation; the LabEx Immuno-Oncology (ANR-18-IDEX-0001); the RHU Torino Lumière; the Seerave Foundation; the SIRIC Stratified Oncology Cell DNA Repair and Tumor Immune Elimination (SOCRATE); and the SIRIC Cancer Research and Personalized Medicine (CARPEM).

Published

2021

18. Risk Factors for Esophageal Cancer, with an Emphasis on the Role of Specificity Protein Transcription Factors in Prognosis and Therapy

Author

Sohail Siraj, Riyaz Basha, Krishna Patel, Nuri Hamby, and Ananya Kurri

Subjects

Sp Transcription Factors, Cancer Research, Poor prognosis, Esophageal Neoplasms, Carcinogenesis, business.industry, Plicamycin, Esophageal cancer, Prognosis, medicine.disease, Metastasis, Tolfenamic acid, Risk Factors, Cancer cell, Cancer research, medicine, Humans, ortho-Aminobenzoates, business, Transcription factor, Gene, medicine.drug

Abstract

Specificity protein (Sp) transcription factors regulate the expression of genes associated with several cellular processes and play a critical role in early development. Typically, Sp protein expression decreases with age in healthy adults. Research has shown that Sp proteins can impact the development and transformation of cancer cells and other oncogenic processes, including survival, proliferation, spread, and metastasis. Among the Sp proteins, Sp1, Sp3, and Sp4 have been the main targets of study as they are shown to be highly expressed in cancer cells compared to healthy cells. Increased levels of Sp1 are correlated with poor prognosis in some malignancies, including gastrointestinal cancers. In this review, we discuss the role of Sp transcription factors and examine their activities as pro-oncogenic factors in esophageal cancer (EC). Other aspects presented in this review are potential therapeutic options for EC that target Sp1. We summarize the published information on preclinical results using mithramycin and tolfenamic acid.

Published

2020

19. Identification of plicamycin, TG02, panobinostat, lestaurtinib, and GDC-0084 as promising compounds for the treatment of central nervous system infections caused by the free-living amebae Naegleria, Acanthamoeba and Balamuthia

Author

Emily I. Chen, Gretchen M. Ehrenkaufer, Monica M. Kangussu-Marcolino, Upinder Singh, and Anjan Debnath

Subjects

0301 basic medicine, Cell Culture Techniques, Drug Evaluation, Preclinical, Acanthamoeba, Balamuthia, chemistry.chemical_compound, 0302 clinical medicine, Panobinostat, ReFRAME library, Pharmacology (medical), Enzyme Inhibitors, CNS infection, biology, Lestaurtinib, Meningoencephalitis, Amebiasis, Naegleria, Plicamycin, 3. Good health, Infectious Diseases, Drug screening, medicine.drug, 030231 tropical medicine, Antiprotozoal Agents, Carbazoles, Central Nervous System Protozoal Infections, Heterocyclic Compounds, 4 or More Rings, Article, Keratitis, Microbiology, lcsh:Infectious and parasitic diseases, Inhibitory Concentration 50, 03 medical and health sciences, Oxazines, parasitic diseases, medicine, lcsh:RC109-216, Furans, Pharmacology, Dose-Response Relationship, Drug, business.industry, medicine.disease, biology.organism_classification, Amoebozoa, Culture Media, Pyrimidines, 030104 developmental biology, chemistry, Parasitology, business

Abstract

The free-living amebae Naegleria, Acanthamoeba, and Balamuthia cause rare but life-threatening infections. All three parasites can cause meningoencephalitis. Acanthamoeba can also cause chronic keratitis and both Balamuthia and Acanthamoeba can cause skin and systemic infections. There are minimal drug development pipelines for these pathogens despite a lack of available treatment regimens and high fatality rates. To identify anti-amebic drugs, we screened 159 compounds from a high-value repurposed library against trophozoites of the three amebae. Our efforts identified 38 compounds with activity against at least one ameba. Multiple drugs that bind the ATP-binding pocket of mTOR and PI3K are active, highlighting these compounds as important inhibitors of these parasites. Importantly, 24 active compounds have progressed at least to phase II clinical studies and overall 15 compounds were active against all three amebae. Based on central nervous system (CNS) penetration or exceptional potency against one amebic species, we identified sixteen priority compounds for the treatment of meningoencephalitis caused by these pathogens. The top five compounds are (i) plicamycin, active against all three free-living amebae and previously U.S. Food and Drug Administration (FDA) approved, (ii) TG02, active against all three amebae, (iii and iv) FDA-approved panobinostat and FDA orphan drug lestaurtinib, both highly potent against Naegleria, and (v) GDC-0084, a CNS penetrant mTOR inhibitor, active against at least two of the three amebae. These results set the stage for further investigation of these clinically advanced compounds for treatment of infections caused by the free-living amebae, including treatment of the highly fatal meningoencephalitis., Graphical abstract Image 1, Highlights • Focused screen of ReFRAME library (159 compounds) on three free-living amebae. • 16 priority compounds selected based on potency, advanced clinical studies and CNS penetration. • Identified compounds with fast killing kinetics against Naegleria and Balamuthia. • Identified compounds capable of delaying Balamuthia trophozoite recrudescence. • 5 compounds of high interest for treatment of CNS infections with free-living amebae.

Published

2019

20. Mithramycin A Inhibits Colorectal Cancer Growth by Targeting Cancer Stem Cells

Author

Shyam S. Mohapatra, Sandhyabanu Katiri, Ryan Green, Waise Quarni, Bhaumik B. Patel, Subhra Mohapatra, and Rinku Dutta

Subjects

0301 basic medicine, Colorectal cancer, lcsh:Medicine, Antineoplastic Agents, Tumor initiation, Article, Metastasis, 03 medical and health sciences, 0302 clinical medicine, Cancer stem cell, Cell Line, Tumor, medicine, Animals, Humans, lcsh:Science, Cell Proliferation, Multidisciplinary, business.industry, Cancer stem cells, lcsh:R, Cancer, Plicamycin, medicine.disease, HCT116 Cells, 3. Good health, Colon cancer, Mice, Inbred C57BL, 030104 developmental biology, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, Neoplastic Stem Cells, lcsh:Q, Stem cell, business, Colorectal Neoplasms, HT29 Cells, Ex vivo

Abstract

The pivotal role of cancer initiating stem cells (CSCs) in tumor initiation, growth, metastasis and drug resistance has led to the postulation of a ‘total cancer therapy’ paradigm, which involves targeting both cancer cells and CSCs for effective therapy. However, the progress in identifying drugs for total cancer therapy has been limited. Herein, we show for the first time that mithramycin A (Mit-A) can successfully inhibit CSC proliferation, in addition to inhibiting bulk cancer cells in a model of colorectal cancer (CRC), the second leading cause of death among men and women in the United States. To this end, a polymeric nanofiber scaffold culture system was established to develop 3D tumor organoids (tumoroids) from CRC cell lines such as HT29, HCT116, KM12, CT26 and MC38 as well as ex vivo mouse tumors. These tumoroids possessed increased expression of CSC markers and transcription factors, expanded the number of CSCs in culture and increased CSC functional properties measured by aldehyde dehydrogenase activity. Screening of an NCI library of FDA approved drugs led to the identification of Mit-A as a potential total cancer therapy drug. In both sphere and tumoroid culture, Mit-A inhibits cancer growth by reducing the expression of cancer stemness markers. In addition, Mit-A inhibits the expression of SP1, a previously known target in CRCs. Moreover, Mit-A significantly reduces growth of tumoroids in ex vivo cultures and CRC tumor growth in vivo. Finally, a dose-dependent treatment on CRC cells indicate that Mit-A significantly induces the cell death and PARP-cleavage of both CSC and non-CSC cells. Taken together the results of these in vitro, ex vivo and in vivo studies lead to the inference that Mit-A is a promising drug candidate for total cancer therapy of CRCs.

Published

2019

21. Cyclin-dependent kinase 1 and survivin as potential therapeutic targets against nasal natural killer/T-cell lymphoma

Author

Toshihiro Nagato, Miki Takahara, Shohei Harabuchi, Kan Kishibe, Seigo Ueda, Takumi Kumai, Michele Bernasconi, Kenzo Ohara, Yui Hirata-Nozaki, Hiroya Kobayashi, Yasuaki Harabuchi, Yuki Komabayashi, David Nadal, Takayuki Ohkuri, and Ryusuke Hayashi

Subjects

Male, 0301 basic medicine, Survivin, Nose Neoplasms, Mice, SCID, Biology, Lymphoma, T-Cell, Pathology and Forensic Medicine, Viral Matrix Proteins, 03 medical and health sciences, 0302 clinical medicine, Downregulation and upregulation, Mice, Inbred NOD, Cell Line, Tumor, Antineoplastic Combined Chemotherapy Protocols, CDC2 Protein Kinase, medicine, Animals, Humans, Molecular Biology, Mice, Knockout, Gene knockdown, Cyclin-dependent kinase 1, Kinase, Plicamycin, Cell Biology, Middle Aged, Natural killer T cell, medicine.disease, Xenograft Model Antitumor Assays, Lymphoma, Killer Cells, Natural, 030104 developmental biology, Cell culture, 030220 oncology & carcinogenesis, Cancer research, Female, RNA Interference, biological phenomena, cell phenomena, and immunity

Abstract

Nasal natural killer/T-cell lymphoma (NNKTL) is closely associated with Epstein-Barr virus (EBV) and is characterized by poor prognosis, resulting from rapid progression of lesions in the affected organs. Recent data have shown that NNKTL is associated with the aberrant expression of cyclin-dependent kinase 1 (CDK1) and its downstream target survivin, but little is known about the functional roles of CDK1 and survivin in NNKTL. In the current study, we show that knockdown of the EBV-encoded oncoprotein latent membrane protein 1 (LMP1) induces downregulation of CDK1 and survivin in NNKTL cells. Immunohistochemistry detected CDK1 and survivin expression in LMP1-positive cells of NNKTL biopsy specimens. Inhibition of CDK1 and survivin in NNKTL cells with several inhibitors led to a dose-dependent decrease in cell proliferation. In addition, the Sp1 inhibitor mithramycin, which can downregulate both CDK1 and survivin, significantly suppressed the growth of established NNKTL in a murine xenograft model. Our results suggest that LMP1 upregulation of CDK1 and survivin may be essential for NNKTL progression. Furthermore, targeting CDK1 and survivin with Sp1 inhibitors such as mithramycin may be an effective approach to treat NNKTL, which is considered to be a treatment-refractory lymphoma.

Published

2019

22. Mithramycin delivery systems to develop effective therapies in sarcomas

Author

Pilar Clemente-Casares, Francisco Morís, Aitana Vallina-Álvarez, Aida Rodríguez, Verónica Blanco-Lorenzo, Juan Tornin, Oscar Estupiñan, Iván Bravo, Borja Gallego, Carlos Alonso-Moreno, Enrique Niza, M. Victoria Gonzalez, Mar Rodríguez-Santamaría, Daniel Hermida-Merino, Alberto Ocaña, Veronica Rey, Rene Rodriguez, Universitat Politècnica de Catalunya. Departament de Ciència i Enginyeria de Materials, Universitat Politècnica de Catalunya. BBT - Biomaterials, Biomecànica i Enginyeria de Teixits, and Instituto de Investigación Sanitaria del Principado de Asturias

Subjects

Oncologia, Drug Compounding, Polyesters, Biomedical Engineering, Chondrosarcoma, Pharmaceutical Science, Medicine (miscellaneous), Mice, Nude, Bioengineering, Antineoplastic Agents, Pharmacology, Polylactide, Applied Microbiology and Biotechnology, Undifferentiated Pleomorphic Sarcoma, Medicaments antineoplàstics, Polymeric nanoparticles, Mice, Therapeutic index, Mithramycin, Antineoplastic agents, medicine, Medical technology, Animals, Humans, R855-855.5, Liposome, Soft tissue sarcoma, Chemistry, Cancer stem cells, Research, Enginyeria biomèdica [Àrees temàtiques de la UPC], In vitro toxicology, Sarcoma, Hydrogels, Plicamycin, medicine.disease, Anti-Bacterial Agents, Self-healing hydrogels, Liposomes, Molecular Medicine, Nanoparticles, Female, Nanocarriers, TP248.13-248.65, Small unilamellar vesicles liposomes, Biotechnology

Abstract

Background Sarcomas comprise a group of aggressive malignancies with very little treatment options beyond standard chemotherapy. Reposition of approved drugs represents an attractive approach to identify effective therapeutic compounds. One example is mithramycin (MTM), a natural antibiotic which has demonstrated a strong antitumour activity in several tumour types, including sarcomas. However, its widespread use in the clinic was limited by its poor toxicity profile. Results In order to improve the therapeutic index of MTM, we have loaded MTM into newly developed nanocarrier formulations. First, polylactide (PLA) polymeric nanoparticles (NPs) were generated by nanoprecipitation. Also, liposomes (LIP) were prepared by ethanol injection and evaporation solvent method. Finally, MTM-loaded hydrogels (HG) were obtained by passive loading using a urea derivative non-peptidic hydrogelator. MTM-loaded NPs and LIP display optimal hydrodynamic radii between 80 and 105 nm with a very low polydispersity index (PdI) and encapsulation efficiencies (EE) of 92 and 30%, respectively. All formulations show a high stability and different release rates ranging from a fast release in HG (100% after 30 min) to more sustained release from NPs (100% after 24 h) and LIP (40% after 48 h). In vitro assays confirmed that all assayed MTM formulations retain the cytotoxic, anti-invasive and anti-stemness potential of free MTM in models of myxoid liposarcoma, undifferentiated pleomorphic sarcoma and chondrosarcoma. In addition, whole genome transcriptomic analysis evidenced the ability of MTM, both free and encapsulated, to act as a multi-repressor of several tumour-promoting pathways at once. Importantly, the treatment of mice bearing sarcoma xenografts showed that encapsulated MTM exhibited enhanced therapeutic effects and was better tolerated than free MTM. Conclusions Overall, these novel formulations may represent an efficient and safer MTM-delivering alternative for sarcoma treatment. Graphical abstract

Published

2021

23. Mithramycin suppresses tumor growth by regulating CD47 and PD-L1 expression

Author

Jianhua Gong, Yuying Ji, Xiujun Liu, Yanbo Zheng, and Yongsu Zhen

Subjects

Pharmacology, Antibiotics, Antineoplastic, Dose-Response Relationship, Drug, THP-1 Cells, Melanoma, Experimental, Gene Expression, CD47 Antigen, Plicamycin, Biochemistry, Xenograft Model Antitumor Assays, B7-H1 Antigen, Mice, Inbred C57BL, Mice, Animals, Humans, Female

Abstract

Mithramycin A (MIT) has reacquired extensive research attention due to its anti-solid tumor activity and improved pharmacological production. Mechanismly, MIT was broadly used as a c-Myc inhibitor, and c-Myc regulated CD47 and PD-L1 expression which has been demonstrated. However, how MIT affects immune check-point molecules remains unknown. In this study, we found CD47 expression was higher in melanoma of pan-tissue array. MIT inhibited CD47 expression both in mRNA and protein level in melanoma cells (SK-MEL-28 and B16). MIT inhibited c-Myc, Sp-1 and CD47 expression in a concentration-dependent way. MIT inhibited the surface CD47 expression and promoted the phagocytosis of SK-MEL-28 cells by THP-1 cells. We found MIT inhibited tumor growth in melanoma allograft mice and CD47 expression in tumor mass. We also found MIT upregulated PD-L1 expression in cancer cells possibly via inhibiting PD-L1 ubiquitination, increasing ROS and IFN-γ. Combination of MIT and anti-PD-1 antibody showed enhanced antitumor activity compared to MIT and anti-PD-1 antibody alone in MC38 allograft mice. Using immune checkpoint array we found MIT inhibited expression of FasL and Galectin3. These results suggest that MIT inhibits CD47 expression, while improves PD-L1 expression. Furthermore, the combination of MIT and anti-PD-1 antibody exerts potent antitumor effect.

Published

2021

24. Combination Therapy of Mithramycin A and Immune Checkpoint Inhibitor for the Treatment of Colorectal Cancer in an Orthotopic Murine Model

Author

Rinku Dutta, Roukiah Khalil, Karthick Mayilsamy, Ryan Green, Mark Howell, Srinivas Bharadwaj, Shyam S. Mohapatra, and Subhra Mohapatra

Subjects

0301 basic medicine, PD-L1, orthotopic tumor, Combination therapy, Mithramycin-A, T cell, Immunology, Cell, colorectal cancer, combination therapy, 03 medical and health sciences, Mice, 0302 clinical medicine, Immune system, Cancer stem cell, Antineoplastic Combined Chemotherapy Protocols, medicine, Immunology and Allergy, Animals, Immune Checkpoint Inhibitors, Original Research, Tumor microenvironment, biology, business.industry, Plicamycin, RC581-607, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, biology.protein, Cancer research, Female, Immunologic diseases. Allergy, business, Colorectal Neoplasms, CD8

Abstract

The axis of Programmed cell death-1 receptor (PD-1) with its ligand (PD-L1) plays a critical role in colorectal cancer (CRC) in escaping immune surveillance, and blocking this axis has been found to be effective in a subset of patients. Although blocking PD-L1 has been shown to be effective in 5–10% of patients, the majority of the cohorts show resistance to this checkpoint blockade (CB) therapy. Multiple factors assist in the growth of resistance to CB, among which T cell exhaustion and immunosuppressive effects of immune cells in the tumor microenvironment (TME) play a critical role along with other tumor intrinsic factors. We have previously shown the polyketide antibiotic, Mithramycin-A (Mit-A), an effective agent in killing cancer stem cells (CSCs) in vitro and in vivo in a subcutaneous murine model. Since TME plays a pivotal role in CB therapy, we tested the immunomodulatory efficacy of Mit-A with anti-PD-L1 mAb (αPD-L1) combination therapy in an immunocompetent MC38 syngeneic orthotopic CRC mouse model. Tumors and spleens were analyzed by flow cytometry for the distinct immune cell populations affected by the treatment, in addition to RT-PCR for tumor samples. We demonstrated the combination treatment decreases tumor growth, thus increasing the effectiveness of the CB. Mit-A in the presence of αPD-L1 significantly increased CD8+ T cell infiltration and decreased immunosuppressive granulocytic myeloid-derived suppressor cells and anti-inflammatory macrophages in the TME. Our results revealed Mit-A in combination with αPD-L1 has the potential for augmented CB therapy by turning an immunologically “cold” into “hot” TME in CRC.

Published

2021

25. Inhibition of the c-Myc Oncogene by the Aureolic Acid Group Antibiotics

Author

A K, Isagulieva, N V, Soshnikova, and A A, Shtil

Subjects

Plicamycin

Abstract

GC-rich stretches in the DNA minor groove are the established intracellular targets for the aureolic acid group of antibiotics such as olivomycin A and its semisynthetic analogue olivamide. We demonstrated here that both antibiotics at nanomolar concentrations inhibited transcription of the c-Myc oncogene in cultured human tumor cells. The mechanism of transcriptional inhibition did not require the full-length binding site for Sp1, a GC-dependent transcriptional factor. GC quartets with the nucleotide sequences optimal for drug binding are sufficient for c-Myc transcriptional block by the aureolic acid derivatives.

Published

2021

26. Molecules against Covid-19: An in silico approach for drug development

Author

Rhythm Bharti and Sandeep Kumar Shukla

Subjects

Computer Networks and Communications, 020209 energy, In silico, viruses, Drug repurposing, 02 engineering and technology, Natural therapeutics, Article, 0202 electrical engineering, electronic engineering, information engineering, medicine, Electrical and Electronic Engineering, ADME, Plicamycin, Chemistry, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), RNA-Dependent RNA polymerase (RdRp), RNA, 021001 nanoscience & nanotechnology, Coronavirus disease 2019 (COVID-19), Drug repositioning, Drug development, Biochemistry, Homoharringtonine, Signal Processing, Molecular docking, Lipinski's rule of five, 0210 nano-technology, medicine.drug

Abstract

A large number of deaths have been caused by the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) worldwide, turning it into a serious and momentous threat to public health. This study tends to contribute to the development of effective treatment strategies through a computational approach, investigating the mechanisms in relation to the binding and subsequent inhibition of SARS-CoV-2 ribonucleic acid (RNA)-dependent RNA polymerase (RdRp). Molecular docking was performed to screen six naturally occurring molecules with antineoplastic properties (Ellipticine, Ecteinascidin, Homoharringtonine, Dolastatin 10, Halichondrin, and Plicamycin). Absorption, distribution, metabolism, and excretion (ADME) investigation was also conducted to analyze the drug-like properties of these compounds. The docked results have clearly shown binding of ligands to the SARS-CoV-2 RdRp protein. Interestingly, all ligands were found to obey Lipinski’s rule of five. These results provide a basis for repurposing and using molecules, derived from plants and animals, as a potential treatment for the coronavirus disease 2019 (COVID-19) infection as they could be effective therapeutics for the same., Graphical abstract Image 1

Published

2021

27. Bacteria as a treasure house of secondary metabolites with anticancer potential

Author

Ragi Jadimurthy, Chakrabhavi Dhananjaya Mohan, Shobith Rangappa, Manoj Garg, Lingzhi Wang, S. Chandra Nayak, Gautam Sethi, and Kanchugarakoppal S. Rangappa

Subjects

0301 basic medicine, Cancer Research, Bryostatin 1, Rebeccamycin, Antineoplastic Agents, Biology, Pharmacology, Romidepsin, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Neoplasms, medicine, Pentostatin, Humans, Biological Products, Plicamycin, Bacteria, Drug discovery, Chartreusin, Ixabepilone, Fungi, 030104 developmental biology, chemistry, 030220 oncology & carcinogenesis, medicine.drug

Abstract

Cancer stands in the frontline among leading killers worldwide and the annual mortality rate is expected to reach 16.4 million by 2040. Humans suffer from about 200 different types of cancers and many of them have a small number of approved therapeutic agents. Moreover, several types of major cancers are diagnosed at advanced stages as a result of which the existing therapies have limited efficacy against them and contribute to a dismal prognosis. Therefore, it is essential to develop novel potent anticancer agents to counteract cancer-driven lethality. Natural sources such as bacteria, plants, fungi, and marine microorganisms have been serving as an inexhaustible source of anticancer agents. Notably, over 13,000 natural compounds endowed with different pharmacological properties have been isolated from different bacterial sources. In the present article, we have discussed about the importance of natural products, with special emphasis on bacterial metabolites for cancer therapy. Subsequently, we have comprehensively discussed the various sources, mechanisms of action, toxicity issues, and off-target effects of clinically used anticancer drugs (such as actinomycin D, bleomycin, carfilzomib, doxorubicin, ixabepilone, mitomycin C, pentostatin, rapalogs, and romidepsin) that have been derived from different bacteria. Furthermore, we have also discussed some of the major secondary metabolites (antimycins, chartreusin, elsamicins, geldanamycin, monensin, plicamycin, prodigiosin, rebeccamycin, salinomycin, and salinosporamide) that are currently in the clinical trials or which have demonstrated potent anticancer activity in preclinical models. Besides, we have elaborated on the application of metagenomics in drug discovery and briefly described about anticancer agents (bryostatin 1 and ET-743) identified through the metagenomics approach.

Published

2021

28. Mithramycin 2′-Oximes with Improved Selectivity, Pharmacokinetics, and Ewing Sarcoma Antitumor Efficacy

Author

Khaled A. Shaaban, Yinan Zhang, Jianjun Zhang, Zheng Cui, Jürgen Rohr, Steven G. Van Lanen, Yang Liu, Reiya Hayden, Jon S. Thorson, Joseph M. Eckenrode, Larissa V. Ponomareva, Oleg V. Tsodikov, Annet Kyomuhangi, and Markos Leggas

Subjects

Apoptosis, Bone Neoplasms, Mice, SCID, Sarcoma, Ewing, 01 natural sciences, Article, 03 medical and health sciences, Mice, Pharmacokinetics, In vivo, Drug Discovery, Oximes, Tumor Cells, Cultured, Animals, Humans, Luciferase, Tissue Distribution, Cytotoxicity, Transcription factor, 030304 developmental biology, Cell Proliferation, 0303 health sciences, Antibiotics, Antineoplastic, Chemistry, Cell growth, Plicamycin, Xenograft Model Antitumor Assays, In vitro, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Cancer research, Molecular Medicine, Female, Conjugate

Abstract

Mithramycin A (MTM) inhibits the oncogenic transcription factor EWS-FLI1 in Ewing sarcoma, but poor pharmacokinetics (PK) and toxicity limit its clinical use. To address this limitation, we report an efficient MTM 2′-oxime (MTM(ox)) conjugation strategy for rapid MTM diversification. Comparative cytotoxicity assays of 41 MTM(ox) analogues using E-twenty-six (ETS) fusion-dependent and ETS fusion-independent cancer cell lines revealed improved ETS fusion-independent/dependent selectivity indices for select 2′-conjugated analogues as compared to MTM. Luciferase-based reporter assays demonstrated target engagement at low nM concentrations, and molecular assays revealed that analogues inhibit the transcriptional activity of EWS-FLI1. These in vitro screens identified MTM(ox)32E (a Phe–Trp dipeptide-based 2′-conjugate) for in vivo testing. Relative to MTM, MTM(ox)32E displayed an 11-fold increase in plasma exposure and improved efficacy in an Ewing sarcoma xenograft. Importantly, these studies are the first to point to simple C3 aliphatic side-chain modification of MTM as an effective strategy to improve PK.

Published

2020

29. Large-Scale Drug Screening in Patient-Derived IDHmut Glioma Stem Cells Identifies Several Efficient Drugs among FDA-Approved Antineoplastic Agents

Author

Rolf Warta, Gerhard Jungwirth, Andreas Unterberg, Philip Dao Trong, Tao Yu, Stefan Pusch, and Christel Herold-Mende

Subjects

Drug, Daunorubicin, media_common.quotation_subject, lower grade glioma, doxorubicin, drug screen, chemistry.chemical_compound, isocitrate dehydrogenase (IDH) mutant glioma stem cells, Glioma, medicine, Propidium iodide, IC50, lcsh:QH301-705.5, media_common, Plicamycin, carfilzomib, Bortezomib, business.industry, plicamycin, bortezomib, General Medicine, medicine.disease, omacetaxine, Carfilzomib, epirubicin, chemistry, daunorubicin, lcsh:Biology (General), Cancer research, business, medicine.drug

Abstract

The discovery of the isocitrate dehydrogenase (IDH) mutation in glioma led to a paradigm shift on how we see glioma biology. Difficulties in cultivating IDH mutant glioma stem cells (IDHmut GSCs) resulted in a paucity of preclinical models in IDHmut glioma, limiting the discovery of new effective chemotherapeutic agents. To fill this gap, we used six recently developed patient-derived IDHmut GSC lines and performed a large-scale drug screening with 147 Food and Drug Administration (FDA)-approved anticancer drugs. GSCs were subjected to the test compounds for 72 h in concentrations ranging from 0.0001 to 1 &micro, M. Cell viability was assessed by CellTiterGlo and the induction of apoptosis by flow cytometry with Annexin V/propidium iodide staining. The initial screen was performed with two IDHmut GSC lines and identified seven drugs (bortezomib, carfilzomib, daunorubicin, doxorubicin, epirubicin, omacetaxine, plicamycin) with a substantial antiproliferative activity, as reflected by half maximal inhibitory concentrations (IC50) below 1 &micro, M and maximum inhibitory effects (Emax) below 25%. These findings were validated in an additional four IDHmut GSC lines. The candidate drugs, of which plicamycin and omacetaxine are known to cross the blood brain barrier, were used for subsequent cell death analyses. A significant induction of apoptosis was observed at IC50 values of the respective drugs. In summary, we were able to identify seven FDA-approved drugs that should be further taken into clinical investigations for the treatment of IDHmut gliomas.

Published

2020

30. Large-Scale Drug Screening in Patient-Derived IDH

Author

Philip, Dao Trong, Gerhard, Jungwirth, Tao, Yu, Stefan, Pusch, Andreas, Unterberg, Christel, Herold-Mende, and Rolf, Warta

Subjects

lower grade glioma, Antineoplastic Agents, doxorubicin, Article, drug screen, Inhibitory Concentration 50, isocitrate dehydrogenase (IDH) mutant glioma stem cells, Cell Line, Tumor, Humans, Annexin A5, Drug Approval, Cell Proliferation, carfilzomib, Cell Death, Dose-Response Relationship, Drug, Brain Neoplasms, United States Food and Drug Administration, plicamycin, bortezomib, Reproducibility of Results, Glioma, omacetaxine, epirubicin, Isocitrate Dehydrogenase, United States, daunorubicin, Mutation, Neoplastic Stem Cells, Drug Screening Assays, Antitumor, Propidium

Abstract

The discovery of the isocitrate dehydrogenase (IDH) mutation in glioma led to a paradigm shift on how we see glioma biology. Difficulties in cultivating IDH mutant glioma stem cells (IDHmut GSCs) resulted in a paucity of preclinical models in IDHmut glioma, limiting the discovery of new effective chemotherapeutic agents. To fill this gap, we used six recently developed patient-derived IDHmut GSC lines and performed a large-scale drug screening with 147 Food and Drug Administration (FDA)-approved anticancer drugs. GSCs were subjected to the test compounds for 72 h in concentrations ranging from 0.0001 to 1 µM. Cell viability was assessed by CellTiterGlo and the induction of apoptosis by flow cytometry with Annexin V/propidium iodide staining. The initial screen was performed with two IDHmut GSC lines and identified seven drugs (bortezomib, carfilzomib, daunorubicin, doxorubicin, epirubicin, omacetaxine, plicamycin) with a substantial antiproliferative activity, as reflected by half maximal inhibitory concentrations (IC50) below 1 µM and maximum inhibitory effects (Emax) below 25%. These findings were validated in an additional four IDHmut GSC lines. The candidate drugs, of which plicamycin and omacetaxine are known to cross the blood brain barrier, were used for subsequent cell death analyses. A significant induction of apoptosis was observed at IC50 values of the respective drugs. In summary, we were able to identify seven FDA-approved drugs that should be further taken into clinical investigations for the treatment of IDHmut gliomas.

Published

2020

31. Mithramycin induces promoter reprogramming and differentiation of rhabdoid tumor

Author

Katie M. Sorensen, Min H. Kang, Bart O. Williams, Lyong Heo, Patrick J. Grohar, Timothy J. Triche, Jessica E Rosien, C. Patrick Reynolds, Maggie H. Chasse, Zachary Madaj, Gabrielle E. Foxa, Benjamin K. Johnson, Ian Beddows, Elissa Boguslawski, and Susan M. Kitchen-Goosen

Subjects

0301 basic medicine, Medicine (General), DNA damage, Chromosomal Proteins, Non-Histone, Cellular differentiation, Biology, QH426-470, Chromatin, Epigenetics, Genomics & Functional Genomics, Chromatin remodeling, Article, 03 medical and health sciences, Mice, 0302 clinical medicine, R5-920, Genetics, Animals, Humans, Epigenetics, SMARCB1, Rhabdoid Tumor, Cancer, epigenetics, mithramycin, Cell Differentiation, Plicamycin, Articles, Pediatric cancer, SWI/SNF, Chromatin, pediatric cancer, 030104 developmental biology, Cancer research, Molecular Medicine, EC8042, 030217 neurology & neurosurgery, Transcription Factors

Abstract

Rhabdoid tumor (RT) is a pediatric cancer characterized by the inactivation of SMARCB1, a subunit of the SWI/SNF chromatin remodeling complex. Although this deletion is the known oncogenic driver, there are limited effective therapeutic options for these patients. Here we use unbiased screening of cell line panels to identify a heightened sensitivity of rhabdoid tumor to mithramycin and the second‐generation analogue EC8042. The sensitivity of MMA and EC8042 was superior to traditional DNA damaging agents and linked to the causative mutation of the tumor, SMARCB1 deletion. Mithramycin blocks SMARCB1‐deficient SWI/SNF activity and displaces the complex from chromatin to cause an increase in H3K27me3. This triggers chromatin remodeling and enrichment of H3K27ac at chromHMM‐defined promoters to restore cellular differentiation. These effects occurred at concentrations not associated with DNA damage and were not due to global chromatin remodeling or widespread gene expression changes. Importantly, a single 3‐day infusion of EC8042 caused dramatic regressions of RT xenografts, recapitulated the increase in H3K27me3, and cellular differentiation described in vitro to completely cure three out of eight mice., EC8042 is identified as an inhibitor of oncogenic SWI/SNF and a promising therapeutic candidate for rhabdoid tumor. The mechanism of target inhibition is elucidated and used to optimize compound administration, characterize an associated biomarker, and cure mice bearing rhabdoid tumor xenografts.

Published

2020

32. DNMT1 and Sp1 competitively regulate the expression of BACE1 in A2E-mediated photo-oxidative damage in RPE cells

Author

Peirong Huang, Xiaodong Sun, Xueting Luo, Qing Gu, Fenghua Wang, Hong Zhu, Junran Sun, Xiangjun Sun, and Te Liu

Subjects

DNA (Cytosine-5-)-Methyltransferase 1, 0301 basic medicine, Sp1 Transcription Factor, Gene Expression, Retinal Pigment Epithelium, DNA methyltransferase, Cell Line, Retinoids, 03 medical and health sciences, Cellular and Molecular Neuroscience, Transcription (biology), mental disorders, Aspartic Acid Endopeptidases, Humans, Binding site, Sp1 transcription factor, Amyloid beta-Peptides, Base Sequence, Dose-Response Relationship, Drug, Chemistry, Promoter, Plicamycin, Cell Biology, Cell biology, Oxidative Stress, 030104 developmental biology, DNA methylation, DNMT1, sense organs, Amyloid Precursor Protein Secretases, Retinal Pigments, Chromatin immunoprecipitation, Photic Stimulation, Protein Binding

Abstract

Numerous studies have focused on the deteriorate role of amyloid-β (Aβ) on retina, implying the potential pathogenic mechanism underlying age-related macular degeneration (AMD). However, the mechanism underlying the Aβ deposition in AMD patients remains unknown. Beta-site amyloid precursor protein-cleaving enzyme 1 (BACE1), rate-limiting enzyme for Aβ production, plays an important role in Aβ deposition in the brain. In the current study, we aimed to clarify the regulation mechanism of BACE1 and explore potential drug targets using a lipofuscinfluorophore A2E-mediated photo-oxidation model. In this model, Aβ1-40 and Aβ1-42 levels increased simultaneously with the enhanced BACE1 expression. These changes were associated with the hypomethylation of specific loci within the BACE1 gene promoter and the decreased levels of DNA methyltransferase 1 (DNMT1). Furthermore, we noticed overlapping regions of differentially methylated CpG islands and specificity protein (Sp1) binding sites within the BACE1 promoter. We employed chromatin immunoprecipitation (ChIP) assay to verify that the decreased BACE1 promoter methylation by DNMT1 enabled increased binding between Sp1 and the BACE1 promoter, which further enhanced BACE1 transcription. The inhibition of Sp1 with mithramycin A (MTM) could down-regulate the expression of BACE1 as well as alleviate the RPE barrier morphology and function impairment. Our results for the first time show the competitive regulation of BACE1 by transcription factor Sp1 and DNMT1 after photo-oxidation and confirm the potential novel protective role of MTM on RPE cells.

Published

2018

33. An efficient blue-white screening system for markerless deletions and stable integrations in Streptomyces chromosomes based on the blue pigment indigoidine biosynthetic gene bpsA

Author

Jesus Cortes, Beatrica Sevcikova, Jan Kormanec, Ludovit Skultety, Lubomira Feckova, Dagmar Homerova, Bronislava Rezuchova, Luz Elena Núñez, and Renata Novakova

Subjects

DNA, Bacterial, Genetic Markers, 0301 basic medicine, Anthraquinones, Applied Microbiology and Biotechnology, Streptomyces, Actinorhodin, Industrial Microbiology, 03 medical and health sciences, chemistry.chemical_compound, Plasmid, Bacterial Proteins, Blue white screen, Gene cluster, Multiple cloning site, Amino Acid Sequence, Piperidones, Reporter gene, biology, Gene Expression Regulation, Bacterial, Plicamycin, General Medicine, Chromosomes, Bacterial, biology.organism_classification, 030104 developmental biology, Biochemistry, chemistry, Genes, Bacterial, Multigene Family, Streptomyces lividans, mCherry, Gene Deletion, Plasmids, Biotechnology

Abstract

We previously developed an efficient deletion system for streptomycetes based on the positive selection of double-crossover events using bpsA, a gene for producing the blue pigment indigoidine. Using this system, we removed interfering secondary metabolite clusters from Streptomyces lividans TK24, resulting in RedStrep strains with dramatically increased heterologous production of mithramycin A (up to 3-g/l culture). This system, however, required a time-consuming step to remove the resistance marker genes. In order to simplify markerless deletions, we prepared a new system based on the plasmid pAMR18A. This plasmid contains a large polylinker with many unique restriction sites flanked by apramycin and kanamycin resistance genes and the bpsA gene for selecting a double-crossover event. The utility of this new markerless deletion system was demonstrated by its deletion of a 21-kb actinorhodin gene cluster from Streptomyces lividans TK24 with 30% efficiency. We used this system to efficiently remove the matA and matB genes in selected RedStrep strains, resulting in biotechnologically improved strains with a highly dispersed growth phenotype involving non-pelleting small and open mycelia. No further increase in mithramycin A production was observed in these new RedStrep strains, however. We also used this system for the markerless insertion of a heterologous mCherry gene, an improved variant of the monomeric red fluorescent protein, under the control of the strong secretory signal sequence of the subtilisin inhibitor protein, into the chromosome of S. lividans TK24. The resulting recombinant strains efficiently secreted mCherry into the growth medium in a yield of 30 mg/l.

Published

2018

34. Development of Mithramycin Analogues with Increased Selectivity toward ETS Transcription Factor Expressing Cancers

Author

Shaimaa M. Salem, Amit Kumar Jha, Joseph M. Eckenrode, Jürgen Rohr, Abhisek Mandal, Prithiba Mitra, and Markos Leggas

Subjects

Male, Oncogene Proteins, Fusion, Antineoplastic Agents, Bone Neoplasms, Peptide, Sarcoma, Ewing, 01 natural sciences, Article, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Drug Development, Transcription (biology), Drug Discovery, Tumor Cells, Cultured, Humans, Cytotoxicity, Transcription factor, Cell Proliferation, Regulation of gene expression, chemistry.chemical_classification, Antibiotics, Antineoplastic, Dipeptide, Molecular Structure, Proto-Oncogene Proteins c-ets, Proto-Oncogene Protein c-fli-1, 010405 organic chemistry, ETS transcription factor family, Prostatic Neoplasms, Plicamycin, 0104 chemical sciences, Gene Expression Regulation, Neoplastic, chemistry, Cell culture, 030220 oncology & carcinogenesis, Cancer research, Molecular Medicine, RNA-Binding Protein EWS

Abstract

Mithramycin A (1) was identified as the top potential inhibitor of the aberrant ETS transcription factor EWS-FLI1, which causes Ewing sarcoma. Unfortunately, 1 has a narrow therapeutic window, compelling us to seek less toxic and more selective analogues. Here, we used MTMSA (2) to generate analogues via peptide coupling and fragment-based drug development strategies. Cytotoxicity assays in ETS and non-ETS dependent cell lines identified two dipeptide analogues, 60 and 61, with 19.1- and 15.6-fold selectivity, respectively, compared to 1.5-fold for 1. Importantly, the cytotoxicity of 60 and 61 is

Published

2018

35. GRP78‐mediated antioxidant response and ABC transporter activity confers chemoresistance to pancreatic cancer cells

Author

Vikas Dudeja, Nikita S. Sharma, Alice Nomura, Sulagna Banerjee, Patricia Dauer, Ashok K. Saluja, and Vineet Gupta

Subjects

0301 basic medicine, Cancer Research, Gene Expression, ATP-binding cassette transporter, Endoplasmic Reticulum, Mice, 0302 clinical medicine, Homeostasis, Endoplasmic Reticulum Chaperone BiP, Research Articles, Heat-Shock Proteins, Regulation of gene expression, Antibiotics, Antineoplastic, Cell Death, chemoresistance, General Medicine, unfolded protein response, Plicamycin, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, 3. Good health, Oncology, 030220 oncology & carcinogenesis, Disease Progression, Molecular Medicine, Research Article, GRP78, NF-E2-Related Factor 2, Sp1 Transcription Factor, Mice, Nude, Biology, lcsh:RC254-282, Sp1, 03 medical and health sciences, Pancreatic cancer, Cell Line, Tumor, Genetics, medicine, Gene silencing, Animals, Humans, Gene Silencing, Transcription factor, medicine.disease, Pancreatic Neoplasms, 030104 developmental biology, Drug Resistance, Neoplasm, Cancer cell, Cancer research, Unfolded protein response, ATP-Binding Cassette Transporters, Reactive Oxygen Species

Abstract

Chemoresistance is a major therapeutic challenge that plays a role in the poor statistical outcomes in pancreatic cancer. Unfolded protein response (UPR) is one of the homeostasis mechanisms in cancer cells that have been correlated with chemoresistance in a number of cancers including pancreatic cancer. In this study, we show that modulating glucose regulatory protein 78 (GRP78), the master regulator of the UPR, can have a profound effect on multiple pathways that mediate chemoresistance. Our study showed for the first time that silencing GRP78 can diminish efflux activity of ATP-binding cassette (ABC) transporters, and it can decrease the antioxidant response resulting in an accumulation of reactive oxygen species (ROS). We also show that these effects can be mediated by the activity of specificity protein 1 (SP1), a transcription factor overexpressed in pancreatic cancer. Thus, inhibition of SP1 negatively affects the UPR, deregulates the antioxidant response of NRF2, as well as ABC transporter activity by inhibiting GRP78-mediated ER homeostasis. Sp1 and NRF2 have been classified as nononcogene addiction genes and thus are imperative to understanding the molecular mechanism of resistance. These finding have huge clinical relevance as both Sp1 and GRP78 are overexpressed in pancreatic cancer patients and increased expression of these proteins is indicative of poor prognosis. Understanding how these proteins may regulate chemoresistance phenotype of this aggressive cancer may pave the way for development of efficacious therapy for this devastating disease.

Published

2018

36. Gene expression dynamics following mithramycin treatment: A possible model for post-chemotherapy cognitive impairment

Author

Eyal Asor and Dorit Ben-Shachar

Subjects

Male, 0301 basic medicine, medicine.medical_specialty, Physiology, medicine.medical_treatment, Anxiety, Spatial memory, 03 medical and health sciences, 0302 clinical medicine, Physiology (medical), Internal medicine, Gene expression, medicine, Animals, Cognitive Dysfunction, Prefrontal cortex, Saline, Gene, Spatial Memory, Pharmacology, Chemotherapy, business.industry, Cancer, Plicamycin, medicine.disease, Rats, Memory, Short-Term, Phenotype, 030104 developmental biology, Endocrinology, Gene Expression Regulation, business, 030217 neurology & neurosurgery, Homeostasis

Abstract

Chemotherapy-induced cognitive changes is a major burden on a substantial number of cancer survivors. The mechanism of this sequel is unknown. In this study, we followed long-term effects of early in life mithramycin (MTR) treatment on behaviour and on the normal course of alterations of gene expression in brain. Between post-natal days (PND) 7 and 10, male rats were divided into 2 groups, 1 receiving MTR (0.1 mg/kg s.c. per day) and the other receiving saline. At PND11, frontal cortex tissue samples were dissected from 4 rats from each group. At PND 65 the remaining rats underwent behavioural tests after which all the rats were decapitated and their prefrontal cortex incised. Rats treated transiently with MTR early in life, showed impairments in spatial working memory and anxious-like behaviour in adulthood. The immediate molecular effect of MTR was expressed in a limited number of altered genes of different unconnected trajectories, which were simultaneously distorted by the drug. In contrast, 3 months later we observed a change in the expression of more than 1000 genes that converged into specific cellular processes. Time-dependent gene expression dynamics of several genes was significantly different between treated and untreated rats. The differences in the total number of altered genes and in gene expression trends, immediately and long after MTR treatment cessation, suggest the evolution of a new cellular homeostatic set point, which can lead to behavioural abnormalities following chemotherapy treatment.

Published

2018

37. Early activation of Egr-1 promotes neuroinflammation and dopaminergic neurodegeneration in an experimental model of Parkinson's disease

Author

Mingtao Li, Qiaoying Huang, Xiaoxiao Du, Shanshan Ma, Shao Xu, and Qing Yu

Subjects

Male, 0301 basic medicine, Time Factors, Parkinson's disease, Tyrosine 3-Monooxygenase, Dopamine, Substantia nigra, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Parkinsonian Disorders, Developmental Neuroscience, Dopaminergic Cell, medicine, Animals, Enzyme Inhibitors, Neuroinflammation, Early Growth Response Protein 1, Inflammation, CD11b Antigen, Pars compacta, MPTP, Calcium-Binding Proteins, Microfilament Proteins, Neurodegeneration, Dopaminergic, Neurodegenerative Diseases, Plicamycin, medicine.disease, Mice, Inbred C57BL, Substantia Nigra, body regions, Disease Models, Animal, 030104 developmental biology, nervous system, Neurology, chemistry, Astrocytes, Phosphopyruvate Hydratase, Cytokines, Neuroscience, hormones, hormone substitutes, and hormone antagonists, 030217 neurology & neurosurgery

Abstract

The progressive loss of dopaminergic neurons in the substantia nigra pars compacta (SNpc) is one of the hallmarks of Parkinson's disease (PD). Neuroinflammation has been proposed to contributes to the progressive nature of the disease. Early growth response-1 (Egr-1), a zinc finger transcription factor, has been shown to have a crucial role in both neuronal death and the inflammatory response. However, whether and how Egr-1 is involved in the pathogenesis of PD has not been investigated. Using the subacute 1-methyl-4-phenyl-1,2,3,6-tetrahydropyridine (MPTP) mouse model of PD, we identified early peak induction of Egr-1 in the SNpc but not in the striatum. In situ immunofluorescent analysis showed that Egr-1 predominantly locates in the nuclei of nigral AldoC (+) astrocytes upon MPTP treatment. Genetic ablation of Egr-1 or inhibition of its transcriptional activity by Mithramycin A significantly suppresses the activation of both astrocytes and microglia, decreases proinflammatory cytokine expression, and protects dopaminergic cell bodies from degeneration in the SNpc. Taken together, these findings demonstrate that the induction of Egr-1 promotes neuroinflammation and dopaminergic cell body loss in the SNpc of MPTP-induced mouse model, suggesting an important role of astrocytic Egr-1 in neuroinflammation in PD.

Published

2018

38. Mithramycin A Enhances Tumor Sensitivity to Mitotic Catastrophe Resulting From DNA Damage

Author

Su I. Chung, Darmood Wei, Luca F. Valle, Grace McKay-Corkum, Ayla O. White, Eun Joo Chung, Kathryn E. Hudak, W. Marston Linehan, Jeffrey Burkeen, Shilpa S. Patil, Bradley T. Scroggins, and Deborah Citrin

Subjects

0301 basic medicine, Radiation-Sensitizing Agents, Cancer Research, Small interfering RNA, DNA Repair, Sp1 Transcription Factor, DNA damage, Mitosis, Apoptosis, Article, Toxicology, Mice, 03 medical and health sciences, 0302 clinical medicine, Transcription (biology), Cell Line, Tumor, Gene expression, Animals, Humans, Medicine, Radiology, Nuclear Medicine and imaging, Radiosensitivity, Fibroblast, Mitotic catastrophe, Gene knockdown, Radiation, business.industry, Cell Cycle, Neoplasms, Experimental, Plicamycin, 030104 developmental biology, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Cancer research, business, DNA Damage

Abstract

Purpose Specificity protein 1 (SP1) is involved in the transcription of several genes implicated in tumor maintenance. We investigated the effects of mithramycin A (MTA), an inhibitor of SP1 DNA binding, on radiation response. Methods and Materials Clonogenic survival after irradiation was assessed in 2 tumor cell lines (A549, UM-UC-3) and 1 human fibroblast line (BJ) after SP1 knockdown or MTA treatment. DNA damage repair was evaluated using γH2AX foci formation, and mitotic catastrophe was assessed using nuclear morphology. Gene expression was evaluated using polymerase chain reaction arrays. In vivo tumor growth delay was used to evaluate the effects of MTA on radiosensitivity. Results Targeting of SP1 with small interfering RNA or MTA sensitized A549 and UM-UC-3 to irradiation, with no effect on the BJ radiation response. MTA did not alter γH2AX foci formation after irradiation in tumor cells but did enhance mitotic catastrophe. Treatment with MTA suppressed transcription of genes involved in cell death. MTA administration to mice bearing A549 and UM-UC-3 xenografts enhanced radiation-induced tumor growth delay. Conclusions These results support SP1 as a target for radiation sensitization and confirm MTA as a radiation sensitizer in human tumor models.

Published

2018

39. A phase I/II trial and pharmacokinetic study of mithramycin in children and adults with refractory Ewing sarcoma and EWS–FLI1 fusion transcript

Author

Lauren Long, Patricia Whitcomb, Cody J. Peer, Brigitte C. Widemann, William D. Figg, John Glod, Patrick J. Grohar, Fernanda I. Arnaldez, Lee J. Helman, and Tristan M. Sissung

Subjects

Adult, Male, 0301 basic medicine, Drug, Cancer Research, Pathology, medicine.medical_specialty, Adolescent, Oncogene Proteins, Fusion, media_common.quotation_subject, Sarcoma, Ewing, Pharmacology, Toxicology, Article, Young Adult, 03 medical and health sciences, Ews fli1, 0302 clinical medicine, Pharmacokinetics, Refractory, medicine, Humans, Pharmacology (medical), Child, Dexamethasone, media_common, Antibiotics, Antineoplastic, Proto-Oncogene Protein c-fli-1, business.industry, Plicamycin, medicine.disease, 030104 developmental biology, Oncology, Fusion transcript, 030220 oncology & carcinogenesis, Elevated transaminases, Female, Sarcoma, RNA-Binding Protein EWS, business, medicine.drug

Abstract

PURPOSE: In a preclinical drug screen, mithramycin was identified as a potent inhibitor of the Ewing sarcoma EWS–FLI1 transcription factor. We conducted a phase I/II trial to determine the dose-limiting toxicities (DLT), maximum tolerated dose (MTD), and pharmacokinetics (PK) of mithramycin in children with refractory solid tumors, and the activity in children and adults with refractory Ewing sarcoma. PATIENTS AND METHODS: Mithramycin was administered intravenously over 6 h once daily for 7 days for 28 day cycles. Adult patients (phase II) initially received mithramycin at the previously determined recommended dose of 25 μg/kg/dose. The planned starting dose for children (phase I) was 17.5 μg/kg/dose. Plasma samples were obtained for mithramycin PK analysis. RESULTS: The first two adult patients experienced reversible grade 4 alanine aminotransferase (ALT)/aspartate aminotransferase (AST) elevation exceeding the MTD. Subsequent adult patients received mithramycin at 17.5 μg/kg/dose, and children at 13 μg/kg/dose with dexamethasone pretreatment. None of the four subsequent adult and two pediatric patients experienced cycle 1 DLT. No clinical responses were observed. The average maximal mithramycin plasma concentration in four patients was 17.8 ± 4.6 ng/mL. This is substantially below the sustained mithramycin concentrations ≥50 nmol/L required to suppress EWS–FLI1 transcriptional activity in preclinical studies. Due to inability to safely achieve the desired mithramycin exposure, the trial was closed to enrollment. CONCLUSIONS: Hepatotoxicity precluded the administration of a mithramycin at a dose required to inhibit EWS–FLI1. Evaluation of mithramycin in patients selected for decreased susceptibility to elevated transaminases may allow for improved drug exposure.

Published

2017

40. Mithramycin-loaded mPEG-PLGA nanoparticles exert potent antitumor efficacy against pancreatic carcinoma

Author

Xiujun Liu, Rui-Qi Wang, Xu-Jie Liu, Yong-Su Zhen, Yi Li, Liang Li, and Zhao Chunyan

Subjects

0301 basic medicine, endocrine system diseases, medicine.medical_treatment, pancreatic cancer, Pharmaceutical Science, Polyethylene Glycols, 0302 clinical medicine, Cancer immunotherapy, International Journal of Nanomedicine, Drug Discovery, Tissue Distribution, CD47, Cytotoxicity, Original Research, Drug Carriers, Mice, Inbred BALB C, Antibiotics, Antineoplastic, Microscopy, Confocal, mithramycin, medicine.diagnostic_test, Chemistry, Plicamycin, General Medicine, 030220 oncology & carcinogenesis, Female, Drug carrier, medicine.drug, Polyesters, Biophysics, Bioengineering, Sp1, Flow cytometry, Biomaterials, 03 medical and health sciences, Cell Line, Tumor, Pancreatic cancer, medicine, Animals, Humans, Particle Size, mPEG-PLGA nanoparticles, Oncogene, Organic Chemistry, technology, industry, and agriculture, medicine.disease, Xenograft Model Antitumor Assays, In vitro, Pancreatic Neoplasms, Drug Liberation, 030104 developmental biology, Cancer research, Nanoparticles

Abstract

Xu-Jie Liu, Liang Li, Xiu-Jun Liu, Yi Li, Chun-Yan Zhao, Rui-Qi Wang, Yong-Su Zhen Institute of Medicinal Biotechnology, Chinese Academy of Medical Sciences and Peking Union Medical College, Beijing, People’s Republic of China Abstract: Previous studies have shown that mithramycin A (MIT) is a promising candidate for the treatment of pancreatic carcinoma through inhibiting transcription factor Sp1. However, systemic toxicities may limit its clinical application. Here, we report a rationally designed formulation of MIT-loaded nanoparticles (MIT-NPs) with a small size and sustained release for improved passive targeting and enhanced therapeutic efficacy. Nearly spherical MIT-NPs with a mean particle size of 25.0±4.6nm were prepared by encapsulating MIT into methoxy poly(ethylene glycol)-block-poly(D,L-lactic-co-glycolic acid) (mPEG-PLGA) nanoparticles (NPs) with drug loading of 2.11%±0.51%. The in vitro release of the MIT-NPs lasted for >48h with a sustained-release pattern. The cytotoxicity of MIT-NPs to human pancreatic cancer BxPC-3 and MIA Paca-2 cells was comparable to that of free MIT. Determined by flow cytometry and confocal microscopy, the NPs internalized into the cells quickly and efficiently, reaching the peak level at 1–2h. In vivo fluorescence imaging showed that the prepared NPs were gradually accumulated in BxPC-3 and MIA Paca-2 xenografts and retained for 168h. The fluorescence intensity in both BxPC-3 and MIA Paca-2 tumors was much stronger than that of various tested organs. Therapeutic efficacy was evaluated with the poorly permeable BxPC-3 pancreatic carcinoma xenograft model. At a well-tolerated dose of 2mg/kg, MIT-NPs suppressed BxPC-3 tumor growth by 96%. Compared at an equivalent dose, MIT-NPs exerted significantly higher therapeutic effect than free MIT (86% versus 51%, P

Published

2017

41. LPS depletes PHLPP levels in macrophages through the inhibition of SP1 dependent transcriptional regulation

Author

Kishore V.L. Parsa, Neeraja P. Alamuru-Yellapragada, Soma Behera, and Sanghamitra Vundyala

Subjects

Lipopolysaccharides, 0301 basic medicine, Transcription, Genetic, Sp1 Transcription Factor, Phosphatase, Biophysics, Inflammation, Biology, Biochemistry, Monocytes, Cell Line, Mice, 03 medical and health sciences, 0302 clinical medicine, Genes, Reporter, Phosphoprotein Phosphatases, medicine, Transcriptional regulation, Animals, Humans, p300-CBP Transcription Factors, RNA, Messenger, RNA, Small Interfering, Luciferases, Promoter Regions, Genetic, Molecular Biology, Transcription factor, Gene knockdown, PHLPP, Macrophages, Nuclear Proteins, Promoter, Plicamycin, Cell Biology, Cell biology, HEK293 Cells, 030104 developmental biology, Gene Expression Regulation, 030220 oncology & carcinogenesis, Cancer research, Ectopic expression, medicine.symptom, Signal Transduction

Abstract

We have previously reported that bacterial endotoxin LPS attenuates expression of PHLPP, a ser/thr phosphatase, at both transcript and protein levels in different immune cells, however the underlying molecular mechanism is unknown and is of significant interest. Here, in line with the decreased transcript levels upon LPS treatment, we observed that LPS caused significant reduction in PHLPP promoter activity. We observed that SP1, a transcription factor frequently associated with inflammation, was recruited to the PHLPP promoter region. Ectopic expression of SP1 enhanced both transcript and protein levels of PHLPP while knockdown of SP1 or pharmacological inhibition of SP1 DNA binding by mithramycin reduced PHLPP expression. Moreover, over-expression of SP1 co-activators CBP/p300 augmented SP1 driven PHLPP promoter activity. Of note, LPS treatment depleted SP1 and CBP protein levels due to which recruitment of SP1 to PHLPP promoter was reduced. Further, we found that re-introduction of SP1 restored promoter activity and transcript levels of PHLPP in LPS stimulated cells. Collectively, our data revealed the molecular mechanism underlying the regulation of PHLPP expression during LPS induced macrophage inflammatory response.

Published

2017

42. Specificity protein 1-zinc finger protein 179 pathway is involved in the attenuation of oxidative stress following brain injury

Author

Shiu Hwa Yeh, Wen Chang Chang, Yi-Chao Lee, Tsung-Ping Su, Jian-Ying Chuang, An Chih Wu, Chung Che Wu, Shu Hui Lin, Pin Tse Lee, and Tzu-Jen Kao

Subjects

Transcriptional Activation, 0301 basic medicine, Zinc finger protein 179, Sp1 Transcription Factor, Clinical Biochemistry, Apoptosis, Mice, Transgenic, Brain damage, Biology, medicine.disease_cause, Biochemistry, Neuroprotection, Mice, 03 medical and health sciences, Traumatic brain injury, Nerve growth factor, Brain Injuries, Traumatic, medicine, Animals, Humans, Autoregulation, Specificity protein 1, lcsh:QH301-705.5, Neurons, chemistry.chemical_classification, Zinc finger, lcsh:R5-920, Reactive oxygen species, Sp1 transcription factor, Organic Chemistry, Hydrogen Peroxide, Plicamycin, Molecular biology, Cell biology, DNA-Binding Proteins, Oxidative Stress, 030104 developmental biology, lcsh:Biology (General), chemistry, medicine.symptom, Reactive Oxygen Species, lcsh:Medicine (General), Oxidative stress, Research Paper, Signal Transduction

Abstract

After sudden traumatic brain injuries, secondary injuries may occur during the following days or weeks, which leads to the accumulation of reactive oxygen species (ROS). Since ROS exacerbate brain damage, it is important to protect neurons against their activity. Zinc finger protein 179 (Znf179) was shown to act as a neuroprotective factor, but the regulation of gene expression under oxidative stress remains unknown. In this study, we demonstrated an increase in Znf179 protein levels in both in vitro model of hydrogen peroxide (H2O2)-induced ROS accumulation and animal models of traumatic brain injury. Additionally, we examined the sub-cellular localization of Znf179, and demonstrated that oxidative stress increases Znf179 nuclear shuttling and its interaction with specificity protein 1 (Sp1). Subsequently, the positive autoregulation of Znf179 expression, which is Sp1-dependent, was further demonstrated using luciferase reporter assay and green fluorescent protein (GFP)-Znf179-expressing cells and transgenic mice. The upregulation of Sp1 transcriptional activity induced by the treatment with nerve growth factor (NGF) led to an increase in Znf179 levels, which further protected cells against H2O2-induced damage. However, Sp1 inhibitor, mithramycin A, was shown to inhibit NGF effects, leading to a decrease in Znf179 expression and lower cellular protection. In conclusion, the results obtained in this study show that Znf179 autoregulation through Sp1-dependent mechanism plays an important role in neuroprotection, and NGF-induced Sp1 signaling may help attenuate more extensive (ROS-induced) damage following brain injury., Graphical abstract fx1, Highlights • Znf179 levels increase in vitro after hydrogen peroxide treatment. • Znf179 levels increase in vivo in traumatic brain injury mouse model. • Oxidative stress increases Znf179 translocation to nucleus. • Znf179 autoregulates its expression through Sp1-dependent mechanism. • Sp1-Znf179 pathway plays an important role in neuroprotection.

Published

2017

43. Heterologous reconstitution of the biosynthesis pathway for 4-demethyl-premithramycinone, the aglycon of antitumor polyketide mithramycin

Author

Gregory L. Challis, Yousef Dashti, José A. Salas, Carmen Méndez, Daniel Zabala, and Lijiang Song

Subjects

lcsh:QR1-502, Aureolic acid, Bioengineering, Applied Microbiology and Biotechnology, Cyclase, lcsh:Microbiology, 03 medical and health sciences, chemistry.chemical_compound, Polyketide, 0302 clinical medicine, Biosynthesis, Bacterial Proteins, Mithramycin, Polyketide synthase, Gene cluster, Acyl-CoA ligase, Gene, Streptomyces albus, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, DNA ligase, Antibiotics, Antineoplastic, biology, Research, Plicamycin, biology.organism_classification, Streptomyces, Streptomyces argillaceus, chemistry, Biochemistry, 030220 oncology & carcinogenesis, Polyketides, biology.protein, Premithramycinone, Biotechnology

Abstract

Spanish Ministry of Economy and Competitiveness [BIO2008-00269, BIO2011-25398]; grant "Apoyo a grupos de excelencia", Principado de Asturias-FEDER [FC-15-GRUPIN14-014]; Spanish Ministry of Economy and Competiveness, This work was supported by grants to C.M. from the Spanish Ministry of Economy and Competitiveness (Grants BIO2008-00269 and BIO2011-25398) and by the grant “Apoyo a grupos de excelencia”, Principado de Asturias-FEDER (FC-15-GRUPIN14-014). D.Z. was recipient of a predoctoral fellowship from the Spanish Ministry of Economy and Competiveness.

Published

2020

44. [High Expression Level of SP1, CSF1R, and PAK1 Correlates with Sensitivity of Leukemia Cells to the Antibiotic Mithramycin]

Author

E R, Vagapova, T D, Lebedev, A D, Tikhonova, B V, Goikhman, K A, Ivanenko, P V, Spirin, and V S, Prassolov

Subjects

Leukemia, Myeloid, Acute, p21-Activated Kinases, Receptors, Granulocyte-Macrophage Colony-Stimulating Factor, Sp1 Transcription Factor, Cell Line, Tumor, Humans, Cell Differentiation, Plicamycin, Sensitivity and Specificity, Anti-Bacterial Agents

Abstract

Acute myeloid leukemia (AML) is a genetically heterogeneous group of oncological diseases of the hematopoietic system, which are extremely difficult to treat. The development of new targeted drugs (Hylteritinib, Venetoclax) significantly improved the survival of patients, but resistance, as well as cytotoxic anti-leukemia drugs, often occurs. The search for new molecular targets for the development of effective approaches for the treatment of AML is very urgent. In blast cells of patients with AML, mutations, chromosomal rearrangements, and increased expression of a number of non-mutant genes, including transcription factor genes, are detected. The transcription factor Sp 1 binds to GC-rich regions of regulatory regions of various genes and thus controls their expression. Sp1 targets include genes responsible for proliferation, cell cycle regulation, and differentiation. In many malignant diseases, a high level of Sp1 gene expression is associated with an unfavorable prognosis, therefore, Sp1 is considered as a promising therapeutic target for cancer. In this paper, we estimated the expression levels of Sp1 in various malignant tissues. Increased Sp1 expression was detected in samples obtained from patients with AML, acute lymphoblastic leukemia, Ewing sarcoma, ovarian and kidney cancer. It is also shown that Sp1 expression correlates with the expression of genes encoding cytokine receptors and growth factors (CSF1R and IL6R), intracellular kinases (CSK, SYK, PAK1, ILK, JAK2), and transcription factor LMO2. The correlation between expression levels of Sp1 and CSF1R, SYK, Jak2 and LMO2 is also characteristic of transplanted human leukemia cells. We measured expression levels of Sp1, CSF1R, ILK, PAK1 in the cells of three transplantable lines of human leukemia and found increased levels of expression of these genes in Kasumi-1 cells. In addition, we showed that Kasumi-1 cells are most sensitive to Mitramycin, a drug that displaces Sp1 from its targets with DNA. Our data indicate the need to identify AML cells that are most sensitive to inhibition of Sp1 activity in order to assess the possibility of suppressing its activity in vivo.

Published

2020

45. Mithramycin A Radiosensitizes EWS:Fli1

Author

Mei Yun, Lin, Timothy A, Damron, Megan E, Oest, and Jason A, Horton

Subjects

Radiation-Sensitizing Agents, DNA Repair, Dose-Response Relationship, Drug, Oncogene Proteins, Fusion, Cell Survival, Proto-Oncogene Protein c-fli-1, Reverse Transcriptase Polymerase Chain Reaction, Down-Regulation, Apoptosis, Plicamycin, Sarcoma, Ewing, Radiation Tolerance, Xenograft Model Antitumor Assays, Histones, Mice, Cell Line, Tumor, Animals, DNA Breaks, Double-Stranded, Comet Assay, RNA-Binding Protein EWS, Cell Proliferation

Abstract

The oncogenic EWS:Fli1 fusion protein is a key transcriptional mediator of Ewing sarcoma initiation, progression, and therapeutic resistance. Mithramycin A (MithA) is a potent and specific inhibitor of transcription mediated by the EWS:Fli1. We tested the hypothesis that pretreatment with MithA could selectively radiosensitize EWS:Fli1A panel of 4 EWS:Fli1We found that MithA alone could potently and selectively inhibit the growth of EWS:Fli1Our data indicate that MithA is an effective radiosensitizer of EWS:Fli1

Published

2020

46. Drug‐Eluting Stent Targeting Sp‐1‐Attenuated Restenosis by Engaging YAP‐Mediated Vascular Smooth Muscle Cell Phenotypic Modulation

Author

Jie Zhao, Chen Huang, and Yuelin Zhu

Subjects

Male, Smooth Muscle Proliferation and Differentiation, Vascular smooth muscle, medicine.medical_treatment, Cell Plasticity, Cell, 030204 cardiovascular system & hematology, Muscle, Smooth, Vascular, Molecular Cardiology, 0302 clinical medicine, Restenosis, Cell Movement, Transcription (biology), drug‐eluting stent, Medicine, Carotid Stenosis, Cells, Cultured, Original Research, 0303 health sciences, phenotypic modulation, Drug-Eluting Stents, Plicamycin, Transfection, Phenotype, Carotid Arteries, medicine.anatomical_structure, Drug-eluting stent, cardiovascular system, Rabbits, Yes‐associated protein, Cardiology and Cardiovascular Medicine, Signal Transduction, Sp1 Transcription Factor, Myocytes, Smooth Muscle, Prosthesis Design, restenosis, 03 medical and health sciences, Animals, Transcription factor, smooth muscle cell, Cell Proliferation, 030304 developmental biology, business.industry, Cardiovascular Agents, YAP-Signaling Proteins, transcription factor specificity protein 1, medicine.disease, Rats, Disease Models, Animal, Animal Models of Human Disease, Cancer research, Apoptosis Regulatory Proteins, Carotid Artery Injuries, business, Angioplasty, Balloon, Basic Science Research

Abstract

Background Activation of the YAP (Yes‐associated protein) pathway has been demonstrated to be related to smooth muscle cells ( SMC s) phenotypic modulation and vessel restenosis. The aim of this study was to illustrate the molecular mechanisms that regulate the expression of YAP during the process of SMC s phenotypic switch. Whether the molecular basis identified in the study could be a potential therapeutic target for drug‐eluting stents is further tested. Methods and Results In cell culture and in rat carotid arterial injury models, Sp‐1 (specificity protein 1) expression was significantly induced, and correlated with SMC s proliferative phenotype. Overexpression of Sp‐1 promoted SMC s proliferation and migration. Conversely, siSp‐1 transfection or Sp‐1 inhibitor Mithramycin A treatment attenuates SMC proliferation and migration. Through gain‐ and loss‐function assays, we demonstrated that YAP was involved in Sp‐1‐mediated SMC phenotypic switch. Mechanistically, activated Sp‐1 regulated YAP transcriptional expression through binding to its promoter. Moreover, we fabricated a Sp‐1 inhibitor Mithramycin A‐eluting stent and further tested it. In the rabbit carotid model, Mithramycin A‐eluting stent inhibited YAP transcription and attenuated in‐stent restenosis through regulating YAP ‐mediated SMC phenotypic switch. Conclusions Sp‐1 controls phenotypic modulation of SMC by regulating transcription factor YAP . Drug‐eluting stent targeting Sp‐1 might represent a novel therapeutic strategy to prevent in‐stent restenosis.

Published

2020

47. Thermodynamics of the Interaction between the Spike Protein of Severe Acute Respiratory Syndrome Coronavirus-2 and the Receptor of Human Angiotensin-Converting Enzyme 2. Effects of Possible Ligands

Author

García-Iriepa, Cristina, Hognon, Cécilia, Francés-Monerris, Antonio, Iriepa, Isabel, Miclot, Tom, Barone, Giampaolo, Monari, Antonio, Marazzi, Marco, 0000-0002-7577-8242, 0000-0001-8232-4989, 0000-0001-8773-2359, 0000-0001-9464-1463, 0000-0001-7158-7994, Garcia-Iriepa C., Hognon C., Frances-Monerris A., Iriepa I., Miclot T., Barone G., Monari A., and Marazzi M.

Subjects

Letter, Pneumonia, Viral, Protein domain, Thermodynamics, Plasma protein binding, Molecular Dynamics Simulation, Peptidyl-Dipeptidase A, Ligands, medicine.disease_cause, Protein-Protein Binding, 01 natural sciences, Docking, Betacoronavirus, 03 medical and health sciences, Protein Domains, 0103 physical sciences, medicine, Humans, General Materials Science, Physical and Theoretical Chemistry, Binding site, Receptor, Pandemics, 030304 developmental biology, Coronavirus, chemistry.chemical_classification, 0303 health sciences, Binding Sites, 010304 chemical physics, SARS-CoV-2, Spike Protein, COVID-19, Plicamycin, Transmembrane protein, Enzyme, chemistry, Settore CHIM/03 - Chimica Generale E Inorganica, Molecular Dynamics Simulations, Spike Glycoprotein, Coronavirus, Angiotensin-converting enzyme 2, Diosmin, Angiotensin-Converting Enzyme 2, Coronavirus Infections, Protein Binding

Abstract

Since the end of 2019, the coronavirus SARS-CoV-2 has caused more than 1000000 deaths all over the world and still lacks a medical treatment despite the attention of the whole scientific community. Human angiotensin-converting enzyme 2 (ACE2) was recently recognized as the transmembrane protein that serves as the point of entry of SARS-CoV-2 into cells, thus constituting the first biomolecular event leading to COVID-19 disease. Here, by means of a state-of-the-art computational approach, we propose a rational evaluation of the molecular mechanisms behind the formation of the protein complex. Moreover, the free energy of binding between ACE2 and the active receptor binding domain of the SARS-CoV-2 spike protein is evaluated quantitatively, providing for the first time the thermodynamics of virus-receptor recognition. Furthermore, the action of different ACE2 ligands is also examined in particular in their capacity to disrupt SARS-CoV-2 recognition, also providing via a free energy profile the quantification of the ligand-induced decreased affinity. These results improve our knowledge on molecular grounds of the SARS-CoV-2 infection and allow us to suggest rationales that could be useful for the subsequent wise molecular design for the treatment of COVID-19 cases.

Published

2020

48. Erb‑B2 Receptor Tyrosine Kinase 2 is negatively regulated by the p53‑responsive microRNA‑3184‑5p in cervical cancer cells

Author

Hongli Liu, Fei Liu, Nan Wu, Hongtao Wang, Xuan Zhang, Yuzhi Li, Suyang Guo, Yuan Zhang, Lihua Wang, Jing Zhang, and Jing Liu

Subjects

p53, Adult, Cancer Research, cervical cancer, Class I Phosphatidylinositol 3-Kinases, Receptor, ErbB-2, Biopsy, Cell, Uterine Cervical Neoplasms, Cervix Uteri, Hysterectomy, Receptor tyrosine kinase, Cell Movement, Cell Line, Tumor, microRNA, medicine, Humans, Neoplasm Invasiveness, skin and connective tissue diseases, Aged, Cell Proliferation, Cervical cancer, biology, Oncogene, business.industry, Cancer, Articles, General Medicine, Plicamycin, Cell cycle, Middle Aged, medicine.disease, Molecular medicine, Erb-B2 Receptor Tyrosine Kinase 2, Gene Expression Regulation, Neoplastic, MicroRNAs, medicine.anatomical_structure, Oncology, biology.protein, Cancer research, Female, Tumor Suppressor Protein p53, business, microRNA-3184-5p

Abstract

The oncogenic role of Erb-B2 Receptor Tyrosine Kinase 2 (ERBB2) has been identified in several types of cancer, but less is known on its function and mechanism of action in cervical cancer cells. The present study employed a multipronged approach to investigate the role of ERBB2 in cervical cancer. ERBB2 and microRNA (miR)-3184-5p expression was assessed in patient-derived cervical cancer biopsy tissues, revealing that higher levels of ERBB2 and lower levels of miR-3184-5p were associated with clinicopathological indicators of cervical cancer progression. Furthermore, ERBB2 stimulated proliferation, migration and sphere-formation of cervical cancer cells in vitro. This effect was mediated by enhanced phosphatidylinositol-4,5-bisphosphate 3-kinase catalytic subunit α activity. Additionally, it was revealed that miR-3184-5p directly suppressed ERBB2 in cervical cancer cells. The p53 activator Mithramycin A stimulated p53 and miR-3184-5p expression, thereby lowering the levels of ERBB2 and attenuating proliferation, migration and sphere-formation of cervical cancer cells. In conclusion, the findings of the present study suggested ERBB2 as an oncogenic protein that may promote invasiveness in cervical cancer cells. Treatment of cervical cancer cells with the p53 activator Mithramycin A restored the levels of the endogenous ERBB2 inhibitor miR-3184-5p and may represent a novel treatment strategy for cervical cancer.

Published

2019

49. Mithramycin suppresses DNA damage repair via targeting androgen receptor in prostate cancer

Author

Collin Gilbreath, Amit K. Das, Shan Wang, Rajni Sonavane, Paul Yenerall, Xiaofang Huo, Ganesh V. Raj, Shihong Ma, Rahul K. Kollipara, and Ralf Kittler

Subjects

0301 basic medicine, Male, Cancer Research, DNA Repair, DNA repair, medicine.drug_class, Bleomycin, Article, 03 medical and health sciences, Prostate cancer, chemistry.chemical_compound, 0302 clinical medicine, Downregulation and upregulation, Cell Line, Tumor, Medicine, Humans, Enhancer, Antibiotics, Antineoplastic, business.industry, Cell growth, Plicamycin, medicine.disease, Androgen, Androgen receptor, Prostatic Neoplasms, Castration-Resistant, 030104 developmental biology, Oncology, chemistry, Receptors, Androgen, 030220 oncology & carcinogenesis, Cancer research, business, DNA Damage

Abstract

The dependency of prostate cancer (PCa) growth on androgen receptor (AR) signaling has been harnessed to develop first-line therapies for high-risk localized and metastatic PCa treatment. However, the occurrence of aberrant expression, mutated or splice variants of AR confers resistance to androgen ablation therapy (ADT), radiotherapy or chemotherapy in AR-positive PCa. Therapeutic strategies that effectively inhibit the expression and/or transcriptional activity of full-length AR, mutated AR and AR splice variants have remained elusive. In this study, we report that mithramycin (MTM), an antineoplastic antibiotic, suppresses cell proliferation and exhibits dual inhibitory effects on expression and transcriptional activity of AR and AR splice variants. MTM blocks AR recruitment to its genomic targets by occupying AR enhancers and causes downregulation of AR target genes, which includes key DNA repair factors in DNA damage repair (DDR). We show that MTM significantly impairs DDR and enhances the effectiveness of ionizing radiation or the radiomimetic agent Bleomycin in PCa. Thus, the combination of MTM treatment with RT or radiomimetic agents, such as bleomycin, may present a novel effective therapeutic strategy for patients with high-risk, clinically localized PCa.

Published

2019

50. Interplay between base excision repair protein XRCC1 and ALDH2 predicts overall survival in lung and liver cancer patients

Author

Xin Chen, Dengfu Yao, Bruno Vaz, Samuel Hume, Siobhan Cunniffe, Mattia Poletto, Grigory L. Dianov, Kristijan Ramadan, and Arnaud J. Legrand

Subjects

0301 basic medicine, Cancer Research, Lung Neoplasms, XRCC1, DNA damage, DNA repair, Cell Survival, Genetic instability, Aldehyde dehydrogenase, Cell Line, Liver and lung carcinomas, 03 medical and health sciences, Cell Line, Tumor, medicine, Humans, Mithramycin a, RNA, Small Interfering, ALDH2, Base excision repair, Original Paper, Aldehydes, biology, Aldehyde Dehydrogenase, Mitochondrial, Liver Neoplasms, General Medicine, Plicamycin, medicine.disease, 3. Good health, 030104 developmental biology, X-ray Repair Cross Complementing Protein 1, Oncology, Cancer cell, biology.protein, Cancer research, Molecular Medicine, Liver cancer

Abstract

Background To deliver efficacious personalised cancer treatment, it is essential to characterise the cellular metabolism as well as the genetic stability of individual tumours. In this study, we describe a new axis between DNA repair and detoxification of aldehyde derivatives with important implications for patient prognosis and treatment. Methods Western blot and qPCR analyses were performed in relevant non-transformed and cancer cell lines from lung and liver tissue origin in combination with bioinformatics data mining of The Cancer Genome Atlas database from lung and hepatocellular cancer patients. Results Using both biochemical and bioinformatics approaches, we revealed an association between the levels of expression of the aldehyde detoxifying enzyme aldehyde dehydrogenase 2 (ALDH2) and the key DNA base excision repair protein XRCC1. Across cancer types, we found that if one of the corresponding genes exhibits a low expression level, the level of the other gene is increased. Surprisingly, we found that low ALDH2 expression levels associated with high XRCC1 expression levels are indicative for a poor overall survival, particularly in lung and liver cancer patients. In addition, we found that Mithramycin A, a XRCC1 expression inhibitor, efficiently kills cancer cells expressing low levels of ALDH2. Conclusions Our data suggest that lung and liver cancers require efficient single-strand break repair for their growth in order to benefit from a low aldehyde detoxification metabolism. We also propose that the ratio of XRCC1 and ALDH2 levels may serve as a useful prognostic tool in these cancer types. Electronic supplementary material The online version of this article (10.1007/s13402-018-0390-8) contains supplementary material, which is available to authorized users.

Published

2019