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122 results on '"Marabese, M"'

1. Efficacy and safety of ramucirumab plus carboplatin and paclitaxel in untreated metastatic thymic carcinoma: RELEVENT phase II trial (NCT03921671)

Author

Proto, C., Ganzinelli, M., Manglaviti, S., Imbimbo, M., Galli, G., Marabese, M., Zollo, F., Alvisi, M.F., Perrino, M., Cordua, N., Borea, F., de Vincenzo, F., Chella, A., Cappelli, S., Pardini, E., Ballatore, Z., Lucarelli, A., Ambrosini, E., Giuliano, M., Pietroluongo, E., Mulargiu, C., Fabbri, A., Prelaj, A., Occhipinti, M., Brambilla, M., Mazzeo, L., Beninato, T., Vigorito, R., Ruggirello, M., Greco, F.G., Calareso, G., Miliziano, D., Rulli, E., De Simone, I., Torri, V., de Braud, F.G.M., Pasello, G., De Placido, P., Berardi, R., Petrini, I., Zucali, P., Garassino, M.C., and Lo Russo, G.

Published
2024
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3. Abstract 4685: The identification of new therapeutic targets in mucinous ovarian carcinoma

Author

Petrella, S, Colombo, M, Marabese, M, Grasselli, C, Panfili, A, Craparotta, I, Barbera, M, Cassanmagnago, G, Bolis, M, Damia, G, Petrella, Serena, Colombo, Marika, Marabese, Mirko, Grasselli, Chiara, Panfili, Andrea, Craparotta, Ilaria, Barbera, Maria Chiara, Cassanmagnago, Giada Andrea, Bolis, Marco, Damia, Giovanna, Petrella, S, Colombo, M, Marabese, M, Grasselli, C, Panfili, A, Craparotta, I, Barbera, M, Cassanmagnago, G, Bolis, M, Damia, G, Petrella, Serena, Colombo, Marika, Marabese, Mirko, Grasselli, Chiara, Panfili, Andrea, Craparotta, Ilaria, Barbera, Maria Chiara, Cassanmagnago, Giada Andrea, Bolis, Marco, and Damia, Giovanna

Published
2024

7. Single-arm, open label prospective trial to assess prediction of the role of ERCC1/XPF complex in the response of advanced NSCLC patients to platinum-based chemotherapy

Author

Ganzinelli, M. Linardou, H. Alvisi, M.F. Caiola, E. Lo Russo, G. Cecere, F.L. Bettini, A.C. Psyrri, A. Milella, M. Rulli, E. Fabbri, A. De Maglie, M. Romanelli, P. Murray, S. Broggini, M. Marabese, M. Garassino, M.C.

Abstract

Background: Platinum-based therapy, combined or not with immune checkpoint inhibitors, represents a front-line choice for patients with non-small-cell lung cancer (NSCLC). Despite the improved outcomes in the last years for this malignancy, only a sub-group of patients have long-term benefit. Excision repair cross-complementation group 1 (ERCC1) has been considered a potential biomarker to predict the outcome of platinum-based chemotherapy in NSCLC. However, the ERCC1 gene is transcribed in four splice variants where the isoform 202 was described as the only one active and able to complex Xeroderma pigmentosum group F-complementing protein (XPF). Here, we prospectively investigated if the active form of ERCC1, as assessed by the ERCC1/XPF complex (ERCC1/XPF), could predict the sensitivity to platinum compounds. Patients and methods: Prospectively enrolled, patients with advanced NSCLC treated with a first-line regimen containing platinum were centrally evaluated for ERCC1/XPF by a proximity ligation assay. Overall survival (OS), progression-free survival (PFS) and objective response rate (ORR) were analyzed. Results: The absence of the ERCC1/XPF in the tumor suggested a trend of worst outcomes in terms of both OS [hazard ratio (HR) 1.41, 95% confidence interval (CI) 0.67-2.94, P = 0.373] and PFS (HR 1.61, 95% CI 0.88-3.03, P = 0.123). ORR was marginally influenced in ERCC1/XPF-negative and -positive groups [odds ratio (stable disease + progressive disease versus complete response + partial response) 0.87, 95% CI 0.25-3.07, P = 0.832]. Conclusion: The lack of ERCC1/XPF complex in NSCLC tumor cells might delineate a group of patients with poor outcomes when treated with platinum compounds. ERCC1/XPF absence might well identify patients for whom a different therapeutic approach could be necessary. © 2020 The Authors

Published
2021

9. Assessment of proportional hazard assumption in aggregate data: a systematic review on statistical methodology in clinical trials using time-to-event endpoint

Author

Rulli, E, Ghilotti, F, Biagioli, E, Porcu, L, Marabese, M, D'Incalci, M, Bellocco, R, Torri, V, Rulli E., Ghilotti F., Biagioli E., Porcu L., Marabese M., D'Incalci M., Bellocco R., Torri V., Rulli, E, Ghilotti, F, Biagioli, E, Porcu, L, Marabese, M, D'Incalci, M, Bellocco, R, Torri, V, Rulli E., Ghilotti F., Biagioli E., Porcu L., Marabese M., D'Incalci M., Bellocco R., and Torri V.

Abstract

Background: The evaluation of the proportional hazards (PH) assumption in survival analysis is an important issue when Hazard Ratio (HR) is chosen as summary measure. The aim is to assess the appropriateness of statistical methods based on the PH assumption in oncological trials. Methods: We selected 58 randomised controlled trials comparing at least two pharmacological treatments with a time-to-event as primary endpoint in advanced non-small-cell lung cancer. Data from Kaplan–Meier curves were used to calculate the relative hazard at each time point and the Restricted Mean Survival Time (RMST). The PH assumption was assessed with a fixed-effect meta-regression. Results: In 19% of the trials, there was evidence of non-PH. Comparison of treatments with different mechanisms of action was associated (P = 0.006) with violation of the PH assumption. In all the superiority trials where non-PH was detected, the conclusions using the RMST corresponded to that based on the Cox model, although the magnitude of the effect given by the HR was systematically greater than the one from the RMST ratio. Conclusion: As drugs with new mechanisms of action are being increasingly employed, particular attention should be paid on the statistical methods used to compare different types of agents.

Published
2018

10. Predicting the role of dna polymerase β alone or with kras mutations in advanced nsclc patients receiving platinum-based chemotherapy

Author

Alvisi, M.F. Ganzinelli, M. Linardou, H. Caiola, E. Russo, G.L. Cecere, F.L. Bettini, A.C. Psyrri, A. Milella, M. Rulli, E. Fabbri, A. De Maglie, M. Romanelli, P. Murray, S. Ndembe, G. Broggini, M. Garassino, M.C. Marabese, M.

Abstract

Clinical data suggest that only a subgroup of non-small cell lung cancer (NSCLC) patients has long-term benefits after front-line platinum-based therapy. We prospectively investigate whether KRAS status and DNA polymerase β expression could help identify patients responding to platinum compounds. Prospectively enrolled, advanced NSCLC patients treated with a first-line regimen containing platinum were genotyped for KRAS and centrally evaluated for DNA polymerase β expression. Overall survival (OS), progression-free survival (PFS), and the objective response rate (ORR) were recorded. Patients with KRAS mutations had worse OS (hazard ratio (HR): 1.37, 95% confidence interval (95% CI): 0.70–2.27). Negative DNA polymerase β staining identified a subgroup with worse OS than patients expressing the protein (HR: 1.43, 95% CI: 0.57–3.57). The addition of KRAS to the analyses further worsened the prognosis of patients with negative DNA polymerase β staining (HR: 1.67, 95% CI: 0.52–5.56). DNA polymerase β did not influence PFS and ORR. KRAS may have a negative role in platinum-based therapy responses in NSCLC, but its impact is limited. DNA polymerase β, when not expressed, might indicate a group of patients with poor outcomes. KRAS mutations in tumors not expressing DNA polymerase β further worsens survival. Therefore, these two biomarkers together might well identify patients for whom alternatives to platinum-based chemotherapy should be used. © 2020 by the authors. Licensee MDPI, Basel, Switzerland.

Published
2020

12. Oral Prolonged-Release Oxycodone-Naloxone: Analgesic Response, Safety Profile, and Factors Influencing the Response in Patients With Advanced Cancer

Author

Corli, O, Iorno, V, Legramandi, L, Rulli, E, Roberto, A, Azzarello, G, Schiavon, S, Cavanna, L, De Santis, S, Cartoni, C, Di Marco, P, Dauri, M, Mistretta, R, Bortolussi, R, Clerico, M, Pacchioni, M, Crispino, C, Marabese, M, Corsi, N, Natoli, S, Lipari, G, Luzi, M, Palumbo, G, and Trentin, L

Subjects
patients with cancer, Constipation, Analgesic, Irritability, Settore MED/06, 03 medical and health sciences, 0302 clinical medicine, 030202 anesthesiology, oxycodone-naloxone, Medicine, factors influencing the response, Adverse effect, Oxycodone/naloxone, business.industry, Cancer, analgesia, constipation, medicine.disease, Safety profile, Anesthesiology and Pain Medicine, Anesthesia, Settore MED/41, medicine.symptom, business, Cancer pain, 030217 neurology & neurosurgery
Abstract

Background Oxycodone-Naloxone (OXN) aims to reduce opioid-related constipation while being successfully analgesic. Methods We evaluated the analgesic response, prevalence, and severity of side effects in 176 cancer patients with moderate to severe pain and treated with OXN. Patients were followed for 28 days and evaluated every seven. Pain intensity, changes of therapy, and adverse drug reactions were recorded at each visit. The primary efficacy endpoint was the proportion of responders (≥30% reduction of pain intensity from baseline to final) and final average pain score ≤4 on a 0-10 scale. Results Average and worst pain intensity, and breakthrough pain (BTP) prevalence decreased over time and 81.3% of patients were responders. The starting daily dose of OXN was raised from 25.1±13.0 mg to 44.1±29.9 mg, and dose escalation >5%/day was observed in 19.4% of patients; 40.8-46.2% and 11.0-17.0% experienced any and severe grade of constipation during the follow-up visit, respectively. Digestive system tumor, thyroid endocrinopathies, psychological irritability, and BTP increased the risk of analgesic non-response. Conclusions OXN had strong analgesic effect in moderate to severe cancer pain patients: the safety profile is in line with the common adverse effects of opioids and severe constipation was uncommon. This article is protected by copyright. All rights reserved.

Published
2019

13. Oral prolonged-release Oxycodone-Naloxone: analgesic response, safety profile, and factors influencing the response in advanced cancer patients

Author

Corli, O, Iorno, V, Legramandi, L, Rulli, E, Roberto, A, Azzarello, G, Schiavon, S, Cavanna, L, De Santis, S, Cartoni, C, Di Marco, P, Dauri, M, Ristretta, R, Bortolussi, R, Clerico, M, Pacchioni, M, Crispino, C, Marabese, M, and Corsi, Nagc

Subjects
Oxycodone-Naloxone, analgesia, cancer patients, constipation, factors influencing the response, Settore MED/41 - Anestesiologia
Published
2019

14. The 5′UTR variant of ERCC5 fails to influence outcomes in ovarian and lung cancer patients undergoing treatment with platinum-based drugs

Author

Rulli, E, Guffanti, F, Caiola, E, Ganzinelli, M, Damia, G, Garassino, M, Piva, S, Ceppi, L, Broggini, M, Marabese, M, Rulli E., Guffanti F., Caiola E., Ganzinelli M., Damia G., Garassino M. C., Piva S., Ceppi L., Broggini M., Marabese M., Rulli, E, Guffanti, F, Caiola, E, Ganzinelli, M, Damia, G, Garassino, M, Piva, S, Ceppi, L, Broggini, M, Marabese, M, Rulli E., Guffanti F., Caiola E., Ganzinelli M., Damia G., Garassino M. C., Piva S., Ceppi L., Broggini M., and Marabese M.

Abstract

The common polymorphic variant in the 5′ untranslated region of the excision repair cross-complementation group 5 (ERCC5) gene was described to generate an upstream open reading frame that regulates both the basal ERCC5 expression and its ability to be synthesized following DNA damage. This variant was reported to affect response to platinum therapy in a cohort of patients with pediatric ependymoma. The role of this variant was investigated in two cohorts of cancer patients, specifically in non-small-cell lung cancer (NSCLC) patients (N = 137) and in epithelial ovarian carcinoma (EOC) patients (N = 240), treated in first-line with platinum-based compounds. Differently from what reported for pediatric ependymoma, the analysis of the polymorphism in NSCLC patients cohort was not able to detect any difference among patients harboring different genotypes both in progression free survival (HR = 0.93; 95%CI 0.64-1.33; p-value = 0.678) and overall survival (HR = 0.90; 95%CI 0.62-1.33; p-value = 0.625). These data were corroborated in a EOC patients cohort, where similar progression free survival (HR = 0.91; 95% CI 0.67-1.24; p-value = 0.561) and overall survival (HR = 0.98; 95% CI 0.71-1.35; p-value = 0.912) were found for the different genotypes. These data, obtained in appropriately sized populations, indicate that the effect of this ERCC5 polymorphism is likely to be relevant only in specific tumors.

Published
2016

15. Metformin +/- cyclic fasting mimicking diet in combination with platinum-pemetrexed chemotherapy for advanced LKB1 inactive lung adenocarcinoma: The FAME trial

Author

Galli, G., primary, Signorelli, D., additional, Vernieri, C., additional, Ganzinelli, M., additional, Moro, M., additional, Fabbri, A., additional, Tamborini, E., additional, Marabese, M., additional, Caiola, E., additional, Broggini, M., additional, Hollander, L., additional, Gallucci, R., additional, Gavazzi, C., additional, Rizzo, A.M., additional, Corsetto, P., additional, Pruneri, G., additional, de Braud, F., additional, Sozzi, G., additional, Torri, V., additional, and Garassino, M.C., additional

Published
2019
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18. KRas-LCS6 polymorphism does not impact on outcomes in ovarian cancer

Author

Caiola, E, Rulli, E, Fruscio, R, Buda, A, Broggini, M, Marabese, M, FRUSCIO, ROBERT, BUDA, ALESSANDRO ANTONIO, Marabese, M., Caiola, E, Rulli, E, Fruscio, R, Buda, A, Broggini, M, Marabese, M, FRUSCIO, ROBERT, BUDA, ALESSANDRO ANTONIO, and Marabese, M.

Abstract

Epithelial ovarian cancer is a malignancy with high rate of death due to an advanced disease at diagnosis and frequent relapse after chemotherapy. Nowadays, there is a lack of knowledge for clear risk factors and predictive and/or prognostic genetic markers although genomic alterations such as mutations in p53, PTEN, BRCA1/BRCA2, HER2, KRAS and PI3K genes have been associated to this pathology. A genomic variant in the 3' untraslated region of cancer related gene KRAS, is able to disrupt the let-7 miRNA binding site. The SNP, commonly named KRAS-LCS6, determines the substitution of the more abundant T-allele to a G-allele which was observed to increase the KRAS expression and in turn to activate the downstream pathway at higher levels if compared to the T-allele. In this study we assessed the role of the KRAS-LCS6 polymorphism (rs61764370) in 97 early (stages I and II) and 232 advanced (stages III and IV) ovarian cancer patients in order to associate this SNP to any physiopathological characteristic of the patients cohort, including progression free survival and overall survival, with a follow up data longer than ten years. Our data indicate that KRAS-LCS6 polymorphism is not relevant in ovarian cancer, in fact, in our cohort of patients, is not associated to any outcome or physiopathological characteristic.

Published
2012

19. 'Incidence of different KRAS mutation in non-small cell lung cancer (NSCLC) patients, TAILOR STUDY

Author

Martelli,O, Rulli,E, Bettini,A, Farina,G, Longo,F, Moscetti,L, Pavese,I, Alabiso,O, Bertolini,A, Tomirotti,M, Farris,A, Veronese,S, Ferrari,V, Marsoni,S, Lauricella,C, Ganzinelli,M, Broggini,M, Marabese,M, Floriani,I, Copreni,E, Pellegrino,A, Ardizzoia,A, Gherardi,G, Bianchi,F, Scanni,A, Garassino,MC, PALMERI, Sergio, Martelli,O, Rulli,E, Bettini,A, Farina,G, Longo,F, Moscetti,L, Pavese,I, Alabiso,O, Bertolini,A, Tomirotti,M, Farris,A, Veronese,S, Ferrari,V, Marsoni,S, Lauricella,C, Ganzinelli,M, Broggini,M, Marabese,M, Floriani,I, Copreni,E, Pellegrino,A, Ardizzoia,A, Palmeri,S, Gherardi,G, Bianchi,F, Scanni,A, and Garassino,MC

Subjects
non-small cell lung cancer,TAILOR,kras
Published
2011

25. DeltaNp63 expression is associated with poor survival in ovarian cancer

Author

Marchini, S, Marabese, M, Marrazzo, E, Mariani, P, Cattaneo, D, Fossati, R, Compagnoni, A, Fruscio, R, Lissoni, A, Broggini, M, Broggini, M., FRUSCIO, ROBERT, LISSONI, ANDREA ALBERTO, Marchini, S, Marabese, M, Marrazzo, E, Mariani, P, Cattaneo, D, Fossati, R, Compagnoni, A, Fruscio, R, Lissoni, A, Broggini, M, Broggini, M., FRUSCIO, ROBERT, and LISSONI, ANDREA ALBERTO

Abstract

P63 belongs to the 'p53 family' whose role in cancer progression has been recently revisited in light of the plethora of splicing variants that are generated. We analyzed the expression of the full-length TAp63 gene and its dominant-negative form deltaNp63 in ovarian cancer biopsies to correlate their expression with clinical outcome.

Published
2008

26. Combination of trabectedin and irinotecan is highly effective in a human rhabomyosarcoma xenografts.

Author

Riccardi, Anna Shirley, Meco, Daniela, Ubezio, Paolo, Mazzarella, Giorgio, Marabese, M, Faircloth, Gt, Jimeno, José, D'Incalci, Maurizio, Riccardi, Riccardo, Riccardi, Riccardo (ORCID:0000-0001-7515-6622), Riccardi, Anna Shirley, Meco, Daniela, Ubezio, Paolo, Mazzarella, Giorgio, Marabese, M, Faircloth, Gt, Jimeno, José, D'Incalci, Maurizio, Riccardi, Riccardo, and Riccardi, Riccardo (ORCID:0000-0001-7515-6622)

Abstract

Our objective was to evaluate in vitro and in vivo the effect of the combination of trabectedin (Yondelis, ET-743) and irinotecan (CPT-11) or its major metabolite SN-38 in a human rhabdomyosarcoma cell line. The schedule trabectedin (1 h) followed by irinotecan or SN-38 (24 h) and the opposite sequence (irinotecan or SN-38 24 h followed by trabectedin 1 h) were analyzed in a rhabdomyosarcoma cell line. In vivo studies were conducted with trabectedin and irinotecan at the doses of 0.2 and 20 mg/kg, respectively, simultaneously administered with a q4d x 3 schedule. In vitro studies indicated an overall additive effect [combination index (CI) relatively close to 1.0], with the former schedule slightly superior to the latter (at the IC50 effect levels: CI=0.89 versus 1.07). Neither transcription nor expression of DNA topoisomerase I was affected by trabectedin treatment. In vivo the therapeutic results of the combination were certainly more impressive: trabectedin and irinotecan combination caused a strong and long-lasting effect on tumor growth (tumor volume inhibition=89%, log10 cell kill=1.6), whereas each drug given as a single agent was only marginally active. The discrepancy between the in vitro and in vivo results suggests possible mechanisms involving host cells, other than tumor cells. The striking effects of the combination observed in vivo could be related to a combination of a direct cytotoxic and an anti-inflammatory indirect effect. The very marked and long-lasting effect of the trabectedin and irinotecan combination in vivo suggests a basis for a clinical evaluation in pediatric patients with rhabdomyosarcoma.

Published
2005

28. Diagnostics

Author

Einert, T. R., primary, Schmidt, G., additional, Binnig, G., additional, Balacescu, O., additional, Balacescu, L., additional, Rus, M., additional, Buiga, R., additional, Tudoran, O., additional, Todor, N., additional, Nagy, V., additional, Irimie, A., additional, Neagoe, I., additional, Yacobi, R., additional, Ustaev, E., additional, Berger, R. R., additional, Barshack, I., additional, Kaur, K., additional, Henderson, S., additional, Cutts, A., additional, Domingo, E., additional, Woods, J., additional, Motley, C., additional, Dougherty, B., additional, Middleton, M., additional, Hassan, B., additional, Wang, Y., additional, Beasley, E., additional, Naley, M., additional, Schuh, A., additional, Tomlinson, I., additional, Taylor, J., additional, Planchard, D., additional, Lueza, B., additional, Rahal, A., additional, Lacroix, L., additional, Ngocamus, M., additional, Auger, N., additional, Saulnier, P., additional, Dorfmuller, P., additional, Le Chevalier, T., additional, Celebic, A., additional, Pignon, J. P., additional, Soria, J. C., additional, Besse, B., additional, Sun, Y. H., additional, Wang, R., additional, Li, C. G., additional, Pan, Y. J., additional, Chen, H. Q., additional, Chouchane, L., additional, Shan, J., additional, Kizhakayil, D., additional, Aigha, I., additional, Dsouza, S., additional, Noureddine, B., additional, Gabbouj, S., additional, Mathew, R., additional, Hassen, E., additional, Shan, S., additional, al-Rumaihi, K., additional, al-Bozom, I., additional, al-Said, S., additional, Rabah, D., additional, Farhat, K., additional, Jakobsen Falk, I. A., additional, Green, K. H. Z., additional, Lotfi, K., additional, Fyrberg, A., additional, Pejovic, T., additional, Li, H., additional, Mhawech-Fauceglia, P., additional, Hoatlin, M., additional, Guo, M. G., additional, Huang, M., additional, Ge, Y., additional, Hess, K., additional, Wei, C., additional, Zhang, W., additional, Bogush, T. A., additional, Dudko, E. A., additional, Nureev, M. V., additional, Kamensky, A. A., additional, Polotsky, B. E., additional, Tjulandin, S. A., additional, Davydov, M. I., additional, Caballero, M., additional, Hasmats, J., additional, Green, H., additional, Quanz, M., additional, Buhler, C., additional, Sun, J. S., additional, Dutreix, M., additional, Cebotaru, C. L., additional, Placintar, A. N., additional, Ghilezan, N., additional, Balogh, Z. B., additional, Reiniger, L., additional, Rajnai, H., additional, Csomor, J., additional, Szepesi, A., additional, Balogh, A., additional, Deak, L., additional, Gagyi, E., additional, Bodor, C., additional, Matolcsy, A., additional, Bozhenko, V. K., additional, Rozhkova, N. I., additional, Kudinova, E. A., additional, Bliznyukov, O. P., additional, Vaskevich, E. N., additional, Trotsenko, I. D., additional, Kharchenko, N. V., additional, Kiandarian, I. V., additional, Pulito, C., additional, Terrenato, I., additional, Sacconi, A., additional, Biagioni, F., additional, Mottolese, M., additional, Blandino, G., additional, Muti, P., additional, Falvo, E., additional, Strano, S., additional, Mori, F., additional, Ganci, F., additional, Covello, R., additional, Zoccali, C., additional, Biagini, R., additional, Palmer, G. A., additional, Wegdam, W., additional, Meijer, D., additional, Kramer, G., additional, Langridge, J., additional, Moerland, P. D., additional, de Jong, S. M., additional, Vissers, J. P., additional, Kenter, G. G., additional, Buist, M. R., additional, Aerts, J. M. F. G., additional, Milione, M., additional, de Braud, F., additional, Buzzoni, R., additional, Pusceddu, S., additional, Mazzaferro, V., additional, Damato, A., additional, Pelosi, G., additional, Garassino, M., additional, Broggini, M., additional, Marabese, M., additional, Veronese, S., additional, Ganzinelli, M., additional, Martelli, O., additional, Bossel, N., additional, Fontemaggi, G., additional, Manciocco, V., additional, Sperduti, I., additional, Strigari, L., additional, Spriano, G., additional, Domany, E., additional, Donzelli, S., additional, Bellissimo, T., additional, Alessandrini, G., additional, Carosi, M. A., additional, Pescarmona, E., additional, Facciolo, F., additional, Telera, S., additional, Pompili, A., additional, de Vriendt, V., additional, de Roock, W., additional, di Narzo, A. F., additional, Tian, S., additional, Biesmans, B., additional, Jacobs, B., additional, de Schutter, J., additional, Budzinska, E., additional, Sagaert, X., additional, Delorenzi, M., additional, Simon, I., additional, Tejpar, S., additional, Zhu, Y., additional, Wang, H. K., additional, Ye, D. W., additional, Denisov, E., additional, Tsyganov, M., additional, Tashireva, L., additional, Zavyalova, M., additional, Perelmuter, V., additional, Cherdyntseva, N., additional, Kim, Y. C., additional, Jang, T., additional, Oh, I. J., additional, Kim, K. S., additional, Ban, H., additional, Na, K. J., additional, Ahn, S. J., additional, Kang, H., additional, Kim, W. J., additional, Park, C., additional, Abousamra, N. K., additional, El-Din, M. S., additional, and Azmy, E. A., additional

Published
2012
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35. KRas-LCS6 polymorphism does not impact on outcomes in ovarian cancer

Author

Caiola E, Eliana Rulli, Fruscio R, Buda A, Broggini M, Marabese M, Caiola, E, Rulli, E, Fruscio, R, Buda, A, Broggini, M, and Marabese, M

Subjects
endocrine system diseases, MED/40 - GINECOLOGIA E OSTETRICIA, KRAS, let-7, ovarian cancer, LCS6, miRNA, rs61764370, Original Article, neoplasms
Abstract

Epithelial ovarian cancer is a malignancy with high rate of death due to an advanced disease at diagnosis and frequent relapse after chemotherapy. Nowadays, there is a lack of knowledge for clear risk factors and predictive and/or prognostic genetic markers although genomic alterations such as mutations in p53, PTEN, BRCA1/BRCA2, HER2, KRAS and PI3K genes have been associated to this pathology. A genomic variant in the 3’ untraslated region of cancer related gene KRAS, is able to disrupt the let-7 miRNA binding site. The SNP, commonly named KRAS-LCS6, determines the substitution of the more abundant T-allele to a G-allele which was observed to increase the KRAS expression and in turn to activate the downstream pathway at higher levels if compared to the T-allele. In this study we assessed the role of the KRAS-LCS6 polymorphism (rs61764370) in 97 early (stages I and II) and 232 advanced (stages III and IV) ovarian cancer patients in order to associate this SNP to any physiopathological characteristic of the patients cohort, including progression free survival and overall survival, with a follow up data longer than ten years. Our data indicate that KRAS-LCS6 polymorphism is not relevant in ovarian cancer, in fact, in our cohort of patients, is not associated to any outcome or physiopathological characteristic.

36. P73a overexpression is associated with resistance to treatment with DNA-damaging agents in a human ovarian cancer cell line

Author

Vikhanskaya F, Marchini S, Marabese M, Galliera E, and MASSIMO BROGGINI

Subjects
Ovarian Neoplasms, DNA Repair, Ultraviolet Rays, Gene Expression Profiling, Tumor Suppressor Proteins, Gene Expression, Nuclear Proteins, Tumor Protein p73, Transfection, Clone Cells, DNA-Binding Proteins, Gene Expression Regulation, Neoplastic, Drug Resistance, Neoplasm, Tumor Cells, Cultured, Humans, Female, Genes, Tumor Suppressor, RNA, Messenger, Cisplatin, Tumor Suppressor Protein p53, Topotecan, Cell Division, DNA Damage
Abstract

We examined the consequences of p73alpha overexpression on gene expression and cellular response to anticancer agents in clones from the human ovarian cancer cell line A2780. Using microarray filters, the expression of 588 genes in two clones overexpressing p73alpha (A2780/p73.4 and A2780/ p73.5) in comparison with empty vector-transfected cells was evaluated. There were clear differences in gene expression profiles. Both of the clones showed a marked increase in the expression of genes involved in DNA repair, including genes participating in nucleotide excision repair and mismatch repair. This was confirmed by reverse transcription-PCR and Northern blot analysis and was associated with an increase in the ability of p73alpha-expressing clones to repair two different DDP (cis-dichlorodiammine platinum)-damaged plasmids in a host reactivation assay. p73alpha overexpressing clones were less sensitive than parental cells to alkylating agents treatment or UV radiation but equally sensitive to the topoisomerase I inhibitor topotecan, which indicated that the increase in expression of DNA repair genes has implications for the response to DNA damaging agents.

37. Assessment of proportional hazard assumption in aggregate data: a systematic review on statistical methodology in clinical trials using time-to-event endpoint

Author

Maurizio D'Incalci, Elena Biagioli, Eliana Rulli, Luca Porcu, Rino Bellocco, Francesca Ghilotti, Mirko Marabese, Valter Torri, Rulli, E, Ghilotti, F, Biagioli, E, Porcu, L, Marabese, M, D'Incalci, M, Bellocco, R, and Torri, V

Subjects
Cancer Research, Lung Neoplasms, Article, 03 medical and health sciences, 0302 clinical medicine, Carcinoma, Non-Small-Cell Lung, Statistics, Clinical endpoint, Medicine, Humans, 030212 general & internal medicine, Time point, Survival analysis, Event (probability theory), Proportional Hazards Models, Randomized Controlled Trials as Topic, Proportional hazards model, business.industry, Hazard ratio, Lung Neoplasm, Clinical trial, Oncology, 030220 oncology & carcinogenesis, RMST, Proportional Hazards Model, Randomized controlled trials, business, Non-small-cell lung cancer, Human
Abstract

Background: The evaluation of the proportional hazards (PH) assumption in survival analysis is an important issue when Hazard Ratio (HR) is chosen as summary measure. The aim is to assess the appropriateness of statistical methods based on the PH assumption in oncological trials. Methods: We selected 58 randomised controlled trials comparing at least two pharmacological treatments with a time-to-event as primary endpoint in advanced non-small-cell lung cancer. Data from Kaplan–Meier curves were used to calculate the relative hazard at each time point and the Restricted Mean Survival Time (RMST). The PH assumption was assessed with a fixed-effect meta-regression. Results: In 19% of the trials, there was evidence of non-PH. Comparison of treatments with different mechanisms of action was associated (P = 0.006) with violation of the PH assumption. In all the superiority trials where non-PH was detected, the conclusions using the RMST corresponded to that based on the Cox model, although the magnitude of the effect given by the HR was systematically greater than the one from the RMST ratio. Conclusion: As drugs with new mechanisms of action are being increasingly employed, particular attention should be paid on the statistical methods used to compare different types of agents.

Published
2018

38. The 5′UTR variant of ERCC5 fails to influence outcomes in ovarian and lung cancer patients undergoing treatment with platinum-based drugs

Author

Federica Guffanti, Giovanna Damia, Massimo Broggini, Marina Chiara Garassino, Lorenzo Ceppi, Eliana Rulli, Sheila Piva, Monica Ganzinelli, Elisa Caiola, Mirko Marabese, Rulli, E, Guffanti, F, Caiola, E, Ganzinelli, M, Damia, G, Garassino, M, Piva, S, Ceppi, L, Broggini, M, and Marabese, M

Subjects
0301 basic medicine, Oncology, Untranslated region, Male, Lung Neoplasms, Pharmacogenomic Variants, Five prime untranslated region, Transcription Factor, Carcinoma, Ovarian Epithelial, Antineoplastic Agent, 0302 clinical medicine, 5' Untranslated Region, Carcinoma, Non-Small-Cell Lung, Genotype, Pediatric ependymoma, Neoplasms, Glandular and Epithelial, Nuclear Protein, Ovarian Neoplasms, Multidisciplinary, Nuclear Proteins, Middle Aged, DNA-Binding Proteins, Treatment Outcome, Pharmacogenomic Variant, 030220 oncology & carcinogenesis, Cohort, Female, Survival Analysi, Human, medicine.medical_specialty, DNA-Binding Protein, Antineoplastic Agents, Article, 03 medical and health sciences, Internal medicine, medicine, Humans, Progression-free survival, Endonuclease, Lung cancer, Survival analysis, Aged, Platinum, Polymorphism, Genetic, business.industry, Ovarian Neoplasm, Endonucleases, medicine.disease, Survival Analysis, Lung Neoplasm, 030104 developmental biology, 5' Untranslated Regions, business, Transcription Factors
Abstract

The common polymorphic variant in the 5′ untranslated region of the excision repair cross-complementation group 5 (ERCC5) gene was described to generate an upstream open reading frame that regulates both the basal ERCC5 expression and its ability to be synthesized following DNA damage. This variant was reported to affect response to platinum therapy in a cohort of patients with pediatric ependymoma. The role of this variant was investigated in two cohorts of cancer patients, specifically in non-small-cell lung cancer (NSCLC) patients (N = 137) and in epithelial ovarian carcinoma (EOC) patients (N = 240), treated in first-line with platinum-based compounds. Differently from what reported for pediatric ependymoma, the analysis of the polymorphism in NSCLC patients cohort was not able to detect any difference among patients harboring different genotypes both in progression free survival (HR = 0.93; 95%CI 0.64–1.33; p-value = 0.678) and overall survival (HR = 0.90; 95%CI 0.62–1.33; p-value = 0.625). These data were corroborated in a EOC patients cohort, where similar progression free survival (HR = 0.91; 95% CI 0.67–1.24; p-value = 0.561) and overall survival (HR = 0.98; 95% CI 0.71–1.35; p-value = 0.912) were found for the different genotypes. These data, obtained in appropriately sized populations, indicate that the effect of this ERCC5 polymorphism is likely to be relevant only in specific tumors.

Published
2016

39. 188TiP Metformin +/- cyclic fasting mimicking diet in combination with platinum-pemetrexed chemotherapy for advanced LKB1 inactive lung adenocarcinoma: The FAME trial.

Author

Galli, G, Signorelli, D, Vernieri, C, Ganzinelli, M, Moro, M, Fabbri, A, Tamborini, E, Marabese, M, Caiola, E, Broggini, M, Hollander, L, Gallucci, R, Gavazzi, C, Rizzo, A M, Corsetto, P, Pruneri, G, Braud, F de, Sozzi, G, Torri, V, and Garassino, M C

Subjects
*COMBINATION drug therapy, *FASTING, *LUNGS, *METFORMIN, *ADENOCARCINOMA
Published
2019
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40. DNA-damage response gene polymorphisms and therapeutic outcomes in ovarian cancer

Author

Rodolfo Milani, Luca Porcu, Mirko Marabese, Massimo Broggini, Elisa Caiola, Robert Fruscio, Daniela Giuliani, Torri, Caiola, E, Porcu, L, Fruscio, R, Giuliani, D, Milani, R, Torri, V, Broggini, M, and Marabese, M

Subjects
mdm2, Oncology, Adult, medicine.medical_specialty, DNA Repair, MED/40 - GINECOLOGIA E OSTETRICIA, SNP, ercc5/xpg, Biomarkers, Pharmacological, Disease-Free Survival, polymorphism, Internal medicine, Genotype, Genetics, medicine, Humans, Genetic variability, Promoter Regions, Genetic, Genotyping, Gene, Genetic Association Studies, Aged, Platinum, Pharmacology, Aged, 80 and over, Ovarian Neoplasms, Polymorphism, Genetic, biology, Nuclear Proteins, ercc1, Proto-Oncogene Proteins c-mdm2, Middle Aged, medicine.disease, Endonucleases, Prognosis, DNA-Binding Proteins, ovarian cancer, Treatment Outcome, biology.protein, Cancer research, Molecular Medicine, Mdm2, Female, ERCC1, Ovarian cancer, DNA Damage, Transcription Factors
Abstract

Epithelial ovarian cancer has a poor prognosis owing to late diagnosis and frequent relapse after first-line therapy. Analysis of individual genetic variability could aid in the identification of markers, which could help in stratifying patients with the aim of optimizing individual therapy. In this study we assessed polymorphisms in three genes important in drugs' response in 97 early and 235 late-stage ovarian cancer patients. The Asp1104His polymorphism in xpg, a gene important for removal of platinum adducts, was associated with progression-free survival in early- and late-stage ovarian cancer. Our data indicate that a simple diagnostic analysis such as xpg genotyping can help in predicting response, and extension to other possibly relevant genotypes could be useful in selecting patients with epithelial ovarian cancer for optimal therapy and hence increase the chance of response.

Published
2011

41. DeltaNp63 expression is associated with poor survival in ovarian cancer

Author

S. Marchini, Dario Cattaneo, Anna Compagnoni, Pietro Mariani, Roldano Fossati, Mirko Marabese, Robert Fruscio, A. A. Lissoni, Massimo Broggini, Eleonora Marrazzo, Marchini, S, Marabese, M, Marrazzo, E, Mariani, P, Cattaneo, D, Fossati, R, Compagnoni, A, Fruscio, R, Lissoni, A, and Broggini, M

Subjects
Oncology, medicine.medical_specialty, Pathology, Tumor suppressor gene, Transcription Factor, DNA-Binding Protein, Biopsy, Malignancy, Internal medicine, medicine, Biomarkers, Tumor, Humans, Stage (cooking), Survival analysis, Neoplasm Staging, Stage III Ovarian Cancer, Ovarian Neoplasms, Tumor Suppressor Protein, business.industry, Tumor Suppressor Proteins, Ovarian Neoplasm, Cancer, Hematology, Middle Aged, medicine.disease, Survival Analysis, DNA-Binding Proteins, Tumor progression, Tumor Markers, Biological, Mutation, Disease Progression, Trans-Activators, Female, Survival Analysi, Ovarian cancer, business, Transcription Factors, Human
Abstract

Background P63 belongs to the 'p53 family' whose role in cancer progression has been recently revisited in light of the plethora of splicing variants that are generated. We analyzed the expression of the full-length TAp63 gene and its dominant-negative form deltaNp63 in ovarian cancer biopsies to correlate their expression with clinical outcome. Materials and methods Real-time RT-PCR analysis was used to determine the levels of TAp63 and deltaNp63 in 83 stage I and in 86 stage III ovarian cancer biopsies and in seven human ovarian cancer cell. Results TAp63 levels were comparable in stage I and stage III, but deltaNp63 levels increased 77-fold in stage III, independently of the p53 status. Patients with high deltaNp63 expression had the worst overall survival (OS); patients with a deltaNp63/TAp63 ratio >2 had a poor OS. Patients with a high deltaNp63/TAp63 ratio were those with a poor response to platinum-based therapy. Conclusions Data indicate a role for deltaNp63 as a potential biomarker to predict patient's outcome and tumor progression in ovarian cancer. This would have particularly clinical relevance in ovarian cancer where the high rate of mortality reflects our lack of knowledge of molecular mechanisms underlying cell progression toward malignancy.

Published
2008

42. Caloric restriction and metformin selectively improved LKB1-mutated NSCLC tumor response to chemo- and chemo-immunotherapy.

Author

Ndembe G, Intini I, Moro M, Grasselli C, Panfili A, Panini N, Bleve A, Occhipinti M, Borzi C, Garassino MC, Marabese M, Canesi S, Scanziani E, Sozzi G, Broggini M, and Ganzinelli M

Subjects
Humans, Mice, Animals, Caloric Restriction, Proto-Oncogene Proteins p21(ras) genetics, Protein Serine-Threonine Kinases genetics, Protein Serine-Threonine Kinases metabolism, Mice, Transgenic, Immunotherapy, Mutation, Tumor Microenvironment, Metformin, Lung Neoplasms drug therapy, Lung Neoplasms genetics, Lung Neoplasms pathology, Carcinoma, Non-Small-Cell Lung drug therapy, Carcinoma, Non-Small-Cell Lung genetics
Abstract

Background: About 10% of NSCLCs are mutated in KRAS and impaired in STK11/LKB1, a genetic background associated with poor prognosis, caused by an increase in metastatic burden and resistance to standard therapy. LKB1 is a protein involved in a number of biological processes and is particularly important for its role in the regulation of cell metabolism. LKB1 alterations lead to protein loss that causes mitochondria and metabolic dysfunction that makes cells unable to respond to metabolic stress. Different studies have shown how it is possible to interfere with cancer metabolism using metformin and caloric restriction (CR) and both modify the tumor microenvironment (TME), stimulating the switch from "cold" to "hot". Given the poor therapeutic response of KRAS mut /LKB1 mut patients, and the role of LKB1 in cell metabolism, we examined whether the addition of metformin and CR enhanced the response to chemo or chemo-immunotherapy in LKB1 impaired tumors., Methods: Mouse cell lines were derived from lung nodules of transgenic mice carrying KRAS G12D with either functional LKB1 (KRAS G12D /LKB1 wt ) or mutated LKB1 (KRAS G12D /LKB1 mut ). Once stabilized in vitro, these cell lines were inoculated subcutaneously and intramuscularly into immunocompetent mice. Additionally, a patient-derived xenograft (PDX) model was established by directly implanting tumor fragments from patient into immunocompromised mice. The mice bearing these tumor models were subjected to treatment with chemotherapy or chemo-immunotherapy, both as standalone regimens and in combination with metformin and CR., Results: Our preclinical results indicate that in NSCLC KRAS mut /LKB1 mut tumors, metformin and CR do enhance the response to chemo and chemo-immunotherapy, inducing a metabolic stress condition that these tumors are not able to overcome. Analysis of immune infiltrating cells did not bring to light any strong correlation between the TME immune-modulation and the tumor response to metformin and CR., Conclusion: Our in vitro and in vivo preliminary studies confirm our hypothesis that the addition of metformin and CR is able to improve the antitumor activity of chemo and chemoimmunotherapy in LKB1 impaired tumors, exploiting their inability to overcome metabolic stress., (© 2023. The Author(s).)

Published
2024
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43. Isolation and characterization of two newly established thymoma PDXs from two relapses of the same patient: a new tool to investigate thymic malignancies.

Author

Mendogni P, Affatato R, Cabri E, Chiappa M, Ndembe G, Tosi D, Del Gobbo A, Fratelli M, Pardini E, Petrini I, Rosso L, Broggini M, and Marabese M

Subjects
Animals, Humans, Neoplasm Recurrence, Local genetics, Disease Models, Animal, Thymoma drug therapy, Thymoma genetics, Thymus Neoplasms drug therapy, Thymus Neoplasms genetics, Neoplasms, Glandular and Epithelial
Abstract

Background: Thymic malignancies are a heterogeneous group of rare cancers for which systemic chemotherapy is the standard treatment in the setting of advanced, recurrent or refractory diseases. Both environmental and genetic risk factors have not been fully clarified and few target-specific drugs have been developed for thymic epithelial tumors. A major challenge in studying thymic epithelial tumors is the lack of preclinical models for translational studies., Main Body: Starting from bioptic material of two consecutive recurrences of the same patient, we generated two patient-derived xenografts. The patient-derived xenografts models were characterized for histology by immunohistochemistry and mutations using next-generation sequencing. When compared to the original tumors resected from the patient, the two patient-derived xenografts had preserved morphology after the stain with hematoxylin and eosin, although there was a moderate degree of de-differentiation. From a molecular point of view, the two patient-derived xenografts maintained 74.3 and 61.8% of the mutations present in the human tumor of origin., Short Conclusion: The newly generated patient-derived xenografts recapitulate both the molecular characteristics and the evolution of the thymoma it derives from well, allowing to address open questions for this rare cancer., (© 2022. The Author(s).)

Published
2022
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44. NSCLC Cells Resistance to PI3K/mTOR Inhibitors Is Mediated by Delta-6 Fatty Acid Desaturase (FADS2).

Author

Colombo M, Passarelli F, Corsetto PA, Rizzo AM, Marabese M, De Simone G, Pastorelli R, Broggini M, Brunelli L, and Caiola E

Subjects
Humans, Cell Proliferation, Drug Resistance, Neoplasm, Phosphatidylinositol 3-Kinases metabolism, Proto-Oncogene Proteins c-akt metabolism, Signal Transduction, TOR Serine-Threonine Kinases metabolism, Carcinoma, Non-Small-Cell Lung drug therapy, Carcinoma, Non-Small-Cell Lung metabolism, Fatty Acid Desaturases metabolism, Lung Neoplasms drug therapy, Lung Neoplasms metabolism, MTOR Inhibitors pharmacology, Phosphoinositide-3 Kinase Inhibitors pharmacology
Abstract

Hyperactivation of the phosphatidylinositol-3-kinase (PI3K) pathway is one of the most common events in human cancers. Several efforts have been made toward the identification of selective PI3K pathway inhibitors. However, the success of these molecules has been partially limited due to unexpected toxicities, the selection of potentially responsive patients, and intrinsic resistance to treatments. Metabolic alterations are intimately linked to drug resistance; altered metabolic pathways can help cancer cells adapt to continuous drug exposure and develop resistant phenotypes. Here we report the metabolic alterations underlying the non-small cell lung cancer (NSCLC) cell lines resistant to the usual PI3K-mTOR inhibitor BEZ235. In this study, we identified that an increased unsaturation degree of lipid species is associated with increased plasma membrane fluidity in cells with the resistant phenotype and that fatty acid desaturase FADS2 mediates the acquisition of chemoresistance. Therefore, new studies focused on reversing drug resistance based on membrane lipid modifications should consider the contribution of desaturase activity.

Published
2022
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45. LKB1: Can We Target an Hidden Target? Focus on NSCLC.

Author

Ndembe G, Intini I, Perin E, Marabese M, Caiola E, Mendogni P, Rosso L, Broggini M, and Colombo M

Abstract

LKB1 (liver kinase B1) is a master regulator of several processes such as metabolism, proliferation, cell polarity and immunity. About one third of non-small cell lung cancers (NSCLCs) present LKB1 alterations, which almost invariably lead to protein loss, resulting in the absence of a potential druggable target. In addition, LKB1-null tumors are very aggressive and resistant to chemotherapy, targeted therapies and immune checkpoint inhibitors (ICIs). In this review, we report and comment strategies that exploit peculiar co-vulnerabilities to effectively treat this subgroup of NSCLCs. LKB1 loss leads to an enhanced metabolic avidity, and treatments inducing metabolic stress were successful in inhibiting tumor growth in several preclinical models. Biguanides, by compromising mitochondria and reducing systemic glucose availability, and the glutaminase inhibitor telaglenastat (CB-839), inhibiting glutamate production and reducing carbon intermediates essential for TCA cycle progression, have provided the most interesting results and entered different clinical trials enrolling also LKB1-null NSCLC patients. Nutrient deprivation has been investigated as an alternative therapeutic intervention, giving rise to interesting results exploitable to design specific dietetic regimens able to counteract cancer progression. Other strategies aimed at targeting LKB1-null NSCLCs exploit its pivotal role in modulating cell proliferation and cell invasion. Several inhibitors of LKB1 downstream proteins, such as mTOR, MEK, ERK and SRK/FAK, resulted specifically active on LKB1 -mutated preclinical models and, being molecules already in clinical experimentation, could be soon proposed as a specific therapy for these patients. In particular, the rational use in combination of these inhibitors represents a very promising strategy to prevent the activation of collateral pathways and possibly avoid the potential emergence of resistance to these drugs. LKB1-null phenotype has been correlated to ICIs resistance but several studies have already proposed the mechanisms involved and potential interventions. Interestingly, emerging data highlighted that LKB1 alterations represent positive determinants to the new KRAS specific inhibitors response in KRAS co-mutated NSCLCs. In conclusion, the absence of the target did not block the development of treatments able to hit LKB1 -mutated NSCLCs acting on several fronts. This will give patients a concrete chance to finally benefit from an effective therapy., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2022 Ndembe, Intini, Perin, Marabese, Caiola, Mendogni, Rosso, Broggini and Colombo.)

Published
2022
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46. LKB1 Down-Modulation by miR-17 Identifies Patients With NSCLC Having Worse Prognosis Eligible for Energy-Stress-Based Treatments.

Author

Borzi C, Ganzinelli M, Caiola E, Colombo M, Centonze G, Boeri M, Signorelli D, Caleca L, Rulli E, Busico A, Capone I, Pastorino U, Marabese M, Milione M, Broggini M, Garassino MC, Sozzi G, and Moro M

Subjects
Cell Line, Tumor, Cell Proliferation, Gene Expression Regulation, Neoplastic, Humans, Prognosis, Protein Serine-Threonine Kinases genetics, Protein Serine-Threonine Kinases metabolism, Retrospective Studies, Lung Neoplasms drug therapy, Lung Neoplasms genetics, MicroRNAs genetics
Abstract

Introduction: Preclinical models recently unveiled the vulnerability of LKB1/KRAS comutated NSCLC to metabolic stress-based treatments. Because miR-17 is a potential epigenetic regulator of LKB1, we hypothesized that wild-type LKB1 (LKB1 WT ) NSCLC with high miR-17 expression may be sensitive to an energetic stress condition, and eligible for metabolic frailties-based therapeutic intervention., Methods: We took advantage of NSCLC cell lines with different combinations of KRAS mutation and LKB1 deletion and of patient-derived xenografts (PDXs) with high (LKB1 WT /miR-17 high) or low (LKB1 WT /miR-17 low) miR-17 expression. We evaluated LKB1 pathway impairment and apoptotic response to metformin. We retrospectively evaluated LKB1 and miR-17 expression levels in tissue specimens of patients with NSCLC and PDXs. In addition, a lung cancer series from The Cancer Genome Atlas data set was analyzed for miR-17 expression and potential correlation with clinical features., Results: We identified miR-17 as an epigenetic regulator of LKB1 in NSCLC and confirmed targeting of miR-17 to LKB1 3' untranslated region by luciferase reporter assay. We found that miR-17 overexpression functionally impairs the LKB1/AMPK pathway. Metformin treatment prompted apoptosis on miR-17 overexpression only in LKB1 WT cell lines, and in LKB1 WT /miR-17 high PDXs. A retrospective analysis in patients with NSCLC revealed an inverse correlation between miR-17 and LKB1 expression and highlighted a prognostic role of miR-17 expression in LKB1 WT patients, which was further confirmed by The Cancer Genome Atlas data analysis., Conclusions: We identified miR-17 as a mediator of LKB1 expression in NSCLC tumors. This study proposes a miR-17 expression score potentially exploitable to discriminate LKB1 WT patients with NSCLC with impaired LKB1 expression and poor outcome, eligible for energy-stress-based treatments., (Copyright © 2021 International Association for the Study of Lung Cancer. All rights reserved.)

Published
2021
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47. Molecular determinants of response to PI3K/akt/mTOR and KRAS pathways inhibitors in NSCLC cell lines.

Author

Iezzi A, Caiola E, Colombo M, Marabese M, and Broggini M

Abstract

Despite the impressive results obtained in the preclinical setting, all the inhibitors targeting two central cascades in cancer, the PI3K/akt/mTOR and the KRAS/MEK/ERK pathways, have shown, apart from very few exceptions, disappointing efficacy when translated to the clinic. One of the main reasons of their clinical failure seems to be the lack of a clear molecular determinant of response to these drugs. In this study, we tried to address this point by evaluating the cytotoxic activity of different inhibitors targeting the two pathways at different levels in a panel of ten NSCLC cell lines harboring alterations in PI3K, KRAS or both. We were not able to highlight a correlation between the presence of KRAS and PI3K mutations and a specific sensitivity to the different drugs used. Molecular analyses performed after equimolar treatments showed that, independently from the entity of the response, the drugs are able to modulate the activation of their targets. Interestingly, we found that p53 mutational status separates the cell lines according to their sensitivity to PI3K pathway inhibitors treatments. The alterations considered in the PI3K/akt/mTOR and in the KRAS/MEK/ERK pathways in the different NSCLC cell lines are not sufficient to drive treatment choice but rather p53 status is a potential biomarker for the activity of this class of drugs., Competing Interests: None., (AJCR Copyright © 2020.)

Published
2020

48. Activity of Birinapant, a SMAC Mimetic Compound, Alone or in Combination in NSCLCs With Different Mutations.

Author

Colombo M, Marabese M, Vargiu G, Broggini M, and Caiola E

Abstract

Liver kinase B1 ( LKB1/STK11 ) is the second tumor suppressor gene most frequently mutated in non-small-cell lung cancer (NSCLC) and its activity is impaired in about half KRAS-mutated NSCLCs. Nowadays, no effective therapies are available for patients having these mutations. To highlight new vulnerabilities of this subgroup of tumors exploitable to design specific therapies we screened an US FDA-approved drug library using an isogenic system of wild-type (WT) or deleted LKB1. Among eight hit compounds, Birinapant, an inhibitor of the Inhibitor of Apoptosis Proteins (IAPs), was the most active compound in LKB1-deleted clone only compared to its LKB1 WT counterpart. We validated the Birinapant cells response and its mechanism of action to be dependent on LKB1 deletion. Indeed, we demonstrated the ability of this compound to induce apoptosis, through activation of caspases in the LKB1-deleted clone only. Expanding our results, we found that the presence of KRAS mutations could mediate Birinapant resistance in a panel of NSCLC cell lines. The combination of Birinapant with Ralimetinib, inhibitor of p38α, restores the sensitivity of LKB1- and KRAS-mutated cell lines to the IAP inhibitor Birinapant. Our study shows how the use of Birinapant could be a viable therapeutic option for patients with LKB1-mutated NSCLCs. In addition, combination of Birinapant and a KRAS pathway inhibitor, as Ralimetinib, could be useful for patients with LKB1 and KRAS-mutated NSCLC., (Copyright © 2020 Colombo, Marabese, Vargiu, Broggini and Caiola.)

Published
2020
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49. Predicting the Role of DNA Polymerase β Alone or with KRAS Mutations in Advanced NSCLC Patients Receiving Platinum-Based Chemotherapy.

Author

Alvisi MF, Ganzinelli M, Linardou H, Caiola E, Lo Russo G, Cecere FL, Bettini AC, Psyrri A, Milella M, Rulli E, Fabbri A, De Maglie M, Romanelli P, Murray S, Ndembe G, Broggini M, Garassino MC, and Marabese M

Abstract

Clinical data suggest that only a subgroup of non-small cell lung cancer (NSCLC) patients has long-term benefits after front-line platinum-based therapy. We prospectively investigate whether KRAS status and DNA polymerase β expression could help identify patients responding to platinum compounds. Prospectively enrolled, advanced NSCLC patients treated with a first-line regimen containing platinum were genotyped for KRAS and centrally evaluated for DNA polymerase β expression. Overall survival (OS), progression-free survival (PFS), and the objective response rate (ORR) were recorded. Patients with KRAS mutations had worse OS (hazard ratio (HR): 1.37, 95% confidence interval (95% CI): 0.70-2.27). Negative DNA polymerase β staining identified a subgroup with worse OS than patients expressing the protein (HR: 1.43, 95% CI: 0.57-3.57). The addition of KRAS to the analyses further worsened the prognosis of patients with negative DNA polymerase β staining (HR: 1.67, 95% CI: 0.52-5.56). DNA polymerase β did not influence PFS and ORR. KRAS may have a negative role in platinum-based therapy responses in NSCLC, but its impact is limited. DNA polymerase β, when not expressed, might indicate a group of patients with poor outcomes. KRAS mutations in tumors not expressing DNA polymerase β further worsens survival. Therefore, these two biomarkers together might well identify patients for whom alternatives to platinum-based chemotherapy should be used.

Published
2020
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50. Glutaminase Inhibition on NSCLC Depends on Extracellular Alanine Exploitation.

Author

Caiola E, Colombo M, Sestito G, Lupi M, Marabese M, Pastorelli R, Broggini M, and Brunelli L

Subjects
Carcinoma, Non-Small-Cell Lung metabolism, Cell Line, Tumor, Humans, Lung Neoplasms metabolism, Alanine metabolism, Carcinoma, Non-Small-Cell Lung genetics, Glutaminase antagonists & inhibitors, Lung Neoplasms genetics
Abstract

Non-small-cell lung cancer (NSCLC) cell lines vary in their sensitivity to glutaminase inhibitors, so it is important to identify the metabolic assets underling their efficacy in cancer cells. Even though specific genetic lesions such as in KRAS and LKB1 have been associated with reliance on glutamine for their metabolic needs, we found no distinction between glutaminase inhibitor CB-839 sensitivity and resistant phenotypes in NSCLC cells with or without these genetic alterations. We demonstrated the close relationship between environmental alanine uptake and catabolism. This response depended on the individual cell's ability to employ alanine aminotransferase (GPT2) to compensate the reduced glutamate availability. It may, therefore, be useful to determine GPT2 levels to predict which NSCLC patients would benefit most from glutaminase inhibitor treatment.

Published
2020
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