Your search keyword '"Valtorta S."' showing total 16 results

1. Frontiers in Anti-Cancer Drug Discovery: Challenges and Perspectives of Metformin as Anti-Angiogenic Add-On Therapy in Glioblastoma

Author

Laura Guarnaccia, Giovanni Marfia, Matteo Maria Masseroli, Stefania Elena Navone, Melissa Balsamo, Manuela Caroli, Silvia Valtorta, Rosa Maria Moresco, Rolando Campanella, Emanuele Garzia, Laura Riboni, Marco Locatelli, Guarnaccia, L, Marfia, G, Masseroli, M, Navone, S, Balsamo, M, Caroli, M, Valtorta, S, Moresco, R, Campanella, R, Garzia, E, Riboni, L, and Locatelli, M

Subjects

Brain tumor, Angiogenesi, Cancer Research, angiogenesis, Angiogenesis, brain tumors, glioblastoma, metformin, Oncology, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Review, RC254-282, oncology_oncogenics

Abstract

Simple Summary Glioblastoma is the most aggressive primary brain tumor, with the highest incidence and the worst prognosis. Life expectancy from diagnosis remains dismal, at around 15 months, despite surgical resection and treatment with radiotherapy and chemotherapy. Given the aggressiveness of the tumor and the inefficiency of the treatments adopted to date, the scientific research investigates innovative therapeutic approaches. Importantly, angiogenesis represents one of the main features of glioblastoma, becoming in the last few years a major candidate for target therapy. Metformin, a well-established therapy for type 2 diabetes, offered excellent results in preventing and fighting tumor progression, particularly against angiogenic mechanisms. Therefore, the purpose of this review is to summarize and discuss experimental evidence of metformin anti-cancer efficacy, with the aim of proposing this totally safe and tolerable drug as add-on therapy against glioblastoma. Abstract Glioblastoma is the most common primitive tumor in adult central nervous system (CNS), classified as grade IV according to WHO 2016 classification. Glioblastoma shows a poor prognosis with an average survival of approximately 15 months, representing an extreme therapeutic challenge. One of its distinctive and aggressive features is aberrant angiogenesis, which drives tumor neovascularization, representing a promising candidate for molecular target therapy. Although several pre-clinical studies and clinical trials have shown promising results, anti-angiogenic drugs have not led to a significant improvement in overall survival (OS), suggesting the necessity of identifying novel therapeutic strategies. Metformin, an anti-hyperglycemic drug of the Biguanides family, used as first line treatment in Type 2 Diabetes Mellitus (T2DM), has demonstrated in vitro and in vivo antitumoral efficacy in many different tumors, including glioblastoma. From this evidence, a process of repurposing of the drug has begun, leading to the demonstration of inhibition of various oncopromoter mechanisms and, consequently, to the identification of the molecular pathways involved. Here, we review and discuss metformin’s potential antitumoral effects on glioblastoma, inspecting if it could properly act as an anti-angiogenic compound to be considered as a safely add-on therapy in the treatment and management of glioblastoma patients.

Published

2022

2. Givinostat-Liposomes: Anti-Tumor Effect on 2D and 3D Glioblastoma Models and Pharmacokinetics

Author

Lorenzo Taiarol, Chiara Bigogno, Silvia Sesana, Marcelo Kravicz, Francesca Viale, Eleonora Pozzi, Laura Monza, Valentina Alda Carozzi, Cristina Meregalli, Silvia Valtorta, Rosa Maria Moresco, Marcus Koch, Federica Barbugian, Laura Russo, Giulio Dondio, Christian Steinkühler, Francesca Re, Taiarol, L, Bigogno, C, Sesana, S, Kravicz, M, Viale, F, Pozzi, E, Monza, L, Carozzi, V, Meregalli, C, Valtorta, S, Moresco, R, Koch, M, Barbugian, F, Russo, L, Dondio, G, Steinkühler, C, and Re, F

Subjects

Cancer Research, HDAC inhibitor, Oncology, brain, liposome, glioblastoma, liposomes, cancer, BIO/10 - BIOCHIMICA

Abstract

Glioblastoma is the most common and aggressive brain tumor, associated with poor prognosis and survival, representing a challenging medical issue for neurooncologists. Dysregulation of histone-modifying enzymes (HDACs) is commonly identified in many tumors and has been linked to cancer proliferation, changes in metabolism, and drug resistance. These findings led to the development of HDAC inhibitors, which are limited by their narrow therapeutic index. In this work, we provide the proof of concept for a delivery system that can improve the in vivo half-life and increase the brain delivery of Givinostat, a pan-HDAC inhibitor. Here, 150-nm-sized liposomes composed of cholesterol and sphingomyelin with or without surface decoration with mApoE peptide, inhibited human glioblastoma cell growth in 2D and 3D models by inducing a time- and dose-dependent reduction in cell viability, reduction in the receptors involved in cholesterol metabolism (from −25% to −75% of protein levels), and reduction in HDAC activity (−25% within 30 min). In addition, liposome-Givinostat formulations showed a 2.5-fold increase in the drug half-life in the bloodstream and a 6-fold increase in the amount of drug entering the brain in healthy mice, without any signs of overt toxicity. These features make liposomes loaded with Givinostat valuable as potential candidates for glioblastoma therapy.

Published

2022

3. [18F](2S,4R)-4-Fluoroglutamine as a New Positron Emission Tomography Tracer in Myeloma

Author

Silvia Valtorta, Denise Toscani, Martina Chiu, Andrea Sartori, Angela Coliva, Arianna Brevi, Giuseppe Taurino, Matteo Grioni, Livia Ruffini, Federica Vacondio, Franca Zanardi, Matteo Bellone, Rosa Maria Moresco, Ovidio Bussolati, Nicola Giuliani, Valtorta, S, Toscani, D, Chiu, M, Sartori, A, Coliva, A, Brevi, A, Taurino, G, Grioni, M, Ruffini, L, Vacondio, F, Zanardi, F, Bellone, M, Moresco, R, Bussolati, O, and Giuliani, N

Subjects

Cancer Research, glutamine, metabolism, mouse model, myeloma, nuclear medicine, positron-emission tomography, In vivo, medicine, RC254-282, Multiple myeloma, medicine.diagnostic_test, Chemistry, Bortezomib, business.industry, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, Glutamine, medicine.anatomical_structure, Oncology, Cell culture, Positron emission tomography, Proteasome inhibitor, Bone marrow, Nuclear medicine, business, medicine.drug

Abstract

The high glycolytic activity of multiple myeloma (MM) cells is the rationale for use of Positron Emission Tomography (PET) with18F-fluorodeoxyglucose ([18F]FDG) to detect both bone marrow (BM) and extramedullary disease. However, new tracers are actively searched because [18F]FDG-PET has some limitations and there is a portion of MM patients who are negative. Glutamine (Gln) addiction has been recently described as a typical metabolic feature of MM cells. Yet, the possible exploitation of Gln as a PET tracer in MM has never been assessed so far and is investigated in this study in preclinical models. Firstly, we have synthesized enantiopure (2S,4R)-4-fluoroglutamine (4-FGln) and validated it as a Gln transport analogue in human MM cell lines, comparing its uptake with that of3H-labelled Gln. We then radiosynthesized [18F]4-FGln, tested its uptake in two differentin vivomurine MM models, and checked the effect of Bortezomib, a proteasome inhibitor currently used in the treatment of MM. Both [18F]4-FGln and [18F]FDG clearly identified the spleen as site of MM cell colonization in C57BL/6 mice, challenged with syngeneic Vk12598 cells and assessed by PET. NOD.SCID mice, subcutaneously injected with human MM JJN3 cells, showed high values of both [18F]4-FGln and [18F]FDG uptake. Bortezomib significantly reduced the uptake of both radiopharmaceuticals in comparison with vehicle at post treatment PET. However, a reduction of glutaminolytic, but not of glycolytic, tumor volume was evident in mice showing the highest response to Bortezomib. Our data indicate that [18F](2S,4R)-4-FGln is a new PET tracer in preclinical MM models, yielding a rationale to design studies in MM patients.

Published

2021

4. Imaging Metformin Efficacy as Add-On Therapy in Cells and Mouse Models of Human EGFR Glioblastoma

Author

Silvia Valtorta, Alessia Lo Dico, Isabella Raccagni, Cristina Martelli, Valentina Pieri, Paolo Rainone, Sergio Todde, Bastian Zinnhardt, Elisabetta De Bernardi, Angela Coliva, Letterio S. Politi, Thomas Viel, Andreas H. Jacobs, Rossella Galli, Luisa Ottobrini, Valentina Vaira, Rosa Maria Moresco, Valtorta, S, Lo Dico, A, Raccagni, I, Martelli, C, Pieri, V, Rainone, P, Todde, S, Zinnhardt, B, De Bernardi, E, Coliva, A, Politi, L, Viel, T, Jacobs, A, Galli, R, Ottobrini, L, Vaira, V, and Moresco, R

Subjects

Cancer Research, EGFR - epidermal growth factor receptor, GBM - glioblastoma multiforme, PET imaging, TSPO, [18F]FLT, inflammation, metformin, In vivo, medicine, Translocator protein, Thymidine kinase 1, F]FLT, Survival rate, RC254-282, Original Research, Tumor microenvironment, Temozolomide, biology, Cell growth, business.industry, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Oncology, Apoptosis, Cancer research, biology.protein, [, business, medicine.drug

Abstract

Glioblastoma (GBM) is a highly aggressive tumor of the brain. Despite the efforts, response to current therapies is poor and 2-years survival rate ranging from 6-12%. Here, we evaluated the preclinical efficacy of Metformin (MET) as add-on therapy to Temozolomide (TMZ) and the ability of [18F]FLT (activity of thymidine kinase 1 related to cell proliferation) and [18F]VC701 (translocator protein, TSPO) Positron Emission Tomography (PET) radiotracers to predict tumor response to therapy. Indeed, TSPO is expressed on the outer mitochondrial membrane of activated microglia/macrophages, tumor cells, astrocytes and endothelial cells. TMZ-sensitive (Gli36ΔEGFR-1 and L0627) or -resistant (Gli36ΔEGFR-2) GBM cell lines representative of classical molecular subtype were tested in vitro and in vivo in orthotopic mouse models. Our results indicate that in vitro, MET increased the efficacy of TMZ on TMZ-sensitive and on TMZ-resistant cells by deregulating the balance between pro-survival (bcl2) and pro-apoptotic (bax/bad) Bcl-family members and promoting early apoptosis in both Gli36ΔEGFR-1 and Gli36ΔEGFR-2 cells. In vivo, MET add-on significantly extended the median survival of tumor-bearing mice compared to TMZ-treated ones and reduced the rate of recurrence in the TMZ-sensitive models. PET studies with the cell proliferation radiopharmaceutical [18F]FLT performed at early time during treatment were able to distinguish responder from non-responder to TMZ but not to predict the duration of the effect. On the contrary, [18F]VC701 uptake was reduced only in mice treated with MET plus TMZ and levels of uptake negatively correlated with animals’ survival. Overall, our data showed that MET addition improved TMZ efficacy in GBM preclinical models representative of classical molecular subtype increasing survival time and reducing tumor relapsing rate. Finally, results from PET imaging suggest that the reduction of cell proliferation represents a common mechanism of TMZ and combined treatment, whereas only the last was able to reduce TSPO. This reduction was associated with the duration of treatment response. TSPO-ligand may be used as a complementary molecular imaging marker to predict tumor microenvironment related treatment effects.

Published

2021

5. Effects of Metformin as Add-On Therapy against Glioblastoma: An Old Medicine for Novel Oncology Therapeutics

Author

Laura Guarnaccia, Stefania E. Navone, Matteo M. Masseroli, Melissa Balsamo, Manuela Caroli, Silvia Valtorta, Rosa M. Moresco, Rolando Campanella, Luigi Schisano, Giorgio Fiore, Valentina Galiano, Emanuele Garzia, Giuseppe C. Appiani, Marco Locatelli, Laura Riboni, Giovanni Marfia, Guarnaccia, L, Navone, S, Masseroli, M, Balsamo, M, Caroli, M, Valtorta, S, Moresco, R, Campanella, R, Schisano, L, Fiore, G, Galiano, V, Garzia, E, Appiani, G, Locatelli, M, Riboni, L, and Marfia, G

Subjects

Cancer Research, glioblastoma, metformin, brain tumors, angiogenesis, Oncology, angiogenesi, brain tumor

Abstract

Simple Summary Glioblastoma is the most common and malignant primary brain tumor, with a median survival of around 14 months. The aggressiveness of glioblastoma is due to intense cell proliferation, angiogenesis, invasiveness, genetic instability, resistance to therapies and high frequency of relapses. These features render glioblastoma almost incurable, considered an extreme therapeutic challenge. In the last few decades, it has been observed a reduced cancer incidence in diabetic patients treated with metformin, an oral hypoglycemic drug. The reported ability of metformin to arrest cancer cell growth in in vitro and in vivo experimental tumor models, have suggested the possibility to reconsider metformin as an anti-cancer add-on therapy, but further investigations about molecular mechanisms and optimal therapeutic regimens are needed. Here, we tested the efficacy of metformin against primary glioblastoma endothelial cells, responsible for tumor angiogenesis, invasiveness and resistance to therapy, reporting promising results and advancing a novel target of metformin, the "sphingolipid rheostat". Background: Glioblastoma is the most aggressive primary brain malignancy in adults, with a poor prognosis of about 14 months. Recent evidence ascribed to metformin (MET), an antihyperglycemic drug, the potential to reduce cancer incidence and progression, but the molecular mechanisms underlying these effects need to be better investigated. Methods: Here, we tested the efficacy of MET on n = 10 primary glioblastoma endothelial cells (GECs), by viability and proliferation tests, as MTT and Live/Dead assays, apoptosis tests, as annexin V assay and caspase 3/7 activity, functional tests as tube-like structure formation and migration assay and by mRNA and protein expression performed by quantitative real-time PCR analysis (qRT-PCR) and Western Blot, respectively. Results: Data resulting revealed a time- and mu-dependent ability of MET to decrease cell viability and proliferation, increasing pro-apoptotic mechanisms mediated by caspases 3/7. Also, MET impacted GEC functionality with a significant decrease of angiogenesis and invasiveness potential. Mechanistically, MET was able to interfere with sphingolipid metabolism, weakening the oncopromoter signaling promoted by sphingosine-1-phosphate (S1P) and shifting the balance toward the production of the pro-apoptotic ceramide. Conclusions: These observations ascribed to MET the potential to serve as add-on therapy against glioblastoma, suggesting a repurposing of an old, totally safe and tolerable drug for novel oncology therapeutics.

Published

2022

6. Metformin and temozolomide, a synergic option to overcome resistance in glioblastoma multiforme models

Author

Sara Belloli, Isabella Raccagni, Rosa Maria Moresco, Silvia Valtorta, Giulia Ercoli, Alessia Lo Dico, Cristina Martelli, Daniela Gaglio, Cecilia Diceglie, Letterio S. Politi, Marcella Bonanomi, Valentina Vaira, Luisa Ottobrini, Valtorta, S, Dico, A, Raccagni, I, Gaglio, D, Belloli, S, Politi, L, Martelli, C, Diceglie, C, Bonanomi, M, Ercoli, G, Vaira, V, Ottobrini, L, and Moresco, R

Subjects

0301 basic medicine, medicine.medical_treatment, Brain tumor, Glioblastoma multiforme, 03 medical and health sciences, Glioma, Temozolomide, medicine, CD90, business.industry, Glioma stem cell, medicine.disease, Metformin, Radiation therapy, Metabolism, 030104 developmental biology, Oncology, Apoptosis, glioma stem cells, Cancer research, Stem cell, business, Research Paper, medicine.drug

Abstract

Glioblastoma multiforme (GBM) is the most aggressive primary brain tumor with poor survival. Cytoreduction in association with radiotherapy and temozolomide (TMZ) is the standard therapy, but response is heterogeneous and life expectancy is limited. The combined use of chemotherapeutic agents with drugs targeting cell metabolism is becoming an interesting therapeutic option for cancer treatment. Here, we found that metformin (MET) enhances TMZ effect on TMZ-sensitive cell line (U251) and overcomes TMZ-resistance in T98G GBM cell line. In particular, combined-treatment modulated apoptosis by increasing Bax/Bcl-2 ratio, and reduced Reactive Oxygen Species (ROS) production. We also observed that MET associated with TMZ was able to reduce the expression of glioma stem cells (GSC) marker CD90 particularly in T98G cells but not that of CD133. In vivo experiments showed that combined treatment with TMZ and MET significantly slowed down growth of TMZ-resistant tumors but did not affect overall survival of TMZ-sensitive tumor bearing mice. In conclusion, our results showed that metformin is able to enhance TMZ effect in TMZ-resistant cell line suggesting its potential use in TMZ refractory GBM patients. However, the lack of effect on a GBM malignancy marker like CD133 requires further evaluation since it might influence response duration.

Published

2017

7. Tumour hypoxia: lessons learnt from preclinical imaging

Author

Silvia Valtorta, Isabella Raccagni, Rosa Maria Moresco, Sara Belloli, Raccagni, I, Valtorta, S, Moresco, R, and Belloli, S

Subjects

Oncology, Pathology, medicine.medical_specialty, medicine.medical_treatment, PET imaging, Hypoxia-specific radiopharmaceutical, 030218 nuclear medicine & medical imaging, 03 medical and health sciences, Preclinical research, Hypoxia-specific radiopharmaceuticals, 0302 clinical medicine, Internal medicine, medicine, Radiology, Nuclear Medicine and imaging, Treatment outcome, Treatment resistance, Hypoxia, business.industry, Pet imaging, Hypoxia (medical), Tumour oxygenation, Preclinical, Radiation therapy, 030220 oncology & carcinogenesis, Tracer uptake, medicine.symptom, business, Preclinical imaging

Abstract

Purpose: In tumour, the imbalance between oxygen supply and demand leads to hypoxia, which represents a negative prognostic factor associated with aggressive tumour phenotype and therapy resistance. This review provides an overview of the use of positron emitter-labelled radiopharmaceutical used to image hypoxia in preclinical models of cancer. Methods: A critical and comprehensive PubMed search was performed identifying articles related to PET imaging for hypoxia assessment in preclinical setting from January 2007 up to January 2017. Results: We have considered and described a total of 54 original articles, exploring tumour-associated hypoxia in preclinical models. Results underlined the potential application together with the advantages and pitfalls of the use of PET in preclinical research. Multi-target imaging allowed to better define the relationship between hypoxia and other biological hallmarks of tumour; imaging of hypoxia was proved as a useful tool for lesions stratification and response prediction to radiotherapy; however, cutoff indexes were identified in few studies. Hypoxia PET showed remarkable tracer delivery limitations in the study of vascular disrupting agents but suggested the potential use of PET as a marker of response or resistance to anti-angiogenics. Finally, the effect of anaesthesia on tracer kinetics and tumour oxygenation as well as perfusion dependency in tracer uptake should be carefully evaluated to avoid artefactual results. Conclusions: Preclinical studies highlight the advantages and the limitations of the available hypoxia-radiotracers and their potential usefulness for the evaluation of treatments outcome and radiotherapy planning.

Published

2017

8. Role of Metformin and AKT Axis Modulation in the Reversion of Hypoxia Induced TMZ-Resistance in Glioma Cells

Author

Alessia Lo Dico, Silvia Valtorta, Luisa Ottobrini, Rosa Maria Moresco, Lo Dico, A, Valtorta, S, Ottobrini, L, and Moresco, R

Subjects

0301 basic medicine, Cancer Research, hypoxia resistance, lcsh:RC254-282, 03 medical and health sciences, 0302 clinical medicine, Glioma, medicine, Viability assay, HIF-1α biomarker, Protein kinase B, PI3K/AKT/mTOR pathway, Original Research, Temozolomide, business.industry, Hypoxia (medical), lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, 3. Good health, Metformin, 030104 developmental biology, AKT pathway, Oncology, Tumor progression, 030220 oncology & carcinogenesis, Cancer research, MET, TMZ responsiveness, medicine.symptom, business, medicine.drug

Abstract

Hypoxia is a key driver of tumor adaptation promoting tumor progression and resistance to therapy. Hypoxia related pathways might represent attractive targets for the treatment of Glioblastoma Multiforme (GBM), that up to date is characterized by a poor prognosis. Primary aim of this study was to investigate the role of hypoxia and hypoxia-related modifications in the effect of temozolomide (TMZ) given alone or in association with the antidiabetic agent Metformin (MET) or the PI3K/mTOR blocker, BEZ235. The study was conducted in the TMZ responsive U251 and resistant T98 GBM cells. Our results showed that during hypoxia, TMZ plus MET reduced viability of U251 cells affecting also CD133 and CD90 expressing cells. This effect was associated with a reduction of HIF-1α activity, VEGF release and AKT activation. In T98 TMZ-resistant cells, TMZ plus MET exerted similar effects on HIF-1α. However, in this cell line, TMZ plus MET failed to reduce CD133 positive cells and AKT phosphorylation. Nevertheless, the administration of the dual PI3K/mTOR inhibitor BEZ235 potentiated the effect of TMZ plus MET on cell viability, inducing a pro-apoptotic phenotype during hypoxic condition also in T98 cells, suggesting the block of the PI3K/AKT/mTOR pathway as a complementary target to further overcome GBM resistance during hypoxia. In conclusion, we proposed TMZ plus MET as suitable treatment to revert TMZ-resistance also during hypoxia, an effect potentiated by the inhibition of PI3K/mTOR axis.

Published

2019

9. Metabolic Evaluation of Non–Small Cell Lung Cancer Patient–Derived Xenograft Models Using 18F-FDG PET: A Potential Tool for Early Therapy Response

Author

Silvia Valtorta* 1, 2, Massimo Moro* 3, Giovanna Prisinzano 1, 4, Giulia Bertolini 3, Monica Tortoreto 5, Isabella Raccagni 2, Ugo Pastorino 6, Luca Roz 3, Gabriella Sozzi +3, Rosa Maria Moresco +2, 4 *Contributed equally to this work. +Contributed equally to this work., Valtorta, S, Moro, M, Prisinzano, G, Bertolini, G, Tortoreto, M, Raccagni, I, Pastorino, U, Roz, L, Sozzi, G, and Moresco, R

Subjects

Male, 0301 basic medicine, Oncology, medicine.medical_specialty, Lung Neoplasms, Mice, Nude, Animal Imaging, Oncology: Lung, PET, [18F]FDG PET, lung cancer, patient-derived xenograft, stem cells, Mice, SCID, 18F-FDG PET, lung cancer, patient-derived xenograft, stem cells, Early Therapy, Sensitivity and Specificity, 18f fdg pet, 03 medical and health sciences, 18F-FDG PET, 0302 clinical medicine, Fluorodeoxyglucose F18, Carcinoma, Non-Small-Cell Lung, Cell Line, Tumor, Internal medicine, Biomarkers, Tumor, Tumor Cells, Cultured, medicine, Animals, Humans, Radiology, Nuclear Medicine and imaging, Therapy efficacy, Lung cancer, Tumor xenograft, business.industry, Reproducibility of Results, Pet imaging, medicine.disease, Molecular Imaging, Glucose, Outcome and Process Assessment, Health Care, Treatment Outcome, 030104 developmental biology, 030220 oncology & carcinogenesis, Female, Non small cell, Radiopharmaceuticals, Stem cell, business

Abstract

PURPOSE: Lung cancer heterogeneity makes response to therapy extremely hard to predict. Patient-derived xenografts (PDXs) represent a reliable preclinical model that closely recapitulates the main characteristics of the primary tumor and could represent a useful asset to test new therapies. Here, using PET imaging, we verify how lung cancer PDXs reproduce the metabolic features of the corresponding primary tumors. METHODS: We performed longitudinal [18F]FDG-PET studies on nine different PDXs, obtained by implants of primary cancer fragments harvested from patients. Max [18F]FDG uptake values of the lesion for each group were calculated and compared to corresponding patient's uptake. RESULTS: Different PDXs showed variable tumor growth rate and [18F]FDG uptake confirming the preservation of individual characteristics. A good intra-group reproducibility of PET measurements was observed. Furthermore, the subgroup of PDXs originating from primary tumors with higher metabolic rate displayed a rank order of [18F]FDG uptake similar to that of patients' original SUV. CONCLUSION: PDXs reproduced the original glucose metabolism of primary lesions and represent therefore a promising preclinical model also for the early assessment of therapy efficacy.

Published

2016

10. [18F]FDG and [18F]FLT PET for the evaluation of response to neo-adjuvant chemotherapy in a model of triple negative breast cancer

Author

Luca Presotto, Isabella Raccagni, Giorgio Ivan Russo, Nadia Zaffaroni, Rosa Maria Moresco, Maria Grazia Daidone, Sara Belloli, Emilio Bombardieri, Anna Bogni, Claudio Pascali, Monica Tortoreto, Silvia Valtorta, Alessandro Di Stefano, Raccagni, I, Belloli, S, Valtorta, S, Stefano, A, Presotto, L, Pascali, C, Bogni, A, Tortoreto, M, Zaffaroni, N, Daidone, M, Russo, G, Bombardieri, E, and Moresco, R

Subjects

Metabolic Processes, Oncology, medicine.medical_treatment, Cancer Treatment, lcsh:Medicine, Triple Negative Breast Neoplasms, Mice, SCID, Pathology and Laboratory Medicine, Biochemistry, Diagnostic Radiology, 030218 nuclear medicine & medical imaging, Mice, chemistry.chemical_compound, 0302 clinical medicine, Breast Tumors, Medicine and Health Sciences, lcsh:Science, Tomography, Neoadjuvant therapy, Triple-negative breast cancer, Multidisciplinary, TNBC, [18F]FDG, [18F]FLT, PET, treatment response, medicine.diagnostic_test, Pharmaceutics, Radiology and Imaging, Neoadjuvant Therapy, Paclitaxel, Positron emission tomography, Response Evaluation Criteria in Solid Tumors, Area Under Curve, 030220 oncology & carcinogenesis, Female, Anatomy, Glycolysis, Research Article, Clinical Oncology, medicine.medical_specialty, Histology, Imaging Techniques, Transplantation, Heterologous, Mice, Nude, Neuroimaging, Research and Analysis Methods, Cancer Chemotherapy, 03 medical and health sciences, Signs and Symptoms, Text mining, Drug Therapy, Fluorodeoxyglucose F18, Diagnostic Medicine, Cell Line, Tumor, Internal medicine, Breast Cancer, medicine, Animals, Humans, Chemotherapy, business.industry, lcsh:R, Cancers and Neoplasms, Biology and Life Sciences, Antineoplastic Agents, Phytogenic, Transplantation, Ki-67 Antigen, Metabolism, ROC Curve, chemistry, Positron-Emission Tomography, Lesions, lcsh:Q, Radiopharmaceuticals, Clinical Medicine, business, Positron Emission Tomography, Biomarkers, Thymidine, Neuroscience

Abstract

Rationale Pathological response to neo-adjuvant chemotherapy (NAC) represents a commonly used predictor of survival in triple negative breast cancer (TNBC) and the need to identify markers that predict response to NAC is constantly increasing. Aim of this study was to evaluate the potential usefulness of PET imaging with [18F]FDG and [18F]FLT for the discrimination of TNBC responders to Paclitaxel (PTX) therapy compared to the response assessed by an adapted Response Evaluation Criteria In Solid Tumors (RECIST) criteria based on tumor volume (Tumor Volume Response). Methods Nu/nu mice bearing TNBC lesions of different size were evaluated with [18F]FDG and [18F]FLT PET before and after PTX treatment. SUVmax, Metabolic Tumor Volume (MTV) and Total Lesion Glycolysis (TLG) and Proliferation (TLP) were assessed using a graph-based random walk algorithm. Results We found that in our TNBC model the variation of [18F]FDG and [18F]FLT SUVmax similarly defined tumor response to therapy and that SUVmax variation represented the most accurate parameter. Response evaluation using Tumor Volume Response (TVR) showed that the effectiveness of NAC with PTX was completely independent from lesions size at baseline. Conclusions Our study provided interesting results in terms of sensitivity and specificity of PET in TNBC, revealing the similar performances of [18F]FDG and [18F]FLT in the identification of responders to Paclitaxel.

Published

2018

11. Divergent in vitro/in vivo responses to drug treatments of highly aggressive NIH-Ras cancer cells: A PET imaging and metabolomics-mass-spectrometry study

Author

Daniela Gaglio 1, 2, 6, 8, Silvia Valtorta 1, 3, 4, Marilena Ripamonti 1, Marcella Bonanomi 2, Chiara Damiani 2, Sergio Todde 5, Alfredo Simone Negri 6, Francesca Sanvito 7, Fabrizia Mastroianni 2, Antonella Di Campli 8, Gabriele Turacchio 8, Giuseppe Di Grigoli 1, Sara Belloli 1, Alberto Luini 8, Maria Carla Gilardi 1, Anna Maria Colangelo 2, 9, Lilia Alberghina 2, Rosa Maria Moresco 2, Gaglio, D, Valtorta, S, Ripamonti, M, Bonanomi, M, Damiani, C, Todde, S, Negri, A, Sanvito, F, Mastroianni, F, Di Campli, A, Turacchio, G, Di Grigoli, G, Belloli, S, Luini, A, Gilardi, M, Colangelo, A, Alberghina, L, and Moresco, R

Subjects

0301 basic medicine, Oncology, Gerontology, medicine.medical_specialty, Mice, Nude, Mass Spectrometry, Metabolomics-mass-spectrometry, Mice, 03 medical and health sciences, Metabolomics, Internal medicine, medicine, Tumor, metabolic rewaring, PET imaging, metabolomics-mass-spectrometry, oncogenic-K-ras, Animals, Tumor growth, PET-imaging, In vitro in vivo, Oncogenic-K-ra, Tumor, business.industry, Environmental adaptation, Neoplasms, Experimental, Pet imaging, 3. Good health, Genes, ras, 030104 developmental biology, Positron-Emission Tomography, Cancer metabolism, Cancer cell, NIH 3T3 Cells, oncogenic-K-ras, Stress conditions, Metabolic rewiring, business, Glycolysis, Research Paper

Abstract

// Daniela Gaglio 1, 2, 6, 8 , Silvia Valtorta 1, 2, 3, 4 , Marilena Ripamonti 1, 2 , Marcella Bonanomi 2 , Chiara Damiani 2 , Sergio Todde 5 , Alfredo Simone Negri 6 , Francesca Sanvito 7 , Fabrizia Mastroianni 2 , Antonella Di Campli 8 , Gabriele Turacchio 8 , Giuseppe Di Grigoli 1, 2, 3 , Sara Belloli 1, 2, 3 , Alberto Luini 8 , Maria Carla Gilardi 1, 2 , Anna Maria Colangelo 2, 9 , Lilia Alberghina 2, 9, * , Rosa Maria Moresco 2, 3, 4, * 1 Institute of Molecular Bioimaging and Physiology, National Research Council (IBFM-CNR), Segrate, Italy 2 SYSBIO.IT, Centre of Systems Biology, Milano, Italy 3 Experimental Imaging Center, IRCCS San Raffaele Scientific Institute, Milan, Italy 4 Department of Medicine and Surgery, University of Milano-Bicocca, Monza, Italy 5 Tecnomed Foundation of University of Milano-Bicocca, Monza, Italy 6 Department of Agricultural and Environmental Sciences - Production, Landscape, Agroenergy University of Milan, Milan, Italy 7 Mouse Histopathology Unit, Department of Pathology, IRCCS San Raffaele Scientific Institute, Milan, Italy 8 Institute of Protein Biochemistry, National Research Council, Naples, Italy 9 Department of Biotechnology and Biosciences, University of Milano-Bicocca, Milan, Italy * These authors have contributed equally to this work Correspondence to: Daniela Gaglio, email: daniela.gaglio@ibfm.cnr.it Rosa Maria Moresco, email: moresco.rosamaria@hsr.it Keywords: tumor, metabolic rewiring, PET-imaging, metabolomics-mass-spectrometry, oncogenic-K-ras Received: February 02, 2016 Accepted: June 17, 2016 Published: July 07, 2016 ABSTRACT Oncogenic K-ras is capable to control tumor growth and progression by rewiring cancer metabolism. In vitro NIH-Ras cells convert glucose to lactate and use glutamine to sustain anabolic processes, but their in vivo environmental adaptation and multiple metabolic pathways activation ability is poorly understood. Here, we show that NIH-Ras cancer cells and tumors are able to coordinate nutrient utilization to support aggressive cell proliferation and survival. Using PET imaging and metabolomics-mass spectrometry, we identified the activation of multiple metabolic pathways such as: glycolysis, autophagy recycling mechanism, glutamine and serine/glycine metabolism, both under physiological and under stress conditions. Finally, differential responses between in vitro and in vivo systems emphasize the advantageous and uncontrolled nature of the in vivo environment, which has a pivotal role in controlling the responses to therapy.

Published

2016

12. Leukocytes recruited by tumor-derived HMGB1 sustain peritoneal carcinomatosis

Author

Cottone, Lucia, Capobianco, Annalisa, Gualteroni, Chiara, Monno, Antonella, Raccagni, Isabella, Valtorta, Silvia, Canu, Tamara, Di Tomaso, Tiziano, Lombardo, Angelo, Esposito, Antonio, Moresco, Rosa Maria, Del Maschio, Alessandro, Naldini, Luigi, Rovere-Querini, Patrizia, Bianchi, Marco E., Manfredi, Angelo A., Cottone, L, Capobianco, A, Gualteroni, C, Monno, A, Raccagni, I, Valtorta, S, Canu, T, Tomaso, T, Lombardo, A, Esposito, A, Moresco, R, Maschio, A, Naldini, L, Rovere Querini, P, Bianchi, M, Manfredi, A, De Tomaso, T, Lombardo, ANGELO LEONE, Esposito, Antonio, Moresco, Rm, DEL MASCHIO, Alessandro, Naldini, Luigi, ROVERE QUERINI, Patrizia, Bianchi, MARCO EMILIO, and Manfredi, ANGELO ANDREA M. A.

Subjects

0301 basic medicine, green fluorescent protein, Pathology, medicine.medical_specialty, Murine colon adenocarcinoma cell line, Phagocyte, Macrophage, Immunology, Damage-associated molecular pattern, chemical and pharmacologic phenomena, High Mobility Box 1, macrophage, HMGB1, GFP, BoxA, damage-associated molecular pattern, Small hairpin RNA, 03 medical and health sciences, 0302 clinical medicine, vascularization, In vivo, Leukocytes, medicine, Extracellular, DAMP, short hairpin RNA, Immunology and Allergy, MC-38, murine colon adenocarcinoma cell line, Original Research, Gene knockdown, peritoneal carcinomatosi, biology, business.industry, Macrophages, Tumor-Derived, Leukocyte, 030104 developmental biology, medicine.anatomical_structure, Alarmin, Oncology, 030220 oncology & carcinogenesis, biology.protein, ShRNA, business, leukocyte, Peritoneal carcinomatosis

Abstract

The factors that determine whether disseminated transformed cells in vivo yield neoplastic lesions have only been partially identified. We established an ad hoc model of peritoneal carcinomatosis by injecting colon carcinoma cells in mice. Tumor cells recruit inflammatory leukocytes, mostly macrophages, and generate neoplastic peritoneal lesions. Phagocyte depletion via clodronate treatment reduces neoplastic growth. Colon carcinoma cells release a prototypic damage-associated molecular pattern (DAMP)/alarmin, High Mobility Group Box1 (HMGB1), which attracts leukocytes. Exogenous HMGB1 accelerates leukocyte recruitment, macrophage infiltration, tumor growth and vascularization. Lentiviral-based HMGB1 knockdown or pharmacological interference with its extracellular impair macrophage recruitment and tumor growth. Our findings provide a preclinical proof of principle that strategies based on preventing HMGB1-driven recruitment of leukocytes could be used for treating peritoneal carcinomatosis.

Published

2016

13. VEGF-targeted therapy stably modulates the glycolytic phenotype of tumor cells

Author

Giovanni Esposito, Rosa Maria Moresco, Elisabetta Zulato, Henrike Schroer, Francesco Ciccarese, Matteo Curtarello, Andrea Rasola, Wolfgang Mueller-Klieser, Luca Persano, Stefan Walenta, Mario Plebani, Aichi Msaki, Giulia Guzzo, Stefano Indraccolo, Elisabetta Rossi, Roberta Bertorelle, Anna Pastò, Alberto Amadori, Silvia Valtorta, Sergio Todde, Giorgia Nardo, Curtarello, M, Zulato, E, Nardo, G, Valtorta, S, Guzzo, G, Rossi, E, Esposito, G, Msaki, A, Pastò, A, Rasola, A, Persano, L, Ciccarese, F, Bertorelle, R, Todde, S, Plebani, M, Schroer, H, Walenta, S, Mueller Klieser, W, Amadori, A, Moresco, R, and Indraccolo, S

Subjects

Vascular Endothelial Growth Factor A, Cancer Research, Pathology, medicine.medical_specialty, Necrosis, medicine.medical_treatment, Angiogenesis Inhibitors, Mice, SCID, Biology, SCID, Antibodies, Monoclonal, Humanized, Antibodies, Cell Line, Targeted therapy, Mice, Random Allocation, Cell Line, Tumor, Neoplasms, Monoclonal, Animals, Bevacizumab, Female, Glycolysis, Humans, MCF-7 Cells, Mice, Inbred BALB C, Molecular Targeted Therapy, Phenotype, Xenograft Model Antitumor Assays, medicine, cancer-cell, Anti-VEGF therapy, Humanized, Inbred BALB C, MED/36 - DIAGNOSTICA PER IMMAGINI E RADIOTERAPIA, Tumor, positron emission tomography, antiangiogenesis, glucose metabolism, hypoxia, Blockade, Vascular endothelial growth factor A, Oncology, Cell culture, Cancer research, MED/06 - ONCOLOGIA MEDICA, medicine.symptom

Abstract

Anti-VEGF therapy perturbs tumor metabolism, severely impairing oxygen, glucose, and ATP levels. In this study, we investigated the effects of anti-VEGF therapy in multiple experimental tumor models that differ in their glycolytic phenotypes to gain insights into optimal modulation of the metabolic features of this therapy. Prolonged treatments induced vascular regression and necrosis in tumor xenograft models, with highly glycolytic tumors becoming treatment resistant more rapidly than poorly glycolytic tumors. By PET imaging, prolonged treatments yielded an increase in both hypoxic and proliferative regions of tumors. A selection for highly glycolytic cells was noted and this metabolic shift was stable and associated with increased tumor aggressiveness and resistance to VEGF blockade in serially transplanted mice. Our results support the hypothesis that the highly glycolytic phenotype of tumor cells studied in xenograft models, either primary or secondary, is a cell-autonomous trait conferring resistance to VEGF blockade. The finding that metabolic traits of tumors can be selected by antiangiogenic therapy suggests insights into the evolutionary dynamics of tumor metabolism. Cancer Res; 75(1); 120–33. ©2014 AACR.

Published

2015

14. A novel AMPK activator reduces glucose uptake and inhibits tumor progression in a mouse xenograft model of colorectal cancer

Author

Guido Cavaletti, Cristina Meregalli, Paola Fusi, Farida Tripodi, Gabriella Nicolini, Luca Crippa, Rosa Maria Moresco, Francesca Sanvito, Silvia Valtorta, Roberto Pagliarin, Fulvia Orsini, F Avezza, Paola Coccetti, Gloria Bertoli, Valtorta, S, Nicolini, G, Tripodi, F, Meregalli, C, Cavaletti, G, Avezza, F, Crippa, L, Bertoli, G, Sanvito, F, Fusi, P, Pagliarin, R, Orsini, F, Moresco, R, and Coccetti, P

Subjects

Male, Colorectal cancer, Cell Survival, Glucose uptake, Antineoplastic Agents, Pharmacology, AMP-Activated Protein Kinases, Mice, AMP-activated protein kinase, In vivo, Cell Line, Tumor, medicine, Animals, Humans, ampk activator,xenograft, colorectal cancer, Pharmacology (medical), Protein kinase A, Combretastatin A4 (CA-4), biology, business.industry, Xenograft, Guaiacol, AMPK, medicine.disease, Xenograft Model Antitumor Assays, BIO/17 - ISTOLOGIA, PET, Glucose, Oncology, Tumor progression, Apoptosis, biology.protein, Azetidines, business, Colorectal Neoplasms, Azetidinones

Abstract

Summary: The anticancer activity of a novel pure 1,4-Diaryl-2-azetidinone (1), endowed with a higher solubility than the well known Combretastatin A4, is tested in mice. We previously reported that Compound (1) showed specific antiproliferative activity against duodenal and colon cancer cells, inducing activation of AMP-activated protein kinase and apoptosis. Here we estimate that the maximum tolerated dose in a mouse model is 40 mg/kg; the drug is well tolerated both in single dose and in repeated administration schedules. The drug displays a significant antitumor activity and a tumor growth delay when administered at the MTD both in single and fractionated i.v. administration in a mouse xenograft model of colorectal cancer. Arrest of tumor growth and relapse after drug suspension are parallel to modification in glucose demand as shown by PET studies with [18∈F] FDG. These data strongly support Compound (1) as a promising molecule for in vivo treatment of colorectal cancer.

Published

2014

15. Therapeutic antibody targeting of Notch1 in T-acute lymphoblastic leukemia xenografts

Author

Timothy Hoey, Angela Grassi, Fumiko Takada Axelrod, Chiara Frasson, Sonia Minuzzo, Alberto Amadori, A. Gurney, Silvia Valtorta, Stefano Indraccolo, S. Satyal, Giuseppe Basso, E Seganfreddo, Valentina Agnusdei, Rosa Maria Moresco, Agnusdei, V, Minuzzo, S, Frasson, C, Grassi, A, Axelrod, F, Satyal, S, Gurney, A, Hoey, T, Seganfreddo, E, Basso, G, Valtorta, S, Moresco, R, Amadori, A, and Indraccolo, S

Subjects

Cancer Research, medicine.medical_treatment, Cell, Nod, Precursor T-Cell Lymphoblastic Leukemia-Lymphoma, Dexamethasone, Targeted therapy, predictive biomarkers, Mice, hemic and lymphatic diseases, Molecular Targeted Therapy, Receptor, Notch1, Child, predictive biomarker, biology, Gene Expression Regulation, Leukemic, apoptosis, Notch1, T-ALL, Antibodies, Monoclonal, Drug Synergism, Hematology, targeted therapy, Tumor Burden, medicine.anatomical_structure, Oncology, Child, Preschool, embryonic structures, Neoplastic Stem Cells, cardiovascular system, biological phenomena, cell phenomena, and immunity, Antibody, medicine.drug, Adolescent, Notch signaling pathway, Antineoplastic Agents, T Acute Lymphoblastic Leukemia, medicine, Animals, Humans, Neoplasm Staging, Chemotherapy, business.industry, Xenograft Model Antitumor Assays, apoptosi, Disease Models, Animal, Immunology, biology.protein, sense organs, business

Abstract

T-acute lymphoblastic leukemia (T-ALL) is characterized by several genetic alterations and poor prognosis in about 20-25% of patients. Notably, about 60% of T-ALL shows increased Notch1 activity, due to activating NOTCH1 mutations or alterations in the FBW7 gene, which confer to the cell a strong growth advantage. Therapeutic targeting of Notch signaling could be clinically relevant, especially for chemotherapy refractory patients. This study investigated the therapeutic efficacy of a novel anti-Notch1 monoclonal antibody by taking advantage of a collection of pediatric T-ALL engrafted systemically in NOD/SCID mice and genetically characterized with respect to NOTCH1/FBW7 mutations. Anti-Notch1 treatment greatly delayed engraftment of T-ALL cells bearing Notch1 mutations, including samples derived from poor responders or relapsed patients. Notably, the therapeutic efficacy of anti-Notch1 therapy was significantly enhanced in combination with dexamethasone. Anti-Notch1 treatment increased T-ALL cell apoptosis, decreased proliferation and caused strong inhibitory effects on Notch-target genes expression along with complex modulations of gene expression profiles involving cell metabolism. Serial transplantation experiments suggested that anti-Notch1 therapy could compromise leukemia-initiating cell functions. These results show therapeutic efficacy of Notch1 blockade for T-ALL, highlight the potential of combination with dexamethasone and identify surrogate biomarkers of the therapeutic response.

Published

2014

16. Validation of an engineered cell model for in vitro and in vivo HIF-1α evaluation by different imaging modalities

Author

Silvano Bosari, Silvia Valtorta, Isabella Raccagni, Delfina Tosi, Cristina Martelli, Luisa Ottobrini, Giovanni Lucignani, Umberto Gianelli, M. Russo, Rosa Maria Moresco, Sara Belloli, Anna Degrassi, A. Lo Dico, Lo Dico, A, Valtorta, S, Martelli, C, Belloli, S, Gianelli, U, Tosi, D, Bosari, S, Degrassi, A, Russo, M, Raccagni, I, Lucignani, G, Moresco, R, and Ottobrini, L

Subjects

Cancer Research, Pathology, medicine.medical_specialty, Fluorescence-lifetime imaging microscopy, Tumor model, Biology, Deferoxamine, Models, Biological, Multimodal Imaging, 03 medical and health sciences, Mice, 0302 clinical medicine, In vivo, Glioma, Cell Line, Tumor, medicine, Bioluminescence imaging, Animals, Humans, Radiology, Nuclear Medicine and imaging, Luciferase, Non-invasive molecular imaging, Hypoxia, Luciferases, Cell Shape, Glioma, Hypoxia, Non-invasive molecular imaging, Reporter gene, Optical imaging, PET, MRI, Tumor model, 030304 developmental biology, 0303 health sciences, medicine.diagnostic_test, Brain Neoplasms, Optical Imaging, Magnetic resonance imaging, medicine.disease, Hypoxia-Inducible Factor 1, alpha Subunit, Immunohistochemistry, Magnetic Resonance Imaging, Xenograft Model Antitumor Assays, Reporter gene, Cell Hypoxia, PET, Oncology, Positron emission tomography, Tumor progression, 030220 oncology & carcinogenesis, Positron-Emission Tomography, Cancer research, MRI, Signal Transduction

Abstract

PURPOSE: The aim of this study was to characterize a cell-based model for the molecular study of hypoxia-inducible factor (HIF)-1? activity, in the context of hypoxia, by means of different imaging techniques. PROCEDURES: Engineered U251-HRE glioma cells were used to analyze the molecular mechanisms underlying HIF-1? activity in vitro in relation to luciferase expression. The same cells were orthotopically implanted in mice to evaluate tumor progression and hypoxia induction by bioluminescence imaging, fluorescence imaging, positron emission tomography (PET), and magnetic resonance imaging (MRI). RESULTS: In vitro analyses highlighted the relationship between HIF-1? and luciferase activity in hypoxic conditions and after pharmacological treatments in U251-HRE cells. Through in vivo studies, it was possible to assess hypoxia establishment in relation to tumor growth by optical imaging, PET and MRI. CONCLUSIONS: The findings of this study indicate that the U251-HRE orthotopic murine model can be used to reliably evaluate processes modulating HIF-1? activity, using both molecular and preclinical non-invasive imaging techniques.

Published

2013