Your search keyword '"Alice Bartolini"' showing total 30 results

1. A Subset of Colorectal Cancers with Cross-Sensitivity to Olaparib and Oxaliplatin

Author

Massimiliano Pagani, Gianluca Mauri, Salvatore Siena, Michael Linnebacher, Claudio Isella, Carola Negrino, Carlotta Cancelliere, Federica Di Nicolantonio, Enzo Medico, Alberto Bardelli, Andrea Cassingena, Giorgio Corti, Monica Montone, Gloria Mittica, Mariangela Russo, Annalisa Lorenzato, Andrea Sartore-Bianchi, Silvia Marsoni, Erika Durinikova, Pamela Arcella, Sabrina Arena, Nicole M. Reilly, Sergio Abrignani, Giuseppe Rospo, Alessio Amatu, Luca Lazzari, and Alice Bartolini

Subjects

Proto-Oncogene Proteins B-raf, 0301 basic medicine, Cancer Research, DNA repair, Colorectal cancer, Antineoplastic Agents, Mice, SCID, Poly(ADP-ribose) Polymerase Inhibitors, medicine.disease_cause, Poly (ADP-Ribose) Polymerase Inhibitor, Piperazines, Olaparib, Proto-Oncogene Proteins p21(ras), Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Maintenance therapy, Mice, Inbred NOD, Cell Line, Tumor, medicine, Animals, Humans, neoplasms, business.industry, Recombinational DNA Repair, medicine.disease, Xenograft Model Antitumor Assays, digestive system diseases, 3. Good health, Oxaliplatin, Gene Expression Regulation, Neoplastic, Treatment Outcome, 030104 developmental biology, Oncology, chemistry, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Mutation, PARP inhibitor, Cancer research, Phthalazines, KRAS, Colorectal Neoplasms, business, medicine.drug

Abstract

Purpose: Defects in the homologous recombination (HR) repair pathway are of clinical interest due to sensitivity of HR-deficient cells to PARP inhibitors. We were interested in defining PARP vulnerability in patients with metastatic colorectal cancer (mCRC) carrying KRAS and BRAF mutations who display poor prognosis, have limited therapeutic options, and represent an unmet clinical need. Experimental Design: We tested colorectal cancer cell lines, patient-derived organoids (PDO), and patient-derived xenografts (PDX) enriched for KRAS and BRAF mutations for sensitivity to the PARP inhibitor olaparib, and the chemotherapeutic agents oxaliplatin and 5-fluorouracil (5-FU). Genomic profiles and DNA repair proficiency of colorectal cancer models were compared with pharmacologic response. Results: Thirteen of 99 (around 13%) colorectal cancer cell lines were highly sensitive to clinically active concentrations of olaparib and displayed functional deficiency in HR. Response to PARP blockade was positively correlated with sensitivity to oxaliplatin in colorectal cancer cell lines as well as patient-derived organoids. Treatment of PDXs with olaparib impaired tumor growth and maintenance therapy with PARP blockade after initial oxaliplatin response delayed disease progression in mice. Conclusions: These results indicate that a colorectal cancer subset characterized by poor prognosis and limited therapeutic options is vulnerable to PARP inhibition and suggest that PDO-based drug-screening assays can be used to identify patients with colorectal cancer likely to benefit from olaparib. As patients with mCRC almost invariably receive therapies based on oxaliplatin, “maintenance” treatment with PARP inhibitors warrants further clinical investigation.

Published

2020

2. Molecular Landscape of Acquired Resistance to Targeted Therapy Combinations in BRAF-Mutant Colorectal Cancer

Author

Andrea Sartore-Bianchi, Margherita Gallicchio, Erin M. Sennott, Alice Bartolini, Federica Di Nicolantonio, Julieta Grasselli, Valentina Boscaro, Alberto Bardelli, Jan H.M. Schellens, Giovanni Crisafulli, Salvatore Siena, Jason T. Godfrey, Andrea Cassingena, Jeffrey A. Engelman, Genny Filiciotto, Giorgio Corti, Giulia Siravegna, Mauro Truini, Josep Tabernero, Giulia Marzolla, Michael Linnebacher, Carlotta Cancelliere, Sabrina Arena, René Bernards, Emanuele Valtorta, Ludovic Barault, Daniele Oddo, Michela Buscarino, Ryan B. Corcoran, Elena Elez, Robin M.J.M. van Geel, MUMC+: DA KFT Laboratorium (9), and RS: FHML non-thematic output

Subjects

Proto-Oncogene Proteins B-raf, 0301 basic medicine, MAPK/ERK pathway, Cancer Research, endocrine system diseases, Colorectal cancer, medicine.medical_treatment, Gene Dosage, colorectal cancer, Drug resistance, medicine.disease_cause, Article, BRAF, ERK inhibitors, Targeted therapy, 03 medical and health sciences, 0302 clinical medicine, cetuximab, medicine, Humans, neoplasms, EGFR inhibitors, drug resistance, Cetuximab, business.industry, BRAF, colorectal cancer, drug resistance, cetuximab, ERK inhibitors, Gene Amplification, Cancer, medicine.disease, digestive system diseases, 3. Good health, 030104 developmental biology, Oncology, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Cancer research, KRAS, Colorectal Neoplasms, business, Signal Transduction, medicine.drug

Abstract

Although recent clinical trials of BRAF inhibitor combinations have demonstrated improved efficacy in BRAF-mutant colorectal cancer, emergence of acquired resistance limits clinical benefit. Here, we undertook a comprehensive effort to define mechanisms underlying drug resistance with the goal of guiding development of therapeutic strategies to overcome this limitation. We generated a broad panel of BRAF-mutant resistant cell line models across seven different clinically relevant drug combinations. Combinatorial drug treatments were able to abrogate ERK1/2 phosphorylation in parental-sensitive cells, but not in their resistant counterparts, indicating that resistant cells escaped drug treatments through one or more mechanisms leading to biochemical reactivation of the MAPK signaling pathway. Genotyping of resistant cells identified gene amplification of EGFR, KRAS, and mutant BRAF, as well as acquired mutations in KRAS, EGFR, and MAP2K1. These mechanisms were clinically relevant, as we identified emergence of a KRAS G12C mutation and increase of mutant BRAF V600E allele frequency in the circulating tumor DNA of a patient at relapse from combined treatment with BRAF and MEK inhibitors. To identify therapeutic combinations capable of overcoming drug resistance, we performed a systematic assessment of candidate therapies across the panel of resistant cell lines. Independent of the molecular alteration acquired upon drug pressure, most resistant cells retained sensitivity to vertical MAPK pathway suppression when combinations of ERK, BRAF, and EGFR inhibitors were applied. These therapeutic combinations represent promising strategies for future clinical trials in BRAF-mutant colorectal cancer. Cancer Res; 76(15); 4504–15. ©2016 AACR.

Published

2016

3. Abstract B11: Whole-exome sequencing analysis of urine transrenal tumor DNA in metastatic colorectal cancer patients

Author

A. Martinetti, Alberto Bardelli, Silvia Marsoni, Giovanni Crisafulli, Alice Bartolini, Ludovic Barault, Federica Di Nicolatonio, Federica Morano, Andrea Sartore-Bianchi, Salvatore Siena, Andrea Cassingena, Monica Montone, Giulia Siravegna, Filippo Pietrantonio, and Benedetta Mussolin

Subjects

Cancer Research, business.industry, Colorectal cancer, Cancer, Urine, medicine.disease_cause, medicine.disease, chemistry.chemical_compound, Oncology, chemistry, Cancer research, Medicine, Digital polymerase chain reaction, KRAS, Liquid biopsy, business, Exome sequencing, DNA

Abstract

Background: The analysis of circulating free tumor DNA (ctDNA) in blood, commonly referred to as liquid biopsy, is being used to characterize patients with solid cancers. Tumor-specific genetic variants can also be present in DNA isolated from other body fluids such as urine. Unlike blood, urine sampling is noninvasive, can be self-performed, and allows recurrent longitudinal monitoring. The features of tumor DNA that clears from the glomerular filtration barrier (transrenal tumor DNA, hereafter trtDNA) are largely unexplored. Patients and Methods: Specimens were collected from 24 patients with KRAS or BRAF mutant metastatic colorectal cancer (mCRC). Driver mutations were assessed by droplet digital PCR (ddPCR) in ctDNA from plasma and trtDNA from urine. Whole-exome sequencing (WES) was performed in DNA isolated from tissue, plasma, and urine. Results: Out of the 24 CRC cases, only four had sufficient DNA to allow WES analyses in urine and plasma. We found that tumor alterations reside primarily in low-molecular-weight fragments. In patients where trtDNA was more than 2.69% of the urine-derived DNA, cancer-specific molecular alterations, mutational signatures, and copy number profiles identified in urine DNA are comparable with those detected in plasma ctDNA. Conclusions: With current technologies, WES analysis of trtDNA is feasible in a small fraction of mCRC patients. Tumor-related genetic information is mainly present in shorter DNA fragments. Although the limited amounts of trtDNA pose analytical challenges, enrichment of low-molecular-weight DNA and optimized computational tools improve detection of tumor-specific genetic information in urine. Citation Format: Giovanni Crisafulli, Benedetta Mussolin, Andrea Cassingena, Monica Montone, Alice Bartolini, Ludovic Barault, Antonio Martinetti, Federica Morano, Filippo Pietrantonio, Andrea Sartore-Bianchi, Salvatore Siena, Federica Di Nicolatonio, Silvia Marsoni, Alberto Bardelli, Giulia Siravegna. Whole-exome sequencing analysis of urine transrenal tumor DNA in metastatic colorectal cancer patients [abstract]. In: Proceedings of the AACR Special Conference on Advances in Liquid Biopsies; Jan 13-16, 2020; Miami, FL. Philadelphia (PA): AACR; Clin Cancer Res 2020;26(11_Suppl):Abstract nr B11.

Published

2020

4. Whole exome sequencing analysis of urine trans-renal tumour DNA in metastatic colorectal cancer patients

Author

Federica Morano, Antonia Martinetti, Federica Di Nicolantonio, Silvia Marsoni, Salvatore Siena, Alberto Bardelli, Ludovic Barault, Alice Bartolini, Andrea Sartore-Bianchi, Filippo Pietrantonio, Benedetta Mussolin, Giulia Siravegna, Giovanni Crisafulli, Andrea Cassingena, and Monica Montone

Subjects

Adult, Male, Proto-Oncogene Proteins B-raf, Cancer Research, Colorectal cancer, colorectal cancer, liquid biopsy, non-invasive, plasma ctDNA, urine trans-renal DNA, DNA Mutational Analysis, Mutant, Urine, medicine.disease_cause, Polymerase Chain Reaction, lcsh:RC254-282, Circulating Tumor DNA, Proto-Oncogene Proteins p21(ras), 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Exome Sequencing, Biomarkers, Tumor, medicine, Humans, Digital polymerase chain reaction, Liquid biopsy, Exome sequencing, Original Research, 030304 developmental biology, 0303 health sciences, business.industry, DNA, Neoplasm, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, 3. Good health, Oncology, chemistry, 030220 oncology & carcinogenesis, Mutation, Cancer research, Feasibility Studies, Female, KRAS, Colorectal Neoplasms, business, DNA

Abstract

Background The analysis of circulating free tumour DNA (ctDNA) in blood, commonly referred as liquid biopsy, is being used to characterise patients with solid cancers. Tumour-specific genetic variants can also be present in DNA isolated from other body fluids, such as urine. Unlike blood, urine sampling is non-invasive, can be self-performed, and allows recurrent longitudinal monitoring. The features of tumour DNA that clears from the glomerular filtration barrier, named trans-renal tumour DNA (trtDNA), are largely unexplored. Patients and methods Specimens were collected from 24 patients with KRAS or BRAF mutant metastatic colorectal cancer (mCRC). Driver mutations were assessed by droplet digital PCR (ddPCR) in ctDNA from plasma and trtDNA from urine. Whole exome sequencing (WES) was performed in DNA isolated from tissue, plasma and urine. Results Out of the 24 CRC cases, only four had sufficient DNA to allow WES analyses in urine and plasma. We found that tumour alterations primarily reside in low molecular weight fragments (less than 112 bp). In patients whose trtDNA was more than 2.69% of the urine derived DNA, cancer-specific molecular alterations, mutational signatures and copy number profiles identified in urine DNA are comparable with those detected in plasma ctDNA. Conclusions With current technologies, WES analysis of trtDNA is feasible in a small fraction of mCRC patients. Tumour-related genetic information is mainly present in low molecular weight DNA fragments. Although the limited amounts of trtDNA poses analytical challenges, enrichment of low molecular weight DNAs and optimised computational tools can improve the detection of tumour-specific genetic information in urine.

Published

2019

5. Acquired Resistance to the TRK Inhibitor Entrectinib in Colorectal Cancer

Author

Luca Novara, Giovanni Crisafulli, Salvatore Siena, Federica Di Nicolantonio, R. Patel, Alberto Bardelli, Giuseppe Rospo, Giorgio Corti, Giulia Siravegna, Ge Wei, Luca Lazzari, Andrea Bianchi, Sandra Misale, Mariangela Russo, Benedetta Mussolin, Nicholas Cam, Robert H. Shoemaker, Gang Li, Alice Bartolini, Robert A. Wild, and Shunqi Yan

Subjects

0301 basic medicine, Indazoles, Oncology, DROPLET DIGITAL PCR, COLON CANCER, REARRANGEMENTS, ENTRECTINIB, Colorectal cancer, Entrectinib, COLON CANCER, Drug resistance, medicine.disease_cause, Bioinformatics, Mice, 03 medical and health sciences, 0302 clinical medicine, Catalytic Domain, Cell Line, Tumor, medicine, Animals, Humans, Neoplasm, Receptor, trkA, Protein Kinase Inhibitors, Gene Rearrangement, Mutation, business.industry, REARRANGEMENTS, Cancer, Gene rearrangement, DROPLET DIGITAL PCR, Neoplastic Cells, Circulating, medicine.disease, 3. Good health, ENTRECTINIB, 030104 developmental biology, Oncology, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Trk receptor, Benzamides, Cancer research, Colorectal Neoplasms, business, Neoplasm Transplantation

Abstract

Entrectinib is a first-in-class pan-TRK kinase inhibitor currently undergoing clinical testing in colorectal cancer and other tumor types. A patient with metastatic colorectal cancer harboring an LMNA–NTRK1 rearrangement displayed a remarkable response to treatment with entrectinib, which was followed by the emergence of resistance. To characterize the molecular bases of the patient's relapse, circulating tumor DNA (ctDNA) was collected longitudinally during treatment, and a tissue biopsy, obtained before entrectinib treatment, was transplanted in mice (xenopatient), which then received the same entrectinib regimen until resistance developed. Genetic profiling of ctDNA and xenopatient samples showed acquisition of two point mutations in the catalytic domain of NTRK1, p.G595R and p.G667C. Biochemical and pharmacologic analysis in multiple preclinical models confirmed that either mutation renders the TRKA kinase insensitive to entrectinib. These findings can be immediately exploited to design next-generation TRKA inhibitors. Significance: We provide proof of principle that analyses of xenopatients (avatar) and liquid biopsies allow the identification of drug resistance mechanisms in parallel with clinical treatment of an individual patient. We describe for the first time that p.G595R and p.G667C TRKA mutations drive acquired resistance to entrectinib in colorectal cancers carrying NTRK1 rearrangements. Cancer Discov; 6(1); 36–44. ©2015 AACR. See related commentary by Okimoto and Bivona, p. 14. This article is highlighted in the In This Issue feature, p. 1

Published

2016

6. Trabectedin and olaparib in patients with advanced and non-resectable bone and soft-tissue sarcomas (TOMAS): an open-label, phase 1b study from the Italian Sarcoma Group

Author

Angelo Paolo Dei Tos, Rossella Bertulli, Alberto Pisacane, Dario Sangiolo, Stefano Ferrari, Massimo Aglietta, Francesco Tolomeo, Lorenzo D'Ambrosio, Luca Novara, Sandra Aliberti, R. Piana, Giovanni Grignani, Emanuela Marchesi, Giulia Chiabotto, Maurizio D'Incalci, Paola Boccone, Alice Bartolini, Alberto Bardelli, Emanuela Palmerini, Sara Miano, Silvia Stacchiotti, Massimo Zucchetti, Piero Picci, Ymera Pignochino, and Grignani G, D'Ambrosio L, Pignochino Y, Palmerini E, Zucchetti M, Boccone P, Aliberti S, Stacchiotti S, Bertulli R, Piana R, Miano S, Tolomeo F, Chiabotto G, Sangiolo D, Pisacane A, Dei Tos AP, Novara L, Bartolini A, Marchesi E, D'Incalci M, Bardelli A, Picci P, Ferrari S, Aglietta M.

Subjects

Male, 0301 basic medicine, Oncology, ope-label, Time Factors, Tabectedin, Soft Tissue Neoplasms, TOMAS, Piperazines, chemistry.chemical_compound, 0302 clinical medicine, Olaparib, Antineoplastic Combined Chemotherapy Protocols, sarcomas, Trabectedin, Osteosarcoma, Sarcoma, Middle Aged, Progression-Free Survival, Tabectedin, Olaparib, sarcomas, TOMAS, ope-label, bone and soft-tissue, phase 1b study, Italian Sarcoma Group, Italy, Tolerability, Response Evaluation Criteria in Solid Tumors, 030220 oncology & carcinogenesis, Female, medicine.drug, Adult, medicine.medical_specialty, phase 1b study, Trabectedin, olaparib, bone sarcoma, soft tissue sarcoma, advanced, non resectable, Bone Neoplasms, Poly(ADP-ribose) Polymerase Inhibitors, Neutropenia, 03 medical and health sciences, Internal medicine, medicine, Humans, Progression-free survival, Antineoplastic Agents, Alkylating, business.industry, Italian Sarcoma Group, medicine.disease, bone and soft-tissue, 030104 developmental biology, chemistry, Phthalazines, business, Febrile neutropenia

Abstract

Summary Background Trabectedin is an alkylating drug with a unique mechanism of action causing single-strand and double-strand DNA breaks that activate DNA damage-response pathways. Based on our preclinical data, we hypothesised that poly(ADP-ribose) polymerase 1 (PARP1) inhibitors might be an ideal partner of trabectedin and aimed to assess the safety, identify the recommended phase 2 dose, and explore preliminary signs of activity of trabectedin and olaparib combination treatment in patients with bone and soft-tissue sarcoma. Methods We did an open-label, multicentre, phase 1b study, recruiting patients from the national Italian sarcoma network aged 18 years and older with histologically confirmed bone and soft-tissue sarcoma progressing after standard treatments with Eastern Cooperative Oncology Group performance status of 1 or less. In a classic 3 + 3 design, patients received a 24 h infusion of trabectedin on day 1 and olaparib orally twice a day in 21-day cycles across six dose levels (trabectedin 0·675–1·3 mg/m2 every 3 weeks; olaparib 100–300 mg twice a day from day 1 to 21). Intermediate dose levels were permitted to improve safety and tolerability. The primary endpoint was determination of the recommended phase 2 dose (the maximum tolerated dose). Safety and antitumour activity were assessed in all patients who received at least one dose of the study drugs. We report the results of the dose-escalation and dose-expansion cohorts. The trial is still active but closed to enrolment, and follow-up for patients who completed treatment is ongoing. This trial is registered with ClinicalTrials.gov, number NCT02398058. Findings Between Nov 17, 2014, and Jan 30, 2017, of 54 patients assessed for eligibility, we enrolled 50 patients: 28 patients in the dose-escalation cohort and 22 patients in the dose-expansion cohort. Patients received a median of four cycles of treatment (IQR 2–6; range 1–17 [the patients who received the highest number of cycles are still on treatment]) with a median follow-up of 10 months (IQR 5–23). Considering all dose levels, the most common grade 3–4 adverse events were lymphopenia (32 [64%] of 50 patients), neutropenia (31 [62%]), thrombocytopenia (14 [28%]), anaemia (13 [26%]), hypophosphataemia (20 [40%]), and alanine aminotransferase concentration increase (9 [18%]). No treatment-related life-threatening adverse events or deaths occurred. One (2%) patient interrupted treatment without progression without reporting any specific toxicity. Observed dose-limiting toxicities were thrombocytopenia, neutropenia for more than 7 days, and febrile neutropenia. We selected intermediate dose level 4b (trabectedin 1·1 mg/m2 every 3 weeks plus olaparib 150 mg twice a day) as the recommended phase 2 dose. Seven (14%; 95% CI 6–27) of 50 patients achieved a partial response according to Response Evaluation Criteria In Solid Tumors 1.1. Interpretation Trabectedin and olaparib in combination showed manageable toxicities at active dose levels for both drugs. Preliminary data on antitumour activity are encouraging. Two dedicated phase 2 studies are planned to assess activity of this combination in both ovarian cancer (EudraCT2018-000230-35) and soft-tissue sarcomas. Funding Italian Association for Cancer Research, Italian Sarcoma Group, Foundation for Research on Musculoskeletal and Rare Tumors, and Italian Ministry of Health.

Published

2018

7. Radiologic and Genomic Evolution of Individual Metastases during HER2 Blockade in Colorectal Cancer

Author

Silvia Marsoni, Giovanni Crisafulli, Rebecca J. Nagy, Salvatore Siena, Erica Bonazzina, Daniele Regge, Emanuele Valtorta, Alice Vanzati, Alessio Amatu, Francesco Leone, Pamela Arcella, Giulia Siravegna, Luca Lazzari, Giorgio Corti, Mariangela Russo, Andrea Cassingena, Andrea Sartore-Bianchi, Monica Montone, Alice Bartolini, Sara Lonardi, Richard B. Lanman, Vittorina Zagonel, Giuseppe Rospo, Stephen R. Fairclough, Antonella Balsamo, Mauro Truini, Annalisa Lorenzato, Federica Di Nicolantonio, Giovanni Cappello, Alberto Bardelli, Andrea Bertotti, Angelo Vanzulli, Francesca Lodi, Cosimo Martino, Benedetta Mussolin, Livio Trusolino, and Silvia Ghezzi

Subjects

Male, 0301 basic medicine, Oncology, Cancer Research, Time Factors, Receptor, ErbB-2, Colorectal cancer, medicine.medical_treatment, DNA Mutational Analysis, clonal evolution, Mice, SCID, Somatic evolution in cancer, Targeted therapy, 0302 clinical medicine, Mice, Inbred NOD, Risk Factors, Antineoplastic Combined Chemotherapy Protocols, Tumor Cells, Cultured, HER2 amplification, Liver Neoplasms, targeted therapy, Magnetic Resonance Imaging, Progression-Free Survival, 3. Good health, Treatment Outcome, Italy, 030220 oncology & carcinogenesis, Disease Progression, Female, medicine.symptom, Colorectal Neoplasms, Signal Transduction, medicine.drug, medicine.medical_specialty, Class I Phosphatidylinositol 3-Kinases, Clinical Decision-Making, colorectal cancer, Mice, Transgenic, Adenocarcinoma, Lapatinib, resistance, Lesion, 03 medical and health sciences, Predictive Value of Tests, rapid autopsy, Internal medicine, medicine, Animals, Humans, Liquid biopsy, Protein Kinase Inhibitors, business.industry, Gene Amplification, Liquid Biopsy, ctDNA, Cell Biology, Trastuzumab, medicine.disease, Blockade, 030104 developmental biology, lapatinib, liquid biopsy, trastuzumab, Drug Resistance, Neoplasm, ras Proteins, Tomography, X-Ray Computed, business, Progressive disease

Abstract

Targeting HER2 is effective in 24% of ERBB2 amplified metastatic colorectal cancer; however, secondary resistance occurs in most of the cases. We studied the evolution of individual metastases during treatment to discover spatially resolved determinants of resistance. Circulating tumor DNA (ctDNA) analysis identified alterations associated with resistance in the majority of refractory patients. ctDNA profiles and lesion-specific radiographic reports revealed organ- or metastasis-private evolutionary patterns. When radiologic assessments documented progressive disease in target lesions, response to HER2 blockade was retained in other metastases. Genomic and functional analyses on samples and cell models from eight metastases of a patient co-recruited to a postmortem study unveiled lesion-specific evolutionary trees and pharmacologic vulnerabilities. Lesion size and contribution of distinct metastases to plasma ctDNA were correlated.

Published

2018

8. Abstract A120: Adaptive mutability of colorectal cancers in response to targeted therapies

Author

Salvatore Siena, Alessandro Magrì, Giovanni Crisafulli, Vito Amodio, Cortt G. Piett, Luca Novara, Zachary D. Nagel, Ivana Sarotto, Federica Di Nicolantonio, Alessio Amatu, Nicole M. Reilly, Alberto Sogari, Alberto Bardelli, Simona Lamba, Andrea Sartore-Bianchi, Andrea Bertotti, Alice Bartolini, Livio Trusolino, Sabrina Arena, and Mariangela Russo

Subjects

Genome instability, Cancer Research, education.field_of_study, DNA repair, Population, Cancer, Biology, medicine.disease, Somatic evolution in cancer, Oncology, MSH2, Cancer cell, medicine, Cancer research, DNA mismatch repair, education

Abstract

Success in eradicating human cancer with targeted therapies is limited by the emergence of secondary resistance. The prevalent view is that resistance is a fait accompli: when treatment is initiated, tumors already contain drug-resistant mutant cells. However, when cancer cells are challenged with targeted agents, the emergence of drug tolerant ‘persister’ cell population is often observed. Persisters survive exposure to targeted therapies through non-genetic, poorly understood mechanisms, and constitute a reservoir from which genetically divergent, drug-resistant derivatives eventually emerge. Analogously, when bacteria are exposed to stress, such as antibiotic treatment, persister cells can survive and, by switching from high-fidelity to low-fidelity DNA replication process, increase transiently their mutation rate (adaptive mutability), thus improving chances of survival. We used colorectal cancer (CRC) as model system to explore the hypothesis that, in addition to pre-existing drug resistant cells, resistance to targeted therapies could be fostered by a transient increase in genomic instability during treatment, leading to de novo genetic alterations. We found that, when exposed to EGFR and/or BRAF inhibition, mismatch repair proficient (MMRp) CRC cell lines exhibited a down-modulation of MMR and Homologous Recombination (HR) DNA repair genes, and a concomitant up-regulation of error-prone polymerases, resulting in reduced MMR and HR proficiency. Therapy-induced modulation of DNA repair genes was transient and returned to initial levels upon removal of the drugs, or when the cells developed permanent resistance to targeted agents. Notably, MLH1 and MSH2 MMR genes were down-regulated in patients-derived xenografts and tissue samples obtained at clinical response (minimal residual disease) compared to pre-treatment samples, confirming the clinical relevance of our findings. Activation of error-prone polymerases was associated with increased ROS production and accumulation of DNA damage marker γ-H2AX, in a time- a dose-dependent manner upon drug administration. The combination of DNA repair down-modulation and error-prone polymerases upregulation increases mutagenic ability and triggers microsatellite instability under drug-induced stress in CRC cells. Our results demonstrate that cancer cells, like unicellular organisms, evade therapeutic pressures by enhancing mutability. The notion that cancer cells exposed to targeted therapies activate a stress-induced adaptive mutability process may prompt the design of novel therapeutic strategies aimed at interfering with clonal evolution, reducing the generation of new variants during therapeutic treatment. Citation Format: MARIANGELA RUSSO, Giovanni Crisafulli, Alberto Sogari, Nicole Megan Reilly, Sabrina Arena, Simona Lamba, Alice Bartolini, Vito Amodio, Alessandro Magrì, Luca Novara, Ivana Sarotto, Zachary Nagel, Cortt Piett, Alessio Amatu, Andrea Sartore-Bianchi, Salvatore Siena, Andrea Bertotti, Livio Trusolino, Federica Di Nicolantonio, Alberto Bardelli. Adaptive mutability of colorectal cancers in response to targeted therapies [abstract]. In: Proceedings of the AACR-NCI-EORTC International Conference on Molecular Targets and Cancer Therapeutics; 2019 Oct 26-30; Boston, MA. Philadelphia (PA): AACR; Mol Cancer Ther 2019;18(12 Suppl):Abstract nr A120. doi:10.1158/1535-7163.TARG-19-A120

Published

2019

9. A Genomic Analysis Workflow for Colorectal Cancer Precision Oncology

Author

Federica Di Nicolantonio, Alberto Bardelli, Salvatore Siena, Alice Bartolini, Monica Montone, Benedetta Mussolin, Giulia Siravegna, Ludovic Barault, Giovanni Crisafulli, Claudio Isella, Michela Buscarino, Luca Novara, Carola Negrino, Enzo Medico, Giorgio Corti, Giuseppe Rospo, and S. Marsoni

Subjects

Proto-Oncogene Proteins B-raf, DNA Copy Number Variations, Genotyping Techniques, Bioinformatics, Receptor, ErbB-2, Colorectal cancer, Sequencing data, Gene Dosage, Genomics, Computational biology, DNA sequencing, Circulating Tumor DNA, Workflow, Proto-Oncogene Proteins p21(ras), 03 medical and health sciences, 0302 clinical medicine, Next generation sequencing, Antineoplastic Combined Chemotherapy Protocols, Biomarkers, Tumor, medicine, Humans, Precision Medicine, Predictive biomarker, business.industry, Patient Selection, Gastroenterology, High-Throughput Nucleotide Sequencing, Lapatinib, Genetic alterations, IDEA, Trastuzumab, Prognosis, medicine.disease, 3. Good health, Treatment Outcome, Italy, Oncology, Precision oncology, Clinical question, 030220 oncology & carcinogenesis, Mutation, 030211 gastroenterology & hepatology, Neoplasm Recurrence, Local, Colorectal Neoplasms, business

Abstract

Background The diagnosis of colorectal cancer (CRC) is routinely accomplished through histopathologic examination. Prognostic information and treatment decisions are mainly determined by TNM classification, first defined in 1968. In the last decade, patient-specific CRC genomic landscapes were shown to provide important prognostic and predictive information. Therefore, there is a need for developing next generation sequencing (NGS) and bioinformatic workflows that can be routinely used for the assessment of prognostic and predictive biomarkers. Materials and Methods To foster the application of genomics in the clinical management of CRCs, the IDEA workflow has been built to easily adapt to the availability of patient specimens and the clinical question that is being asked. Initially, IDEA deploys ad-hoc NGS assays to interrogate predefined genomic target sequences (from 600 kb to 30 Mb) with optimal detection sensitivity. Next, sequencing data are processed through an integrated bioinformatic pipeline to assess single nucleotide variants, insertions and deletions, gene copy-number alterations, and chromosomal rearrangements. The overall results are gathered into a user-friendly report. Results We provide evidence that IDEA is capable of identifying clinically relevant molecular alterations. When optimized to analyze circulating tumor DNA, IDEA can be used to monitor response and relapse in the blood of patients with metastatic CRC receiving targeted agents. IDEA detected primary and secondary resistance mechanisms to ERBB2 blockade including sub-clonal RAS and BRAF mutations. Conclusions The IDEA workflow provides a flexible platform to integrate NGS and bioinformatic tools for refined diagnosis and management of patients with advanced CRC.

Published

2019

10. BRAF V600E Is a Determinant of Sensitivity to Proteasome Inhibitors

Author

Federica Di Nicolantonio, Alberto Bardelli, Enzo Medico, Davide Zecchin, Sabrina Arena, Margherita Gallicchio, Miriam Martini, Alice Bartolini, Valentina Boscaro, Carlotta Cancelliere, Emily Crowley, and Ludovic Barault

Subjects

Cancer Research, Indoles, Colorectal cancer, medicine.disease_cause, Bortezomib, chemistry.chemical_compound, 0302 clinical medicine, Cluster Analysis, Telomerase, Sulfonamides, 0303 health sciences, biology, BRAF, Proteasome inhibitors, cancer mutations, EGFR, Pharmacogenomics, 3. Good health, Oncology, 030220 oncology & carcinogenesis, Female, KRAS, Signal Transduction, medicine.drug, Proto-Oncogene Proteins B-raf, Genotype, Antineoplastic Agents, 03 medical and health sciences, Cell Line, Tumor, Biomarkers, Tumor, medicine, Humans, PTEN, neoplasms, 030304 developmental biology, Cancer, medicine.disease, Xenograft Model Antitumor Assays, Carfilzomib, digestive system diseases, 14-3-3 Proteins, Proteasome, chemistry, Drug Resistance, Neoplasm, Exoribonucleases, Mutation, biology.protein, Proteasome inhibitor, Cancer research, Drug Screening Assays, Antitumor

Abstract

A critical step toward defining tailored therapy in patients with cancer is the identification of genetic interactions that may impair—or boost—the efficacy of selected therapeutic approaches. Cell models able to recapitulate combinations of genetic aberrations are important to find drug–genotype interactions poorly affected by the heterogeneous genetics of human tumors. In order to identify novel pharmacogenomic relationships, we employed an isogenic cell panel that reconstructs cancer genetic scenarios. We screened a library of 43 compounds in human hTERT-HME1 epithelial cells in which PTEN or RB1 were silenced in combination with the targeted knockin of cancer-associated mutations in EGFR, KRAS, BRAF, or PIK3CA oncogenes. Statistical analysis and clustering algorithms were applied to display similar drug response profiles and mutation-specific patterns of activity. From the screen, we discovered that proteasome inhibitors show selectivity toward BRAF V600E–mutant cells, irrespective of PTEN or RB1 expression. Preferential targeting of BRAF-mutant cells by proteasome inhibitors was corroborated in a second BRAF V600E isogenic model, as well as in a panel of colorectal cancer cell lines by the use of the proteasome inhibitor carfilzomib. Notably, carfilzomib also showed striking in vivo activity in a BRAF-mutant human colorectal cancer xenograft model. Vulnerability to proteasome inhibitors is dependent on persistent BRAF signaling, because BRAF V600E blockade by PLX4720 reversed sensitivity to carfilzomib in BRAF-mutant colorectal cancer cells. Our findings indicated that proteasome inhibition might represent a valuable targeting strategy in BRAF V600E–mutant colorectal tumors. Mol Cancer Ther; 12(12); 2950–61. ©2013 AACR.

Published

2013

11. Inactivation of DNA repair triggers neoantigen generation and impairs tumour growth

Author

Giulia Lerda, Federica Morano, Salvatore Siena, Mariangela Russo, Alice Bartolini, Ludovic Barault, Federica Maione, Alessandro Magrì, Filippo Pietrantonio, Giovanni Germano, Enrico Giraudo, Monica Montone, Benedetta Mussolin, Maurizio D'Incalci, Silvia Marsoni, Federica Di Nicolantonio, Giulia Siravegna, Giovanni Crisafulli, Alberto Bardelli, Andrea Sartore-Bianchi, Armando Orlandi, Giuseppe Rospo, Filippo de Braud, Roberta Frapolli, Nabil Amirouchene-Angelozzi, and Simona Lamba

Subjects

Male, 0301 basic medicine, Antibodies, Neoplasm, DNA repair, Receptors, Antigen, T-Cell, cancer genetics, Mice, SCID, MLH1, DNA Mismatch Repair, Mice, 03 medical and health sciences, Antigen, Antigens, Neoplasm, Mice, Inbred NOD, Cell Line, Tumor, Neoplasms, medicine, Animals, cancer, Multidisciplinary, cancer, cancer genetics, Cell Proliferation, Genetics, Mice, Inbred BALB C, Settore MED/06 - ONCOLOGIA MEDICA, Multidisciplinary, biology, Cancer, medicine.disease, neoantigen, digestive system diseases, 3. Good health, Mice, Inbred C57BL, Transplantation, 030104 developmental biology, Cancer cell, Cancer research, biology.protein, Female, Tumor Escape, DNA mismatch repair, Immunotherapy, Antibody, MutL Protein Homolog 1

Abstract

Molecular alterations in genes involved in DNA mismatch repair (MMR) promote cancer initiation and foster tumour progression. Cancers deficient in MMR frequently show favourable prognosis and indolent progression. The functional basis of the clinical outcome of patients with tumours that are deficient in MMR is not clear. Here we genetically inactivate MutL homologue 1 (MLH1) in colorectal, breast and pancreatic mouse cancer cells. The growth of MMR-deficient cells was comparable to their proficient counterparts in vitro and on transplantation in immunocompromised mice. By contrast, MMR-deficient cancer cells grew poorly when transplanted in syngeneic mice. The inactivation of MMR increased the mutational burden and led to dynamic mutational profiles, which resulted in the persistent renewal of neoantigens in vitro and in vivo, whereas MMR-proficient cells exhibited stable mutational load and neoantigen profiles over time. Immune surveillance improved when cancer cells, in which MLH1 had been inactivated, accumulated neoantigens for several generations. When restricted to a clonal population, the dynamic generation of neoantigens driven by MMR further increased immune surveillance. Inactivation of MMR, driven by acquired resistance to the clinical agent temozolomide, increased mutational load, promoted continuous renewal of neoantigens in human colorectal cancers and triggered immune surveillance in mouse models. These results suggest that targeting DNA repair processes can increase the burden of neoantigens in tumour cells; this has the potential to be exploited in therapeutic approaches.

Published

2017

12. Emergence of MET hyper-amplification at progression to MET and BRAF inhibition in colorectal cancer

Author

Giovanni Fucà, Michela Buscarino, Daniele Oddo, Alice Bartolini, Annunziata Gloghini, Filippo de Braud, Philip D Dunne, Chiara Costanza Volpi, Federica Di Nicolantonio, Emanuele Valtorta, Monica Niger, Giulia Siravegna, Alberto Bardelli, Federica Morano, Giovanni Crisafulli, Antonia Martinetti, Giorgio Corti, Filippo Pietrantonio, Maria Di Bartolomeo, Giuseppe Rospo, Claudio Vernieri, Benedetta Mussolin, Simona Lamba, and Rosa Berenato

Subjects

0301 basic medicine, Oncology, Cancer Research, Indoles, Pyridines, Colorectal cancer, Drug resistance, Prostate cancer, Fatal Outcome, 0302 clinical medicine, Antineoplastic Combined Chemotherapy Protocols, Vemurafenib, Sulfonamides, DNA, Neoplasm, Middle Aged, Proto-Oncogene Proteins c-met, 3. Good health, 030220 oncology & carcinogenesis, MET, Disease Progression, Liver cancer, medicine.drug, Proto-Oncogene Proteins B-raf, medicine.medical_specialty, colorectal cancer, BRAF, Cell Line, 03 medical and health sciences, Breast cancer, SDG 3 - Good Health and Well-being, Internal medicine, Journal Article, medicine, Humans, crizotinib, drug resistance, Oncogene, target therapy, Rectal Neoplasms, business.industry, Gene Amplification, medicine.disease, 030104 developmental biology, Drug Resistance, Neoplasm, Pyrazoles, Skin cancer, Translational Therapeutics, business

Abstract

BACKGROUND: Combined MET and BRAF inhibition showed clinical benefit in a patient with rectal cancer carrying BRAF(V600E) and MET amplification. However after 4 months, acquired resistance emerged and the patient deceased shortly after disease progression. The mechanism of resistance to this drug combination is unknown.METHODS: We analysed plasma circulating tumour DNA obtained at progression by exome sequencing and digital PCR. MET gene and mRNA in situ hybridisation analyses in two bioptic specimens obtained at progression were used to confirm the plasma data.RESULTS: We identified in plasma MET gene hyper-amplification as a potential mechanism underlying therapy resistance. Increased MET gene copy and transcript levels were detected in liver and lymph node metastatic biopsies. Finally, transduction of MET in BRAF mutant colorectal cancer cells conferred refractoriness to BRAF and MET inhibition.CONCLUSIONS: We identified in a rectal cancer patient MET gene hyper-amplification as mechanism of resistance to dual BRAF and MET inhibition.

Published

2017

13. Acquired RAS or EGFR mutations and duration of response to EGFR blockade in colorectal cancer

Author

Agostino Ponzetti, Giulia Siravegna, Salvatore Siena, Beatriz Bellosillo, Federica Baldi, Filippo Pietrantonio, Federica Di Nicolantonio, Luca Lazzari, Alberto Bardelli, Benedetta Mussolin, Sabrina Arena, Giovanni Crisafulli, Alice Bartolini, Emanuele Valtorta, Beth O. Van Emburgh, Michela Buscarino, Giorgio Corti, Giovanni Germano, Andrea Sartore-Bianchi, Joan Albanell, Clara Montagut, and Joana Vidal

Subjects

0301 basic medicine, Male, Colorectal cancer, General Physics and Astronomy, CLONAL DYNAMICS, LUNG-CANCER, CELL-LINES, RESISTANCE, EVOLUTION, KRAS, HETEROGENEITY, ALIGNMENT, THERAPY, TUMORS, medicine.disease_cause, Somatic evolution in cancer, 0302 clinical medicine, Antineoplastic Agents, Immunological, Epidermal growth factor receptor, Aged, 80 and over, Mutation, Multidisciplinary, Cetuximab, Middle Aged, 3. Good health, ErbB Receptors, Còlon -- Càncer, 030220 oncology & carcinogenesis, Female, Colorectal Neoplasms, medicine.drug, Adult, Science, Biology, General Biochemistry, Genetics and Molecular Biology, Article, Clonal Evolution, 03 medical and health sciences, medicine, Panitumumab, Humans, Aged, General Chemistry, Genes, erbB-1, medicine.disease, Blockade, 030104 developmental biology, Genes, ras, Drug Resistance, Neoplasm, Immunology, Cancer research, biology.protein

Abstract

Blockade of the epidermal growth factor receptor (EGFR) with the monoclonal antibodies cetuximab or panitumumab is effective in a subset of colorectal cancers (CRCs), but the emergence of resistance limits the efficacy of these therapeutic agents. At relapse, the majority of patients develop RAS mutations, while a subset acquires EGFR extracellular domain (ECD) mutations. Here we find that patients who experience greater and longer responses to EGFR blockade preferentially develop EGFR ECD mutations, while RAS mutations emerge more frequently in patients with smaller tumour shrinkage and shorter progression-free survival. In circulating cell-free tumour DNA of patients treated with anti-EGFR antibodies, RAS mutations emerge earlier than EGFR ECD variants. Subclonal RAS but not EGFR ECD mutations are present in CRC samples obtained before exposure to EGFR blockade. These data indicate that clonal evolution of drug-resistant cells is associated with the clinical outcome of CRC patients treated with anti-EGFR antibodies., Some colorectal cancer patients respond well to treatment with anti-EGFR antibodies, however response is almost invariably followed by acquired resistance. Here, the authors show that patients with shorter responses acquire RAS mutations, while those relapsing later preferentially develop mutations in the extracellular domain of EGFR.

Published

2016

14. Abstract B069: Temozolomide drives mismatch repair deficiency and fosters neoantigen generation in tumor cells

Author

Maurizio D'Incalci, Enrico Giraudo, Giovanni Crisafulli, Giovanni Randon, Andrea Satore-Bianchi, Nabil Amirouchene Angelozzi, Federica Di Nicolantonio, Alberto Bardelli, Simona Lamba, Alessandro Magrì, Salvatore Siena, Silvia Marsoni, Roberta Frappolli, Monica Montone, Giulia Lerda, Armando Orlandi, Ludovic Barault, Vito Amodio, Giuseppe Rospo, Alice Bartolini, Filippo de Braud, Filippo Pietrantonio, Benedetta Mussolin, Giulia Siravegna, Carlotta Cancelliere, Federica Maione, and Giovanni Grmano

Subjects

Cancer Research, Temozolomide, business.industry, medicine.medical_treatment, Immunology, Cancer, medicine.disease, Immune checkpoint, MSH6, Cancer immunotherapy, MSH2, Cancer cell, Cancer research, Medicine, DNA mismatch repair, business, medicine.drug

Abstract

The tumor mutational burden affects immune surveillance and is associated with response to immune checkpoint blockade. We recently reported that inactivation of the DNA mismatch repair (MMR) pathway in cancer cells increases the mutational burden and modifies the neoantigen landscapes of cancer cells leading to their increased recognition by the immune system. We designed a pharmacologic screening to identify FDA-approved drugs capable of differentially affecting cancer cells MMR proficient and deficient. MMR-deficienT-cells displayed lower sensitivity to the alkylating agent Temozolomide (TMZ) and to the antimetabolite 6-Thioguanine (6-TG). Cells lacking key elements of the MMR pathway such as MutL homolog1, MutS homolog2 (MSH2) or MutS homolog 6 (MSH6), displayed an increased resistance to both TMZ and 6-TG. Next we treated two mouse colorectal cancer cell lines (MC38 and CT26) with TMZ until resistant populations emerged. MC38 cells acquired TMZ resistance through inactivation of the MMR pathway. Bioinformatic analysis revealed that these cells had higher numbers of neoantigens compared to parental cells. Importantly, when MC38 MMRd cells were injected in syngeneic mice, they were unable to form tumors. On the contrary, CT26 cells that acquired TMZ-resistance through other mechanisms, efficiently formed tumors in mice. Therefore, TMZ-induced MMR inactivation, and not TMZ treatment per se, triggered immune surveillance. To assess whether results obtained in mouse cancer models might translate to human disease, we tested TMZ in 47 molecularly annotated colorectal cancer (CRC) cancer cell lines. Only MMR-proficienT-cells and cells in which O6-methylguanine-DNA- methyltransferase (MGMT, the enzyme responsible for repairing the DNA adducts formed by TMZ) was not expressed were sensible to TMZ. Ten sensitive cell lines were chronically treated with TMZ until resistant populations emerged; we found that MGMT re-expression and loss of MMR genes were the main mechanisms of acquired resistance. In agreement with in vitro observations, analysis of biopsies from eight patients relapsing upon TMZ-based therapeutic regimens revealed MGMT re-expression (5 patients) and MMR genes mutations (i.e., MSH2 or MSH6) as main resistance mechanism. In both cell lines and biopsies, MMR inactivation led to increased mutational load and, consequently, to higher levels of predicted neo-antigens, suggesting an augmented immunogenicity. These preclinical data led to the clinical trial Arethusa (NCT03519412; https://clinicaltrials.gov/ct2/show/NCT03519412). Within Arethusa MMR-proficient patients will be tested for (MGMT) expression (IHC) and then for MGMT promoter methylation. MGMT negative patients will be treated with temozolomide (TMZ). Patients progressing under temozolomide will be tested for tumor mutational burden (TMB) and proceed to pembrolizumab if TMB is > 20 mutations/Mb. The primary study hypothesis is that tumors with acquired resistance to temozolomide might become hypermutated and could be sensitive to the anti PD-1 antibody, pembrolizumab. Citation Format: Vito Amodio, Giovanni Grmano, Ludovic Barault, Simona Lamba, Giuseppe Rospo, Alessandro Magrì, Federica Maione, Giovanni Crisafulli, Carlotta Cancelliere, Giulia Lerda, Alice Bartolini, Giulia Siravegna, Benedetta Mussolin, Roberta Frappolli, Monica Montone, Giovanni Randon, Filippo de Braud, Nabil Amirouchene Angelozzi, Silvia Marsoni, Maurizio D'Incalci, Armando Orlandi, Enrico Giraudo, Andrea Satore-Bianchi, Salvatore Siena, Filippo Pietrantonio, Federica Di Nicolantonio, Alberto Bardelli. Temozolomide drives mismatch repair deficiency and fosters neoantigen generation in tumor cells [abstract]. In: Proceedings of the Fourth CRI-CIMT-EATI-AACR International Cancer Immunotherapy Conference: Translating Science into Survival; Sept 30-Oct 3, 2018; New York, NY. Philadelphia (PA): AACR; Cancer Immunol Res 2019;7(2 Suppl):Abstract nr B069.

Published

2019

15. Abstract 2848: Radiographic and genomic evolution of individual metastases during HER2 blockade in colorectal cancer

Author

Alice Vanzati, Erica Bonazzina, Cosimo Martino, Salvatore Siena, Giovanni Crisafulli, Francesco Leone, Richard B. Lanman, Giorgio Corti, Andrea Sartore-Bianchi, Sara Lonardi, Mariangela Russo, Livio Trusolino, Vittorina Zagonel, Silvia Ghezzi, Luca Lazzari, Alessio Amatu, Andrea Cassingena, Angelo Vanzulli, Alice Bartolini, Giulia Siravegna, Monica Montone, Benedetta Mussolin, Antonella Balsamo, Silvia Marsoni, Federica Di Nicolantonio, Alberto Bardelli, Francesca Lodi, Pamela Arcella, Daniele Regge, Rebecca Nagy, Emanuele Valtorta, Giovanni Cappello, Mauro Truini, and Andrea Bertotti

Subjects

Oncology, Cancer Research, medicine.medical_specialty, business.industry, Colorectal cancer, Cancer, medicine.disease, Lapatinib, Blockade, ERBB2 Amplification, Trastuzumab, Circulating tumor DNA, Precision oncology, Internal medicine, medicine, skin and connective tissue diseases, business, medicine.drug

Abstract

Targeting HER2 with trastuzumab and lapatinib is effective in ERBB2 amplified metastatic colorectal cancer (mCRC). Although at least 30% of the patients initially respond, secondary resistance occurs in most of the cases. Since the drivers of secondary resistance to trastuzumab and lapatinib in ERBB2 amplified mCRC are unknown, we exploited longitudinal plasma collections and patient-derived cell models to define the molecular bases of resistance to HER2 blockade. Levels of ERBB2 amplification in plasma circulating tumor DNA (ctDNA) paralleled response and relapse. The emergence of EGFR, ERBB2, RAS, BRAF and PIK3CA variants in ctDNA was associated with resistance. Radiographic measurements of individual metastases coupled with longitudinal liquid biopsies unveiled lesion-specific patterns of heterogeneous response in several patients. Phylogenetic tracking and functional analyses on tissue samples and patient-derived cell models established from eight metastases of a single case revealed new druggable oncogenic dependencies and genomic evolution associated with resistance. These data highlight the relevance of coupling imaging and liquid biopsies analyses in precision oncology and provide the rationale for additional lines of therapies in HER2 positive mCRC relapsing upon HER2 blockade. Citation Format: Giulia Siravegna, Luca Lazzari, Andrea Sartore-Bianchi, Giovanni Crisafulli, Benedetta Mussolin, Andrea Cassingena, Cosimo Martino, Richard Lanman, Rebecca Nagy, Giorgio Corti, Alice Bartolini, Pamela Arcella, Monica Montone, Francesca Lodi, Alice Vanzati, Emanuele Valtorta, Giovanni Cappello, Andrea Bertotti, Sara Lonardi, Vittorina Zagonel, Francesco Leone, Mariangela Russo, Antonella Balsamo, Mauro Truini, Federica Di Nicolantonio, Alessio Amatu, Erica Bonazzina, Silvia Ghezzi, Daniele Regge, Angelo Vanzulli, Livio Trusolino, Salvatore Siena, Silvia Marsoni, Alberto Bardelli. Radiographic and genomic evolution of individual metastases during HER2 blockade in colorectal cancer [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2018; 2018 Apr 14-18; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2018;78(13 Suppl):Abstract nr 2848.

Published

2018

16. Abstract 5723: Inactivation of DNA repair triggers neoantigen generation and impairs tumor growth

Author

Salvatore Siena, Filippo de Braud, Enrico Giraudo, Mariangela Russo, Federica Maione, Benedetta Mussolin, Ludovic Barault, Giulia Siravegna, Nabil Amirouchene-Angelozzi, Giovanni Germano, Andrea Sartore-Bianchi, Roberta Frapolli, Alice Bartolini, Federica Morano, Monica Montone, Armando Orlandi, Maurizio D'Incalci, Giuseppe Rospo, Giulia Lerda, Alberto Bardelli, Giovanni Crisafulli, Alessandro Magrì, Silvia Marsoni, Simona Lamba, Federica DiNicolantonio, and Filippo Pietrantonio

Subjects

0301 basic medicine, Cancer Research, DNA repair, Cancer, Biology, MLH1, medicine.disease, Immune checkpoint, Transplantation, 03 medical and health sciences, 030104 developmental biology, Immune system, Oncology, Cancer cell, Cancer research, medicine, DNA mismatch repair

Abstract

Colorectal, ovarian, endometrial and other tumors carrying defects in DNA mismatch repair often show favorable prognosis and indolent progression. The genomes of these tumors bear hundreds of thousands of somatic mutations, a feature which fosters cancer progression and might lead to rapid evolution of resistance to targeted therapies. Recent evidences that a subset of MSI (microsatellite instable) tumors respond prominently to immune checkpoint blockade led to the hypothesis that the presence of high number of somatic mutations may be responsible for effective immune-surveillance. However, several reports indicate that a relevant fraction of hyper-mutated tumors have unfavorable prognosis and do not respond to immune-modulators. To understand the molecular and functional bases of response to immune checkpoint inhibitors, we genetically inactivated MutL homolog 1 (MLH1) in colorectal, breast and pancreatic mouse cancer cells. The growth of MMR deficient cells was comparable to their proficient counterparts in vitro and upon transplantation in immune-compromised mice. However, isogenic MMR deficient cancer cells, acquiring alterations over time, were unable to form tumors when injected subcutaneously or orthotopically in syngeneic mouse models according to cell-passage number. Moreover, we found that MMR-driven dynamic generation of neoantigens, when restricted to a clonal population, further increases immune detection. Mechanistically, MLH1 inactivation increased the mutational burden and led to dynamic mutational profiles, resulting in persistent renewal of neoantigens in vitro and in vivo, while control cells exhibited stable mutational loads and neoantigen profiles over time. These results led us hypothesize that enforced increase of the number of mutations in cancer cells could restrict cancer growth and might be beneficial for therapeutic purposes. We therefore performed a pharmacological screen to identify agents capable of permanent inactivation of MMR in colorectal, breast and PDAC cancer cells. We found that temozolomide triggers MLH1 inactivation in cancer cells that -as a result- are unable to form tumors in syngeneic animals. Genomic analysis of temozolomide resistant cells revealed that fluctuating levels of neoantigens, rather than the absolute number of mutations, might be critical to provoke immune surveillance. Overall, these results provide the rationale for developing innovative anticancer therapies based on inhibition of DNA repair mechanisms. Citation Format: Giovanni Germano, Simona Lamba, Giuseppe Rospo, Ludovic Barault, Alessandro Magri', Federica Maione, Mariangela Russo, Giovanni Crisafulli, Alice Bartolini, Giulia Lerda, Giulia Siravegna, Benedetta Mussolin, Roberta Frapolli, Monica Montone, Federica Morano, Filippo de Braud, Nabil Amirouchene-Angelozzi, Silvia Marsoni, Maurizio D'Incalci, Armando Orlandi, Enrico Giraudo, Andrea Sartore-Bianchi, Salvatore Siena, Filippo Pietrantonio, Federica DiNicolantonio, Alberto Bardelli. Inactivation of DNA repair triggers neoantigen generation and impairs tumor growth [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2018; 2018 Apr 14-18; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2018;78(13 Suppl):Abstract nr 5723.

Published

2018

17. Abstract 2743: Accumulation of predicted neoantigens by MMR deficiency triggered by temozolomide treatment of human colorectal cancer

Author

Giulia Siravegna, Armando Orlandi, Alessandro Magrì, Filippo de Braud, Giovanni Crisafulli, Chiara Falcomatà, Alice Bartolini, Salvatore Siena, Carlotta Cancelliere, Andrea Sartore-Bianchi, Roberta Frapolli, Enrico Giraudo, Giovanni Randon, Giuseppe Rospo, Monica Montone, Giulia Lerda, Nabil Amirouchene-Angelozzi, Mariangela Russo, Maurizio D'Incalci, Federica Di Nicolantonio, Silvia Marsoni, Giovanni Germano, Alberto Bardelli, Simona Lamba, Ludovic Barault, Federica Maione, Filippo Pietrantonio, and Benedetta Mussolin

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Temozolomide, Methyltransferase, Colorectal cancer, business.industry, Dacarbazine, Cancer, medicine.disease, digestive system diseases, MSH6, MSH2, Internal medicine, medicine, DNA mismatch repair, business, medicine.drug

Abstract

Recent clinical trials have reported that alkylating agents, such as dacarbazine and temozolomide (TMZ) are effective in 10-15% metastatic colorectal cancer (mCRC) patients. In a retrospective analysis of 105 mCRC patients enrolled in clinical trials with alkylating agents, we saw that O6-methylguanine-DNA- methyltransferase (MGMT, the enzyme responsible for repairing drug induced DNA adducts), promoter methylation and protein status could identify a patient subgroup more likely to benefit from these drugs. However, the time to progression of patients treated with alkylating agents was limited by the onset of resistance. In order to identify determinants of response to these agents, we tested TMZ in a collection of 47 molecularly annotated CRC cell lines. We found that only cells displaying mismatch repair (MMR) proficiency as well as promoter methylation and transcriptional silencing of MGMT were sensitive to the treatment. Sensitive cells were chronically exposed to TMZ until the emergence of resistance occurred in seven out of ten models. We identified the mechanisms of acquired drug resistance to be either re-expression of MGMT and/or mutations in MMR genes. Biopsies of eight patients, relapsing upon TMZ based regimen after a long lasting clinical benefit (>3 months), were analyzed for MGMT re-expression and for exome or target panel next generation sequencing. These analyses confirmed the results found in preclinical models: five biopsies showed MGMT re-expression, two demonstrated mutations in the MMR genes (i.e. MSH6 or MSH2), and one displayed a mutation in BRCA2. Interestingly, biopsies and cell lines in which resistance was associated to alterations in DNA repair genes displayed increased mutational loads compared to pre-treatment samples. Despite the absence of the microsatellite switch commonly found in MMR deficient driven cancer, follow up over time in absence of drug of a subset of resistant cell line models demonstrated that those which displayed a mutation in the MMR had an accumulation of predicted neo-antigens, suggesting an increased immunogenicity. This work has implications for the design of future trials incorporating TMZ as part of a multi-modality strategy for treating MGMT deficient and MMR proficient CRC. Citation Format: Ludovic Barault, Giovanni Germano, Simona Lamba, Giuseppe Rospo, Alessandro Magri, Federica Maione, Mariangela Russo, Giovanni Crisafulli, Chiara Falcomatà, Carlotta Cancelliere, Alice Bartolini, Giulia Lerda, Giulia Siravegna, Benedetta Mussolin, Roberta Frapolli, Monica Montone, Giovanni Randon, Filippo de Braud, Nabil Amirouchene-Angelozzi, Silvia Marsoni, Maurizio D'Incalci, Armando Orlandi, Enrico Giraudo, Andrea Sartore-Bianchi, Salvatore Siena, Filippo Pietrantonio, Alberto Bardelli, Federica Di Nicolantonio. Accumulation of predicted neoantigens by MMR deficiency triggered by temozolomide treatment of human colorectal cancer [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2018; 2018 Apr 14-18; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2018;78(13 Suppl):Abstract nr 2743.

Published

2018

18. Neuroblastoma-targeted nanocarriers improve drug delivery and penetration, delay tumor growth and abrogate metastatic diffusion

Author

Alessandro Gori, Fabio Pastorino, Mirco Ponzoni, Renato Longhi, Angelo Corti, Flavio Curnis, Daniela Di Paolo, Gianluca Bottoni, Alice Bartolini, Maria Cristina Gagliani, Serena Marchiò, Chiara Brignole, Carlo Tacchetti, Daniele Murgia, Monica Loi, Michele Cilli, Francesca Piaggio, Cecilia Marini, Silvia Bruno, Irene Cossu, Patrizia Perri, Gianmario Sambuceti, Angela Rita Sementa, Angelina Sacchi, Laura Emionite, Cossu, I, Bottoni, G, Loi, M, Emionite, L, Bartolini, A, Di Paolo, D, Brignole, C, Piaggio, F, Perri, P, Sacchi, A, Curnis, F, Gagliani, Mc, Bruno, S, Marini, C, Gori, A, Longhi, R, Murgia, D, Sementa, Ar, Cilli, M, Tacchetti, Carlo, Corti, Angelo, Sambuceti, G, Marchiò, S, Ponzoni, M, and Pastorino, F.

Subjects

Drug delivery, Micro-PET, Neuroblastoma, Targeted therapy, Tumor penetration, Biomaterials, Bioengineering, Ceramics and Composites, Mechanics of Materials, Biophysics, Cell Survival, medicine.medical_treatment, Mice, Nude, Ceramics and Composite, Pharmacology, Diffusion, Mice, Therapeutic index, Nanocapsules, Cell Line, Tumor, Bioluminescence imaging, Medicine, Animals, Doxorubicin, Neoplasm Invasiveness, Mechanics of Material, Neoplasm Metastasis, Cell Proliferation, Antibiotics, Antineoplastic, Cell growth, business.industry, Drug Synergism, medicine.disease, Biomaterial, Female, Nanocarriers, business, medicine.drug

Abstract

Selective tumor targeting is expected to enhance drug delivery and to decrease toxicity, resulting in an improved therapeutic index. We have recently identified the HSYWLRS peptide sequence as a specific ligand for aggressive neuroblastoma, a childhood tumor mostly refractory to current therapies. Here we validated the specific binding of HSYWLRS to neuroblastoma cell suspensions obtained either from cell lines, animal models, or Schwannian-stroma poor, stage IV neuroblastoma patients. Binding of the biotinylated peptide and of HSYWLRS-functionalized fluorescent quantum dots or liposomal nanoparticles was dose-dependent and inhibited by an excess of free peptide. In animal models obtained by the orthotopic implant of either MYCN-amplified or MYCN single copy human neuroblastoma cell lines, treatment with HSYWLRS-targeted, doxorubicin-loaded Stealth Liposomes increased tumor vascular permeability and perfusion, enhancing tumor penetration of the drug. This formulation proved to exert a potent antitumor efficacy, as evaluated by bioluminescence imaging and micro-PET, leading to (i) delay of tumor growth paralleled by decreased tumor glucose consumption, and (ii) abrogation of metastatic spreading, accompanied by absence of systemic toxicity and significant increase in the animal life span. Our findings are functional to the design of targeted nanocarriers with potentiated therapeutic efficacy towards the clinical translation.

Published

2015

19. The neuronal pentraxin-2 pathway is an unrecognized target in human neuroblastoma which also offers prognostic value in patients

Author

Angela Rita Sementa, Alice Bartolini, Daniele Murgia, Serena Marchiò, Mirco Ponzoni, Daniela Di Paolo, Federico Bussolino, Alessio Noghero, Michele Cilli, Fabio Pastorino, Renata Pasqualini, and Wadih Arap

Subjects

Cancer Research, Nerve Tissue Proteins, Ligands, Mice, Neuroblastoma, In vivo, Cell Line, Tumor, medicine, Animals, Humans, Protein Interaction Domains and Motifs, Molecular Targeted Therapy, Receptor, Pentraxins, biology, Antibodies, Monoclonal, medicine.disease, Prognosis, Molecular biology, Neuroblastic Tumor, Xenograft Model Antitumor Assays, In vitro, Disease Models, Animal, C-Reactive Protein, Oncology, Targeted drug delivery, Cancer research, biology.protein, Signal transduction, Peptides, Protein Binding, Signal Transduction

Abstract

Neuronal pentraxins (NPTX) and their corresponding receptors (NPTXR) have been studied as synapse-associated proteins in the nervous system, but their role in cancer is largely unknown. By applying a multidisciplinary, high-throughput proteomic approach, we have recently identified a peptide ligand motif for targeted drug delivery to neuroblastoma. Here, we report the sequence similarity between this peptide and a conserved portion of the pentraxin domain that is involved in the homo- and hetero-oligomerization of NPTX2 and NPTXR. We show that, in comparison with normal tissues, NPTX2 and NPTXR are overexpressed in vivo in mouse models, as well as in human Schwannian stroma-poor, stage IV neuroblastoma. Both proteins are concentrated in the vicinity of tumor blood vessels, with NPTXR also present on neuroblastic tumor cells. In vivo targeting of NPTX2 and NPTXR with the selected peptide or with specific antibodies reduces tumor burden in orthotopic mouse models of human neuroblastoma. In vitro interference with this ligand/receptor system inhibits the organization of neuroblastoma cells in tumor-like masses in close contact with vascular cells, as well as their adhesion to normal microenvironment-derived cells, suggesting a role in the cross-talk between tumor and normal cells in the early steps of neuroblastoma development. Finally, we show that NPTX2 is a marker of poor prognosis for neuroblastoma patients. Cancer Res; 75(20); 4265–71. ©2015 AACR.

Published

2015

20. Abstract 3834: Tracking CAD-ALK gene translocation in urine and plasma of a colorectal cancer patient treated with ALK blockade

Author

Salvatore Siena, Giovanni Crisafulli, Alice Bartolini, Federica Tosi, Federica Di Nicolantonio, Benedetta Mussolin, Giulia Siravegna, Luca Novara, Laura Palmieri, Alberto Bardelli, Michela Buscarino, Mark G. Erlander, Andrea Cassingena, Andrea Sartore-Bianchi, and Giorgio Corti

Subjects

Cancer Research, Pathology, medicine.medical_specialty, Oncology, business.industry, Colorectal cancer, ALK Gene Translocation, Cancer research, Medicine, Urine, business, medicine.disease, Blockade

Abstract

A metastatic colorectal cancer (mCRC) patient carrying CAD-ALK translocation achieved partial response to an experimental ALK inhibitor and then progressed after 5 months. We studied whether urine cell-free, trans-renal DNA (tr-DNA) could be used to monitor tumor burden and patient’s response. A NGS panel was developed to interrogate 52 common cancer gene rearrangements and 14 frequently mutated genes in cancer patients. A TP53 p.R248W mutation and the CAD-ALK genomic breakpoint (rearrangement) were identified in the tumor tissue and matched plasma circulating tumor DNA (ctDNA) Urine samples were longitudinally obtained from the patient during ALK inhibitor treatment in parallel with blood. To detect the CAD-ALK translocation in urine tr-DNA we designed ultra-short (51 bp amplicon) primer pairs spanning the genomic breakpoint as a unique tumor marker. This approach allowed the non-invasive monitoring of the gene fusion in urine with amounts paralleling tumor burden. Of note, CAD-ALK gene fusion was apparent in urine tr-DNA before radiological confirmation of disease progression. The same strategy was applied to plasma ctDNA and the results were compared. To detect point mutations in urine tr-DNA, we exploited a peptide nucleic acids (PNA)-CLAMP PCR coupled with droplet digital PCR (ddPCR) analysis to specifically suppress amplification of wild-type DNA fragments. Custom PNA probes were designed for TP53 codon 248, and a ddPCR assay was optimized to detect the TP53 p.R248W mutation, which was then identified in all urine tr-DNA samples, with absolute copies correlating with tumor burden throughout ALK inhibitor treatment. In conclusion, we find that urine tr-DNA can be exploited to non-invasively monitor tumor burden by detecting tumor-specific gene fusions as well as point mutations. Citation Format: Giulia Siravegna, Andrea Sartore-Bianchi, Benedetta Mussolin, Laura Palmieri, Federica Tosi, Andrea Cassingena, Luca Novara, Michela Buscarino, Giorgio Corti, Giovanni Crisafulli, Alice Bartolini, Mark Erlander, Federica Di Nicolantonio, Salvatore Siena, Alberto Bardelli. Tracking CAD-ALK gene translocation in urine and plasma of a colorectal cancer patient treated with ALK blockade [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2017; 2017 Apr 1-5; Washington, DC. Philadelphia (PA): AACR; Cancer Res 2017;77(13 Suppl):Abstract nr 3834. doi:10.1158/1538-7445.AM2017-3834

Published

2017

21. Abstract 1778: Characterization and anti-tumor functionality of a neuroblastoma-specific peptide, either free or conjugated to nanocarriers

Author

Angelo Corti, Mirco Ponzoni, Daniela Di Paolo, Carlo Tacchetti, Flavio Curnis, Michele Cilli, Angelina Sacchi, Gianmario Sambuceti, Silvia Bruno, Michela Massollo, Laura Emionite, Renato Longhi, Gianluca Bottoni, Serena Marchiò, Alice Bartolini, Fabio Pastorino, Alessandro Gori, Cristina Gagliani, and Monica Loi

Subjects

chemistry.chemical_classification, Cancer Research, Peptide, Transfection, Cell morphology, medicine.disease, Molecular biology, In vitro, Oncology, Biochemistry, chemistry, In vivo, Cell culture, Neuroblastoma, medicine, Nanocarriers

Abstract

Introduction. The identification of peptide ligands specific for solid tumors is expected to provide targeting moieties to improve delivery and to decrease toxicity of chemotherapy. We have recently identified the peptide HSYWLRS as a specific ligand for neuroblastoma (NB), a childhood tumor mostly refractory to current therapies. Experimental procedures. The capability of peptide HSYWLRS to recognize NB cells was evaluated by coupling Qdot fluorescent nanoparticles with HSYWLRS or its scrambled version (SCR). NB cell association and internalization of HSYWLRS-targeted liposomes were tested by FACS and confocal microscopy studies. We further evaluated a potential role of this peptide in perturbing tumor-stroma interactions and tumor growth. NB cell lines stably transfected with eGFP were mixed with endothelial cells in the presence of either SCR or HSYWLRS peptides. Cell morphology and reciprocal cellular interactions were evaluated by optical and fluorescence microscopy. We finally performed therapeutic experiments with mice orthotopically injected with luc-trasfected NB cells and treated with HSYWLRS-targeted, doxorubicin-loaded liposomes (HSYWLRS-SL[DXR]). Anti-tumor efficacy was evaluated by BLI imaging. In vivo imaging was also performed by injecting mice with a bolus of fluorodeoxyglucose during a list mode acquisition lasting one hour using a dedicated micro-PET system. After framing rate optimization, tumor glucose consumption was measured using Patlak graphical approach and normalizing the slope of regression line for serum glucose level. Results. FACS analysis showed that HSYWLRS-Qdot and SCR-Qdot bound NB cells in a dose-dependent manner, however with different intensity, being HSYWLRS-Qdot the more potent. The binding of HSYWLRS-Qdot was efficiently inhibited by an excess of HSYWLRS, but not by control SCR peptide. In contrast, the binding of SCR-Qdot was not inhibited neither by an excess of SCR nor by HSYWLRS peptide, suggesting that the binding of SCR-Qdot is not specific. Again, the specific peptide-driven binding of HSYWLRS-SL to NB cells was inhibited by an excess of HSYWLRS peptide. In all cases, HSYWLRS specifically altered in vitro the interactions of NB cells with endothelium. Similarly, this peptide statistically decreased tumor take and growth when co-injected with tumor cells in the adrenal gland of nude mice. Preliminary in vivo results obtained by BLI and micro-PET devises indicated that HSYWLRS-SL[DXR] decrease tumor growth through a reduction of tumor glucose consumption, leading to an enhanced life span in treated mice. Conclusion. Our findings demonstrate that HSYWLRS peptide recognizes NB cells and is functional in the design of nanocarriers with therapeutic efficacy paving the way to its clinical development. Citation Format: Alice Bartolini, Monica Loi, Daniela Di Paolo, Laura Emionite, Angelina Sacchi, Flavio Curnis, Gianluca Bottoni, Michela Massollo, Cristina Gagliani, Silvia Bruno, Alessandro Gori, Renato Longhi, Michele Cilli, Carlo Tacchetti, Angelo Corti, Gianmario Sambuceti, Mirco Ponzoni, Serena Marchiò, Fabio Pastorino. Characterization and anti-tumor functionality of a neuroblastoma-specific peptide, either free or conjugated to nanocarriers. [abstract]. In: Proceedings of the 105th Annual Meeting of the American Association for Cancer Research; 2014 Apr 5-9; San Diego, CA. Philadelphia (PA): AACR; Cancer Res 2014;74(19 Suppl):Abstract nr 1778. doi:10.1158/1538-7445.AM2014-1778

Published

2014

22. Genotyping tumour DNA in cerebrospinal fluid and plasma of a HER2-positive breast cancer patient with brain metastases

Author

Filippo Montemurro, Giovanni Crisafulli, Maurizio Scaltriti, Alberto Bardelli, Ivana Sarotto, Benedetta Mussolin, Giulia Siravegna, Alice Bartolini, Danilo Galizia, Elena Geuna, Anna Sapino, and Laura Casorzo

Subjects

HER2 positive, 0301 basic medicine, Cancer Research, Pathology, medicine.medical_specialty, Central nervous system, cerebrospinal fluid, 03 medical and health sciences, breast cancer, 0302 clinical medicine, Cerebrospinal fluid, Breast cancer, Medicine, Digital polymerase chain reaction, Liquid biopsy, skin and connective tissue diseases, neoplasms, Genotyping, Exome sequencing, Original Research, liquid biopsy, business.industry, Cancer, medicine.disease, 3. Good health, heterogeneity, 030104 developmental biology, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, business

Abstract

Background Central nervous system (CNS) involvement contributes to significant morbidity and mortality in patients with human epidermal growth factor receptor 2 (HER2)-positive metastatic breast cancer (mBC) and represents a major challenge for clinicians. Liquid biopsy of cerebrospinal fluid (CSF)-derived circulating tumour DNA (ctDNA) harbours clinically relevant genomic alterations in patients with CNS metastases and could be effective in tracking tumour evolution. Methods In a HER2-positive mBC patient with brain metastases, we applied droplet digital PCR (ddPCR) and next-generation whole exome sequencing (WES) analysis to measure ctDNA dynamic changes in CSF and plasma collected during treatment. Results Baseline CSF-derived ctDNA analysis revealed TP53 and PIK3CA mutations as well as ERBB2 and c MYC amplification. Post-treatment ctDNA analysis showed decreased markers level in plasma, consistent with extra-CNS disease control, while increased in the CSF, confirming poor treatment benefit in the CNS. Discussion Analysis of ctDNA in the CSF of HER2-positive mBC is feasible and could represent a useful companion for clinical management of brain metastases.

Published

2017

23. A complex of α(6) integrin and E-cadherin drives liver metastasis of colorectal cancer cells through hepatic angiopoietin-like 6

Author

Antonella Bugatti, Sabrina Cardaci, Sofia Asioli, Wadih Arap, Federico Bussolino, Dario Ribero, Paola Bovino, Renata Pasqualini, Paola Cassoni, Alice Bartolini, Maria Chiara Monti, Jessica Sun, Lorenzo Capussotti, Vanessa Barone, Andrea Muratore, Raffaella Giavazzi, Marco Soster, Marco Rusnati, Piero Pucci, Serena Marchiò, Marchiò, S, Soster, M, Cardaci, S, Muratore, A, Bartolini, A, Barone, V, Ribero, D, Monti, Maria, Bovino, P, Sun, J, Giavazzi, R, Asioli, S, Cassoni, P, Capussotti, L, Pucci, Pietro, Bugatti, A, Rusnati, M, Pasqualini, R, Arap, W, Bussolino, F., Marchiò S, Soster M, Cardaci S, Muratore A, Bartolini A, Barone V, Ribero D, Monti M, Bovino P, Sun J, Giavazzi R, Asioli S, Cassoni P, Capussotti L, Pucci P, Bugatti A, Rusnati M, Pasqualini R, Arap W, and Bussolino F

Subjects

Pathology, medicine.medical_specialty, Colorectal cancer, Amino Acid Motifs, Mice, Nude, colorectal cancer, Biology, Integrin alpha6, Metastasis, Angiopoietin, Mice, integrins, Angiopoietins, metastasis, Cell Line, Tumor, medicine, Animals, Humans, Angiopoietin-Like Protein 6, Neoplasm Metastasis, Receptor, Research Articles, alpha(6) integrin, Cadherin, metastatic colorectal cancer, Liver Neoplasms, angiopoietin-like 6, E-cadherin, medicine.disease, Cadherins, α6 integrin, a6 integrin, microenvironment, digestive system diseases, Crosstalk (biology), Angiopoietin-like Proteins, Liver, Cancer cell, Cancer research, Molecular Medicine, Blood Vessels, Female, Colorectal Neoplasms, Homing (hematopoietic), Protein Binding

Abstract

Homing of colorectal cancer (CRC) cells to the liver is a non-random process driven by a crosstalk between tumour cells and components of the host tissue. Here we report the isolation of a liver metastasis-specific peptide ligand (CGIYRLRSC) that binds a complex of E-cadherin and α(6) integrin on the surface of CRC cells. We identify angiopoietin-like 6 protein as a peptide-mimicked natural ligand enriched in hepatic blood vessels of CRC patients. We demonstrate that an interaction between hepatic angiopoietin-like 6 and tumoural α(6) integrin/E-cadherin drives liver homing and colonization by CRC cells, and that CGIYRLRSC inhibits liver metastasis through interference with this ligand/receptor system. Our results indicate a mechanism for metastasis whereby a soluble factor accumulated in normal vessels functions as a specific ligand for circulating cancer cells. Consistently, we show that high amounts of coexpressed α(6) integrin and E-cadherin in primary tumours represent a poor prognostic factor for patients with advanced CRC.

Published

2012

24. Abstract 3625: Novel phage-display derived peptides for tumor- and vasculature-targeted therapies in neuroblastoma

Author

Wadih Arap, Renata Pasqualini, Alice Bartolini, Mirco Ponzoni, Fabio Pastorino, Daniela Di Paolo, Claudio Gambini, Jessica Sun, Renato Longhi, Angelo Corti, Serena Marchiò, Michele Cilli, Marco Soster, Monica Loi, and Flavio Curnis

Subjects

Cancer Research, Pathology, medicine.medical_specialty, Phage display, business.industry, Cell, medicine.disease, Minimal residual disease, Primary tumor, Therapeutic index, medicine.anatomical_structure, Oncology, Antigen, Neuroblastoma, Cancer cell, medicine, Cancer research, business

Abstract

Disseminated neuroblastoma (NB) is refractory to most current therapeutic regimens. The therapeutic index of anticancer drugs is increased by liposome encapsulation and further improvements is obtained by coupling tumor-targeting ligands to the surface of the lipidic envelop. Phage display technology is a powerful tool in discovering novel ligands specific to receptors on the surface of tumor epithelial and endothelial cells. Therapeutic targeting to tumor blood vessels combines blood vessel destruction with the expected anti-tumor activities of the drug, resulting in increased efficacy and reduced toxicity. To find NB-specific targeting moieties, we established a protocol for the isolation of heterogeneous cell populations by tissue fractionation of primary tumors and metastases from two models of human NB (with tumor cells injected either intravenously, to mimic minimal residual disease, or orthotopically in the adrenal gland of mice, to reflect the growth of advanced NB in children with large adrenal gland tumors and small metastatic lesions) and from stage IV, stroma poor, NB-derived specimens immediately after surgical removal. Cells extracted from corresponding healthy organs from mice and patients were used both in a negative pre-selection step and as a negative control for specific phage enrichment. The NB cell suspensions were subjected to multi-step screenings with the phage-displayed peptide library CX7C (where C = cysteine and X = any aminoacid). We globally isolated 135 NB-binding peptides. Of these, 31 were selected for binding to the primary tumor mass, 16 to the metastatic mass, 63 to tumor endothelial cells, and 25 to endothelial cells of metastases. Several proteins presenting sequence homology with the discovered peptides have been identified by BLAST analysis and were evaluated for their expression in NB tumors, derived from both mouse xenogratfs and patient specimens. Specifically, 5 novel phage display derived-peptides showed specific binding on NB specimens and homing to tumor cells and tumor vasculature, 10 minutes and 24 hours after injection through the tail vein of NB-bearing mice. We are testing the new molecular, tumor- and vasculature-specific peptides for generating novel tumor-specific liposomal therapies against NB. The availability of novel ligands binding to additional tumor-associated antigens and to targets on both endothelial and perivascular tumor cells will allow to design more sophisticated liposomal targeted anticancer strategies that exhibit high levels of selective toxicity for the cancer cells. Citation Format: {Authors}. {Abstract title} [abstract]. In: Proceedings of the 102nd Annual Meeting of the American Association for Cancer Research; 2011 Apr 2-6; Orlando, FL. Philadelphia (PA): AACR; Cancer Res 2011;71(8 Suppl):Abstract nr 3625. doi:10.1158/1538-7445.AM2011-3625

Published

2011

25. Fast Walking And Resistance Exercise Program In Cancer Survivors

Author

Giorgio Galanti, Lisa Sequi, Andrea Cattozzo, Laura Stefani, Alice Bartolini, Fabio Buralli, Lorenzo Francini, Gabriele Mascherini, Cristian Petri, and Maira Marques

Subjects

medicine.medical_specialty, Physical medicine and rehabilitation, business.industry, Resistance training, Medicine, Cancer, Physical Therapy, Sports Therapy and Rehabilitation, Orthopedics and Sports Medicine, business, medicine.disease

Published

2015

26. Abstract 1163: Microenvironment targets in KRAS-mutated metastatic colorectal cancer

Author

Giorgio Corti, Alice Bartolini, Federico Bussolino, Simona Lamba, Marco Soster, Davide Corà, Sabrina Cardaci, Federica Di Nicolantonio, and Serena Marchiò

Subjects

Cancer Research, Tumor microenvironment, Colorectal cancer, business.industry, Biopanning, medicine.disease, medicine.disease_cause, Metastasis, Oncology, In vivo, Immunology, medicine, Cancer research, Immunohistochemistry, KRAS, business, Ex vivo

Abstract

The introduction of biodrugs, e.g. the anti-EGFR antibodies, was initially seen as a promise to radically change the landscape for patients with metastatic colorectal cancer. However, although EGFR-targeted therapies, combined with chemotherapy, have prolonged survival expectancy to 24 months, cure remains anecdotal. Target therapies suffer of high costs, important side effects, and low response rates: it is now clear that this approach as it was originally conceived failed to meet the majority of its expectations. Importantly, because of novel prescription guidelines, patients with KRAS-mutated tumors are excluded from EGFR-targeted therapies: for these patients alternative treatments are urgently needed. We here propose an innovative strategy based on the identification of molecular targets specifically associated with the microenvironment of metastatic colorectal cancer in patients carrying oncogenic KRAS. For this purpose, we set up mice models of metastatic colorectal cancer by intrasplenic (to evaluate liver homing) and intrahepatic (to investigate liver colonization) implantation of human colorectal cancer cell lines (SW48 and LIM1215) in which oncogenic KRAS (G12D, G12V, G13D) variants have been somatically knocked-in. We based our “target fishing” strategy on high-throughput, phage display-mediated proteomic screenings of deriving tumor samples ex vivo. Proteome signatures from the cognate cell lines in vitro served as a subtractive reference for the ex vivo biopanning, aimed at the identification of peptide ligands specific for non-epithelial components. By this combined biological-genetic-bioinformatics approach, we identified peptide/protein signatures selectively associated to metastasis microenvironments with controlled genetic backgrounds in vitro and in vivo. We selected 2 target proteins and 2 targeting peptides, which were exploited for diagnostic and therapeutic purposes. First, we evaluated by IHC the presence and localization of the target proteins in samples (tumor, healthy liver) from a panel of human biopsies and from the described in vivo models. This analysis confirmed a specific enrichment in KRAS-mutated microenvironments. Second, we tested the capability of dye-conjugated targeting peptides to home to these same tumor microenvironments, observing a specific accumulation in target tissues, compared to their scrambled versions and to control tissues. Third, we investigated a potential anti-metastatic effect of these peptides when orthotopically co-injected with colorectal cancer cell lines; preliminary experiments revealed that the targeting peptides, but not the scrambled variants, inhibit the onset of liver metastases from KRAS-mutated cell lines. In summary, we obtained proof-of-concept results in preclinical studies and produced prototype compounds to provide innovative tools that can be translated into the clinical practice with a mid-term perspective. Citation Format: Serena Marchio, Alice Bartolini, Sabrina Cardaci, Marco Soster, Giorgio Corti, Simona Lamba, Federico Bussolino, Davide Cora', Federica Di Nicolantonio. Microenvironment targets in KRAS-mutated metastatic colorectal cancer. [abstract]. In: Proceedings of the 105th Annual Meeting of the American Association for Cancer Research; 2014 Apr 5-9; San Diego, CA. Philadelphia (PA): AACR; Cancer Res 2014;74(19 Suppl):Abstract nr 1163. doi:10.1158/1538-7445.AM2014-1163

Published

2014

27. Abstract 5620: Novel phage display-derived neuroblastoma-targeting peptides potentiate the effect of drug nanocarriers in preclinical settings

Author

Marco Soster, Theresa M. Allen, Renato Longhi, Chiara Brignole, Jessica Sun, Alice Bartolini, Claudio Gambini, Monica Sani, Renata Pasqualini, Wadih Arap, Flavio Curnis, Angelo Corti, Pamela Becherini, Michele Cilli, Mirco Ponzoni, Daniela Di Paolo, Federico Bussolino, Alessandro Gori, Laura Emionite, Fabio Pastorino, Andrea Petretto, Serena Marchiò, and Monica Loi

Subjects

Cancer Research, Phage display, Stromal cell, business.industry, medicine.disease, Primary tumor, In vitro, Therapeutic index, Oncology, In vivo, Neuroblastoma, Immunology, Cancer research, Medicine, Nanocarriers, business

Abstract

Purpose: Molecular targeting of drug delivery nanocarriers is expected to improve their therapeutic index while decreasing their toxicity. The identification of novel peptide ligands specific for cells present in high-risk neuroblastoma, a childhood tumor mostly refractory to current therapies, is needed. Experimental design: We performed combined in vitro/ex-vivo phage display screenings on human neuroblastoma cell lines and on tumors derived from orthotopic mouse models of human neuroblastoma. Binding validation and homing in vivo of selected phage clones were tested by immunohistochemistry/immunofluorescent analyses. Cell association experiments in vitro with the corresponding synthetic biotin-labeled peptides were performed. In vitro cytotoxicity and in vivo tumor accumulation and therapeutic experiments were performed using peptide-targeted, doxorubicin-loaded, nanocarriers. Results: By designing proper subtractive protocols, we identified phage clones specific either for the primary tumor, its metastases, or for the stromal components. Globally, we isolated 121 phage-displayed neuroblastoma-binding peptides; of these, 26 bound the primary tumor, 15 the metastatic mass, 57 and 23 their respective microenvironments. Of these, five phage clones were further validated for their specific binding ex-vivo to biopsies from stage IV neuroblastoma patients and to neuroblastoma tumors derived from mice. All five clones also targeted tumor cells and vasculature in vivo when injected into neuroblastoma-bearing mice. Coupling of the corresponding targeting peptides with doxorubicin-loaded nanocarriers led to a significant inhibition in tumor volume and enhanced survival in preclinical neuroblastoma models. Conclusions: Our findings demonstrate that novel ligands of neuroblastoma-associated markers are functional in the design of nanocarriers with therapeutic efficacy paving the way to their clinical development. Citation Format: Monica Loi, Daniela Di Paolo, Marco Soster, Chiara Brignole, Alice Bartolini, Laura Emionite, Jessica Sun, Pamela Becherini, Flavio Curnis, Andrea Petretto, Monica Sani, Alessandro Gori, Claudio Gambini, Renato Longhi, Michele Cilli, Theresa M. Allen, Federico Bussolino, Wadih Arap, Renata Pasqualini, Angelo Corti, Mirco Ponzoni, Serena Marchiò, Fabio Pastorino. Novel phage display-derived neuroblastoma-targeting peptides potentiate the effect of drug nanocarriers in preclinical settings. [abstract]. In: Proceedings of the 104th Annual Meeting of the American Association for Cancer Research; 2013 Apr 6-10; Washington, DC. Philadelphia (PA): AACR; Cancer Res 2013;73(8 Suppl):Abstract nr 5620. doi:10.1158/1538-7445.AM2013-5620

Published

2013

28. Adaptive mutability of colorectal cancers in response to targeted therapies

Author

Andrea Sartore-Bianchi, Salvatore Siena, Marco Gherardi, Alessandro Magrì, Mariangela Russo, Marco Cosentino Lagomarsino, Ivana Sarotto, Alberto Sogari, Giovanni Crisafulli, Cortt G. Piett, Livio Trusolino, Luca Novara, Nicole M. Reilly, Vito Amodio, Simona Lamba, Andrea Bertotti, Alice Bartolini, Zachary D. Nagel, Mattia Corigliano, Sabrina Arena, Alessio Amatu, Federica Di Nicolantonio, and Alberto Bardelli

Subjects

Proto-Oncogene Proteins B-raf, DNA damage, Colorectal cancer, Adaptation, Biological, Down-Regulation, Mutagenesis (molecular biology technique), Drug resistance, DNA Mismatch Repair, 03 medical and health sciences, 0302 clinical medicine, medicine, Humans, Molecular Targeted Therapy, Epidermal growth factor receptor, Selection, Genetic, 030304 developmental biology, 0303 health sciences, Multidisciplinary, biology, Microsatellite instability, medicine.disease, 3. Good health, ErbB Receptors, Drug Resistance, Neoplasm, Mutagenesis, 030220 oncology & carcinogenesis, Cancer research, biology.protein, DNA mismatch repair, Colorectal Neoplasms, Homologous recombination

Abstract

A cross-kingdom tale of drug resistance Physicians who treat bacterial infections and those who treat cancer often face a common challenge: the development of drug resistance. It is well known that when bacteria are exposed to antibiotics, they temporarily increase their mutation rate, thus increasing the chance that a descendant antibiotic-resistant cell will arise. Russo et al. now provide evidence that cancer cells exploit a similar mechanism to ensure their survival after drug exposure (see the Perspective by Gerlinger). They found that human colorectal cancer cells treated with certain targeted therapies display a transient up-regulation of errorprone DNA polymerases and a reduction in their ability to repair DNA damage. Thus, like bacteria, cancer cells can adapt to therapeutic pressure by enhancing their mutability. Science , this issue p. 1473 ; see also p. 1458

29. Tracking aCAD-ALK gene rearrangement in urine and blood of a colorectal cancer patient treated with an ALK inhibitor

Author

Salvatore Siena, Alessio Amatu, Giovanni Crisafulli, Mark G. Erlander, Giulia Siravegna, Andrea Cassingena, Luca Novara, Federica Tosi, Alice Bartolini, Alberto Bardelli, Michela Buscarino, Giorgio Corti, Andrea Sartore-Bianchi, F. Di Nicolantonio, and Benedetta Mussolin

Subjects

0301 basic medicine, Oncology, medicine.medical_specialty, Indazoles, Colorectal cancer, medicine.drug_class, Entrectinib, colorectal cancer, ALK translocation, trans-renal DNA, ALK inhibitor, Polymerase Chain Reaction, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Biopsy, medicine, Aspartate Carbamoyltransferase, Biomarkers, Tumor, Humans, Anaplastic Lymphoma Kinase, Liquid biopsy, Dihydroorotase, Gene Rearrangement, medicine.diagnostic_test, liquid biopsy, ALK Gene Rearrangement, business.industry, circulating DNA, Receptor Protein-Tyrosine Kinases, Hematology, Gene rearrangement, Middle Aged, medicine.disease, Minimal residual disease, 6. Clean water, 3. Good health, 030104 developmental biology, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Benzamides, Carbamoyl-Phosphate Synthase (Glutamine-Hydrolyzing), Female, Gene Fusion, business, Colorectal Neoplasms

Abstract

Background Monitoring response and resistance to kinase inhibitors is essential to precision cancer medicine, and is usually investigated by molecular profiling of a tissue biopsy obtained at progression. However, tumor heterogeneity and tissue sampling bias limit the effectiveness of this strategy. In addition, tissue biopsies are not always feasible and are associated with risks due to the invasiveness of the procedure. To overcome these limitations, blood-based liquid biopsy analysis has proven effective to non-invasively follow tumor clonal evolution. Patients and methods We exploited urine cell-free, trans-renal DNA (tr-DNA) and matched plasma circulating tumor DNA (ctDNA) to monitor a metastatic colorectal cancer patient carrying aCAD-ALK translocation during treatment with an ALK inhibitor. Results Using a custom next generation sequencing panel we identified the genomicCAD-ALK rearrangement and aTP53 mutation in plasma ctDNA. Sensitive assays were developed to detect both alterations in urine tr-DNA. The dynamics of theCAD-ALK rearrangement in plasma and urine were concordant and paralleled the patient’s clinical course. Detection of theCAD-ALK gene fusion in urine tr-DNA anticipated radiological confirmation of disease progression. Analysis of plasma ctDNA identifiedALK kinase mutations that emerged during treatment with the ALK inhibitor entrectinib. Conclusion We find that urine-based genetic testing allows tracing of tumor-specific oncogenic rearrangements. This strategy could be effectively applied to non-invasively monitor tumor evolution during therapy. The same approach could be exploited to monitor minimal residual disease after surgery with curative intent in patients whose tumors carry gene fusions. The latter could be implemented without the need of patient hospitalization since urine tr-DNA can be self-collected, is stable over time and can be shipped at specified time-points to central labs for testing.

30. Novel phage display-derived neuroblastoma-targeting peptides potentiate the effect of drug nanocarriers in preclinical settings

Author

Serena Marchiò, Marco Soster, Claudio Gambini, Jessica Sun, Mirco Ponzoni, Monica Loi, Daniela Di Paolo, Theresa M. Allen, Federico Bussolino, Flavio Curnis, Marco Milanese, Renata Pasqualini, Andrea Petretto, Michele Cilli, Alice Bartolini, Renato Longhi, Monica Sani, Fabio Pastorino, Alessandro Gori, Pamela Becherini, Laura Emionite, Chiara Brignole, Wadih Arap, Angelo Corti, Loi, M, Di Paolo, D, Soster, M, Brignole, C, Bartolini, A, Emionite, L, Sun, J, Becherini, P, Curnis, F, Petretto, A, Sani, M, Gori, A, Milanese, M, Gambini, C, Longhi, R, Cilli, M, Allen, Tm, Bussolino, F, Arap, W, Pasqualini, R, Corti, Angelo, Ponzoni, M, Marchiò, S, and Pastorino, F.

Subjects

Phage display, Cell Survival, medicine.medical_treatment, Mice, Nude, Pharmaceutical Science, Biology, Article, Targeted therapy, Mice, Neuroblastoma, Therapeutic index, In vivo, Cell Line, Tumor, medicine, Human Umbilical Vein Endothelial Cells, Animals, Humans, Cells, Cultured, medicine.disease, Molecular biology, Primary tumor, Xenograft Model Antitumor Assays, Tumor Burden, Phage display screening, Doxorubicin, Drug delivery, Liposomes, Nanoparticles, Female, Nanocarriers, Cell Surface Display Techniques, Peptides

Abstract

Molecular targeting of drug delivery nanocarriers is expected to improve their therapeutic index while decreasing their toxicity. Here we report the identification and characterization of novel peptide ligands specific for cells present in high-risk neuroblastoma (NB), a childhood tumor mostly refractory to current therapies. To isolate such targeting moieties, we performed combined in vitro/ex-vivo phage display screenings on NB cell lines and on tumors derived from orthotopic mouse models of human NB.By designing proper subtractive protocols, we identified phage clones specific either for the primary tumor, its metastases, or for their respective stromal components. Globally, we isolated 121 phage-displayed NB-binding peptides: 26 bound the primary tumor, 15 the metastatic mass, 57 and 23 their respective microenvironments. Of these, five phage clones were further validated for their specific binding ex-vivo to biopsies from stage IV NB patients and to NB tumors derived from mice. All five clones also targeted tumor cells and vasculature in vivo when injected into NB-bearing mice. Coupling of the corresponding targeting peptides with doxorubicin-loaded liposomes led to a significant inhibition in tumor volume and enhanced survival in preclinical NB models, thereby paving the way to their clinical development.