Your search keyword '"Berrino, Enrico"' showing total 9 results

1. Comprehensive Molecular Profiling of NPM1-Mutated Acute Myeloid Leukemia Using RNAseq Approach.

Author

Petiti, Jessica, Pignochino, Ymera, Schiavon, Aurora, Giugliano, Emilia, Berrino, Enrico, Giordano, Giorgia, Itri, Federico, Dragani, Matteo, Cilloni, Daniela, and Lo Iacono, Marco

Subjects

ACUTE myeloid leukemia, RNA sequencing, CLONE cells, GENE expression, GENETIC variation

Abstract

Acute myeloid leukemia (AML) is a complex hematologic malignancy with high morbidity and mortality. Nucleophosmin 1 (NPM1) mutations occur in approximately 30% of AML cases, and NPM1-mutated AML is classified as a distinct entity. NPM1-mutated AML patients without additional genetic abnormalities have a favorable prognosis. Despite this, 30–50% of them experience relapse. This study aimed to investigate the potential of total RNAseq in improving the characterization of NPM1-mutated AML patients. We explored genetic variations independently of myeloid stratification, revealing a complex molecular scenario. We showed that total RNAseq enables the uncovering of different genetic alterations and clonal subtypes, allowing for a comprehensive evaluation of the real expression of exome transcripts in leukemic clones and the identification of aberrant fusion transcripts. This characterization may enhance understanding and guide improved treatment strategies for NPM1mut AML patients, contributing to better outcomes. Our findings underscore the complexity of NPM1-mutated AML, supporting the incorporation of advanced technologies for precise risk stratification and personalized therapeutic strategies. The study provides a foundation for future investigations into the clinical implications of identified genetic variations and highlights the importance of evolving diagnostic approaches in leukemia management. [ABSTRACT FROM AUTHOR]

Published

2024

2. Integrated Antitumor Activities of Cellular Immunotherapy with CIK Lymphocytes and Interferons against KIT/PDGFRA Wild Type GIST.

Author

Fiorino, Erika, Merlini, Alessandra, D'Ambrosio, Lorenzo, Cerviere, Ilaria, Berrino, Enrico, Marchiò, Caterina, Giraudo, Lidia, Basiricò, Marco, Massa, Annamaria, Donini, Chiara, Leuci, Valeria, Rotolo, Ramona, Galvagno, Federica, Vitali, Letizia, Proment, Alessia, Ferrone, Soldano, Pisacane, Alberto, Pignochino, Ymera, Aglietta, Massimo, and Grignani, Giovanni

Subjects

INTERFERONS, GASTROINTESTINAL stromal tumors, ANTINEOPLASTIC agents, LYMPHOCYTES, CELL receptors, PROGRAMMED cell death 1 receptors

Abstract

Gastrointestinal stromal tumors (GISTs) are rare, mesenchymal tumors of the gastrointestinal tract, characterized by either KIT or PDGFRA mutation in about 85% of cases. KIT/PDGFRA wild type gastrointestinal stromal tumors (wtGIST) account for the remaining 15% of GIST and represent an unmet medical need: their prevalence and potential medical vulnerabilities are not completely defined, and effective therapeutic strategies are still lacking. In this study we set a patient-derived preclinical model of wtGIST to investigate their phenotypic features, along with their susceptibility to cellular immunotherapy with cytokine-induced killer lymphocytes (CIK) and interferons (IFN). We generated 11 wtGIST primary cell lines (wtGISTc). The main CIK ligands (MIC A/B; ULBPs), along with PD-L1/2, were expressed by wtGISTc and the expression of HLA-I molecules was preserved. Patient-derived CIK were capable of intense killing in vitro against wtGISTc resistant to both imatinib and sunitinib. We found that CIK produce a high level of granzyme B, IFNα and IFNγ. CIK-conditioned supernatant was responsible for part of the observed tumoricidal effect, along with positive bystander modulatory activities enhancing the expression of PD-L1/2 and HLA-I molecules. IFNα, but not In, had direct antitumor effects on 50% (4/8) of TKI-resistant wtGISTc, positively correlated with the tumor expression of IFN receptors. wtGIST cells that survived IFNα were still sensitive to CIK immunotherapy. Our data support the exploration of CIK immunotherapy in clinical studies for TKI-resistant wtGIST, proposing reevaluation for IFNα within this challenging setting. [ABSTRACT FROM AUTHOR]

Published

2022

3. The Tumor-Specific Expression of L1 Retrotransposons Independently Correlates with Time to Relapse in Hormone-Negative Breast Cancer Patients.

Author

Berrino, Enrico, Miglio, Umberto, Bellomo, Sara Erika, Debernardi, Carla, Bragoni, Alberto, Petrelli, Annalisa, Cascardi, Eliano, Giordano, Silvia, Montemurro, Filippo, Marchiò, Caterina, Venesio, Tiziana, and Sapino, Anna

Subjects

*PROGRAMMED cell death 1 receptors, *RETROTRANSPOSONS, *CANCER patients, *BREAST cancer, *GENE expression, *PROGRESSION-free survival

Abstract

Background: Long-Interspersed Nuclear Element (L1) retrotransposons are silenced in healthy tissues but unrepressed in cancer. Even if L1 reactivation has been associated with reduced overall survival in breast cancer (BC) patients, a comprehensive correlation with clinicopathological features is still missing. Methods: Using quantitative, reverse-transcription PCR, we assessed L1 mRNA expression in 12 BC cells, 210 BC patients and in 47 normal mammary tissues. L1 expression was then correlated with molecular and clinicopathological data. Results: We identified a tumor-exclusive expression of L1s, absent in normal mammary cells and tissues. A positive correlation between L1 expression and tumor dedifferentiation, lymph-node involvement and increased immune infiltration was detected. Molecular subtyping highlighted an enrichment of L1s in basal-like cells and cancers. By exploring disease-free survival, we identified L1 overexpression as an independent biomarker for patients with a high risk of recurrence in hormone-receptor-negative BCs. Conclusions: Overall, L1 reactivation identified BCs with aggressive features and patients with a worse clinical fate. [ABSTRACT FROM AUTHOR]

Published

2022

4. PARP1 Inhibitor and Trabectedin Combination Does Not Increase Tumor Mutational Burden in Advanced Sarcomas—A Preclinical and Translational Study.

Author

Pignochino, Ymera, Crisafulli, Giovanni, Giordano, Giorgia, Merlini, Alessandra, Berrino, Enrico, Centomo, Maria Laura, Chiabotto, Giulia, Brusco, Silvia, Basiricò, Marco, Maldi, Elena, Pisacane, Alberto, Leuci, Valeria, Sangiolo, Dario, D'Ambrosio, Lorenzo, Aglietta, Massimo, Kasper, Bernd, Bardelli, Alberto, and Grignani, Giovanni

Subjects

THERAPEUTIC use of antineoplastic agents, GENETIC mutation, XENOGRAFTS, CONFIDENCE intervals, CANCER patients, DESCRIPTIVE statistics, TRANSLATIONAL research, CELL lines, DATA analysis software, ODDS ratio, ENZYME inhibitors, SARCOMA

Abstract

Simple Summary: Immunotherapy has revolutionized cancer treatment, but not for all tumor types. Indeed, sarcomas are considered "immune-cold" tumors, which are relatively unresponsive to immunotherapy. One strategy to potentiate immunotherapy efficacy is to increase tumor immunogenicity, for instance by boosting the number of candidate targets (neoantigens) to be recognized by the immune system. Tumor mutational burden indicates the number of somatic mutations identified in the tumor and normalized per megabase. Tumor mutational burden is considered as an acceptable, measurable surrogate of tumor neoantigens. Here, we explored whether the combination of two DNA-damaging agents, trabectedin and olaparib, could increase tumor mutational burden in sarcomas, to prime subsequent immunotherapy. We found no variation in tumor mutational burden after trabectedin + olaparib in preclinical and clinical samples. Therefore, other aspects should be considered to increase sarcoma immunogenicity, by exploiting different pathways such as the potential modulation of the tumor microenvironment induced by trabectedin + olaparib. Drug-induced tumor mutational burden (TMB) may contribute to unleashing the immune response in relatively "immune-cold" tumors, such as sarcomas. We previously showed that PARP1 inhibition perpetuates the DNA damage induced by the chemotherapeutic agent trabectedin in both preclinical models and sarcoma patients. In the present work, we explored acquired genetic changes in DNA repair genes, mutational signatures, and TMB in a translational platform composed of cell lines, xenografts, and tumor samples from patients treated with trabectedin and olaparib combination, compared to cells treated with temozolomide, an alkylating agent that induces hypermutation. Whole-exome and targeted panel sequencing data analyses revealed that three cycles of trabectedin and olaparib combination neither affected the mutational profiles, DNA repair gene status, or copy number alterations, nor increased TMB both in homologous recombinant-defective and proficient cells or in xenografts. Moreover, TMB was not increased in tumor specimens derived from trabectedin- and olaparib-treated patients (5–6 cycles) when compared to pre-treatment biopsies. Conversely, repeated treatments with temozolomide induced a massive TMB increase in the SJSA-1 osteosarcoma model. In conclusion, a trabectedin and olaparib combination did not show mutagenic effects and is unlikely to prime subsequent immune-therapeutic interventions based on TMB increase. On the other hand, these findings are reassuring in the increasing warning of treatment-induced hematologic malignancies correlated to PARP1 inhibitor use. [ABSTRACT FROM AUTHOR]

Published

2021

5. Pursuit of Gene Fusions in Daily Practice: Evidence from Real-World Data in Wild-Type and Microsatellite Instable Patients.

Author

Berrino, Enrico, Bragoni, Alberto, Annaratone, Laura, Fenocchio, Elisabetta, Carnevale-Schianca, Fabrizio, Garetto, Lucia, Aglietta, Massimo, Sarotto, Ivana, Casorzo, Laura, Venesio, Tiziana, Sapino, Anna, and Marchiò, Caterina

Subjects

*ADENOCARCINOMA, *LUNG cancer, *GENETIC mutation, *MELANOMA, *IMMUNOHISTOCHEMISTRY, *ACQUISITION of data, *RNA, *FISHER exact test, *COLORECTAL cancer, *GENES, *DESCRIPTIVE statistics, *BIOLOGICAL assay, *POLYMERASE chain reaction, *DATA analysis software, *DEGENERATION (Pathology)

Abstract

Simple Summary: The main aim of our study is to provide real-world data on the enrichment of gene fusions in patients affected by colorectal carcinomas, melanomas, and lung adenocarcinomas characterized by the absence of mutations in the main driver genes and in colorectal tumours with microsatellite instability, using a comprehensive method. By demonstrating this enrichment in a "real-world" cohort, we confirm the feasibility of this approach, suggesting a workflow applicable in diagnostic practice. A second aim points towards a thorough investigation of NTRK gene fusions detected in the study by applying different techniques. We therefore provide comparative data across in situ methods and in vitro nucleic acid-based assays to document effective NTRK gene fusion detection. Agnostic biomarkers such as gene fusions allow to address cancer patients to targeted therapies; however, the low prevalence of these alterations across common malignancies poses challenges and needs a feasible and sensitive diagnostic process. RNA-based targeted next generation sequencing was performed on 125 samples of patients affected either by colorectal carcinoma, melanoma, or lung adenocarcinoma lacking genetic alterations in canonical driver genes, or by a colorectal carcinoma with microsatellite instability. Gene fusion rates were compared with in silico data from MSKCC datasets. For NTRK gene fusion detection we also employed a multitarget qRT-PCR and pan-TRK immunohistochemistry. Gene fusions were detected in 7/55 microsatellite instable colorectal carcinomas (12.73%), and in 4/70 of the "gene driver free" population (5.71%: 3/28 melanomas, 10.7%, and 1/12 lung adenocarcinomas, 8.3%). Fusion rates were significantly higher compared with the microsatellite stable and "gene driver positive" MSKCC cohorts. Pan-TRK immunohistochemistry showed 100% sensitivity, 91.7% specificity, and the occurrence of heterogeneous and/or subtle staining patterns. The enrichment of gene fusions in this "real-world" cohort highlights the feasibility of a workflow applicable in clinical practice. The heterogeneous expression in NTRK fusion positive tumours unveils challenging patterns to recognize and raises questions on the effective translation of the chimeric protein. [ABSTRACT FROM AUTHOR]

Published

2021

6. Pazopanib and Trametinib as a Synergistic Strategy against Osteosarcoma: Preclinical Activity and Molecular Insights.

Author

Chiabotto, Giulia, Grignani, Giovanni, Todorovic, Maja, Martin, Valentina, Centomo, Maria Laura, Prola, Elisa, Giordano, Giorgia, Merlini, Alessandra, Miglio, Umberto, Berrino, Enrico, Napione, Lucia, Isella, Claudio, Capozzi, Federica, Basiricò, Marco, Marsero, Cristina, Gerardi, Ilaria, Venesio, Tiziana, Sangiolo, Dario, Aglietta, Massimo, and D'Ambrosio, Lorenzo

Subjects

CELL proliferation, ANIMAL experimentation, ANTINEOPLASTIC agents, BIOLOGICAL models, CELL lines, CELL receptors, CELLULAR signal transduction, GENE expression, INTERLEUKINS, MEMBRANE proteins, MICE, NANOTECHNOLOGY, OSTEOSARCOMA, MOLECULAR pathology, TRANSFERASES, WESTERN immunoblotting, XENOGRAFTS, PROTEIN-tyrosine kinase inhibitors, MITOGEN-activated protein kinases, IN vitro studies, IN vivo studies

Abstract

Receptor tyrosine kinases (RTKs) inhibitors' activity in advanced osteosarcoma is significant but short-lived. To prevent or at least delay drug resistance, we explored a vertical inhibition by combining drugs acting at different levels of the RTK pathways (pazopanib + trametinib). We studied pazopanib + trametinib antitumor activity both in vitro and in vivo (MNNG-HOS and KHOS xenografts in NOD/SCID mice) investigating the molecular mechanisms and potential escapes. The involvement of MAPK-PI3K pathways was validated by Nanostring technology, western blot and by silencing/overexpression experiments. Pazopanib targets were expressed on seven osteosarcoma cell lines and their pathways were activated. Pazopanib + trametinib exhibited synergistic antitumor activity by inducing apoptosis and inhibiting ERK1/2 and Akt. In vivo antitumor activity was shown in osteosarcoma-bearing mice. The drug combination significantly down-modulated RTK Ephrin Type-A Receptor 2 (EphA2) and Interleukin-7 Receptor (IL-7R), whereas induced mitogen-activated protein-kinase kinase (MAPKK) MEK6. EphA2 silencing significantly reduced osteosarcoma cell proliferation and migration, while impeding MEK6 up-regulation in the treated cells significantly increased the antitumor effect of the studied drugs. Moreover, the up-regulation of MEK6 reduced combination activity. Pazopanib + trametinib demonstrated synergistic antitumor effects in osteosarcoma models through ERK and Akt inhibition and EphA2 and IL-7R down-modulation. MEK6 up-regulation might evoke escaping mechanism. [ABSTRACT FROM AUTHOR]

Published

2020

7. PIK3R1W624R Is an Actionable Mutation in High Grade Serous Ovarian Carcinoma.

Author

D'Ambrosio, Concetta, Erriquez, Jessica, Arigoni, Maddalena, Capellero, Sonia, Mittica, Gloria, Ghisoni, Eleonora, Borella, Fulvio, Katsaros, Dionyssios, Privitera, Silvana, Ribotta, Marisa, Maldi, Elena, Di Nardo, Giovanna, Berrino, Enrico, Venesio, Tiziana, Ponzone, Riccardo, Vaira, Marco, Hall, Douglas, Jimenez-Linan, Mercedes, Paterson, Anna L., and Calogero, Raffaele A.

Subjects

OVARIAN epithelial cancer, CARCINOMA, GENETIC mutation, PYROSEQUENCING, OVARIAN cancer, INTEGERS

Abstract

Identifying cancer drivers and actionable mutations is critical for precision oncology. In epithelial ovarian cancer (EOC) the majority of mutations lack biological or clinical validation. We fully characterized 43 lines of Patient-Derived Xenografts (PDXs) and performed copy number analysis and whole exome sequencing of 12 lines derived from naïve, high grade EOCs. Pyrosequencing allowed quantifying mutations in the source tumours. Drug response was assayed on PDX Derived Tumour Cells (PDTCs) and in vivo on PDXs. We identified a PIK3R1W624R variant in PDXs from a high grade serous EOC. Allele frequencies of PIK3R1W624R in all the passaged PDXs and in samples of the source tumour suggested that it was truncal and thus possibly a driver mutation. After inconclusive results in silico analyses, PDTCs and PDXs allowed the showing actionability of PIK3R1W624R and addiction of PIK3R1W624R carrying cells to inhibitors of the PI3K/AKT/mTOR pathway. It is noteworthy that PIK3R1 encodes the p85α regulatory subunit of PI3K, that is very rarely mutated in EOC. The PIK3R1W624R mutation is located in the cSH2 domain of the p85α that has never been involved in oncogenesis. These data show that patient-derived models are irreplaceable in their role of unveiling unpredicted driver and actionable variants in advanced ovarian cancer. [ABSTRACT FROM AUTHOR]

Published

2020

8. Establishment and Characterization of a New Intrahepatic Cholangiocarcinoma Cell Line Resistant to Gemcitabine.

Author

Varamo, Chiara, Peraldo-Neia, Caterina, Ostano, Paola, Basiricò, Marco, Raggi, Chiara, Bernabei, Paola, Venesio, Tiziana, Berrino, Enrico, Aglietta, Massimo, Leone, Francesco, and Cavalloni, Giuliana

Subjects

ANTIMETABOLITES, BIOLOGICAL models, CELL cycle, CELL lines, DRUG resistance in cancer cells, PACLITAXEL, POLYMERASE chain reaction, XENOBIOTICS, CHOLANGIOCARCINOMA, REVERSE transcriptase polymerase chain reaction, GENE expression profiling, DOXYCYCLINE, PATHOLOGIC neovascularization, IN vitro studies, IN vivo studies

Abstract

Intrahepatic cholangiocarcinoma (ICC) is one of the most lethal liver cancers. Late diagnosis and chemotherapy resistance contribute to the scarce outfit and poor survival. Resistance mechanisms are still poorly understood. Here, we established a Gemcitabine (GEM) resistant model, the MT-CHC01R1.5 cell line, obtained by a GEM gradual exposure (up to 1.5 µM) of the sensitive counterpart, MT-CHC01. GEM resistance was irreversible, even at high doses. The in vitro and in vivo growth was slower than MT-CHC01, and no differences were highlighted in terms of migration and invasion. Drug prediction analysis suggested that Paclitaxel and Doxycycline might overcome GEM resistance. Indeed, in vitro MT-CHC01R1.5 growth was reduced by Paclitaxel and Doxycycline. Importantly, Doxycycline pretreatment at very low doses restored GEM sensitivity. To assess molecular mechanisms underlying the acquisition of GEM resistance, a detailed analysis of the transcriptome in MT-CHC01R1.5 cells versus the corresponding parental counterpart was performed. Transcriptomic analysis showed that most up-regulated genes were involved in cell cycle regulation and in the DNA related process, while most down-regulated genes were involved in the response to stimuli, xenobiotic metabolism, and angiogenesis. Furthermore, additional panels of drug resistance and epithelial to mesenchymal transition genes (n = 168) were tested by qRT-PCR and the expression of 20 genes was affected. Next, based on a comparison between qRT-PCR and microarray data, a list of up-regulated genes in MT-CHC01R1.5 was selected and further confirmed in a primary cell culture obtained from an ICC patient resistant to GEM. In conclusion, we characterized a new GEM resistance ICC model that could be exploited either to study alternative mechanisms of resistance or to explore new therapies. [ABSTRACT FROM AUTHOR]

Published

2019

9. PIK3R1 W624R Is an Actionable Mutation in High Grade Serous Ovarian Carcinoma.

Author

D'Ambrosio C, Erriquez J, Arigoni M, Capellero S, Mittica G, Ghisoni E, Borella F, Katsaros D, Privitera S, Ribotta M, Maldi E, Di Nardo G, Berrino E, Venesio T, Ponzone R, Vaira M, Hall D, Jimenez-Linan M, Paterson AL, Calogero RA, Brenton JD, Valabrega G, Di Renzo MF, and Olivero M

Subjects

Animals, Carcinoma, Ovarian Epithelial drug therapy, Carcinoma, Ovarian Epithelial enzymology, Cell Line, Tumor, Class Ia Phosphatidylinositol 3-Kinase metabolism, Cystadenocarcinoma, Serous drug therapy, Cystadenocarcinoma, Serous enzymology, Female, Heterografts, Humans, Mice, Mice, Inbred NOD, Mice, SCID, Molecular Targeted Therapy, Mutation, Neoplasm Grading, Ovarian Neoplasms drug therapy, Ovarian Neoplasms enzymology, Random Allocation, Carcinoma, Ovarian Epithelial genetics, Class Ia Phosphatidylinositol 3-Kinase genetics, Cystadenocarcinoma, Serous genetics, Ovarian Neoplasms genetics

Abstract

Identifying cancer drivers and actionable mutations is critical for precision oncology. In epithelial ovarian cancer (EOC) the majority of mutations lack biological or clinical validation. We fully characterized 43 lines of Patient-Derived Xenografts (PDXs) and performed copy number analysis and whole exome sequencing of 12 lines derived from naïve, high grade EOCs. Pyrosequencing allowed quantifying mutations in the source tumours. Drug response was assayed on PDX Derived Tumour Cells (PDTCs) and in vivo on PDXs. We identified a PIK3R1 W624R variant in PDXs from a high grade serous EOC. Allele frequencies of PIK3R1 W624R in all the passaged PDXs and in samples of the source tumour suggested that it was truncal and thus possibly a driver mutation. After inconclusive results in silico analyses, PDTCs and PDXs allowed the showing actionability of PIK3R1 W624R and addiction of PIK3R1 W624R carrying cells to inhibitors of the PI3K/AKT/mTOR pathway. It is noteworthy that PIK3R1 encodes the p85α regulatory subunit of PI3K, that is very rarely mutated in EOC. The PIK3R1 W624R mutation is located in the cSH2 domain of the p85α that has never been involved in oncogenesis. These data show that patient-derived models are irreplaceable in their role of unveiling unpredicted driver and actionable variants in advanced ovarian cancer., Competing Interests: The authors declare no competing interests.

Published

2020