Your search keyword '"Laura Bonmassar"' showing total 22 results

1. Circulating interleukin-8 and osteopontin are promising biomarkers of clinical outcomes in advanced melanoma patients treated with targeted therapy

Author

Lauretta Levati, Claudio Tabolacci, Antonio Facchiano, Francesco Facchiano, Ester Alvino, Gian Carlo Antonini Cappellini, Enrico Scala, Laura Bonmassar, Simona Caporali, Pedro Miguel Lacal, Antonella Bresin, Federica De Galitiis, Giandomenico Russo, and Stefania D’Atri

Subjects

Melanoma, Targeted therapy, Cytokines, IL-8, Osteopontin, BDNF, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Circulating cytokines can represent non-invasive biomarkers to improve prediction of clinical outcomes of cancer patients. Here, plasma levels of IL-8, CCL4, osteopontin, LIF and BDNF were determined at baseline (T0), after 2 months of therapy (T2) and, when feasible, at progression (TP), in 70 melanoma patients treated with BRAF and MEK inhibitors. The association of baseline cytokine levels with clinical response, progression-free survival (PFS) and overall survival (OS) was evaluated. Methods Cytokine concentrations were measured using the xMAP technology. Their ability to discriminate between responding (Rs) and non-responding (NRs) patients was assessed by Receiver Operating Characteristics analysis. PFS and OS were estimated with the Kaplan–Meier method. The Cox proportional hazard model was used in the univariate and multivariate analyses to estimate crude and adjusted hazard ratios with 95% confidence intervals. Results CCL4 and LIF were undetectable in the majority of samples. The median osteopontin concentration at T0 and T2 was significantly higher in NRs than in Rs. The median T0 and T2 values of IL-8 were also higher in NRs than in Rs, although the statistical significance was not reached. No differences were detected for BDNF. In 39 Rs with matched T0, T2, and TP samples, osteopontin and IL-8 significantly decreased from T0 to T2 and rose again at TP, while BDNF levels remained unchanged. In NRs, none of the cytokines showed a significant decrease at T2. Only osteopontin demonstrated a good ability to discriminate between Rs and NRs. A high IL-8 T0 level was associated with significantly shorter PFS and OS and higher risk of progression and mortality, and remained an independent negative prognostic factor for OS in multivariate analysis. An elevated osteopontin T0 concentration was also significantly associated with worse OS and increased risk of death. Patients with high IL-8 and high osteopontin showed the lowest PFS and OS, and in multivariate analysis this cytokine combination remained independently associated with a three- to six-fold increased risk of mortality. Conclusion Circulating IL-8 and osteopontin appear useful biomarkers to refine prognosis evaluation of patients undergoing targeted therapy, and deserve attention as potential targets to improve its clinical efficacy.

Published

2024

2. Targeting of PDGF-C/NRP-1 autocrine loop as a new strategy for counteracting the invasiveness of melanoma resistant to braf inhibitors

Author

Federica Ruffini, Claudia Ceci, Maria Grazia Atzori, Simona Caporali, Lauretta Levati, Laura Bonmassar, Gian Carlo Antonini Cappellini, Stefania D’Atri, Grazia Graziani, and Pedro Miguel Lacal

Subjects

Melanoma, BRAF inhibitors, Neuropilin-1, PDGF-C, Dabrafenib, Extracellular matrix invasion, Therapeutics. Pharmacology, RM1-950

Abstract

Melanoma resistance to BRAF inhibitors (BRAFi) is often accompanied by a switch from a proliferative to an invasive phenotype. Therefore, the identification of signaling molecules involved in the development of metastatic properties by resistant melanoma cells is of primary importance. We have previously demonstrated that activation of neuropilin-1 (NRP-1) by platelet-derived growth factor (PDGF)-C confers melanoma cells with an invasive behavior similar to that of BRAFi resistant tumors. Aims of the present study were to evaluate the role of PDGF-C/NRP-1 autocrine loop in the acquisition of an invasive and BRAFi-resistant phenotype by melanoma cells and the effect of its inhibition on drug resistance and extracellular matrix (ECM) invasion. Furthermore, we investigated whether PDGF-C serum levels were differentially modulated by drug treatment in metastatic melanoma patients responsive or refractory to BRAFi as single agents or in combination with MEK inhibitors (MEKi). The results indicated that human melanoma cells resistant to BRAFi express higher levels of PDGF-C and NRP-1 as compared to their susceptible counterparts. Overexpression occurs early during development of drug resistance and contributes to the invasive properties of resistant cells. Accordingly, silencing of NRP-1 or PDGF-C reduces tumor cell invasiveness. Analysis of PDGF-C in the serum collected from patients treated with BRAFi or BRAFi+MEKi, showed that in responders PDGF-C levels decrease after treatment and raise again at tumor progression. Conversely, in non-responders treatment does not affect PDGF-C serum levels. Thus, blockade of NRP-1 activation by PDGF-C might represent a new therapeutic approach to counteract the invasiveness of BRAFi-resistant melanoma.

Published

2023

3. miR-126-3p down-regulation contributes to dabrafenib acquired resistance in melanoma by up-regulating ADAM9 and VEGF-A

Author

Simona Caporali, Adriana Amaro, Lauretta Levati, Ester Alvino, Pedro Miguel Lacal, Simona Mastroeni, Federica Ruffini, Laura Bonmassar, Gian Carlo Antonini Cappellini, Nadia Felli, Alessandra Carè, Ulrich Pfeffer, and Stefania D’Atri

Subjects

miR-126-3p, melanoma, BRAF inhibitors, acquired resistance, proliferation, invasiveness, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Development of resistance to inhibitors of BRAF (BRAFi) and MEK (MEKi) remains a great challenge for targeted therapy in patients with BRAF-mutant melanoma. Here, we explored the role of miRNAs in melanoma acquired resistance to BRAFi. Methods miRNA expression in two BRAF-mutant melanoma cell lines and their dabrafenib-resistant sublines was determined using Affymetrix GeneChip® miRNA 3.1 microarrays and/or qRT-PCR. The effects of miR-126-3p re-expression on proliferation, apoptosis, cell cycle, ERK1/2 and AKT phosphorylation, dabrafenib sensitivity, invasiveness and VEGF-A secretion were evaluated in the dabrafenib-resistant sublines using MTT assays, flow cytometry, immunoblotting, invasion assays in Boyden chambers and ELISA. ADAM9, PIK3R2, MMP7 and CXCR4 expression in the sensitive and dabrafenib-resistant cells was determined by immunoblotting. Small RNA interference was performed to investigate the consequence of VEGFA or ADAM9 silencing on proliferation, invasiveness or dabrafenib sensitivity of the resistant sublines. Long-term proliferation assays were carried out in dabrafenib-sensitive cells to assess the effects of enforced miR-126-3p expression or ADAM9 silencing on resistance development. VEGF-A serum levels in melanoma patients treated with BRAFi or BRAFi+MEKi were evaluated at baseline (T0), after two months of treatment (T2) and at progression (TP) by ELISA. Results miR-126-3p was significantly down-regulated in the dabrafenib-resistant sublines as compared with their parental counterparts. miR-126-3p replacement in the drug-resistant cells inhibited proliferation, cell cycle progression, phosphorylation of ERK1/2 and/or AKT, invasiveness, VEGF-A and ADAM9 expression, and increased dabrafenib sensitivity. VEGFA or ADAM9 silencing impaired proliferation and invasiveness of the drug-resistant sublines. ADAM9 knock-down in the resistant cells increased dabrafenib sensitivity, whereas miR-126-3p enforced expression or ADAM9 silencing in the drug-sensitive cells delayed the development of resistance. At T0 and T2, statistically significant differences were observed in VEGF-A serum levels between patients who responded to therapy and patients who did not. In responder patients, a significant increase of VEGF-A levels was observed at TP versus T2. Conclusions Strategies restoring miR-126-3p expression or targeting VEGF-A or ADAM9 could restrain growth and metastasis of dabrafenib-resistant melanomas and increase their drug sensitivity. Circulating VEGF-A is a promising biomarker for predicting patients’ response to BRAFi or BRAFi+MEKi and for monitoring the onset of resistance.

Published

2019

4. Reduction of T Lymphoma Cells and Immunological Invigoration in a Patient Concurrently Affected by Melanoma and Sezary Syndrome Treated With Nivolumab

Author

Maria Grazia Narducci, Anna Tosi, Alessandra Frezzolini, Enrico Scala, Francesca Passarelli, Laura Bonmassar, Alessandro Monopoli, Maria Pina Accetturi, Maria Cantonetti, Gian Carlo Antonini Cappellini, Federica De Galitiis, Antonio Rosato, Mario Picozza, Giandomenico Russo, and Stefania D’Atri

Subjects

cutaneous T-cell lymphoma, PD-1 blockade therapy, immune sub-populations, Ki67 proliferation index, granzyme B, Immunologic diseases. Allergy, RC581-607

Abstract

Despite the recent availability of several new drugs in hemato-oncology, T-cell lymphomas are still incurable and PD-1 blockade could represent a therapeutic chance for selected patients affected by these malignancies, although further studies are required to understand the biological effects of anti-PD-1 mAbs on neoplastic T-cells and to identify biomarkers for predicting and/or monitoring patients’ response to therapy. Sezary Syndrome (SS) represents a rare and aggressive variant of cutaneous T cell lymphoma (CTCL) with a life expectancy of less than 5 years, characterized by the co-presence of neoplastic lymphocytes mainly in the blood, lymph nodes and skin. In this study we analyzed longitudinal blood samples and lesional skin biopsies of a patient concurrently affected by SS and melanoma who underwent 22 nivolumab administrations. In blood, we observed a progressive reduction of SS cell number and a raise in the percentage of normal CD4+ and CD8+ T cells and NK cells over total leukocytes. Eight weeks from the start of nivolumab, these immune cell subsets showed an increase of Ki67 proliferation index that positively correlated with their PD-1 expression. Conversely, SS cells displayed a strong reduction of Ki67 positivity despite their high PD-1 expression. On skin biopsies we observed a marked reduction of SS cells which were no more detectable at the end of therapy. We also found an increase in the percentage of normal CD4+ T cells with a concomitant decrease of that of CD8+ and CD4+ CD8+ T cells, two cell subsets that, however, acquired a cytotoxic phenotype. In summary, our study demonstrated that nivolumab marked reduced SS tumor burden and invigorated immune responses in our patient. Our data also suggest, for the first time, that Ki67 expression in circulating neoplastic and immune cell subsets, as well as an enrichment in T cells with a cytotoxic phenotype in lesional skin could be valuable markers to assess early on treatment SS patients’ response to PD-1 blockade, a therapeutic strategy under clinical investigation in CTCL (ClinicalTrials.gov NCT03385226, NCT04118868).

Published

2020

5. Exogenous Control of the Expression of Group I CD1 Molecules Competent for Presentation of Microbial Nonpeptide Antigens to Human T Lymphocytes

Author

Angelo Aquino, Grazia Graziani, Ornella Franzese, Salvatore P. Prete, Enzo Bonmassar, Laura Bonmassar, and Stefania D'Atri

Subjects

Immunologic diseases. Allergy, RC581-607

Abstract

Group I CD1 (CD1a, CD1b, and CD1c) glycoproteins expressed on immature and mature dendritic cells present nonpeptide antigens (i.e., lipid or glycolipid molecules mainly of microbial origin) to T cells. Cytotoxic CD1-restricted T lymphocytes recognizing mycobacterial lipid antigens were found in tuberculosis patients. However, thanks to a complex interplay between mycobacteria and CD1 system, M. tuberculosis possesses a successful tactic based, at least in part, on CD1 downregulation to evade CD1-dependent immunity. On the ground of these findings, it is reasonable to hypothesize that modulation of CD1 protein expression by chemical, biological, or infectious agents could influence host's immune reactivity against M. tuberculosis-associated lipids, possibly affecting antitubercular resistance. This scenario prompted us to perform a detailed analysis of the literature concerning the effect of external agents on Group I CD1 expression in order to obtain valuable information on the possible strategies to be adopted for driving properly CD1-dependent immune functions in human pathology and in particular, in human tuberculosis.

Published

2011

6. Circulating miR-1246 and miR-485-3p as Promising Biomarkers of Clinical Response and Outcome in Melanoma Patients Treated with Targeted Therapy

Author

Lauretta Levati, Cristian Bassi, Simona Mastroeni, Laura Lupini, Gian Carlo Antonini Cappellini, Laura Bonmassar, Ester Alvino, Simona Caporali, Pedro Miguel Lacal, Maria Grazia Narducci, Ivan Molineris, Federica De Galitiis, Massimo Negrini, Giandomenico Russo, and Stefania D’Atri

Subjects

resistance, Cancer Research, Oncology, BRAF inhibitors, MEK inhibitors, circulating miRNAs, melanoma

Abstract

Despite the significant improvements in advanced melanoma therapy, there is still a pressing need for biomarkers that can predict patient response and prognosis, and therefore support rational treatment decisions. Here, we investigated whether circulating miRNAs could be biomarkers of clinical outcomes in patients treated with targeted therapy. Using next-generation sequencing, we profiled plasma miRNAs at baseline and at progression in patients treated with BRAF inhibitors (BRAFi) or BRAFi + MEKi. Selected miRNAs associated with response to therapy were subjected to validation by real-time quantitative RT-PCR. Receiver Operating Characteristics (ROC), Kaplan–Meier and univariate and multivariate Cox regression analyses were performed on the validated miR-1246 and miR-485-3p baseline levels. The median baseline levels of miR-1246 and miR-485-3p were significantly higher and lower, respectively, in the group of patients not responding to therapy (NRs) as compared with the group of responding patients (Rs). In Rs, a trend toward an increase in miR-1246 and a decrease in miR-485-3p was observed at progression. Baseline miR-1246 level and the miR-1246/miR-485-3p ratio showed a good ability to discriminate between Rs and NRs. Poorer PFS and OS were observed in patients with unfavorable levels of at least one miRNA. In multivariate analysis, a low level of miR-485-3p and a high miR-1246/miR-485-3p ratio remained independent negative prognostic factors for PFS, while a high miR-1246/miR-485-3p ratio was associated with an increased risk of mortality, although statistical significance was not reached. Evaluation of miR-1246 and miR-485-3p baseline plasma levels might help clinicians to identify melanoma patients most likely to be unresponsive to targeted therapy or at higher risk for short-term PFS and mortality, thus improving their management.

Published

2022

7. Targeting the PTTG1 oncogene impairs proliferation and invasiveness of melanoma cells sensitive or with acquired resistance to the BRAF inhibitor dabrafenib

Author

Ester Alvino, Federica Ruffini, Gian Carlo Antonini Cappellini, Laura Bonmassar, Lauretta Levati, Stefania D'Atri, Pedro Miguel Lacal, Alessandro Scoppola, Simona Mastroeni, Paolo Marchetti, and Simona Caporali

Subjects

0301 basic medicine, Trametinib, Oncogene, Cell growth, Melanoma, Cell, Dabrafenib, Biology, medicine.disease, Extracellular matrix, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, Oncology, Cell culture, 030220 oncology & carcinogenesis, medicine, Cancer research, medicine.drug

Abstract

The pituitary tumor transforming gene 1 (PTTG1) is implicated in tumor growth, metastasis and drug resistance. Here, we investigated the involvement of PTTG1 in melanoma cell proliferation, invasiveness and response to the BRAF inhibitor (BRAFi) dabrafenib. We also preliminary assessed the potential value of circulating PTTG1 protein to monitor melanoma patient response to BRAFi or to dabrafenib plus trametinib. Dabrafenib-resistant cell lines (A375R and SK-Mel28R) were more invasive than their drug-sensitive counterparts (A375 and SK-Mel28), but expressed comparable PTTG1 levels. Dabrafenib abrogated PTTG1 expression and impaired invasion of the extracellular matrix (ECM) in A375 and SK-Mel28 cells. In contrast, it affected neither PTTG1 expression in A375R and SK-Mel28R cells, nor ECM invasion in the latter cells, while further stimulated A375R cell invasiveness. Assessment of proliferation and ECM invasion in control and PTTG1-silenced A375 and SK-Mel28 cells, exposed or not to dabrafenib, demonstrated that the inhibitory effects of this drug were, at least in part, dependent on its ability to down-regulate PTTG1 expression. PTTG1-silencing also impaired proliferation and invasiveness of A375R and SK-Mel28R cells, and counteracted dabrafenib-induced stimulation of ECM invasion in A375R cells. Further experiments performed in A375R cells indicated that PTTG1-silencing impaired cell invasiveness through inhibition of MMP-9 and that PTTG1 expression and ECM invasion could be also reduced by the CDK4/6 inhibitor LEE011. PTTG1 targeting might, therefore, represent a useful strategy to impair proliferation and metastasis of melanomas resistant to BRAFi. Circulating PTTG1 also appeared to deserve further investigation as biomarker to monitor patient response to targeted therapy.

Published

2017

8. miR-126-3p down-regulation contributes to dabrafenib acquired resistance in melanoma by up-regulating ADAM9 and VEGF-A

Author

Gian Carlo Antonini Cappellini, Lauretta Levati, Ester Alvino, Alessandra Carè, Ulrich Pfeffer, Pedro Miguel Lacal, Simona Caporali, Stefania D'Atri, Federica Ruffini, Adriana Amaro, Simona Mastroeni, Laura Bonmassar, and Nadia Felli

Subjects

0301 basic medicine, Male, Vascular Endothelial Growth Factor A, Cancer Research, 0302 clinical medicine, Oximes, Aged, 80 and over, medicine.diagnostic_test, Melanoma, Imidazoles, BRAF inhibitors, Cell cycle, Middle Aged, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Up-Regulation, Gene Expression Regulation, Neoplastic, Vascular endothelial growth factor A, Oncology, 030220 oncology & carcinogenesis, Female, medicine.drug, Adult, Proto-Oncogene Proteins B-raf, proliferation, invasiveness, Down-Regulation, lcsh:RC254-282, Flow cytometry, 03 medical and health sciences, Cell Line, Tumor, microRNA, medicine, miR-126-3p, melanoma, Gene silencing, Humans, Protein kinase B, Aged, Cell Proliferation, business.industry, Research, acquired resistance, Membrane Proteins, Dabrafenib, medicine.disease, ADAM Proteins, MicroRNAs, 030104 developmental biology, Drug Resistance, Neoplasm, Mutation, Cancer research, business

Abstract

Background Development of resistance to inhibitors of BRAF (BRAFi) and MEK (MEKi) remains a great challenge for targeted therapy in patients with BRAF-mutant melanoma. Here, we explored the role of miRNAs in melanoma acquired resistance to BRAFi. Methods miRNA expression in two BRAF-mutant melanoma cell lines and their dabrafenib-resistant sublines was determined using Affymetrix GeneChip® miRNA 3.1 microarrays and/or qRT-PCR. The effects of miR-126-3p re-expression on proliferation, apoptosis, cell cycle, ERK1/2 and AKT phosphorylation, dabrafenib sensitivity, invasiveness and VEGF-A secretion were evaluated in the dabrafenib-resistant sublines using MTT assays, flow cytometry, immunoblotting, invasion assays in Boyden chambers and ELISA. ADAM9, PIK3R2, MMP7 and CXCR4 expression in the sensitive and dabrafenib-resistant cells was determined by immunoblotting. Small RNA interference was performed to investigate the consequence of VEGFA or ADAM9 silencing on proliferation, invasiveness or dabrafenib sensitivity of the resistant sublines. Long-term proliferation assays were carried out in dabrafenib-sensitive cells to assess the effects of enforced miR-126-3p expression or ADAM9 silencing on resistance development. VEGF-A serum levels in melanoma patients treated with BRAFi or BRAFi+MEKi were evaluated at baseline (T0), after two months of treatment (T2) and at progression (TP) by ELISA. Results miR-126-3p was significantly down-regulated in the dabrafenib-resistant sublines as compared with their parental counterparts. miR-126-3p replacement in the drug-resistant cells inhibited proliferation, cell cycle progression, phosphorylation of ERK1/2 and/or AKT, invasiveness, VEGF-A and ADAM9 expression, and increased dabrafenib sensitivity. VEGFA or ADAM9 silencing impaired proliferation and invasiveness of the drug-resistant sublines. ADAM9 knock-down in the resistant cells increased dabrafenib sensitivity, whereas miR-126-3p enforced expression or ADAM9 silencing in the drug-sensitive cells delayed the development of resistance. At T0 and T2, statistically significant differences were observed in VEGF-A serum levels between patients who responded to therapy and patients who did not. In responder patients, a significant increase of VEGF-A levels was observed at TP versus T2. Conclusions Strategies restoring miR-126-3p expression or targeting VEGF-A or ADAM9 could restrain growth and metastasis of dabrafenib-resistant melanomas and increase their drug sensitivity. Circulating VEGF-A is a promising biomarker for predicting patients’ response to BRAFi or BRAFi+MEKi and for monitoring the onset of resistance. Electronic supplementary material The online version of this article (10.1186/s13046-019-1238-4) contains supplementary material, which is available to authorized users.

Published

2019

9. Influence of fatty acid synthase inhibitor orlistat on the DNA repair enzyme O6-methylguanine-DNA methyltransferase in human normal or malignant cells in vitro

Author

Laura Bonmassar, Maria Pia Fuggetta, Enzo Bonmassar, Elena Pagani, Giorgia Cioccoloni, Stefania D'Atri, Angelo Aquino, and Simona Caporali

Subjects

Cancer Research, Methyltransferase, DNA damage, DNA repair, human cancer cells, anti-obesity drugs, carcinogenesis, O6-methylguanine-DNA methyltransferase, temozolomide, In Vitro Techniques, Biology, medicine.disease_cause, DNA methyltransferase, Lactones, Cell Line, Tumor, Neoplasms, medicine, Humans, Enzyme Inhibitors, MGMT inhibitors, DNA Modification Methylases, neoplasms, orlistat, O-6-methylguanine-DNA methyltransferase, Tumor Suppressor Proteins, Settore BIO/14, Cell cycle, HCT116 Cells, Molecular biology, digestive system diseases, Dacarbazine, Orlistat, DNA Repair Enzymes, Oncology, Purines, Leukocytes, Mononuclear, Cancer research, Carcinogenesis, HT29 Cells, lomeguatrib, medicine.drug

Abstract

Tetrahydrolipstatin (orlistat), an inhibitor of lipases and fatty acid synthase, is used orally for long-term treatment of obesity. Although the drug possesses striking antitumor activities in vitro against human cancer cells and in vitro and in vivo against animal tumors, it also induces precancerous lesions in rat colon. Therefore, we tested the in vitro effect of orlistat on the expression of O-6-methylguanine-DNA methyltransferase (MGMT), a DNA repair enzyme that plays an essential role in the control of mutagenesis and carcinogenesis. Western blot analysis demonstrated that 2-day continuous exposure to 40 mu M orlistat did not affect MGMT levels in a human melanoma cell line, but downregulated the repair protein by 30-70% in human peripheral blood mononuclear cells, in two leukemia and two colon cancer cell lines. On the other hand, orlistat did not alter noticeably MGMT mRNA expression. Differently from lomeguatrib (a false substrate, strong inhibitor of MGMT) orlistat did not reduce substantially MGMT function after 2-h exposure of target cells to the agent, suggesting that this drug is not a competitive inhibitor of the repair protein. Combined treatment with orlistat and lomeguatrib showed additive reduction of MGMT levels. More importantly, orlistat-mediated downregulation of MGMT protein expression was markedly amplified when the drug was combined with a DNA methylating agent endowed with carcinogenic properties such as temozolomide. In conclusion, even if orlistat is scarcely absorbed by oral route, it is possible that this drug could reduce local MGMT-mediated protection against DNA damage provoked by DNA methylating compounds on gastrointestinal tract epithelial cells, thus favoring chemical carcinogenesis.

Published

2015

10. Targeting the

Author

Simona, Caporali, Ester, Alvino, Pedro Miguel, Lacal, Federica, Ruffini, Lauretta, Levati, Laura, Bonmassar, Alessandro, Scoppola, Paolo, Marchetti, Simona, Mastroeni, Gian Carlo, Antonini Cappellini, and Stefania, D'Atri

Subjects

proliferation, melanoma, dabrafenib, invasion, PTTG1, Research Paper

Abstract

The pituitary tumor transforming gene 1 (PTTG1) is implicated in tumor growth, metastasis and drug resistance. Here, we investigated the involvement of PTTG1 in melanoma cell proliferation, invasiveness and response to the BRAF inhibitor (BRAFi) dabrafenib. We also preliminary assessed the potential value of circulating PTTG1 protein to monitor melanoma patient response to BRAFi or to dabrafenib plus trametinib. Dabrafenib-resistant cell lines (A375R and SK-Mel28R) were more invasive than their drug-sensitive counterparts (A375 and SK-Mel28), but expressed comparable PTTG1 levels. Dabrafenib abrogated PTTG1 expression and impaired invasion of the extracellular matrix (ECM) in A375 and SK-Mel28 cells. In contrast, it affected neither PTTG1 expression in A375R and SK-Mel28R cells, nor ECM invasion in the latter cells, while further stimulated A375R cell invasiveness. Assessment of proliferation and ECM invasion in control and PTTG1-silenced A375 and SK-Mel28 cells, exposed or not to dabrafenib, demonstrated that the inhibitory effects of this drug were, at least in part, dependent on its ability to down-regulate PTTG1 expression. PTTG1-silencing also impaired proliferation and invasiveness of A375R and SK-Mel28R cells, and counteracted dabrafenib-induced stimulation of ECM invasion in A375R cells. Further experiments performed in A375R cells indicated that PTTG1-silencing impaired cell invasiveness through inhibition of MMP-9 and that PTTG1 expression and ECM invasion could be also reduced by the CDK4/6 inhibitor LEE011. PTTG1 targeting might, therefore, represent a useful strategy to impair proliferation and metastasis of melanomas resistant to BRAFi. Circulating PTTG1 also appeared to deserve further investigation as biomarker to monitor patient response to targeted therapy.

Published

2017

11. Antitumour activity of resveratrol on human melanoma cells: A possible mechanism related to its interaction with malignant cell telomerase

Author

Daniela Montesarchio, Enzo Bonmassar, Giampiero Ravagnan, Maria Pia Fuggetta, Giovanni N. Roviello, Domenica Musumeci, Laura Bonmassar, Serena Guida, Chiara Platella, Angelo Aquino, Platella, Chiara, Guida, Serena, Bonmassar, Laura, Aquino, Angelo, Bonmassar, Enzo, Ravagnan, Giampiero, Montesarchio, Daniela, Roviello, Giovanni N., Musumeci, Domenica, and Fuggetta, Maria Pia

Subjects

0301 basic medicine, Telomerase, Melanoma cell, Settore MED/06 - Oncologia Medica, Biophysics, Antineoplastic Agents, Biology, Resveratrol, Biochemistry, Biophysical Phenomena, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Resveratrol Telomerase activity hTERT Telomeres G-quadruplex DNA Melanoma cells, Cell Line, Tumor, Stilbenes, medicine, Cytotoxic T cell, Bioassay, Humans, Telomerase reverse transcriptase, Melanoma cells, Molecular Biology, Telomerase activity, Melanoma, Cell Proliferation, Cell growth, Circular Dichroism, Spectrum Analysis, Settore BIO/14, Telomere, medicine.disease, G-Quadruplexes, 030104 developmental biology, G-quadruplex DNA, Telomeres, Spectrometry, Fluorescence, chemistry, Biophysic, 030220 oncology & carcinogenesis, Nucleic Acid Conformation, hTERT, Copper

Abstract

Background trans-Resveratrol (tRES) is a polyphenolic stilbene found in plant products which has attracted great attention because of its antioxidant, anti-inflammatory and anticancer properties. Methods The possible correlation between tRES-induced suppression of melanoma cell growth and its influence on telomerase expression has been investigated by biological assays. Moreover, in order to gain new knowledge about possible mechanisms of action of tRES as antineoplastic agent, its interaction with biologically relevant secondary structure-forming DNA sequences, its aggregation properties and copper-binding activity have been studied by CD, UV and fluorescence spectroscopies. Results Biological assays have confirmed that growth inhibitory properties of tRES well correlate with the reduction of telomerase activity and hTERT gene transcript levels in human melanoma cells. Biophysical studies in solution have proved that tRES binds all the studied DNA model systems with low affinity, however showing high ability to discriminate G-quadruplex vs. duplex DNA. In addition, tRES has shown no propensity to form aggregates in the explored concentration range and has been found able to bind Cu2+ ions with a 2:1 stoichiometry. Conclusions From these biological and biophysical analyses it has emerged that tRES produces cytotoxic effects on human melanoma cells and, at a molecular level, is able to bind Cu2+ and cancer-involved G-quadruplexes, suggesting that multiple mechanisms of action could be involved in its antineoplastic activity. General significance Expanding the knowledge on the putative mechanisms of action of tRES as antitumour agent can help to develop novel, effective tRES-based anticancer drugs.

Published

2017

12. Circulating tumor cells in colorectal cancer patients

Author

Ettore Capoluongo, Francesco Torino, Angelo Aquino, Liana De Vecchis, Enzo Bonmassar, Cecilia Zuppi, Laura Bonmassar, Agnese Barnabei, Torino, F, Bonmassar, E, Bonmassar, L, De Vecchis, L, Barnabei, A, Zuppi, C, Capoluongo, E, and Aquino, A

Subjects

Oncology, medicine.medical_specialty, Prognostic factor, Pathology, Settore MED/06 - Oncologia Medica, Colorectal cancer, Settore BIO/12 - BIOCHIMICA CLINICA E BIOLOGIA MOLECOLARE CLINICA, Circulating tumor cell, Internal medicine, Biomarkers, Tumor, medicine, Humans, Radiology, Nuclear Medicine and imaging, In patient, Neoplasm Metastasis, business.industry, Liver Neoplasms, Settore BIO/14, Circulating tumor cells, General Medicine, Predictive factor, Neoplastic Cells, Circulating, Prognosis, medicine.disease, CTC, Peripheral blood, medicine.anatomical_structure, Neoplastic Stem Cells, Bone marrow, Colorectal Neoplasms, business

Abstract

The availability of sensitive methods has allowed the detailed study of circulating tumor cells only recently. Evolving evidence support the prognostic and predictive role of these cells in patients affected by several solid tumors, including colorectal cancer. Ongoing studies are aimed at confirming that the molecular characterization of circulating tumor cells in peripheral blood and in bone marrow of patients is a powerful tool to improve the patient risk-stratification, to monitor activity of the drugs, to develop more appropriate targeted therapies and tailored treatments. In parallel, results from these correlative studies promise to gain a better biological understanding of the metastatic process. The clinical utility of the detection of circulating tumor cells in patients affected by colorectal cancer is still hampered by a number of specific hurdles. Improvement in sensitivity and specificity of the available methods of detection, standardization of these methods and functional characterization of circulating tumor cells in well designed and statistically well powered studies are the key steps to reach these ambitious objectives in colorectal cancer patients as well.

Published

2013

13. Abstract 474: Alterations of micro-RNAs are associated with melanoma resistance to BRAF inhibitors: Role of miR-126

Author

Ester Alvino, Cristian Bassi, Adriana Amaro, Gian Carlo Antonini Cappellini, Massimo Negrini, Pedro Miguel Lacal, Lauretta Levati, Laura Bonmassar, Giandomenico Russo, Ulrich Pfeffer, Nadia Felli, Alessandra Carè, Stefania D'Atri, Laura Lupini, and Simona Caporali

Subjects

Cancer Research, Oncology, Melanoma, medicine, Cancer research, Biology, medicine.disease

Abstract

Altered expression of miRNAs has been demonstrated in tumor tissue and plasma/serum of cancer patients. miRNAs have been shown to have both diagnostic and prognostic significance and to potentially constitute novel targets and therapeutic agents for cancer treatment. Experimental evidences also support an involvement of miRNAs in tumor cell response to therapy. In this study, we explored the role of miRNAs in melanoma resistance to BRAF inhibitors (BRAFi). The melanoma cell line A375 and its dabrafenib-resistant subline A375R, which displays increased invasiveness and VEGF secretion, were analyzed for miRNA expression using Affymetrix GeneChip® miRNA 3.1 microarrays. Differential expression of selected miRNAs was confirmed in the two cell lines using qRT-PCR. miR-126, previously shown to act as a tumor suppressor gene in melanoma, was chosen for additional studies that were performed also in a second pair of matched melanoma cell lines, sensitive or resistant to dabrafenib (i.e SK-Mel28 and SK-Mel28R). The resistant sublines were transfected with 50 nM Pre-miR hsa-miR-126 miRNA Precursor (pre-miRNA-126) or Pre-miR miRNA Precursor Negative Control#1 (Ambion®) and analyzed for proliferation 6 days later using the MTT assay. Seventy-two hours after transfection, the cells were also assayed for invasion of the extracellular matrix and VEGF-A secretion using Boyden Chamber and ELISA assays, respectively. In 33 melanoma patients treated with BRAFi, alone or in combination with MEKi, plasma samples were collected before the beginning of therapy (T0), and two months later (T2) and subjected to miRNA expression profiling by small RNA-seq. A375R cells displayed 13 up-regulated miRNAs and 32 down-regulated miRNAs with respect to A375 cells (SAM analysis; fold change ≥ 2). Down-regulation of miR-126 was confirmed by qRT-PCR analysis in both A375R and SK-Mel28R cells. Restoration of miR-126 expression in A375R and SK-Mel28R cells by pre-miRNA-126 transfection impaired proliferation, invasion and secretion of VEGF-A, a validated target of miR-126. Fifthy and 28 circulating miRNAs were differentially expressed at T0 and at T2, respectively, between patients who responded to therapy (n=28) and patients who did not (n=5). Our results demonstrate that down-regulation of miR-126 expression is associated with acquired resistance to dabrafenib in melanoma cells and suggest that restoration of this miRNA in dabrafenib-resistant melanomas might restrain tumor growth and metastasis. They also show that in melanoma patients with primary resistance to BRAFi, a set of circulating miRNAs is differentially expressed with respect to patients responding to therapy, suggesting a potential role of circulating miRNAs as biomarkers for early prediction of drug response. Supported by the Italian Ministry of Health, grant 5PerMille-2010 and AIRC, IGP 17585 Citation Format: Simona Caporali, Lauretta Levati, Ester Alvino, Adriana Amaro, Pedro Miguel Lacal, Laura Bonmassar, Cristian Bassi, Laura Lupini, Gian Carlo Antonini Cappellini, Ulrich Pfeffer, Massimo Negrini, Nadia Felli, Alessandra Carè, Giandomenico Russo, Stefania D'Atri. Alterations of micro-RNAs are associated with melanoma resistance to BRAF inhibitors: Role of miR-126 [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2018; 2018 Apr 14-18; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2018;78(13 Suppl):Abstract nr 474.

Published

2018

14. A novel telomerase-based approach to detect natural cell-mediated cytotoxic activity against tumor cells in vitro

Author

Laura Bonmassar, Isabella Faraoni, Lorena Rossi, Anna Giuliani, Enzo Bonmassar, and Andrea Cottarelli

Subjects

Telomerase, Lymphokine-activated killer cell, Effector, ELISPOT, Immunology, Biology, Cytotoxicity Tests, Immunologic, Chromium Radioisotopes, Natural killer cell, Killer Cells, Natural, Cell killing, medicine.anatomical_structure, Neoplasms, Cancer research, medicine, Humans, Immunology and Allergy, Cytotoxic T cell, K562 Cells, Killer Cells, Lymphokine-Activated, T-Lymphocytes, Cytotoxic, K562 cells

Abstract

This study was designed to develop a novel technical approach based on tumor-associated telomerase activity to detect cytotoxic activity of effector cells of the natural immune system against neoplastic cells. Human K562, DAUDI or Raji leukemia cells were co-cultured with NK or LAK effector cells at 37 degrees C for 4 h. Target cell killing was evaluated by 51Cr-release assay (CRA) or reduction of telomerase activity (R-TRAPCTX) of the target after exposure to effector cells. NK and LAK effector cells tested against K562 target cells at effector/target ratio of 50:1 showed cytotoxicity of 65% and 78%, respectively, with CRA and 51% and 74%, respectively, with R-TRAPCTX. Incorrect results were obtained with CRA when target cells were admixed with normal fibroblasts, whereas R-TRAPCTX was not influenced by the presence of normal cells. Control experiments performed with telomerase-negative cells showed that telomerase activity of effector cells was not altered during the cytolytic reaction. Moreover, supernatants obtained from effector-target cell co-cultures did not influence telomerase activity of targets. This novel R-TRAPCTX method to assay anti-tumor natural and possibly antigen-dependent cell-mediated cytotoxicity appears to provide sensible advantages over classical CRA or gamma-interferon release by effector cells in presence of target cells (ELISPOT), since (a) it furnishes reliable data on effector cell killing against neoplastic cells, even when malignant cells are admixed with normal cells, as frequently occurs in tumor biopsies, not manageable with CRA; (b) it provides an actual measure of target cell killing, not furnished by ELISPOT technique.

Published

2005

15. The antiretroviral agent saquinavir enhances hTERT expression and telomerase activity in human T leukaemia cells in vitro

Author

Enzo Bonmassar, Loredana Guglielmi, A. Comandini, Riccardo Adamo, Laura Bonmassar, Angelo Aquino, and Ornella Franzese

Subjects

Cancer Research, Telomerase, Leukemia, T-Cell, Transcription, Genetic, Settore MED/06 - Oncologia Medica, viruses, Biology, Jurkat cells, Proto-Oncogene Proteins c-myc, Jurkat Cells, Catalytic Domain, Cell Line, Tumor, medicine, Leukaemia, Humans, Telomerase reverse transcriptase, Transcription factor, Saquinavir, Cell Proliferation, Gene Expression Regulation, Leukemic, Cell growth, Research, Settore BIO/14, HIV Protease Inhibitors, Transfection, Molecular biology, Enzyme Activation, c-Myc, Oncology, Cell culture, hTERT, medicine.drug

Abstract

Background Saquinavir, a protease inhibitor utilized in HIV infection, shows antitumor activity in various experimental models. In previous studies performed in our laboratory the drug was found to induce a substantial increase of telomerase activity in normal peripheral blood mononuclear cells. Aim of the present investigation was to test whether saquinavir was able to increase telomerase activity and the expression of the catalytic subunit of telomerase, hTERT, in human malignant hematopoietic cells. Methods Human Jurkat CD4+ T cell leukaemia cell line was used throughout the present study. The antiproliferative effect of saquinavir was tested by the MTT assay. Telomerase activity was determined according to the telomeric repeat amplification protocol. The expression of hTERT mRNA was semi-quantitative evaluated by RT-PCR amplification and quantitative Real Time PCR. The binding of the transcription factor c-Myc to its specific E-Box DNA binding-site of hTERT promoter was analyzed by Electophoretic Mobility Shift Assay (EMSA). The amount of c-Myc in cytoplasm and nucleus of leukemia cells was determined by Western Blot analysis, and c-Myc down-regulation was obtained by siRNA transfection. Results Saquinavir produced a substantial increase of telomerase activity in Jurkat cells in vitro without increasing but rather reducing target cell proliferation rate. Telomerase up-regulation appeared to be the result of enhanced expression of hTERT. Saquinavir-mediated up-regulation of hTERT gene was the result of the increased binding of proteins to the E-Box sequence of the promoter. Moreover, saquinavir amplified the expression of c-Myc especially in the nuclear cell fraction. The direct influence of saquinavir on this transcription factor was also demonstrated by the antagonistic effect of the drug on siRNA induced c-Myc suppression. Since c-Myc is the main responsible for hTERT transcription, these findings suggest that the main mechanism underlying saquinavir-induced telomerase activation is mediated by c-Myc up-regulation. Conclusions Saquinavir augments hTERT expression while inhibiting leukemic cell growth. Experimental evidences show that this effect is mediated by saquinavir-influenced increase of c-Myc levels. This could have relevance in terms of enhanced hTERT-dependent tumor cell immunogenicity and suggests new paharmacological approaches interfering with c-Myc dependent pathways.

Published

2013

16. Interferon-Beta combined with interleukin-2 restores human natural cytotoxicity impaired in vitro by ionizing radiations

Author

Ornella Franzese, Andrea Cottarelli, Maria Pia Fuggetta, Rita Pepponi, Laura Bonmassar, Giuseppe Starace, and Maria Tricarico

Subjects

Cytotoxicity, Immunologic, Antigens, CD56, Apoptosis, Cell Line, Tumor, GPI-Linked Proteins, Gamma Rays, Humans, Immunity, Innate, Interferon-beta, Interleukin-2, K562 Cells, Killer Cells, Natural, Leukocytes, Mononuclear, Lymphocyte Subsets, Proto-Oncogene Proteins c-bcl-2, Receptors, IgG, Cytotoxicity, Immunologic, Interferon, Receptors, Leukocytes, Innate, Killer Cells, Tumor, Settore BIO/14, CD56 Antigen, Natural, CD56, medicine.drug, Interleukin 2, IgG, Mononuclear, Immunology, chemical and pharmacologic phenomena, Biology, CD16, Peripheral blood mononuclear cell, Cell Line, Virology, medicine, Antigens, radiation interferon, Innate immune system, Immunity, Cell Biology, In vitro, Cancer research

Abstract

It is well known that ionizing radiations induce a marked downregulation of antigen-dependent and natural immunity for a prolonged period of time. This is due, at least in part, to radiation-induced apoptosis of different lymphocyte subpopulations, including natural killer (NK) cells. Aim of this study was to investigate the capability of Beta Interferon (β-IFN) and Interleukin-2 (IL2), alone or in combination, to restore the functional activity of the natural immune system. Mononuclear cells (MNCs) obtained from intact or in vitro irradiated human peripheral blood were treated in vitro with β-IFN immediately before or at the end of the 4-day treatment with IL2. Time-course analysis was performed on the NK activity, the total number and the apoptotic fraction of CD16+ and CD56+ cells, the 2 main NK effector cell subpopulations. The results indicate that radiation-induced impairment of natural cytotoxicity of MNC could be successfully antagonized by the β-IFN+IL2 combination, mainly when exposure to β-IFN preceded IL2 treatment. This radioprotective effect is paralleled by lower levels of radiation-induced apoptosis and increased expression of the antiapoptotic Bcl-2 protein. Since natural immunity can play a significant role in antitumor host's resistance, these results could provide the rational basis for a cytokine-based pharmacological strategy able to restore immune responsiveness and to afford possible therapeutic benefits in cancer patients undergoing radiotherapy.

Published

2013

17. Cetuximab +/- chemotherapy enhances dendritic cell-mediated phagocytosis of colon cancer cells and ignites a highly efficient colon cancer antigen-specific cytotoxic T-cell response in vitro

Author

M. M. De Santi, Elena Bestoso, Mario Turriziani, Susanna Mannucci, Alberto Abbruzzese, M. Marra, Serena Apollinari, M. Del Vecchio, Pierosandro Tagliaferri, Angelo Aquino, C. Botta, Michele Caraglia, G. Gori Savellini, Pierpaolo Correale, Laura Bonmassar, Maria Grazia Cusi, Correale P., Botta C., Cusi M.G., Del Vecchio M.T., De Santi M.M., Gori Savellini G., Bestoso E., Apollinari S., Mannucci S., Marra M., Abbruzzese A., Aquino A., Turriziani M., Bonmassar L., Caraglia M., and Tagliaferri P.

Subjects

cetuximab, chemotherapy, danger signal, cytotoxic-T-lymphocytes, phagocytosis, Cancer Research, Colorectal cancer, Settore MED/06 - Oncologia Medica, Antigen-Presenting Cells, Antibodies, Monoclonal, Humanized, Cross-Priming, Antigen, Antigens, Neoplasm, Cell Line, Tumor, Antineoplastic Combined Chemotherapy Protocols, Humans, Medicine, Cytotoxic T cell, Cetuximab, business.industry, Settore BIO/14, Antibodies, Monoclonal, Dendritic Cells, Dendritic cell, medicine.disease, cytotoxic-T-lymphocyte, digestive system diseases, Tumor antigen, CTL, Oncology, Colonic Neoplasms, Cancer cell, Immunology, Leukocytes, Mononuclear, Cancer research, business, HT29 Cells, T-Lymphocytes, Cytotoxic, medicine.drug

Abstract

Cetuximab is a human/mouse chimeric IgG1 monoclonal antibody (mAb) to epidermal growth factor receptor, approved for colorectal carcinoma treatment in combination with chemotherapy. The immune-mediated effects elicited by its human fraction of crystallization moiety might critically contribute to the overall anti-tumor effectiveness of the antibody. We therefore investigated cetuximab ability to promote colon cancer cell opsonization and phagocytosis by human dendritic cells (DCs) that are subsequently engaged in antigen-cross presentation to cytotoxic T-lymphocyte (CTL) precursors. Human colon cancer cell lines were evaluated for susceptibility to DC-mediated phagocytosis before and after treatment with chemotherapy ± cetuximab in vitro. Human DCs loaded with control or drug-treated cetuximab-coated colon cancer cells were used to in vitro generate cytotoxic T cell clones from peripheral blood mononuclear cells of human leucocyte antigen-A(*)02.01 + donors. T-cell cultures were characterized for immune-phenotype and tumor-antigen specific CTL activity. The results confirmed that treatment of tumor cells with irinotecan + L-folinate + 5-flurouracil (ILF) or with gemcitabine + ILF increased tumor antigen expression. Moreover, malignant cells exposed to chemotherapy and cetuximab were highly susceptible to phagocytosis by human DCs and were able to promote their activation. The consequent DC-mediated cross-priming of antigens derived from mAb-covered/drug-treated cancer cells elicited a robust CTL anti-tumor response. On the basis of our data, we suggest a possible involvement of CTL-dependent immunity in cetuximab anti-cancer effects. Copyright © 2011 UICC.

Published

2012

18. Exogenous Control of the Expression of Group I CD1 Molecules Competent for Presentation of Microbial Nonpeptide Antigens to Human T Lymphocytes

Author

Stefania D'Atri, S.P. Prete, Laura Bonmassar, Grazia Graziani, Enzo Bonmassar, Ornella Franzese, and Angelo Aquino

Subjects

lcsh:Immunologic diseases. Allergy, T-Lymphocytes, Immunology, Antigen presentation, CD1, chemical and pharmacologic phenomena, HIV Infections, Review Article, Biology, complex mixtures, Mycobacterium, Antigens, CD1, Immune system, Antigen, Immunity, parasitic diseases, Immunology and Allergy, Cytotoxic T cell, Animals, Humans, Immunologic Factors, Tuberculosis, Pan-T antigens, Antigen Presentation, Antigens, Bacterial, Settore BIO/14, hemic and immune systems, General Medicine, Dendritic Cells, biology.organism_classification, Gene Expression Regulation, HIV-1, lipids (amino acids, peptides, and proteins), lcsh:RC581-607

Abstract

Group I CD1 (CD1a, CD1b, and CD1c) glycoproteins expressed on immature and mature dendritic cells present nonpeptide antigens (i.e., lipid or glycolipid molecules mainly of microbial origin) to T cells. Cytotoxic CD1-restricted T lymphocytes recognizing mycobacterial lipid antigens were found in tuberculosis patients. However, thanks to a complex interplay betweenmycobacteriaand CD1 system,M. tuberculosispossesses a successful tactic based, at least in part, on CD1 downregulation to evade CD1-dependent immunity. On the ground of these findings, it is reasonable to hypothesize that modulation of CD1 protein expression by chemical, biological, or infectious agents could influence host's immune reactivity againstM. tuberculosis-associated lipids, possibly affecting antitubercular resistance. This scenario prompted us to perform a detailed analysis of the literature concerning the effect of external agents on Group I CD1 expression in order to obtain valuable information on the possible strategies to be adopted for driving properly CD1-dependent immune functions in human pathology and in particular, in human tuberculosis.

Published

2011

19. Treatment of peripheral blood with staurosporine increases detection of circulating carcinoembryonic antigen positive tumor cells

Author

Angelo Aquino, S.P. Prete, Alessandra Balduzzi, F. Concolino, Laura Bonmassar, Enzo Bonmassar, Vincenzo Formica, Grazia Graziani, and Emanuela Fossile

Subjects

micrometastasis, Cancer Research, Pathology, medicine.medical_specialty, Settore MED/06 - Oncologia Medica, Colorectal cancer, medicine.medical_treatment, colorectal cancer, Sensitivity and Specificity, Antibodies, carcinoembryonic antigen, immunobead RT-PCR, staurosporine, Carcinoembryonic antigen, Monoclonal, medicine, Carcinoma, Tumor Cells, Cultured, Staurosporine, Humans, Antibodies, Monoclonal, Immunomagnetic Separation, Blood, Carcinoembryonic Antigen, Enzyme Inhibitors, Reverse Transcriptase Polymerase Chain Reaction, Protein Kinase C, Colonic Neoplasms, Protein kinase C, Chemotherapy, Cultured, biology, business.industry, Settore BIO/14, medicine.disease, Tumor Cells, Carcinoembryonic Antigen Positive, Reverse transcription polymerase chain reaction, Oncology, Cancer research, biology.protein, business, medicine.drug

Published

2002

20. Tolerance of human MSH2+/- lymphoblastoid cells to the methylating agent temozolomide

Author

Zdena Bartosova, Giancarlo Marra, Pascal Schweizer, Josef Jiricny, Chantal Corti, Laura Bonmassar, Maria Sofia Cattaruzza, Stefania D'Atri, Karl Heinimann, and Minna Nyström-Lahti

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, Heterozygote, DNA Repair, DNA repair, Cell Survival, Biology, medicine.disease_cause, Malignant transformation, Cell Line, Germline mutation, Proto-Oncogene Proteins, medicine, Temozolomide, Tumor Cells, Cultured, Humans, Lymphocytes, Antineoplastic Agents, Alkylating, Adaptor Proteins, Signal Transducing, Mutation, Multidisciplinary, nutritional and metabolic diseases, Nuclear Proteins, Heterozygote advantage, Biological Sciences, Molecular biology, Phenotype, Colorectal Neoplasms, Hereditary Nonpolyposis, digestive system diseases, Neoplasm Proteins, DNA-Binding Proteins, Dacarbazine, MutS Homolog 2 Protein, MSH2, DNA mismatch repair, Carrier Proteins, MutL Protein Homolog 1

Abstract

Members of hereditary nonpolyposis colon cancer (HNPCC) families harboring heterozygous germline mutations in the DNA mismatch repair genes hMSH2 or hMLH1 present with tumors generally two to three decades earlier than individuals with nonfamilial sporadic colon cancer. We searched for phenotypic features that might predispose heterozygous cells from HNPCC kindreds to malignant transformation. hMSH2 +/− lymphoblastoid cell lines were found to be on average about 4-fold more tolerant than wild-type cells to killing by the methylating agent temozolomide, a phenotype that is invariably linked with impairment of the mismatch repair system. This finding was associated with an average 2-fold decrease of the steady-state level of hMSH2 protein in hMSH2 +/− cell lines. In contrast, hMLH1 +/− heterozygous cells were indistinguishable from normal controls in these assays. Thus, despite the fact that HNPCC families harboring mutations in hMSH2 or hMLH1 cannot be distinguished clinically, the early stages of the carcinogenic process in hMSH2 and hMLH1 mutation carriers may be different. Should hMSH2 +/− colonocytes and lymphoblasts harbor a similar phenotype, the increased tolerance of the former to DNA-damaging agents present in the human colon may play a key role in the initiation of the carcinogenic process.

Published

2001

21. DNA repair enzymes and cytotoxic effects of temozolomide: Comparative studies between tumor cells and normal cells of the immune system

Author

Francesca Passarelli, Ester Alvino, Sabrina Falcinelli, Stefania D'Atri, Laura Bonmassar, P Lacal, Mario Turriziani, Maria Pia Fuggetta, Elena Pagani, S.P. Prete, Rita Pepponi, and F. Guadagni

Subjects

Skin Neoplasms, DNA Repair, DNA repair, Lymphocyte, Biology, Peripheral blood mononuclear cell, O(6)-Methylguanine-DNA Methyltransferase, Immune system, Temozolomide, Tumor Cells, Cultured, medicine, Humans, Cytotoxic T cell, Pharmacology (medical), Lymphocytes, Killer Cells, Lymphokine-Activated, Antineoplastic Agents, Alkylating, Melanoma, Pharmacology, Cell growth, Lymphokine, Burkitt Lymphoma, Dacarbazine, Infectious Diseases, medicine.anatomical_structure, Oncology, Drug Resistance, Neoplasm, Immunology, Leukocytes, Mononuclear, Cancer research, Interleukin-2, Leukemia, Erythroblastic, Acute, Cell Division, DNA Damage, Alkyltransferase

Abstract

O6-alkylguanine-DNA alkyltransferase (OGAT) and the mismatch repair system (MRS) play a crucial role in the susceptibility of tumor cells to the cytotoxic effects of agents that generate O6-methylguanine in DNA, including the triazene compound temozolomide (TMZ). Studies performed with peripheral blood mononuclear cells (MNC) showed that TMZ was scarcely active on lymphocyte functions not dependent on cell proliferation (e.g. NK activity and cytokine-mediated induction of CD1b molecule in adherent MNC). In contrast, TMZ depressed proliferation and lymphokine activated killer (LAK) cell generation in response to IL-2. In this case, a reasonably good inverse relationship was found between OGAT levels of MNC and their susceptibility to TMZ. This study also analyzed the ratio of the toxic effect of TMZ on MNC and on tumor cells (i.e. "Tumor-Immune Function Toxicity Index", TIFTI). A particularly favorable TIFTI can be obtained when OGAT levels are extremely high in MNC and markedly low in tumor cells. This holds true for MRS-proficient neoplastic cells, but not for MRS-deficient tumors. In conclusion, strategies aimed at modulating OGAT and MRS may improve the clinical response to TMZ. However, the use of OGAT inhibitors to potentiate the antitumor activity of TMZ might result in a concomitant increase of the immunosuppressive effects of the drug, thus reducing the relative TIFTI.

22. Combined effects of 5-Fluorouracil, Folinic acid and Oxaliplatin on the expression of carcinoembryonic antigen in human colon cancer cells: pharmacological basis to develop an active antitumor immunochemotherapy

Author

Pierpaolo Correale, Liana De Vecchis, Maria Chiara Massara, Francesco Torino, Angelo Aquino, Mario Turriziani, Alessia De Rossi, Laura Bonmassar, and S.P. Prete

Subjects

Oncology, Cancer Research, medicine.medical_specialty, RNA, Messenger, Carcinoembryonic Antigen, Antineoplastic Agents, Humans, Fluorouracil, Organoplatinum Compounds, Leucovorin, Flow Cytometry, Cell Line, Tumor, Colonic Neoplasms, Colorectal cancer, Settore MED/06 - Oncologia Medica, medicine.medical_treatment, Messenger, lcsh:RC254-282, Cell Line, Folinic acid, Carcinoembryonic antigen, Internal medicine, medicine, neoplasms, Chemotherapy, Tumor, biology, business.industry, Research, Settore BIO/14, Cancer, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, digestive system diseases, Oxaliplatin, Apoptosis, biology.protein, Cancer research, RNA, business, medicine.drug

Abstract

Background Five-fluorouracil (FU), mainly associated with leucovorin (L), plays an essential role in chemotherapy of colorectal carcinoma. Moreover, FU ± L has been found to increase the expression of tumor-associated carcinoembryonic antigen (CEA), that may be an important target in therapeutic protocols of active specific immunotherapy. FU + L (FUL) are frequently combined with oxaliplatin (OXA) in advanced colon cancer patients. Thus, we investigated whether FUL in combination with OXA according to 2 different schedules may influence CEA expression in human colon cancer cells in vitro. Methods CEA protein expression was evaluated by cytofluorimetric and western blot analysis. Relative quantification of CEA mRNA was assessed by real time RT-PCR analysis. Results Levels of CEA protein and transcript were found to be higher in FUL-treated cells than in controls. However, when target cells were exposed to OXA before but not after FUL treatment, the up-regulation of CEA was partially inhibited. Conclusion These results suggest that target cells must be exposed to OXA after but not before treatment with the fluoropyrimidine in order to exploit drug-induced up-regulation of CEA. This finding appears to provide useful information to design chemo-immunotherapy protocols based on FUL + OXA, combined with host's immunity against CEA directed cancer vaccines.