Your search keyword '"Boothman DA"' showing total 120 results

1. Expanding antitumor therapeutic windows by targeting cancer-specific nicotinamide adenine dinucleotide phosphate-biogenesis pathways

Author

Chakrabarti G, Gerber DE, and Boothman DA

Subjects

Therapeutics. Pharmacology, RM1-950

Abstract

Gaurab Chakrabarti,1,2,4 David E Gerber,3,4 David A Boothman1,2,4 1Department of Pharmacology, 2Department of Radiation Oncology, 3Division of Hematology and Oncology, 4Harold C Simmons Comprehensive Cancer Center, UT Southwestern Medical Center, Dallas, TX, USA Abstract: Nicotinamide adenine dinucleotide phosphate (NADPH) biogenesis is an essential mechanism by which both normal and cancer cells maintain redox balance. While antitumor approaches to treat cancers through elevated reactive oxygen species (ROS) are not new ideas, depleting specific NADPH-biogenesis pathways that control recovery and repair pathways are novel, viable approaches to enhance cancer therapy. However, to elicit efficacious therapies exploiting NADPH-biogenic pathways, it is crucial to understand and specifically define the roles of NADPH-biogenesis pathways used by cancer cells for survival or recovery from cell stress. It is equally important to select NADPH-biogenic pathways that are expendable or not utilized in normal tissue to avoid unwanted toxicity. Here, we address recent literature that demonstrates specific tumor-selective NADPH-biogenesis pathways that can be exploited using agents that target specific cancer cell pathways normally not utilized in normal cells. Defining NADPH-biogenesis profiles of specific cancer-types should enable novel strategies to exploit these therapeutic windows for increased efficacy against recalcitrant neoplastic disease, such as pancreatic cancers. Accomplishing the goal of using ROS as a weapon against cancer cells will also require agents, such as NQO1 bioactivatable drugs, that selectively induce elevated ROS levels in cancer cells, while normal cells are protected. Keywords: reactive oxygen species (ROS), NQO1-bioactivatable drugs, nicotinamide adenine dinucleotide phosphate (NADPH), glutathione (GSH), biogenic pathways, antioxidant

Published

2015

2. Abstract P2-06-03: A Polymorphic AAAG Repeat in the Estrogen Receptor-Related-Gamma Gene May Represent a Breast Cancer Predisposition Biomarker

Author

Garner, HR, primary, McCormick, JF, additional, Li, L-S, additional, McIver, LJ, additional, Bubb, VJ, additional, George, AC, additional, Boothman, DA, additional, Quinn, JP, additional, and Galindo, C., additional

Published

2010

3. Synergisitic inhibition of DNA repair by combining ß-lapachone with Nu7026 as a strategy for killing primary and metastatic breast cancers.

Author

Bey, EA, primary, Kessinger, C, additional, Blanco, E, additional, Bachoo, R, additional, Williams, N, additional, and Boothman, DA, additional

Published

2009

4. Improved protein arrays for quantitative systems analysis of the dynamics of signaling pathway interactions

Author

Pastor Johanne, Zou Yonglong, Jiwani Ameena J, Dong Ying, Wang Xiaoyu, Kuro-o Makoto, Habib Amyn A, Ruan Minzi, Boothman David A, and Yang Chin-Rang

Subjects

protein array, quantum dot, quantitative analysis, signaling pathway, cross-talk, image analysis, glioma, systems biology, Cytology, QH573-671

Abstract

Abstract An improved version of quantitative protein array platform utilizing linear Quantum dot signaling for systematically measuring protein levels and phosphorylation states is presented. The signals are amplified linearly by a confocal laser Quantum dot scanner resulting in ~1000-fold more sensitivity than traditional Western blots, but are not linear by the enzyme-based amplification. Software is developed to facilitate the quantitative readouts of signaling network activities. Kinetics of EGFRvIII mutant signaling was analyzed to quantify cross-talks between EGFR and other signaling pathways.

Published

2011

5. IB-DNQ and Rucaparib dual treatment alters cell cycle regulation and DNA repair in triple negative breast cancer cells.

Author

Runnebohm AM, Wijeratne HRS, Justice SAP, Wijeratne AB, Roy G, Singh N, Hergenrother P, Boothman DA, Motea EA, and Mosley AL

Abstract

Background: Triple negative breast cancer (TNBC), characterized by the lack of three canonical receptors, is unresponsive to commonly used hormonal therapies. One potential TNBC-specific therapeutic target is NQO1, as it is highly expressed in many TNBC patients and lowly expressed in non-cancer tissues. DNA damage induced by NQO1 bioactivatable drugs in combination with Rucaparib-mediated inhibition of PARP1-dependent DNA repair synergistically induces cell death., Methods: To gain a better understanding of the mechanisms behind this synergistic effect, we used global proteomics, phosphoproteomics, and thermal proteome profiling to analyze changes in protein abundance, phosphorylation and protein thermal stability., Results: Very few protein abundance changes resulted from single or dual agent treatment; however, protein phosphorylation and thermal stability were impacted. Histone H2AX was among several proteins identified to have increased phosphorylation when cells were treated with the combination of IB-DNQ and Rucaparib, validating that the drugs induced persistent DNA damage. Thermal proteome profiling revealed destabilization of H2AX following combination treatment, potentially a result of the increase in phosphorylation. Kinase substrate enrichment analysis predicted altered activity for kinases involved in DNA repair and cell cycle following dual agent treatment. Further biophysical analysis of these two processes revealed alterations in SWI/SNF complex association and tubulin / p53 interactions., Conclusions: Our findings that the drugs target DNA repair and cell cycle regulation, canonical cancer treatment targets, in a way that is dependent on increased expression of a protein selectively found to be upregulated in cancers without impacting protein abundance illustrate that multi-omics methodologies are important to gain a deeper understanding of the mechanisms behind treatment induced cancer cell death., Competing Interests: Competing interests The authors declare that they have no competing interests.

Published

2024

6. Synergistic Effect of β-Lapachone and Aminooxyacetic Acid on Central Metabolism in Breast Cancer.

Author

Chang MC, Mahar R, McLeod MA, Giacalone AG, Huang X, Boothman DA, and Merritt ME

Subjects

Cell Line, Tumor, Citrates, Female, Glutamates metabolism, Humans, NAD metabolism, NAD(P)H Dehydrogenase (Quinone) metabolism, Succinates metabolism, Aminooxyacetic Acid therapeutic use, Breast Neoplasms drug therapy, Breast Neoplasms metabolism, Naphthoquinones pharmacology, Naphthoquinones therapeutic use

Abstract

The compound β-lapachone, a naturally derived naphthoquinone, has been utilized as a potent medicinal nutrient to improve health. Over the last twelve years, numerous reports have demonstrated distinct associations of β-lapachone and NAD(P)H: quinone oxidoreductase 1 (NQO1) protein in the amelioration of various diseases. Comprehensive research of NQO1 bioactivity has clearly confirmed the tumoricidal effects of β-lapachone action through NAD + -keresis, in which severe DNA damage from reactive oxygen species (ROS) production triggers a poly-ADP-ribose polymerase-I (PARP1) hyperactivation cascade, culminating in NAD + /ATP depletion. Here, we report a novel combination strategy with aminooxyacetic acid (AOA), an aspartate aminotransferase inhibitor that blocks the malate-aspartate shuttle (MAS) and synergistically enhances the efficacy of β-lapachone metabolic perturbation in NQO1 + breast cancer. We evaluated metabolic turnover in MDA-MB-231 NQO1 + , MDA-MB-231 NQO1 - , MDA-MB-468, and T47D cancer cells by measuring the isotopic labeling of metabolites from a [U- 13 C]glucose tracer. We show that β-lapachone treatment significantly hampers lactate secretion by ~85% in NQO1 + cells. Our data demonstrate that combinatorial treatment decreases citrate, glutamate, and succinate enrichment by ~14%, ~50%, and ~65%, respectively. Differences in citrate, glutamate, and succinate fractional enrichments indicate synergistic effects on central metabolism based on the coefficient of drug interaction. Metabolic modeling suggests that increased glutamine anaplerosis is protective in the case of MAS inhibition.

Published

2022

7. Personalized Genome-Scale Metabolic Models Identify Targets of Redox Metabolism in Radiation-Resistant Tumors.

Author

Lewis JE, Forshaw TE, Boothman DA, Furdui CM, and Kemp ML

Subjects

Humans, NADP chemistry, NADP genetics, Oxidation-Reduction, Reactive Oxygen Species chemistry, Hydrogen Peroxide, Neoplasms genetics, Neoplasms radiotherapy

Abstract

Redox cofactor production is integral toward antioxidant generation, clearance of reactive oxygen species, and overall tumor response to ionizing radiation treatment. To identify systems-level alterations in redox metabolism that confer resistance to radiation therapy, we developed a bioinformatics pipeline for integrating multi-omics data into personalized genome-scale flux balance analysis models of 716 radiation-sensitive and 199 radiation-resistant tumors. These models collectively predicted that radiation-resistant tumors reroute metabolic flux to increase mitochondrial NADPH stores and reactive oxygen species (ROS) scavenging. Simulated genome-wide knockout screens agreed with experimental siRNA gene knockdowns in matched radiation-sensitive and radiation-resistant cancer cell lines, revealing gene targets involved in mitochondrial NADPH production, central carbon metabolism, and folate metabolism that allow for selective inhibition of glutathione production and H 2 O 2 clearance in radiation-resistant cancers. This systems approach represents a significant advancement in developing quantitative genome-scale models of redox metabolism and identifying personalized metabolic targets for improving radiation sensitivity in individual cancer patients., Competing Interests: Declaration of Interests The authors declare no competing interests., (Copyright © 2020 Elsevier Inc. All rights reserved.)

Published

2021

8. MTHFD2 Blockade Enhances the Efficacy of β-Lapachone Chemotherapy With Ionizing Radiation in Head and Neck Squamous Cell Cancer.

Author

Shukla K, Singh N, Lewis JE, Tsang AW, Boothman DA, Kemp ML, and Furdui CM

Abstract

Head and Neck Squamous Cell Cancer (HNSCC) presents with multiple treatment challenges limiting overall survival rates and affecting patients' quality of life. Amongst these, resistance to radiation therapy constitutes a major clinical problem in HNSCC patients compounded by origin, location, and tumor grade that limit tumor control. While cisplatin is considered the standard radiosensitizing agent for definitive or adjuvant radiotherapy, in recurrent tumors or for palliative care other chemotherapeutics such as the antifolates methotrexate or pemetrexed are also being utilized as radiosensitizers. These drugs inhibit the enzyme dihydrofolate reductase, which is essential for DNA synthesis and connects the 1-C/folate metabolism to NAD(P)H and NAD(P) + balance in cells. In previous studies, we identified MTHFD2, a mitochondrial enzyme involved in folate metabolism, as a key contributor to NAD(P)H levels in the radiation-resistant cells and HNSCC tumors. In the study presented here, we investigated the role of MTHFD2 in the response to radiation alone and in combination with β-lapachone, a NQO1 bioactivatable drug, which generates reactive oxygen species concomitant with NAD(P)H oxidation to NAD(P) + . These studies are performed in a matched HNSCC cell model of response to radiation: the radiation resistant rSCC-61 and radiation sensitive SCC-61 cells reported earlier by our group. Radiation resistant rSCC-61 cells had increased sensitivity to β-lapachone compared to SCC-61 and knockdown of MTHFD2 in rSCC-61 cells further potentiated the cytotoxicity of β-lapachone with radiation in a dose and time-dependent manner. rSCC-61 MTHFD2 knockdown cells irradiated and treated with β-lapachone showed increased PARP1 activation, inhibition of mitochondrial respiration, decreased respiration-linked ATP production, and increased mitochondrial superoxide and protein oxidation as compared to control rSCC-61 scrambled shRNA. Thus, these studies point to MTHFD2 as a potential target for development of radiosensitizing chemotherapeutics and potentiator of β-lapachone cytotoxicity., (Copyright © 2020 Shukla, Singh, Lewis, Tsang, Boothman, Kemp and Furdui.)

Published

2020

9. Targeting Base Excision Repair in Cancer: NQO1-Bioactivatable Drugs Improve Tumor Selectivity and Reduce Treatment Toxicity Through Radiosensitization of Human Cancer.

Author

Starcher CL, Pay SL, Singh N, Yeh IJ, Bhandare SB, Su X, Huang X, Bey EA, Motea EA, and Boothman DA

Abstract

Ionizing radiation (IR) creates lethal DNA damage that can effectively kill tumor cells. However, the high dose required for a therapeutic outcome also damages healthy tissue. Thus, a therapeutic strategy with predictive biomarkers to enhance the beneficial effects of IR allowing a dose reduction without losing efficacy is highly desirable. NAD(P)H:quinone oxidoreductase 1 (NQO1) is overexpressed in the majority of recalcitrant solid tumors in comparison with normal tissue. Studies have shown that NQO1 can bioactivate certain quinone molecules (e.g., ortho-naphthoquinone and β-lapachone) to induce a futile redox cycle leading to the formation of oxidative DNA damage, hyperactivation of poly(ADP-ribose) polymerase 1 (PARP1), and catastrophic depletion of NAD + and ATP, which culminates in cellular lethality via NAD + -Keresis. However, NQO1-bioactivatable drugs induce methemoglobinemia and hemolytic anemia at high doses. To circumvent this, NQO1-bioactivatable agents have been shown to synergize with PARP1 inhibitors, pyrimidine radiosensitizers, and IR. This therapeutic strategy allows for a reduction in the dose of the combined agents to decrease unwanted side effects by increasing tumor selectivity. In this review, we discuss the mechanisms of radiosensitization between NQO1-bioactivatable drugs and IR with a focus on the involvement of base excision repair (BER). This combination therapeutic strategy presents a unique tumor-selective and minimally toxic approach for targeting solid tumors that overexpress NQO1., (Copyright © 2020 Starcher, Pay, Singh, Yeh, Bhandare, Su, Huang, Bey, Motea and Boothman.)

Published

2020

10. Inhibition of TXNRD or SOD1 overcomes NRF2-mediated resistance to β-lapachone.

Author

Torrente L, Prieto-Farigua N, Falzone A, Elkins CM, Boothman DA, Haura EB, and DeNicola GM

Subjects

Carcinoma, Non-Small-Cell Lung drug therapy, Cell Line, Tumor, Cell Proliferation drug effects, Cell Survival drug effects, HEK293 Cells, Humans, Kelch-Like ECH-Associated Protein 1 genetics, Lung Neoplasms drug therapy, Mutation, Superoxide Dismutase-1 antagonists & inhibitors, Thioredoxin Reductase 1 antagonists & inhibitors, Carcinoma, Non-Small-Cell Lung genetics, Drug Resistance, Neoplasm, Lung Neoplasms genetics, NAD(P)H Dehydrogenase (Quinone) genetics, NF-E2-Related Factor 2 genetics, Naphthoquinones pharmacology

Abstract

Alterations in the NRF2/KEAP1 pathway result in the constitutive activation of NRF2, leading to the aberrant induction of antioxidant and detoxification enzymes, including NQO1. The NQO1 bioactivatable agent β-lapachone can target cells with high NQO1 expression but relies in the generation of reactive oxygen species (ROS), which are actively scavenged in cells with NRF2/KEAP1 mutations. However, whether NRF2/KEAP1 mutations influence the response to β-lapachone treatment remains unknown. To address this question, we assessed the cytotoxicity of β-lapachone in a panel of NSCLC cell lines bearing either wild-type or mutant KEAP1. We found that, despite overexpression of NQO1, KEAP1 mutant cells were resistant to β-lapachone due to enhanced detoxification of ROS, which prevented DNA damage and cell death. To evaluate whether specific inhibition of the NRF2-regulated antioxidant enzymes could abrogate resistance to β-lapachone, we systematically inhibited the four major antioxidant cellular systems using genetic and/or pharmacologic approaches. We demonstrated that inhibition of the thioredoxin-dependent system or copper-zinc superoxide dismutase (SOD1) could abrogate NRF2-mediated resistance to β-lapachone, while depletion of catalase or glutathione was ineffective. Interestingly, inhibition of SOD1 selectively sensitized KEAP1 mutant cells to β-lapachone exposure. Our results suggest that NRF2/KEAP1 mutational status might serve as a predictive biomarker for response to NQO1-bioactivatable quinones in patients. Further, our results suggest SOD1 inhibition may have potential utility in combination with other ROS inducers in patients with KEAP1/NRF2 mutations., (Copyright © 2020 The Authors. Published by Elsevier B.V. All rights reserved.)

Published

2020

11. Combinatorial Therapy of Zinc Metallochaperones with Mutant p53 Reactivation and Diminished Copper Binding.

Author

Zaman S, Yu X, Bencivenga AF, Blanden AR, Liu Y, Withers T, Na B, Blayney AJ, Gilleran J, Boothman DA, Loh SN, Kimball SD, and Carpizo DR

Subjects

Animals, Antineoplastic Agents pharmacology, Cell Line, Combined Modality Therapy, Humans, Metallochaperones genetics, Mice, Protein Binding, Pyridines pharmacology, Radiation, Reactive Oxygen Species metabolism, Signal Transduction drug effects, Signal Transduction radiation effects, Copper metabolism, Metallochaperones metabolism, Mutation, Transcriptional Activation drug effects, Transcriptional Activation radiation effects, Tumor Suppressor Protein p53 genetics, Tumor Suppressor Protein p53 metabolism, Zinc metabolism

Abstract

Chemotherapy and radiation are more effective in wild-type (WT) p53 tumors due to p53 activation. This is one rationale for developing drugs that reactivate mutant p53 to synergize with chemotherapy and radiation. Zinc metallochaperones (ZMC) are a new class of mutant p53 reactivators that restore WT structure and function to zinc-deficient p53 mutants. We hypothesized that the thiosemicarbazone, ZMC1, would synergize with chemotherapy and radiation. Surprisingly, this was not found. We explored the mechanism of this and found the reactive oxygen species (ROS) activity of ZMC1 negates the signal on p53 that is generated with chemotherapy and radiation. We hypothesized that a zinc scaffold generating less ROS would synergize with chemotherapy and radiation. The ROS effect of ZMC1 is generated by its chelation of redox active copper. ZMC1 copper binding ( K Cu ) studies reveal its affinity for copper is approximately 10 8 greater than Zn 2+ We identified an alternative zinc scaffold (nitrilotriacetic acid) and synthesized derivatives to improve cell permeability. These compounds bind zinc in the same range as ZMC1 but bound copper much less avidly (10 6 - to 10 7 -fold lower) and induced less ROS. These compounds were synergistic with chemotherapy and radiation by inducing p53 signaling events on mutant p53. We explored other combinations with ZMC1 based on its mechanism of action and demonstrate that ZMC1 is synergistic with MDM2 antagonists, BCL2 antagonists, and molecules that deplete cellular reducing agents. We have identified an optimal Cu 2+ :Zn 2+ binding ratio to facilitate development of ZMCs as chemotherapy and radiation sensitizers. Although ZMC1 is not synergistic with chemotherapy and radiation, it is synergistic with a number of other targeted agents., (©2019 American Association for Cancer Research.)

Published

2019

12. NQO1 targeting prodrug triggers innate sensing to overcome checkpoint blockade resistance.

Author

Li X, Liu Z, Zhang A, Han C, Shen A, Jiang L, Boothman DA, Qiao J, Wang Y, Huang X, and Fu YX

Subjects

A549 Cells, Animals, Cell Line, Tumor, Humans, Immunity, Innate drug effects, Immunity, Innate immunology, Mice, Inbred C57BL, Mice, Inbred NOD, Mice, Knockout, Mice, SCID, NAD(P)H Dehydrogenase (Quinone) genetics, NAD(P)H Dehydrogenase (Quinone) metabolism, Neoplasms genetics, Neoplasms immunology, Neoplasms, Experimental drug therapy, Neoplasms, Experimental genetics, Neoplasms, Experimental metabolism, Reactive Oxygen Species metabolism, Signal Transduction drug effects, Signal Transduction genetics, Signal Transduction immunology, T-Lymphocytes drug effects, T-Lymphocytes immunology, T-Lymphocytes metabolism, NAD(P)H Dehydrogenase (Quinone) antagonists & inhibitors, Naphthoquinones pharmacology, Neoplasms drug therapy, Prodrugs pharmacology, Xenograft Model Antitumor Assays

Abstract

Lack of proper innate sensing inside tumor microenvironment (TME) limits T cell-targeted immunotherapy. NAD(P)H:quinone oxidoreductase 1 (NQO1) is highly enriched in multiple tumor types and has emerged as a promising target for direct tumor-killing. Here, we demonstrate that NQO1-targeting prodrug β-lapachone triggers tumor-selective innate sensing leading to T cell-dependent tumor control. β-Lapachone is catalyzed and bioactivated by NQO1 to generate ROS in NQO1 high tumor cells triggering oxidative stress and release of the damage signals for innate sensing. β-Lapachone-induced high mobility group box 1 (HMGB1) release activates the host TLR4/MyD88/type I interferon pathway and Batf3 dendritic cell-dependent cross-priming to bridge innate and adaptive immune responses against the tumor. Furthermore, targeting NQO1 is very potent to trigger innate sensing for T cell re-activation to overcome checkpoint blockade resistance in well-established tumors. Our study reveals that targeting NQO1 potently triggers innate sensing within TME that synergizes with immunotherapy to overcome adaptive resistance.

Published

2019

13. NQO1-dependent, Tumor-selective Radiosensitization of Non-small Cell Lung Cancers.

Author

Motea EA, Huang X, Singh N, Kilgore JA, Williams NS, Xie XJ, Gerber DE, Beg MS, Bey EA, and Boothman DA

Subjects

Animals, Carcinoma, Non-Small-Cell Lung metabolism, Carcinoma, Non-Small-Cell Lung radiotherapy, Cell Line, Tumor, Disease Models, Animal, Dose-Response Relationship, Radiation, Humans, Lung Neoplasms metabolism, Lung Neoplasms radiotherapy, Mice, Naphthoquinones pharmacology, Poly(ADP-ribose) Polymerases metabolism, Radiation, Ionizing, Radiation-Sensitizing Agents pharmacology, Treatment Outcome, Xenograft Model Antitumor Assays, Carcinoma, Non-Small-Cell Lung genetics, Lung Neoplasms genetics, NAD(P)H Dehydrogenase (Quinone) genetics, Radiation Tolerance genetics

Abstract

Purpose: Development of tumor-specific therapies for the treatment of recalcitrant non-small cell lung cancers (NSCLC) is urgently needed. Here, we investigated the ability of β-lapachone (β-lap, ARQ761 in clinical form) to selectively potentiate the effects of ionizing radiation (IR, 1-3 Gy) in NSCLCs that overexpress NAD(P)H:Quinone Oxidoreductase 1 (NQO1)., Experimental Design: The mechanism of lethality of low-dose IR in combination with sublethal doses of β-lap was evaluated in NSCLC lines in vitro and validated in subcutaneous and orthotopic xenograft models in vivo . Pharmacokinetics and pharmacodynamics (PK/PD) studies comparing single versus cotreatments were performed to validate therapeutic efficacy and mechanism of action., Results: β-Lap administration after IR treatment hyperactivated PARP, greatly lowered NAD + /ATP levels, and increased double-strand break (DSB) lesions over time in vitro . Radiosensitization of orthotopic, as well as subcutaneous, NSCLCs occurred with high apparent cures (>70%), even though 1/8 β-lap doses reach subcutaneous versus orthotopic tumors. No methemoglobinemia or long-term toxicities were noted in any normal tissues, including mouse liver that expresses the highest level of NQO1 (∼12 units) of any normal tissue. PK/PD responses confirm that IR + β-lap treatments hyperactivate PARP activity, greatly lower NAD + /ATP levels, and dramatically inhibit DSB repair in exposed NQO1 + cancer tissue, whereas low NQO1 levels and high levels of catalase in associated normal tissue were protective., Conclusions: Our data suggest that combination of sublethal doses of β-lap and IR is a viable approach to selectively treat NQO1-overexpressing NSCLC and warrant a clinical trial using low-dose IR + β-lap against patients with NQO1 + NSCLCs., (©2019 American Association for Cancer Research.)

Published

2019

14. Kub5-Hera RPRD1B Deficiency Promotes "BRCAness" and Vulnerability to PARP Inhibition in BRCA-proficient Breast Cancers.

Author

Motea EA, Fattah FJ, Xiao L, Girard L, Rommel A, Morales JC, Patidar P, Zhou Y, Porter A, Xie Y, Minna JD, and Boothman DA

Subjects

Animals, Breast Neoplasms pathology, CDC2 Protein Kinase chemistry, CDC2 Protein Kinase metabolism, Cell Cycle Proteins chemistry, Cell Cycle Proteins metabolism, Cell Line, Tumor, DNA Damage, Disease Models, Animal, Female, Gene Expression Regulation, Neoplastic, Genes, Reporter, Humans, Mice, Mutation, Neoplasm Proteins chemistry, Neoplasm Proteins metabolism, Poly(ADP-ribose) Polymerase Inhibitors pharmacology, Promoter Regions, Genetic, Synthetic Lethal Mutations, Xenograft Model Antitumor Assays, Breast Neoplasms etiology, Breast Neoplasms metabolism, Cell Cycle Proteins deficiency, Genes, BRCA1, Genes, BRCA2, Neoplasm Proteins deficiency, Poly(ADP-ribose) Polymerases metabolism

Abstract

Purpose: Identification of novel strategies to expand the use of PARP inhibitors beyond BRCA deficiency is of great interest in personalized medicine. Here, we investigated the unannotated role of Kub5-Hera RPRD1B (K-H) in homologous recombination (HR) repair and its potential clinical significance in targeted cancer therapy., Experimental Design: Functional characterization of K-H alterations on HR repair of double-strand breaks (DSB) were assessed by targeted gene silencing, plasmid reporter assays, immunofluorescence, and Western blots. Cell survival with PARP inhibitors was evaluated through colony-forming assays and statistically analyzed for correlation with K-H expression in various BRCA1/2 nonmutated breast cancers. Gene expression microarray/qPCR analyses, chromatin immunoprecipitation, and rescue experiments were used to investigate molecular mechanisms of action., Results: K-H expression loss correlates with rucaparib LD 50 values in a panel of BRCA1/2 nonmutated breast cancers. Mechanistically, K-H depletion promotes BRCAness , where extensive upregulation of PARP1 activity was required for the survival of breast cancer cells. PARP inhibition in these cells led to synthetic lethality that was rescued by wild-type K-H reexpression, but not by a mutant K-H (p.R106A) that weakly binds RNAPII. K-H mediates HR by facilitating recruitment of RNAPII to the promoter region of a critical DNA damage response and repair effector, cyclin-dependent kinase 1 ( CDK1 )., Conclusions: Cancer cells with low K-H expression may have exploitable BRCAness properties that greatly expand the use of PARP inhibitors beyond BRCA mutations. Our results suggest that aberrant K-H alterations may have vital translational implications in cellular responses/survival to DNA damage, carcinogenesis, and personalized medicine., (©2018 American Association for Cancer Research.)

Published

2018

15. Following anticancer drug activity in cell lysates with DNA devices.

Author

Kahanda D, Singh N, Boothman DA, and Slinker JD

Subjects

Antineoplastic Agents analysis, Biosensing Techniques standards, Cell Line, Tumor, DNA Damage drug effects, DNA Repair drug effects, Humans, NAD(P)H Dehydrogenase (Quinone) genetics, Naphthoquinones analysis, Antineoplastic Agents pharmacology, Biosensing Techniques instrumentation, DNA analysis, Gene Expression Regulation, Enzymologic drug effects, Naphthoquinones pharmacology

Abstract

There is a great need to track the selectivity of anticancer drug activity and to understand the mechanisms of associated biological activity. Here we focus our studies on the specific NQO1 bioactivatable drug, ß-lapachone, which is in several Phase I clinical trials to treat human non-small cell lung, pancreatic and breast cancers. Multi-electrode chips with electrochemically-active DNA monolayers are used to track anticancer drug activity in cellular lysates and correlate cell death activity with DNA damage. Cells were prepared from the triple-negative breast cancer (TNBC) cell line, MDA-MB-231 (231) to be proficient or deficient in expression of the NAD(P)H:quinone oxidoreductase 1 (NQO1) enzyme, which is overexpressed in most solid cancers and lacking in control healthy cells. Cells were lysed and added to chips, and the impact of β-lapachone (β-lap), an NQO1-dependent DNA-damaging drug, was tracked with DNA electrochemical signal changes arising from drug-induced DNA damage. Electrochemical DNA devices showed a 3.7-fold difference in the electrochemical responses in NQO1+ over NQO1- cell lysates, as well as 10-20-fold selectivity to catalase and dicoumarol controls that deactivate DNA damaging pathways. Concentration-dependence studies revealed that 1.4 µM β-lap correlated with the onset of cell death from viability assays and the midpoint of DNA damage on the chip, and 2.5 µM β-lap correlated with the midpoint of cell death and the saturation of DNA damage on the chip. Results indicate that these devices could inform therapeutic decisions for cancer treatment., (Copyright © 2018 Elsevier B.V. All rights reserved.)

Published

2018

16. Phase 1 study of ARQ 761, a β-lapachone analogue that promotes NQO1-mediated programmed cancer cell necrosis.

Author

Gerber DE, Beg MS, Fattah F, Frankel AE, Fatunde O, Arriaga Y, Dowell JE, Bisen A, Leff RD, Meek CC, Putnam WC, Kallem RR, Subramaniyan I, Dong Y, Bolluyt J, Sarode V, Luo X, Xie Y, Schwartz B, and Boothman DA

Subjects

Adult, Aged, Aged, 80 and over, Cell Line, Tumor, DNA Damage drug effects, Female, Humans, Male, Middle Aged, Naphthoquinones chemistry, Reactive Oxygen Species metabolism, Apoptosis drug effects, NAD(P)H Dehydrogenase (Quinone) analysis, NAD(P)H Dehydrogenase (Quinone) biosynthesis, Naphthoquinones therapeutic use, Necrosis chemically induced, Neoplasms drug therapy

Abstract

Background: NAD(P)H:quinone oxidoreductase 1 (NQO1) is a two-electron oxidoreductase expressed in multiple tumour types. ARQ 761 is a β-lapachone (β-lap) analogue that exploits the unique elevation of NQO1 found in solid tumours to cause tumour-specific cell death., Methods: We performed a 3+3 dose escalation study of 3 schedules (weekly, every other week, 2/3 weeks) of ARQ 761 in patients with refractory advanced solid tumours. Tumour tissue was analysed for NQO1 expression. After 20 patients were analysed, enrolment was restricted to patients with NQO1-high tumours (H-score ≥ 200)., Results: A total of 42 patients were treated. Median number of prior lines of therapy was 4. Maximum tolerated dose was 390 mg/m 2 as a 2-h infusion every other week. Dose-limiting toxicity was anaemia. The most common treatment-related adverse events were anaemia (79%), fatigue (45%), hypoxia (33%), nausea (17%), and vomiting (17%). Transient grade 3 hypoxia, reflecting possible methemoglobinaemia, occurred in 26% of patients. Among 32 evaluable patients, best response was stable disease (n = 12); 6 patients had tumour shrinkage. There was a trend towards improved efficacy in NQO1-high tumours (P = 0.06)., Conclusions: ARQ 761 has modest single-agent activity, which appears associated with tumour NQO1 expression. Principal toxicities include anaemia and possible methemoglobinaemia.

Published

2018

17. The NQO1 bioactivatable drug, β-lapachone, alters the redox state of NQO1+ pancreatic cancer cells, causing perturbation in central carbon metabolism.

Author

Silvers MA, Deja S, Singh N, Egnatchik RA, Sudderth J, Luo X, Beg MS, Burgess SC, DeBerardinis RJ, Boothman DA, and Merritt ME

Subjects

Activation, Metabolic, Antineoplastic Agents metabolism, Biomarkers metabolism, Carbon Isotopes, Cell Line, Tumor, Cell Survival drug effects, Citric Acid Cycle drug effects, DNA Damage, Enzyme Inhibitors metabolism, Glycolysis drug effects, Humans, Metabolomics methods, NAD(P)H Dehydrogenase (Quinone) genetics, NAD(P)H Dehydrogenase (Quinone) metabolism, Naphthoquinones metabolism, Neoplasm Proteins antagonists & inhibitors, Neoplasm Proteins genetics, Neoplasm Proteins metabolism, Oxidation-Reduction, Oxidative Stress drug effects, Pancreatic Neoplasms enzymology, Pancreatic Neoplasms metabolism, Principal Component Analysis, Prodrugs metabolism, Recombinant Proteins chemistry, Recombinant Proteins metabolism, Antineoplastic Agents pharmacology, Energy Metabolism drug effects, Enzyme Inhibitors pharmacology, NAD(P)H Dehydrogenase (Quinone) antagonists & inhibitors, Naphthoquinones pharmacology, Pancreatic Neoplasms drug therapy, Prodrugs pharmacology

Abstract

Many cancer treatments, such as those for managing recalcitrant tumors like pancreatic ductal adenocarcinoma, cause off-target toxicities in normal, healthy tissue, highlighting the need for more tumor-selective chemotherapies. β-Lapachone is bioactivated by NAD(P)H:quinone oxidoreductase 1 (NQO1). This enzyme exhibits elevated expression in most solid cancers and therefore is a potential cancer-specific target. β-Lapachone's therapeutic efficacy partially stems from the drug's induction of a futile NQO1-mediated redox cycle that causes high levels of superoxide and then peroxide formation, which damages DNA and causes hyperactivation of poly(ADP-ribose) polymerase, resulting in extensive NAD + /ATP depletion. However, the effects of this drug on energy metabolism due to NAD + depletion were never described. The futile redox cycle rapidly consumes O 2 , rendering standard assays of Krebs cycle turnover unusable. In this study, a multimodal analysis, including metabolic imaging using hyperpolarized pyruvate, points to reduced oxidative flux due to NAD + depletion after β-lapachone treatment of NQO1+ human pancreatic cancer cells. NAD + -sensitive pathways, such as glycolysis, flux through lactate dehydrogenase, and the citric acid cycle (as inferred by flux through pyruvate dehydrogenase), were down-regulated by β-lapachone treatment. Changes in flux through these pathways should generate biomarkers useful for in vivo dose responses of β-lapachone treatment in humans, avoiding toxic side effects. Targeting the enzymes in these pathways for therapeutic treatment may have the potential to synergize with β-lapachone treatment, creating unique NQO1-selective combinatorial therapies for specific cancers. These findings warrant future studies of intermediary metabolism in patients treated with β-lapachone., (© 2017 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2017

18. Aerosol delivery of stabilized polyester-siRNA nanoparticles to silence gene expression in orthotopic lung tumors.

Author

Yan Y, Zhou K, Xiong H, Miller JB, Motea EA, Boothman DA, Liu L, and Siegwart DJ

Subjects

A549 Cells, Administration, Inhalation, Aerosols administration & dosage, Aerosols chemical synthesis, Animals, Cell Line, Tumor, Drug Stability, Female, Gene Expression Regulation, Neoplastic genetics, Gene Silencing, Humans, Mice, Mice, Nude, Nanocapsules administration & dosage, Nanocapsules ultrastructure, Treatment Outcome, Genetic Therapy methods, Lung Neoplasms genetics, Lung Neoplasms therapy, Nanocapsules chemistry, Polyesters chemistry, RNA, Small Interfering administration & dosage, RNA, Small Interfering genetics

Abstract

Tremendous progress has been made in the development of delivery carriers for small RNA therapeutics. However, most achievements have focused on the treatment of liver-associated diseases because conventional lipid and lipidoid nanoparticles (LNPs) readily accumulate in the liver after intravenous (i.v.) administration. Delivering RNAs to other organs and tumor tissues remains an ongoing challenge. Here, we utilized a 540-member combinatorial functional polyester library to discover nanoparticles (NPs) that enable efficacious siRNA delivery to A549 lung cancer cells in vitro and in vivo. PE4K-A13-0.33C6 and PE4K-A13-0.33C10 NPs were efficiently internalized into A549-Luc cells within 4 h. The addition of PEG 2000 DMG lipid or Pluronic F-127 onto the surface of the polyplexes reduced the surface charge of NPs, resulting in an increase of serum stability. We then explored aerosol delivery of stabilized PE4K-A13-0.33C6 and PE4K-A13-0.33C10 NPs to implanted orthotopic lung tumors. We found that by altering the administration route from i.v. to aerosol, the NPs could avoid liver accumulation and instead be specifically localized only in the lungs. This resulted in significant gene silencing in the A549 orthotopic lung tumors. Due to the ability to deliver siRNA to non-liver targets, this approach provides a privileged route for gene silencing in the lungs., (Copyright © 2016 Elsevier Ltd. All rights reserved.)

Published

2017

19. Leveraging an NQO1 Bioactivatable Drug for Tumor-Selective Use of Poly(ADP-ribose) Polymerase Inhibitors.

Author

Huang X, Motea EA, Moore ZR, Yao J, Dong Y, Chakrabarti G, Kilgore JA, Silvers MA, Patidar PL, Cholka A, Fattah F, Cha Y, Anderson GG, Kusko R, Peyton M, Yan J, Xie XJ, Sarode V, Williams NS, Minna JD, Beg M, Gerber DE, Bey EA, and Boothman DA

Subjects

Animals, Carcinoma, Non-Small-Cell Lung genetics, Cell Line, Tumor, Cell Proliferation drug effects, Cell Survival drug effects, DNA Damage, Drug Synergism, Gene Expression Regulation, Neoplastic, Humans, Lung Neoplasms genetics, Mice, Naphthoquinones pharmacology, Pancreatic Neoplasms genetics, Reactive Oxygen Species metabolism, Up-Regulation, Xenograft Model Antitumor Assays, Carcinoma, Non-Small-Cell Lung drug therapy, Lung Neoplasms drug therapy, NAD(P)H Dehydrogenase (Quinone) genetics, Naphthoquinones administration & dosage, Pancreatic Neoplasms drug therapy, Poly(ADP-ribose) Polymerase Inhibitors administration & dosage

Abstract

Therapeutic drugs that block DNA repair, including poly(ADP-ribose) polymerase (PARP) inhibitors, fail due to lack of tumor-selectivity. When PARP inhibitors and β-lapachone are combined, synergistic antitumor activity results from sustained NAD(P)H levels that refuel NQO1-dependent futile redox drug recycling. Significant oxygen-consumption-rate/reactive oxygen species cause dramatic DNA lesion increases that are not repaired due to PARP inhibition. In NQO1 + cancers, such as non-small-cell lung, pancreatic, and breast cancers, cell death mechanism switches from PARP1 hyperactivation-mediated programmed necrosis with β-lapachone monotherapy to synergistic tumor-selective, caspase-dependent apoptosis with PARP inhibitors and β-lapachone. Synergistic antitumor efficacy and prolonged survival were noted in human orthotopic pancreatic and non-small-cell lung xenograft models, expanding use and efficacy of PARP inhibitors for human cancer therapy., (Published by Elsevier Inc.)

Published

2016

20. Focal Adhesion Kinase Regulates the DNA Damage Response and Its Inhibition Radiosensitizes Mutant KRAS Lung Cancer.

Author

Tang KJ, Constanzo JD, Venkateswaran N, Melegari M, Ilcheva M, Morales JC, Skoulidis F, Heymach JV, Boothman DA, and Scaglioni PP

Subjects

A549 Cells, Animals, Carcinoma, Non-Small-Cell Lung drug therapy, Carcinoma, Non-Small-Cell Lung genetics, Carcinoma, Non-Small-Cell Lung metabolism, Cell Line, Tumor, DNA Damage drug effects, Female, Humans, Lung Neoplasms drug therapy, Mice, Mice, Nude, Mutation drug effects, Protein Kinase Inhibitors pharmacology, RNA Interference drug effects, Xenograft Model Antitumor Assays, DNA Damage genetics, Focal Adhesion Protein-Tyrosine Kinases metabolism, Lung Neoplasms genetics, Lung Neoplasms metabolism, Mutation genetics, Proto-Oncogene Proteins p21(ras) genetics, Radiation-Sensitizing Agents metabolism

Abstract

Purpose: Non-small cell lung cancer (NSCLC) is the leading cause of cancer-related deaths worldwide due to the limited availability of effective therapeutic options. For instance, there are no effective strategies for NSCLCs that harbor mutant KRAS, the most commonly mutated oncogene in NSCLC. Thus, our purpose was to make progress toward the generation of a novel therapeutic strategy for NSCLC., Experimental Design: We characterized the effects of suppressing focal adhesion kinase (FAK) by RNA interference (RNAi), CRISPR/CAS9 gene editing or pharmacologic approaches in NSCLC cells and in tumor xenografts. In addition, we tested the effects of suppressing FAK in association with ionizing radiation (IR), a standard-of-care treatment modality., Results: FAK is a critical requirement of mutant KRAS NSCLC cells. With functional experiments, we also found that, in mutant KRAS NSCLC cells, FAK inhibition resulted in persistent DNA damage and susceptibility to exposure to IR. Accordingly, administration of IR to FAK-null tumor xenografts causes a profound antitumor effect in vivo CONCLUSIONS: FAK is a novel regulator of DNA damage repair in mutant KRAS NSCLC and its pharmacologic inhibition leads to radiosensitizing effects that could be beneficial in cancer therapy. Our results provide a framework for the rationale clinical testing of FAK inhibitors in NSCLC patients. Clin Cancer Res; 22(23); 5851-63. ©2016 AACR., Competing Interests: No potential conflicts of interest were disclosed DISCLOSURE OF POTENTIAL CONFLICT OF INTEREST The other authors disclosed no potential conflicts of interest., (©2016 American Association for Cancer Research.)

Published

2016

21. XRN2 Links Transcription Termination to DNA Damage and Replication Stress.

Author

Morales JC, Richard P, Patidar PL, Motea EA, Dang TT, Manley JL, and Boothman DA

Subjects

Antineoplastic Agents chemistry, Cell Nucleus metabolism, DNA Helicases, DNA Repair, Gene Expression Regulation, Neoplastic, Genomic Instability, Genomics, HeLa Cells, Humans, Microscopy, Fluorescence, Multifunctional Enzymes, Neoplasms drug therapy, Neoplasms genetics, Plasmids metabolism, RNA Helicases metabolism, RNA, Small Interfering metabolism, DNA Damage, DNA Replication, Exoribonucleases genetics, Exoribonucleases physiology, Transcription, Genetic, Tumor Suppressor p53-Binding Protein 1 genetics

Abstract

XRN2 is a 5'-3' exoribonuclease implicated in transcription termination. Here we demonstrate an unexpected role for XRN2 in the DNA damage response involving resolution of R-loop structures and prevention of DNA double-strand breaks (DSBs). We show that XRN2 undergoes DNA damage-inducible nuclear re-localization, co-localizing with 53BP1 and R loops, in a transcription and R-loop-dependent process. XRN2 loss leads to increased R loops, genomic instability, replication stress, DSBs and hypersensitivity of cells to various DNA damaging agents. We demonstrate that the DSBs that arise with XRN2 loss occur at transcriptional pause sites. XRN2-deficient cells also exhibited an R-loop- and transcription-dependent delay in DSB repair after ionizing radiation, suggesting a novel role for XRN2 in R-loop resolution, suppression of replication stress, and maintenance of genomic stability. Our study highlights the importance of regulating transcription-related activities as a critical component in maintaining genetic stability.

Published

2016

22. NQO1-Mediated Tumor-Selective Lethality and Radiosensitization for Head and Neck Cancer.

Author

Li LS, Reddy S, Lin ZH, Liu S, Park H, Chun SG, Bornmann WG, Thibodeaux J, Yan J, Chakrabarti G, Xie XJ, Sumer BD, Boothman DA, and Yordy JS

Subjects

Adenosine Triphosphate metabolism, Animals, Catalase genetics, Catalase metabolism, Cell Death drug effects, Cell Death genetics, Cell Line, Tumor, Cell Survival genetics, Cell Survival radiation effects, Disease Models, Animal, Enzyme Activation, Gene Expression Regulation, Neoplastic drug effects, Head and Neck Neoplasms drug therapy, Head and Neck Neoplasms metabolism, Head and Neck Neoplasms pathology, Humans, NAD(P)H Dehydrogenase (Quinone) metabolism, Naphthoquinones pharmacology, Radiation-Sensitizing Agents pharmacology, Reactive Oxygen Species metabolism, Survival Analysis, Xenograft Model Antitumor Assays, Gene Expression, Head and Neck Neoplasms genetics, NAD(P)H Dehydrogenase (Quinone) genetics, Radiation Tolerance genetics, Radiation, Ionizing

Abstract

Unlabelled: Ionizing radiation (IR) is a key therapeutic regimen for many head and neck cancers (HNC). However, the 5-year overall survival rate for locally advanced HNCs is approximately 50% and better therapeutic efficacy is needed., Nad(p)h: quinone oxidoreductase 1 (NQO1) is overexpressed in many cancers, and β-lapachone (β-lap), a unique NQO1 bioactivatable drug, exploits this enzyme to release massive reactive oxygen species (ROS) that synergize with IR to kill by programmed necrosis. β-Lap represents a novel therapeutic opportunity in HNC leading to tumor-selective lethality that will enhance the efficacy of IR. Immunohistochemical staining and Western blot assays were used to assess the expression levels of NQO1 in HNC cells and tumors. Forty-five percent of endogenous HNCs expressed elevated NQO1 levels. In addition, multiple HNC cell lines and tumors demonstrated elevated levels of NQO1 expression and activity and were tested for anticancer lethality and radiosensitization by β-lap using long-term survival assays. The combination of nontoxic β-lap doses and IR significantly enhanced NQO1-dependent tumor cell lethality, increased ROS, TUNEL-positive cells, DNA damage, NAD(+), and ATP consumption, and resulted in significant antitumor efficacy and prolonged survival in two xenograft murine HNC models, demonstrating β-lap radiosensitization of HNCs through a NQO1-dependent mechanism. This translational study offers a potential biomarker-driven strategy using NQO1 expression to select tumors susceptible to β-lap-induced radiosensitization. Mol Cancer Ther; 15(7); 1757-67. ©2016 AACR., Competing Interests: of Potential Conflicts of Interest: No potential conflicts of interest were disclosed., (©2016 American Association for Cancer Research.)

Published

2016

23. Using DNA devices to track anticancer drug activity.

Author

Kahanda D, Chakrabarti G, Mcwilliams MA, Boothman DA, and Slinker JD

Subjects

Catalase chemistry, Cell Line, Tumor, DNA Damage drug effects, Gold chemistry, Humans, NAD(P)H Dehydrogenase (Quinone) chemistry, Naphthoquinones pharmacology, Antineoplastic Agents pharmacology, Biosensing Techniques, DNA Repair

Abstract

It is beneficial to develop systems that reproduce complex reactions of biological systems while maintaining control over specific factors involved in such processes. We demonstrated a DNA device for following the repair of DNA damage produced by a redox-cycling anticancer drug, beta-lapachone (β-lap). These chips supported ß-lap-induced biological redox cycle and tracked subsequent DNA damage repair activity with redox-modified DNA monolayers on gold. We observed drug-specific changes in square wave voltammetry from these chips at therapeutic ß-lap concentrations of high statistical significance over drug-free control. We also demonstrated a high correlation of this change with the specific ß-lap-induced redox cycle using rational controls. The concentration dependence of ß-lap revealed significant signal changes at levels of high clinical significance as well as sensitivity to sub-lethal levels of ß-lap. Catalase, an enzyme decomposing peroxide, was found to suppress DNA damage at a NQO1/catalase ratio found in healthy cells, but was clearly overcome at a higher NQO1/catalase ratio consistent with cancer cells. We found that it was necessary to reproduce key features of the cellular environment to observe this activity. Thus, this chip-based platform enabled tracking of ß-lap-induced DNA damage repair when biological criteria were met, providing a unique synthetic platform for uncovering activity normally confined to inside cells., (Copyright © 2016 Elsevier B.V. All rights reserved.)

Published

2016

24. The Kub5-Hera/RPRD1B interactome: a novel role in preserving genetic stability by regulating DNA mismatch repair.

Author

Patidar PL, Motea EA, Fattah FJ, Zhou Y, Morales JC, Xie Y, Garner HR, and Boothman DA

Subjects

Antigens, Nuclear genetics, Cell Cycle Proteins genetics, DNA Breaks, Double-Stranded, DNA Topoisomerases, Type I genetics, DNA-Binding Proteins genetics, HeLa Cells, Humans, Ku Autoantigen, Multiprotein Complexes genetics, Neoplasm Proteins genetics, Neoplasms metabolism, RNA Helicases genetics, RNA Polymerase II genetics, Repressor Proteins genetics, Cell Cycle Proteins metabolism, DNA Mismatch Repair genetics, Genomic Instability, Neoplasm Proteins metabolism, Neoplasms genetics

Abstract

Ku70-binding protein 5 (Kub5)-Hera (K-H)/RPRD1B maintains genetic integrity by concomitantly minimizing persistent R-loops and promoting repair of DNA double strand breaks (DSBs). We used tandem affinity purification-mass spectrometry, co-immunoprecipitation and gel-filtration chromatography to define higher-order protein complexes containing K-H scaffolding protein to gain insight into its cellular functions. We confirmed known protein partners (Ku70, RNA Pol II, p15RS) and discovered several novel associated proteins that function in RNA metabolism (Topoisomerase 1 and RNA helicases), DNA repair/replication processes (PARP1, MSH2, Ku, DNA-PKcs, MCM proteins, PCNA and DNA Pol δ) and in protein metabolic processes, including translation. Notably, this approach directed us to investigate an unpredicted involvement of K-H in DNA mismatch repair (MMR) where K-H depletion led to concomitant MMR deficiency and compromised global microsatellite stability. Mechanistically, MMR deficiency in K-H-depleted cells was a consequence of reduced stability of the core MMR proteins (MLH1 and PMS2) caused by elevated basal caspase-dependent proteolysis. Pan-caspase inhibitor treatment restored MMR protein loss. These findings represent a novel mechanism to acquire MMR deficiency/microsatellite alterations. A significant proportion of colon, endometrial and ovarian cancers exhibit k-h expression/copy number loss and may have severe mutator phenotypes with enhanced malignancies that are currently overlooked based on sporadic MSI+ screening., (© The Author(s) 2016. Published by Oxford University Press on behalf of Nucleic Acids Research.)

Published

2016

25. Depleting Tumor-NQO1 Potentiates Anoikis and Inhibits Growth of NSCLC.

Author

Madajewski B, Boatman MA, Chakrabarti G, Boothman DA, and Bey EA

Subjects

Animals, Anoikis, Carcinoma, Non-Small-Cell Lung metabolism, Carcinoma, Non-Small-Cell Lung pathology, Cell Line, Tumor, Cell Proliferation drug effects, Dicumarol pharmacology, Enzyme Inhibitors pharmacology, Gene Expression Regulation, Neoplastic drug effects, Gene Knockdown Techniques, Humans, Lung Neoplasms metabolism, Lung Neoplasms pathology, Mice, Prognosis, Reactive Oxygen Species metabolism, Survival Analysis, Treatment Outcome, Xenograft Model Antitumor Assays, Carcinoma, Non-Small-Cell Lung drug therapy, Dicumarol administration & dosage, Enzyme Inhibitors administration & dosage, Lung Neoplasms drug therapy, NAD(P)H Dehydrogenase (Quinone) antagonists & inhibitors

Abstract

Unlabelled: The fundamental role that NAD(P)H/quinone oxidoreductase 1 (NQO1) plays, in normal cells, as a cytoprotective enzyme guarding against stress induced by reactive oxygen species (ROS) is well documented. However, what is not known is whether the observed overexpression of NQO1 in neoplastic cells contributes to their survival. The current study discovered that depleting NQO1 expression in A549 and H292 lung adenocarcinoma cells caused an increase in ROS formation, inhibited anchorage-independent growth, increased anoikis sensitization, and decreased three-dimensional tumor spheroid invasion. These in vivo data further implicate tumor-NQO1 expression in a protumor survival role, because its depletion suppressed cell proliferation and decreased lung tumor xenograft growth. Finally, these data reveal an exploitable link between tumor-NQO1 expression and the survival of lung tumors because NQO1 depletion significantly decreased the percentage of ALDH((high)) cancer cells within the tumor population., Implications: Loss of tumor-NQO1 expression inhibits tumor growth and suggests that novel therapeutics directed at tumor-NQO1 may have clinical benefit., (©2015 American Association for Cancer Research.)

Published

2016

26. Fibulin-5 Blocks Microenvironmental ROS in Pancreatic Cancer.

Author

Wang M, Topalovski M, Toombs JE, Wright CM, Moore ZR, Boothman DA, Yanagisawa H, Wang H, Witkiewicz A, Castrillon DH, and Brekken RA

Subjects

Animals, Carcinoma, Pancreatic Ductal pathology, Cell Line, Tumor, Extracellular Matrix metabolism, Extracellular Matrix pathology, Extracellular Matrix Proteins biosynthesis, Humans, Mice, Mice, Transgenic, Oxidative Stress physiology, Pancreatic Neoplasms pathology, Recombinant Proteins biosynthesis, Tumor Microenvironment physiology, Carcinoma, Pancreatic Ductal metabolism, Extracellular Matrix Proteins metabolism, Pancreatic Neoplasms metabolism, Reactive Oxygen Species metabolism, Recombinant Proteins metabolism

Abstract

Elevated oxidative stress is an aberration seen in many solid tumors, and exploiting this biochemical difference has the potential to enhance the efficacy of anticancer agents. Homeostasis of reactive oxygen species (ROS) is important for normal cell function, but excessive production of ROS can result in cellular toxicity, and therefore ROS levels must be balanced finely. Here, we highlight the relationship between the extracellular matrix and ROS production by reporting a novel function of the matricellular protein Fibulin-5 (Fbln5). We used genetically engineered mouse models of pancreatic ductal adenocarcinoma (PDAC) and found that mutation of the integrin-binding domain of Fbln5 led to decreased tumor growth, increased survival, and enhanced chemoresponse to standard PDAC therapies. Through mechanistic investigations, we found that improved survival was due to increased levels of oxidative stress in Fbln5-mutant tumors. Furthermore, loss of the Fbln5-integrin interaction augmented fibronectin signaling, driving integrin-induced ROS production in a 5-lipooxygenase-dependent manner. These data indicate that Fbln5 promotes PDAC progression by functioning as a molecular rheostat that modulates cell-ECM interactions to reduce ROS production, and thus tip the balance in favor of tumor cell survival and treatment-refractory disease., (©2015 American Association for Cancer Research.)

Published

2015

27. Tumor-selective use of DNA base excision repair inhibition in pancreatic cancer using the NQO1 bioactivatable drug, β-lapachone.

Author

Chakrabarti G, Silvers MA, Ilcheva M, Liu Y, Moore ZR, Luo X, Gao J, Anderson G, Liu L, Sarode V, Gerber DE, Burma S, DeBerardinis RJ, Gerson SL, and Boothman DA

Subjects

Animals, Autophagy drug effects, Catalase genetics, Catalase metabolism, Cell Line, Tumor, Cell Survival drug effects, DNA Breaks, Double-Stranded drug effects, DNA Glycosylases antagonists & inhibitors, DNA Glycosylases metabolism, DNA-Binding Proteins antagonists & inhibitors, DNA-Binding Proteins metabolism, Dicumarol pharmacology, Female, Humans, Hydroxylamines pharmacology, Hydroxylamines therapeutic use, Mice, Mice, Nude, NAD(P)H Dehydrogenase (Quinone) metabolism, Naphthoquinones pharmacology, Naphthoquinones therapeutic use, Pancreatic Neoplasms drug therapy, Pancreatic Neoplasms metabolism, Pancreatic Neoplasms pathology, Poly(ADP-ribose) Polymerases metabolism, Reactive Oxygen Species metabolism, Transplantation, Heterologous, X-ray Repair Cross Complementing Protein 1, DNA Repair drug effects, NAD(P)H Dehydrogenase (Quinone) antagonists & inhibitors

Abstract

Base excision repair (BER) is an essential pathway for pancreatic ductal adenocarcinoma (PDA) survival. Attempts to target this repair pathway have failed due to lack of tumor-selectivity and very limited efficacy. The, Nad(p)h: Quinone Oxidoreductase 1 (NQO1) bioactivatable drug, ß-lapachone (ARQ761 in clinical form), can provide tumor-selective and enhanced synergy with BER inhibition. ß-Lapachone undergoes NQO1-dependent futile redox cycling, generating massive intracellular hydrogen peroxide levels and oxidative DNA lesions that stimulate poly(ADP-ribose) polymerase 1 (PARP1) hyperactivation. Rapid NAD(+)/ATP depletion and programmed necrosis results. To identify BER modulators essential for repair of ß-lapachone-induced DNA base damage, a focused synthetic lethal RNAi screen demonstrated that silencing the BER scaffolding protein, XRCC1, sensitized PDA cells. In contrast, depleting OGG1 N-glycosylase spared cells from ß-lap-induced lethality and blunted PARP1 hyperactivation. Combining ß-lapachone with XRCC1 knockdown or methoxyamine (MeOX), an apyrimidinic/apurinic (AP)-modifying agent, led to NQO1-dependent synergistic killing in PDA, NSCLC, breast and head and neck cancers. OGG1 knockdown, dicoumarol-treatment or NQO1- cancer cells were spared. MeOX + ß-lapachone exposure resulted in elevated DNA double-strand breaks, PARP1 hyperactivation and TUNEL+ programmed necrosis. Combination treatment caused dramatic antitumor activity, enhanced PARP1-hyperactivation in tumor tissue, and improved survival of mice bearing MiaPaca2-derived xenografts, with 33% apparent cures., Significance: Targeting base excision repair (BER) alone has limited therapeutic potential for pancreatic or other cancers due to a general lack of tumor-selectivity. Here, we present a treatment strategy that makes BER inhibition tumor-selective and NQO1-dependent for therapy of most solid neoplasms, particularly for pancreatic cancer.

Published

2015

28. Targeting glutamine metabolism sensitizes pancreatic cancer to PARP-driven metabolic catastrophe induced by ß-lapachone.

Author

Chakrabarti G, Moore ZR, Luo X, Ilcheva M, Ali A, Padanad M, Zhou Y, Xie Y, Burma S, Scaglioni PP, Cantley LC, DeBerardinis RJ, Kimmelman AC, Lyssiotis CA, and Boothman DA

Abstract

Background: Pancreatic ductal adenocarcinomas (PDA) activate a glutamine-dependent pathway of cytosolic nicotinamide adenine dinucleotide phosphate (NADPH) production to maintain redox homeostasis and support proliferation. Enzymes involved in this pathway (GLS1 (mitochondrial glutaminase 1), GOT1 (cytoplasmic glutamate oxaloacetate transaminase 1), and GOT2 (mitochondrial glutamate oxaloacetate transaminase 2)) are highly upregulated in PDA, and among these, inhibitors of GLS1 were recently deployed in clinical trials to target anabolic glutamine metabolism. However, single-agent inhibition of this pathway is cytostatic and unlikely to provide durable benefit in controlling advanced disease., Results: Here, we report that reducing NADPH pools by genetically or pharmacologically (bis-2-(5-phenylacetamido-1,2,4-thiadiazol-2-yl)ethyl sulfide (BPTES) or CB-839) inhibiting glutamine metabolism in mutant Kirsten rat sarcoma viral oncogene homolog (KRAS) PDA sensitizes cell lines and tumors to ß-lapachone (ß-lap, clinical form ARQ761). ß-Lap is an NADPH:quinone oxidoreductase (NQO1)-bioactivatable drug that leads to NADPH depletion through high levels of reactive oxygen species (ROS) from the futile redox cycling of the drug and subsequently nicotinamide adenine dinucleotide (NAD)+ depletion through poly(ADP ribose) polymerase (PARP) hyperactivation. NQO1 expression is highly activated by mutant KRAS signaling. As such, ß-lap treatment concurrent with inhibition of glutamine metabolism in mutant KRAS, NQO1 overexpressing PDA leads to massive redox imbalance, extensive DNA damage, rapid PARP-mediated NAD+ consumption, and PDA cell death-features not observed in NQO1-low, wild-type KRAS expressing cells., Conclusions: This treatment strategy illustrates proof of principle that simultaneously decreasing glutamine metabolism-dependent tumor anti-oxidant defenses and inducing supra-physiological ROS formation are tumoricidal and that this rationally designed combination strategy lowers the required doses of both agents in vitro and in vivo. The non-overlapping specificities of GLS1 inhibitors and ß-lap for PDA tumors afford high tumor selectivity, while sparing normal tissue.

Published

2015

29. Metabolic reprogramming during TGFβ1-induced epithelial-to-mesenchymal transition.

Author

Jiang L, Xiao L, Sugiura H, Huang X, Ali A, Kuro-o M, Deberardinis RJ, and Boothman DA

Subjects

Animals, Carbohydrate Metabolism, Cell Line, Tumor, Cell Movement, Enzyme Repression, Fatty Acid Synthase, Type I genetics, Fatty Acid Synthase, Type I metabolism, Female, Gene Expression, Gene Expression Regulation, Enzymologic, Gene Expression Regulation, Neoplastic, Humans, Lipid Metabolism, Lung Neoplasms metabolism, Lung Neoplasms secondary, Mice, Inbred NOD, Mice, SCID, Neoplasm Transplantation, Snail Family Transcription Factors, Transcription Factors physiology, Epithelial-Mesenchymal Transition, Transforming Growth Factor beta1 physiology

Abstract

Metastatic progression, including extravasation and micrometastatic outgrowth, is the main cause of cancer patient death. Recent studies suggest that cancer cells reprogram their metabolism to support increased proliferation through increased glycolysis and biosynthetic activities, including lipogenesis pathways. However, metabolic changes during metastatic progression, including alterations in regulatory gene expression, remain undefined. We show that transforming growth factor beta 1 (TGFβ1)-induced epithelial-to-mesenchymal transition (EMT) is accompanied by coordinately reduced enzyme expression required to convert glucose into fatty acids, and concomitant enhanced respiration. Overexpressed Snail1, a transcription factor mediating TGFβ1-induced EMT, was sufficient to suppress carbohydrate-responsive-element-binding protein (ChREBP, a master lipogenic regulator), and fatty acid synthase (FASN), its effector lipogenic gene. Stable FASN knockdown was sufficient to induce EMT, stimulate migration and extravasation in vitro. FASN silencing enhanced lung metastasis and death in vivo. These data suggest that a metabolic transition that suppresses lipogenesis and favors energy production is an essential component of TGFβ1-induced EMT and metastasis.

Published

2015

30. NAMPT inhibition sensitizes pancreatic adenocarcinoma cells to tumor-selective, PAR-independent metabolic catastrophe and cell death induced by β-lapachone.

Author

Moore Z, Chakrabarti G, Luo X, Ali A, Hu Z, Fattah FJ, Vemireddy R, DeBerardinis RJ, Brekken RA, and Boothman DA

Subjects

Acrylamides pharmacology, Cell Death drug effects, Cell Line, Tumor, DNA Breaks, Double-Stranded drug effects, Drug Synergism, Energy Metabolism drug effects, Glycolysis drug effects, Humans, NAD(P)H Dehydrogenase (Quinone) metabolism, Nicotinamide Phosphoribosyltransferase metabolism, Pancreatic Neoplasms enzymology, Piperidines pharmacology, Reactive Oxygen Species metabolism, Naphthoquinones pharmacology, Nicotinamide Phosphoribosyltransferase antagonists & inhibitors, Pancreatic Neoplasms metabolism, Pancreatic Neoplasms pathology, Poly Adenosine Diphosphate Ribose metabolism

Abstract

Nicotinamide phosphoribosyltransferase (NAMPT) inhibitors (e.g., FK866) target the most active pathway of NAD(+) synthesis in tumor cells, but lack tumor-selectivity for use as a single agent. Reducing NAD(+) pools by inhibiting NAMPT primed pancreatic ductal adenocarcinoma (PDA) cells for poly(ADP ribose) polymerase (PARP1)-dependent cell death induced by the targeted cancer therapeutic, β-lapachone (β-lap, ARQ761), independent of poly(ADP ribose) (PAR) accumulation. β-Lap is bioactivated by NADPH:quinone oxidoreductase 1 (NQO1) in a futile redox cycle that consumes oxygen and generates high levels of reactive oxygen species (ROS) that cause extensive DNA damage and rapid PARP1-mediated NAD(+) consumption. Synergy with FK866+β-lap was tumor-selective, only occurring in NQO1-overexpressing cancer cells, which is noted in a majority (∼85%) of PDA cases. This treatment strategy simultaneously decreases NAD(+) synthesis while increasing NAD(+) consumption, reducing required doses and treatment times for both drugs and increasing potency. These complementary mechanisms caused profound NAD(P)(+) depletion and inhibited glycolysis, driving down adenosine triphosphate levels and preventing recovery normally observed with either agent alone. Cancer cells died through an ROS-induced, μ-calpain-mediated programmed cell death process that kills independent of caspase activation and is not driven by PAR accumulation, which we call NAD(+)-Keresis. Non-overlapping specificities of FK866 for PDA tumors that rely heavily on NAMPT-catalyzed NAD(+) synthesis and β-lap for cancer cells with elevated NQO1 levels affords high tumor-selectivity. The concept of reducing NAD(+) pools in cancer cells to sensitize them to ROS-mediated cell death by β-lap is a novel strategy with potential application for pancreatic and other types of NQO1+ solid tumors.

Published

2015

31. The cancer cell 'energy grid': TGF-β1 signaling coordinates metabolism for migration.

Author

Jiang L, Deberardinis R, and Boothman DA

Abstract

Cancer cells have an increased reliance on lipogenesis, which is required for uncontrolled cell division. We recently reported transcriptional and functional 'reprogramming' of the cellular energy grid, allowing cancer cells to divert metabolism from biosynthesis to bioenergetic pathways and thus supplying enhanced mobility during epithelial-mesenchymal transition (EMT) induced by transforming growth factor β (TGF-β1) (Fig. 1).

Published

2015

32. EGFR wild type antagonizes EGFRvIII-mediated activation of Met in glioblastoma.

Author

Li L, Puliyappadamba VT, Chakraborty S, Rehman A, Vemireddy V, Saha D, Souza RF, Hatanpaa KJ, Koduru P, Burma S, Boothman DA, and Habib AA

Subjects

Brain Neoplasms drug therapy, Cell Line, Tumor, Dacarbazine analogs & derivatives, Dacarbazine chemistry, Epidermal Growth Factor metabolism, Glioblastoma drug therapy, Humans, Phenotype, Phosphorylation, Receptor Protein-Tyrosine Kinases antagonists & inhibitors, Temozolomide, Brain Neoplasms metabolism, ErbB Receptors metabolism, Gene Expression Regulation, Neoplastic, Glioblastoma metabolism, Proto-Oncogene Proteins c-met metabolism

Abstract

Epidermal growth factor receptor (EGFR)vIII is the most common EGFR mutant found in glioblastoma (GBM). EGFRvIII does not bind ligand, is highly oncogenic and is usually coexpressed with EGFR wild type (EGFRwt). EGFRvIII activates Met, and Met contributes to EGFRvIII-mediated oncogenicity and resistance to treatment. Here, we report that addition of EGF results in a rapid loss of EGFRvIII-driven Met phosphorylation in glioma cells. Met is associated with EGFRvIII in a physical complex. Addition of EGF results in a dissociation of the EGFRvIII-Met complex with a concomitant loss of Met phosphorylation. Consistent with the abrogation of Met activation, addition of EGF results in the inhibition of EGFRvIII-mediated resistance to chemotherapy. Thus, our study suggests that ligand in the milieu of EGFRvIII-expressing GBM cells is likely to influence the EGFRvIII-Met interaction and resistance to treatment, and highlights a novel antagonistic interaction between EGFRwt and EGFRvIII in glioma cells.

Published

2015

33. Constitutive and ligand-induced EGFR signalling triggers distinct and mutually exclusive downstream signalling networks.

Author

Chakraborty S, Li L, Puliyappadamba VT, Guo G, Hatanpaa KJ, Mickey B, Souza RF, Vo P, Herz J, Chen MR, Boothman DA, Pandita TK, Wang DH, Sen GC, and Habib AA

Subjects

Adaptor Proteins, Signal Transducing, Antineoplastic Agents pharmacology, Apoptosis drug effects, Brain Neoplasms genetics, Brain Neoplasms pathology, Carrier Proteins genetics, Carrier Proteins metabolism, Cell Line, Tumor, Epidermal Growth Factor pharmacology, ErbB Receptors genetics, Extracellular Signal-Regulated MAP Kinases genetics, Extracellular Signal-Regulated MAP Kinases metabolism, Glioblastoma genetics, Glioblastoma pathology, Humans, Interferon Regulatory Factor-3 genetics, Interferon Regulatory Factor-3 metabolism, Membrane Proteins genetics, Membrane Proteins metabolism, Phosphorylation drug effects, Primary Cell Culture, Protein Serine-Threonine Kinases genetics, Protein Serine-Threonine Kinases metabolism, Proto-Oncogene Proteins c-akt genetics, Proto-Oncogene Proteins c-akt metabolism, RNA-Binding Proteins, Shc Signaling Adaptor Proteins genetics, Shc Signaling Adaptor Proteins metabolism, TNF-Related Apoptosis-Inducing Ligand genetics, TNF-Related Apoptosis-Inducing Ligand metabolism, Brain Neoplasms metabolism, ErbB Receptors metabolism, Gene Expression Regulation, Neoplastic, Glioblastoma metabolism, Signal Transduction genetics

Abstract

Epidermal growth factor receptor (EGFR) overexpression plays an important oncogenic role in cancer. Regular EGFR protein levels are increased in cancer cells and the receptor then becomes constitutively active. However, downstream signals generated by constitutively activated EGFR are unknown. Here we report that the overexpressed EGFR oscillates between two distinct and mutually exclusive modes of signalling. Constitutive or non-canonical EGFR signalling activates the transcription factor IRF3 leading to expression of IFI27, IFIT1 and TRAIL. Ligand-mediated activation of EGFR switches off IRF3-dependent transcription, activates canonical extracellular signal-regulated kinase (ERK) and Akt signals, and confers sensitivity to chemotherapy and virus-induced cell death. Mechanistically, the distinct downstream signals result from a switch of EGFR-associated proteins. EGFR constitutively complexes with IRF3 and TBK1 leading to TBK1 and IRF3 phosphorylation. Addition of epidermal growth factor dissociates TBK1, IRF3 and EGFR leading to a loss of IRF3 activity, Shc-EGFR association and ERK activation. Finally, we provide evidence for non-canonical EGFR signalling in glioblastoma.

Published

2014

34. An EGFR wild type-EGFRvIII-HB-EGF feed-forward loop regulates the activation of EGFRvIII.

Author

Li L, Chakraborty S, Yang CR, Hatanpaa KJ, Cipher DJ, Puliyappadamba VT, Rehman A, Jiwani AJ, Mickey B, Madden C, Raisanen J, Burma S, Saha D, Wang Z, Pingle SC, Kesari S, Boothman DA, and Habib AA

Subjects

Animals, Cell Line, Tumor, ErbB Receptors genetics, Feedback, Physiological, Gene Expression Regulation, Neoplastic, Heparin-binding EGF-like Growth Factor, Humans, Mice, Mice, Nude, Neoplasm Transplantation, Phosphorylation, Protein Multimerization, Protein Processing, Post-Translational, Transcriptional Activation, Brain Neoplasms metabolism, ErbB Receptors metabolism, Glioblastoma metabolism, Intercellular Signaling Peptides and Proteins physiology

Abstract

EGFRvIII is a key oncogene in glioblastoma (GBM). EGFRvIII results from an in-frame deletion in the extracellular domain of EGFR, does not bind ligand and is thought to be constitutively active. Although EGFRvIII dimerization is known to activate EGFRvIII, the factors that drive EGFRvIII dimerization and activation are not well understood. Here we present a new model of EGFRvIII activation and propose that oncogenic activation of EGFRvIII in glioma cells is driven by co-expressed activated EGFR wild type (EGFRwt). Increasing EGFRwt leads to a striking increase in EGFRvIII tyrosine phosphorylation and activation while silencing EGFRwt inhibits EGFRvIII activation. Both the dimerization arm and the kinase activity of EGFRwt are required for EGFRvIII activation. EGFRwt activates EGFRvIII by facilitating EGFRvIII dimerization. We have previously identified HB-EGF, a ligand for EGFRwt, as a gene induced specifically by EGFRvIII. In this study, we show that HB-EGF is induced by EGFRvIII only when EGFRwt is present. Remarkably, altering HB-EGF recapitulates the effect of EGFRwt on EGFRvIII activation. Thus, increasing HB-EGF leads to a striking increase in EGFRvIII tyrosine phosphorylation while silencing HB-EGF attenuates EGFRvIII phosphorylation, suggesting that an EGFRvIII-HB-EGF-EGFRwt feed-forward loop regulates EGFRvIII activation. Silencing EGFRwt or HB-EGF leads to a striking inhibition of EGFRvIII-induced tumorigenicity, while increasing EGFRwt or HB-EGF levels resulted in accelerated EGFRvIII-mediated oncogenicity in an orthotopic mouse model. Furthermore, we demonstrate the existence of this loop in human GBM. Thus, our data demonstrate that oncogenic activation of EGFRvIII in GBM is likely maintained by a continuous EGFRwt-EGFRvIII-HB-EGF loop, potentially an attractive target for therapeutic intervention.

Published

2014

35. ATM regulates insulin-like growth factor 1-secretory clusterin (IGF-1-sCLU) expression that protects cells against senescence.

Author

Luo X, Suzuki M, Ghandhi SA, Amundson SA, and Boothman DA

Subjects

Cell Line, Clusterin metabolism, DNA Damage, DNA Repair, Humans, MAP Kinase Signaling System, Stress, Physiological, Transcriptional Activation, Ataxia Telangiectasia Mutated Proteins physiology, Cellular Senescence, Clusterin genetics, Insulin-Like Growth Factor I physiology

Abstract

Downstream factors that regulate the decision between senescence and cell death have not been elucidated. Cells undergo senescence through three pathways, replicative senescence (RS), stress-induced premature senescence (SIPS) and oncogene-induced senescence. Recent studies suggest that the ataxia telangiectasia mutant (ATM) kinase is not only a key protein mediating cellular responses to DNA damage, but also regulates cellular senescence induced by telomere end exposure (in RS) or persistent DNA damage (in SIPS). Here, we show that expression of secretory clusterin (sCLU), a known pro-survival extracellular chaperone, is transcriptionally up-regulated during both RS and SIPS, but not in oncogene-induced senescence, consistent with a DNA damage-inducible mechanism. We demonstrate that ATM plays an important role in insulin-like growth factor 1 (IGF-1) expression, that in turn, regulates downstream sCLU induction during senescence. Loss of ATM activity, either by genomic mutation (ATM-deficient fibroblasts from an ataxia telangiectasia patient) or by administration of a chemical inhibitor (AAI, an inhibitor of ATM and ATR), blocks IGF-1-sCLU expression in senescent cells. Downstream, sCLU induction during senescence is mediated by IGF-1R/MAPK/Egr-1 signaling, identical to its induction after DNA damage. In contrast, administration of an IGF-1 inhibitor caused apoptosis of senescent cells. Thus, IGF-1 signaling is required for survival, whereas sCLU appears to protect cells from premature senescence, as IMR-90 cells with sCLU knockdown undergo senescence faster than control cells. Thus, the ATM-IGF-1-sCLU pathway protects cells from lethality and suspends senescence.

Published

2014

36. The transcription factor TFII-I promotes DNA translesion synthesis and genomic stability.

Author

Fattah FJ, Hara K, Fattah KR, Yang C, Wu N, Warrington R, Chen DJ, Zhou P, Boothman DA, and Yu H

Subjects

Cell Line, Tumor, DNA-Binding Proteins biosynthesis, DNA-Directed DNA Polymerase biosynthesis, Genomic Instability, HEK293 Cells, HeLa Cells, Humans, Mad2 Proteins biosynthesis, Mad2 Proteins genetics, Nuclear Proteins biosynthesis, Nucleotidyltransferases biosynthesis, Proliferating Cell Nuclear Antigen biosynthesis, Proliferating Cell Nuclear Antigen metabolism, Transcription Factors, TFII biosynthesis, Transcription Factors, TFII metabolism, DNA Damage genetics, DNA Repair genetics, DNA Replication genetics, Mad2 Proteins metabolism, Transcription Factors, TFII genetics

Abstract

Translesion synthesis (TLS) enables DNA replication through damaged bases, increases cellular DNA damage tolerance, and maintains genomic stability. The sliding clamp PCNA and the adaptor polymerase Rev1 coordinate polymerase switching during TLS. The polymerases Pol η, ι, and κ insert nucleotides opposite damaged bases. Pol ζ, consisting of the catalytic subunit Rev3 and the regulatory subunit Rev7, then extends DNA synthesis past the lesion. Here, we show that Rev7 binds to the transcription factor TFII-I in human cells. TFII-I is required for TLS and DNA damage tolerance. The TLS function of TFII-I appears to be independent of its role in transcription, but requires homodimerization and binding to PCNA. We propose that TFII-I bridges PCNA and Pol ζ to promote TLS. Our findings extend the general principle of component sharing among divergent nuclear processes and implicate TLS deficiency as a possible contributing factor in Williams-Beuren syndrome.

Published

2014

37. Kub5-Hera, the human Rtt103 homolog, plays dual functional roles in transcription termination and DNA repair.

Author

Morales JC, Richard P, Rommel A, Fattah FJ, Motea EA, Patidar PL, Xiao L, Leskov K, Wu SY, Hittelman WN, Chiang CM, Manley JL, and Boothman DA

Subjects

Animals, Antineoplastic Agents toxicity, Cell Cycle Proteins chemistry, Cell Cycle Proteins genetics, Cell Cycle Proteins physiology, Cells, Cultured, DNA Breaks, Double-Stranded, DNA End-Joining Repair, DNA-Binding Proteins, Endonucleases, Genomic Instability, Humans, Mice, Neoplasm Proteins chemistry, Neoplasm Proteins genetics, Neoplasm Proteins physiology, Nuclear Proteins metabolism, Protein Structure, Tertiary, Saccharomyces cerevisiae Proteins genetics, Transcription Factors genetics, Cell Cycle Proteins metabolism, DNA Repair, Neoplasm Proteins metabolism, Transcription Termination, Genetic

Abstract

Functions of Kub5-Hera (In Greek Mythology Hera controlled Artemis) (K-H), the human homolog of the yeast transcription termination factor Rtt103, remain undefined. Here, we show that K-H has functions in both transcription termination and DNA double-strand break (DSB) repair. K-H forms distinct protein complexes with factors that repair DSBs (e.g. Ku70, Ku86, Artemis) and terminate transcription (e.g. RNA polymerase II). K-H loss resulted in increased basal R-loop levels, DSBs, activated DNA-damage responses and enhanced genomic instability. Significantly lowered Artemis protein levels were detected in K-H knockdown cells, which were restored with specific K-H cDNA re-expression. K-H deficient cells were hypersensitive to cytotoxic agents that induce DSBs, unable to reseal complex DSB ends, and showed significantly delayed γ-H2AX and 53BP1 repair-related foci regression. Artemis re-expression in K-H-deficient cells restored DNA-repair function and resistance to DSB-inducing agents. However, R loops persisted consistent with dual roles of K-H in transcription termination and DSB repair.

Published

2014

38. Catalase abrogates β-lapachone-induced PARP1 hyperactivation-directed programmed necrosis in NQO1-positive breast cancers.

Author

Bey EA, Reinicke KE, Srougi MC, Varnes M, Anderson VE, Pink JJ, Li LS, Patel M, Cao L, Moore Z, Rommel A, Boatman M, Lewis C, Euhus DM, Bornmann WG, Buchsbaum DJ, Spitz DR, Gao J, and Boothman DA

Subjects

Breast Neoplasms genetics, Breast Neoplasms pathology, Catalase genetics, Catalase metabolism, DNA Breaks, Single-Stranded drug effects, DNA Damage drug effects, Female, Gene Expression Regulation, Neoplastic drug effects, Humans, Hydrogen Peroxide metabolism, NAD(P)H Dehydrogenase (Quinone) genetics, Necrosis genetics, Necrosis pathology, Poly (ADP-Ribose) Polymerase-1, Reactive Oxygen Species metabolism, Breast Neoplasms drug therapy, NAD(P)H Dehydrogenase (Quinone) metabolism, Naphthoquinones administration & dosage, Poly(ADP-ribose) Polymerases genetics

Abstract

Improving patient outcome by personalized therapy involves a thorough understanding of an agent's mechanism of action. β-Lapachone (clinical forms, Arq501/Arq761) has been developed to exploit dramatic cancer-specific elevations in the phase II detoxifying enzyme NAD(P)H:quinone oxidoreductase (NQO1). NQO1 is dramatically elevated in solid cancers, including primary and metastatic [e.g., triple-negative (ER-, PR-, Her2/Neu-)] breast cancers. To define cellular factors that influence the efficacy of β-lapachone using knowledge of its mechanism of action, we confirmed that NQO1 was required for lethality and mediated a futile redox cycle where ∼120 moles of superoxide were formed per mole of β-lapachone in 2 minutes. β-Lapachone induced reactive oxygen species (ROS), stimulated DNA single-strand break-dependent poly(ADP-ribose) polymerase-1 (PARP1) hyperactivation, caused dramatic loss of essential nucleotides (NAD(+)/ATP), and elicited programmed necrosis in breast cancer cells. Although PARP1 hyperactivation and NQO1 expression were major determinants of β-lapachone-induced lethality, alterations in catalase expression, including treatment with exogenous enzyme, caused marked cytoprotection. Thus, catalase is an important resistance factor and highlights H2O2 as an obligate ROS for cell death from this agent. Exogenous superoxide dismutase enhanced catalase-induced cytoprotection. β-Lapachone-induced cell death included apoptosis-inducing factor (AIF) translocation from mitochondria to nuclei, TUNEL+ staining, atypical PARP1 cleavage, and glyceraldehyde 3-phosphate dehydrogenase S-nitrosylation, which were abrogated by catalase. We predict that the ratio of NQO1:catalase activities in breast cancer versus associated normal tissue are likely to be the major determinants affecting the therapeutic window of β-lapachone and other NQO1 bioactivatable drugs., (©2013 AACR.)

Published

2013

39. The mechanism of DAB2IP in chemoresistance of prostate cancer cells.

Author

Wu K, Xie D, Zou Y, Zhang T, Pong RC, Xiao G, Fazli L, Gleave M, He D, Boothman DA, and Hsieh JT

Subjects

Animals, Cell Line, Tumor, Cell Proliferation drug effects, Clusterin genetics, Docetaxel, Early Growth Response Protein 1 genetics, Gene Expression Regulation, Neoplastic, Humans, Male, Mice, Knockout, Prostatic Neoplasms genetics, Prostatic Neoplasms pathology, Wnt Signaling Pathway drug effects, ras GTPase-Activating Proteins metabolism, Drug Resistance, Neoplasm genetics, Prostatic Neoplasms drug therapy, Taxoids administration & dosage, ras GTPase-Activating Proteins genetics

Abstract

Purpose: The docetaxel-based chemotherapy is the standard of care for castration-resistant prostate cancer (CRPC), inevitably, patients develop resistance and decease. Until now, the mechanism and predictive marker for chemoresistance are poorly understood., Experimental Design: Immortalized normal prostate and cancer cell lines stably manipulated with different DAB2IP expression levels were used and treated with chemotherapeutic drugs commonly used in prostate cancer therapy. Cell proliferation was measured using MTT assay; Western blot, quantitative PCR, and luciferase reporter assays were used to analyze Clusterin gene regulation by DAB2IP. Immunohistochemical analysis was conducted for evaluating DAB2IP, Clusterin and Egr-1 expression in human prostate cancer tissue., Results: DAB2IP Knockdown (KD) cells exhibited resistance to several chemotherapeutic drugs, whereas increased DAB2IP in C4-2 cells restored the drug sensitivity. Parallel, DAB2IP KD cells exhibited higher expression of Clusterin, an antiapoptotic factor, whereas elevated DAB2IP in C4-2 cells decreased Clusterin expression. Functionally, knocking down Clusterin by short-hairpin RNA or antisense oligonucleotide OGX-011 decreased drug resistance, whereas overexpressing Clusterin in C4-2 D2 enhanced drug resistance. Mechanistically, DAB2IP blocked the cross-talk between Wnt/β-catenin and IGF-I signaling, leading to the suppression of Egr-1 that is responsible for Clusterin expression. A similar result was observed in the prostate of DAB2IP knockout animals. In addition, we observed a significantly inverse correlation between DAB2IP and Egr-1 or Clusterin expression from clinical tissue microarray., Conclusions: This study unveils a new regulation of the Egr-1/Clusterin signaling network by DAB2IP. Loss of DAB2IP expression in CRPC cells signifies their chemoresistance. Clusterin is a key target for developing more effective CRPC therapy., (©2013 AACR.)

Published

2013

40. Opposing effect of EGFRWT on EGFRvIII-mediated NF-κB activation with RIP1 as a cell death switch.

Author

Puliyappadamba VT, Chakraborty S, Chauncey SS, Li L, Hatanpaa KJ, Mickey B, Noorani S, Shu HK, Burma S, Boothman DA, and Habib AA

Subjects

Animals, Brain Neoplasms metabolism, Carcinogenesis, Caspase 8 metabolism, Cell Death, Cell Line, Tumor, Fas-Associated Death Domain Protein metabolism, Glioblastoma metabolism, Humans, I-kappa B Kinase metabolism, MAP Kinase Kinase Kinases metabolism, Mice, Mice, Nude, Mutation, Protein Binding, Receptor-Interacting Protein Serine-Threonine Kinases genetics, Signal Transduction, Ubiquitin-Protein Ligases metabolism, ErbB Receptors metabolism, NF-kappa B metabolism, Receptor-Interacting Protein Serine-Threonine Kinases metabolism

Abstract

RIP1 is a central mediator of cell death in response to cell stress but can also mediate cell survival by activating NF-κB. Here, we show that RIP1 acts as a switch in EGFR signaling. EGFRvIII is an oncogenic mutant that does not bind ligand and is coexpressed with EGFRWT in glioblastoma multiforme (GBM). EGFRvIII recruits ubiquitin ligases to RIP1, resulting in K63-linked ubiquitination of RIP1. RIP1 binds to TAK1 and NEMO, forming an EGFRvIII-RIP1 signalosome that activates NF-κB. RIP1 is essential for EGFRvIII-mediated oncogenicity and correlates with NF-κB activation in GBM. Surprisingly, activation of EGFRWT with EGF results in a negative regulation of EGFRvIII, with dissociation of the EGFRvIII-RIP1 signalosome, loss of RIP1 ubiquitination and NF-κB activation, and association of RIP1 with FADD and caspase-8. If EGFRWT is overexpressed with EGFRvIII, the addition of EGF leads to a RIP1 kinase-dependent cell death. The EGFRWT-EGFRvIII-RIP1 interplay may regulate oncogenicity and vulnerability to targeted treatment in GBM., (Copyright © 2013 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2013

41. Cytoplasmic TRADD confers a worse prognosis in glioblastoma.

Author

Chakraborty S, Li L, Tang H, Xie Y, Puliyappadamba VT, Raisanen J, Burma S, Boothman DA, Cochran B, Wu J, and Habib AA

Subjects

Adult, Aged, Antineoplastic Agents, Alkylating pharmacology, Blotting, Western, Brain Neoplasms genetics, Brain Neoplasms pathology, Cell Line, Tumor, Cell Proliferation drug effects, Dacarbazine analogs & derivatives, Dacarbazine pharmacology, Drug Resistance, Neoplasm drug effects, Female, Glioblastoma genetics, Glioblastoma pathology, Humans, Immunohistochemistry, Kaplan-Meier Estimate, Male, Middle Aged, Multivariate Analysis, NF-kappa B metabolism, Neoplastic Stem Cells metabolism, Neoplastic Stem Cells pathology, Prognosis, RNA Interference, TNF Receptor-Associated Death Domain Protein genetics, Temozolomide, Tissue Array Analysis, Brain Neoplasms metabolism, Cytoplasm metabolism, Glioblastoma metabolism, TNF Receptor-Associated Death Domain Protein metabolism

Abstract

Tumor necrosis factor receptor 1 (TNFR1)-associated death domain protein (TRADD) is an important adaptor in TNFR1 signaling and has an essential role in nuclear factor kappa-light-chain-enhancer of activated B cells (NF-κB) activation and survival signaling. Increased expression of TRADD is sufficient to activate NF-κB. Recent studies have highlighted the importance of NF-κB activation as a key pathogenic mechanism in glioblastoma multiforme (GBM), the most common primary malignant brain tumor in adults.We examined the expression of TRADD by immunohistochemistry (IHC) and find that TRADD is commonly expressed at high levels in GBM and is detected in both cytoplasmic and nuclear distribution. Cytoplasmic IHC TRADD scoring is significantly associated with worse progression-free survival (PFS) both in univariate and multivariate analysis but is not associated with overall survival (n = 43 GBMs). PFS is a marker for responsiveness to treatment. We propose that TRADD-mediated NF-κB activation confers chemoresistance and thus a worse PFS in GBM. Consistent with the effect on PFS, silencing TRADD in glioma cells results in decreased NF-κB activity, decreased proliferation of cells, and increased sensitivity to temozolomide. TRADD expression is common in glioma-initiating cells. Importantly, silencing TRADD in GBM-initiating stem cell cultures results in decreased viability of stem cells, suggesting that TRADD may be required for maintenance of GBM stem cell populations. Thus, our study suggests that increased expression of cytoplasmic TRADD is both an important biomarker and a key driver of NF-κB activation in GBM and supports an oncogenic role for TRADD in GBM.

Published

2013

42. Low dose IR-induced IGF-1-sCLU expression: a p53-repressed expression cascade that interferes with TGFβ1 signaling to confer a pro-survival bystander effect.

Author

Klokov D, Leskov K, Araki S, Zou Y, Goetz EM, Luo X, Willson D, and Boothman DA

Subjects

Animals, Apoptosis genetics, Bone Marrow metabolism, Bone Marrow radiation effects, Cell Line, Tumor, Clusterin metabolism, Colon metabolism, Colon radiation effects, Epithelial Cells metabolism, Epithelial Cells pathology, Epithelial Cells radiation effects, Female, HCT116 Cells, Humans, Insulin-Like Growth Factor I metabolism, MCF-7 Cells, Male, Mice, Mice, Transgenic, Molecular Chaperones genetics, Molecular Chaperones metabolism, Promoter Regions, Genetic, Signal Transduction radiation effects, Smad Proteins genetics, Smad Proteins metabolism, Transforming Growth Factor beta1 metabolism, Tumor Suppressor Protein p53 metabolism, Clusterin genetics, Gamma Rays, Insulin-Like Growth Factor I genetics, Transforming Growth Factor beta1 genetics, Tumor Suppressor Protein p53 genetics, Whole-Body Irradiation

Abstract

Inadvertent mammalian tissue exposures to low doses of ionizing radiation (IR) after radiation accidents, remediation of radioactive-contaminated areas, space travel or a dirty bomb represent an interesting trauma to an organism. Possible low-dose IR-induced bystander effects could impact our evaluation of human health effects, as cells within tissue are not equally damaged after doses of IR ≤10 cGy. To understand tissue responses after low IR doses, we generated a reporter system using the human clusterin promoter fused to firefly luciferase (hCLUp-Luc). Secretory clusterin (sCLU), an extracellular molecular chaperone, induced by low doses of cytotoxic agents, clears cell debris. Low-dose IR (≥2 cGy) exposure induced hCLUp-Luc activity with peak levels at 96 h, consistent with endogenous sCLU levels. As doses increased (≥1 Gy), sCLU induction amplitudes increased and time-to-peak response decreased. sCLU expression was stimulated by insulin-like growth factor-1, but suppressed by p53. Responses in transgenic hCLUp-Luc reporter mice after low IR doses showed that specific tissues (that is, colon, spleen, mammary, thymus and bone marrow) of female mice induced hCLUp-Luc activity more than male mice after whole body (≥10 cGy) irradiation. Tissue-specific, non-linear dose- and time-responses of hCLUp-Luc and endogenous sCLU levels were noted. Colon maintained homeostatic balance after 10 cGy. Bone marrow responded with delayed, but prolonged and elevated expression. Intraperitoneal administration of α-transforming growth factor (TGF)β1 (1D11), but not control (13C4) antibodies, immediately following IR exposure abrogated CLU induction responses. Induction in vivo also correlated with Smad signaling by activated TGFβ1 after IR. Mechanistically, media with elevated sCLU levels suppressed signaling, blocked apoptosis and increased survival of TGFβ1-exposed tumor or normal cells. Thus, sCLU is a pro-survival bystander factor that abrogates TGFβ1 signaling and most likely promotes wound healing.

Published

2013

43. Superparamagnetic iron oxide nanoparticles: amplifying ROS stress to improve anticancer drug efficacy.

Author

Huang G, Chen H, Dong Y, Luo X, Yu H, Moore Z, Bey EA, Boothman DA, and Gao J

Subjects

Cell Line, Tumor, Epithelial Cells drug effects, Humans, Molecular Imaging methods, Nanomedicine methods, Oxidative Stress, Reactive Oxygen Species metabolism, Antineoplastic Agents therapeutic use, Ferric Compounds therapeutic use, Magnetics, Molecular Targeted Therapy methods, Nanoparticles therapeutic use, Naphthoquinones therapeutic use, Oxidants therapeutic use

Abstract

Superparamagnetic iron oxide nanoparticles (SPION) are an important and versatile nano- platform with broad biological applications. Despite extensive studies, the biological and pharmacological activities of SPION have not been exploited in therapeutic applications. Recently, β-lapachone (β-lap), a novel anticancer drug, has shown considerable cancer specificity by selectively increasing reactive oxygen species (ROS) stress in cancer cells. In this study, we report that pH-responsive SPION-micelles can synergize with β-lap for improved cancer therapy. These SPION-micelles selectively release iron ions inside cancer cells, which interact with hydrogen peroxide (H(2)O(2)) generated from β-lap in a tumor-specific, NQO1-dependent manner. Through Fenton reactions, these iron ions escalate the ROS stress in β-lap-exposed cancer cells, thereby greatly enhancing the therapeutic index of β-lap. More specifically, a 10-fold increase in ROS stress was detected in β-lap-exposed cells pretreated with SPION-micelles over those treated with β-lap alone, which also correlates with significantly increased cell death. Catalase treatment of cells or administration of an iron chelator can block the therapeutic synergy. Our data suggest that incorporation of SPION-micelles with ROS-generating drugs can potentially improve drug efficacy during cancer treatment, thereby provides a synergistic strategy to integrate imaging and therapeutic functions in the development of theranostic nanomedicine.

Published

2013

44. An NQO1 substrate with potent antitumor activity that selectively kills by PARP1-induced programmed necrosis.

Author

Huang X, Dong Y, Bey EA, Kilgore JA, Bair JS, Li LS, Patel M, Parkinson EI, Wang Y, Williams NS, Gao J, Hergenrother PJ, and Boothman DA

Subjects

Adenosine Triphosphate metabolism, Calcium metabolism, Cell Line, Tumor, DNA Damage drug effects, Egtazic Acid analogs & derivatives, Egtazic Acid pharmacology, Humans, NAD metabolism, NAD(P)H Dehydrogenase (Quinone) genetics, Naphthoquinones pharmacology, Necrosis, Neoplasms metabolism, Neoplasms pathology, Oxidation-Reduction drug effects, Poly (ADP-Ribose) Polymerase-1, Poly(ADP-ribose) Polymerases genetics, RNA Interference, RNA, Small Interfering, Reactive Oxygen Species metabolism, Antineoplastic Agents pharmacology, NAD(P)H Dehydrogenase (Quinone) metabolism, Neoplasms drug therapy, Poly(ADP-ribose) Polymerases metabolism, Quinones pharmacology

Abstract

Agents, such as β-lapachone, that target the redox enzyme, NAD(P)H:quinone oxidoreductase 1 (NQO1), to induce programmed necrosis in solid tumors have shown great promise, but more potent tumor-selective compounds are needed. Here, we report that deoxynyboquinone kills a wide spectrum of cancer cells in an NQO1-dependent manner with greater potency than β-lapachone. Deoxynyboquinone lethality relies on NQO1-dependent futile redox cycling that consumes oxygen and generates extensive reactive oxygen species (ROS). Elevated ROS levels cause extensive DNA lesions, PARP1 hyperactivation, and severe NAD+ /ATP depletion that stimulate Ca2+ -dependent programmed necrosis, unique to this new class of NQO1 "bioactivated" drugs. Short-term exposure of NQO1+ cells to deoxynyboquinone was sufficient to trigger cell death, although genetically matched NQO1- cells were unaffected. Moreover, siRNA-mediated NQO1 or PARP1 knockdown spared NQO1+ cells from short-term lethality. Pretreatment of cells with BAPTA-AM (a cytosolic Ca2+ chelator) or catalase (enzymatic H2O2 scavenger) was sufficient to rescue deoxynyboquinone-induced lethality, as noted with β-lapachone. Investigations in vivo showed equivalent antitumor efficacy of deoxynyboquinone to β-lapachone, but at a 6-fold greater potency. PARP1 hyperactivation and dramatic ATP loss were noted in the tumor, but not in the associated normal lung tissue. Our findings offer preclinical proof-of-concept for deoxynyboquinone as a potent chemotherapeutic agent for treatment of a wide spectrum of therapeutically challenging solid tumors, such as pancreatic and lung cancers.

Published

2012

45. CRM1 protein-mediated regulation of nuclear clusterin (nCLU), an ionizing radiation-stimulated, Bax-dependent pro-death factor.

Author

Leskov KS, Araki S, Lavik JP, Gomez JA, Gama V, Gonos ES, Trougakos IP, Matsuyama S, and Boothman DA

Subjects

Active Transport, Cell Nucleus drug effects, Active Transport, Cell Nucleus genetics, Active Transport, Cell Nucleus radiation effects, Animals, Antibiotics, Antineoplastic pharmacology, Apoptosis drug effects, Apoptosis genetics, Cell Nucleus genetics, Clusterin genetics, Fatty Acids, Unsaturated pharmacology, Humans, Karyopherins genetics, Mice, Mice, Knockout, Protein Isoforms genetics, Protein Isoforms metabolism, Radiation Tolerance drug effects, Radiation Tolerance genetics, Receptors, Cytoplasmic and Nuclear genetics, bcl-2 Homologous Antagonist-Killer Protein genetics, bcl-2 Homologous Antagonist-Killer Protein metabolism, bcl-2-Associated X Protein genetics, Exportin 1 Protein, Apoptosis radiation effects, Cell Nucleus metabolism, Clusterin metabolism, Gamma Rays, Karyopherins metabolism, Receptors, Cytoplasmic and Nuclear metabolism, bcl-2-Associated X Protein metabolism

Abstract

Expression of the clusterin (CLU) gene results in the synthesis of a conventional secretory isoform set (pre- and mature secretory clusterin proteins, psCLU/sCLU), as well as another set of intracellular isoforms, appearing in the cytoplasm (pre-nuclear CLU, pnCLU) and in the nucleus as an ∼55-kDa mature nuclear clusterin (nCLU) form. These two isoform sets have opposing cell functions: pro-survival and pro-death, respectively. Although much is known about the regulation and function of sCLU as a pro-survival factor, the regulation and function of endogenous nCLU in cell death are relatively unexplored. Here, we show that depletion of endogenous nCLU protein using siRNA specific to its truncated mRNA increased clonogenic survival of ionizing radiation (IR)-exposed cells. nCLU-mediated apoptosis was Bax-dependent, and lethality correlated with accumulation of mature nCLU protein. nCLU accumulation was regulated by CRM1 because binding between CRM1 and nCLU proteins was significantly diminished by leptomycin B (LMB), and nuclear levels of nCLU protein were significantly enhanced by LMB and IR co-treatment. Moreover, LMB treatment significantly enhanced IR-induced nCLU-mediated cell death responses. Importantly, bax(-/-) and bax(-/-)/bak(-/-) double knock-out cells were resistant to nCLU-mediated cell death, whereas bak(-/-) or wild-type bax(+/+)/bak(+/+) cells were hypersensitive. The regulation of nCLU by CRM1 nuclear export/import may explain recent clinical results showing that highly malignant tumors have lost the ability to accumulate nCLU levels, thereby avoiding growth inhibition and cell death.

Published

2011

46. Improved protein arrays for quantitative systems analysis of the dynamics of signaling pathway interactions.

Author

Wang X, Dong Y, Jiwani AJ, Zou Y, Pastor J, Kuro-O M, Habib AA, Ruan M, Boothman DA, and Yang CR

Abstract

An improved version of quantitative protein array platform utilizing linear Quantum dot signaling for systematically measuring protein levels and phosphorylation states is presented. The signals are amplified linearly by a confocal laser Quantum dot scanner resulting in ~1000-fold more sensitivity than traditional Western blots, but are not linear by the enzyme-based amplification. Software is developed to facilitate the quantitative readouts of signaling network activities. Kinetics of EGFRvIII mutant signaling was analyzed to quantify cross-talks between EGFR and other signaling pathways.

Published

2011

47. ATM-dependent IGF-1 induction regulates secretory clusterin expression after DNA damage and in genetic instability.

Author

Goetz EM, Shankar B, Zou Y, Morales JC, Luo X, Araki S, Bachoo R, Mayo LD, and Boothman DA

Subjects

Ataxia Telangiectasia Mutated Proteins, CCAAT-Binding Factor metabolism, Cell Cycle Proteins genetics, Cell Line, DNA-Binding Proteins genetics, Humans, Neoplasms pathology, Promoter Regions, Genetic, Protein Serine-Threonine Kinases genetics, Transcription, Genetic, Tumor Suppressor Protein p53 metabolism, Tumor Suppressor Proteins genetics, Cell Cycle Proteins metabolism, Clusterin genetics, DNA Damage, DNA-Binding Proteins metabolism, Gene Expression Regulation, Neoplastic, Genomic Instability, Insulin-Like Growth Factor I genetics, Neoplasms genetics, Protein Serine-Threonine Kinases metabolism, Tumor Suppressor Proteins metabolism

Abstract

Secretory clusterin (sCLU) is a stress-induced, pro-survival glycoprotein elevated in early-stage cancers, in particular in APC/Min-defective colon cancers. sCLU is upregulated after exposure to various cytotoxic agents, including ionizing radiation (IR), leading to a survival advantage. We found that stimulation of insulin-like growth factor-1 (IGF-1) and IGF-1R protein kinase signaling was required for sCLU induction after IR exposure. Here, we show that activation of Ataxia telangiectasia-mutated kinase (ATM) by endogenous or exogenous forms of DNA damage was required to relieve basal repression of IGF-1 transcription by the p53/NF-YA complex, leading to sCLU expression. Although p53 levels were stabilized and elevated after DNA damage, dissociation of NF-YA, and thereby p53, from the IGF-1 promoter resulted in IGF-1 induction, indicating that NF-YA was rate limiting. Cells with elevated endogenous DNA damage (deficient in H2AX, MDC1, NBS1, mTR or hMLH1) or cells exposed to DNA-damaging agents had elevated IGF-1 expression, resulting in activation of IGF-1R signaling and sCLU induction. In contrast, ATM-deficient cells were unable to induce sCLU after DNA damage. Our results integrate DNA damage resulting from genetic instability, IR, or chemotherapeutic agents, to ATM activation and abrogation of p53/NF-YA-mediated IGF-1 transcriptional repression, that induces IGF-1-sCLU expression. Elucidation of this pathway should uncover new mechanisms for cancer progression and reveal new targets for drug development to overcome resistance to therapy.

Published

2011

48. Klotho inhibits transforming growth factor-beta1 (TGF-beta1) signaling and suppresses renal fibrosis and cancer metastasis in mice.

Author

Doi S, Zou Y, Togao O, Pastor JV, John GB, Wang L, Shiizaki K, Gotschall R, Schiavi S, Yorioka N, Takahashi M, Boothman DA, and Kuro-O M

Subjects

Animals, Cell Line, Tumor, Epithelial-Mesenchymal Transition genetics, Fibrosis genetics, Fibrosis metabolism, Fibrosis pathology, Gene Expression Regulation, Neoplastic genetics, Glucuronidase genetics, HEK293 Cells, Humans, Insulin-Like Growth Factor I genetics, Insulin-Like Growth Factor I metabolism, Kidney pathology, Kidney Neoplasms genetics, Kidney Neoplasms pathology, Klotho Proteins, Mice, Neoplasm Metastasis, Neoplasm Transplantation, Neoplasms, Experimental genetics, Neoplasms, Experimental pathology, Protein Serine-Threonine Kinases genetics, Protein Serine-Threonine Kinases metabolism, Rats, Receptor, Transforming Growth Factor-beta Type I, Receptors, Transforming Growth Factor beta genetics, Receptors, Transforming Growth Factor beta metabolism, Transforming Growth Factor beta1 genetics, Transplantation, Heterologous, Wnt Proteins genetics, Wnt Proteins metabolism, Glucuronidase metabolism, Kidney metabolism, Kidney Neoplasms metabolism, Neoplasms, Experimental metabolism, Signal Transduction, Transforming Growth Factor beta1 metabolism

Abstract

Fibrosis is a pathological process characterized by infiltration and proliferation of mesenchymal cells in interstitial space. A substantial portion of these cells is derived from residing non-epithelial and/or epithelial cells that have acquired the ability to migrate and proliferate. The mesenchymal transition is also observed in cancer cells to confer the ability to metastasize. Here, we show that renal fibrosis induced by unilateral ureteral obstruction and metastasis of human cancer xenografts are suppressed by administration of secreted Klotho protein to mice. Klotho is a single-pass transmembrane protein expressed in renal tubular epithelial cells. The extracellular domain of Klotho is secreted by ectodomain shedding. Secreted Klotho protein directly binds to the type-II TGF-β receptor and inhibits TGF-β1 binding to cell surface receptors, thereby inhibiting TGF-β1 signaling. Klotho suppresses TGF-β1-induced epithelial-to-mesenchymal transition (EMT) responses in cultured cells, including decreased epithelial marker expression, increased mesenchymal marker expression, and/or increased cell migration. In addition to TGF-β1 signaling, secreted Klotho has been shown to inhibit Wnt and IGF-1 signaling that can promote EMT. These results have raised the possibility that secreted Klotho may function as an endogenous anti-EMT factor by inhibiting multiple growth factor signaling pathways simultaneously.

Published

2011

49. Modulating endogenous NQO1 levels identifies key regulatory mechanisms of action of β-lapachone for pancreatic cancer therapy.

Author

Li LS, Bey EA, Dong Y, Meng J, Patra B, Yan J, Xie XJ, Brekken RA, Barnett CC, Bornmann WG, Gao J, and Boothman DA

Subjects

Animals, Antineoplastic Agents pharmacology, Cell Death, Cell Line, Tumor, DNA Damage, Drug Evaluation, Preclinical, Gene Knockdown Techniques, Humans, Mice, Mice, Nude, Naphthoquinones therapeutic use, Pancreatic Neoplasms enzymology, Reactive Oxygen Species metabolism, Antineoplastic Agents therapeutic use, NAD(P)H Dehydrogenase (Quinone) metabolism, Naphthoquinones pharmacology, Pancreatic Neoplasms drug therapy

Abstract

Purpose: Pancreatic cancer is the fourth leading cause of cancer-related deaths, in which the 5-year survival rate is less than 5%. Current standard of care therapies offer little selectivity and high toxicity. Novel, tumor-selective approaches are desperately needed. Although prior work suggested that β-lapachone (β-lap) could be used for the treatment of pancreatic cancers, the lack of knowledge of the compound's mechanism of action prevented optimal use of this agent., Experimental Design: We examined the role of NAD(P)H:quinone oxidoreductase-1 (NQO1) in β-lap-mediated antitumor activity, using a series of MIA PaCa-2 pancreatic cancer clones varying in NQO1 levels by stable shRNA knockdown. The antitumor efficacy of β-lap was determined using an optimal hydroxypropyl-β-cyclodextran (HPβ-CD) vehicle formulation in metastatic pancreatic cancer models., Results: β-Lap-mediated cell death required ∼90 enzymatic units of NQO1. Essential downstream mediators of lethality were as follows: (i) reactive oxygen species (ROS); (ii) single-strand DNA breaks induced by ROS; (iii) poly(ADP-ribose)polymerase-1 (PARP1) hyperactivation; (iv) dramatic NAD(+)/ATP depletion; and (v) programmed necrosis. We showed that 1 regimen of β-lap therapy (5 treatments every other day) efficaciously regressed and reduced human pancreatic tumor burden and dramatically extended the survival of athymic mice, using metastatic pancreatic cancer models., Conclusions: Because NQO1 enzyme activities are easily measured and commonly overexpressed (i.e., >70%) in pancreatic cancers 5- to 10-fold above normal tissue, strategies using β-lap to efficaciously treat pancreatic cancers are indicated. On the basis of optimal drug formulation and efficacious antitumor efficacy, such a therapy should be extremely safe and not accompanied with normal tissue toxicity or hemolytic anemia., (©2011 AACR.)

Published

2011

50. Prostate cancer radiosensitization through poly(ADP-Ribose) polymerase-1 hyperactivation.

Author

Dong Y, Bey EA, Li LS, Kabbani W, Yan J, Xie XJ, Hsieh JT, Gao J, and Boothman DA

Subjects

Animals, Apoptosis, Cell Death, Colony-Forming Units Assay, Comet Assay, DNA Damage, DNA, Neoplasm genetics, Dicumarol pharmacology, Enzyme Activation, Enzyme Inhibitors pharmacology, Glutathione metabolism, Humans, In Situ Nick-End Labeling, Male, Mice, Mice, Nude, Naphthoquinones therapeutic use, Poly (ADP-Ribose) Polymerase-1, Poly(ADP-ribose) Polymerases genetics, Poly(ADP-ribose) Polymerases radiation effects, Prostatic Neoplasms drug therapy, Prostatic Neoplasms enzymology, Prostatic Neoplasms genetics, Prostatic Neoplasms pathology, Radiation-Sensitizing Agents therapeutic use, Regression Analysis, Poly(ADP-ribose) Polymerases metabolism

Abstract

The clinical experimental agent, β-lapachone (β-lap; Arq 501), can act as a potent radiosensitizer in vitro through an unknown mechanism. In this study, we analyzed the mechanism to determine whether β-lap may warrant clinical evaluation as a radiosensitizer. β-Lap killed prostate cancer cells by NAD(P)H:quinone oxidoreductase 1 (NQO1) metabolic bioactivation, triggering a massive induction of reactive oxygen species, irreversible DNA single-strand breaks (SSB), poly(ADP-ribose) polymerase-1 (PARP-1) hyperactivation, NAD(+)/ATP depletion, and μ-calpain-induced programmed necrosis. In combination with ionizing radiation (IR), β-lap radiosensitized NQO1(+) prostate cancer cells under conditions where nontoxic doses of either agent alone achieved threshold levels of SSBs required for hyperactivation of PARP-1. Combination therapy significantly elevated SSB level, γ-H2AX foci formation, and poly(ADP-ribosylation) of PARP-1, which were associated with ATP loss and induction of μ-calpain-induced programmed cell death. Radiosensitization by β-lap was blocked by the NQO1 inhibitor dicoumarol or the PARP-1 inhibitor DPQ. In a mouse xenograft model of prostate cancer, β-lap synergized with IR to promote antitumor efficacy. NQO1 levels were elevated in ∼60% of human prostate tumors evaluated relative to adjacent normal tissue, where β-lap might be efficacious alone or in combination with radiation. Our findings offer a rationale for the clinical utilization of β-lap (Arq 501) as a radiosensitizer in prostate cancers that overexpress NQO1, offering a potentially synergistic targeting strategy to exploit PARP-1 hyperactivation., (©2010 AACR.)

Published

2010