Your search keyword '"Andrey Ugolkov"' showing total 68 results

1. VISTA expression and patient selection for immune-based anticancer therapy

Author

Alexander S. Martin, Michael Molloy, Andrey Ugolkov, Reinhard W. von Roemeling, Randolph J. Noelle, Lionel D. Lewis, Melissa Johnson, Laszlo Radvanyi, and Robert E. Martell

Subjects

VISTA, immune checkpoint, cancer, biomarkers, cancer immunotherapy, tumor immunity, Immunologic diseases. Allergy, RC581-607

Abstract

V-domain Ig suppressor of T-cell activation (VISTA) is a B7 family member that plays key roles in maintaining T cell quiescence and regulation of myeloid cell populations, which together establish it as a novel immunotherapy target for solid tumors. Here we review the growing literature on VISTA expression in relation to various malignancies to better understand the role of VISTA and its interactions with both tumor cells and immune cells expressing other checkpoint molecules within the tumor microenvironment (TME). The biology of VISTA creates several mechanisms to maintain the TME, including supporting the function of myeloid-derived suppressor cells, regulating natural killer cell activation, supporting the survival of regulatory T cells, limiting antigen presentation on antigen-presenting cells and maintaining T cells in a quiescent state. Understanding these mechanisms is an important foundation of rational patient selection for anti-VISTA therapy. We provide a general framework to describe distinct patterns of VISTA expression in correlation with other known predictive immunotherapy biomarkers (programmed cell death ligand 1 and tumor-infiltrating lymphocytes) across solid tumors to facilitate investigation of the most efficacious TMEs for VISTA-targeted treatment as a single agent and/or in combination with anti-programmed death 1/anti-cytotoxic T lymphocyte antigen-4 therapies.

Published

2023

2. 9-ING-41, a small molecule inhibitor of GSK-3beta, potentiates the effects of anticancer therapeutics in bladder cancer

Author

Hiroo Kuroki, Tsutomu Anraku, Akira Kazama, Vladimir Bilim, Masayuki Tasaki, Daniel Schmitt, Andrew P. Mazar, Francis J Giles, Andrey Ugolkov, and Yoshihiko Tomita

Subjects

Medicine, Science

Abstract

Abstract Glycogen synthase kinase-3 beta (GSK-3β), a serine/threonine kinase, has been identified as a potential therapeutic target in human bladder cancer. In the present study, we investigated the antitumor effect of a small molecule GSK-3β inhibitor, 9-ING-41, currently in clinical studies in patients with advanced cancer, in bladder cancer cell lines. We found that treatment with 9-ING-41 leads to cell cycle arrest, autophagy and apoptosis in bladder cancer cells. The autophagy inhibitor chloroquine potentiated the antitumor effects of 9-ING-41 when tested in combination studies. Our findings also demonstrate that 9-ING-41 enhanced the growth inhibitory effects of gemcitabine or cisplatin when used in combination in bladder cancer cells. Finally, we found that 9-ING-41 sensitized bladder cancer cells to the cytotoxic effects of human immune effector cells. Our results provide a rationale for the inclusion of patients with advanced bladder cancer in clinical studies of 9-ING-41.

Published

2019

3. Combination Treatment with the GSK-3 Inhibitor 9-ING-41 and CCNU Cures Orthotopic Chemoresistant Glioblastoma in Patient-Derived Xenograft Models

Author

Andrey Ugolkov, Wenan Qiang, Gennadiy Bondarenko, Daniel Procissi, Irina Gaisina, C. David James, James Chandler, Alan Kozikowski, Hendra Gunosewoyo, Thomas O'Halloran, Jeffrey Raizer, and Andrew P. Mazar

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Resistance to chemotherapy remains a major challenge in the treatment of human glioblastoma (GBM). Glycogen synthase kinase-3β (GSK-3β), a positive regulator of NF-κB–mediated survival and chemoresistance of cancer cells, has been identified as a potential therapeutic target in human GBM. Our objective was to determine the antitumor effect of GSK-3 inhibitor 9-ING-41 in combination with chemotherapy in patient-derived xenograft (PDX) models of human GBM. We utilized chemoresistant PDX models of GBM, GBM6 and GBM12, to study the effect of 9-ING-41 used alone and in combination with chemotherapy on tumor progression and survival. GBM6 and GBM12 were transfected by reporter constructs to enable bioluminescence imaging, which was used to stage animals prior to treatment and to follow intracranial GBM tumor growth. Immunohistochemical staining, apoptosis assay, and immunoblotting were used to assess the expression of GSK-3β and the effects of treatment in these models. We found that 9-ING-41 significantly enhanced 1-(2-chloroethyl)-3-cyclohexyl-1-nitrosourea (CCNU) antitumor activity in staged orthotopic GBM12 (no response to CCNU) and GBM6 (partial response to CCNU) PDX models, as indicated by a decrease in tumor bioluminescence in mouse brain and a significant increase in overall survival. Treatment with the combination of CCNU and 9-ING-41 resulted in histologically confirmed cures in these studies. Our results demonstrate that the GSK-3 inhibitor 9-ING-41, a clinical candidate currently in Investigational New Drug (IND)-enabling development, significantly enhances the efficacy of CCNU therapy for human GBM and warrants consideration for clinical evaluation in this difficult-to-treat patient population.

Published

2017

4. Patient-Derived Tumor Xenografts Are Susceptible to Formation of Human Lymphocytic Tumors

Author

Gennadiy Bondarenko, Andrey Ugolkov, Stephen Rohan, Piotr Kulesza, Oleksii Dubrovskyi, Demirkan Gursel, Jeremy Mathews, Thomas V. O’Halloran, Jian J. Wei, and Andrew P. Mazar

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Patient-derived xenograft (PDX) tumor models have emerged as a new approach to evaluate the effects of cancer drugs on patients’ personalized tumor grafts enabling to select the best treatment for the cancer patient and providing a new tool for oncology drug developers. Here, we report that human tumors engrafted in immunodeficient mice are susceptible to formation of B-and T-cell PDX tumors. We xenografted human primary and metastatic tumor samples into immunodeficient mice and found that a fraction of PDX tumors generated from patients’ samples of breast, colon, pancreatic, bladder and renal cancer were histologically similar to lymphocytic neoplasms. Moreover, we found that the first passage of breast and pancreatic cancer PDX tumors after initial transplantation of the tumor pieces from the same human tumor graft could grow as a lymphocytic tumor in one mouse and as an adenocarcinoma in another mouse. Whereas subcutaneous PDX tumors resembling human adenocarcinoma histology were slow growing and non-metastatic, we found that subcutaneous PDX lymphocytic tumors were fast growing and formed large metastatic lesions in mouse lymph nodes, liver, lungs, and spleen. PDX lymphocytic tumors were comprised of B-cells which were Epstein-Barr virus positive and expressed CD45 and CD20. Because B-cells are typically present in malignant solid tumors, formation of B-cell tumor may evolve in a wide range of PDX tumor models. Although PDX tumor models show great promise in the development of personalized therapy for cancer patients, our results suggest that confidence in any given PDX tumor model requires careful screening of lymphocytic markers.

Published

2015

5. Identification of a new epitope in uPAR as a target for the cancer therapeutic monoclonal antibody ATN-658, a structural homolog of the uPAR binding integrin CD11b (αM).

Author

Xiang Xu, Yuan Cai, Ying Wei, Fernando Donate, Jose Juarez, Graham Parry, Liqing Chen, Edward J Meehan, Richard W Ahn, Andrey Ugolkov, Oleksii Dubrovskyi, Thomas V O'Halloran, Mingdong Huang, and Andrew P Mazar

Subjects

Medicine, Science

Abstract

The urokinase plasminogen activator receptor (uPAR) plays a role in tumor progression and has been proposed as a target for the treatment of cancer. We recently described the development of a novel humanized monoclonal antibody that targets uPAR and has anti-tumor activity in multiple xenograft animal tumor models. This antibody, ATN-658, does not inhibit ligand binding (i.e. uPA and vitronectin) to uPAR and its mechanism of action remains unclear. As a first step in understanding the anti-tumor activity of ATN-658, we set out to identify the epitope on uPAR to which ATN-658 binds. Guided by comparisons between primate and human uPAR, epitope mapping studies were performed using several orthogonal techniques. Systematic site directed and alanine scanning mutagenesis identified the region of aa 268-275 of uPAR as the epitope for ATN-658. No known function has previously been attributed to this epitope Structural insights into epitope recognition were obtained from structural studies of the Fab fragment of ATN-658 bound to uPAR. The structure shows that the ATN-658 binds to the DIII domain of uPAR, close to the C-terminus of the receptor, corroborating the epitope mapping results. Intriguingly, when bound to uPAR, the complementarity determining region (CDR) regions of ATN-658 closely mimic the binding regions of the integrin CD11b (αM), a previously identified uPAR ligand thought to be involved in leukocyte rolling, migration and complement fixation with no known role in tumor progression of solid tumors. These studies reveal a new functional epitope on uPAR involved in tumor progression and demonstrate a previously unrecognized strategy for the therapeutic targeting of uPAR.

Published

2014

6. Nwani et al., Supplementary figures 1-11 from Melanoma Cells Block PEDF Production in Fibroblasts to Induce the Tumor-Promoting Phenotype of Cancer-Associated Fibroblasts

Author

Olga V. Volpert, Andrew P. Mazar, Andrey Ugolkov, Oleksii Dubrovskyi, Elena Vinokour, Benilde Jimenez, Maria L. Deguiz, and Nkechiyere G. Nwani

Abstract

Supplemental Figure 1. Verification of PEDF knockdown Supplemental Figure 2. Verification of PEDF silencing in fibroblasts Supplemental Figure 3. The effect of PEDF expression in fibroblasts on tumor growth Supplemental Figure 4. The effect of endogenous PEDF on fibroblast proliferation and recruitment Supplemental Figure 5. The effect of exogenous TGFb and PDGF on PEDF mRNA in fibroblasts Supplemental Figure 6. The contribution of of TGFb and PDGF to PEDF repression assessed by shRNA silencing Supplemental Figure 7. The effect of TGFb on PDGFR mRNA levels Supplemental Figure 8. Regulation of PDGFB mRNA by TGFb Supplemental Figure 9. The role of PI3K in PEDF control by PDGF-BB Supplemental Figure 10. Inhibition of non-canonical TGFb signaling by PEDF Supplemental Figure 11. Altered expression of select genes in PEDF-null fibroblasts

Published

2023

7. Supplementary Figures 1 - 5, Tables 1 - 4 from αB-Crystallin: A Novel Regulator of Breast Cancer Metastasis to the Brain

Author

Vincent L. Cryns, Carey K. Anders, Eric V. Shusta, Lisa Carey, Matt Ewend, Joseph Geradts, Kimberly Blackwell, Erika Hamilton, Karen Fritchie, Chad Livasy, Andrey Ugolkov, C. Ryan Miller, Barbara Adamo, Abraham Al Ahmad, Allison M. Deal, Vladimir Petrovic, Elena Strekalova, and Dmitry Malin

Abstract

PDF file - 797K, Figure S1. Barrier phenotype of human brain microvascular endothelial cells and astrocytes in monocultures and co-cultures. Figure S2. alpha/beta-crystallin does not affect cell viability of TNBC cells in standard monolayer culture. Figure S3. alpha/beta-crystallin overexpression increases liver metastases in an orthotopic model of TNBC. Figure S4. Silencing alpha/beta-crystallin inhibits liver metastases in an orthotopic model of TNBC. Figure S5. alpha/beta-crystallin does not affect proliferation or apoptosis in primary mammary tumors and brain metastatic lesions determined at autopsy. Table S1. Patient characteristics Table S2. alpha/beta-crystallin expression in paired tumors. Table S3. Association of alpha/beta-crystallin expression with breast cancer subtype. Table S4. Incidence of metastases in mice in orthotopic models of TNBC .

Published

2023

8. Supplemental Figure Legends from Glycogen Synthase Kinase-3β: A Prognostic Marker and a Potential Therapeutic Target in Human Bladder Cancer

Author

Yoshihiko Tomita, Tomoyuki Kato, Akira Nagaoka, Teiichi Motoyama, Andrey Ugolkov, Kaori Yuuki, Vladimir Bilim, and Sei Naito

Abstract

Supplemental Figure Legends

Published

2023

9. Data from Melanoma Cells Block PEDF Production in Fibroblasts to Induce the Tumor-Promoting Phenotype of Cancer-Associated Fibroblasts

Author

Olga V. Volpert, Andrew P. Mazar, Andrey Ugolkov, Oleksii Dubrovskyi, Elena Vinokour, Benilde Jimenez, Maria L. Deguiz, and Nkechiyere G. Nwani

Abstract

Loss of pigment epithelium-derived factor (PEDF, SERPINF1) in cancer cells is associated with poor prognosis and metastasis, but the contribution of stromal PEDF to cancer evolution is poorly understood. Therefore, we investigated the role of fibroblast-derived PEDF in melanoma progression. We demonstrate that normal dermal fibroblasts expressing high PEDF levels attenuated melanoma growth and angiogenesis in vivo, whereas PEDF-depleted fibroblasts exerted tumor-promoting effects. Accordingly, mice with global PEDF knockout were more susceptible to melanoma metastasis. We also demonstrate that normal fibroblasts in close contact with PEDF-null melanoma cells lost PEDF expression and tumor-suppressive properties. Further mechanistic investigations underlying the crosstalk between tumor and stromal cells revealed that melanoma cells produced PDGF-BB and TGFβ, which blocked PEDF production in fibroblasts. Notably, cancer-associated fibroblasts (CAF) isolated from patient-derived tumors expressed markedly low levels of PEDF. Treatment of patient CAF and TGFβ-treated normal fibroblasts with exogenous PEDF decreased the expression of CAF markers and restored PEDF expression. Finally, expression profiling of PEDF-depleted fibroblasts revealed induction of IL8, SERPINB2, hyaluronan synthase-2, and other genes associated with tumor promotion and metastasis. Collectively, our results demonstrate that PEDF maintains tumor-suppressive functions in fibroblasts to prevent CAF conversion and illustrate the mechanisms by which melanoma cells silence stromal PEDF to promote malignancy. Cancer Res; 76(8); 2265–76. ©2016 AACR.

Published

2023

10. Data from Whole-body Imaging of Cell Death Provides a Systemic, Minimally Invasive, Dynamic, and Near-real Time Indicator for Chemotherapeutic Drug Toxicity

Author

Ming Zhao, Andrew Mazar, Thomas V. O'Halloran, Andy Tran, Raymond Bergan, Emily A. Waters, Lin Li, Gennadiy Bondarenko, Chad R. Haney, Andrey Ugolkov, and Steven E. Johnson

Abstract

Purpose:Response to toxicity in chemotherapies varies considerably from tissue to tissue and from patient to patient. An ability to monitor the tissue damage done by chemotherapy may have a profound impact on treatment and prognosis allowing for a proactive management in understanding and mitigating such events. For the first time, we investigated the feasibility of using whole-body imaging to map chemotherapeutic drug–induced toxicity on an individual basis.Experimental Design:In a preclinical proof-of-concept, rats were treated with a single clinical dose of cyclophosphamide, methotrexate, or cisplatin. In vivo whole-body imaging data were acquired using 99mTc-duramycin, which identifies dead and dying cells as an unambiguous marker for tissue injury in susceptible organs. Imaging results were cross-validated using quantitative ex vivo measurements and histopathology and compared with standard blood and serum panels for toxicology.Results:The in vivo whole-body imaging data detected widespread changes, where spatially heterogeneous toxic effects were identified across different tissues, within substructures of organs, as well as among different individuals. The signal changes were consistent with established toxicity profiles of these chemotherapeutic drugs. Apart from generating a map of susceptible tissues, this in vivo imaging approach was more sensitive compared with conventional blood and serum markers used in toxicology. Also, repeated imaging during the acute period after drug treatment captured different kinetics of tissue injury among susceptible organs in males and females.Conclusions:This novel and highly translational imaging approach shows promise in optimizing therapeutic decisions by detecting and managing drug toxicity on a personalized basis.Toxicity to normal tissues is a significant limitation in chemotherapies. This work demonstrated an in vivo imaging-based approach for characterizing toxicity-induced tissue injury in a systemic, dynamic, and near-real time fashion. This novel approach shows promise in optimizing therapeutic decisions by monitoring drug toxicity on a personalized basis.

Published

2023

11. Data from αB-Crystallin: A Novel Regulator of Breast Cancer Metastasis to the Brain

Author

Vincent L. Cryns, Carey K. Anders, Eric V. Shusta, Lisa Carey, Matt Ewend, Joseph Geradts, Kimberly Blackwell, Erika Hamilton, Karen Fritchie, Chad Livasy, Andrey Ugolkov, C. Ryan Miller, Barbara Adamo, Abraham Al Ahmad, Allison M. Deal, Vladimir Petrovic, Elena Strekalova, and Dmitry Malin

Abstract

Purpose: Basal-like breast tumors are typically (ER/PR/HER2) triple-negative and are associated with a high incidence of brain metastases and poor clinical outcomes. The molecular chaperone αB-crystallin is predominantly expressed in triple-negative breast cancer (TNBC) and contributes to an aggressive tumor phenotype in preclinical models. We investigated the potential role of αB-crystallin in brain metastasis in TNBCs.Experimental Design: αB-crystallin expression in primary breast carcinomas and brain metastases was analyzed by immunohistochemistry among patients with breast cancer with brain metastases. αB-crystallin was overexpressed or silenced in two different TNBC cell lines. The effects on cell adhesion to human brain microvascular endothelial cells (HBMEC) or extracellular matrix proteins, transendothelial migration, and transmigration across a HBMEC/astrocyte coculture blood–brain barrier (BBB) model were examined. In addition, the effects of overexpressing or silencing αB-crystallin on brain metastasis in vivo were investigated using orthotopic TNBC models.Results: In a cohort of women with breast cancer brain metastasis, αB-crystallin expression in primary breast carcinomas was associated with poor overall survival and poor survival after brain metastasis, even among patients with TNBC. Stable overexpression of αB-crystallin in TNBC cells enhanced adhesion to HBMECs, transendothelial migration, and BBB transmigration in vitro, whereas silencing αB-crystallin inhibited these events. αB-crystallin promoted adhesion of TNBC cells to HBMECs, at least in part, through an α3β1 integrin–dependent mechanism. αB-crystallin overexpression promoted brain metastasis, whereas silencing αB-crystallin inhibited brain metastasis in orthotopic TNBC models.Conclusion: αB-crystallin is a novel regulator of brain metastasis in TNBC and represents a potential biomarker and drug target for this aggressive disease. Clin Cancer Res; 20(1); 56–67. ©2013 AACR.

Published

2023

12. Supplemental Figures from Glycogen Synthase Kinase-3β: A Prognostic Marker and a Potential Therapeutic Target in Human Bladder Cancer

Author

Yoshihiko Tomita, Tomoyuki Kato, Akira Nagaoka, Teiichi Motoyama, Andrey Ugolkov, Kaori Yuuki, Vladimir Bilim, and Sei Naito

Abstract

Supplemental Figure 1. Immunohistochemical staining of GSK-3β in low (A-C) and high (D-F) grade urothelial tumors. Supplemental Figure 2. Hoechst staining of T24 cancer cells treated with 3 distinct small molecule inhibitors of GSK-3 (AR-A014418, SB-415286, and TDZD-8). The arrows point at apoptotic cells. The percentage of apoptotic cells is shown as indicated on each picture. Supplemental Figure 3. HT1376 and T24 cancer cells were treated with indicated doses of AR-A014418; 48, 72 and 96 h after treatment, cell lysates were separated by SDS-PAGE, transferred to PVDF membrane and probed with antibodies to indicated proteins.

Published

2023

13. Nwani et al, Supplementary figure legends from Melanoma Cells Block PEDF Production in Fibroblasts to Induce the Tumor-Promoting Phenotype of Cancer-Associated Fibroblasts

Author

Olga V. Volpert, Andrew P. Mazar, Andrey Ugolkov, Oleksii Dubrovskyi, Elena Vinokour, Benilde Jimenez, Maria L. Deguiz, and Nkechiyere G. Nwani

Abstract

Legends for supplementary figures

Published

2023

14. Supplementary Tables from Whole-body Imaging of Cell Death Provides a Systemic, Minimally Invasive, Dynamic, and Near-real Time Indicator for Chemotherapeutic Drug Toxicity

Author

Ming Zhao, Andrew Mazar, Thomas V. O'Halloran, Andy Tran, Raymond Bergan, Emily A. Waters, Lin Li, Gennadiy Bondarenko, Chad R. Haney, Andrey Ugolkov, and Steven E. Johnson

Abstract

supplementary Tables

Published

2023

15. Development of patient‑derived tumor organoids and a drug testing model for renal cell carcinoma

Author

Yuko Shirono, Masaki Murata, Vladimir Bilim, Hiroo Kuroki, Tsutomu Anraku, Akira Kazama, Yoshihiko Tomita, Kazuhide Saito, and Andrey Ugolkov

Subjects

renal cell carcinoma, Cancer Research, Cabozantinib, precision medicine, tumor organoid, urologic and male genital diseases, Pazopanib, chemistry.chemical_compound, Renal cell carcinoma, Cell Line, Tumor, Humans, Medicine, Viability assay, Carcinoma, Renal Cell, Protein Kinase Inhibitors, personalized therapy, business.industry, Sunitinib, Receptor Protein-Tyrosine Kinases, Cancer, Articles, General Medicine, medicine.disease, female genital diseases and pregnancy complications, Organoids, Axitinib, Oncology, chemistry, Cancer research, business, Ex vivo, medicine.drug

Abstract

The selection of effective therapeutic agents is critical for improving the survival of patients with renal cell carcinoma (RCC). The aim of the present study was to develop an ex vivo drug testing assay using patient-derived tumor organoid (TO) cultures. For this purpose, surgical tumor specimens were obtained from 20 patients with RCC. TOs were developed ex vivo from freshly resected RCC tumors, and their histopathological and molecular characteristics were evaluated using histological staining and whole-exome sequencing (WES). Using a cell viability assay, the therapeutic efficacy of standard of care tyrosine kinase inhibitors in RCC TOs was determined. It was found that TOs recapitulated the histological features of primary RCC tumors. Using WES, a strong concordance was identified at the genetic level between the primary tumors and their corresponding TOs. Using patient-derived TO models, a prototype of an ex vivo drug testing assay was developed, and it was found that RCC TOs exhibited differential responses to sunitinib, pazopanib, cabozantinib, axitinib and sorafenib treatment. On the whole, although the predictive value of the current assay has to be tested and validated in future clinical studies, the findings of the present study demonstrate a novel approach for ex vivo drug testing in patient-derived TO models, which may have potential for use in the personalized treatment of cancer patients.

Published

2021

16. Correction: Glycogen Synthase Kinase-3 Inhibition Sensitizes Pancreatic Cancer Cells to Chemotherapy by Abrogating the TopBP1/ATR-mediated DNA Damage Response

Author

Li, Ding, Vijay S, Madamsetty, Spencer, Kiers, Olga, Alekhina, Andrey, Ugolkov, John, Dube, Yu, Zhang, Jin-San, Zhang, Enfeng, Wang, Shamit K, Dutta, Daniel M, Schmitt, Francis J, Giles, Alan P, Kozikowski, Andrew P, Mazar, Debabrata, Mukhopadhyay, and Daniel D, Billadeau

Subjects

Article

Abstract

PURPOSE: Pancreatic ductal adenocarcinoma (PDAC) is a predominantly fatal common malignancy with inadequate treatment options. Glycogen synthase kinase 3β (GSK-3β) is an emerging target in human malignancies including PDAC. EXPERIMENTAL DESIGN: Pancreatic cancer cell lines and patient-derived xenografts were treated with a novel GSK-3 inhibitor 9-ING-41 alone or in combination with chemotherapy. Activation of the DNA damage response pathway and S-phase arrest induced by gemcitabine were assessed in pancreatic tumor cells with pharmacologic inhibition or siRNA depletion of GSK-3 kinases by immunoblotting, flow cytometry and immunofluorescence. RESULTS: 9-ING-41 treatment significantly increased pancreatic tumor cell killing when combined with chemotherapy. Inhibition of GSK-3 by 9-ING-41 prevented gemcitabine-induced S-phase arrest suggesting an impact on the ATR-mediated DNA damage response. Both 9-ING-41 and siRNA depletion of GSK-3 kinases impaired the activation of ATR leading to the phosphorylation and activation of Chk1. Mechanistically, depletion or knockdown of GSK-3 kinases resulted in the degradation of the ATR-interacting protein TopBP1, thus limiting the activation of ATR in response to single-strand DNA damage. CONCLUSIONS: These data identify a previously unknown role for GSK-3 kinases in the regulation of the TopBP1/ATR/Chk1 DNA damage response pathway. The data also support the inclusion of patients with PDAC in clinical studies of 9-ING-41 alone and in combination with gemcitabine.

Published

2021

17. Glycogen Synthase Kinase-3 Inhibition Sensitizes Pancreatic Cancer Cells to Chemotherapy by Abrogating the TopBP1/ATR-Mediated DNA Damage Response

Author

Shamit K. Dutta, Debabrata Mukhopadhyay, Andrey Ugolkov, Francis J. Giles, Vijay Sagar Madamsetty, Li Ding, Andrew P. Mazar, Daniel Schmitt, Enfeng Wang, John R. Dube, Daniel D. Billadeau, Olga Alekhina, Spencer Kiers, Alan P. Kozikowski, Yu Zhang, and Jin San Zhang

Subjects

0301 basic medicine, Cancer Research, Indoles, DNA damage, Apoptosis, Ataxia Telangiectasia Mutated Proteins, Adenocarcinoma, Deoxycytidine, Maleimides, Mice, 03 medical and health sciences, 0302 clinical medicine, Pancreatic tumor, GSK-3, Cell Line, Tumor, Pancreatic cancer, medicine, Animals, Humans, CHEK1, Phosphorylation, Protein Kinase Inhibitors, Cell Proliferation, Glycogen Synthase Kinase 3 beta, Kinase, Chemistry, Nuclear Proteins, Flow Cytometry, medicine.disease, Gemcitabine, DNA-Binding Proteins, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Cell killing, Oncology, 030220 oncology & carcinogenesis, Checkpoint Kinase 1, Cancer research, Carrier Proteins, Carcinoma, Pancreatic Ductal, DNA Damage, Signal Transduction, medicine.drug

Abstract

Purpose: Pancreatic ductal adenocarcinoma (PDAC) is a predominantly fatal common malignancy with inadequate treatment options. Glycogen synthase kinase 3β (GSK-3β) is an emerging target in human malignancies including PDAC. Experimental Design: Pancreatic cancer cell lines and patient-derived xenografts were treated with a novel GSK-3 inhibitor 9-ING-41 alone or in combination with chemotherapy. Activation of the DNA damage response pathway and S-phase arrest induced by gemcitabine were assessed in pancreatic tumor cells with pharmacologic inhibition or siRNA depletion of GSK-3 kinases by immunoblotting, flow cytometry, and immunofluorescence. Results: 9-ING-41 treatment significantly increased pancreatic tumor cell killing when combined with chemotherapy. Inhibition of GSK-3 by 9-ING-41 prevented gemcitabine-induced S-phase arrest suggesting an impact on the ATR-mediated DNA damage response. Both 9-ING-41 and siRNA depletion of GSK-3 kinases impaired the activation of ATR leading to the phosphorylation and activation of Chk1. Mechanistically, depletion or knockdown of GSK-3 kinases resulted in the degradation of the ATR-interacting protein TopBP1, thus limiting the activation of ATR in response to single-strand DNA damage. Conclusions: These data identify a previously unknown role for GSK-3 kinases in the regulation of the TopBP1/ATR/Chk1 DNA damage response pathway. The data also support the inclusion of patients with PDAC in clinical studies of 9-ING-41 alone and in combination with gemcitabine.

Published

2019

18. Whole-body Imaging of Cell Death Provides a Systemic, Minimally Invasive, Dynamic, and Near-real Time Indicator for Chemotherapeutic Drug Toxicity

Author

Emily A. Waters, Andrey Ugolkov, Raymond C. Bergan, Gennadiy Bondarenko, Andrew P. Mazar, Lin Li, Steven E. Johnson, Ming Zhao, Andy Tran, Chad R. Haney, and Thomas V. O'Halloran

Subjects

0301 basic medicine, Cancer Research, Drug-Related Side Effects and Adverse Reactions, Cyclophosphamide, medicine.medical_treatment, Whole body imaging, Apoptosis, Bioinformatics, Article, 03 medical and health sciences, 0302 clinical medicine, Bacteriocins, In vivo, Neoplasms, medicine, Animals, Humans, Whole Body Imaging, Chemotherapy, Cell Death, business.industry, Organotechnetium Compounds, Rats, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Toxicity, Methotrexate, Cisplatin, business, Preclinical imaging, Ex vivo, medicine.drug

Abstract

Purpose: Response to toxicity in chemotherapies varies considerably from tissue to tissue and from patient to patient. An ability to monitor the tissue damage done by chemotherapy may have a profound impact on treatment and prognosis allowing for a proactive management in understanding and mitigating such events. For the first time, we investigated the feasibility of using whole-body imaging to map chemotherapeutic drug–induced toxicity on an individual basis. Experimental Design: In a preclinical proof-of-concept, rats were treated with a single clinical dose of cyclophosphamide, methotrexate, or cisplatin. In vivo whole-body imaging data were acquired using 99mTc-duramycin, which identifies dead and dying cells as an unambiguous marker for tissue injury in susceptible organs. Imaging results were cross-validated using quantitative ex vivo measurements and histopathology and compared with standard blood and serum panels for toxicology. Results: The in vivo whole-body imaging data detected widespread changes, where spatially heterogeneous toxic effects were identified across different tissues, within substructures of organs, as well as among different individuals. The signal changes were consistent with established toxicity profiles of these chemotherapeutic drugs. Apart from generating a map of susceptible tissues, this in vivo imaging approach was more sensitive compared with conventional blood and serum markers used in toxicology. Also, repeated imaging during the acute period after drug treatment captured different kinetics of tissue injury among susceptible organs in males and females. Conclusions: This novel and highly translational imaging approach shows promise in optimizing therapeutic decisions by detecting and managing drug toxicity on a personalized basis. Toxicity to normal tissues is a significant limitation in chemotherapies. This work demonstrated an in vivo imaging-based approach for characterizing toxicity-induced tissue injury in a systemic, dynamic, and near-real time fashion. This novel approach shows promise in optimizing therapeutic decisions by monitoring drug toxicity on a personalized basis.

Published

2019

19. Aberrant expression of glycogen synthase kinase-3β in human breast and head and neck cancer

Author

Vincent L. Cryns, Thomas V. O'Halloran, Timothy Taxter, Andrew P. Mazar, Andrey Ugolkov, Maria Matsangou, and Francis J. Giles

Subjects

0301 basic medicine, Cancer Research, macromolecular substances, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, breast cancer, GSK-3, expression, Medicine, Oncogene, business.industry, Head and neck cancer, Cancer, Articles, Cell cycle, medicine.disease, Molecular medicine, 3. Good health, nuclear, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer research, Immunohistochemistry, head and neck cancer, business

Abstract

Glycogen Synthase Kinase-3β (GSK-3β), a serine/threonine protein kinase, has been implicated as a potential therapeutic target in human cancer. The objective of the present study was to evaluate aberrant expression of GSK-3β as a potential biomarker in human breast and head and neck cancers. Nuclear/cytosolic fractionation, immunoblotting and immunohistochemical staining was used to study the expression of GSK-3β in human breast and head and neck cancer. Aberrant nuclear accumulation of GSK-3β in five human breast cancer cell lines was demonstrated and in 89/128 (70%) human breast carcinomas, whereas no detectable expression of GSK-3β was found in benign breast tissue. Nuclear GSK-3β expression was associated with HER-2 positive tumors (P=0.02) and non-triple negative breast carcinomas (P=0.0001), although nuclear GSK-3β was observed in some samples across all breast cancer subtypes. Aberrant nuclear expression of GSK-3β was found in 11/15 (73%) squamous cell head and neck carcinomas, whereas weak or no detectable expression of GSK-3β was found in benign salivary gland and other benign head and neck tissues. These results support the hypothesis that aberrant nuclear GSK-3β may represent a potential target for the clinical treatment of human breast and squamous cell carcinoma.

Published

2018

20. Abstract 385: Identification of NF-kappaB phospho-p50 as a predictive biomarker for IRAK4 inhibitor CA-4948 in patients with non-Hodgkin's lymphoma

Author

Rosanna Hok, Robert E. Martell, Andrey Ugolkov, Maria Samson, and Reinhard von Roemeling

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Chemotherapy, business.industry, medicine.medical_treatment, Phases of clinical research, Cancer, medicine.disease, Lymphoma, Non-Hodgkin's lymphoma, Clinical trial, Internal medicine, medicine, Biomarker (medicine), business, Progressive disease

Abstract

Background: IRAK4, a serine/threonine kinase, was identified as a therapeutic target in hematological malignancies. IRAK4-mediated activation of NF-kappaB could play an important role in NF-kappaB-regulated survival and chemoresistance of cancer cells. CA-4948, a first-in-class small molecule inhibitor of IRAK4, has been tested in Phase 1 clinical trial with evidence of clinical activity in Non-Hodgkin's Lymphoma (NHL) patients. To support the development of companion diagnostic for CA-4948, we developed an immunohistochemical (IHC) assay and explored expression of potential biomarkers of response to CA-4948 in tumor biopsy samples obtained from NHL patients. Materials and Methods: IHC assay was developed and used for analysis of NF-kappaB p-p50 and p-IRAK1 expression in tumor biopsy samples obtained from 14 patients with NHL. Patients were defined according to their clinical response to CA-4948 treatment: stable disease (SD), 6 cases and progressive disease (PD), 8 cases. Results: We found nuclear and/or cytoplasmic expression of NF-kappaB p-p50 in all 6 SD cases treated with 50 mg QD (2 cases, tumor regression), 50 mg BID (1 case), 200 mg BID (1 case, tumor regression) and 400 mg BID (2 cases). Expression of NF-kappaB p-p50 was not detected in 7 of 8 cases with PD including patients treated with 50 mg QD (1 case), 100 mg QD (1 case), 100 mg BID (3 cases), 200 mg BID (1 case) and 400 mg BID (1 case). We found statistically significant correlation between expression of NF-kappaB p-p50 in tumor biopsy and SD in NHL patients treated with CA-4948 (p Conclusions: Although the cohort size is small, our findings suggest that expression of NF-kappaB p-p50 can serve as biomarker to predict SD in response to the treatment with IRAK4 inhibitor CA-4948 in NHL patients. NF-kappaB p-p50 selection strategy might be used in future clinical trials to identify NHL patients which are most likely to respond to CA-4948 in combination with chemotherapy or targeted therapeutics. Citation Format: Andrey Ugolkov, Maria Samson, Rosanna Hok, Reinhard von Roemeling, Robert Martell. Identification of NF-kappaB phospho-p50 as a predictive biomarker for IRAK4 inhibitor CA-4948 in patients with non-Hodgkin's lymphoma [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2021; 2021 Apr 10-15 and May 17-21. Philadelphia (PA): AACR; Cancer Res 2021;81(13_Suppl):Abstract nr 385.

Published

2021

21. GSK-3β inhibitor, 9-ING-41, reduces cell viability and halts proliferation of B-cell lymphoma cell lines as a single agent and in combination with novel agents

Author

Leo I. Gordon, Jeffrey A. Borgia, Francis J. Giles, Andrew P. Mazar, Andrey Ugolkov, Reem Karmali, and Vineela Chukkapalli

Subjects

0301 basic medicine, Cell, CDK9 inhibitor, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Myc+ Lymphoma, medicine, Viability assay, B-cell lymphoma, PI3K/AKT/mTOR pathway, Venetoclax, medicine.disease, Bcl-2 inhibitor, Lymphoma, 030104 developmental biology, medicine.anatomical_structure, Oncology, chemistry, Apoptosis, DLBCL, 030220 oncology & carcinogenesis, Cancer research, Idelalisib, GSK-3β inhibitor, Research Paper

Abstract

The complexities of GSK-3β function and interactions with PI3K/AKT/mTOR signaling, cell cycling, and apoptotic pathways are poorly understood in the context of lymphomagenesis and cancer therapeutics. In this study, we explored the anti-tumor effects of the GSK-3β inhibitor, 9-ING-41, in lymphoma cell lines as a single agent and in combination with novel agents comprising BCL-2 inhibitor (Venetoclax), CDK-9 inhibitor (BAY-1143572) and p110δ-PI3K inhibitor (Idelalisib). Treatment of Daudi, SUDHL-4, Karpas 422, KPUM-UH1, and TMD8 lymphoma cell lines with 1 μM 9-ING-41 reduced cell viability by 40-70% (p

Published

2017

22. Macrogenomic engineering via modulation of the scaling of chromatin packing density

Author

Shohreh Shahabi, Vadim Backman, Di Zhang, Daniel D. Billadeau, Greta M. Bauer, Thomas V. O'Halloran, Igal Szleifer, Andrew P. Mazar, Hemant K. Roy, Wenli Wu, David VanDerway, Alexis Kendra, Lusik Cherkezyan, John E. Chandler, Luay M. Almassalha, Scott Gladstein, Andrey Ugolkov, and Brandon Luke L. Seagle

Subjects

0301 basic medicine, Transcriptional activity, Chemistry, Biomedical Engineering, Medicine (miscellaneous), Bioengineering, Article, Computer Science Applications, Chromatin, Cell biology, 03 medical and health sciences, 030104 developmental biology, Physical structure, Modulation, Gene expression, Cancer cell, Genomic information, Gene, Biotechnology

Abstract

Many human diseases result from the dysregulation of the complex interactions between tens to thousands of genes. However, approaches for the transcriptional modulation of many genes simultaneously in a predictive manner are lacking. Here, through the combination of simulations, systems modelling and in vitro experiments, we provide a physical regulatory framework based on chromatin packing-density heterogeneity for modulating the genomic information space. Because transcriptional interactions are essentially chemical reactions, they depend largely on the local physical nanoenvironment. We show that the regulation of the chromatin nanoenvironment allows for the predictable modulation of global patterns in gene expression. In particular, we show that the rational modulation of chromatin density fluctuations can lead to a decrease in global transcriptional activity and intercellular transcriptional heterogeneity in cancer cells during chemotherapeutic responses to achieve near-complete cancer cell killing in vitro. Our findings represent a ‘macrogenomic engineering’ approach to modulating the physical structure of chromatin for whole-scale transcriptional modulation.

Published

2017

23. Combination Treatment with the GSK-3 Inhibitor 9-ING-41 and CCNU Cures Orthotopic Chemoresistant Glioblastoma in Patient-Derived Xenograft Models

Author

Daniel Procissi, Gennadiy Bondarenko, Hendra Gunosewoyo, C. David James, Andrew P. Mazar, Jeffrey Raizer, Irina N. Gaisina, James P. Chandler, Thomas V. O'Halloran, Andrey Ugolkov, Wenan Qiang, and Alan P. Kozikowski

Subjects

0301 basic medicine, Cancer Research, Chemotherapy, Pathology, medicine.medical_specialty, business.industry, medicine.medical_treatment, Transfection, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, lcsh:RC254-282, 3. Good health, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Oncology, GSK-3, Apoptosis, Tumor progression, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, medicine, Bioluminescence imaging, Immunohistochemistry, business

Abstract

Resistance to chemotherapy remains a major challenge in the treatment of human glioblastoma (GBM). Glycogen synthase kinase-3β (GSK-3β), a positive regulator of NF-κB-mediated survival and chemoresistance of cancer cells, has been identified as a potential therapeutic target in human GBM. Our objective was to determine the antitumor effect of GSK-3 inhibitor 9-ING-41 in combination with chemotherapy in patient-derived xenograft (PDX) models of human GBM. We utilized chemoresistant PDX models of GBM, GBM6 and GBM12, to study the effect of 9-ING-41 used alone and in combination with chemotherapy on tumor progression and survival. GBM6 and GBM12 were transfected by reporter constructs to enable bioluminescence imaging, which was used to stage animals prior to treatment and to follow intracranial GBM tumor growth. Immunohistochemical staining, apoptosis assay, and immunoblotting were used to assess the expression of GSK-3β and the effects of treatment in these models. We found that 9-ING-41 significantly enhanced 1-(2-chloroethyl)-3-cyclohexyl-1-nitrosourea (CCNU) antitumor activity in staged orthotopic GBM12 (no response to CCNU) and GBM6 (partial response to CCNU) PDX models, as indicated by a decrease in tumor bioluminescence in mouse brain and a significant increase in overall survival. Treatment with the combination of CCNU and 9-ING-41 resulted in histologically confirmed cures in these studies. Our results demonstrate that the GSK-3 inhibitor 9-ING-41, a clinical candidate currently in Investigational New Drug (IND)-enabling development, significantly enhances the efficacy of CCNU therapy for human GBM and warrants consideration for clinical evaluation in this difficult-to-treat patient population.

Published

2017

24. Molecular Pathways: Revisiting Glycogen Synthase Kinase-3β as a Target for the Treatment of Cancer

Author

Benedito A. Carneiro, Alan P. Kozikowski, Francis J. Giles, Sunandana Chandra, Daniel D. Billadeau, Thomas V. O'Halloran, Amy L. Walz, Andrew P. Mazar, and Andrey Ugolkov

Subjects

0301 basic medicine, Cancer Research, Regulator, Antineoplastic Agents, Inflammation, macromolecular substances, Biology, Article, 03 medical and health sciences, 0302 clinical medicine, GSK-3, Neoplasms, medicine, Animals, Humans, Molecular Targeted Therapy, Protein kinase A, Glycogen synthase, Protein Kinase Inhibitors, Glycogen Synthase Kinase 3 beta, Kinase, Cancer, medicine.disease, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer cell, Immunology, Cancer research, biology.protein, medicine.symptom

Abstract

Glycogen synthase kinase-3β (GSK-3β), a serine/threonine protein kinase, is a complex regulator of numerous cellular functions. GSK-3β is a unique kinase which is constitutively active in resting and nonstimulated cells. GSK-3β has been implicated in a wide range of diseases including neurodegeneration, inflammation and fibrosis, noninsulin-dependent diabetes mellitus, and cancer. It is a regulator of NF-κB–mediated survival of cancer cells, which provided a rationale for the development of GSK-3 inhibitors targeting malignant tumors. Recent studies, many of them reported over the past decade, have identified GSK-3β as a potential therapeutic target in more than 15 different types of cancer. Whereas only active GSK-3β is expressed in cancer cell nucleus, aberrant nuclear accumulation of GSK-3β has been identified as a hallmark of cancer cells in malignant tumors of different origin. This review focuses on the preclinical and clinical development of GSK-3 inhibitors and the potential therapeutic impact of targeting GSK-3β in human cancer. Clin Cancer Res; 23(8); 1891–7. ©2017 AACR.

Published

2017

25. 9-ING-41, a small molecule inhibitor of GSK-3beta, potentiates the effects of anticancer therapeutics in bladder cancer

Author

Francis J. Giles, Yoshihiko Tomita, Daniel Schmitt, Vladimir Bilim, Hiroo Kuroki, Akira Kazama, Masayuki Tasaki, Tsutomu Anraku, Andrey Ugolkov, and Andrew P. Mazar

Subjects

0301 basic medicine, Indoles, Cell Survival, Science, Urology, Antineoplastic Agents, Article, Maleimides, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, medicine, Autophagy, Cytotoxic T cell, Humans, Protein Kinase Inhibitors, Cancer, Cell Proliferation, Cisplatin, Multidisciplinary, Bladder cancer, Glycogen Synthase Kinase 3 beta, business.industry, Kinase, Drug Synergism, Cell Cycle Checkpoints, medicine.disease, Gemcitabine, 030104 developmental biology, Oncology, Urinary Bladder Neoplasms, Apoptosis, 030220 oncology & carcinogenesis, Cancer research, Medicine, business, medicine.drug

Abstract

Glycogen synthase kinase-3 beta (GSK-3β), a serine/threonine kinase, has been identified as a potential therapeutic target in human bladder cancer. In the present study, we investigated the antitumor effect of a small molecule GSK-3β inhibitor, 9-ING-41, currently in clinical studies in patients with advanced cancer, in bladder cancer cell lines. We found that treatment with 9-ING-41 leads to cell cycle arrest, autophagy and apoptosis in bladder cancer cells. The autophagy inhibitor chloroquine potentiated the antitumor effects of 9-ING-41 when tested in combination studies. Our findings also demonstrate that 9-ING-41 enhanced the growth inhibitory effects of gemcitabine or cisplatin when used in combination in bladder cancer cells. Finally, we found that 9-ING-41 sensitized bladder cancer cells to the cytotoxic effects of human immune effector cells. Our results provide a rationale for the inclusion of patients with advanced bladder cancer in clinical studies of 9-ING-41.

Published

2019

26. Invasion, metastasis, and tumour dormancy

Author

Andrew P. Mazar and Andrey Ugolkov

Subjects

fungi, Cancer research, Invasion metastasis, Biology, Tumour dormancy

Abstract

Tumours can be either benign or malignant. A first difference is that the primary malignant tumour infiltrates the surrounding tissue while, with very few exceptions, the benign tumours do not infiltrate. The second and main one is that, by definition, the malignant tumours are able to produce metastatic lesions in other organs. Finally, metastases can declare themselves even after period of years from the appearance of the first lesion. This is because of the third property of the malignant cells i.e. their ability to spread and then do not immediately grow into a detectable metastasis, but to be ‘dormant’ for a variable period.

Published

2019

27. GSK-3 inhibition overcomes chemoresistance in human breast cancer

Author

Kevin P. White, Sarika Jain, Andrew P. Mazar, Daniel D. Billadeau, Thomas V. O'Halloran, Vincent L. Cryns, Jin San Zhang, Francis J. Giles, Irina N. Gaisina, Andrey Ugolkov, Massimo Cristofanilli, and Alan P. Kozikowski

Subjects

0301 basic medicine, Cancer Research, Indoles, Time Factors, Cell Survival, Breast Neoplasms, Mice, SCID, Irinotecan, Article, Maleimides, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, Mice, Inbred NOD, GSK-3, Cell Line, Tumor, Antineoplastic Combined Chemotherapy Protocols, Tumor Cells, Cultured, Animals, Humans, Medicine, Molecular Targeted Therapy, Protein Kinase Inhibitors, GSK3B, Protein kinase B, Cell Proliferation, Glycogen Synthase Kinase 3 beta, Dose-Response Relationship, Drug, business.industry, Cancer, medicine.disease, Antineoplastic Agents, Phytogenic, Xenograft Model Antitumor Assays, Metastatic breast cancer, Tumor Burden, 030104 developmental biology, Oncology, Drug Resistance, Neoplasm, Drug Design, 030220 oncology & carcinogenesis, Cancer research, Camptothecin, Female, business, Signal Transduction, medicine.drug

Abstract

Glycogen Synthase Kinase-3β (GSK-3β), a serine/threonine protein kinase, is an emerging therapeutic target in the treatment of human breast cancer. In this study, we demonstrate that the pharmacological inhibition of GSK-3 by two novel small molecule GSK-3 inhibitors, 9-ING-41 and 9-ING-87, reduced the viability of breast cancer cells but had little effect on non-tumorigenic cell growth. Moreover, treatment with 9-ING-41 enhanced the antitumor effect of irinotecan (CPT-11) against breast cancer cells in vitro. We next established two patient-derived xenograft tumor models (BC-1 and BC-2) from metastatic pleural effusions obtained from patients with progressive, chemorefractory breast cancer and demonstrated that 9-ING-41 also potentiated the effect of the chemotherapeutic drug CPT-11 in vivo, leading to regression of established BC-1 and BC-2 tumors in mice. Our results suggest that the inhibition of GSK-3 is a promising therapeutic approach to overcome chemoresistance in human breast cancer, and identify the GSK-3 inhibitor 9-ING-41 as a candidate targeted agent for metastatic breast cancer therapy.

Published

2016

28. Melanoma Cells Block PEDF Production in Fibroblasts to Induce the Tumor-Promoting Phenotype of Cancer-Associated Fibroblasts

Author

Elena Vinokour, María Laura Deguiz, Andrew P. Mazar, Nkechiyere G. Nwani, Benilde Jiménez, Oleksii Dubrovskyi, Olga V. Volpert, Andrey Ugolkov, Baskes Family Foundation, National Cancer Institute (US), and Ministerio de Economía y Competitividad (España)

Subjects

0301 basic medicine, Cancer Research, Stromal cell, Angiogenesis, Mice, Nude, Biology, Article, Metastasis, Mice, 03 medical and health sciences, 0302 clinical medicine, PEDF, Transforming Growth Factor beta, Cell Line, Tumor, medicine, Animals, Humans, Nerve Growth Factors, Eye Proteins, Melanoma, Serpins, Cell Proliferation, Mice, Inbred BALB C, Fibroblasts, medicine.disease, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, Cancer-Associated Fibroblasts, Tumor promotion

Abstract

PMCID: PMC4873437.-- et al., Loss of pigment epithelium-derived factor (PEDF, SERPINF1) in cancer cells is associated with poor prognosis and metastasis, but the contribution of stromal PEDF to cancer evolution is poorly understood. Therefore, we investigated the role of fibroblast-derived PEDF in melanoma progression. We demonstrate that normal dermal fibroblasts expressing high PEDF levels attenuated melanoma growth and angiogenesis in vivo, whereas PEDF-depleted fibroblasts exerted tumor-promoting effects. Accordingly, mice with global PEDF knockout were more susceptible to melanoma metastasis. We also demonstrate that normal fibroblasts in close contact with PEDF-null melanoma cells lost PEDF expression and tumor-suppressive properties. Further mechanistic investigations underlying the crosstalk between tumor and stromal cells revealed that melanoma cells produced PDGF-BB and TGFb, which blocked PEDF production in fibroblasts. Notably, cancer-associated fibroblasts (CAF) isolated from patient-derived tumors expressed markedly low levels of PEDF. Treatment of patient CAF and TGFβ-treated normal fibroblasts with exogenous PEDF decreased the expression of CAF markers and restored PEDF expression. Finally, expression profiling of PEDF-depleted fibroblasts revealed induction of IL8, SERPINB2, hyaluronan synthase-2, and other genes associated with tumor promotion and metastasis. Collectively, our results demonstrate that PEDF maintains tumor-suppressive functions in fibroblasts to prevent CAF conversion and illustrate the mechanisms by which melanoma cells silence stromal PEDF to promote malignancy., This study was funded by the following grants: T32 Carcinogenesis Training grant CA60013828 (N.G. Nwani), NCI R01 CA172669 (O.V. Volpert), and SAF2014-53819-R grant from Ministerio de Ciencia y Competitividad of Spain (B. Jimenez). A.P. Mazar, A. Ugolkov, and O. Dubrovskyi were supported by the Baskes Family Research Fund.

Published

2016

29. GSK-3ß INHIBITOR, 9-ING-41 REDUCES CELL VIABILITY AND HALTS PROLIFERATION OF B-CELL LYMPHOMA

Author

Vineela Chukkapalli, Jeffrey A. Borgia, Andrew P. Mazar, Barbara Pro, Andrey Ugolkov, Reem Karmali, and Francis J. Giles

Subjects

Cancer Research, Oncology, Chemistry, Cancer research, medicine, Hematology, General Medicine, Viability assay, B-cell lymphoma, medicine.disease

Published

2017

30. Human Organoids Share Structural and Genetic Features with Primary Pancreatic Adenocarcinoma Tumors

Author

Mary M. Buschmann, Kori Kirby, Hedy L. Kindler, Andrew P. Mazar, Yilin Zhang, Wenan Qiang, Mohana Ray, Ralph R. Weichselbaum, Christopher R. Weber, Miguel Brown, Tiha M. Long, Jeremy P. Segal, Samantha M. Sparrow, Andrey Rzhetsky, Tonya M. Brunetti, Isabel Romero Calvo, Kevin P. White, Andrey Ugolkov, Rajib K. Nandi, and Kevin K. Roggin

Subjects

0301 basic medicine, Cancer Research, FOLFIRINOX, Biology, Adenocarcinoma, Article, Transcriptome, 03 medical and health sciences, Mice, 0302 clinical medicine, In vivo, medicine, Organoid, Animals, Humans, Molecular Biology, Genetic heterogeneity, medicine.disease, Precision medicine, Primary tumor, Organoids, Pancreatic Neoplasms, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer research

Abstract

Patient-derived pancreatic ductal adenocarcinoma (PDAC) organoid systems show great promise for understanding the biological underpinnings of disease and advancing therapeutic precision medicine. Despite the increased use of organoids, the fidelity of molecular features, genetic heterogeneity, and drug response to the tumor of origin remain important unanswered questions limiting their utility. To address this gap in knowledge, primary tumor- and patient-derived xenograft (PDX)-derived organoids, and 2D cultures for in-depth genomic and histopathologic comparisons with the primary tumor were created. Histopathologic features and PDAC representative protein markers (e.g., claudin 4 and CA19-9) showed strong concordance. DNA- and RNA-sequencing (RNAseq) of single organoids revealed patient-specific genomic and transcriptomic consistency. Single-cell RNAseq demonstrated that organoids are primarily a clonal population. In drug response assays, organoids displayed patient-specific sensitivities. In addition, the in vivo PDX response to FOLFIRINOX and gemcitabine/abraxane treatments were examined, which was recapitulated in vitro with organoids. This study has demonstrated that organoids are potentially invaluable for precision medicine as well as preclinical drug treatment studies because they maintain distinct patient phenotypes and respond differently to drug combinations and dosage. Implications: The patient-specific molecular and histopathologic fidelity of organoids indicate that they can be used to understand the etiology of the patient's tumor and the differential response to therapies and suggests utility for predicting drug responses.

Published

2018

31. Pancreatic adenocarcinoma human organoids share structural and genetic features with primary tumors

Author

Andrey Rzhetsky, Mohana Ray, Wenan Qiang, Kevin K. Roggin, Ralph R. Weichselbaum, Rajib K. Nandi, Jeremy P. Segal, Andrew P. Mazar, Andrey Ugolkov, Miguel Brown, Kevin P. White, Hedy L. Kindler, Isabel Romero Calvo, Tiha M. Long, Kori Kirby, Samantha M. Sparrow, Christopher R. Weber, Yilin Zhang, Mary M. Buschmann, and Tonya M. Brunetti

Subjects

0303 health sciences, FOLFIRINOX, Genetic heterogeneity, Biology, medicine.disease, Precision medicine, Primary tumor, 3. Good health, Transcriptome, 03 medical and health sciences, 0302 clinical medicine, In vivo, 030220 oncology & carcinogenesis, Organoid, medicine, Cancer research, Adenocarcinoma, 030304 developmental biology

Abstract

Patient-derived pancreatic ductal adenocarcinoma (PDAC) organoid systems show great promise for understanding the biological underpinnings of disease and advancing therapeutic precision medicine. Despite the increased use of organoids, the fidelity of molecular features, genetic heterogeneity, and drug response to the tumor of origin remain important unanswered questions limiting their utility. To address this gap in knowledge, we created primary tumor- and PDX-derived organoids, and 2D cultures for in-depth genomic and histopathological comparisons to the primary tumor. Histopathological features and PDAC representative protein markers showed strong concordance. DNA and RNA sequencing of single organoids revealed patient-specific genomic and transcriptomic consistency. Single-cell RNAseq demonstrated that organoids are primarily a clonal population. In drug response assays, organoids displayed patient-specific sensitivities. Additionally, we examined the in vivo PDX response to FOLFIRINOX and Gemcitabine/Abraxane treatments, which was recapitulated in vitro by organoids. The patient-specific molecular and histopathological fidelity of organoids indicate that they can be used to understand the etiology of the patient’s tumor and the differential response to therapies and suggests utility for predicting drug responses.

Published

2018

32. 9-ING-41, a small-molecule glycogen synthase kinase-3 inhibitor, is active in neuroblastoma

Author

Andrey Ugolkov, Ana P. Berbegall, Rosa Noguera, Andrew P. Mazar, Samuel Navarro, Mary J.C. Hendrix, Thomas V. O'Halloran, Gennadiy Bondarenko, Oleksii Dubrovskyi, and Francis J. Giles

Subjects

0301 basic medicine, Cancer Research, Indoles, Mice, Nude, Cell Growth Processes, Irinotecan, Article, Maleimides, 03 medical and health sciences, Mice, Neuroblastoma, 0302 clinical medicine, GSK-3, Cell Line, Tumor, Antineoplastic Combined Chemotherapy Protocols, medicine, Animals, Humans, Pharmacology (medical), Enzyme Inhibitors, Glycogen synthase, Pharmacology, Glycogen Synthase Kinase 3 beta, biology, Chemistry, Drug Synergism, medicine.disease, Pediatric cancer, Xenograft Model Antitumor Assays, XIAP, 030104 developmental biology, Oncology, Cell culture, Apoptosis, 030220 oncology & carcinogenesis, Cancer research, biology.protein, Immunohistochemistry, Female

Abstract

Advanced stage neuroblastoma is a very aggressive pediatric cancer with limited treatment options and a high mortality rate. Glycogen Synthase Kinase-3β (GSK-3β) is a potential therapeutic target in neuroblastoma. Using immunohistochemical staining, we observed positive GSK-3β expression in 67% of human neuroblastomas (34 out of 51 cases). Chemically distinct GSK-3 inhibitors (AR-A014418, TDZD8 and 9-ING-41), suppressed the growth of neuroblastoma cells whereas 9-ING-41, a clinically relevant small molecule GSK-3β inhibitor with broad spectrum pre-clinical antitumor activity, being the most potent. Inhibition of GSK-3 resulted in a decreased expression of the antiapoptotic molecule XIAP and an increase in neuroblastoma cell apoptosis. Mouse xenograft studies showed that the combination of clinically relevant doses of CPT-11 and 9-ING-41 led to greater antitumor effect than was observed with either agent alone. These data support the inclusion of patients with advanced neuroblastoma in clinical studies of 9-ING-41, especially in combination with CPT-11.

Published

2018

33. Identification of HDAC6-Selective Inhibitors of Low Cancer Cell Cytotoxicity

Author

Sida Shen, Andrew P. Mazar, Werner Tueckmantel, Daniel D. Billadeau, Andrey Ugolkov, Oleksii Dubrovskyi, Alan P. Kozikowski, Jessica Hoffen, Renee A. Schoon, and Irina N. Gaisina

Subjects

0301 basic medicine, Antineoplastic Agents, Apoptosis, Biology, Histone Deacetylase 6, Biochemistry, Histone Deacetylases, Article, Structure-Activity Relationship, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, Drug Discovery, medicine, Humans, Cytotoxic T cell, General Pharmacology, Toxicology and Pharmaceutics, Cytotoxicity, Cell Proliferation, Pharmacology, Dose-Response Relationship, Drug, Molecular Structure, Cell growth, HDAC10, Organic Chemistry, Cancer, HDAC6, medicine.disease, Histone Deacetylase Inhibitors, Pancreatic Neoplasms, 030104 developmental biology, Cell culture, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, Molecular Medicine, Drug Screening Assays, Antitumor

Abstract

The histone deacetylases (HDACs) occur in 11 different isoforms, and these enzymes regulate the activity of a large number of proteins involved in cancer initiation and progression. The discovery of isoform-selective HDAC inhibitors (HDACIs) is desirable, as it is likely that such compounds would avoid some of the undesirable side effects found with the first-generation inhibitors. A series of HDACIs previously reported by us were found to display some selectivity for HDAC6 and to induce cell-cycle arrest and apoptosis in pancreatic cancer cells. In the present work, we show that structural modification of these isoxazole-based inhibitors leads to high potency and selectivity for HDAC6 over HDAC1-3 and HDAC10, while unexpectedly abolishing their ability to block cell growth. Three inhibitors with lower HDAC6 selectivity inhibit the growth of cell lines BxPC3 and L3.6pl, and they only induce apoptosis in L3.6pl cells. We conclude that HDAC6 inhibition alone is insufficient for disruption of cell growth, and that some degree of class 1 HDAC inhibition is required. Moreover, the highly selective HDAC6Is reported herein that are weakly cytotoxic may find use in cancer immune system reactivation.

Published

2015

34. ERK-regulated αB-crystallin induction by matrix detachment inhibits anoikis and promotes lung metastasis in vivo

Author

William J. Gradishar, Bhawna Sharma, Andrey Ugolkov, Vincent L. Cryns, Vladimir Petrovic, Dmitry Malin, Elena Strekalova, and Harisha Rajanala

Subjects

MAPK/ERK pathway, Cancer Research, Lung Neoplasms, MAP Kinase Signaling System, Mice, Nude, Breast Neoplasms, Apoptosis, Biology, Article, Extracellular matrix, Mice, 03 medical and health sciences, 0302 clinical medicine, Circulating tumor cell, Cell Line, Tumor, Cell Adhesion, Genetics, Extracellular, Animals, Humans, Anoikis, Viability assay, Neoplasm Metastasis, Extracellular Signal-Regulated MAP Kinases, Molecular Biology, 030304 developmental biology, 0303 health sciences, alpha-Crystallin B Chain, αB-crystallin, eye diseases, Neoplasm Proteins, 3. Good health, Cell biology, Cell culture, Caspases, 030220 oncology & carcinogenesis, Cancer cell, Female, sense organs

Abstract

Evasion of extracellular matrix detachment-induced apoptosis ('anoikis') is a defining characteristic of metastatic tumor cells. The ability of metastatic carcinoma cells to survive matrix detachment and escape anoikis enables them to disseminate as viable circulating tumor cells and seed distant organs. Here we report that αB-crystallin, an antiapoptotic molecular chaperone implicated in the pathogenesis of diverse poor-prognosis solid tumors, is induced by matrix detachment and confers anoikis resistance. Specifically, we demonstrate that matrix detachment downregulates extracellular signal-regulated kinase (ERK) activity and increases αB-crystallin protein and messenger RNA (mRNA) levels. Moreover, we show that ERK inhibition in adherent cancer cells mimics matrix detachment by increasing αB-crystallin protein and mRNA levels, whereas constitutive ERK activation suppresses αB-crystallin induction during matrix detachment. These findings indicate that ERK inhibition is both necessary and sufficient for αB-crystallin induction by matrix detachment. To examine the functional consequences of αB-crystallin induction in anoikis, we stably silenced αB-crystallin in two different metastatic carcinoma cell lines. Strikingly, silencing αB-crystallin increased matrix detachment-induced caspase activation and apoptosis but did not affect cell viability of adherent cancer cells. In addition, silencing αB-crystallin in metastatic carcinoma cells reduced the number of viable circulating tumor cells and inhibited lung metastasis in two orthotopic models, but had little or no effect on primary tumor growth. Taken together, our findings point to αB-crystallin as a novel regulator of anoikis resistance that is induced by matrix detachment-mediated suppression of ERK signaling and promotes lung metastasis. Our results also suggest that αB-crystallin represents a promising molecular target for antimetastatic therapies.

Published

2015

35. αB-Crystallin: A Novel Regulator of Breast Cancer Metastasis to the Brain

Author

Eric V. Shusta, Erika Hamilton, Carey K. Anders, Joseph Geradts, C. Ryan Miller, Vincent L. Cryns, Karen J. Fritchie, Barbara Adamo, Kimberly L. Blackwell, Elena Strekalova, Dmitry Malin, Lisa A. Carey, Matthew G. Ewend, Vladimir Petrovic, Allison M. Deal, Andrey Ugolkov, Chad A. Livasy, and Abraham Al Ahmad

Subjects

Cancer Research, Pathology, medicine.medical_specialty, Gene Expression, Triple Negative Breast Neoplasms, Kaplan-Meier Estimate, Mice, SCID, Biology, Blood–brain barrier, Article, Breast cancer, Mice, Inbred NOD, Cell Line, Tumor, Cell Adhesion, medicine, Animals, Humans, Gene silencing, Cell adhesion, Mice, Knockout, Brain Neoplasms, Transendothelial and Transepithelial Migration, alpha-Crystallin B Chain, Cancer, medicine.disease, eye diseases, medicine.anatomical_structure, Oncology, Blood-Brain Barrier, Gene Knockdown Techniques, Cancer research, Female, Endothelium, Vascular, sense organs, Neoplasm Transplantation, Brain metastasis, Astrocyte

Abstract

Purpose: Basal-like breast tumors are typically (ER/PR/HER2) triple-negative and are associated with a high incidence of brain metastases and poor clinical outcomes. The molecular chaperone αB-crystallin is predominantly expressed in triple-negative breast cancer (TNBC) and contributes to an aggressive tumor phenotype in preclinical models. We investigated the potential role of αB-crystallin in brain metastasis in TNBCs. Experimental Design: αB-crystallin expression in primary breast carcinomas and brain metastases was analyzed by immunohistochemistry among patients with breast cancer with brain metastases. αB-crystallin was overexpressed or silenced in two different TNBC cell lines. The effects on cell adhesion to human brain microvascular endothelial cells (HBMEC) or extracellular matrix proteins, transendothelial migration, and transmigration across a HBMEC/astrocyte coculture blood–brain barrier (BBB) model were examined. In addition, the effects of overexpressing or silencing αB-crystallin on brain metastasis in vivo were investigated using orthotopic TNBC models. Results: In a cohort of women with breast cancer brain metastasis, αB-crystallin expression in primary breast carcinomas was associated with poor overall survival and poor survival after brain metastasis, even among patients with TNBC. Stable overexpression of αB-crystallin in TNBC cells enhanced adhesion to HBMECs, transendothelial migration, and BBB transmigration in vitro, whereas silencing αB-crystallin inhibited these events. αB-crystallin promoted adhesion of TNBC cells to HBMECs, at least in part, through an α3β1 integrin–dependent mechanism. αB-crystallin overexpression promoted brain metastasis, whereas silencing αB-crystallin inhibited brain metastasis in orthotopic TNBC models. Conclusion: αB-crystallin is a novel regulator of brain metastasis in TNBC and represents a potential biomarker and drug target for this aggressive disease. Clin Cancer Res; 20(1); 56–67. ©2013 AACR.

Published

2014

36. Abstract B09: GSK-3β blockade with 9-ING-41 in pancreas cancer: The 1801 phase 1/2 study

Author

Ludimila Cavalcante, Brittany A. Borden, Malika Dhawan, Andrew P. Mazar, Benedito A. Carneiro, Daniel D. Billadeau, Andrey Ugolkov, Pamela N. Munster, Francis J. Giles, and Howard Safran

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Chemotherapy, business.industry, medicine.medical_treatment, Cancer, Phases of clinical research, medicine.disease, Gemcitabine, Blockade, Tolerability, Response Evaluation Criteria in Solid Tumors, Internal medicine, Pancreatic cancer, medicine, business, medicine.drug

Abstract

Background: We have previously identified Glycogen Synthase Kinase-3 beta (GSK-3β) nuclear accumulation as a hallmark of pancreatic ductal adenocarcinoma (PDAC) and demonstrated the antitumor effects of GSK-3β tool compound inhibitors in vivo (Ougolkov, Clin Cancer Res 2006). 9-ING-41 (Actuate Therapeutics Inc), a first-in-class, small-molecule potent selective GSK-3β inhibitor, has significant preclinical antitumor activity in PDAC. 9-ING-41 is synergistic with gemcitabine (GEM) in significantly reducing PDAC cell proliferation via impairment of ATR/Chk1 DNA damage response (Ding, Clin Cancer Res 2019). These data provided the rationale for inclusion of patients with PDAC in the 1801 phase 1/2 study evaluating 9-ING-41 alone and in combination with chemotherapy, including GEM and GEM plus nab-paclitaxel. Methods: Parts 1 and 2 of the 1801 phase 1/2 study evaluate the safety and tolerability of 9-ING-41 in patients with refractory malignancies. Part 1 establishes the recommended phase 2 study dose (RP2D) for 9-ING-41 monotherapy, while Part 2 assesses 9-ING-41 in combination with chemotherapies. For Part 1, patients received twice-weekly IV infusions of 9-ING-41 (21-day cycle). Based on prior treatment, Part 2 for those with PDAC consists of 9-ING-41 plus GEM (1000 to 1250 mg/m2 days 1 and 8; 21-day cycle) or 9-ING-41 plus GEM and nab-paclitaxel (125 mg/m2). Part 3 (Simon 2-stage phase 2 at the RP2D) will assess clinical benefit in patients with refractory PDAC treated with 9-ING-41-based combinations at the RP2D established in Part 2. Response is defined by response evaluation criteria in solid tumors (RECIST) criteria in evaluable lesions. The study is opening in 25 sites globally and will accrue approximately 300 patients. Results: To date, the study has accrued 34 patients with advanced solid tumors (n=33) or hematologic malignancies (n=1). Four dose levels (1, 2, 3.3, and 5 mg/kg) have been completed without dose-limiting toxicities (DLT). Part 2 of the study evaluating combination of 9-ING-41 with chemotherapy agents has been activated. Six patients with advanced PDAC have enrolled. One patient has completed 5 cycles of treatment with 9-ING-41 (1mg/kg) with stable disease (SD) as the best response. Another patient with SD as the best response has completed 6 cycles and now is joining the arm combining 9-ING-41 with GEM after disease progression. Four additional patients are awaiting first response assessment with enrollment ongoing. 9-ING-41-attributable AE to date are Grade 1 transient visual changes (color perception). Conclusions: 9-ING-41 is well tolerated. Preclinical data support the inclusion of patients with advanced PDAC on clinical studies of 9-ING-41. Citation Format: Benedito A. Carneiro, Malika Dhawan, Brittany Borden, Ludimila Cavalcante, Howard Safran, Andrey Ugolkov, Andrew P. Mazar, Daniel D. Billadeau, Francis J. Giles, Pamela Munster. GSK-3β blockade with 9-ING-41 in pancreas cancer: The 1801 phase 1/2 study [abstract]. In: Proceedings of the AACR Special Conference on Pancreatic Cancer: Advances in Science and Clinical Care; 2019 Sept 6-9; Boston, MA. Philadelphia (PA): AACR; Cancer Res 2019;79(24 Suppl):Abstract nr B09.

Published

2019

37. Abstract 4812: 9-ING-41, a novel inhibitor of glycogen synthase kinase-3beta (GSK-3β), is active as a single agent and within combination therapies in bladder cancer cell lines

Author

Vladimir Bilim, Daniel Schmitt, Tsutomu Anraku, Andrey Ugolkov, Masayuki Tasaki, Francis J. Giles, Yoshihiko Tomita, Hiroo Kuroki, and Andrew Mazer

Subjects

Cisplatin, Cancer Research, Cabozantinib, Chemistry, Kinase, Cancer, Cell cycle, medicine.disease, XIAP, chemistry.chemical_compound, Oncology, GSK-3, medicine, Cancer research, Protein kinase A, medicine.drug

Abstract

Glycogen synthase kinase-3beta (GSK-3β) is a serine/threonine protein kinase that has been established as a therapeutic target in a broad spectrum of human malignancies. We have previously identified aberrant GSK-3β nuclear expression in bladder cancer (BC), and demonstrated that GSK-3β positively regulated BC cell survival and proliferation. Our objective was to evaluate the antitumor effects of the clinically viable agent 9-ING-41, a maleimide-based ATP-competitive GSK-3 inhibitor, which has broad spectrum antitumor activity and marked activity in reversing chemoresistance in a variety of pre-clinical models of human cancers. We used flow cytometry, Western immunoblotting, quantitative RT-PCR, BrDU incorporation and MTS assays to examine antitumor activity of 9-ING-41 in BC (T24, HT1376, RT4 cell lines). Additionally, we studied combination therapy of 9-ING-41 with gemcitabine and cisplatin, standard agents used for the treatment of patients with advanced BC, with cabozantinib, a multi kinase inhibitor, and with chloroquine, an autophagy inhibitor. A dose-dependent decrease in cancer cell proliferation was observed by MTS assay and BrdU incorporation assay with GI50 0.7μM (T24), 4.7 μM(HT1376), 2.2μM(RT4). Treatment with 9-ING-41 induced prominent cell cycle arrest (predominantly G2 arrest) in BC cells. Expression of cell cycle related proteins, including Cyclin D, and anti-apoptotic proteins, such as XIAP and Bcl-2, were significantly decreased as detected by Western immunoblotting and real time RT-PCR. Treatment with 9-ING-41 significantly potentiated the growth inhibitory effect of cisplatin and gemcitabine in cultured cells. In addition, combination therapy with 9-ING-41 and cabozantinib or chloroquine, significantly potentiated the effect of either single agent. Our data proved that a single treatment using 9-ING-41 is effective in BC cells. Combination treatment of 9-ING-41 with standard chemotherapeutic drugs or novel agents may provide a new therapeutic approaches in BC. These data provide a rational for the inclusion of patients with advanced BC in clinical studies of 9-ING-41. Citation Format: Hiroo Kuroki, Tsutomu Anraku, Vladimir Bilim, Masayuki Tasaki, Daniel Schmitt, Andrew Mazer, Francis J. Giles, Andrey Ugolkov, Yoshihiko Tomita. 9-ING-41, a novel inhibitor of glycogen synthase kinase-3beta (GSK-3β), is active as a single agent and within combination therapies in bladder cancer cell lines [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2019; 2019 Mar 29-Apr 3; Atlanta, GA. Philadelphia (PA): AACR; Cancer Res 2019;79(13 Suppl):Abstract nr 4812.

Published

2019

38. Invasion and metastasis

Author

Andrew P. Mazar, Andrey Ugolkov, Jack Henkin, Richard W. Ahn, and Thomas V. O’Halloran

Abstract

Mortality in cancer patients usually occurs as a result of dissemination of their disease, a multi-factorial process called metastasis. This chapter discusses current understanding of how metastasis occurs and the pathways and cellular interactions that contribute to this process. Current views on lymphatic, haematogenous, and direct dissemination of metastatic cells through body cavities are considered, along with the contribution of tumour stromal cells, immune, and infiltrating cells derived from bone marrow, and angiogenesis to the metastatic process. Recent advances in characterizing metastatic niches and the contribution of specific organ sites and microenvironments to metastatic progression are presented, and the identification and characterization of circulating tumour cells and their role in metastasis are considered. Finally, representative molecular pathways as well as a sampling of new drugs in development for the treatment of metastatic disease are presented and referenced.

Published

2016

39. GSK-3 inhibition in vitro and in vivo enhances antitumor effect of sorafenib in renal cell carcinoma (RCC)

Author

Andrey Ugolkov, Akira Nagaoka, Yoshihiko Tomita, Sei Naito, Vladimir Bilim, Hisashi Kawazoe, Kaori Yuuki, and Tomoyuki Kato

Subjects

Niacinamide, Sorafenib, Pyridines, medicine.drug_class, Biophysics, Antineoplastic Agents, urologic and male genital diseases, Biochemistry, Tyrosine-kinase inhibitor, Glycogen Synthase Kinase 3, Mice, In vivo, Renal cell carcinoma, GSK-3, Antineoplastic Combined Chemotherapy Protocols, medicine, Animals, Humans, heterocyclic compounds, Glycogen synthase, Carcinoma, Renal Cell, Protein Kinase Inhibitors, neoplasms, Molecular Biology, Cell Proliferation, biology, Cell growth, business.industry, Phenylurea Compounds, Benzenesulfonates, Cell Biology, medicine.disease, Xenograft Model Antitumor Assays, Kidney Neoplasms, digestive system diseases, female genital diseases and pregnancy complications, In vitro, biology.protein, Cancer research, business, medicine.drug

Abstract

Sorafenib is a multikinase inhibitor approved for the systemic treatment of renal cell carcinoma (RCC). However, sorafenib treatment has a limited effect due to acquired chemoresistance of RCC. Previously, we identified glycogen synthase kinase-3 (GSK-3) as a new therapeutic target in RCC. Here, we observed that sorafenib inhibits proliferation and survival of RCC cells. Significantly, we revealed that sorafenib enhances GSK-3 activity in RCC cells, which could be a potential mechanism of acquired chemoresistance. We found that pharmacological inhibition of GSK-3 potentiates sorafenib antitumor effect in vitro and in vivo. Our results suggest that combining GSK-3 inhibitor and sorafenib might be a potential new therapeutic approach for RCC treatment.

Published

2012

40. The enhancer of zeste homolog 2 (EZH2), a potential therapeutic target, is regulated by miR-101 in renal cancer cells

Author

Kaori Yuuki, Andrey Ugolkov, Masaaki Tsukigi, Toshihiko Sakurai, Teiichi Motoyama, Vladimir Bilim, and Yoshihiko Tomita

Subjects

Adult, Male, Enhancer of zeste homolog 2, Biophysics, macromolecular substances, Biology, urologic and male genital diseases, Biochemistry, Negative regulator, Renal cell carcinoma, medicine, Biomarkers, Tumor, Tumor Cells, Cultured, Humans, Enhancer of Zeste Homolog 2 Protein, MicroRNA-101, Carcinoma, Renal Cell, Molecular Biology, Aged, Cell Proliferation, Aged, 80 and over, Cell Nucleus, Cell growth, Cancer cell proliferation, EZH2, Polycomb Repressive Complex 2, Cell Biology, Middle Aged, medicine.disease, Molecular biology, Kidney Neoplasms, female genital diseases and pregnancy complications, DNA-Binding Proteins, Gene Expression Regulation, Neoplastic, MicroRNAs, Enhancer Elements, Genetic, Histone methyltransferase, Cancer cell, Cancer research, Female, RNA Interference, Cyclin-Dependent Kinase Inhibitor p27, Transcription Factors

Abstract

We investigated a prognostic significance and the mechanism of aberrant nuclear expression of EZH2, a histone methyltransferase, in human renal cell carcinoma (RCC). We found nuclear EZH2 in 48 of 100 RCCs and it was significantly correlated with worse survival in RCC patients. We detected a decreased expression of miR-101 in 15 of 54 RCCs. We found that re-expression of miR-101 resulted in EZH2 depletion and decreased renal cancer cell proliferation. Our results show nuclear EZH2 as a prognostic marker of worse survival in human RCC, and identify miR-101 as a negative regulator of EZH2 expression and renal cancer cell proliferation.

Published

2012

41. Expression analysis of putative stem cell markers in human benign and malignant prostate

Author

Ximing J. Yang, Laurie J. Eisengart, Andrey Ugolkov, and Chunyan Luan

Subjects

PCA3, Pathology, medicine.medical_specialty, Urology, Biology, medicine.disease, Stem cell marker, Prostate cancer, medicine.anatomical_structure, Oncology, SOX2, Cancer stem cell, Prostate, medicine, High-grade prostatic intraepithelial neoplasia, Stem cell

Abstract

BACKGROUND Stem cells were suggested to be present in human prostate cancer as a small population of distinct cells, which may contribute to carcinogenesis, tumor recurrence, and chemoresistance. To identify potential prostatic stem cells, we analyzed the expression of several potential stem cell markers in benign prostate and prostatic adenocarcinoma. METHODS CD44, CD133, Oct4, SOX2, and EZH2 expression was detected by immunohistochemical (IHC) staining using tissue microarray assays (TMA) composed of benign (non-neoplastic) prostatic tissue, high grade prostatic intraepithelial neoplasia (HGPIN), and prostatic adenocarcinoma. Positive staining was defined as 1+ ( 50%). RESULTS We found CD44 staining in 97% and 72% of benign + HGPIN and malignant lesions, respectively. CD133 staining was detected in a small fraction (4 of 67) of prostate carcinomas. We found that Oct4 nuclear expression was strongly associated with benign lesions and HGPIN but not prostate cancer (P

Published

2010

42. 9-ING-41, a clinically relevant inhibitor of glycogen synthase kinase-3 (GSK-3), is active pre-clinically in human bladder and renal cell cancers

Author

D. Schmitt, Vladimir Bilim, Yoshihiko Tomita, Tsutomu Anraku, Masayuki Tasaki, Hiroo Kuroki, Andrey Ugolkov, and A. Mazar

Subjects

0301 basic medicine, business.industry, Human bladder, Hematology, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Oncology, GSK-3, 030220 oncology & carcinogenesis, Cancer research, Medicine, Renal Cell Cancers, business

Published

2018

43. Glycogen Synthase Kinase-3β: A Prognostic Marker and a Potential Therapeutic Target in Human Bladder Cancer

Author

Sei Naito, Yoshihiko Tomita, Vladimir Bilim, Kaori Yuuki, Tomoyuki Kato, Teiichi Motoyama, Andrey Ugolkov, and Akira Nagaoka

Subjects

Adult, Male, Cancer Research, Pathology, medicine.medical_specialty, Cell Survival, medicine.medical_treatment, Antineoplastic Agents, macromolecular substances, Targeted therapy, Glycogen Synthase Kinase 3, GSK-3, Cell Line, Tumor, Biomarkers, Tumor, medicine, Humans, Molecular Targeted Therapy, Neoplasm Metastasis, Glycogen synthase, GSK3B, Aged, Cell Proliferation, Neoplasm Staging, Aged, 80 and over, Cell Nucleus, Glycogen Synthase Kinase 3 beta, Bladder cancer, biology, Kinase, Carcinoma, Cancer, Middle Aged, Prognosis, medicine.disease, Survival Analysis, Urinary Bladder Neoplasms, Oncology, Cancer research, biology.protein, Female, Kidney cancer

Abstract

Purpose: Although recent studies have shown glycogen synthase kinase-3β (GSK-3β), a serine/threonine kinase, as a positive regulator of pancreatic, colon, and kidney cancer cell survival and proliferation, the role of GSK-3 in bladder cancer remains unknown. Our objectives were to determine the subcellular localization of GSK-3β and to evaluate the effect of GSK-3 inhibition in bladder cancer. Experimental Design: We used immunohistochemical staining and nuclear/cytosolic fractionation to determine the expression pattern of GSK-3β in human urothelial carcinomas. To study the effect of GSK-3 inhibition on bladder cancer cell proliferation and survival, we used pharmacologic inhibitors of GSK-3, RNA interference, MTS assay, bromodeoxyuridine incorporation assay, quantitative reverse transcriptase-PCR, and Western blotting. Results: We found aberrant nuclear accumulation of GSK-3β in 62% (43 of 69) and 91% (21 of 23) of noninvasive and invasive human urothelial carcinomas, respectively. GSK-3β nuclear staining was significantly associated with high-grade tumors (P < 0.001), advanced stage of bladder cancer (P < 0.05), metastasis (P < 0.05), and worse cause-specific survival (P < 0.05) in bladder cancer patients. Moreover, we found that pharmacologic inhibition or genetic depletion of GSK-3β resulted in decreased viability of bladder cancer cells. Conclusions: Our results suggest nuclear accumulation of GSK-3β as a novel prognostic marker in bladder cancer, show that GSK-3 contributes to urothelial cancer cell proliferation and survival, and identify GSK-3 as a potential therapeutic target in human bladder cancer. Clin Cancer Res; 16(21); 5124–32. ©2010 AACR.

Published

2010

44. Abstract 1127: Aberrant nuclear expression of GSK-3beta in human head and neck carcinoma

Author

Francis J. Giles, Andrey Ugolkov, Timothy Taxter, Andrew P. Mazar, Sandeep Samant, and Maria Matsangou

Subjects

0301 basic medicine, Cancer Research, biology, Salivary gland, 010405 organic chemistry, business.industry, Cancer, medicine.disease, 01 natural sciences, Head and neck squamous-cell carcinoma, 0104 chemical sciences, 03 medical and health sciences, 030104 developmental biology, medicine.anatomical_structure, Breast cancer, Oncology, In vivo, Cancer research, Carcinoma, biology.protein, Medicine, business, Protein kinase A, Glycogen synthase

Abstract

Background: Recurrent/metastatic head and neck squamous cell carcinoma (SCCHN) and salivary gland malignancies are difficult to treat with limited standard of care options at the present time. Glycogen Synthase Kinase-3beta (GSK-3beta), a serine/threonine protein kinase, has been implicated as a potential therapeutic target in human cancer. Our in vivo studies demonstrated that our novel GSK-3 inhibitors significantly potentiated the effects of conventional chemotherapy in patient-derived xenograft models of glioblastoma and breast cancer leading to regression of tumors. In order to develop a rationale to test our novel GSK-3 inhibitors in head and neck (H&N) malignancies, we evaluated the expression pattern of GSK-3beta in human H&N benign tissue and malignant tumors. Methods: We used immunohistochemical staining of H&N tumor tissue Microarray (TMA), 48 total cases (20 benign tissues, 28 malignant), to study the expression pattern of GSK-3beta. GSK-3beta nuclear accumulation was defined as positive staining of more than 50% of cancer cell nuclei throughout the tumor regardless of cytoplasmic staining. Results: Of the 20 malignant H&N samples (15 SCCHN, 1 nasopharyngeal and 5 other histology), 13 (65%) were found to have aberrant nuclear accumulation of GSK-3beta. Amongst SCCHN, 73% (11 of 15 samples) had aberrant nuclear accumulation of GSK-3beta. In contrast, none (0%) of the 11 benign non-salivary H&N tissue showed detectable expression of GSK-3beta. Of interest, 60% of salivary adenoid cystic carcinoma specimens and 44% of benign salivary gland tissue showed GSK-3beta expression. Conclusions: Our results demonstrate for the first time, that there is aberrant nuclear expression of GSK-3beta in SCCHN. This finding supports further exploring of our novel GSK-3beta inhibitor as a potential therapeutic target for recurrent/metastatic SCCHN and also, as a potential prognostic and predictive biomarker for risk of recurrent disease and chemo- or radio-resistance. Its role in salivary gland malignancies requires further studying. Citation Format: Maria Matsangou, Andrey Ugolkov, Timothy J. Taxter, Sandeep Samant, Andrew P. Mazar, Francis J. Giles. Aberrant nuclear expression of GSK-3beta in human head and neck carcinoma [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2017; 2017 Apr 1-5; Washington, DC. Philadelphia (PA): AACR; Cancer Res 2017;77(13 Suppl):Abstract nr 1127. doi:10.1158/1538-7445.AM2017-1127

Published

2017

45. Biodistribution and in Vivo Toxicity of Aptamer-Loaded Gold Nanostars

Author

Kavita Chandra, Kayla S. B. Culver, Irawati Kandela, Raymond C. Lee, Andrew P. Mazar, Christine Mantis, Teri W. Odom, Andrey Ugolkov, Hyojin Lee, and Duncan Hieu M. Dam

Subjects

Male, Biodistribution, Pathology, medicine.medical_specialty, Materials science, Fibrosarcoma, Biomedical Engineering, Pharmaceutical Science, Medicine (miscellaneous), Metal Nanoparticles, Mice, Nude, Bioengineering, Article, Mice, Breast cancer, In vivo, Cell Line, Tumor, medicine, Distribution (pharmacology), Animals, General Materials Science, Sex Characteristics, Mammary Neoplasms, Experimental, Aptamers, Nucleotide, medicine.disease, Acute toxicity, Rats, Toxicity, Cancer research, Molecular Medicine, Female, Gold, Drug Screening Assays, Antitumor, Ex vivo

Abstract

This paper reports an in vivo evaluation of toxicology and biodistribution of a highly anisotropic Au nanoconstruct composed of a gold nanostar (AuNS) core and a ligand shell of a G-quadruplex DNA aptamer AS1411 (Apt) supporting both targeting and therapy capabilities. We examined the toxicity of the nanoconstructs (Apt-AuNS) at four different injected concentrations. At the highest dose tested (48 mg/kg), maximal tolerated dose was not reached. Clinical pathology showed no apparent signs of acute toxicity. Interestingly, the nanoconstructs circulated longer in female rats compared to male rats. In two different tumor models, the biodistribution of Apt-AuNS, especially tumor accumulation, was different. Accumulation of Apt-AuNS was 5 times higher in invasive breast cancer tumors compared to fibrosarcoma tumors. These results provide insight on identifying a tumor model and nanoconstruct for in vivo studies, especially when an in vitro therapeutic response is observed in multiple cancer cell lines. From the clinical editor: This study investigated the toxicity and distribution of aptamer loaded gold nanostars in a rodent model of invasive breast cancer and fibrosarcoma. Acute toxicity was not identified even in the highest studied doses. Fivefold accumulation was demonstrated in the breast cancer model compared to the fibrosarcoma model. Studies like this are critically important in further clarifying the potential therapeutic use of these nanoconstructs, especially when ex vivo effects are clearly demonstrated.

Published

2014

46. Biomimetic, synthetic HDL nanostructures for lymphoma

Author

Andrea J. Luthi, Andrey Ugolkov, Leo I. Gordon, Shuo Yang, Sandeep S. Dave, Marina G. Damiano, C. Shad Thaxton, Jonathan S. Rink, Heng Zhang, Sushant Tripathy, and Amareshwar T.K. Singh

Subjects

Lymphoma, B-Cell, Blotting, Western, Immunoblotting, Metal Nanoparticles, Apoptosis, Biology, Jurkat cells, Mass Spectrometry, chemistry.chemical_compound, Jurkat Cells, Mice, High-density lipoprotein, Microscopy, Electron, Transmission, Biomimetics, medicine, Animals, Humans, Scavenger receptor, Annexin A5, Multidisciplinary, Cholesterol, Scavenger Receptors, Class B, Biological Sciences, medicine.disease, Lymphoma, chemistry, Mechanism of action, Biochemistry, Cancer research, lipids (amino acids, peptides, and proteins), medicine.symptom, Lipoproteins, HDL, Fluorescein-5-isothiocyanate

Abstract

New therapies that challenge existing paradigms are needed for the treatment of cancer. We report a nanoparticle-enabled therapeutic approach to B-cell lymphoma using synthetic high density lipoprotein nanoparticles (HDL-NPs). HDL-NPs are synthesized using a gold nanoparticle template to control conjugate size and ensure a spherical shape. Like natural HDLs, biomimetic HDL-NPs target scavenger receptor type B-1, a high-affinity HDL receptor expressed by lymphoma cells. Functionally, compared with natural HDL, the gold NP template enables differential manipulation of cellular cholesterol flux in lymphoma cells, promoting cellular cholesterol efflux and limiting cholesterol delivery. This combination of scavenger receptor type B-1 binding and relative cholesterol starvation selectively induces apoptosis. HDL-NP treatment of mice bearing B-cell lymphoma xenografts selectively inhibits B-cell lymphoma growth. As such, HDL-NPs are biofunctional therapeutic agents, whose mechanism of action is enabled by the presence of a synthetic nanotemplate. HDL-NPs are active in B-cell lymphomas and potentially, other malignancies or diseases of pathologic cholesterol accumulation.

Published

2013

47. Abstract 4272: Organoids and patient-derived tumor xenograft of pancreatic adenocarcinoma share morphological and genetic features with the primary tumor

Author

Christopher R. Weber, Tongjun Gu, Isabel Romero Calvo, Margaret Eber, William Dale, Samantha M. Sparrow, Hedy L. Kindler, Andrey Ugolkov, Kevin P. White, Teresa Barry, Kevin K. Roggin, Shuang Qin Zhang, Ashwin Akki, Andrew P. Mazar, and Mary M. Buschmann

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Pancreatic ductal adenocarcinoma, endocrine system diseases, business.industry, Cancer, medicine.disease, Primary tumor, Paraffin embedded tissue, Internal medicine, Female patient, Organoid, Cancer research, Medicine, Adenocarcinoma, business, Tumor xenograft

Abstract

Pancreatic ductal adenocarcinoma (PDAC) is the fourth leading cause of cancer death, with a 5-year overall survival rate Histopathological comparison of sections from PDX tumor, organoids, and primary PDAC from a 63-year-old female patient were performed on paraffin embedded tissue. H&E and immunohistochemical staining for cytokeratins (CK7, CK20), p53, Claudin-4, and CEA were performed. DNA and mRNA sequencing was performed. Both PDX and organoids exhibited histopathological features remarkably consistent with the original patient tumor including the histologic grade (moderately differentiated), cytological appearance (irregular nuclear membranes, open chromatin and prominent nucleoli), mitotic activity (5 -7/10 HPF), and immunohistochemical profile. The PDX and organoids demonstrated diffuse moderate-to-strong positivity for CK7, CEA, p53, and Claudin-4 and focal weak positivity for CK20 - all similar to the primary tumor. The immunohistochemical staining pattern was consistent with mRNA sequencing of the primary tumor which showed that CEA, Claudin-4 and p53 expression were ∼960-fold, ∼27-fold and ∼3 fold higher respectively (vs. benign pancreatic tissue). DNA sequencing revealed somatic mutations in KRAS and TP53 genes seen in >90% and ∼70% of PDACs respectively, and a few rare somatic mutations, such as a sodium leak channel (NALCN) mutation, seen in ∼3% of PDAC. Both PDX and organoid models of PDAC maintain key histological features, immunohistochemical profile and basic gene expression pattern akin to the primary tumor. These findings suggest that PDXs and organoids have the potential to serve as reliable pathophysiological models for optimizing individual therapy for patients with PDAC. Citation Format: Isabel Romero Calvo, Ashwin Akki, Andrey Ugolkov, Mary M. Buschmann, Samantha M. Sparrow, Teresa Barry, Margaret Eber, Tongjun Gu, Shuang Qin Zhang, Hedy Kindler, William Dale, Kevin Roggin, Andrew P. Mazar, Kevin P. White, Christopher R. Weber. Organoids and patient-derived tumor xenograft of pancreatic adenocarcinoma share morphological and genetic features with the primary tumor. [abstract]. In: Proceedings of the 107th Annual Meeting of the American Association for Cancer Research; 2016 Apr 16-20; New Orleans, LA. Philadelphia (PA): AACR; Cancer Res 2016;76(14 Suppl):Abstract nr 4272.

Published

2016

48. Abstract 3078: GSK-3 inhibitor 9ING41 potentiates the antitumor effects of CPT-11 in human breast cancer

Author

Andrey Ugolkov, Alan P. Kozikowski, Thomas V. O'Halloran, Andrew P. Mazar, Kevin P. White, and Irina N. Gaisina

Subjects

Cisplatin, Cancer Research, Chemotherapy, business.industry, medicine.medical_treatment, Estrogen receptor, Cancer, medicine.disease, Targeted therapy, Breast cancer, Oncology, GSK-3, medicine, Cancer research, business, Estrogen receptor alpha, medicine.drug

Abstract

Glycogen Synthase Kinase-3beta (GSK-3beta), a serine/threonine protein kinase, has been demonstrated to be potential therapeutic target in human breast cancer. Our objective was to evaluate novel GSK-3 inhibitors alone and in combination with chemotherapeutic drugs for the targeted therapy of breast cancer. Using a short-term treatment, we found that the GSK-3 inhibitor 9ING41 significantly potentiates the antitumor effects of CPT-11, cisplatin and 5-FU to inhibit breast cancer cell growth. We established hormone-refractory BC-1 and BC-2 patient-derived xenograft (PDX) tumor models from metastatic pleural effusions that were obtained from breast cancer patients. We considered BC-1 and BC-2 PDX tumors as chemoresistant, because metastatic disease progressed in both cases in despite of the fact that patients received many cycles of chemotherapy. Although we found that BC-1 and BC-2 PDX tumors express estrogen receptor (ER), both PDX tumors carried activating mutations in ESR1. These mutations confer ligand-independent activity of the ER in tamoxifen-resistant breast tumors. We found that BC-1 and BC-2 PDX tumors grew without estradiol supplementation in immunodeficient mice, which suggests a hormone-refractory nature of these tumors. We found that GSK-3 inhibitor 9ING41 potentiates the effects of chemotherapeutic drug CPT-11, and leads to the regression of BC-1 and BC-2 breast PDX tumors. Our results demonstrate inhibition of GSK-3 as a promising therapeutic approach to overcome breast cancer chemoresistance, and identify GSK-3 inhibitor 9ING41 as a drug candidate for the targeted therapy of human breast cancer. Citation Format: Andrey Ugolkov, Irina Gaisina, Kevin White, Alan Kozikowski, Thomas O’Halloran, Andrew Mazar. GSK-3 inhibitor 9ING41 potentiates the antitumor effects of CPT-11 in human breast cancer. [abstract]. In: Proceedings of the 107th Annual Meeting of the American Association for Cancer Research; 2016 Apr 16-20; New Orleans, LA. Philadelphia (PA): AACR; Cancer Res 2016;76(14 Suppl):Abstract nr 3078.

Published

2016

49. Coassembled cytotoxic and pegylated peptide amphiphiles form filamentous nanostructures with potent antitumor activity in models of breast cancer

Author

Daniel J. Toft, Samuel I. Stupp, Yves Ruff, Andrey Ugolkov, Tyson J. Moyer, Vincent L. Cryns, and Stephany M. Standley

Subjects

Biodistribution, Materials science, medicine.medical_treatment, General Physics and Astronomy, Mice, Nude, Peptide, Antineoplastic Agents, Breast Neoplasms, Article, Polyethylene Glycols, Mice, Surface-Active Agents, Cell Line, Tumor, Amphiphile, Materials Testing, medicine, Peptide amphiphile, Organic chemistry, Animals, Humans, General Materials Science, chemistry.chemical_classification, Protease, General Engineering, Trypsin, Nanostructures, Treatment Outcome, chemistry, Nanofiber, PEGylation, Biophysics, Female, Peptides, medicine.drug

Abstract

Self-assembled peptide amphiphiles (PAs) consisting of hydrophobic, hydrogen bonding, and charged hydrophilic domains form cylindrical nanofibers in physiological conditions and allow for the presentation of a high density of bioactive epitopes on the nanofiber surface. We report here on the use of PAs to form multifunctional nanostructures with tumoricidal activity. The combination of a cationic, membrane-lytic PA co-assembled with a serum-protective, pegylated PA was shown to self-assemble into nanofibers. Addition of the pegylated PA to the nanostructure substantially limited degradation of the cytolytic PA by the protease trypsin, with an eight-fold increase in the amount of intact PA observed after digestion. At the same time, addition of up to 50% pegylated PA to the nanofibers did not decrease the in vitro cytotoxicity of the cytolytic PA. Using a fluorescent tag covalently attached to PA nanofibers we were able to track the biodistribution in plasma and tissues of tumor bearing mice over time after intraperitoneal administration of the nanoscale filaments. Using an orthotopic mouse xenograft model of breast cancer, systemic administration of the cytotoxic pegylated nanostructures significantly reduced tumor cell proliferation and overall tumor growth, demonstrating the potential of multifunctional PA nanostructures as versatile cancer therapeutics.

Published

2012

50. Re-expression of miR-199a suppresses renal cancer cell proliferation and survival by targeting GSK-3β

Author

Tomoyuki Kato, Sei Naito, Vladimir Bilim, Kaori Yuuki, Masaaki Tsukigi, Teiichi Motoyama, Akira Nagaoka, Andrey Ugolkov, and Yoshihiko Tomita

Subjects

Adult, Male, Cancer Research, Cell Survival, medicine.medical_treatment, Blotting, Western, Down-Regulation, macromolecular substances, Biology, urologic and male genital diseases, Targeted therapy, Glycogen Synthase Kinase 3, Downregulation and upregulation, Renal cell carcinoma, Cell Line, Tumor, medicine, Humans, Carcinoma, Renal Cell, Aged, Cell Proliferation, Regulation of gene expression, Aged, 80 and over, Cell growth, Middle Aged, medicine.disease, Molecular biology, Immunohistochemistry, female genital diseases and pregnancy complications, Gene Expression Regulation, Neoplastic, MicroRNAs, Oncology, Cell culture, Apoptosis, Cancer cell, Cancer research, Female

Abstract

Recently, we have identified GSK-3 as a new therapeutic target in renal cell cancer (RCC). miR-199a could potentially downregulate GSK-3β expression. Here, we found a decreased miR-199a expression in 59% (32 of 54) of RCCs and it was correlated with higher tumor stage (p < 0.05) and nuclear overexpression of GSK-3β (p < 0.05). We show that re-expression of miR-199a downregulates GSK-3β and suppresses cancer cell growth. Our results demonstrate low miR-199a expression as a feature of advanced RCCs, identify miR-199a as a negative regulator of GSK-3β, and suggest re-expression of pre-miR-199a as a new potential treatment of RCC.

Published

2011