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102. Complessi trans di rutenio come agenti antineoplastici

Author

G. MESTRONI, F. QUADRIFOGLIO, S. CAUCI, ALESSIO, ENZO, SAVA, GIANNI, ZORZET, SONIA, G., Mestroni, F., Quadrifoglio, S., Cauci, Alessio, Enzo, Sava, Gianni, and Zorzet, Sonia

Subjects
ruthenium, anticancer
Published
1987

104. Chemical, biological and antitumor properties of ruthenium-dimethylsulfoxide complexes

Author

Mestroni, G., Alessio, Enzo, Calligaris, M., Attia, W. M., Quadrifoglio, F., Cauci, S., Sava, Gianni, Zorzet, Sonia, Pacor, Sabrina, MONTI BRAGADIN, C., Tamaro, M., Dolzani, Lucilla, AUTORI VARI, G., Mestroni, Alessio, Enzo, M., Calligari, W. M., Attia, F., Quadrifoglio, S., Cauci, Sava, Gianni, Zorzet, Sonia, Pacor, Sabrina, C., MONTI BRAGADIN, M., Tamaro, and Dolzani, Lucilla

Subjects
metal anticancer compounds, ruthenium, DNA, metal anticancer compound
Published
1989

106. DTIC e i suoi derivati: farmaci citotossici o antimetastatici?

Author

GIRALDI, TULLIO, SAVA, GIANNI, PERISSIN, LAURA, ZORZET, SONIA, TAMARO, MARISA, DOLZANI, LUCILLA, Giraldi, Tullio, Sava, Gianni, Perissin, Laura, Zorzet, Sonia, Tamaro, Marisa, and Dolzani, Lucilla

Subjects
DTIC, farmaci antimetastatici
Published
1985

107. Metal complexes of platinum group: the promising antitumor features of cis-dichlorotetrakis(dimethylsulfoxide)Ru(II) (cis- RuCl2(DMSO)4) and related complexes

Author

Alessio, Enzo, Attia, W., Calligaris, M., Cauci, S., Dolzani, Lucilla, Mestroni, G., MONTI BRAGADIN, C., Nardin, G., Quadrifoglio, F., Sava, Gianni, Tamaro, M., Zorzet, Sonia, AUTORI VARI, Alessio, Enzo, W., Attia, M., Calligari, S., Cauci, Dolzani, Lucilla, G., Mestroni, C., MONTI BRAGADIN, G., Nardin, F., Quadrifoglio, Sava, Gianni, M., Tamaro, and Zorzet, Sonia

Subjects
metal anticancer compounds, ruthenium, metal anticancer compound
Published
1988

108. Is effectiveness of cancer chemotherapy influenced by stress?

Author

Giraldi, T., Perissin, L., Sava, Gianni, Zorzet, Sonia, Nicpali, S., Rodani, M. G., A Lobo, A Tres, Giraldi, T., Perissin, L., Sava, Gianni, Zorzet, Sonia, Nicpali, S., and Rodani, M. G.

Subjects
Psicosomatica, Cancer, Drug response
Published
1988

109. Therapeutic activity of ICRF-159 combined with surgery: effects of postsurgical treatment with cyclophosphamide in mice bearing Lewis lung carcinoma lines

Author

Sava, G., Zorzet Sonia, Perissin, L., Sava, Gianni, Zorzet, Sonia, and Perissin, L.

Subjects
Lung Neoplasms, Time Factors, Animal, Antineoplastic Agents, Razoxane, Cyclophosphamide, Tumours, Animals, Therapy, Combined Modality Therapy, Piperazines, Cell Line, Mice, Inbred C57BL, Mice, Antineoplastic Combined Chemotherapy Protocols, Tumour
Abstract

The therapeutic activity of the combined treatment with surgery and ICRF-159, measured in terms of increase of the survival time, has been tested in mice bearing two Lewis lung carcinoma lines having different potential to spontaneously metastasize (M1087 high; BM21548 low). As expected from the characteristics of this drug, a significant prolongation of the survival time of the treated hosts can be achieved only after presurgical treatment; the overall effect is greater using the tumor line with low metastatic ability. The response of the two tumor lines used to postoperative treatment with Cyclophosphamide also depends upon the tumor line used. The preoperative treatment of the animals with ICRF-159 markedly increases the response to Cyclophosphamide of the low responding M1087 line.

Published
1985

110. Proteinases and proteinase inhibition by cytotoxic and antimetastatic drugs in transplantable solid metastasizing tumors in mice

Author

Giraldi, T., Sava, G., Perissin, L., Zorzet Sonia, Giraldi, Tullio, Sava, Gianni, Perissin, L., and Zorzet, Sonia

Subjects
Lung Neoplasms, Inbred Strains, Mice, Inbred Strains, Antineoplastic Agents, Cathepsin, Cathepsin B, Cell Line, Antineoplastic Agent, Experimental, Mice, Plasminogen Activators, Neoplasms, Endopeptidases, Animals, Neoplasm Metastasis, Melanoma, Endopeptidase, Animal, Mammary Neoplasms, Cathepsins, Cysteine Endopeptidases, Mammary Neoplasms, Experimental, Mammary Neoplasm, Neoplasms, Experimental, Lung Neoplasm, Inbred Strain, Neoplasm Metastasi, Neoplasm, Cysteine Endopeptidase
Abstract

The tissue levels of two proteolytic enzymes, plasminogen activator and cathepsin B - like cysteine proteinase, which were found to be increased in malignant tumors and to be proportional to tumor metastatic potential in some instances, have been determined in a panel of solid metastasizing tumors in mice. The examination of B16 melanoma, MCa mammary carcinoma and of two lines of Lewis lung carcinoma with widely different potential to spontaneously metastasize, showed no correlation between metastatic potential and the tissue content of the proteinases considered. The treatment of the animals with cytotoxic antitumor drugs (CCNU, GANU, cisplatin, and cyclophosphamide) or with antimetastatic drugs acting with a mechanism unrelated with cytotoxicity (ICRF 159 and DM-COOK) caused only marginal inhibition in some instances, whereas no meaningful pattern of inhibition either based in terms of metastatic potential of the tumor or on drug mechanism of action was recognizable. A direct involvement of the two proteinases examined in the process of metastasis in the tumor panel used is thus not apparent, although a more complex interaction with other latent proteinases and inhibitors might be operative.

Published
1985

111. Ruthenium complexes with anti-neoplastic agent

Author

Mestroni, G, Alessio, Enzo, Quadrifoglio, F, Cauci, S, Sava, Gianni, Zorzet, Sonia, Mestroni, G, Alessio, Enzo, Quadrifoglio, F, Cauci, S, Sava, Gianni, and Zorzet, Sonia

Subjects
Chemotherapy, Antineoplastic, Ruthenium, Cancer
Published
1987

116. Infiltration of Liver and Brain by Tumor Cells in Leukemic Mice: Prevention by Dimethyltriazenes and Cyclophosphamide

Author

Sava, Gianni, Giraldi, Tullio, Perissin, Laura, Zorzet, Sonia, Maliardi, Franco, and Grill, Vittorio

Abstract

The dimethyltriazenes p-(3,3-dimethyl-1-triazeno)benzoic acid potassium salt (DM-COOK) and 5-(3,3-dimethyl-1-triazeno)-imidazole-4-carboxamide (DTIC) increase, unlike cyclophosphamide (Cy), the survival time of mice bearing L1210 lymphoid leukemia, P388 lymphocytic leukemia and TLX5 lymphoma with a mechanism unrelated to cytotoxicity for tumor cells. The in vivo bioassays of brains, and the histologic examinations of the livers of leukemic mice show that DM-COOK and DTIC prevent leukemic infiltration in these organs at dosages devoid of cytotoxic effects for peritoneal tumor cells. At a dosage equitoxic with that of dimethyltriazenes, cyclophosphamide causes the absence of tumor cells in the peritoneal cavity and in the brains and livers of mice bearing P388 and L1210 leukemias. DM-COOK and DTIC thus possess a mild or insignificant cytotoxic action together with antimetastatic properties also on mouse transplantable leukemias. The use of DM-COOK appears advantageous over that of cyclophosphamide and DTIC because of a reduced host toxicity, which is particularly evident for cyclophosphamide and DTIC on liver parenchyma and bone marrow.

Published
1984
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117. Suppression of metastatic potential and up-regulation of gelatinases and uPA in LLC by protracted <TOGGLE>in vivo</TOGGLE> treatment with dacarbazine or razoxane

Author

Garbisa, Spiridione, Onisto, Maurizio, Peron, Antonella, Perissin, Laura, Rapozzi, Valentina, Zorzet, Sonia, and Giraldi, Tullio

Abstract

Treatment of mouse Lewis lung carcinoma with razoxane or dacarbazine was protracted for 10 transplant generations. While the capacity of the treated tumors to grow locally in immuno-competent or in immuno-depressed hosts was retained and not significantly modified, the metastatic phenotype was eliminated when the treated tumor cells were transplanted into immuno-competent hosts. The reduction in metastatic potential was slightly less pronounced, in terms of both number and volume of metastases, when the treated tumor cells were transplanted into immuno-depressed hosts. These properties were retained after 3 transplant generations without treatment. Northern blotting and zymography of primary-tumor crude extracts revealed that treatment with either razoxane or dacarbazine for one generation approximately doubled the expression of MMP-2 and MMP-9, while lacking any effect on that of 1.0 and of 3.5 kb TIMP-2. When the treatment was maintained for 10 generations, the expression of MMP-2 and MMP-9 for both drugs showed up-regulation of approximately 10- and 2-fold respectively. TIMP-2 mRNA of 1.0 kb doubled its expression, while that of 3.5 kb registered just above the control. Dacarbazine doubled the expression of uPA after 10 generations, while razoxane boosted it approximately 3-fold after either 1 or 10 generations. The permanent loss of metastatic phenotype induced in Lewis lung carcinoma by dacarbazine and razoxane is thus attributable to biological mechanisms independent of down-regulation of expression and/or activation of the 2 gelatinases. Int. J. Cancer 72:1056–1061, 1997. © 1997 Wiley-Liss, Inc.

Published
1997
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119. Blockers of adrenergic neurons and receptors, tumor progression and effects of rotational stress in mice

Author

Perissin, L., Rapozzi, V., Zorzet Sonia, Giraldi, T., Perissin, L, Rapozzi, V, Zorzet, Sonia, and Giraldi, Tullio

Subjects
Lung Neoplasms, Reserpine, Rotation, Stre, Physiological, Stress, Adrenergic Agent, Carcinoma, Lewis Lung, Mice, Adrenergic Agents, Stress, Physiological, Inbred DBA, Animals, noma, Cyclophosphamide, Inbred BALB C, Mice, Inbred BALB C, Carci, Disease Progression, Female, Lewis Lung, Animal, Lung Neoplasm, Mice, Inbred DBA
Abstract

The aim of this work was to determine the possible participation of adrenergic responses to the increase in tumor dissemination induced by rotational stress using drugs affecting monoaminergic function. The growth of the primary tumor and the formation of lung metastasis were determined in mice implanted with Lewis lung carcinoma, subjected to rotational stress and treated with the adrenergic neuron blocker reserpine, the alpha-receptor blocker phenoxybenzamine, and the beta-blocker propranolol. Treatment with reserpine markedly reduced the formation of spontaneous lung metastasis and completely abolished the increase in metastases caused by rotational stress without direct effect on tumor cells or blood vessels. Phenoxybenzamine and propranolol caused opposite effects on tumor progression. Previous immunosuppression by cyclophosphamide in mice with tumors reduced the antimetastatic effects of reserpine. These results suggesting the importance of the adrenergic modulation of immune resistance factors in controlling metastasis development and indicate a possible role in monitoring the use and effects of monoaminergic drugs in cancer patients.

121. Antitumor properties of the immunoadjuvant peptidoglycan monomer PGM

Author

Sava, Gianni, Perssin, Laura, Zorzet, Sonia, Tomašić, Jelka, and Hrsak, Ivo

Subjects
peptidoglycan monomer, MCa mammary carcinoma, Lewis lung carcinoma, antitumor properties
Abstract

The antitumor effects of therapy with peptidoglycan monomer, combined with surgery were investigated. Timing od administration plays an important role on the overall effectiveness of such therapy.

Published
1984

122. RUTHENIUM (II) COMPLEXES WITH HIGH ANTITUMORAL AND ANTIMETASTATIC ACTIVITIES

Author

SIGEA SRL, MESTRONI GIOVANNI, ALESSIO ENZO, SAVA GIANNI, IENGO ELISABETTA, ZORZET SONIA, and BERGAMO ALBERTA

Subjects
C07F15/00
Abstract

The present invention is related to Ruthenium derived antitumoral compounds with high antimetastatic activity and with low toxicity for the host. It is described the use of inorganic Ruthenium complexes in the therapy of solid tumors, in particular of those tumors characterized by high metastatizing ability. Pharmaceutical compositions containing Ruthenium complexes in formulations suitable for the administration and a kit for the preparation of such complexes at the moment of use or immediately before use, are moreover described.

125. Activity and inhibition by cytotoxic and antimetastatic drugs of cathepsin B-like cysteine proteinase in transplantable leukemias in mice

Author

Giraldi, T., Sava, G., Zorzet Sonia, Perissin, L., and Piccini, P.

Subjects
Leukemia, Experimental, Lymphoma, Antineoplastic Agents, Mice, Inbred Strains, Cathepsin B, Cysteine Endopeptidases, Mice, Endopeptidases, Animals, Female, Protease Inhibitors, Neoplasm Metastasis, Triazenes, Razoxane, Neoplasm Transplantation
Abstract

The cellular levels of cathepsin B-like cysteine proteinases have been determined in a panel of transplantable mouse leukemias possessing a different potential to metastatize to the liver after i.p. implantation. The higher enzymatic activity observed in L1210 leukemic cells matches their higher capacity for hepatic infiltration. No significant difference is observed for TLX5 lymphoma and P388 leukemia, in spite of their different liver invasiveness, and their enzymatic levels do not significantly differ from that of the non-invasive Ehrlich ascitic carcinoma. The in vivo administration of the antimetastatic drugs ICRF159 and DM-COOK, or of the cytotoxic drugs cyclophosphamide, cisplatin, CCNU and GANU, does not cause a pattern of enzyme inhibition matching the tumor metastatic potential and the increase in life-span of the treated tumor bearing mice, indicating that the inhibition of cathepsin B-like cysteine proteinase is not involved in either their cytotoxic or their antimetastatic action.

133. The Inflammatory Feed-Forward Loop Triggered by the Complement Component C3 as a Potential Target in Endometriosis

Author

Andrea Balduit, Sonia Zorzet, Chiara Agostinis, Paolo Macor, Anna Martorana, Gaia Morello, Beatrice Belmonte, Alessandro Mangogna, Miriam Toffoli, Federico Romano, Roberta Bulla, Violetta Borelli, Giuseppe Ricci, Gabriella Zito, Uday Kishore, Agostinis C., Zorzet S., Balduit A., Zito G., Mangogna A., Macor P., Romano F., Toffoli M., Belmonte B., Morello G., Martorana A., Borelli V., Ricci G., Kishore U., Bulla R., Agostinis, Chiara, Zorzet, Sonia, Balduit, Andrea, Zito, Gabriella, Mangogna, Alessandro, Macor, Paolo, Romano, Federico, Toffoli, Miriam, Belmonte, Beatrice, Morello, Gaia, Martorana, Anna, Borelli, Violetta, Ricci, Giuseppe, Kishore, Uday, and Bulla, Roberta

Subjects
endometriosis, THP-1 Cells, TNF-a, mast cells, Peritoneal Diseases, Cell Degranulation, Endometrium, Immunology and Allergy, Original Research, Mice, Knockout, medicine.diagnostic_test, endometriosi, Complement C3, Hep G2 Cells, Antibody opsonization, medicine.anatomical_structure, Complement C3a, Tumor necrosis factor alpha, Female, Inflammation Mediators, Signal Transduction, Immunology, Biology, Settore MED/08 - Anatomia Patologica, Immunofluorescence, Peritoneal cavity, Peritoneum, medicine, Animals, Humans, Settore MED/05 - Patologia Clinica, C3, complement system, Innate immune system, Tumor Necrosis Factor-alpha, Peritoneal fluid, RC581-607, Coculture Techniques, Immunity, Innate, Complement system, Immunity, Humoral, Mice, Inbred C57BL, Disease Models, Animal, Case-Control Studies, TNF-α, Cancer research, Peritoneal Disease, Immunologic diseases. Allergy, mast cell
Abstract

Copyright © 2021 Agostinis, Zorzet, Balduit, Zito, Mangogna, Macor, Romano, Toffoli, Belmonte, Morello, Martorana, Borelli, Ricci, Kishore and Bulla. The complement system is a major component of humoral innate immunity, acting as a first line of defense against microbes via opsonization and lysis of pathogens. However, novel roles of the complement system in inflammatory and immunological processes, including in cancer, are emerging. Endometriosis (EM), a benign disease characterized by ectopic endometrial implants, shows certain unique features of cancer, such as the capacity to invade surrounding tissues, and in severe cases, metastatic properties. A defective immune surveillance against autologous tissue deposited in the peritoneal cavity allows immune escape for endometriotic lesions. There is evidence that the glandular epithelial cells found in endometriotic implants produce and secrete the complement component C3. Here, we show, using immunofluorescence and RT-qPCR, the presence of locally synthesized C3 in the ectopic endometriotic tissue, but not in the eutopic tissue. We generated a murine model of EM via injection of minced uterine tissue from a donor mouse into the peritoneum of recipient mice. The wild type mice showed greater amount of cyst formation in the peritoneum compared to C3 knock-out mice. Peritoneal washings from the wild type mice with EM showed more degranulated mast cells compared to C3 knock-out mice, consistent with higher C3a levels in the peritoneal fluid of EM patients. We provide evidence that C3a participates in an auto-amplifying loop leading to mast cell infiltration and activation, which is pathogenic in EM. Thus, C3 can be considered a marker of EM and its local synthesis can promote the engraftment of the endometriotic cysts. Ministry of Health: Project code: ENDO-2020-23670288 “Pathogenesis of endometriosis: the role of genes, inflammation and environment”; Institute for Maternal and Child Health, IRCCS Burlo Garofolo, Trieste, Italy (RC20/16, RC23/18; 5MILLE15D; PORFESR 2014/2020 FVG (“TiCheP” project).

Published
2021

134. C1q as a unique player in angiogenesis with therapeutic implication in wound healing.

Author

Bossi, Fleur, Tripodo, Claudio, Rizzi, Lucia, Bulla, Roberta, Agostinis, Chiara, Guarnotta, Carla, Munaut, Carine, Baldassarre, Gustavo, Papa, Giovanni, Zorzet, Sonia, Ghebrehiwet, Berhane, Guang Sheng Ling, Botto, Marina, and Tedesco, Francesco

Subjects
*NEOVASCULARIZATION, *WOUND healing, *ENDOTHELIAL cells, *MESSENGER RNA, *IN situ hybridization
Abstract

We have previously shown that C1q is expressed on endothelial cells (ECs) of newly formed decidual tissue. Here we demonstrate that C1q is deposited in wound-healing skin in the absence of C4 and C3 and that C1q mRNA is locally expressed as revealed by real-time PCR and in situ hybridization. C1q was found to induce permeability of the EC monolayer, to stimulate EC proliferation and migration, and to promote tube formation and sprouting of new vessels in a rat aortic ring assay. Using a murine model of wound healing we observed that vessel formation was defective in C1qa-/- mice and was restored to normal after local application of C1q. The mean vessel density of wound-healing tissue and the healed wound area were significantly increased in C1q-treated rats. On the basis of these results we suggest that C1q may represent a valuable therapeutic agent that can be used to treat chronic ulcers or other pathological conditions in which angiogenesis is impaired, such as myocardial ischemia. [ABSTRACT FROM AUTHOR]

Published
2014
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135. Profiling the molecular mechanism of fullerene cytotoxicity on tumor cells by RNA-seq.

Author

Lucafò, Marianna, Gerdol, Marco, Pallavicini, Alberto, Pacor, Sabrina, Zorzet, Sonia, Da Ros, Tatiana, Prato, Maurizio, and Sava, Gianni

Subjects
*FULLERENES, *CELL-mediated cytotoxicity, *NUCLEOTIDE sequence, *GENE expression, *GENETIC transcription, *PROTEIN synthesis
Abstract

Abstract: The interest on functionalized fullerenes in the field of nanomedicine has seen a significant increase in the past decade. However, the different methods employed to increase C60 solubility profoundly influence the physicochemical properties and the toxicological effects of these compounds, thus complicating the evaluation of their toxicity and potential therapeutic use. Here we report a whole-transcriptome RNA-seq analysis assessing the effect of two fullerenes (1 and 2) on gene expression in the human MCF7 cell line. Although these two compounds had previously been characterized by in vitro studies as having a cytotoxic and null effect respectively, to date the mechanisms at the basis of this different behavior and, more in general, at the basis of the effect of most fullerene derivatives in living cells are still completely unknown. Our data evidence that: (a) fullerene 2 caused a significant, time-dependent alteration of gene expression, whereas 1 only had a negligible effect; (b) the biological processes mostly influenced over the 48h experimental time course were transcription, protein synthesis, cell cycle progression and cell adhesion; (c) the gene expression signature of 2-treated cells was strikingly similar to those induced by selective inhibitors of mTOR signaling, thus suggesting an effect on this pathway for fullerene 2. Our work represents the first approach toward the application of RNA-seq to the study of the molecular mechanisms underlying the interaction of fullerenes with cellular systems and provides an objective view of the feasibility and the safety of these nanomaterials for a medical application. [Copyright &y& Elsevier]

Published
2013
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136. Features and full reversibility of the renal toxicity of the ruthenium-based drug NAMI-A in mice

Author

Vadori, Marta, Pacor, Sabrina, Vita, Francesca, Zorzet, Sonia, Cocchietto, Moreno, and Sava, Gianni

Subjects
*NEPHROTOXICOLOGY, *RUTHENIUM compounds, *LABORATORY mice, *IMIDAZOLES, *ANTIBODY-dependent cell cytotoxicity, *KIDNEY tubules, *DRUG administration
Abstract

Abstract: The ruthenium-based compound imidazolium trans-imidazoledimethylsulfoxide-tetrachlororuthenate (NAMI-A) is free of cytotoxicity up to 1mM concentration after 1h in vitro exposure of the LLC-PK1 renal tubule cells. In vivo, one cycle of i.p. administrations of 35mg/kg/day NAMI-A (1cycle=6 consecutive days), is free of a measurable toxicity on mouse kidneys. After two cycles with a one-week drug-free washout between cycles, mitochondrial membrane potential of the renal cells drops by 37% (p <0.05), serum creatinine increases by 30% (p <0.05) and a significant decrease of body weight of 12% (p <0.05) occurs. These parameters return to normal within 7days after the end of treatment. A cycle-dependent alteration of glomeruli and a diffused swelling of renal tubules are also evident leading to a significant alteration of these structures after the third cycle. These effects are completely prevented if a 2-week drug free washout is used between two consecutive cycles. These data support the toxic accumulation of NAMI-A or of its products of transformation in the kidneys and stress the need of at least 14days washout between two treatment cycles when the drug is given daily for 6 consecutive days. [Copyright &y& Elsevier]

Published
2013
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137. Study of a potential drug delivery system based on carbon nanoparticles: effects of fullerene derivatives in MCF7 mammary carcinoma cells.

Author

Lucafò, Marianna, Pacor, Sabrina, Fabbro, Chiara, Ros, Tatiana, Zorzet, Sonia, Prato, Maurizio, and Sava, Gianni

Subjects
*FULLERENES, *DRUG delivery systems, *DRUG synergism, *CANCER cells, *SURFACE area, *CELL-mediated cytotoxicity, *ANTINEOPLASTIC agents
Abstract

Fullerenes (C) represent important carbon nanoparticles, widely investigated for diagnostic and therapeutic uses, mainly because they are characterized by a small size (between 7 and 10 Å) and a large surface area. The cytotoxicity of two fullerene derivatives, functionalized by 1,3-dipolar cycloaddition of azomethine ylides to the C cage ( 1 and 2), the mechanism of cellular uptake (studied with a fluorescein-bearing derivative of 1, hereafter called derivative 3), and the intracellular distribution are the subject of this work. Cell cytotoxicity on human mammary carcinoma cell line (MCF7), evaluated with the MTT test and further confirmed by a flow cytometry approach with DiOC and PI probes, showed that derivative 1 was free of necrotic or apoptotic effects even after a long lasting cell exposure. Cell uptake and internalization of derivative 3 reach their zenith within 12 h after treatment, with a tendency to persist up to 72 h; this process was evaluated by flow cytometry and confirmed by confocal microscopy. Thus, it appears that a compound such as derivative 1 may be unspecifically taken up by MCF7 cells, in which it distributes throughout the cytoplasm, apparently avoiding any co-localization within the nucleus and secretory granules. These results suggest a strong interaction between the tested fullerene and mammalian cells and a significant ability of this compound to enter tumor cells, therefore resulting to be a suitable vector to deliver anticancer agents to tumor cells. [ABSTRACT FROM AUTHOR]

Published
2012
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138. Photodynamic Therapy for ras-Driven Cancers: Targeting G-Quadruplex RNA Structures with Bifunctional Alkyl-Modified Porphyrins

Author

Giulia Nicoletto, Alexander S. Tikhomirov, Sonia Zorzet, Annalisa Ferino, Francesca D'Este, Luigi E. Xodo, Andrey E. Shchekotikhin, Sara Lago, Sara N. Richter, Ferino, Annalisa, Nicoletto, Giulia, D'Este, Francesca, Zorzet, Sonia, Lago, Sara, Richter, Sara N, Tikhomirov, Alexander, Shchekotikhin, Andrey, and Xodo, Luigi E

Subjects
Neuroblastoma RAS viral oncogene homolog, medicine.medical_treatment, Caspase 3, Photodynamic therapy, G-quadruplex, porphyrins, 01 natural sciences, Caspase 7, 03 medical and health sciences, chemistry.chemical_compound, Drug Discovery, medicine, Propidium iodide, K-ras, Alkyl, ras, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, K-ras, Cancers, ras, G-quadruplex, porphyrins,photodynamic therapy, Photodynamic Therapy, Cell sorting, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, chemistry, Biochemistry, photodynamic therapy, Molecular Medicine, Cancers
Abstract

Designing small molecules able to break down G4 structures in mRNA (RG4s) offers an interesting approach to cancer therapy. Here, we have studied cationic porphyrins (CPs) bearing an alkyl chain up to 12 carbons, as they bind to RG4s while generating reactive oxygen species upon photoirradiation. Fluorescence-activated cell sorting (FACS) and confocal microscopy showed that the designed alkyl CPs strongly penetrate cell membranes, binding to KRAS and NRAS mRNAs under low-abundance cell conditions. In Panc-1 cells, alkyl CPs at nanomolar concentrations promote a dramatic downregulation of KRAS and NRAS expression, but only if photoactivated. Alkyl CPs also reduce the metabolic activity of pancreatic cancer cells and the growth of a Panc-1 xenograft in SCID mice. Propidium iodide/annexin assays and caspase 3, caspase 7, and PARP-1 analyses show that these compounds activate apoptosis. All these data demonstrate that the designed alkyl CPs are efficient photosensitizers for the photodynamic therapy of ras-driven cancers.

Published
2020

139. HSA-Binding Prodrugs-Based Nanoparticles Endowed with Chemo and Photo-Toxicity against Breast Cancer.

Author

Rapozzi, Valentina, Moret, Francesca, Menilli, Luca, Guerrini, Andrea, Tedesco, Daniele, Naldi, Marina, Bartolini, Manuela, Gani, Mariachiara, Zorzet, Sonia, Columbaro, Marta, Milani, Celeste, Martini, Cecilia, Ferroni, Claudia, and Varchi, Greta

Subjects
*GLUTATHIONE, *PRODRUGS, *CANCER chemotherapy, *PHOTOTHERAPY, *PHOTOSENSITIZERS, *TREATMENT effectiveness, *COMBINED modality therapy, *REACTIVE oxygen species, *CELL lines, *NANOPARTICLES, *BREAST tumors
Abstract

Simple Summary: In this study, we developed novel bioresponsive HSA-binding nanoparticles co-delivering paclitaxel (PTX) prodrugs and the photosensitizer pheophorbide a (Pba) for the combined photo- and chemo-treatment of breast cancer. Extensive structural characterization allowed us to evaluate the size, stability and morphology of nanoparticles, which exhibited sustained and controlled drug release under the distinctive redox conditions of the tumor environment. HSA-binding PTX/Pba nanoparticles showed higher Pba uptake in human breast cancer cells and a synergistic antitumor effect upon light irradiation. Preliminary in vivo experiments using low drug doses showed the potential of our bioresponsive nanoparticles to reduce the primary tumor mass while diminishing the number of lung metastases, thus suggesting the effectiveness of this novel approach. Exploiting the tumor environment features (EPR effect, elevated glutathione, reactive oxygen species levels) might allow attaining a selective and responsive carrier capable of improving the therapeutic outcome. To this purpose, the in situ covalent binding of drugs and nanoparticles to circulating human serum albumin (HSA) might represent a pioneering approach to achieve an effective strategy. This study describes the synthesis, in vitro and in vivo evaluation of bioresponsive HSA-binding nanoparticles (MAL-PTX2S@Pba), co-delivering two different paclitaxel (PTX) prodrugs and the photosensitizer pheophorbide a (Pba), for the combined photo- and chemo-treatment of breast cancer. Stable and reproducible MAL-PTX2S@Pba nanoparticles with an average diameter of 82 nm and a PTX/Pba molar ratio of 2.5 were obtained by nanoprecipitation. The in vitro 2D combination experiments revealed that MAL-PTX2S@Pba treatment induces a strong inhibition of cell viability of MDA-MB-231, MCF7 and 4T1 cell lines, whereas 3D experiments displayed different trends: while MAL-PTX2S@Pba effectiveness was confirmed against MDA-MB-231 spheroids, the 4T1 model exhibited marked resistance. Lastly, despite using a low PTX-PDT regimen (e.g., 8.16 mg/Kg PTX and 2.34 mg/Kg Pba), our formulation showed to foster primary tumor reduction and curb lung metastases growth in 4T1 tumor-bearing mice, thus setting the basis for further preclinical validations. [ABSTRACT FROM AUTHOR]

Published
2022
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141. A new approach for the treatment of CLL using chlorambucil/hydroxychloroquine-loaded anti-CD20 nanoparticles

Author

Claudio Tripodo, Marilena Granzotto, Sara Capolla, Gabriele Pozzato, Ruben Spretz, Michele Dal Bo, Luis Nunez, Sonia Zorzet, Paolo Macor, Gustavo Larsen, Sandra Noriega, Nelly Mezzaroba, Eduardo Mansilla, Francesca Vita, Ramiro Mendoza-Maldonado, Valter Gattei, Capolla, S., Mezzaroba, N., Zorzet, S., Tripodo, C., Mendoza-Maldonado, R., Granzotto, M., Vita, F., Spretz, R., Larsen, G., Noriega, S., Mansilla, E., Dal Bo, M., Gattei, V., Pozzato, G., Núñez, L., Macor, P., Capolla, Sara, Mezzaroba, Nelly, Zorzet, Sonia, Tripodo, Claudio, Mendoza Maldonado, Ramiro, Granzotto, Marilena, Vita, Francesca, Spretz, Ruben, Larsen, Gustavo, Noriega, Sandra, Mansilla, Eduardo, Dal Bo, Michele, Gattei, Valter, Pozzato, Gabriele, Núñez, Lui, and Macor, Paolo

Subjects
0301 basic medicine, Chronic lymphocytic leukemia, xenograft model, chronic lymphocytic leukemia, immune targeted nanoparticles, treatment, Electrical and Electronic Engineering, Materials Science (all), Nanotechnology, 03 medical and health sciences, Therapeutic approach, 0302 clinical medicine, hemic and lymphatic diseases, medicine, General Materials Science, Cytotoxicity, CD20, immune targeted nanoparticle, Chlorambucil, biology, business.industry, Therapeutic effect, Hydroxychloroquine, Condensed Matter Physics, medicine.disease, Atomic and Molecular Physics, and Optics, Leukemia, 030104 developmental biology, 030220 oncology & carcinogenesis, Cancer research, biology.protein, business, medicine.drug
Abstract

Current approaches for the treatment of chronic lymphocytic leukemia (CLL) have greatly improved the prognosis for survival, but some patients remain refractive to these therapeutic regimens. Hence, in addition to reducing the long-term sideeffects of therapeutics for all leukemia patients, there is an urgent need for novel therapeutic strategies for difficult-to-treat leukemia cases. Due to the cytotoxicity of drugs, the major challenge currently is to deliver the therapeutic agents to neoplastic cells while preserving the viability of non-malignant cells. In this study, we propose a therapeutic approach in which high doses of hydroxychloroquine and chlorambucil were loaded into biodegradable polymeric nanoparticles coated with an anti-CD20 antibody.We first demonstrated the ability of the nanoparticles to target and internalize in tumor B-cells. Moreover, these nanoparticles could kill not only p53-mutated/deleted leukemia cells expressing a low amount of CD20, but also circulating primary cells isolated from chronic lymphocytic leukemia patients. The safety of these nanoparticles was also demonstrated in healthy mice, and their therapeutic effects were shown in a new model of aggressive leukemia. These results showed that anti-CD20 nanoparticles containing hydroxychloroquine and chlorambucil can be effective in controlling aggressive leukemia and provided a rationale for adopting this approach for the treatment of other B-cell disorders. [Figure not available: see fulltext.]

Published
2015
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142. Potent Apoptotic Response Induced by Chloroacetamidine Anthrathiophenediones in Bladder Cancer Cells

Author

Susanna Cogoi, Sonia Zorzet, Andrey E. Shchekotikhin, Luigi E. Xodo, Cogoi, S., Zorzet, Sonia, Shchekotikhin, A. E., and Xodo, L. E.

Subjects
experimental model, Antineoplastic Agents, Apoptosis, Chloroacetamidine-Anthrathiophenedione, Thiophenes, urologic and male genital diseases, Acetamides, Alleles, Animals, Biological Transport, Cell Line, Tumor, Cell Proliferation, Cyclin D1, Drug Design, G-Quadruplexes, G2 Phase Cell Cycle Checkpoints, Genes, ras, Humans, Mice, Substrate Specificity, Survival Analysis, Urinary Bladder Neoplasms, Xenograft Model Antitumor Assays, Molecular Medicine, Drug Discovery3003 Pharmaceutical Science, Medicine (all), Cell Line, chemistry.chemical_compound, Annexin, Chloroacetamidine-Anthrathiophenediones, Bladder cancer, Drug Discovery, Propidium iodide, HRAS, ras, Caspase, Tumor, biology, Cell cycle, Genes, chemistry, Biochemistry, Cell culture, Cancer cell, biology.protein, Cancer research
Abstract

We previously found that two neighboring G-quadruplexes behave as a molecular switch controlling the expression of HRAS (Cogoi, S.; Schekotikhin, A. E.; Xodo, L. E. Nucl. Acids Res. 2014, DOI: 10.1093/nar/gku574). In this study we have designed anthrathiophenediones with two chloroacetamidine-containing side chains (CATDs) as G-quadruplex binders and have examined their anticancer activity in T24 bladder cancer cells bearing mutant HRAS and in T24 xenografts. The designed CATDs (3a-e), bearing alkyl side chains of different length, penetrate T24 cancer cells more than their analogues with guanidine-containing side chains. The lead compounds 3a and 3c inhibit HRAS expression, metabolic activity, and colony formation in T24 cancer cells. They also activate a strong apoptotic response, as indicated by PARP-1, caspases 3/7, and annexin V/propidium iodide assays. Apoptosis occurs under conditions where cyclin D1 is down-regulated and the cell cycle arrested in G2 phase. Finally, compound 3a inhibits the growth of T24 xenografts and increases the median survival time of nude mice.

Published
2015
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143. The Combination of N-Acetyl Cysteine, Alpha-Lipoic Acid, and Bromelain Shows High Anti-Inflammatory Properties in NovelIn VivoandIn VitroModels of Endometriosis

Author

Roberta Bulla, Chiara Agostinis, Giorgio Zauli, Sonia Zorzet, R. De Leo, F. De Seta, Agostinis, C., Zorzet, Sonia, De Leo, R., Zauli, G., DE SETA, Francesco, and Bulla, Roberta

Subjects
Pathology, Anti-Inflammatory Agents, Apoptosis, Mice, SCID, Pharmacology, Acetylcysteine, Mice, and bromelain, Endometriosi, Cells, Cultured, Caspase, Microscopy, Cultured, Thioctic Acid, biology, Bromelains, endothelial cells, N-acetyl cystein, endothelial cell, Female, Tumor necrosis factor alpha, Research Article, lcsh:RB1-214, medicine.drug, medicine.medical_specialty, Article Subject, medicine.drug_class, Cells, Immunology, Endometriosis, Vascular Cell Adhesion Molecule-1, SCID, Fluorescence, Anti-inflammatory, NO, Proinflammatory cytokine, In vivo, lcsh:Pathology, medicine, Animals, Humans, Animal, Tumor Necrosis Factor-alpha, Cell Biology, inflammation, alpha-lipoic acid, and bromelain, business.industry, alpha-lipoic acid, Uterus, Disease Models, Animal, Endothelial Cells, Inflammation, Microscopy, Fluorescence, In vitro, Disease Models, biology.protein, business
Abstract

To evaluate the efficacy of an association of N-acetyl cystein, alpha-lipoic acid, and bromelain (NAC/LA/Br) in the treatment of endometriosis we set up a newin vivomurine model. We explored the anti-inflammatory and proapoptotic effect of this combination on human endometriotic endothelial cells (EECs) and on endothelial cells isolated from normal uterus (UtMECs). We implanted fragments of human endometriotic cysts intraperitoneally into SCID mice to evaluate the efficacy of NAC/LA/Br treatment. UtMECs and EECs, untreated or treated with NAC/LA/Br, were activated with the proinflammatory stimulus TNF-αand their response in terms of VCAM1 expression was evaluated. The proapoptotic effect of higher doses of NAC/LA/Br on UtMECs and EECs was measured with a fluorogenic substrate for activated caspases 3 and 7. The preincubation of EECs with NAC/LA/Br prior to cell stimulation with TNF-αprevents the upregulation of the expression of the inflammatory “marker” VCAM1. Furthermore NAC/LA/Br were able to induce EEC, but not UtMEC, apoptosis. Finally, the novel mouse model allowed us to demonstrate that mice treated with NAC/LA/Br presented a lower number of cysts, smaller in size, compared to untreated mice. Our findings suggest that these dietary supplements may have potential therapeutic uses in the treatment of chronic inflammatory diseases like endometriosis.

Published
2015
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144. Pharmacological Activities of Ruthenium Complexes Related to Their NO Scavenging Properties

Author

Anna Castellarin, Sonia Zorzet, Alberta Bergamo, Gianni Sava, Castellarin, Anna, Zorzet, Sonia, Bergamo, Alberta, and Sava, Gianni

Subjects
0301 basic medicine, Male, Angiogenesis, Angiogenesis Inhibitors, Pharmacology, Catalysi, lcsh:Chemistry, Anticancer, Cell cultures, Nitric oxide, Ruthenium, Catalysis, Molecular Biology, Spectroscopy, Computer Science Applications1707 Computer Vision and Pattern Recognition, Physical and Theoretical Chemistry, Organic Chemistry, Inorganic Chemistry, chemistry.chemical_compound, Mice, angiogenesis, 0302 clinical medicine, Laminin, Coordination Complexes, lcsh:QH301-705.5, biology, General Medicine, Free Radical Scavengers, Computer Science Applications, Angiogenesi, Drug Combinations, Biochemistry, 030220 oncology & carcinogenesis, Proteoglycans, Collagen, Cell Survival, Sodium, chemistry.chemical_element, Nitric Oxide, anticancer, Article, Cell Line, 03 medical and health sciences, Inhibitory Concentration 50, Animals, Humans, Matrigel, cell cultures, In vitro, 030104 developmental biology, chemistry, lcsh:Biology (General), lcsh:QD1-999, Cell culture, biology.protein, Macrophages, Peritoneal, ruthenium, nitric oxide
Abstract

Angiogenesis is considered responsible for the growth of primary tumours and of their metastases. With the present study, the effects of three ruthenium compounds, potassiumchlorido (ethylendiamminotetraacetate)rutenate(III) (RuEDTA), sodium (bis-indazole)tetrachloro-ruthenate(III), Na[trans-RuCl4Ind2] (KP1339) and trans-imidazoledimethylsulphoxidetetrachloro-ruthenate (NAMI-A), are studied in vitro in models mimicking the angiogenic process. The ruthenium compounds reduced the production and the release of nitrosyls from either healthy macrophages and immortalized EA.hy926 endothelial cells. The effects of NAMI-A are qualitatively similar and sometimes quantitatively superior to those of RuEDTA and KP1339. NAMI-A reduces the production and release of nitric oxide (NO) by the EA.hy926 endothelial cells and correspondingly inhibits their invasive ability; it also strongly inhibits the angiogenesis in matrigel sponges implanted subcutaneously in healthy mice. Taken together, these data support the anti-angiogenic activity of the tested ruthenium compounds and they contribute to explain the selective activity of NAMI-A against solid tumour metastases, the tumour compartment on which angiogenesis is strongly involved. This anti-angiogenic effect may also contribute to the inhibition of the release of metastatic cells from the primary tumour. Investigations on the anti-angiogenic effects of NAMI-A at this level will increase knowledge of its pharmacological properties and it will give a further impulse to the development of this class of innovative metal-based drugs.

Published
2016

145. C1q acts in the tumour microenvironment as a cancer-promoting factor independently of complement activation

Author

Damiano Rami, Roberta Bulla, Claudio Tripodo, Marina Botto, Carla Guarnotta, Guang Sheng Ling, Paolo Durigutto, Sonia Zorzet, Chiara Agostinis, Francesco Tedesco, Bulla, Roberta, Tripodo, Claudio, Rami, Damiano, Ling, Guang Sheng, Agostinis, Chiara, Guarnotta, Carla, Zorzet, Sonia, Durigutto, Paolo, Botto, Marina, Tedesco, Francesco, Bulla, R., Tripodo, C., Rami, D., Ling, G., Agostinis, C., Guarnotta, C., Zorzet, S., Durigutto, P., Botto, M., Tedesco, F., and Wellcome Trust

Subjects
Genetics and Molecular Biology (all), 0301 basic medicine, PROTEIN, General Physics and Astronomy, MELANOMA, Apoptosis, Inbred C57BL, Biochemistry, DISEASE, Animals, Cell Line, Tumor, Cell Movement, Cell Proliferation, Complement Activation, Complement C1q, Complement C3, Complement C5, Humans, Mice, Mice, Inbred C57BL, Mice, Knockout, Neoplasms, Biochemistry, Genetics and Molecular Biology (all), Chemistry (all), Physics and Astronomy (all), fluids and secretions, immune system diseases, IMMUNE-RESPONSE, skin and connective tissue diseases, Complement component 5, Tumor, Multidisciplinary, 3. Good health, Cell biology, Multidisciplinary Sciences, DEFICIENCY, medicine.anatomical_structure, Science & Technology - Other Topics, Human, Knockout, Science, chemical and pharmacologic phenomena, Biology, Article, General Biochemistry, Genetics and Molecular Biology, TROPHOBLAST INVASION, MECHANISMS, Cell Line, 03 medical and health sciences, Classical complement pathway, Immune system, INFLAMMATION, medicine, Science & Technology, Animal, Cell growth, EFFECTOR SYSTEM, Apoptosi, General Chemistry, Complement system, 030104 developmental biology, Cancer cell, Neoplasm, Bone marrow, ANTIBODY THERAPY
Abstract

Complement C1q is the activator of the classical pathway. However, it is now recognized that C1q can exert functions unrelated to complement activation. Here we show that C1q, but not C4, is expressed in the stroma and vascular endothelium of several human malignant tumours. Compared with wild-type (WT) or C3- or C5-deficient mice, C1q-deficient (C1qa−/−) mice bearing a syngeneic B16 melanoma exhibit a slower tumour growth and prolonged survival. This effect is not attributable to differences in the tumour-infiltrating immune cells. Tumours developing in WT mice display early deposition of C1q, higher vascular density and an increase in the number of lung metastases compared with C1qa−/− mice. Bone marrow (BM) chimeras between C1qa−/− and WT mice identify non-BM-derived cells as the main local source of C1q that can promote cancer cell adhesion, migration and proliferation. Together these findings support a role for locally synthesized C1q in promoting tumour growth., C1q is known to initiate the activation of the complement classical pathway. Here, the authors show the C1q is expressed in the tumour microenvironment and can promote cancer cell migration and adhesion in a complement activation-independent manner.

Published
2016
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146. A novel retinoic/butyric hyaluronan ester for the treatment of acute promyelocytic leukemia: preliminary preclinical results

Author

Gianni Sava, Sonia Zorzet, C. Pellizzaro, Gabriella Abolafio, Silvia Cantoni, Danila Coradini, C. Garrovo, Alberto Perbellini, Maria Grazia Daidone, Ignazio Scarlata, Maya Fedeli, Annalisa Speranza, Coradini, D., Pellizzaro, C., Scarlata, I., Zorzet, Sonia, Garrovo, C., Abolafio, G., Speranza, A., Fedeli, M., Cantoni, S., Sava, Gianni, Daidone, M. G., and Perbellini, A.

Subjects
Acute promyelocytic leukemia, Cancer Research, Myeloid, Oncogene Proteins, Fusion, medicine.drug_class, Retinoic acid, Apoptosis, Tretinoin, Caspase 3, In Vitro Techniques, Biology, Histones, chemistry.chemical_compound, Leukemia, Promyelocytic, Acute, In vivo, Histone deacetylase inhibitors, Cell Line, Tumor, Ha-But, CCAAT-Enhancer-Binding Protein-alpha, Tumor Cells, Cultured, medicine, Humans, Hyaluronic Acid, Cell Proliferation, Histone deacetylase inhibitor, CCAAT-Enhancer-Binding Protein-beta, Promyelocytic leukemia, Preclinical, Cell Differentiation, Esters, Hematology, medicine.disease, Neoplasm Proteins, medicine.anatomical_structure, Oncology, chemistry, Cell culture, Immunology, Cancer research, Butyric Acid, Drug Screening Assays, Antitumor, Protein Binding
Abstract

All-trans retinoic acid (ATRA) represents the therapy of choice for patients with acute promyelocytic leukemia (APL). However, patients often relapse due to ATRA-resistance. The molecular basis of APL alterations indicates that addition of a histone deacetylase inhibitor to ATRA may restore the sensitivity to retinoids. We explored the in vitro and in vivo effects of a novel retinoic/butyric hyaluronan ester (HBR) on a retinoic acid (RA)-sensitive human myeloid cell line, NB4, and on its RA-resistant subclone, NB4.007/6. In vitro, HBR induced growth arrest and terminal differentiation in RA-sensitive NB4 cells (as confirmed by an increased expression of CD11 family members and nitroblue tetrazolium assay), whereas it inhibited the growth of RA-resistant cells by apoptosis, paralleled by an increase in the levels of caspase 3 and 7. In vivo, HBR treatment of NB4-inoculated severe combined immunodeficient mice resulted in a statistically significant increase in survival time (P

Published
2006
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147. Primary Tumor, Lung and Kidney Retention and Antimetastasis Effect of NAMI-A Following Different Routes of Administration

Author

Alenka Sorc, Sonia Zorzet, Moreno Cocchietto, Gianni Sava, Cocchietto, M., Zorzet, Sonia, Sorc, A., Sava, Gianni, M., Cocchietto, and A., Sorc

Subjects
Pathology, medicine.medical_specialty, Lung Neoplasms, Administration, Oral, Antineoplastic Agents, Mammary Neoplasms, Animal, Mice, Inbred Strains, Pharmacology, Kidney, Ruthenium, Metastasis, Carcinoma, Lewis Lung, Mice, Route of administration, chemistry.chemical_compound, Species Specificity, Pharmacokinetics, Antimetastatic Agent, Administration, Inhalation, Organometallic Compounds, medicine, Animals, NAMI-A, Dimethyl Sulfoxide, Pharmacology (medical), Neoplasm Metastasis, Lung, Aerosols, business.industry, Lewis lung carcinoma, respiratory system, medicine.disease, Primary tumor, Disease Models, Animal, medicine.anatomical_structure, Liver, Oncology, chemistry, Ruthenium Compounds, Female, business, Injections, Intraperitoneal
Abstract

Imidazolium-trans-dimethylsulfoxideimidazoletetrachlororuthenate (NAMI-A) is a ruthenium compound effective on solid tumor metastases. In this study, we evaluated the effects of different routes of administration of NAMI-A on the distribution to primary tumor, lungs and kidneys in BD2F1 hybrids with Lewis lung carcinoma or in CBA inbred mice with MCa mammary carcinoma. NAMI-A concentration and the percentage of cumulative dose (%Dtot) retained in these tissues is independent of the animal strain and of the tumor model used. Also the presence of the tumor does not change the distribution of NAMI-A in the lungs and in the kidneys. A dose-dependent antimetastatic effect is evident with intraperitoneal (i.p.) treatments at three different doses. Treatment of tumor bearing mice with NAMI-A administered i.p., per os or by aerosol showed a similar effect on lung metastases, although the concentration of ruthenium reached in the lungs was markedly different. On the basis of the data obtained, we can conclude that the antimetastatic effects are related to the amount of NAMI-A administered, rather than to the lung's concentration of the compound.

Published
2003
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148. The antimetastatic drug NAMI-A potentiates the phenylephrine-induced contraction of aortic smooth muscle cells and induces a transient increase in systolic blood pressure

Author

Moreno Cocchietto, L. Candussio, Marta Vadori, Gianni Sava, Sabrina Pacor, Sonia Zorzet, C. Florio, B. Groppo, Vadori, M., Florio, Chiara, Groppo, B., Cocchietto, M., Pacor, S., Zorzet, Sonia, Candussio, Luigi, and Sava, Gianni

Subjects
Male, Contraction (grammar), Myocytes, Smooth Muscle, Anticancer drug, Binding affinity, Biomedicine, Heavy metal, Toxicity, Antineoplastic Agents, Blood Pressure, Pharmacology, Biochemistry, Inorganic Chemistry, chemistry.chemical_compound, Phenylephrine, Structure-Activity Relationship, In vivo, medicine, Organometallic Compounds, Myocyte, NAMI-A, Animals, Dimethyl Sulfoxide, Rats, Wistar, Aorta, Kidney, Dose-Response Relationship, Drug, Chemistry, Rats, Dose–response relationship, Blood pressure, medicine.anatomical_structure, Ruthenium Compounds, medicine.drug, Muscle Contraction
Abstract

The ruthenium-based drug imidazolium trans-imidazoledimethylsulphoxidetetrachlorido ruthenate (NAMI-A) is a novel antitumour drug under clinical evaluation. In this study, NAMI-A is tested on aortic rings in vitro and on the systolic blood pressure in vivo with the aim of evaluating its effects on smooth muscle cells and, more in general, on the vascular system. Pre-incubation of aortic rings with 10 µM NAMI-A for 10 min potentiates the contraction induced by phenylephrine (PE). The reduction of the B max value of [(3)H]-prazosin bound to NAMI-A-treated aortic rings and the ability of NAMI-A to displace [(3)H]-prazosin and [(3)H]-IP3 binding by 25 and 42%, respectively, suggest the involvement of α1-adrenoceptor in mediating the effects on smooth muscle cells. NAMI-A also decreases the number of maximal sites of [(3)H]-prazosin bound to kidney membrane preparation from 34 to 24 fmol/mg proteins. A single i.p. dose (105 mg/kg) or a repeated treatment for 6 consecutive days (17 mg/kg/day) in Wistar rats increases the systolic blood pressure, respectively, 1 h and 3 days after treatment, and the responsiveness of rat aortic rings to PE. Atomic absorption spectroscopy confirms the presence of ruthenium in the aortic rings excised from the treated rats. These findings suggest monitoring the cardiovascular parameters when the drug is used in humans for treating cancer patients, particularly if the drug is associated with chemicals that are potentially active at the cardiovascular level.

Published
2015

149. Targeted tumor imaging of anti-CD20-polymeric nanoparticles developed for the diagnosis of B-cell malignancies

Author

Stefania Biffi, Sara Capolla, Enrico Rampazzo, Paolo Macor, Chiara Garrovo, Sonia Zorzet, Andrea Lorenzon, Gabriele Pozzato, Luis Nunez, Claudio Tripodo, Ruben Spretz, Capolla, Sara, Garrovo, Chiara, Zorzet, Sonia, Lorenzon, Andrea, Rampazzo, Enrico, Spretz, Ruben, Pozzato, Gabriele, Núñez, Lui, Tripodo, Claudio, Macor, Paolo, Biffi, Stefania, Capolla, S., Garrovo, C., Zorzet, S., Lorenzon, A., Rampazzo, E., Spretz, R., Pozzato, G., Núñez, L., Tripodo, C., Macor, P., and Biffi, S.

Subjects
Medicine (General), Active targeting, Optical imaging, Tumor accumulation, Animals, Antigens, CD20, Cell Line, Tumor, Humans, Leukemia, B-Cell, Mice, Molecular Imaging, Nanoparticles, Polymers, Drug Delivery Systems, Bioengineering, Biophysics, Biomaterials, Drug Discovery3003 Pharmaceutical Science, Organic Chemistry, Pharmaceutical Science, Pharmacology, Nanoparticle, International Journal of Nanomedicine, Drug Discovery, Polymer, Original Research, Tumor, Leukemia, tumor accumulation, General Medicine, Drug delivery, Systemic administration, Preclinical imaging, Human, active targeting, Materials science, Cell Line, optical imaging, R5-920, In vivo, medicine, Distribution (pharmacology), CD20, Antigens, Animal, B-Cell, Cancer, medicine.disease, Biomaterial, Targeted drug delivery, Biophysic, Molecular imaging, Drug Delivery System
Abstract

Sara Capolla,1 Chiara Garrovo,2 Sonia Zorzet,1 Andrea Lorenzon,3 Enrico Rampazzo,4 Ruben Spretz,5 Gabriele Pozzato,6 Luis Núñez,7 Claudio Tripodo,8 Paolo Macor,1,9 Stefania Biffi2 1Department of Life Sciences, University of Trieste, 2Institute for Maternal and Child Health – IRCCS “Burlo Garofolo”, Trieste, 3Animal Care Unit, Cluster in Biomedicine (CBM scrl), Trieste, Italy; 4Department of Chemistry “G. Ciamician”, University of Bologna, Bologna, Italy; 5LNK Chemsolutions LLC, Lincoln, NE, USA; 6Department of Medical, Surgery and Health Sciences, University of Trieste, Trieste, Italy; 7Bio-Target, Inc., University of Chicago, Chicago, IL, USA; 8Department of Human Pathology, University of Palermo, Palermo, Italy; 9Callerio Foundation Onlus, Institutes of Biological Researches, Trieste, Italy Abstract: The expectations of nanoparticle (NP)-based targeted drug delivery systems in cancer, when compared with convectional therapeutic methods, are greater efficacy and reduced drug side effects due to specific cellular-level interactions. However, there are conflicting literature reports on enhanced tumor accumulation of targeted NPs, which is essential for translating their applications as improved drug-delivery systems and contrast agents in cancer imaging. In this study, we characterized biodegradable NPs conjugated with an anti-CD20 antibody for in vivo imaging and drug delivery onto tumor cells. NPs’ binding specificity mediated by anti-CD20 antibody was evaluated on MEC1 cells and chronic lymphocytic leukemia patients’ cells. The whole-body distribution of untargeted NPs and anti-CD20 NPs were compared by time-domain optical imaging in a localized human/mouse model of B-cell malignancy. These studies provided evidence that NPs’ functionalization by an anti-CD20 antibody improves tumor pharmacokinetic profiles in vivo after systemic administration and increases in vivo imaging of tumor mass compared to non-targeted NPs. Together, drug delivery and imaging probe represents a promising theranostics tool for targeting B-cell malignancies. Keywords: active targeting, optical imaging, tumor accumulation

Published
2015

150. Effects of Two Fullerene Derivatives on Monocytes and Macrophages

Author

Marianna Lucafò, Alberto Grillo, Maurizio Prato, Sonia Zorzet, Luka Đorđević, Tatiana Da Ros, Gianni Sava, Sabrina Pacor, Pacor, Sabrina, Grillo, Alberto, Đorđević, Luka, Zorzet, Sonia, Lucafo, Marianna, DA ROS, Tatiana, Prato, Maurizio, and Sava, Gianni

Subjects
Fullerene, Article Subject, Nitrogen, lcsh:Medicine, Antineoplastic Agents, Apoptosis, Monocytes, General Biochemistry, Genetics and Molecular Biology, Flow cytometry, Immune system, Cell Line, Tumor, Neoplasms, medicine, Humans, Cytotoxicity, General Immunology and Microbiology, medicine.diagnostic_test, Chemistry, fullerene, flow cytometry, Macrophages, Purinergic receptor, lcsh:R, fullerene, macrophages, cytotoxicity, flow cytometry, drug-delivery, General Medicine, In vitro, drug-delivery, Biochemistry, Drug delivery, cytotoxicity, Neoplastic cell, Fullerenes, Receptors, Purinergic P2X7, Hydrophobic and Hydrophilic Interactions, Research Article
Abstract

Two fullerene derivatives (fullerenes1and2), bearing a hydrophilic chain on the pyrrolidinic nitrogen, were developed with the aim to deliver anticancer agents to solid tumors. These two compounds showed a significantly different behaviour on human neoplastic cell linesin vitroin respect to healthy leukocytes. In particular, the pyrrolidinium ring on the fullerene carbon cage brings to a more active compound. In the present work, we describe the effects of these fullerenes on primary cultures of human monocytes and macrophages, two kinds of immune cells representing the first line of defence in the immune response to foreign materials. These compounds are not recognized by circulating monocytes while they get into macrophages. The evaluation of the pronecrotic or proapoptotic effects, analysed by means of analysis of the purinergic receptor P2X7 activation and of ROS scavenging activity, has allowed us to show that fullerene2, but not its analogue fullerene1, displays toxicity, even though at concentrations higher than those shown to be active on neoplastic cells.

Published
2015

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