Your search keyword '"Szokalska A"' showing total 23 results

1. Zinc protoporphyrin IX, a heme oxygenase-1 inhibitor, demonstrates potent antitumor effects but is unable to potentiate antitumor effects of chemotherapeutics in mice

Author

Jozkowicz Alicja, Was Halina, Issat Tadeusz, Salwa Pawel, Szokalska Angelika, Bil Jacek, Winiarska Magdalena, Bugajski Marek, Nowis Dominika, Dulak Jozef, Stoklosa Tomasz, and Golab Jakub

Subjects

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

Abstract

Abstract Background HO-1 participates in the degradation of heme. Its products can exert unique cytoprotective effects. Numerous tumors express high levels of HO-1 indicating that this enzyme might be a potential therapeutic target. In this study we decided to evaluate potential cytostatic/cytotoxic effects of zinc protoporphyrin IX (Zn(II)PPIX), a selective HO-1 inhibitor and to evaluate its antitumor activity in combination with chemotherapeutics. Methods Cytostatic/cytotoxic effects of Zn(II)PPIX were evaluated with crystal violet staining and clonogenic assay. Western blotting was used for the evaluation of protein expression. Flow cytometry was used to evaluate the influence of Zn(II)PPIX on the induction of apoptosis and generation of reactive oxygen species. Knock-down of HO-1 expression was achieved with siRNA. Antitumor effects of Zn(II)PPIX alone or in combination with chemotherapeutics were measured in transplantation tumor models. Results Zn(II)PPIX induced significant accumulation of reactive oxygen species in tumor cells. This effect was partly reversed by administration of exogenous bilirubin. Moreover, Zn(II)PPIX exerted potent cytostatic/cytotoxic effects against human and murine tumor cell lines. Despite a significant time and dose-dependent decrease in cyclin D expression in Zn(II)PPIX-treated cells no accumulation of tumor cells in G1 phase of the cell cycle was observed. However, incubation of C-26 cells with Zn(II)PPIX increased the percentage of cells in sub-G1 phase of the cells cycle. Flow cytometry studies with propidium iodide and annexin V staining as well as detection of cleaved caspase 3 by Western blotting revealed that Zn(II)PPIX can induce apoptosis of tumor cells. B16F10 melanoma cells overexpressing HO-1 and transplanted into syngeneic mice were resistant to either Zn(II)PPIX or antitumor effects of cisplatin. Zn(II)PPIX was unable to potentiate antitumor effects of 5-fluorouracil, cisplatin or doxorubicin in three different tumor models, but significantly potentiated toxicity of 5-FU and cisplatin. Conclusion Inhibition of HO-1 exerts antitumor effects but should not be used to potentiate antitumor effects of cancer chemotherapeutics unless procedures of selective tumor targeting of HO-1 inhibitors are developed.

Published

2008

2. Supplementary Figure 1 from Proteasome Inhibition Potentiates Antitumor Effects of Photodynamic Therapy in Mice through Induction of Endoplasmic Reticulum Stress and Unfolded Protein Response

Author

Jakub Golab, Marek Jakóbisiak, Paweł Mróz, Michael R. Hamblin, Tomasz Stoklosa, Piotr Mrówka, Eliza Głodkowska, Tadeusz Issat, Jan Gietka, Marek Bugajski, Tom Verfaillie, Patrizia Agostinis, Sylwia Janowska, Jacek Bil, Pawel Salwa, Izabela Młynarczuk-Biały, Cezary Wójcik, Marek Kujawa, Grzegorz M. Wilczyński, Dominika Nowis, Marcin Makowski, and Angelika Szokalska

Abstract

Supplementary Figure 1 from Proteasome Inhibition Potentiates Antitumor Effects of Photodynamic Therapy in Mice through Induction of Endoplasmic Reticulum Stress and Unfolded Protein Response

Published

2023

3. Supplementary Figure 6 from Proteasome Inhibition Potentiates Antitumor Effects of Photodynamic Therapy in Mice through Induction of Endoplasmic Reticulum Stress and Unfolded Protein Response

Author

Jakub Golab, Marek Jakóbisiak, Paweł Mróz, Michael R. Hamblin, Tomasz Stoklosa, Piotr Mrówka, Eliza Głodkowska, Tadeusz Issat, Jan Gietka, Marek Bugajski, Tom Verfaillie, Patrizia Agostinis, Sylwia Janowska, Jacek Bil, Pawel Salwa, Izabela Młynarczuk-Biały, Cezary Wójcik, Marek Kujawa, Grzegorz M. Wilczyński, Dominika Nowis, Marcin Makowski, and Angelika Szokalska

Abstract

Supplementary Figure 6 from Proteasome Inhibition Potentiates Antitumor Effects of Photodynamic Therapy in Mice through Induction of Endoplasmic Reticulum Stress and Unfolded Protein Response

Published

2023

4. Supplementary Figure 4 from Proteasome Inhibition Potentiates Antitumor Effects of Photodynamic Therapy in Mice through Induction of Endoplasmic Reticulum Stress and Unfolded Protein Response

Author

Jakub Golab, Marek Jakóbisiak, Paweł Mróz, Michael R. Hamblin, Tomasz Stoklosa, Piotr Mrówka, Eliza Głodkowska, Tadeusz Issat, Jan Gietka, Marek Bugajski, Tom Verfaillie, Patrizia Agostinis, Sylwia Janowska, Jacek Bil, Pawel Salwa, Izabela Młynarczuk-Biały, Cezary Wójcik, Marek Kujawa, Grzegorz M. Wilczyński, Dominika Nowis, Marcin Makowski, and Angelika Szokalska

Abstract

Supplementary Figure 4 from Proteasome Inhibition Potentiates Antitumor Effects of Photodynamic Therapy in Mice through Induction of Endoplasmic Reticulum Stress and Unfolded Protein Response

Published

2023

5. Supplementary Table 1, Methods and Materials, Figure Legends 1-6 from Proteasome Inhibition Potentiates Antitumor Effects of Photodynamic Therapy in Mice through Induction of Endoplasmic Reticulum Stress and Unfolded Protein Response

Author

Jakub Golab, Marek Jakóbisiak, Paweł Mróz, Michael R. Hamblin, Tomasz Stoklosa, Piotr Mrówka, Eliza Głodkowska, Tadeusz Issat, Jan Gietka, Marek Bugajski, Tom Verfaillie, Patrizia Agostinis, Sylwia Janowska, Jacek Bil, Pawel Salwa, Izabela Młynarczuk-Biały, Cezary Wójcik, Marek Kujawa, Grzegorz M. Wilczyński, Dominika Nowis, Marcin Makowski, and Angelika Szokalska

Abstract

Supplementary Table 1, Methods and Materials, Figure Legends 1-6 from Proteasome Inhibition Potentiates Antitumor Effects of Photodynamic Therapy in Mice through Induction of Endoplasmic Reticulum Stress and Unfolded Protein Response

Published

2023

6. Supplementary Figure 5 from Proteasome Inhibition Potentiates Antitumor Effects of Photodynamic Therapy in Mice through Induction of Endoplasmic Reticulum Stress and Unfolded Protein Response

Author

Jakub Golab, Marek Jakóbisiak, Paweł Mróz, Michael R. Hamblin, Tomasz Stoklosa, Piotr Mrówka, Eliza Głodkowska, Tadeusz Issat, Jan Gietka, Marek Bugajski, Tom Verfaillie, Patrizia Agostinis, Sylwia Janowska, Jacek Bil, Pawel Salwa, Izabela Młynarczuk-Biały, Cezary Wójcik, Marek Kujawa, Grzegorz M. Wilczyński, Dominika Nowis, Marcin Makowski, and Angelika Szokalska

Abstract

Supplementary Figure 5 from Proteasome Inhibition Potentiates Antitumor Effects of Photodynamic Therapy in Mice through Induction of Endoplasmic Reticulum Stress and Unfolded Protein Response

Published

2023

7. Data from Proteasome Inhibition Potentiates Antitumor Effects of Photodynamic Therapy in Mice through Induction of Endoplasmic Reticulum Stress and Unfolded Protein Response

Author

Jakub Golab, Marek Jakóbisiak, Paweł Mróz, Michael R. Hamblin, Tomasz Stoklosa, Piotr Mrówka, Eliza Głodkowska, Tadeusz Issat, Jan Gietka, Marek Bugajski, Tom Verfaillie, Patrizia Agostinis, Sylwia Janowska, Jacek Bil, Pawel Salwa, Izabela Młynarczuk-Biały, Cezary Wójcik, Marek Kujawa, Grzegorz M. Wilczyński, Dominika Nowis, Marcin Makowski, and Angelika Szokalska

Abstract

Photodynamic therapy (PDT) is an approved therapeutic procedure that exerts cytotoxic activity toward tumor cells by inducing production of reactive oxygen species such as singlet oxygen. PDT leads to oxidative damage of cellular macromolecules, including proteins that undergo multiple modifications such as fragmentation, cross-linking, and carbonylation that result in protein unfolding and aggregation. Because the major mechanism for elimination of carbonylated proteins is their degradation by proteasomes, we hypothesized that a combination of PDT with proteasome inhibitors might lead to accumulation of carbonylated proteins in endoplasmic reticulum (ER), aggravated ER stress, and potentiated cytotoxicity toward tumor cells. We observed that Photofrin-mediated PDT leads to robust carbonylation of cellular proteins and induction of unfolded protein response. Pretreatment of tumor cells with three different proteasome inhibitors, including bortezomib, MG132, and PSI, gave increased accumulation of carbonylated and ubiquitinated proteins in PDT-treated cells. Proteasome inhibitors effectively sensitized tumor cells of murine (EMT6 and C-26) as well as human (HeLa) origin to PDT-mediated cytotoxicity. Significant retardation of tumor growth with 60% to 100% complete responses was observed in vivo in two different murine tumor models (EMT6 and C-26) when PDT was combined with either bortezomib or PSI. Altogether, these observations indicate that combination of PDT with proteasome inhibitors leads to potentiated antitumor effects. The results of these studies are of immediate clinical application because bortezomib is a clinically approved drug that undergoes extensive clinical evaluations for the treatment of solid tumors. [Cancer Res 2009;69(10):4235–43]

Published

2023

8. Supplementary Figure 2 from Proteasome Inhibition Potentiates Antitumor Effects of Photodynamic Therapy in Mice through Induction of Endoplasmic Reticulum Stress and Unfolded Protein Response

Author

Jakub Golab, Marek Jakóbisiak, Paweł Mróz, Michael R. Hamblin, Tomasz Stoklosa, Piotr Mrówka, Eliza Głodkowska, Tadeusz Issat, Jan Gietka, Marek Bugajski, Tom Verfaillie, Patrizia Agostinis, Sylwia Janowska, Jacek Bil, Pawel Salwa, Izabela Młynarczuk-Biały, Cezary Wójcik, Marek Kujawa, Grzegorz M. Wilczyński, Dominika Nowis, Marcin Makowski, and Angelika Szokalska

Abstract

Supplementary Figure 2 from Proteasome Inhibition Potentiates Antitumor Effects of Photodynamic Therapy in Mice through Induction of Endoplasmic Reticulum Stress and Unfolded Protein Response

Published

2023

9. Supplementary Figure 3 from Proteasome Inhibition Potentiates Antitumor Effects of Photodynamic Therapy in Mice through Induction of Endoplasmic Reticulum Stress and Unfolded Protein Response

Author

Jakub Golab, Marek Jakóbisiak, Paweł Mróz, Michael R. Hamblin, Tomasz Stoklosa, Piotr Mrówka, Eliza Głodkowska, Tadeusz Issat, Jan Gietka, Marek Bugajski, Tom Verfaillie, Patrizia Agostinis, Sylwia Janowska, Jacek Bil, Pawel Salwa, Izabela Młynarczuk-Biały, Cezary Wójcik, Marek Kujawa, Grzegorz M. Wilczyński, Dominika Nowis, Marcin Makowski, and Angelika Szokalska

Abstract

Supplementary Figure 3 from Proteasome Inhibition Potentiates Antitumor Effects of Photodynamic Therapy in Mice through Induction of Endoplasmic Reticulum Stress and Unfolded Protein Response

Published

2023

10. Stable synthetic bacteriochlorins overcome the resistance of melanoma to photodynamic therapy

Author

Artemissia-Phoebe Nifli, K. Eszter Borbas, Margaret E. Sherwood, Pawel Mroz, Dewey Holten, Thiagarajan Balasubramanian, James R. Diers, Christian Ruzié, Angelika Szokalska, Michael R. Hamblin, Dazhong Fan, Sahar Janjua, Timur Zhiyentayev, Eunkyung Yang, Michael Krayer, Jonathan S. Lindsey, Ying-Ying Huang, Hooi Ling Kee, Christine Kirmaier, and David F. Bocian

Subjects

Male, Fluorescence-lifetime imaging microscopy, Pathology, medicine.medical_specialty, Porphyrins, medicine.medical_treatment, Photodynamic therapy, Biology, Biochemistry, Research Communications, Melanin, Mice, Microscopy, Electron, Transmission, In vivo, Cell Line, Tumor, Genetics, medicine, Animals, Melanoma, Molecular Biology, Melanosome, Molecular Structure, medicine.disease, In vitro, Mice, Inbred C57BL, Cell killing, Microscopy, Fluorescence, Photochemotherapy, Cancer research, Biotechnology

Abstract

Cutaneous malignant melanoma remains a therapeutic challenge, and patients with advanced disease have limited survival. Photodynamic therapy (PDT) has been successfully used to treat many malignancies, and it may show promise as an antimelanoma modality. However, high melanin levels in melanomas can adversely affect PDT effectiveness. Herein the extent of melanin contribution to melanoma resistance to PDT was investigated in a set of melanoma cell lines that markedly differ in the levels of pigmentation; 3 new bacteriochlorins successfully overcame the resistance. Cell killing studies determined that bacteriochlorins are superior at (LD50≈0.1 μM) when compared with controls such as the FDA-approved Photofrin (LD50≈10 μM) and clinically tested LuTex (LD50≈1 μM). The melanin content affects PDT effectiveness, but the degree of reduction is significantly lower for bacteriochlorins than for Photofrin. Microscopy reveals that the least effective bacteriochlorin localizes predominantly in lysosomes, while the most effective one preferentially accumulates in mitochondria. Interestingly all bacteriochlorins accumulate in melanosomes, and subsequent illumination leads to melanosomal damage shown by electron microscopy. Fluorescent probes show that the most effective bacteriochlorin produces significantly higher levels of hydroxyl radicals, and this is consistent with the redox properties suggested by molecular-orbital calculations. The best in vitro performing bacteriochlorin was tested in vivo in a mouse melanoma model using spectrally resolved fluorescence imaging and provided significant survival advantage with 20% of cures (P

Published

2010

11. Approaches to improve photodynamic therapy of cancer

Author

Marta Swiech, Dominika Nowis, Pawel Salwa, Magdalena Winiarska, Angelika Szokalska, Kamil Bojarczuk, Malgorzata Firczuk, and Malgorzata Jodlowska

Subjects

Skin Neoplasms, medicine.medical_treatment, High selectivity, Photodynamic therapy, Antineoplastic Agents, Adaptive Immunity, Immune system, Neoplasms, medicine, Ambulatory Care, Combined Modality Therapy, Animals, Humans, Nanotechnology, Photosensitizing Agents, business.industry, Cancer, Tumor therapy, medicine.disease, Tumor Cell Biology, Radiation therapy, Oxidative Stress, Photochemotherapy, Cancer research, business, Reactive Oxygen Species

Abstract

Photodynamic therapy (PDT) is a clinically approved method of tumor treatment. Its unique mechanism of action results from minimal invasiveness and high selectivity towards transformed cells. However, visible light used to excite most photosensitizers has rather limited ability to penetrate tissues resulting in insufficient destruction of deeply seated malignant cells. Therefore, novel strategies for further potentiation of the anticancer effectiveness of PDT have been developed. These include combined treatments with surgery, chemo- and radiotherapy, strategies targeting cytoprotective mechanisms induced in PDT-treated cells, as well as attempts aimed at enhancement of PDT-mediated antitumor immune response. Moreover, new photosensitizers and novel light sources are being developed. Impressive progress in nanotechnology and understanding of tumor cell biology rise hopes for further improvements in this elegant and promising method of cancer treatment.

Published

2011

12. Photodynamic Therapy of Tumors Can Lead to Development of Systemic Antigen-Specific Immune Response

Author

Angelika Szokalska, Michael R. Hamblin, Pawel Mroz, Mei X. Wu, Harvard University--MIT Division of Health Sciences and Technology, Hamblin, Michael R., and Wu, Mei X.

Subjects

Anatomy and Physiology, Mouse, medicine.medical_treatment, Cancer Treatment, lcsh:Medicine, Photodynamic therapy, CD8-Positive T-Lymphocytes, Epitope, Mice, 0302 clinical medicine, Immune Physiology, Cytotoxic T cell, Pharmacology (medical), lcsh:Science, Mice, Inbred BALB C, Multidisciplinary, Photosensitizing Agents, T Cells, Animal Models, Acquired immune system, Flow Cytometry, Tumor antigen, 3. Good health, Oncology, 030220 oncology & carcinogenesis, Colonic Neoplasms, Medicine, Immunotherapy, Dimerization, Research Article, Tumor Immunology, Immune Cells, Immunology, Biophysics, Radiation Therapy, Antineoplastic Agents, Dermatology, Biology, 03 medical and health sciences, Interferon-gamma, Immune system, Model Organisms, Antigen, Immunity, Cell Line, Tumor, Gastrointestinal Tumors, medicine, Animals, Antigens, business.industry, Tumor Necrosis Factor-alpha, lcsh:R, Cancers and Neoplasms, Immunologic Subspecialties, Disease Models, Animal, Photochemotherapy, Immune System, Cancer research, lcsh:Q, business, Reactive Oxygen Species, 030215 immunology

Abstract

Background: The mechanism by which the immune system can effectively recognize and destroy tumors is dependent on recognition of tumor antigens. The molecular identity of a number of these antigens has recently been identified and several immunotherapies have explored them as targets. Photodynamic therapy (PDT) is an anti-cancer modality that uses a non-toxic photosensitizer and visible light to produce cytotoxic reactive oxygen species that destroy tumors. PDT has been shown to lead to local destruction of tumors as well as to induction of anti-tumor immune response. Methodology/Principal Findings: We used a pair of equally lethal BALB/c colon adenocarcinomas, CT26 wild-type (CT26WT) and CT26.CL25 that expressed a tumor antigen, β-galactosidase (β-gal), and we treated them with vascular PDT. All mice bearing antigen-positive, but not antigen-negative tumors were cured and resistant to rechallenge. T lymphocytes isolated from cured mice were able to specifically lyse antigen positive cells and recognize the epitope derived from beta-galactosidase antigen. PDT was capable of destroying distant, untreated, established, antigen-expressing tumors in 70% of the mice. The remaining 30% escaped destruction due to loss of expression of tumor antigen. The PDT anti-tumor effects were completely abrogated in the absence of the adaptive immune response. Conclusion: Understanding the role of antigen-expression in PDT immune response may allow application of PDT in metastatic as well as localized disease. To the best of our knowledge, this is the first time that PDT has been shown to lead to systemic, antigen- specific anti-tumor immunity., United States. National Cancer Institute (grant RO1CA/AI838801), United States. National Cancer Institute (grant R01AI050875)

Published

2010

13. Proteasome inhibition potentiates antitumor effects of photodynamic therapy in mice through induction of endoplasmic reticulum stress and unfolded protein response

Author

Tom Verfaillie, Eliza Glodkowska, Pawel Salwa, Angelika Szokalska, Dominika Nowis, Sylwia Janowska, Izabela Mlynarczuk-Bialy, Marek Jakóbisiak, Jacek Bil, Tomasz Stoklosa, Tadeusz Issat, Michael R. Hamblin, Piotr Mrowka, Jan Gietka, Pawel Mroz, Marek Kujawa, Patrizia Agostinis, Cezary Wojcik, Jakub Golab, Marcin Makowski, Marek Bugajski, and Grzegorz M. Wilczynski

Subjects

Cancer Research, Protein Denaturation, Porphyrins, medicine.medical_treatment, Photodynamic therapy, Antineoplastic Agents, Biology, Adenocarcinoma, Endoplasmic Reticulum, Article, chemistry.chemical_compound, Mice, Ubiquitin, Cell Line, Tumor, Neoplasms, MG132, medicine, Animals, Humans, Mice, Inbred BALB C, Singlet Oxygen, Bortezomib, Endoplasmic reticulum, Verteporfin, Molecular biology, Oncology, chemistry, Proteasome, Photochemotherapy, Colonic Neoplasms, Cancer research, biology.protein, Proteasome inhibitor, Unfolded protein response, Dihematoporphyrin Ether, Reactive Oxygen Species, Proteasome Inhibitors, medicine.drug, HeLa Cells

Abstract

Photodynamic therapy (PDT) is an approved therapeutic procedure that exerts cytotoxic activity toward tumor cells by inducing production of reactive oxygen species such as singlet oxygen. PDT leads to oxidative damage of cellular macromolecules, including proteins that undergo multiple modifications such as fragmentation, cross-linking, and carbonylation that result in protein unfolding and aggregation. Because the major mechanism for elimination of carbonylated proteins is their degradation by proteasomes, we hypothesized that a combination of PDT with proteasome inhibitors might lead to accumulation of carbonylated proteins in endoplasmic reticulum (ER), aggravated ER stress, and potentiated cytotoxicity toward tumor cells. We observed that Photofrin-mediated PDT leads to robust carbonylation of cellular proteins and induction of unfolded protein response. Pretreatment of tumor cells with three different proteasome inhibitors, including bortezomib, MG132, and PSI, gave increased accumulation of carbonylated and ubiquitinated proteins in PDT-treated cells. Proteasome inhibitors effectively sensitized tumor cells of murine (EMT6 and C-26) as well as human (HeLa) origin to PDT-mediated cytotoxicity. Significant retardation of tumor growth with 60% to 100% complete responses was observed in vivo in two different murine tumor models (EMT6 and C-26) when PDT was combined with either bortezomib or PSI. Altogether, these observations indicate that combination of PDT with proteasome inhibitors leads to potentiated antitumor effects. The results of these studies are of immediate clinical application because bortezomib is a clinically approved drug that undergoes extensive clinical evaluations for the treatment of solid tumors. [Cancer Res 2009;69(10):4235–43]

Published

2009

14. Zinc protoporphyrin IX, a heme oxygenase-1 inhibitor, demonstrates potent antitumor effects but is unable to potentiate antitumor effects of chemotherapeutics in mice

Author

Pawel Salwa, Jakub Golab, Tadeusz Issat, Marek Bugajski, Angelika Szokalska, Jacek Bil, Tomasz Stoklosa, Magdalena Winiarska, Alicja Jozkowicz, Jozef Dulak, Halina Was, and Dominika Nowis

Subjects

Cancer Research, Melanoma, Experimental, Protoporphyrins, Apoptosis, Biology, Transfection, lcsh:RC254-282, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, Cell Line, Tumor, Antineoplastic Combined Chemotherapy Protocols, Genetics, Cytotoxic T cell, Animals, Humans, Propidium iodide, Enzyme Inhibitors, RNA, Small Interfering, Clonogenic assay, 030304 developmental biology, 0303 health sciences, Mice, Inbred BALB C, Cell Cycle, Neoplasms, Experimental, Cell cycle, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Cytostatic Agents, Molecular biology, 3. Good health, Heme oxygenase, Transplantation, Oncology, chemistry, Cell culture, 030220 oncology & carcinogenesis, Cancer research, Female, Heme Oxygenase-1, Neoplasm Transplantation, Research Article

Abstract

Background HO-1 participates in the degradation of heme. Its products can exert unique cytoprotective effects. Numerous tumors express high levels of HO-1 indicating that this enzyme might be a potential therapeutic target. In this study we decided to evaluate potential cytostatic/cytotoxic effects of zinc protoporphyrin IX (Zn(II)PPIX), a selective HO-1 inhibitor and to evaluate its antitumor activity in combination with chemotherapeutics. Methods Cytostatic/cytotoxic effects of Zn(II)PPIX were evaluated with crystal violet staining and clonogenic assay. Western blotting was used for the evaluation of protein expression. Flow cytometry was used to evaluate the influence of Zn(II)PPIX on the induction of apoptosis and generation of reactive oxygen species. Knock-down of HO-1 expression was achieved with siRNA. Antitumor effects of Zn(II)PPIX alone or in combination with chemotherapeutics were measured in transplantation tumor models. Results Zn(II)PPIX induced significant accumulation of reactive oxygen species in tumor cells. This effect was partly reversed by administration of exogenous bilirubin. Moreover, Zn(II)PPIX exerted potent cytostatic/cytotoxic effects against human and murine tumor cell lines. Despite a significant time and dose-dependent decrease in cyclin D expression in Zn(II)PPIX-treated cells no accumulation of tumor cells in G1 phase of the cell cycle was observed. However, incubation of C-26 cells with Zn(II)PPIX increased the percentage of cells in sub-G1 phase of the cells cycle. Flow cytometry studies with propidium iodide and annexin V staining as well as detection of cleaved caspase 3 by Western blotting revealed that Zn(II)PPIX can induce apoptosis of tumor cells. B16F10 melanoma cells overexpressing HO-1 and transplanted into syngeneic mice were resistant to either Zn(II)PPIX or antitumor effects of cisplatin. Zn(II)PPIX was unable to potentiate antitumor effects of 5-fluorouracil, cisplatin or doxorubicin in three different tumor models, but significantly potentiated toxicity of 5-FU and cisplatin. Conclusion Inhibition of HO-1 exerts antitumor effects but should not be used to potentiate antitumor effects of cancer chemotherapeutics unless procedures of selective tumor targeting of HO-1 inhibitors are developed.

Published

2008

15. Ciglitazone, an agonist of peroxisome proliferator-activated receptor γ, exerts potentiated cytostatic/cytotoxic effects against tumor cells when combined with lovastatin

Author

Tomasz Stoklosa, Magdalena Legat, Eliza Glodkowska, Marcin Makowski, Dominika Nowis, Jakub Golab, Marek Jakóbisiak, Angelika Szokalska, Sylwia Janowska, Tadeusz Issat, and Piotr Mrowka

Subjects

chemistry.chemical_classification, Agonist, Cancer Research, medicine.medical_specialty, Cell growth, medicine.drug_class, Peroxisome proliferator-activated receptor, Cell cycle, Pharmacology, Biology, Endocrinology, Oncology, chemistry, Internal medicine, Ciglitazone, HMG-CoA reductase, medicine, biology.protein, lipids (amino acids, peptides, and proteins), Lovastatin, Thiazolidinedione, medicine.drug

Abstract

Thiazolidinediones are ligands of PPAR-gamma, a member of the nuclear receptor family. These drugs have shown promising pre-clinical activity in tumor models but clinical studies failed to confirm their beneficial effect. We have studied the in vitro antitumor effects of a combination of ciglitazone, a thiazolidinedione drug, and lovastatin, an inhibitor of 3-hydroxy-3-methylglutaryl-coenzyme A reductase. We observed a marked synergism in several different tumor cell lines resulting from both inhibition of cell proliferation and induction of apoptosis. These results strongly suggest that combining PPAR-gamma agonists with statins can produce significant antitumor effects.

Published

2008

16. Zinc protoporphyrin IX, a heme oxygenase-I inhibitor, demonstrates potent antitumor effects but is unable to potentiate antitumor effects of chemotherapeutics in mice

Author

Nowis, Dominika, Bugajski, Marek, Winiarska, Magdalena, Bil, Jacek, Szokalska, Angelika, Salwa, Pawel, Issat, Tadeusz, Waś, Halina, Józkowicz, Alicja, Dulak, Józef, Stoklosa, Tomasz, and Golab, Jakub

Subjects

zinc protoporphyrin, B16F10 cell, antitumor effect, biliverdin, crystal violet staining

Published

2008

17. Photodynamic Therapy of Tumors Can Lead to Development of Systemic Antigen-Specific Immune Response

Author

Harvard University--MIT Division of Health Sciences and Technology, Hamblin, Michael R., Wu, Mei X., Mroz, Pawel, Szokalska, Angelika, Harvard University--MIT Division of Health Sciences and Technology, Hamblin, Michael R., Wu, Mei X., Mroz, Pawel, and Szokalska, Angelika

Abstract

Background: The mechanism by which the immune system can effectively recognize and destroy tumors is dependent on recognition of tumor antigens. The molecular identity of a number of these antigens has recently been identified and several immunotherapies have explored them as targets. Photodynamic therapy (PDT) is an anti-cancer modality that uses a non-toxic photosensitizer and visible light to produce cytotoxic reactive oxygen species that destroy tumors. PDT has been shown to lead to local destruction of tumors as well as to induction of anti-tumor immune response. Methodology/Principal Findings: We used a pair of equally lethal BALB/c colon adenocarcinomas, CT26 wild-type (CT26WT) and CT26.CL25 that expressed a tumor antigen, β-galactosidase (β-gal), and we treated them with vascular PDT. All mice bearing antigen-positive, but not antigen-negative tumors were cured and resistant to rechallenge. T lymphocytes isolated from cured mice were able to specifically lyse antigen positive cells and recognize the epitope derived from beta-galactosidase antigen. PDT was capable of destroying distant, untreated, established, antigen-expressing tumors in 70% of the mice. The remaining 30% escaped destruction due to loss of expression of tumor antigen. The PDT anti-tumor effects were completely abrogated in the absence of the adaptive immune response. Conclusion: Understanding the role of antigen-expression in PDT immune response may allow application of PDT in metastatic as well as localized disease. To the best of our knowledge, this is the first time that PDT has been shown to lead to systemic, antigen- specific anti-tumor immunity., United States. National Cancer Institute (grant RO1CA/AI838801), United States. National Cancer Institute (grant R01AI050875)

Published

2011

18. Stable synthetic bacteriochlorins overcome the resistance of melanoma to photodynamic therapy.

Author

Mroz, Pawel, Huang, Ying-Ying, Szokalska, Angelika, Zhiyentayev, Timur, Janjua, Sahar, Nifli, Artemissia-Phoebe, Sherwood, Margaret E, Ruzié, Christian, Borbas, K Eszter, Fan, Dazhong, Krayer, Michael, Balasubramanian, Thiagarajan, Yang, Eunkyung, Kee, Hooi Ling, Kirmaier, Christine, Diers, James R, Bocian, David F, Holten, Dewey, Lindsey, Jonathan S, Hamblin, Michael R, Mroz, Pawel, Huang, Ying-Ying, Szokalska, Angelika, Zhiyentayev, Timur, Janjua, Sahar, Nifli, Artemissia-Phoebe, Sherwood, Margaret E, Ruzié, Christian, Borbas, K Eszter, Fan, Dazhong, Krayer, Michael, Balasubramanian, Thiagarajan, Yang, Eunkyung, Kee, Hooi Ling, Kirmaier, Christine, Diers, James R, Bocian, David F, Holten, Dewey, Lindsey, Jonathan S, and Hamblin, Michael R

Abstract

Cutaneous malignant melanoma remains a therapeutic challenge, and patients with advanced disease have limited survival. Photodynamic therapy (PDT) has been successfully used to treat many malignancies, and it may show promise as an antimelanoma modality. However, high melanin levels in melanomas can adversely affect PDT effectiveness. Herein the extent of melanin contribution to melanoma resistance to PDT was investigated in a set of melanoma cell lines that markedly differ in the levels of pigmentation; 3 new bacteriochlorins successfully overcame the resistance. Cell killing studies determined that bacteriochlorins are superior at (LD(50) approximately 0.1 microM) when compared with controls such as the FDA-approved Photofrin (LD(50) approximately 10 microM) and clinically tested LuTex (LD(50) approximately 1 microM). The melanin content affects PDT effectiveness, but the degree of reduction is significantly lower for bacteriochlorins than for Photofrin. Microscopy reveals that the least effective bacteriochlorin localizes predominantly in lysosomes, while the most effective one preferentially accumulates in mitochondria. Interestingly all bacteriochlorins accumulate in melanosomes, and subsequent illumination leads to melanosomal damage shown by electron microscopy. Fluorescent probes show that the most effective bacteriochlorin produces significantly higher levels of hydroxyl radicals, and this is consistent with the redox properties suggested by molecular-orbital calculations. The best in vitro performing bacteriochlorin was tested in vivo in a mouse melanoma model using spectrally resolved fluorescence imaging and provided significant survival advantage with 20% of cures (P<0.01)., Journal Article, Research Support, N.I.H. Extramural, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published

2010

19. Photodynamic Therapy of Tumors Can Lead to Development of Systemic Antigen-Specific Immune Response

Author

Mroz, Pawel, primary, Szokalska, Angelika, additional, Wu, Mei X., additional, and Hamblin, Michael R., additional

Published

2010

20. Proteasome Inhibition Potentiates Antitumor Effects of Photodynamic Therapy in Mice through Induction of Endoplasmic Reticulum Stress and Unfolded Protein Response

Author

Szokalska, Angelika, primary, Makowski, Marcin, additional, Nowis, Dominika, additional, Wilczyński, Grzegorz M., additional, Kujawa, Marek, additional, Wójcik, Cezary, additional, Młynarczuk-Biały, Izabela, additional, Salwa, Pawel, additional, Bil, Jacek, additional, Janowska, Sylwia, additional, Agostinis, Patrizia, additional, Verfaillie, Tom, additional, Bugajski, Marek, additional, Gietka, Jan, additional, Issat, Tadeusz, additional, Głodkowska, Eliza, additional, Mrówka, Piotr, additional, Stoklosa, Tomasz, additional, Hamblin, Michael R., additional, Mróz, Paweł, additional, Jakóbisiak, Marek, additional, and Golab, Jakub, additional

Published

2009

21. Zinc protoporphyrin IX, a heme oxygenase-1 inhibitor, demonstrates potent antitumor effects but is unable to potentiate antitumor effects of chemotherapeutics in mice

Author

Nowis, Dominika, primary, Bugajski, Marek, additional, Winiarska, Magdalena, additional, Bil, Jacek, additional, Szokalska, Angelika, additional, Salwa, Pawel, additional, Issat, Tadeusz, additional, Was, Halina, additional, Jozkowicz, Alicja, additional, Dulak, Jozef, additional, Stoklosa, Tomasz, additional, and Golab, Jakub, additional

Published

2008

22. Photodynamic Therapy of Tumors Can Lead to Development of Systemic Antigen-Specific Immune Response

Author

Szokalska, Angelika, Mroz, Pawel A., Wu, Mei X., and Hamblin, Michael

Abstract

Background: The mechanism by which the immune system can effectively recognize and destroy tumors is dependent on recognition of tumor antigens. The molecular identity of a number of these antigens has recently been identified and several immunotherapies have explored them as targets. Photodynamic therapy (PDT) is an anti-cancer modality that uses a non-toxic photosensitizer and visible light to produce cytotoxic reactive oxygen species that destroy tumors. PDT has been shown to lead to local destruction of tumors as well as to induction of anti-tumor immune response. Methodology/Principal Findings: We used a pair of equally lethal BALB/c colon adenocarcinomas, CT26 wild-type (CT26WT) and CT26.CL25 that expressed a tumor antigen, β-galactosidase (β-gal), and we treated them with vascular PDT. All mice bearing antigen-positive, but not antigen-negative tumors were cured and resistant to rechallenge. T lymphocytes isolated from cured mice were able to specifically lyse antigen positive cells and recognize the epitope derived from beta-galactosidase antigen. PDT was capable of destroying distant, untreated, established, antigen-expressing tumors in 70% of the mice. The remaining 30% escaped destruction due to loss of expression of tumor antigen. The PDT anti-tumor effects were completely abrogated in the absence of the adaptive immune response. Conclusion: Understanding the role of antigen-expression in PDT immune response may allow application of PDT in metastatic as well as localized disease. To the best of our knowledge, this is the first time that PDT has been shown to lead to systemic, antigen- specific anti-tumor immunity.

Published

2010

23. Photodynamic therapy of tumors can lead to development of systemic antigen-specific immune response.

Author

Pawel Mroz, Angelika Szokalska, Mei X Wu, and Michael R Hamblin

Subjects

Medicine, Science

Abstract

The mechanism by which the immune system can effectively recognize and destroy tumors is dependent on recognition of tumor antigens. The molecular identity of a number of these antigens has recently been identified and several immunotherapies have explored them as targets. Photodynamic therapy (PDT) is an anti-cancer modality that uses a non-toxic photosensitizer and visible light to produce cytotoxic reactive oxygen species that destroy tumors. PDT has been shown to lead to local destruction of tumors as well as to induction of anti-tumor immune response.We used a pair of equally lethal BALB/c colon adenocarcinomas, CT26 wild-type (CT26WT) and CT26.CL25 that expressed a tumor antigen, β-galactosidase (β-gal), and we treated them with vascular PDT. All mice bearing antigen-positive, but not antigen-negative tumors were cured and resistant to rechallenge. T lymphocytes isolated from cured mice were able to specifically lyse antigen positive cells and recognize the epitope derived from beta-galactosidase antigen. PDT was capable of destroying distant, untreated, established, antigen-expressing tumors in 70% of the mice. The remaining 30% escaped destruction due to loss of expression of tumor antigen. The PDT anti-tumor effects were completely abrogated in the absence of the adaptive immune response.Understanding the role of antigen-expression in PDT immune response may allow application of PDT in metastatic as well as localized disease. To the best of our knowledge, this is the first time that PDT has been shown to lead to systemic, antigen- specific anti-tumor immunity.

Published

2010