Your search keyword '"Claudio Scuoppo"' showing total 21 results

1. Dysregulation of cell polarity proteins synergize with oncogenes or the microenvironment to induce invasive behavior in epithelial cells.

Author

Samit Chatterjee, Laurie Seifried, Michael E Feigin, Don L Gibbons, Claudio Scuoppo, Wei Lin, Zain H Rizvi, Evan Lind, Dilan Dissanayake, Jonathan Kurie, Pam Ohashi, and Senthil K Muthuswamy

Subjects

Medicine, Science

Abstract

Changes in expression and localization of proteins that regulate cell and tissue polarity are frequently observed in carcinoma. However, the mechanisms by which changes in cell polarity proteins regulate carcinoma progression are not well understood. Here, we report that loss of polarity protein expression in epithelial cells primes them for cooperation with oncogenes or changes in tissue microenvironment to promote invasive behavior. Activation of ErbB2 in cells lacking the polarity regulators Scribble, Dlg1 or AF-6, induced invasive properties. This cooperation required the ability of ErbB2 to regulate the Par6/aPKC polarity complex. Inhibition of the ErbB2-Par6 pathway was sufficient to block ErbB2-induced invasion suggesting that two polarity hits may be needed for ErbB2 to promote invasion. Interestingly, in the absence of ErbB2 activation, either a combined loss of two polarity proteins, or exposure of cells lacking one polarity protein to cytokines IL-6 or TNFα induced invasive behavior in epithelial cells. We observed the invasive behavior only when cells were plated on a stiff matrix (Matrigel/Collagen-1) and not when plated on a soft matrix (Matrigel alone). Cells lacking two polarity proteins upregulated expression of EGFR and activated Akt. Inhibition of Akt activity blocked the invasive behavior identifying a mechanism by which loss of polarity promotes invasion of epithelial cells. Thus, we demonstrate that loss of polarity proteins confers phenotypic plasticity to epithelial cells such that they display normal behavior under normal culture conditions but display aggressive behavior in response to activation of oncogenes or exposure to cytokines.

Published

2012

2. Repurposing dasatinib for diffuse large B cell lymphoma

Author

Mirjana Persaud, Laura Pasqualucci, Katia Basso, Jiguang Wang, Raul Rabadan, Riccardo Dalla-Favera, Carla Grandori, Claudio Scuoppo, Francesc Bosch, Sandeep K. Mittan, and Giorgio Inghirami

Subjects

Dasatinib, Mechanistic Target of Rapamycin Complex 2, Proof of Concept Study, Mice, Phosphatidylinositol 3-Kinases, chemistry.chemical_compound, Piperidines, immune system diseases, In vivo, Cell Line, Tumor, hemic and lymphatic diseases, medicine, Animals, Humans, PTEN, PI3K/AKT/mTOR pathway, Multidisciplinary, biology, business.industry, Kinase, Adenine, PTEN Phosphohydrolase, Biological Sciences, medicine.disease, Xenograft Model Antitumor Assays, Pyrimidines, chemistry, Drug Resistance, Neoplasm, Cell culture, Ibrutinib, biology.protein, Cancer research, Pyrazoles, Lymphoma, Large B-Cell, Diffuse, business, Diffuse large B-cell lymphoma, medicine.drug

Abstract

To repurpose compounds for diffuse large B cell lymphoma (DLBCL), we screened a library of drugs and other targeted compounds approved by the US Food and Drug Administration on 9 cell lines and validated the results on a panel of 32 genetically characterized DLBCL cell lines. Dasatinib, a multikinase inhibitor, was effective against 50% of DLBCL cell lines, as well as against in vivo xenografts. Dasatinib was more broadly active than the Bruton kinase inhibitor ibrutinib and overcame ibrutinib resistance. Tumors exhibiting dasatinib resistance were commonly characterized by activation of the PI3K pathway and loss of PTEN expression as a specific biomarker. PI3K suppression by mTORC2 inhibition synergized with dasatinib and abolished resistance in vitro and in vivo. These results provide a proof of concept for the repurposing approach in DLBCL, and point to dasatinib as an attractive strategy for further clinical development in lymphomas.

Published

2019

3. Repurposing NAD Salvage Inhibitors for GCB Diffuse Large-B Cell Lymphoma

Author

Bowen Cai, Laura Pasqualucci, Kenneth Ofori, Riccardo Dalla-Favera, Claudio Scuoppo, Hanna Scholze, and Katia Basso

Subjects

Chemistry, hemic and lymphatic diseases, Immunology, medicine, Cancer research, NAD salvage, Cell Biology, Hematology, medicine.disease, Biochemistry, Diffuse large B-cell lymphoma, Repurposing

Abstract

Diffuse large B-cell lymphomas (DLBCLs) are a heterogeneous group of diseases in terms of cell of origin, genetics and clinical outcome. About 30% of all DLBCL patients represent an unmet clinical need as they either do not respond to the standard first line chemo-immunotherapy or recur after initial remission. DLBCL classifications based on the NMF (Non-Negative Matrix Factorization) and LymphGen algorithms have led to the identification of genetic subtypes based on the co-occurrence of specific lesions. Repositioning drugs that are approved or in active clinical development for other indications can be a powerful strategy to match these newly uncovered DLBCL subtypes to targeted therapies. We have previously shown that the screening of large panels of DLBCL cell lines representative of the genetics of the disease can facilitate the repositioning of approved drugs for biomarker-selected populations of DLBCL patients. Repositioned drugs can then be rapidly translated to the clinical use, as they have already been extensively characterized for their safety profile. As a proof of concept, we have demonstrated that Dasatinib, a Src/Abl inhibitor approved for B-cell Acute Lymphoblastic Leukemia and Chronic Myelogenous Leukemia, is highly effective in PTEN-positive DLBCLs, irrespective of their COO class (Scuoppo et al., PNAS 2019). Here we present the results of a new screening that was performed on a panel of eight cell lines (4 ABC- and 4 GCB-DLBCLs) to test the activity of 212 drugs, either approved or in advanced clinical development, for repositioning in DLBCL, followed by validation in a larger panel of 34 genetically characterized cell lines. Our results point to inhibitors of the Nicotinamide Phosphoribosyl Transferase (NAMPT) as potently active in 63% of GCB-DLBCLs. NAMPT catalyzes the conversion of Nicotinamide (NAM) to Beta-Nicotinamide Mononucleotide (Beta-NMN). This reaction is the rate-limiting step of the Nicotinamide Adenine Dinucleotide (NAD) salvage pathway, the major metabolic route of NAD regeneration in mammalian cells. We validated the on-target activity of NAMPT inhibitors by multiple genetic and pharmacological approaches. First, we found that the activities of three chemically distinct drugs (FK-866, STF-118804 and KPT-9274) were highly correlated across the 34 lines DLBCL panel. Second, we were able to abolish the activity of all three NAMPT inhibitors by supplementing cells with Beta-NMN. Third, we showed that transduction of the drug-resistant mutant NAMPT H191R offsets the activity of the drugs. Dose-response assays on the full DLBCL cell line panel confirmed ABC-DLBCL resistance and also highlighted the presence of sensitive (GCB-S) and resistant (GCB-R) GCB subsets that can be separated by a subnanomolar IC50 threshold. To generate biomarkers capable of predicting GCB-S patients, we examined the RNA-seq profiles and genetic make-ups of the DLBCL cell lines collection and observed that the GCB-S subset was associated to the LymphGen EZB subtype, characterized by the presence of EZH2 mutations and BCL2 translocations. Conversely, the GCB-R subtype was linked to a 5-gene expression signature for the Kynurenine De Novo pathway, an alternative route for NAD synthesis. Accordingly, expression of each of the five De Novo Kynurenine pathway genes induced resistance to NAMPT inhibitors. These results were validated in xenotransplants of luciferized DLBCL lines and Patient Derived Xenotransplant models (PDXs) that were transcriptionally classified for the status of the Kynurenine De Novo signature. Together, these data support the repositioning of NAMPT inhibitors as a therapeutically relevant strategy for EZB-type GCB-DLBCLs. Disclosures Pasqualucci: Astra Zeneca: Research Funding; Sanofi: Research Funding.

Published

2021

4. LMO2 as a Biomarker for Hypersensitivity to Genotoxic Therapy

Author

Claudio Scuoppo and Shan Zha

Subjects

0301 basic medicine, LMO2, Cancer Research, DNA repair, DNA damage, Poly ADP ribose polymerase, Poly(ADP-ribose) Polymerase Inhibitors, Poly (ADP-Ribose) Polymerase Inhibitor, Article, 03 medical and health sciences, 0302 clinical medicine, hemic and lymphatic diseases, Proto-Oncogene Proteins, Medicine, Adaptor Proteins, Signal Transducing, business.industry, Cell Biology, LIM Domain Proteins, Isogenic human disease models, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, Biomarker (medicine), business, Synthetic Lethal Mutations, DNA Damage

Abstract

Deficiency in DNA double-strand break (DSB) repair mechanisms has been widely exploited for the treatment of different malignances, including homologous recombination (HR)-deficient breast and ovarian cancers. Here we demonstrate that diffuse large B cell lymphomas (DLBCL) expressing LMO2 protein are functionally deficient in HR-mediated DSB repair. Mechanistically, LMO2 inhibits BRCA1 recruitment to DSBs by interacting with 53BP1 during repair. Similar to BRCA1-deficient cells, LMO2 positive DLBCL and T cell acute lymphoblastic leukemia (T-ALL) cells exhibit a high sensitivity to Poly (ADP-ribose) polymerase (PARP) inhibitors. Further, chemotherapy and PARP inhibitors synergize to inhibit the growth of LMO2 positive tumors. Together, our results reveal that LMO2 expression predicts HR-deficiency and the potential therapeutic utility of PARP inhibitors in DLBCL and T-ALL.

Published

2019

5. Deletions linked to TP53 loss drive cancer through p53-independent mechanisms

Author

Nikolaus Schultz, Qingguo Wang, Sarah Ackermann, Ross L. Levine, Lihua Cheng, Zhengmin Xu, Claudio Scuoppo, Benedikt Bosbach, Jianjiong Gao, Timour Baslan, Yu Liu, Ting Niu, Edward R. Kastenhuber, Scott W. Lowe, Alea A. Mills, Chong Chen, Cory D. Rillahan, and Barbara Spitzer

Subjects

Male, 0301 basic medicine, Heterozygote, Lymphoma, Biology, medicine.disease_cause, Synteny, law.invention, Loss of heterozygosity, Mice, 03 medical and health sciences, Peptide Initiation Factors, law, Neoplasms, medicine, Animals, Humans, Missense mutation, Allele, Gene, Alleles, Sequence Deletion, Genetics, Multidisciplinary, RNA-Binding Proteins, Cancer, Heterozygote advantage, Genes, p53, medicine.disease, Chromosomes, Mammalian, Disease Models, Animal, Leukemia, Myeloid, Acute, Cell Transformation, Neoplastic, 030104 developmental biology, Disease Progression, Suppressor, Female, Tumor Suppressor Protein p53, Carcinogenesis, Chromosomes, Human, Pair 17

Abstract

Mutations disabling the TP53 tumour suppressor gene represent the most frequent events in human cancer and typically occur through a two-hit mechanism involving a missense mutation in one allele and a 'loss of heterozygosity' deletion encompassing the other. While TP53 missense mutations can also contribute gain-of-function activities that impact tumour progression, it remains unclear whether the deletion event, which frequently includes many genes, impacts tumorigenesis beyond TP53 loss alone. Here we show that somatic heterozygous deletion of mouse chromosome 11B3, a 4-megabase region syntenic to human 17p13.1, produces a greater effect on lymphoma and leukaemia development than Trp53 deletion. Mechanistically, the effect of 11B3 loss on tumorigenesis involves co-deleted genes such as Eif5a and Alox15b (also known as Alox8), the suppression of which cooperates with Trp53 loss to produce more aggressive disease. Our results imply that the selective advantage produced by human chromosome 17p deletion reflects the combined impact of TP53 loss and the reduced dosage of linked tumour suppressor genes.

Published

2016

6. Somatic CLL mutations occur at multiple distinct hematopoietic maturation stages: Documentation and cautionary note regarding cell fraction purity

Author

Mohammad Hadigol, Kanti R. Rai, Sonia Marsilio, Pedro Marín, Nicholas Chiorazzi, Raul Rabadan, Laura Pasqualucci, Stephen Devereux, Elizabeth J. Shpall, Emili Montserrat, Stefano Vergani, Giulia Fabbri, Claudio Scuoppo, and Hossein Khiabanian

Subjects

0301 basic medicine, Male, medicine.medical_specialty, Cancer Research, Somatic cell, Chronic lymphocytic leukemia, Antigens, CD19, Disease, Biology, CD5 Antigens, Monocytes, Pathogenesis, 03 medical and health sciences, hemic and lymphatic diseases, Internal medicine, Hematology, Oncology, medicine, Humans, Allele, Letter to the Editor, Alleles, Aged, Hematopoietic Stem Cell Transplantation, Cell Fraction, Middle Aged, medicine.disease, Hematopoietic Stem Cells, Leukemia, Lymphocytic, Chronic, B-Cell, Leukemia, 030104 developmental biology, Mutation, Cancer research, Female, Tumor Suppressor Protein p53

Abstract

Somatic CLL mutations occur at multiple distinct hematopoietic maturation stages: documentation and cautionary note regarding cell fraction purity

Published

2018

7. Common nonmutational NOTCH1 activation in chronic lymphocytic leukemia

Author

Davide Rossi, Nicholas Chiorazzi, Xiao-Jie Yan, Antony B. Holmes, Giulia Fabbri, Gianluca Gaidano, Yasmine Kieso, Daniel Herranz, Adolfo A. Ferrando, Laura Belver, Mara Viganotti, Claudio Scuoppo, and Riccardo Dalla-Favera

Subjects

0301 basic medicine, Chronic lymphocytic leukemia, Genes, myc, Gene mutation, Biology, medicine.disease_cause, Pathogenesis, 03 medical and health sciences, hemic and lymphatic diseases, medicine, Humans, Receptor, Notch1, Gene, Cell Proliferation, B-Lymphocytes, Mutation, Multidisciplinary, Oncogene, Gene Expression Regulation, Leukemic, medicine.disease, Leukemia, Lymphocytic, Chronic, B-Cell, 030104 developmental biology, PNAS Plus, embryonic structures, Immunology, cardiovascular system, sense organs, biological phenomena, cell phenomena, and immunity, Signal transduction, Intracellular

Abstract

Significance A pathogenetic role of NOTCH1 in chronic lymphocytic leukemia (CLL) has been implied by the presence of deregulating mutations in a relatively small fraction of cases. Our results now indicate that ∼50% of CLL cases devoid of mutations express the active form of NOTCH1 ICN1 (intracellular portion of NOTCH1), thus implicating a much broader role of this transcription factor in the disease. ICN1 + CLL cases display equivalent NOTCH1-dependent transcriptional responses regardless of the gene mutation status, indicating that the detection of ICN1 represents a reliable biomarker of NOTCH1 activation for diagnostic and therapeutic targeting. Finally, our results identify the NOTCH1-dependent transcriptional program in CLL cells, thus providing direct insights into the pathogenesis of a large fraction of CLL cases.

Published

2017

8. Lentiviral-based approach for the validation of cancer therapeutic targets in vivo

Author

Chiara Ambrogio, Patrick Stern, David Santamaría, Harald Kranz, Mariano Barbacid, and Claudio Scuoppo

Subjects

Computational biology, Biology, Pharmacology, General Biochemistry, Genetics and Molecular Biology, Target validation, Cell Line, Viral vector, Proto-Oncogene Proteins p21(ras), Cancer mouse model, Mice, 03 medical and health sciences, 0302 clinical medicine, Human disease, In vivo, Cell Line, Tumor, Neoplasms, medicine, Animals, Humans, 030304 developmental biology, 0303 health sciences, Tumor, Animal, Tumor biology, Lentivirus, Lentiviral delivery, DNA, Disease Models, Animal, Plasmids, Proto-Oncogene Proteins c-raf, Reproducibility of Results, Cancer, medicine.disease, 3. Good health, Experimental strategy, 030220 oncology & carcinogenesis, Disease Models, Biotechnology

Abstract

Despite the pressing need for novel cancer treatments, our improved understanding of tumor biology is not being successfully translated into better therapies. Here we present a lentiviral vector that enables in vivo validation of cancer therapeutic targets when combined with existing cancer animal models that faithfully reproduce the natural history of human disease. Unlike the conventional genetic approaches with targeted alleles, the outlined experimental strategy could be used to assess the preclinical efficacy of a growing number of putative therapeutic hits in a rapid and cost-effective manner.

Published

2014

9. A common functional consequence of tumor-derived mutations within c-MYC

Author

Lance R. Thomas, Scott W. Lowe, Soumyadeep Dey, Claudio Scuoppo, William P. Tansey, Abhishek A. Chakraborty, and Shelly L. Lorey

Subjects

Cancer Research, Lymphoma, Mutant, Mutation, Missense, MYC, Biology, medicine.disease_cause, Article, Conserved sequence, Proto-Oncogene Proteins c-myc, Mice, lymphomagenesis, Cell Line, Tumor, Genetics, medicine, Animals, Humans, Amino Acid Sequence, Molecular Biology, Conserved Sequence, Phenocopy, Oncogene, Wild type, DNA, mutations, Cancer research, NIH 3T3 Cells, Degron, Carcinogenesis

Abstract

The relevance of changes to the coding sequence of the c-MYC oncogene to malignancy is controversial. Overexpression of a pristine form of MYC is observed in many cancers and is sufficient to drive tumorigenesis in most contexts. Yet missense changes to MYC are found in ~50% of Burkitt’s lymphomas, aggregate within an amino-terminal degron important for proteasomal destruction of MYC, and where examined profoundly enhance the tumorigenic properties of MYC in vitro and in vivo. Much of the controversy surrounding these mutants stems from the limited number of mutations that have been evaluated and their clustering within a single region of the MYC protein; the highly-conserved Myc box I (MbI) element. Here, by analysis of extant genomic data sets, we identify a previously-unrecognized hotspot for tumor-associated MYC mutations, located in a conserved central portion of the protein. We show that, despite their distal location in MYC, mutations in this region precisely phenocopy those in MbI in terms of stability, in vitro transformation, growth-promoting properties, in vivo tumorigenesis, and ability to escape p53-dependent tumor surveillance mechanisms. The striking parallels between the behavior of tumor-derived mutations in disparate regions of the MYC protein reveals that a common molecular process is disrupted by these mutations, implying an active role for these mutations in tumorigenesis and suggesting that different therapeutic strategies may be needed for treatment of lymphomas expressing wild-type versus mutant forms of MYC protein.

Published

2014

10. A CRISPR/Cas9 Functional Screen Identifies Rare Tumor Suppressors

Author

Regina Cencic, Jerry Pelletier, Francis Robert, Claudio Scuoppo, Alexandra Katigbak, and Patrick Sénécha

Subjects

0301 basic medicine, Cancer Model, Biology, medicine.disease_cause, Article, law.invention, 03 medical and health sciences, Mice, Genome editing, law, medicine, Bystander effect, CRISPR, Animals, Genes, Tumor Suppressor, Genetics, Mutation, Multidisciplinary, Cas9, Burkitt Lymphoma, 030104 developmental biology, Cell Transformation, Neoplastic, Suppressor, Female, CRISPR-Cas Systems, Large-Scale Sequencing

Abstract

An enormous amount of tumor sequencing data has been generated through large scale sequencing efforts. The functional consequences of the majority of mutations identified by such projects remain an open, unexplored question. This problem is particularly complicated in the case of rare mutations where frequency of occurrence alone or prediction of functional consequences are insufficient to distinguish driver from passenger or bystander mutations. We combine genome editing technology with a powerful mouse cancer model to uncover previously unsuspected rare oncogenic mutations in Burkitt’s lymphoma. We identify two candidate tumor suppressors whose loss cooperate with MYC over-expression to accelerate lymphomagenesis. Our results highlight the utility of in vivo CRISPR/Cas9 screens combined with powerful mouse models to identify and validate rare oncogenic modifier events from tumor mutational data.

Published

2016

11. A tumour suppressor network relying on the polyamine–hypusine axis

Author

Jerry Pelletier, José Reyes, Cristian I. Ruse, Lisa M Lindqvist, Alexander Krasnitz, Scott W. Lowe, Seungtai Yoon, Julie Teruya-Feldstein, Darryl J. Pappin, Claudio Scuoppo, Iris Appelmann, and Cornelius Miething

Subjects

Lymphoma, B-Cell, Biology, medicine.disease_cause, Article, law.invention, Small hairpin RNA, Mice, chemistry.chemical_compound, law, Cell Line, Tumor, Polyamines, medicine, Animals, Humans, Gene Regulatory Networks, Genetic Testing, RNA, Small Interfering, Gene, Hypusine, Genetics, Multidisciplinary, Lysine, Tumor Suppressor Proteins, Point mutation, Reproducibility of Results, RNA, Mice, Inbred C57BL, Disease Models, Animal, chemistry, Cancer research, Suppressor, Female, Carcinogenesis, EIF5A, Gene Deletion

Abstract

Tumour suppressor genes encode a broad class of molecules whose mutational attenuation contributes to malignant progression. In the canonical situation, the tumour suppressor is completely inactivated through a two-hit process involving a point mutation in one allele and chromosomal deletion of the other1. Here, to identify tumour suppressor genes in lymphoma, we screen a short hairpin RNA library targeting genes deleted in human lymphomas. We functionally identify those genes whose suppression promotes tumorigenesis in a mouse lymphoma model. Of the nine tumour suppressors we identified, eight correspond to genes occurring in three physically linked ‘clusters’, suggesting that the common occurrence of large chromosomal deletions in human tumours reflects selective pressure to attenuate multiple genes. Among the new tumour suppressors are adenosylmethionine decarboxylase 1 (AMD1) and eukaryotic translation initiation factor 5A (eIF5A), two genes associated with hypusine, a unique amino acid produced as a product of polyamine metabolism through a highly conserved pathway2. Through a secondary screen surveying the impact of all polyamine enzymes on tumorigenesis, we establish the polyamine–hypusine axis as a new tumour suppressor network regulating apoptosis. Unexpectedly, heterozygous deletions encompassing AMD1 and eIF5A often occur together in human lymphomas and co-suppression of both genes promotes lymphomagenesis in mice. Thus, some tumour suppressor functions can be disabled through a two-step process targeting different genes acting in the same pathway.

Published

2012

12. Control of the senescence-associated secretory phenotype by NF-κB promotes senescence and enhances chemosensitivity

Author

Scott C. Kogan, Xiaowo Wang, Weijun Luo, Cheng S. Lee, Jessica E. Bolden, Xueping Fang, Claudio Scuoppo, Prem K. Premsrirut, Scott W. Lowe, Agustin Chicas, Yuchen Chien, and Brian M. Balgley

Subjects

Senescence, Cell cycle checkpoint, Lymphoma, Cell Survival, Drug Resistance, Biology, medicine.disease_cause, Cell Line, Mice, chemistry.chemical_compound, Cell Line, Tumor, Genetics, medicine, Animals, Humans, RNA, Small Interfering, Transcription factor, Cellular Senescence, Protein Synthesis Inhibitors, Transcription Factor RelA, NF-κB, Tetracycline, Chromatin, Gene Expression Regulation, Neoplastic, Phenotype, chemistry, Cell culture, Cancer research, Tumor Suppressor Protein p53, Carcinogenesis, Cell aging, Developmental Biology

Abstract

Cellular senescence acts as a potent barrier to tumorigenesis and contributes to the anti-tumor activity of certain chemotherapeutic agents. Senescent cells undergo a stable cell cycle arrest controlled by RB and p53 and, in addition, display a senescence-associated secretory phenotype (SASP) involving the production of factors that reinforce the senescence arrest, alter the microenvironment, and trigger immune surveillance of the senescent cells. Through a proteomics analysis of senescent chromatin, we identified the nuclear factor-κB (NF-κB) subunit p65 as a major transcription factor that accumulates on chromatin of senescent cells. We found that NF-κB acts as a master regulator of the SASP, influencing the expression of more genes than RB and p53 combined. In cultured fibroblasts, NF-κB suppression causes escape from immune recognition by natural killer (NK) cells and cooperates with p53 inactivation to bypass senescence. In a mouse lymphoma model, NF-κB inhibition bypasses treatment-induced senescence, producing drug resistance, early relapse, and reduced survival. Our results demonstrate that NF-κB controls both cell-autonomous and non-cell-autonomous aspects of the senescence program and identify a tumor-suppressive function of NF-κB that contributes to the outcome of cancer therapy.

Published

2011

13. Targeting Histone Acetyltransferase Gene Inactivation in Diffuse Large B Cell Lymphoma

Author

Stefanie N. Meyer, Sofija Vlasevska, Riccardo Dalla-Favera, Laura Garcia Ibanez, Claudio Scuoppo, and Laura Pasqualucci

Subjects

Histone Acetyltransferases, biology, Chemistry, 010401 analytical chemistry, Immunology, Follicular lymphoma, 02 engineering and technology, Cell Biology, Hematology, Histone acetyltransferase, 021001 nanoscience & nanotechnology, medicine.disease, 01 natural sciences, Biochemistry, Molecular biology, 0104 chemical sciences, Lymphoma, Cell culture, Acetyltransferase, biology.protein, medicine, Gene silencing, 0210 nano-technology, Diffuse large B-cell lymphoma

Abstract

Diffuse Large B-cell Lymphoma (DLBCL) is the most common form of non-Hodgkin lymphoma, accounting for ~30% of de-novo diagnoses and also arising as a frequent clinical evolution of indolent lymphomas. Although curable in a substantial fraction of cases, one third of patients do not achieve durable remissions, highlighting the need for novel, targeted therapies. Over the past decade, we and others have identified the CREBBP acetyltransferase and, less frequently, its paralogue EP300 as highly recurrent targets of inactivating somatic mutations/deletions in DLBCL and follicular lymphoma (FL) (30% and 60% of patients, respectively), indicating a prominent role in the pathogenesis of these tumors (Pasqualucci et al., Nature 2011). In most cases, mutations are heterozygous and the residual wildtype (WT) allele is expressed, suggesting a haploinsufficient tumor suppressor role. Indeed, germinal center (GC)-specific loss of Crebbp perturbs the expression of genes that are relevant to the normal biology of this structure, i.e. the lymphoma cell of origin, and cooperates with BCL2 deregulation to increase the incidence of tumors recapitulating the features of the human disease (Zhang et al., Cancer Discovery 2017). Intringuingly, while CREBBP binds to virtually all GC-specific superenhancers, no detrimental effects were observed upon its deletion in mice, suggesting the existence of compensatory mechanisms. Consistent with this hypothesis, inactivation of CREBBP and EP300 rarely coexist in human DLBCL and FL, suggesting that cells require a certain amount of acetyltransferase activity. To investigate whether EP300 compensates for CREBBP loss in the GC, we analyzed the GC responses in compound mouse models engineered to specifically delete these two genes (alone and in combination) upon SRBC immunization and induction of a Cγ1-driven Cre-recombinase. While CrebbpKOmice showed a mild increase in GC formation, as reported, loss of Ep300 led to ~40% reduction in the percentage of GC cells (mean: 1.8% vs 3.1% in WT littermates; p In order to probe if a similar dependency exists in neoplastic GC B cells, we used an inducible CRISPR/Cas9 system to delete EP300 (or a control non-genic region) in 4 DLBCL cell lines representative of the various CREBBP genotypes found in DLBCL, and monitored cell proliferation and survival in competition assays over 12 days. Compared to CREBBPWT, CREBBP heterozygous and homozygous mutant cells were significantly counter-selected from the total population following doxycycline induced EP300 deletion (~30% at day 7). Moreover, no EP300-edited clones were recovered from the CREBBP mutant lines in single cell plating assays, compared to CREBBP WT (p To explore this concept further, we generated isogenic DLBCL clones carrying WT or defective CREBBP alleles (n=4 each), and performed drug-sensitivity assays with 2 novel small molecule inhibitors that specifically target the CREBBP/EP300 HAT or BRD domain. While, at higher doses, both inhibitors interfered with cell growth in all clones, CREBBPKO cells were significantly more sensitive than their isogenic WT pairsat low nanomolar ranges (IC50: 60nM vs 300nM). Importantly, we were able to design an in vitro protocol that was toxic to CREBBPKO cells but tolerated by CREBBPWT cells, providing a proof of concept for therapeutically targeting these molecules. In conclusion, we show that CREBBP and EP300 have differential roles in normal GC B cell development and that CREBBP mutated cells are addicted to the residual EP300 activity. This dependency is maintained in DLBCL cells, providing the basis for the potential application of acetyl transferase inhibition into the clinical settings. Disclosures No relevant conflicts of interest to declare.

Published

2018

14. An In vivo Model of Met-Driven Lymphoma as a Tool to Explore the Therapeutic Potential of Met Inhibitors

Author

Francesca Bersani, Riccardo Taulli, Silvia Miretti, Tony Mangano, Carola Ponzetto, Paolo E. Forni, Giuseppe Lattanzio, Walter Dastrù, James G. Christensen, Paolo Accornero, Roberto Chiarle, Tiziana Crepaldi, and Claudio Scuoppo

Subjects

Genetically modified mouse, Cancer Research, Indoles, Lymphoma, Transgene, PHA-665752, Blotting, Western, Mice, Transgenic, Receptor tyrosine kinase, Mice, medicine, Animals, Humans, Sulfones, Protein Kinase Inhibitors, Met inhibitors, biology, Kinase, Gene Transfer Techniques, Cancer, Met-driven lymphoma, Proto-Oncogene Proteins c-met, medicine.disease, Immunohistochemistry, Disease Models, Animal, Oncology, Immunology, Cancer cell, Met, biology.protein, Cancer research, Hepatocyte growth factor, medicine.drug

Abstract

Purpose: Met, the tyrosine kinase receptor for hepatocyte growth factor, is frequently deregulated in human cancer. Recent evidence indicates that Met amplification may confer resistance to treatments directed toward other receptor tyrosine kinases. Thus, there is a need to develop Met inhibitors into therapeutic tools, to be used alone or in combination with other molecularly targeted drugs. Preclinical validation of Met inhibitors has thus far been done in nude mice bearing cancer cells xenogratfs. A far superior model would be a transgenic line developing spontaneous Met-driven tumors with high penetrance and short latency. Experimental Design: To this end, we introduced into the mouse genome TPR-MET, the oncogenic form of MET. The Tpr-Met protein ensures deregulation of Met signaling because dimerization motifs in the Tpr moiety cause ligand-independent activation of the Met kinase. Results: Here, we describe a TPR-MET transgenic line that develops thymic T-cell lymphoma with full penetrance and very short latency. In the tumors, Tpr-Met and its effectors were phosphorylated. Treatment of tumor-derived T lymphocytes with the selective Met inhibitor PHA-665752 at nanomolar concentrations abolished phosphorylation of Met and downstream effectors and led to caspase-mediated apoptosis. I.v. administration of PHA-665752 to transgenic mice bearing lymphomas in exponential growth phase led to a significant decrease in tumor growth and, in some cases, to tumor regression. Conclusions: Our transgenic line, which within 2 months reliably develops Tpr-Met–driven T-cell lymphoma, represents a valuable tool to explore the efficacy and therapeutic potential of Met kinase inhibitors as anticancer drugs.

Published

2008

15. Conditional Activation of MET in Differentiated Skeletal Muscle Induces Atrophy

Author

Paolo Accornero, David J. Glass, Tiziana Crepaldi, Claudio Scuoppo, Chiara Prunotto, Riccardo Taulli, Jennifer A. Griffiths, Carola Ponzetto, Paolo E. Forni, Roberto Chiarle, Christian Leo, and Francesca Bersani

Subjects

medicine.medical_specialty, Satellite Cells, Skeletal Muscle, Green Fluorescent Proteins, Mice, Transgenic, Protein degradation, Biology, p38 Mitogen-Activated Protein Kinases, Biochemistry, Mice, Atrophy, Internal medicine, Myosin, medicine, Animals, Phosphorylation, Molecular Biology, Protein kinase B, Myogenesis, Skeletal muscle, Cell Biology, Proto-Oncogene Proteins c-met, medicine.disease, Cell biology, Muscular Atrophy, medicine.anatomical_structure, Endocrinology, Gene Expression Regulation, ITGA7

Abstract

Skeletal muscle atrophy is a common debilitating feature of many systemic diseases, including cancer. Here we examined the effects of inducing expression of an oncogenic version of the Met receptor (Tpr-Met) in terminally differentiated skeletal muscle. A responder mouse containing the Tpr-Met oncogene and GFP (green fluorescent protein) as a reporter was crossed with a transactivator mouse expressing tTA under the control of the muscle creatine kinase promoter. Tpr-Met induction during fetal development and in young adult mice caused severe muscle wasting, with decreased fiber size and loss of myosin heavy chain protein. Concomitantly, in the Tpr-Met-expressing muscle the mRNA of the E3 ubiquitin ligases atrogin-1/MAFbx, MuRF1, and of the lysosomal protease cathepsin L, which are markers of skeletal muscle atrophy, was significantly increased. In the same muscles phosphorylation of the Met downstream effectors Akt, p38 MAPK, and IkappaBalpha was higher than in normal controls. Induction of Tpr-Met in differentiating satellite cells derived from the double transgenics caused aberrant cell fusion, protein loss, and myotube collapse. Increased phosphorylation of Met downstream effectors was also observed in the Tpr-Met-expressing myotubes cultures. Treatment of these cultures with either a proteasomal or a p38 inhibitor prevented Tpr-Met-mediated myotube breakdown, establishing accelerated protein degradation consequent to inappropriate activation of p38 as the major route for the Tpr-Met-induced muscle phenotype.

Published

2007

16. RNAi technology and lentiviral delivery as a powerful tool to suppress Tpr-Met-mediated tumorigenesis

Author

Antonia Follenzi, Paolo E. Forni, Tiziana Crepaldi, Carola Ponzetto, Riccardo Taulli, Claudio Scuoppo, Alessandro Morotti, Francesca Bersani, Luigi Naldini, Tony Mangano, Paolo Accornero, Roberto Chiarle, Taulli, R., Accornero, P., Follenzi, A., Mangano, T., Morotti, A., Scuoppo, C., Forni, P. E., Bersani, F., Crepaldi, T., Chiarle, R., Naldini, Luigi, and AND PONZETTO, C.

Subjects

Cancer Research, Small interfering RNA, Oncogene Proteins, Fusion, Genetic Vectors, Down-Regulation, Biology, medicine.disease_cause, Viral vector, Small hairpin RNA, Mice, Transduction, Genetic, RNA interference, Cell Line, Tumor, medicine, Animals, Humans, RNA, Small Interfering, Receptor, Molecular Biology, Cell Proliferation, Point mutation, Lentivirus, Genetic Therapy, Neoplasms, Experimental, Molecular biology, Transformation (genetics), Gene Expression Regulation, Cancer research, Molecular Medicine, RNA Interference, Carcinogenesis

Abstract

Tpr-Met, the oncogenic counterpart of the Met receptor, has been detected in gastric cancers, as well as in precursor lesions and in the adjacent normal gastric mucosa. This has prompted the suggestion that Tpr-Met may predispose to the development of gastric tumors. Given the sequence specificity of RNA interference, oncogenes activated by point mutation or rearrangements can be targeted while spearing the product of the wild-type allele. In this work, we report specific suppression of Tpr-Met expression and inhibition of Tpr-Met-mediated transformation and tumorigenesis by means of a short interfering RNA (siRNA) directed toward the Tpr-Met junction (anti-TM2). When delivered by a lentiviral vector, anti-TM2 siRNA was effective also in mouse embryonal fibroblasts or epithelial cells expressing high levels of Tpr-Met. Our results suggest that lentiviral-mediated delivery of anti-TM2 siRNA may be developed into a powerful tool to treat Tpr-Met-positive cancers.

Published

2005

17. Dysregulation of Cell Polarity Proteins Synergize with Oncogenes or the Microenvironment to Induce Invasive Behavior in Epithelial Cells

Author

Evan F. Lind, Claudio Scuoppo, Jonathan M. Kurie, Senthil K. Muthuswamy, Michael E. Feigin, Zain H. Rizvi, Pamela S. Ohashi, Wei Lin, Samit Chatterjee, Don L. Gibbons, Dilan Dissanayake, and Laurie A. Seifried

Subjects

Male, Receptor, ErbB-2, lcsh:Medicine, Gene Expression, Kinesins, Metastasis, Discs Large Homolog 1 Protein, Mice, 0302 clinical medicine, Cell Movement, Cell polarity, Molecular Cell Biology, Basic Cancer Research, Signaling in Cellular Processes, lcsh:Science, skin and connective tissue diseases, Epithelial polarity, 0303 health sciences, Multidisciplinary, Cell Polarity, Cell migration, Cell biology, ErbB Receptors, Oncology, Cellular Microenvironment, 030220 oncology & carcinogenesis, Medicine, Cytokines, Female, Inflammation Mediators, Cell Movement Signaling, Research Article, Signal Transduction, Cell type, Mice, 129 Strain, Polarity (physics), Biology, Myosins, Cell Line, 03 medical and health sciences, Animals, Humans, 030304 developmental biology, Adaptor Proteins, Signal Transducing, Matrigel, lcsh:R, Membrane Proteins, Epithelial Cells, Oncogenes, Membrane protein, Gene Expression Regulation, Cell culture, lcsh:Q, Proto-Oncogene Proteins c-akt

Abstract

Changes in expression and localization of proteins that regulate cell and tissue polarity are frequently observed in carcinoma. However, the mechanisms by which changes in cell polarity proteins regulate carcinoma progression are not well understood. Here, we report that loss of polarity protein expression in epithelial cells primes them for cooperation with oncogenes or changes in tissue microenvironment to promote invasive behavior. Activation of ErbB2 in cells lacking the polarity regulators Scribble, Dlg1 or AF-6, induced invasive properties. This cooperation required the ability of ErbB2 to regulate the Par6/aPKC polarity complex. Inhibition of the ErbB2-Par6 pathway was sufficient to block ErbB2-induced invasion suggesting that two polarity hits may be needed for ErbB2 to promote invasion. Interestingly, in the absence of ErbB2 activation, either a combined loss of two polarity proteins, or exposure of cells lacking one polarity protein to cytokines IL-6 or TNFα induced invasive behavior in epithelial cells. We observed the invasive behavior only when cells were plated on a stiff matrix (Matrigel/Collagen-1) and not when plated on a soft matrix (Matrigel alone). Cells lacking two polarity proteins upregulated expression of EGFR and activated Akt. Inhibition of Akt activity blocked the invasive behavior identifying a mechanism by which loss of polarity promotes invasion of epithelial cells. Thus, we demonstrate that loss of polarity proteins confers phenotypic plasticity to epithelial cells such that they display normal behavior under normal culture conditions but display aggressive behavior in response to activation of oncogenes or exposure to cytokines.

Published

2012

18. The oncogenic transcription factor PAX3-FKHR can convert fibroblasts into contractile myotubes

Author

Tiziana Crepaldi, Ilan Riess, Claudio Scuoppo, Riccardo Taulli, Paolo E. Forni, Carola Ponzetto, Michel Schmitt-Ney, Paola Allegra, Francesca Bersani, and Paolo Accornero

Subjects

medicine.medical_specialty, Oncogene Proteins, Fusion, Muscle Fibers, Skeletal, PAX3, Biology, Muscle Development, Transfection, Cell Line, Mice, Internal medicine, Precursor cell, medicine, Animals, Humans, Paired Box Transcription Factors, Transcription factor, Myogenesis, Contact inhibition, Pax3 fkhr, Cell Differentiation, Cell Biology, Fibroblasts, musculoskeletal system, medicine.disease, Cell biology, Transformation (genetics), Endocrinology, Cell Transformation, Neoplastic, embryonic structures, Alveolar rhabdomyosarcoma

Abstract

PAX3-FKHR, the product of a rearrangement of PAX3 with FKHR is the pathogenetic marker for alveolar rhabdomyosarcoma, an aggressive form of childhood cancer. In this work we show that PAX3-FKHR, which is a stronger transcriptional activator relative to PAX3, can lead to two apparently irreconcilable outcomes: transformation and terminal myogenic differentiation. Fibroblasts (10T1/2, NIH3T3, and a newly established murine line named 'Plus') transduced by PAX3-FKHR acquire transformed features such as anchorage independence and loss of contact inhibition and concomitantly undergo various degrees of myogenic conversion depending on the host cells, including, in the case of the Plus line, terminal differentiation into contractile myotubes. This work highlights the potential of PAX3-FKHR to functionally operate as a deregulated Pangene and may have implications with regard to the identity of the precursor cell giving rise to alveolar rhabdomyosarcoma.

Published

2006

19. Validation of met as a therapeutic target in alveolar and embryonal rhabdomyosarcoma

Author

Riccardo Taulli, Francesca Bersani, Paola Allegra, Alberto Grinza, Michel Schmitt-Ney, Carola Ponzetto, Silvia Miretti, Paolo Accornero, Paolo E. Forni, Tiziana Crepaldi, and Claudio Scuoppo

Subjects

Cancer Research, Pathology, medicine.medical_specialty, Oncogene Proteins, Fusion, Mice, Nude, Apoptosis, Cell Growth Processes, Biology, Small hairpin RNA, Mice, Transduction, Genetic, Proto-Oncogene Proteins, medicine, Animals, Humans, Paired Box Transcription Factors, Neoplasm Invasiveness, Receptors, Growth Factor, Rhabdomyosarcoma, Embryonal, Gene Silencing, RNA, Small Interfering, Rhabdomyosarcoma, Receptor, PAX3 Transcription Factor, Rhabdomyosarcoma, Alveolar, Forkhead Box Protein O1, Hepatocyte Growth Factor, Forkhead Transcription Factors, Proto-Oncogene Proteins c-met, musculoskeletal system, medicine.disease, Up-Regulation, Cell Transformation, Neoplastic, Oncology, Cell culture, embryonic structures, Alveolar rhabdomyosarcoma, Cancer research, NIH 3T3 Cells, Hepatocyte growth factor, Female, RNA Interference, Embryonal rhabdomyosarcoma, PAX7, medicine.drug, HeLa Cells

Abstract

Rhabdomyosarcoma (RMS) is a highly malignant soft-tissue tumor of childhood deriving from skeletal muscle cells. RMS can be classified in two major histologic subtypes: embryonal (ERMS) and alveolar (ARMS), the latter being characterized by the PAX3/7-FKHR translocation. Here we first investigated whether the Met receptor, a transcriptional target of PAX3 and PAX7, has a role in PAX3-FKHR–mediated transformation. Following PAX3-FKHR transduction, Met was up-regulated in mouse embryonal fibroblasts (MEF), NIH 3T3 and C2C12 cells, and they all acquired anchorage independence. This property was lost in low serum but addition of hepatocyte growth factor/scatter factor (HGF/SF) rescued soft-agar growth. Genetic proof that Met is necessary for this PAX3-FKHR–mediated effect was obtained by transducing with PAX3-FKHR MEFs derived from Met mutant (MetD/D) and wild-type (Met+/+) embryos. Only Met+/+ MEFs acquired anchorage-independent growth whereas PAX3-FKHR–transduced MetD/D cells were unable to form colonies in soft agar. To verify if Met had a role in RMS maintenance, we silenced the receptor by transducing ERMS and ARMS cell lines with an inducible lentivirus expressing an anti-Met short hairpin RNA (shRNA). Met down-regulation significantly affected RMS cells proliferation, survival, invasiveness, and anchorage-independent growth. Finally, induction of the Met-directed shRNA promoted a dramatic reduction of tumor mass in a xenograft model of RMS. Our data show that both ARMS- and ERMS-derived cell lines, in spite of the genetic drift which may have occurred in years of culture, seem to have retained an “addiction” to the Met oncogene and suggest that Met may represent a target of choice to develop novel therapeutic strategies for ARMS. (Cancer Res 2006; 66(9): 4742-9)

Published

2006

20. Suppression of EZH2 Accelerates MYC-Driven Lymphomagenesis By Inhibition of Apoptosis

Author

Iris Appelmann, Daniela Ledezma, Vishal Thapar, Claudio Scuoppo, Agustin Chicas, Amaia Lujambio, and Scott W. Lowe

Subjects

Oncogene, Cellular differentiation, Immunology, EZH2, Wild type, Follicular lymphoma, macromolecular substances, Cell Biology, Hematology, Biology, medicine.disease, Biochemistry, hemic and lymphatic diseases, Cancer research, medicine, SUZ12, Diffuse large B-cell lymphoma, Burkitt's lymphoma

Abstract

EZH2 is the catalytic component of the polycomb repressive complex 2 (PRC2), which also contains the non-catalytic subunits suppressor of zeste 12 (SUZ12) and embryonic ectoderm development (EED). This complex methylates histone H3 at lysine 27 (H3K27) which, together with H3K4 methylation, generates a bivalent “code” that primes genes for either expression or silencing. EZH2 is highly expressed in stem cells and many proliferating cells, downregulated in differentiated cells and frequently altered in cancer in ways that point to a context dependent role for this gene. For instance, overexpression of EZH2 has been described in prostate and breast cancer, where this overexpression is associated with invasive growth metastatic potential and poor clinical outcome. More recently, both gain and loss of function mutations of EZH2 were identified in human cancer. In particular, activating mutations of EZH2 affecting a tyrosine at position 641 located within the SET domain (Y641) were observed in lymphoma. In striking contrast to wild type EZH2 which catalyzes the monomethylation of H3K27 very efficiently and shows less efficient catalytic activity in the subsequent di- and trimethylation reactions, the mutation generates a neomorphic protein with enhanced catalytic activity and efficiency for di- and tri-methylation, hinting toward a “cooperation” of both wild type and mutant EZH2 to increase total H3K27me3 levels and representing a functional equivalent of EZH2 overexpression in human lymphoma. Gain of function mutations in EZH2 are frequent in Diffuse Large B-cell Lymphoma (DLBCL; 22%) and in Follicular Lymphoma (FL; 7%) and recent data implicate EZH2 as an oncogene in DLBCL and FL lymphomas. In contrast to DLBCL and FL, EZH2 mutations have so far never been identified in MYC-driven B-cell Non-Hodgkin Lymphoma (B-NHL), and EZH2 expression is suppressed in Burkitt’s Lymphoma (BL), a lymphoma for which a MYC translocation is pathognomonic, suggesting that in this context EZH2 could have a role different from its role in DLBCL and FL. We probed the role of EZH2 in MYC-driven lymphomagenesis by mimicking the loss of function mutations by RNAi mediated suppression of EZH2 and the gain of function mutations by over-expression of the Y641 mutant. Our results show that suppression of EZH2, but not overexpression of the EZH2 Y641 mutant, accelerates MYC-driven lymphomagenesis by attenuating apoptosis. Our model recapitulates the transcriptional signature of a subset of B-NHLs driven by MYC overactivation and EZH2 suppression. Taken together, our data imply EZH2 as a tumor suppressor in the context of MYC activation and thus raise a warning for the use of EZH2-targeted therapies in some B-NHLs subtypes. Disclosures No relevant conflicts of interest to declare.

Published

2014

21. Abstract B34: The impact of chromosome 17p loss on cancer

Author

Yu Liu, Scott W. Lowe, and Claudio Scuoppo

Subjects

Genetics, Cancer Research, Chemotherapy, medicine.medical_treatment, Cancer, Chromosome, Biology, medicine.disease, law.invention, Lymphoma, Oncology, law, RNA interference, medicine, Suppressor, Gene, Short survival

Abstract

Chromosome 17p deletions are associated with short survival and poor response to current chemotherapy treatment in non-Hodgkin's lymphomas. Although the prevailing view is that these deletions serve as a “second hit” event to inactivate p53, these deletions often hundreds of other genes. Using an in vivo RNAi screening approach for tumor suppressor genes, we identified and validated two additional tumor suppressors adjacent to p53 suggesting these deletions may do more than merely inactivate p53. To test this hypothesis, we constructed a new mouse model conditionally targeting a broad region of 17p and are intending to investigate whether and how genes co-deleted with well-known tumor suppressor p53 affect lymphoma development and chemotherapy responses. These results will elucidate the aggressive nature of tumors harboring 17p deletions and create the first mouse model that can be used to test strategies to overcome its deleterious effects. Citation Format: Yu Liu, Claudio Scuoppo, Scott Lowe. The impact of chromosome 17p loss on cancer. [abstract]. In: Proceedings of the Third AACR International Conference on Frontiers in Basic Cancer Research; Sep 18-22, 2013; National Harbor, MD. Philadelphia (PA): AACR; Cancer Res 2013;73(19 Suppl):Abstract nr B34.

Published

2013