Your search keyword '"Alberto J. Arribas"' showing total 94 results

1. A first-in-class Wiskott-Aldrich syndrome protein activator with anti-tumor activity in hematologic cancers

Author

Filippo Spriano, Giulio Sartori, Jacopo Sgrignani, Laura Barnabei, Alberto J. Arribas, Matilde Guala, Ana Maria Carrasco Del Amor, Meagan R. Tomasso, Chiara Tarantelli, Luciano Cascione, Gaetanina Golino, Maria E Riveiro, Roberta Bortolozzi, Antonio Lupia, Francesco Paduano, Samuel Huguet, Keyvan Rezai, Andrea Rinaldi, Francesco Margheriti, Pedro Ventura, Greta Guarda, Giosuè Costa, Roberta Rocca, Alberto Furlan, Luuk M. Verdonk, Paolo Innocenti, Nathaniel I. Martin, Giampietro Viola, Christoph Driessen, Emanuele Zucca, Anastasios Stathis, Digvijay Gahtory, Maurits van den Nieuwboer, Beat Bornhauser, Stefano Alcaro, Francesco Trapasso, Susana Cristobal, Shae B. Padrick, Natalina Pazzi, Franco Cavalli, Andrea Cavalli, Eugenio Gaudio, and Francesco Bertoni

Subjects

Diseases of the blood and blood-forming organs, RC633-647.5

Abstract

Hematological cancers are among the most common cancers in adults and children. Despite significant improvements in therapies, many patients still succumb to the disease. Therefore, novel therapies are needed. The Wiskott-Aldrich syndrome protein (WASp) family regulates actin assembly in conjunction with the Arp2/3 complex, a ubiquitous nucleation factor. WASp is expressed exclusively in hematopoietic cells and exists in two allosteric conformations: autoinhibited or activated. Here, we describe the development of EG-011, a first-in-class small molecule activator of the WASp auto-inhibited form. EG-011 possesses in vitro and in vivo anti-tumor activity as a single agent in lymphoma, leukemia, and multiple myeloma, including models of secondary resistance to PI3K, BTK, and proteasome inhibitors. The in vitro activity was confirmed in a lymphoma xenograft. Actin polymerization and WASp binding was demonstrated using multiple techniques. Transcriptome analysis highlighted homology with drugs-inducing actin polymerization.

Published

2024

2. Targeting CD19-positive lymphomas with the antibody-drug conjugate loncastuximab tesirine: preclinical evidence as single agent and in combination therapy

Author

Chiara Tarantelli, David Wald, Nicolas Munz, Filippo Spriano, Alessio Bruscaggin, Eleonora Cannas, Luciano Cascione, Eugenio Gaudio, Alberto J. Arribas, Shivaprasad Manjappa, Gaetanina Golino, Lorenzo Scalise, Maria Teresa Cacciapuoti, Emanuele Zucca, Anastasios Stathis, Giorgio Inghirami, Patrick H. van Berkel, Davide Rossi, Paolo F. Caimi, Francesca Zammarchi, and Francesco Bertoni

Subjects

Diseases of the blood and blood-forming organs, RC633-647.5

Abstract

Antibody-drug conjugates (ADCs) represent one of the most successful therapeutic approaches introduced in clinical practice in the last few years. Loncastuximab tesirine (ADCT-402) is a CD19 targeting ADC, in which the antibody is conjugated through a protease cleavable dipeptide linker to a pyrrolobenzodiazepine (PBD) dimer warhead (SG3199). Based on the results of a phase 2 study, loncastuximab tesirine was recently approved for adult patients with relapsed/refractory large B-cell lymphoma. We assessed the activity of loncastuximab tesirine using in vitro and in vivo models of lymphomas, correlated its activity with CD19 expression levels, and identified combination partners providing synergy with loncastuximab tesirine. Loncastuximab tesirine was tested across 60 lymphoma cell lines. Loncastuximab tesirine had strong cytotoxic activity in B-cell lymphoma cell lines. The in vitro activity was correlated with CD19 expression level and intrinsic sensitivity of cell lines to the ADC’s warhead. Loncastuximab tesirine was more potent than other anti-CD19 ADCs (coltuximab ravtansine, huB4-DGN462), albeit the pattern of activity across cell lines was correlated. Loncastuximab tesirine activity was also largely correlated with cell line sensitivity to R-CHOP. Combinatorial in vitro and in vivo experiments identified the benefit of adding loncastuximab tesirine to other agents, especially BCL2 and PI3K inhibitors. Our data support the further development of loncastuximab tesirine as a single agent and in combination for patients affected by mature B-cell neoplasms. The results also highlight the importance of CD19 expression and the existence of lymphoma populations characterized by resistance to multiple therapies.

Published

2024

3. Pharmacologic screen identifies active combinations with BET inhibitors and LRRK2 as a novel putative target in lymphoma

Author

Filippo Spriano, Giulio Sartori, Chiara Tarantelli, Marilia Barreca, Gaetanina Golino, Andrea Rinaldi, Sara Napoli, Michele Mascia, Lorenzo Scalise, Alberto J. Arribas, Luciano Cascione, Emanuele Zucca, Anastasios Stathis, Eugenio Gaudio, and Francesco Bertoni

Subjects

BET, HDAC, JAK, LRRK2, LYMPHOMAS, Diseases of the blood and blood-forming organs, RC633-647.5

Abstract

Abstract Inhibitors of the Bromo‐ and Extra‐Terminal domain (BET) family proteins have strong preclinical antitumor activity in multiple tumor models, including lymphomas. Limited single‐agent activity has been reported in the clinical setting. Here, we have performed a pharmacological screening to identify compounds that can increase the antitumor activity of BET inhibitors in lymphomas. The germinal center B‐cell like diffuse large B‐cell lymphoma (DLBCL) cell lines OCI‐LY‐19 and WSU‐DLCL2 were exposed to 348 compounds given as single agents at two different concentrations and in combination with the BET inhibitor birabresib. The combination partners included small molecules targeting important biologic pathways such as PI3K/AKT/MAPK signaling and apoptosis, approved anticancer agents, kinase inhibitors, epigenetic compounds. The screening identified a series of compounds leading to a stronger antiproliferative activity when given in combination than as single agents: the histone deacetylase (HDAC) inhibitors panobinostat and dacinostat, the mTOR (mechanistic target of rapamycin) inhibitor everolimus, the ABL/SRC (ABL proto‐oncogene/SRC proto oncogene) inhibitor dasatinib, the AKT1/2/3 inhibitor MK‐2206, the JAK2 inhibitor TG101209. The novel finding was the benefit given by the addition of the LRRK2 inhibitor LRRK2‐IN‐1, which was validated in vitro and in vivo. Genetic silencing demonstrated that LRRK2 sustains the proliferation of lymphoma cells, a finding paired with the association between high expression levels and inferior outcome in DLBCL patients. We identified combinations that can improve the response to BET inhibitors in lymphomas, and LRRK2 as a gene essential for lymphomas and as putative novel target for this type of tumors.

Published

2022

4. Resistance to PI3Kδ inhibitors in marginal zone lymphoma can be reverted by targeting the IL-6/PDGFRA axis

Author

Alberto J. Arribas, Sara Napoli, Luciano Cascione, Giulio Sartori, Laura Barnabei, Eugenio Gaudio, Chiara Tarantelli, Afua Adjeiwaa Mensah, Filippo Spriano, Antonella Zucchetto, Francesca M Rossi, Andrea Rinaldi, Manuel Castro de Moura, Sandra Jovic, Roberta Bordone-Pittau, Alessandra Di Veroli, Anastasios Stathis, Gabriele Cruciani, Georg Stussi, Valter Gattei, Jennifer R. Brown, Manel Esteller, Emanuele Zucca, Davide Rossi, and Francesco Bertoni

Subjects

Diseases of the blood and blood-forming organs, RC633-647.5

Abstract

PI3Kδ inhibitors are active in patients with lymphoid neoplasms and a first series of them have been approved for the treatment of multiple types of B-cell lymphoid tumors, including marginal zone lymphoma (MZL). The identification of the mechanisms underlying either primary or secondary resistance is fundamental to optimize the use of novel drugs. Here we present a model of secondary resistance to PI3Kδ inhibitors obtained by prolonged exposure of a splenic MZL cell line to idelalisib. The VL51 cell line was kept under continuous exposure to idelalisib. The study included detailed characterization of the model, pharmacological screens, silencing experiments, and validation experiments on multiple cell lines and on clinical specimens. VL51 developed resistance to idelalisib, copanlisib, duvelisib, and umbralisib. An integrative analysis of transcriptome and methylation data highlighted an enrichment of upregulated transcripts and low-methylated promoters in resistant cells, including IL-6/STAT3- and PDGFRA-related genes and surface CD19 expression, alongside the repression of the let-7 family of miRNA, and miR-125, miR-130, miR-193 and miR-20. The IL-6R blocking antibody tocilizumab, the STAT3 inhibitor stattic, the LIN28 inhibitor LIN1632, the PDGFR inhibitor masitinib and the anti-CD19 antibody drug conjugate loncastuximab tesirine were active compounds in the resistant cells as single agents and/or in combination with PI3Kδ inhibition. Findings were validated on additional in vitro lymphoma models and on clinical specimens. A novel model of resistance obtained from splenic MZL allowed the identification of therapeutic approaches able to improve the antitumor activity of PI3Kδ inhibitors in B-cell lymphoid tumors.

Published

2022

5. Targeting CD205 with the antibody drug conjugate MEN1309/OBT076 is an active new therapeutic strategy in lymphoma models

Author

Eugenio Gaudio, Chiara Tarantelli, Filippo Spriano, Francesca Guidetti, Giulio Sartori, Roberta Bordone, Alberto J. Arribas, Luciano Cascione, Mario Bigioni, Giuseppe Merlino, Alessio Fiascarelli, Alessandro Bressan, Afua Adjeiwaa Mensah, Gaetanina Golino, Renzo Lucchini, Elena Bernasconi, Davide Rossi, Emanuele Zucca, Georg Stussi, Anastasios Stathis, Robert S. Boyd, Rachel L. Dusek, Arnima Bisht, Nickolas Attanasio, Christian Rohlff, Andrea Pellacani, Monica Binaschi, and Francesco Bertoni

Subjects

Diseases of the blood and blood-forming organs, RC633-647.5

Abstract

Antibody drug conjugates represent an important class of anti-cancer drugs in both solid tumors and hematological cancers. Here, we report preclinical data on the anti-tumor activity of the first-in-class antibody drug conjugate MEN1309/OBT076 targeting CD205. The study included preclinical in vitro activity screening on a large panel of cell lines, both as single agent and in combination and validation experiments on in vivo models. CD205 was first shown frequently expressed in lymphomas, leukemias and multiple myeloma by immunohistochemistry on tissue microarrays. Anti-tumor activity of MEN1309/OBT076 as single agent was then shown across 42 B-cell lymphoma cell lines with a median IC50 of 200 pM and induction of apoptosis in 25/42 (59.5%) of the cases. The activity appeared highly correlated with its target expression. After in vivo validation as the single agent, the antibody drug conjugate synergized with the BCL2 inhibitor venetoclax, and the anti-CD20 monoclonal antibody rituximab. The first-in-class antibody drug targeting CD205, MEN1309/OBT076, demonstrated strong pre-clinical anti-tumor activity in lymphoma, warranting further investigations as a single agent and in combination.

Published

2020

6. Novel insights into the genetics and epigenetics of MALT lymphoma unveiled by next generation sequencing analyses

Author

Luciano Cascione, Andrea Rinaldi, Alessio Bruscaggin, Chiara Tarantelli, Alberto J. Arribas, Ivo Kwee, Lorenza Pecciarini, Afua A. Mensah, Valeria Spina, Elaine Y.L. Chung, Lodovico Terzi di Bergamo, Stephan Dirnhofer, Alexandar Tzankov, Roberto N. Miranda, Ken H. Young, Alexandra Traverse-Glehen, Gianluca Gaidano, Steven H. Swerdlow, Randy Gascoyne, Raul Rabadan, Maurilio Ponzoni, Govind Bhagat, Davide Rossi, Emanuele Zucca, and Francesco Bertoni

Subjects

Diseases of the blood and blood-forming organs, RC633-647.5

Published

2019

7. The novel CD19-targeting antibody-drug conjugate huB4-DGN462 shows improved anti-tumor activity compared to SAR3419 in CD19-positive lymphoma and leukemia models

Author

Stuart W. Hicks, Chiara Tarantelli, Alan Wilhem, Eugenio Gaudio, Min Li, Alberto J. Arribas, Filippo Spriano, Roberta Bordone, Luciano Cascione, Katharine C. Lai, Qifeng Qiu, Monica Taborelli, Davide Rossi, Georg Stussi, Emanuele Zucca, Anastasios Stathis, Callum M. Sloss, and Francesco Bertoni

Subjects

Diseases of the blood and blood-forming organs, RC633-647.5

Abstract

Antibody-drug conjugates (ADC) are a novel way to deliver potent cytotoxic compounds to cells expressing a specific antigen. Four ADC targeting CD19, including SAR3419 (coltuximab ravtansine), have entered clinical development. Here, we present huB4-DGN462, a novel ADC based on the SAR3419 anti-CD19 antibody linked via sulfo-SPDB to the potent DNA-alkylating agent DGN462. huB4-DGN462 had improved in vitro anti-proliferative and cytotoxic activity compared to SAR3419 across multiple B-cell lymphoma and human acute lymphoblastic leukemia cell lines. In vivo experiments using lymphoma xenografts models confirmed the in vitro data. The response of B-cell lymphoma lines to huB4-DGN462 was not correlated with CD19 expression, the presence of BCL2 or MYC translocations, TP53 inactivation or lymphoma histology. In conclusion, huB4-DGN462 is an attractive candidate for clinical investigation in patients with B-cell malignancies.

Published

2019

8. The Bruton tyrosine kinase inhibitor zanubrutinib (BGB-3111) demonstrated synergies with other anti-lymphoma targeted agents

Author

Chiara Tarantelli, Lu Zhang, Elisabetta Curti, Eugenio Gaudio, Filippo Spriano, Valdemar Priebe, Luciano Cascione, Alberto J. Arribas, Emanuele Zucca, Davide Rossi, Anastasios Stathis, and Francesco Bertoni

Subjects

Diseases of the blood and blood-forming organs, RC633-647.5

Published

2019

9. A Reliable Method to Remove Batch Effects Maintaining Group Differences in Lymphoma Methylation Case Study.

Author

Giulia Pontali, Luciano Cascione, Alberto J. Arribas, Andrea Rinaldi, Francesco Bertoni, and Rosalba Giugno

Published

2019

10. Supplementary Data from Subcapsular Sinus Macrophages Promote Melanoma Metastasis to the Sentinel Lymph Nodes via an IL1α–STAT3 Axis

Author

Santiago F. Gonzalez, Francesco Bertoni, Ron N. Apte, Silvia Monticelli, Elena Voronov, Lorenzo Mortara, Antonino Bruno, Robert E. Hunger, Fausto Sessa, Anna Maria Chiaravalli, Ivo Kwee, Aner Ottolenghi, Marina Bersudsky, S. Morteza Seyed Jafari, Diego Morone, Alberto J. Arribas, Andrea Rinaldi, Murodzhon Akhmedov, Cristina Leoni, Daniel Molina Romero, Irene Latino, Giulio Sartori, Luciano Cascione, Joy Bordini, and Tommaso Virgilio

Abstract

Supplementary Data from Subcapsular Sinus Macrophages Promote Melanoma Metastasis to the Sentinel Lymph Nodes via an IL1α–STAT3 Axis

Published

2023

11. Data from Subcapsular Sinus Macrophages Promote Melanoma Metastasis to the Sentinel Lymph Nodes via an IL1α–STAT3 Axis

Author

Santiago F. Gonzalez, Francesco Bertoni, Ron N. Apte, Silvia Monticelli, Elena Voronov, Lorenzo Mortara, Antonino Bruno, Robert E. Hunger, Fausto Sessa, Anna Maria Chiaravalli, Ivo Kwee, Aner Ottolenghi, Marina Bersudsky, S. Morteza Seyed Jafari, Diego Morone, Alberto J. Arribas, Andrea Rinaldi, Murodzhon Akhmedov, Cristina Leoni, Daniel Molina Romero, Irene Latino, Giulio Sartori, Luciano Cascione, Joy Bordini, and Tommaso Virgilio

Abstract

During melanoma metastasis, tumor cells originating in the skin migrate via lymphatic vessels to the sentinel lymph node (sLN). This process facilitates tumor cell spread across the body. Here, we characterized the innate inflammatory response to melanoma in the metastatic microenvironment of the sLN. We found that macrophages located in the subcapsular sinus (SS) produced protumoral IL1α after recognition of tumoral antigens. Moreover, we confirmed that the elimination of LN macrophages or the administration of an IL1α-specific blocking antibody reduced metastatic spread. To understand the mechanism of action of IL1α in the context of the sLN microenvironment, we applied single-cell RNA sequencing to microdissected metastases obtained from animals treated with the IL1α-specific blocking antibody. Among the different pathways affected, we identified STAT3 as one of the main targets of IL1α signaling in metastatic tumor cells. Moreover, we found that the antitumoral effect of the anti-IL1α was not mediated by lymphocytes because Il1r1 knockout mice did not show significant differences in metastasis growth. Finally, we found a synergistic antimetastatic effect of the combination of IL1α blockade and STAT3 inhibition with stattic, highlighting a new immunotherapy approach to preventing melanoma metastasis.

Published

2023

12. Supplementary Figure from Subcapsular Sinus Macrophages Promote Melanoma Metastasis to the Sentinel Lymph Nodes via an IL1α–STAT3 Axis

Author

Santiago F. Gonzalez, Francesco Bertoni, Ron N. Apte, Silvia Monticelli, Elena Voronov, Lorenzo Mortara, Antonino Bruno, Robert E. Hunger, Fausto Sessa, Anna Maria Chiaravalli, Ivo Kwee, Aner Ottolenghi, Marina Bersudsky, S. Morteza Seyed Jafari, Diego Morone, Alberto J. Arribas, Andrea Rinaldi, Murodzhon Akhmedov, Cristina Leoni, Daniel Molina Romero, Irene Latino, Giulio Sartori, Luciano Cascione, Joy Bordini, and Tommaso Virgilio

Abstract

Supplementary Figure from Subcapsular Sinus Macrophages Promote Melanoma Metastasis to the Sentinel Lymph Nodes via an IL1α–STAT3 Axis

Published

2023

13. Supplementary Figure from Functional Testing to Characterize and Stratify PI3K Inhibitor Responses in Chronic Lymphocytic Leukemia

Author

Sigrid S. Skånland, Tero Aittokallio, Geir E. Tjønnfjord, Jennifer R. Brown, Emmanuel Normant, Anthony R. Mato, Francesco Bertoni, Kjetil Taskén, Abdul K. Hilli, Alberto J. Arribas, Stacey M. Fernandes, Ishwarya Murali, Haifeng Xu, Aleksandra Urban, Linda Karlsen, Paschalis Athanasiadis, and Yanping Yin

Abstract

Supplementary Figure from Functional Testing to Characterize and Stratify PI3K Inhibitor Responses in Chronic Lymphocytic Leukemia

Published

2023

14. Supplementary Table from Functional Testing to Characterize and Stratify PI3K Inhibitor Responses in Chronic Lymphocytic Leukemia

Author

Sigrid S. Skånland, Tero Aittokallio, Geir E. Tjønnfjord, Jennifer R. Brown, Emmanuel Normant, Anthony R. Mato, Francesco Bertoni, Kjetil Taskén, Abdul K. Hilli, Alberto J. Arribas, Stacey M. Fernandes, Ishwarya Murali, Haifeng Xu, Aleksandra Urban, Linda Karlsen, Paschalis Athanasiadis, and Yanping Yin

Abstract

Supplementary Table from Functional Testing to Characterize and Stratify PI3K Inhibitor Responses in Chronic Lymphocytic Leukemia

Published

2023

15. Data from Functional Testing to Characterize and Stratify PI3K Inhibitor Responses in Chronic Lymphocytic Leukemia

Author

Sigrid S. Skånland, Tero Aittokallio, Geir E. Tjønnfjord, Jennifer R. Brown, Emmanuel Normant, Anthony R. Mato, Francesco Bertoni, Kjetil Taskén, Abdul K. Hilli, Alberto J. Arribas, Stacey M. Fernandes, Ishwarya Murali, Haifeng Xu, Aleksandra Urban, Linda Karlsen, Paschalis Athanasiadis, and Yanping Yin

Abstract

Purpose:PI3K inhibitors (PI3Ki) are approved for relapsed chronic lymphocytic leukemia (CLL). Although patients may show an initial response to these therapies, development of treatment intolerance or resistance remain clinical challenges. To overcome these, prediction of individual treatment responses based on actionable biomarkers is needed. Here, we characterized the activity and cellular effects of 10 PI3Ki and investigated whether functional analyses can identify treatment vulnerabilities in PI3Ki-refractory/intolerant CLL and stratify responders to PI3Ki.Experimental Design:Peripheral blood mononuclear cell samples (n = 51 in total) from treatment-naïve and PI3Ki-treated patients with CLL were studied. Cells were profiled against 10 PI3Ki and the Bcl-2 antagonist venetoclax. Cell signaling and immune phenotypes were analyzed by flow cytometry. Cell viability was monitored by detection of cleaved caspase-3 and the CellTiter-Glo assay.Results:pan-PI3Kis were most effective at inhibiting PI3K signaling and cell viability, and showed activity in CLL cells from both treatment-naïve and idelalisib-refractory/intolerant patients. CLL cells from idelalisib-refractory/intolerant patients showed overall reduced protein phosphorylation levels. The pan-PI3Ki copanlisib, but not the p110δ inhibitor idelalisib, inhibited PI3K signaling in CD4+ and CD8+ T cells in addition to CD19+ B cells, but did not significantly affect T-cell numbers. Combination treatment with a PI3Ki and venetoclax resulted in synergistic induction of apoptosis. Analysis of drug sensitivities to 73 drug combinations and profiling of 31 proteins stratified responders to idelalisib and umbralisib, respectively.Conclusions:Our findings suggest novel treatment vulnerabilities in idelalisib-refractory/intolerant CLL, and indicate that ex vivo functional profiling may stratify PI3Ki responders.

Published

2023

16. Table S2 from PQR309 Is a Novel Dual PI3K/mTOR Inhibitor with Preclinical Antitumor Activity in Lymphomas as a Single Agent and in Combination Therapy

Author

Francesco Bertoni, Doriano Fabbro, Vladimir Cmiljanovic, Emanuele Zucca, Andreas Wicki, Matthias P. Wymann, Massimo Broggini, Georg Stussi, Anastasios Stathis, Davide Rossi, Valter Gattei, Monica Taborelli, Antonella Zucchetto, Francesca Maria Rossi, Barbara Dossena, Alexander Sele, Denise Rageot, Reto Ritschard, Florent Beaufils, Roberta Bordone Pittau, Laura Carrassa, Francesca Guidetti, Elena Bernasconi, Filippo Spriano, Luciano Cascione, Andrea Rinaldi, Petra Hillmann, Ivo Kwee, Alberto J. Arribas, Eugenio Gaudio, and Chiara Tarantelli

Abstract

PQR309 activity, combinations of PQR309 with additional drugs, BCL2, MYC and TP53 status in lymphoma cell lines.

Published

2023

17. Data from PQR309 Is a Novel Dual PI3K/mTOR Inhibitor with Preclinical Antitumor Activity in Lymphomas as a Single Agent and in Combination Therapy

Author

Francesco Bertoni, Doriano Fabbro, Vladimir Cmiljanovic, Emanuele Zucca, Andreas Wicki, Matthias P. Wymann, Massimo Broggini, Georg Stussi, Anastasios Stathis, Davide Rossi, Valter Gattei, Monica Taborelli, Antonella Zucchetto, Francesca Maria Rossi, Barbara Dossena, Alexander Sele, Denise Rageot, Reto Ritschard, Florent Beaufils, Roberta Bordone Pittau, Laura Carrassa, Francesca Guidetti, Elena Bernasconi, Filippo Spriano, Luciano Cascione, Andrea Rinaldi, Petra Hillmann, Ivo Kwee, Alberto J. Arribas, Eugenio Gaudio, and Chiara Tarantelli

Abstract

Purpose: Activation of the PI3K/mTOR signaling pathway is recurrent in different lymphoma types, and pharmacologic inhibition of the PI3K/mTOR pathway has shown activity in lymphoma patients. Here, we extensively characterized the in vitro and in vivo activity and the mechanism of action of PQR309 (bimiralisib), a novel oral selective dual PI3K/mTOR inhibitor under clinical evaluation, in preclinical lymphoma models.Experimental Design: This study included preclinical in vitro activity screening on a large panel of cell lines, both as single agent and in combination, validation experiments on in vivo models and primary cells, proteomics and gene-expression profiling, and comparison with other signaling inhibitors.Results: PQR309 had in vitro antilymphoma activity as single agent and in combination with venetoclax, panobinostat, ibrutinib, lenalidomide, ARV-825, marizomib, and rituximab. Sensitivity to PQR309 was associated with specific baseline gene-expression features, such as high expression of transcripts coding for the BCR pathway. Combining proteomics and RNA profiling, we identified the different contribution of PQR309-induced protein phosphorylation and gene expression changes to the drug mechanism of action. Gene-expression signatures induced by PQR309 and by other signaling inhibitors largely overlapped. PQR309 showed activity in cells with primary or secondary resistance to idelalisib.Conclusions: On the basis of these results, PQR309 appeared as a novel and promising compound that is worth developing in the lymphoma setting. Clin Cancer Res; 24(1); 120–9. ©2017 AACR.

Published

2023

18. Supplementary figures, table legends, Table S1, S9 from PQR309 Is a Novel Dual PI3K/mTOR Inhibitor with Preclinical Antitumor Activity in Lymphomas as a Single Agent and in Combination Therapy

Author

Francesco Bertoni, Doriano Fabbro, Vladimir Cmiljanovic, Emanuele Zucca, Andreas Wicki, Matthias P. Wymann, Massimo Broggini, Georg Stussi, Anastasios Stathis, Davide Rossi, Valter Gattei, Monica Taborelli, Antonella Zucchetto, Francesca Maria Rossi, Barbara Dossena, Alexander Sele, Denise Rageot, Reto Ritschard, Florent Beaufils, Roberta Bordone Pittau, Laura Carrassa, Francesca Guidetti, Elena Bernasconi, Filippo Spriano, Luciano Cascione, Andrea Rinaldi, Petra Hillmann, Ivo Kwee, Alberto J. Arribas, Eugenio Gaudio, and Chiara Tarantelli

Abstract

Supplementary figures, table legends, Table S1, S9 Figure S1. In vitro antitumor activity of the dual PI3K/mTOR inhibitor apitolisib and its correlation with PQR309. Figure S2. Antitumor In vivo activity of PQR309 in the treatment of RI-1 and SU-DHL-6 xenograft model. Figure S3. Apoptosis is induced by co-treatment of PQR309 with venetoclax or panobinostat in primary cells and in the DLBCL SU-DHL-6 cell line. Figure S4. Specific baseline gene expression signatures are associated with higher or lower sensitivity to PQR309. Figure S5. In vitro antitumor activity of the PI3K� inhibitor idelalisib and its correlation with PQR309. Figure S6. PQR309 induced decrease in phosphorylation of AKT-Ser473 and p70S6K-Thr389 in DLBCL cell lines. Figure S7. PQR309 reduces AKT-Ser473 phosphorylation in lymphoma cell lines. Figure S8. Transcriptional expression signature of ABC DLBCL cell lines induced by PQR309. Figure S9. ABC and GCB DLBCL PQR309-treated signatures were highly overlapping. Figure S10. Transcript expression levels of PQR309-treated samples. Figure S11. Changes in protein phosphorylation and RNA expression differently contribute to PQR309 affected biologic pathways in ABC DLBCL. Figure S12. PQR309 can largely regulate the same genes affected by the BTK inhibitor ibrutinib, the PI3K� idelalisib, the dual PI3K�/� inhibitor duvelisib (A), the dual PI3K�/� inhibitor AZD8835 or the AKT inhibitor AZD5363 (B). Figure S13. BCR pathway signature is similarly affected after ibrutinib, idelalisib and duvelisib treatments in ABC DLBCL cell lines. Figure S14. The dual PI3K/mTOR inhibitor PQR309 and the PIM inhibitor AZD1208 synergize in DLBCL cell lines. Supplementary Table 1. List of phosphoresidues investigated by Carna Bioscience to perform RPPA analysis. Supplementary Table 9. Transcripts differentially expressed in ABC DLBCL cell lines treated with ibrutinib (A), idelalisib (B) or duvelisib (C) versus DMSO.

Published

2023

19. The ATR inhibitor elimusertib exhibits anti-lymphoma activity and synergizes with the PI3K inhibitor copanlisib

Author

Giulio Sartori, Chiara Tarantelli, Filippo Spriano, Eugenio Gaudio, Luciano Cascione, Michele Mascia, Marilia Barreca, Alberto J. Arribas, Luca Licenziato, Gaetanina Golino, Adele Ferragamo, Stefano Pileri, Giovanna Damia, Emanuele Zucca, Anastasios Stathis, Oliver Politz, Antje M. Wengner, and Francesco Bertoni

Abstract

PurposeThe DNA damage response (DDR) is the cellular process devoted to the preservation of an intact genome. The DDR is often deregulated in lymphoma cells due to high levels of DNA damage, tumor suppressor inactivation, increased replication stress observed after oncogene activation, or high amounts of reactive oxygen species. The ataxia telangiectasia and Rad3-related (ATR) kinase is a crucial factor of DDR in the response to DNA single strand breaks. ATR inhibitors are a class of agents that have shown considerable clinical potential in this context.Experimental DesignWe characterized the activity of the ATR inhibitor elimusertib (BAY 1895344) in a panel of lymphoma cell lines. Furthermore, we evaluated the activity of elimusertib in combination with the clinically approved PI3K inhibitor copanlisib inin vitroandin vivolymphoma models.ResultsElimusertib exhibitedin vitroactivity across a variety of lymphoma subtypes which was associated with expression of genes related to replication stress. Elimusertib also demonstrated wide-spread anti-tumor activity that was stronger compared to ceralasertib, another ATR inhibitor, in several tumor models. This activity was present in both DDR-proficient and DDR-deficient lymphoma models. Furthermore, elimusertib had synergistic antitumor activity in combination with copanlisib.ConclusionsPotent antitumor activity of elimusertib was demonstrated in several lymphoma models which is associated with high expression of gene transcripts coding for proteins that are involved in DDR and cell cycle regulation. Combination of ATR and PI3K inhibition by treatment with elimusertib and copanlisib had synergistic efficacy providing a potential new treatment option for lymphoma patients.Translational relevanceThe DNA damage response (DDR) is often deregulated in lymphoma cells. Here, we characterized the activity of elimusertib, an inhibitor of the ataxia telangiectasia and Rad3-related kinase (ATR) that is involved in the DDR. Elimusertib was demonstrated to exhibit anti-lymphoma activity across several lymphoma cell lines and tumor models. Copanlisib is an inhibitor of PI3K kinase family which has also shown activity in various lymphomas. Combined treatment with elimusertib and copanlisib resulted in a synergistic antitumor effect in lymphoma models. The combination of elimusertib and copanlisib could potentially constitute a new chemotherapy-free treatment option for lymphomas.

Published

2023

20. Targeting IRAK4 with Emavusertib in Lymphoma Models with Secondary Resistance to PI3K and BTK Inhibitors

Author

Francesca Guidetti, Alberto J. Arribas, Giulio Sartori, Filippo Spriano, Laura Barnabei, Chiara Tarantelli, Reinhard Von Roemeling, Elizabeth Martinez, Emanuele Zucca, and Francesco Bertoni

Subjects

General Medicine, IRAK4, PI3K, BTK, marginal zone lymphoma, MYD88

Abstract

Inhibitors of phosphatidylinositol 3-kinase (PI3K) and Bruton tyrosine kinase (BTK) represent a recognized option for the treatment of patients affected by indolent B cell lymphomas. However, small molecules as single agents show limited success in their ability in inducing complete responses, with only partial remission achieved in most patients, suggesting the need for combination therapies. IRAK4 is a protein kinase downstream of the Toll-like receptor signaling (TLR), a driver pathway of secondary tumor° resistance in both hematological and solid tumor malignancies. Activation of IRAK4 upon TLRs and IL-1 receptor (IL-1R) stimulation and through the adaptor protein MYD88 initiates a signaling cascade that induces cytokine and survival factor expression mediated by the transcription factor NF-κB. MYD88-L265P encoding mutations occur in diffuse large B-cell lymphomas, in lymphoplasmacytic lymphomas and in few marginal zone lymphomas (MZL). The IRAK4 inhibitor emavusertib (CA-4948) has shown early safety and clinical activity in lymphoma and leukemia patients. In this preclinical study, we assessed emavusertib effectiveness in MZL, both as single agent and in combination with targeted agents, with a particular focus on its capability to overcome resistance to BTK and PI3K inhibitors. We showed that the presence of MYD88 L265P mutation in bona fide MZL cell lines confers sensitivity to the IRAK4 inhibitor emavusertib as single agent. Emavusertib-based combinations improved the sensitivity of MZL cells to BTK and PI3K inhibitors, including cells with a secondary resistance to these agents. Emavusertib exerted its activity via inhibition of NF-κB signaling and induction of apoptosis. Considering the early safety data from clinical trials, our study identifies the IRAK4 inhibitor emavusertib as a novel compound to be explored in trials for patients with MYD88-mutated indolent B cell lymphomas as single agent and as combination partner with BTK or PI3K inhibitors in unselected populations of patients.

Published

2023

21. Assessment of lisavanbulin (BAL101553) as an anti-lymphoma agent

Author

Filippo Spriano, Luca Aresu, Luciano Cascione, Giorgia Risi, Alberto J. Arribas, Sara Napoli, Andrea Rinaldi, Nicole Forster-Gross, Felix Bachmann, Marc Engelhardt, Heidi Lane, and Francesco Bertoni

Abstract

Microtubules are major components of the cellular cytoskeleton, ubiquitously founded in all eukaryotic cells. They are involved in mitosis, cell motility, intracellular protein and organelle transport, and maintenance of cytoskeletal shape. Avanbulin (BAL27862) is a microtubule-targeted agent (MTA) that promotes tumor cell death by destabilization of microtubules. Due to its unique binding to the colchicine site of tubulin, differently from other MTAs, avanbulin has previously shown activity in solid tumor cell lines. Its prodrug, lisavanbulin (BAL101553), has shown early signs of clinical activity, especially in tumors with high EB1 expression. Here, we assessed the preclinical anti-tumor activity of avanbulin in diffuse large B cell lymphoma (DLBCL) and the pattern of expression of EB1 in DLBCL cell lines and clinical specimens.Avanbulin showed a potentin vitroanti-lymphoma activity, which was mainly cytotoxic with potent and rapid apoptosis induction. Median IC50 was around 10nM in both activated B cell like (ABC) and germinal center B cell like (GCB) DLBCL. Half of the cell lines tested showed an induction of apoptosis already in the first 24h of treatment, the other half in the first 48h. EB1 showed expression in DLBCL clinical specimens, opening the possibility for a cohort of patients that could potentially benefit from treatment with lisavanbulin.These data show the basis for further preclinical and clinical evaluation of lisavanbulin in the lymphoma field.

Published

2023

22. ERBB4-mediated signaling is a mediator of resistance to BTK and PI3K inhibitors in B cell lymphoid neoplasms

Author

Alberto J. Arribas, Sara Napoli, Luciano Cascione, Laura Barnabei, Giulio Sartori, Eleonora Cannas, Eugenio Gaudio, Chiara Tarantelli, Afua A. Mensah, Filippo Spriano, Antonella Zucchetto, Francesca M. Rossi, Andrea Rinaldi, Manuel Castro de Moura, Sandra Jovic, Roberta Bordone Pittau, Anastasios Stathis, Georg Stussi, Valter Gattei, Jennifer R. Brown, Manel Esteller, Emanuele Zucca, Davide Rossi, and Francesco Bertoni

Subjects

Article

Abstract

BTK and PI3K inhibitors are among the drugs approved for the treatment of patients with lymphoid neoplasms. Although active, their ability to lead as single agents to long-lasting complete remission is rather limited especially in the lymphoma setting. This indicates that tumor cells often develop resistance to the drugs. Here, we show that the overexpression of ERBB4 and its ligands represents a modality for B cell neoplastic cells to bypass the anti-tumor activity of BTK and PI3K inhibitors and that targeted pharmacological interventions can restore sensitivity to the small molecules.We started from a marginal zone lymphoma (MZL) cell line, Karpas-1718, kept under prolonged exposure to the PI3Kδ inhibitor idelalisib until acquisition of resistance, or with no drug. Cells underwent transcriptome, miRNA and methylation profiling, whole exome sequencing, and pharmacological screening which led to the identification of the overexpression of ERBB4 and its ligands HBEGF and NRG2 in the resistant cells. Cellular and genetic experiments demonstrated the involvement of this axis in blocking the anti-tumor activity of various BTK and PI3K inhibitors, currently used in the clinical setting. Addition of recombinant HBEGF induced resistance to BTK and PI3K inhibitors in parental cells but also in additional lymphoma models. Combination with the ERBB inhibitor lapatinib was beneficial in resistant cells and in other lymphoma models already expressing the identified resistance factors. Multi-omics analysis underlined that an epigenetic reprogramming affected the expression of the resistance-related factors, and pretreatment with demethylating agents or EZH2 inhibitors overcame the resistance. Resistance factors were shown to be expressed in clinical samples, further extending the findings of the study.In conclusions, we identified a novel ERBB4-driven mechanism of resistance to BTK and PI3K inhibitors and treatments that appear to overcome it.Key pointsA mechanism of secondary resistance to the PI3Kδ and BTK inhibitors in B cell neoplasms driven by secreted factors.Resistance can be reverted by targeting ERBB signaling.

Published

2023

23. A first-in-class Wiskott-Aldrich syndrome protein (WASp) activator with anti-tumor activity in hematological cancers

Author

Filippo Spriano, Giulio Sartori, Laura Barnabei, Alberto J. Arribas, Matilde Guala, Ana Maria Carrasco Del Amor, Meagan R. Tomasso, Chiara Tarantelli, Luciano Cascione, Gaetanina Golino, Maria E Riveiro, Roberta Bortolozzi, Antonio Lupia, Francesco Paduano, Samuel Huguet, Keyvan Rezai, Francesco Margheriti, Pedro Ventura, Greta Guarda, Giosuè Costa, Roberta Rocca, Andrea Cavalli, Giampietro Viola, Christoph Driessen, Emanuele Zucca, Anastasios Stathis, Beat Bornhauser, Stefano Alcaro, Francesco Trapasso, Susana Cristobal, Shae B. Padrick, Natalina Pazzi, Franco Cavalli, Francesco Bertoni, and Eugenio Gaudio

Abstract

Hematological cancers are among the most common cancers in adults and in children. Despite significant improvements in therapies, many patients still succumb to the disease, therefore, novel therapies are needed. The Wiskott-Aldrich syndrome protein (WASp) family proteins regulate actin assembly in conjunction with the Arp2/3 complex, a ubiquitous nucleation factor. WASp is expressed exclusively in hematopoietic cells and exists in two allosteric conformations, auto-inhibited and active conformations. Here, we describe the development of EG-011, a first-in-class small molecule activator of the WASp auto-inhibited form. EG-011 possesses in vitro and in vivo anti-tumor activity as single agent in lymphoma, leukemia and multiple myeloma, including models of secondary resistance to PI3K, BTK and proteasome inhibitors. The in vitro activity was confirmed in a lymphoma xenograft. Actin polymerization induced by EG-011 was demonstrated with multiple techniques. Transcriptome analysis highlighted homology with drugs inducing actin polymerization.Key pointsEG-011 is a novel small molecule with anti-tumor activity in hematological cancers, including resistant lymphoma and multiple myeloma modelsEG-011 is a first-in-class small molecule activator of the auto-inhibited form of the Wiskott-Aldrich syndrome protein (WASp)

Published

2022

24. PI3K and BTK Inhibition Induces the Upregulation of CD19 and Increases Sensitivity to CAR T Cells in a Model of Marginal Zone Lymphoma (MZL)

Author

Sisi Wang, Alberto J Arribas, Chiara Tarantelli, Amandine Pradier, Lodovico Terzi Di Bergamo, Emanuele Zucca, Davide Rossi, Federico Simonetta, and Francesco Bertoni

Subjects

Immunology, Cell Biology, Hematology, Biochemistry

Published

2022

25. Abstract 492: Pharmacological inhibition of CXCR4 increases the anti-tumor activity of conventional and targeted therapies in B cell lymphoma models

Author

Laura Barnabei, Alberto J. Arribas, Luciano Cascione, Francesca Guidetti, Filippo Spriano, Chiara Tarantelli, Andrea Rinaldi, Anastasios Stathis, Davide Rossi, Emanuele Zucca, Johann Zimmermann, and Francesco Bertoni

Subjects

Cancer Research, Oncology

Abstract

Introduction: CXCR4 is expressed in different B cell lymphoid neoplasms, and its levels are upregulated by BCR/PI3K blockade. High expression has been associated with resistance to BCR/PI3K inhibitors and gene mutations with reduced sensitivity to BTK inhibitors. We assessed whether its pharmacological inhibition with the potent CXCR4 inhibitor SPX5551 (POL5551) increases the antitumor activity of anti-lymphoma agents in lymphoma models, including some with secondary resistance to PI3K/BTK inhibitors. Methods: Antiproliferative activity was measured in mantle cell lymphoma (MCL, n=10), chronic lymphocytic leukemia (CLL,2), and marginal zone lymphoma (MZL, 2 + 4 derivatives with secondary resistance to PI3K and BTK inhibitors) cell lines exposed (72h) to increasing doses of compounds as single and in combination. Drugs included ibrutinib, copanlisib, idelalisib. The beneficial effect of the combinations versus the single agents was considered both as synergism (Chou-Talalay combination index), and as potency and efficacy (MuSyC algorithm). Mechanisms of action were studied by RNA-Seq, cell cycle and apoptosis assays, and immunofluorescence. Results: Combination of SPX5551 with conventional or targeted therapies was beneficial, either additive or synergistic, across all tested lymphomas. The combination of SPX5551 and ibrutinib was superior to single treatments in MCL, MZL or CLL, with stronger benefit in MZL and MCL than CLL. SPX5551/copanlisib showed synergism in both MCL and MZL, and SPX5551 addition overcame resistance in MZL with secondary resistance to idelalisib, copanlisib or ibrutinib. These results were confirmed using the clinically available drug candidate balixafortide (SPX6326, POL6326).RNA-Seq in the MCL REC1 model showed a much bigger impact of the SPX5551+ibrutinib on transcriptome than single agents: 2100 transcripts differentially expressed in the combination group vs DMSO (P Conclusions: Results suggest that a combination with the CXCR4 inhibitor SPX5551 adds beneficial effect to BCR inhibitors and might overcome resistance to PI3K/BTK inhibitors. Adding SPX551 to the treatment of patients with B cell lymphoma warrants further exploration. Citation Format: Laura Barnabei, Alberto J. Arribas, Luciano Cascione, Francesca Guidetti, Filippo Spriano, Chiara Tarantelli, Andrea Rinaldi, Anastasios Stathis, Davide Rossi, Emanuele Zucca, Johann Zimmermann, Francesco Bertoni. Pharmacological inhibition of CXCR4 increases the anti-tumor activity of conventional and targeted therapies in B cell lymphoma models [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2023; Part 1 (Regular and Invited Abstracts); 2023 Apr 14-19; Orlando, FL. Philadelphia (PA): AACR; Cancer Res 2023;83(7_Suppl):Abstract nr 492.

Published

2023

26. Abstract 394: ERBB4-mediated signaling is a mediator of resistance to BTK and PI3K inhibitors in B cell lymphoid neoplasms

Author

Alberto J. Arribas, Sara Napoli, Luciano Cascione, Laura Barnabei, Giulio Sartori, Eleonora Cannas, Eugenio Gaudio, Chiara Tarantelli, Afua A. Mensah, Filippo Spriano, Antonella Zucchetto, Francesca M. Rossi, Andrea Rinaldi, Manuel Castro de Moura, Anastasios Stathis, Georg Stussi, Valter Gattei, Jennifer R. Brown, Manel Esteller, Emanuele Zucca, Davide Rossi, and Francesco Bertoni

Subjects

Cancer Research, Oncology

Abstract

Background: Marginal zone lymphoma (MZL) is an indolent yet incurable B cell malignancy. Two BTK inhibitors, ibrutinib and zanubrutinib, are FDA approved for relapsed/refractory MZL patients. PI3K inhibitors have also shown clinical activity. The identification of the mechanisms of resistance can provide useful information to optimize the use of the agents. We previously reported an IL6 driven MZL model of PI3K inhibitors resistance developed by prolonged exposure to the PI3Kδ inhibitor idelalisib (Arribas, Haematologica 2022). Here, we present the detailed characterization of a second model with resistance to both BTK and PI3K inhibitors. Methods: MTT assay. RNA-Seq, whole exome sequencing, miRNA and methylation profiling. FACS and ELISA analyses. Results: Resistant cells, developed by continuous exposure of the cell line Karpas1718 to idelalisib, showed resistance to various inhibitors of BTK (ibrutinib, zanubrutinib, acalabrutinib and pirtobrutinib) and PI3K (idelalisib, duvelisib, copanlisib and umbralisib). No mutations affecting BTK, PLCG2 or CXCR4 were identified in resistant cells, which had higher expression of genes involved in ERBB signaling (HBEGF, NRG2, ERBB4), cell proliferation (PBK, MKI67, TCL1A) and DNA recombination (RAG1, RAG2) than parental cells. We confirmed cell surface ERBB4 up-regulation, and the cytoplasmatic expression and secretion of its ligand HBEGF in resistant cells, which led to increased levels of p-AKT and p-ERK. The miRNAs miR-29c and let-7c, known negative regulators of the HBEGF-ERBB axis, were fully methylated and down-regulated in resistant compared to parental cells. ERBB4 genetic silencing improved sensitivity to PI3Kδ inhibitor, and exposure to let-7c or miR-29c mimics decreased secreted HBEGF and recovered sensitivity to PI3K inhibitors in resistant cells. Addition of recombinant HBEGF (rHBEGF) induced resistance to BTK and to PI3K inhibitors in parental cells and in other lymphoma models including mantle cell lymphomas and diffuse large B cell lymphomas (DLBCL). The rHBEGF induced resistance was reverted adding the ERBB inhibitor lapatinib. To extend our findings to the clinical context, using two MZL and one DLBCL expression datasets, we showed HBEGF and ERBB4 expression in clinical specimens. Finally, HBEGF levels appeared elevated in the serum of CLL patients with primary or acquired resistance to PI3Kδ or to BTK inhibitors, compared to patients responding to the drugs and paired for similar clinical features. Conclusions: We characterized a novel B cell lymphoma model of secondary resistance to BTK and PI3K inhibitors. Our results indicate that epigenetic plasticity led to the activation of HBEGF-ERBB signaling sustaining resistance to BTK/PI3K inhibitors, which can be overcome using epigenetic agents and ERBB inhibitors. These therapeutics approaches could be tested in novel clinical trials. AJA, SN: equally contributed. Citation Format: Alberto J. Arribas, Sara Napoli, Luciano Cascione, Laura Barnabei, Giulio Sartori, Eleonora Cannas, Eugenio Gaudio, Chiara Tarantelli, Afua A. Mensah, Filippo Spriano, Antonella Zucchetto, Francesca M. Rossi, Andrea Rinaldi, Manuel Castro de Moura, Anastasios Stathis, Georg Stussi, Valter Gattei, Jennifer R. Brown, Manel Esteller, Emanuele Zucca, Davide Rossi, Francesco Bertoni. ERBB4-mediated signaling is a mediator of resistance to BTK and PI3K inhibitors in B cell lymphoid neoplasms [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2023; Part 1 (Regular and Invited Abstracts); 2023 Apr 14-19; Orlando, FL. Philadelphia (PA): AACR; Cancer Res 2023;83(7_Suppl):Abstract nr 394.

Published

2023

27. Functional testing of PI3K inhibitors stratifies responders to idelalisib and identifies treatment vulnerabilities in idelalisib-refractory/intolerant chronic lymphocytic leukemia

Author

Yanping Yin, Paschalis Athanasiadis, Linda Karlsen, Aleksandra Urban, Ishwarya Murali, Stacey M. Fernandes, Alberto J. Arribas, Abdul K. Hilli, Kjetil Taskén, Francesco Bertoni, Anthony R. Mato, Emmanuel Normant, Jennifer R. Brown, Geir E. Tjønnfjord, Tero Aittokallio, and Sigrid S. Skånland

Abstract

PurposePhosphatidylinositol 3-kinase inhibitors (PI3Ki) are approved for relapsed chronic lymphocytic leukemia (CLL). While patients may show an initial response, development of treatment intolerance or resistance remains a clinically challenging. Prediction of individual treatment responses based on clinically actionable biomarkers is needed to overcome these challenges. Here, we investigated whetherex vivofunctional responses to targeted therapies can stratify responders to idelalisib and guide precision medicine in CLL.Experimental designCLL cells from treatment naïve, idelalisib-responding, and idelalisib-refractory/intolerant patients (n=33 in total) were profiled against ten PI3Ki and the Bcl-2 antagonist venetoclax. Cell signaling and immune phenotypes were analyzed by flow cytometry. Cell viability was monitored by detection of cleaved caspase-3 and the CellTiter-Glo assay.ResultsAmong the ten PI3Ki studied, pan-PI3Ki were most effective at inhibiting PI3K signaling and cell viability, and they showed activity also in CLL cells from idelalisib-refractory/intolerant patients. The pan-PI3Ki copanlisib, but not the p110δ inhibitor idelalisib, inhibited PI3K signaling in CD4+and CD8+T cells in addition to CD19+B cells, while it did not significantly affect T cell numbers. Combination treatment with a PI3Ki and venetoclax resulted in synergistic induction of apoptosis. Based onex vivodrug sensitivity testing, a relapsed CLL patient was treated with idelalisib plus venetoclax, and the patient achieved a partial response. A more systematic analysis revealed that CLL cells from patients with a long-term response to idelalisib showed significantly higher drug sensitivities to 73 drug combinations at baseline compared to short-term responders.ConclusionsOur findings suggest novel treatment vulnerabilities in idelalisib-refractory/intolerant CLL, and demonstrate thatex vivofunctional profiling may guide precision medicine and predict treatment responses of individual CLL patients.TRANSLATIONAL RELEVANCEThe phosphatidylinositol 3-kinase inhibitors (PI3Ki) idelalisib and duvelisib are approved for relapsed chronic lymphocytic leukemia (CLL), but their use has been limited by severe toxicity and acquired resistance. Identification of biomarkers that predict individual treatment responses, as well as alternative treatment vulnerabilities in PI3Ki refractory/intolerant patients, is needed to optimally tailor CLL therapy. We performed functional analyses of CLL cells from treatment naïve, idelalisib-responding and idelalisib-refractory/intolerant patients to identify clinically actionable biomarkers. We show that CLL cells from idelalisib-refractory/intolerant patients remain sensitive to pan-PI3Ki and PI3Ki plus venetoclax combinations.Ex vivodrug sensitivity testing was used to guide treatment of a relapsed CLL patient who obtained a partial response after idelalisib plus venetoclax therapy. A systematic analysis of drug sensitivities to 73 drug combinations stratified responders to idelalisib using baseline samples from short-term and long-term responders to idelalisib. Our study demonstrates the power of functional precision medicine in relapsed CLL.

Published

2022

28. Targeting CD205 with the antibody drug conjugate MEN1309/OBT076 is an active new therapeutic strategy in lymphoma models

Author

Chiara Tarantelli, Giulio Sartori, Emanuele Zucca, Monica Binaschi, Francesca Guidetti, Filippo Spriano, Renzo Lucchini, Gaetanina Golino, Anastasios Stathis, Roberta Pittau Bordone, Eugenio Gaudio, Georg Stussi, Rachel L. Dusek, Luciano Cascione, Alessandro Bressan, Davide Rossi, Christian Rohlff, Arnima Bisht, Mario Bigioni, Robert S. Boyd, Andrea Pellacani, Nickolas Attanasio, Francesco Bertoni, Afua Adjeiwaa Mensah, Merlino Giuseppe, Elena Bernasconi, Alessio Fiascarelli, and Alberto J. Arribas

Subjects

0301 basic medicine, Antibody-drug conjugate, medicine.drug_class, business.industry, Venetoclax, Hematology, Monoclonal antibody, medicine.disease, Article, Lymphoma, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, chemistry, Targeted drug delivery, In vivo, hemic and lymphatic diseases, 030220 oncology & carcinogenesis, medicine, Cancer research, Rituximab, business, Diffuse large B-cell lymphoma, medicine.drug

Abstract

Antibody drug conjugates represent an important class of anti-cancer drugs in both solid tumors and hematological cancers. Here, we report preclinical data on the anti-tumor activity of the first-in-class antibody drug conjugate MEN1309/OBT076 targeting CD205. The study included preclinical in vitro activity screening on a large panel of cell lines, both as single agent and in combination and validation experiments on in vivo models. CD205 was first shown frequently expressed in lymphomas, leukemias and multiple myeloma by immunohistochemistry on tissue microarrays. Anti-tumor activity of MEN1309/OBT076 as single agent was then shown across 42 B-cell lymphoma cell lines with a median IC50 of 200 pM and induction of apoptosis in 25/42 (59.5%) of the cases. The activity appeared highly correlated with its target expression. After in vivo validation as the single agent, the antibody drug conjugate synergized with the BCL2 inhibitor venetoclax, and the anti-CD20 monoclonal antibody rituximab. The first-in-class antibody drug targeting CD205, MEN1309/OBT076, demonstrated strong pre-clinical anti-tumor activity in lymphoma, warranting further investigations as a single agent and in combination.

Published

2020

29. Subcapsular sinus macrophages promote melanoma metastasis to the sentinel lymph nodes via an IL-1α-STAT3 axis

Author

Tommaso Virgilio, Joy Bordini, Luciano Cascione, Giulio Sartori, Irene Latino, Daniel Molina Romero, Cristina Leoni, Murodzhon Akhmedov, Andrea Rinaldi, Alberto J. Arribas, Diego Morone, S. Morteza Seyed Jafari, Marina Bersudsky, Aner Ottolenghi, Ivo Kwee, Anna Maria Chiaravalli, Fausto Sessa, Robert E. Hunger, Antonino Bruno, Lorenzo Mortara, Elena Voronov, Silvia Monticelli, Ron N. Apte, Francesco Bertoni, and Santiago F. Gonzalez

Subjects

Cancer Research, Skin Neoplasms, Sentinel Lymph Node Biopsy, Macrophages, Immunology, 610 Medicine & health, Mice, Melanoma. Subcapsular sinus macrophages. Sentinel lymph nodes. IL1a–STAT3 axis. Immunotherapy approach, Lymphatic Metastasis, Tumor Microenvironment, Animals, Lymph Nodes, Sentinel Lymph Node, Melanoma, Lymphatic Vessels

Abstract

During melanoma metastasis, tumor cells originating in the skin migrate via lymphatic vessels to the sentinel lymph node (sLN). This process facilitates tumor cell spread across the body. Here, we characterized the innate inflammatory response to melanoma in the metastatic microenvironment of the sLN. We found that macrophages located in the subcapsular sinus (SS) produced protumoral IL1α after recognition of tumoral antigens. Moreover, we confirmed that the elimination of LN macrophages or the administration of an IL1α-specific blocking antibody reduced metastatic spread. To understand the mechanism of action of IL1α in the context of the sLN microenvironment, we applied single-cell RNA sequencing to microdissected metastases obtained from animals treated with the IL1α-specific blocking antibody. Among the different pathways affected, we identified STAT3 as one of the main targets of IL1α signaling in metastatic tumor cells. Moreover, we found that the antitumoral effect of the anti-IL1α was not mediated by lymphocytes because Il1r1 knockout mice did not show significant differences in metastasis growth. Finally, we found a synergistic antimetastatic effect of the combination of IL1α blockade and STAT3 inhibition with stattic, highlighting a new immunotherapy approach to preventing melanoma metastasis.

Published

2022

30. Resistance to PI3Kδ inhibitors in marginal zone lymphoma can be reverted by targeting the IL-6/PDGFRA axis

Author

Alberto J, Arribas, Sara, Napoli, Luciano, Cascione, Giulio, Sartori, Laura, Barnabei, Eugenio, Gaudio, Chiara, Tarantelli, Afua Adjeiwaa, Mensah, Filippo, Spriano, Antonella, Zucchetto, Francesca M, Rossi, Andrea, Rinaldi, Manuel, Castro de Moura, Sandra, Jovic, Roberta, Bordone-Pittau, Alessandra, Di Veroli, Anastasios, Stathis, Gabriele, Cruciani, Georg, Stussi, Valter, Gattei, Jennifer R, Brown, Manel, Esteller, Emanuele, Zucca, Davide, Rossi, and Francesco, Bertoni

Subjects

multiple, MicroRNAs, PDGFRA, Interleukin-6, expression, Humans, Lymphoma, B-Cell, Marginal Zone, gene, Leukemia, Lymphocytic, Chronic, B-Cell, Protein Kinase Inhibitors

Abstract

PI3Kδ inhibitors are active in patients with lymphoid neoplasms and a first series of them have been approved for the treatment of multiple types of B-cell lymphoid tumors, including marginal zone lymphoma (MZL). The identification of the mechanisms underlying either primary or secondary resistance is fundamental to optimize the use of novel drugs. Here we present a model of secondary resistance to PI3Kδ inhibitors obtained by prolonged exposure of a splenic MZL cell line to idelalisib. The VL51 cell line was kept under continuous exposure to idelalisib. The study included detailed characterization of the model, pharmacological screens, silencing experiments, and validation experiments on multiple cell lines and on clinical specimens. VL51 developed resistance to idelalisib, copanlisib, duvelisib, and umbralisib. An integrative analysis of transcriptome and methylation data highlighted an enrichment of upregulated transcripts and low-methylated promoters in resistant cells, including IL-6/STAT3- and PDGFRA-related genes and surface CD19 expression, alongside the repression of the let-7 family of miRNA, and miR-125, miR-130, miR-193 and miR-20. The IL-6R blocking antibody tocilizumab, the STAT3 inhibitor stattic, the LIN28 inhibitor LIN1632, the PDGFR inhibitor masitinib and the anti-CD19 antibody drug conjugate loncastuximab tesirine were active compounds in the resistant cells as single agents and/or in combination with PI3Kδ inhibition. Findings were validated on additional in vitro lymphoma models and on clinical specimens. A novel model of resistance obtained from splenic MZL allowed the identification of therapeutic approaches able to improve the antitumor activity of PI3Kδ inhibitors in B-cell lymphoid tumors.

Published

2022

31. Functional testing to characterize and stratify PI3K inhibitor responses in chronic lymphocytic leukemia

Author

Yanping Yin, Paschalis Athanasiadis, Linda Karlsen, Aleksandra Urban, Haifeng Xu, Ishwarya Murali, Stacey M. Fernandes, Alberto J. Arribas, Abdul K. Hilli, Kjetil Taskén, Francesco Bertoni, Anthony R. Mato, Emmanuel Normant, Jennifer R. Brown, Geir E. Tjønnfjord, Tero Aittokallio, and Sigrid S. Skånland

Subjects

Sulfonamides, Cancer Research, Caspase 3, Antineoplastic Agents, Bridged Bicyclo Compounds, Heterocyclic, Leukemia, Lymphocytic, Chronic, B-Cell, Article, Phosphatidylinositol 3-Kinases, Proto-Oncogene Proteins c-bcl-2, Oncology, Leukocytes, Mononuclear, Humans, Phosphoinositide-3 Kinase Inhibitors, Quinazolinones

Abstract

Purpose:PI3K inhibitors (PI3Ki) are approved for relapsed chronic lymphocytic leukemia (CLL). Although patients may show an initial response to these therapies, development of treatment intolerance or resistance remain clinical challenges. To overcome these, prediction of individual treatment responses based on actionable biomarkers is needed. Here, we characterized the activity and cellular effects of 10 PI3Ki and investigated whether functional analyses can identify treatment vulnerabilities in PI3Ki-refractory/intolerant CLL and stratify responders to PI3Ki.Experimental Design:Peripheral blood mononuclear cell samples (n = 51 in total) from treatment-naïve and PI3Ki-treated patients with CLL were studied. Cells were profiled against 10 PI3Ki and the Bcl-2 antagonist venetoclax. Cell signaling and immune phenotypes were analyzed by flow cytometry. Cell viability was monitored by detection of cleaved caspase-3 and the CellTiter-Glo assay.Results:pan-PI3Kis were most effective at inhibiting PI3K signaling and cell viability, and showed activity in CLL cells from both treatment-naïve and idelalisib-refractory/intolerant patients. CLL cells from idelalisib-refractory/intolerant patients showed overall reduced protein phosphorylation levels. The pan-PI3Ki copanlisib, but not the p110δ inhibitor idelalisib, inhibited PI3K signaling in CD4+ and CD8+ T cells in addition to CD19+ B cells, but did not significantly affect T-cell numbers. Combination treatment with a PI3Ki and venetoclax resulted in synergistic induction of apoptosis. Analysis of drug sensitivities to 73 drug combinations and profiling of 31 proteins stratified responders to idelalisib and umbralisib, respectively.Conclusions:Our findings suggest novel treatment vulnerabilities in idelalisib-refractory/intolerant CLL, and indicate that ex vivo functional profiling may stratify PI3Ki responders.

Published

2022

32. In vitro anti-lymphoma activity of the first-in-class pan-NOTCH transcription inhibitor CB-103

Author

Filippo Spriano, Chiara Tarantelli, Alberto J. Arribas, Eugenio Gaudio, Luciano Cascione, Luca Aresu, Andrea Rinaldi, Emanuele Zucca, Davide Rossi, Anastasios Stathis, Maximilien Murone, Freddy Radtke, Rajwinder Lehal, and Francesco Bertoni

Subjects

tumor, expression, leukemia, activation, Hematology, b-cell lymphoma, survival

Published

2022

33. IL-1α secreted by subcapsular sinus macrophages promotes melanoma metastasis in the sentinel lymph node by upregulating STAT3 signaling in the tumor

Author

Fausto Sessa, Alberto J. Arribas, Lorenzo Mortara, Daniel Molina-Romero, Santiago F. Gonzalez, Silvia Monticelli, Ivo Kwee, S. Morteza Seyed Jafari, Diego Morone, Aner Ottolenghi, Cristina Leoni, Ron N. Apte, Elena Voronov, Andrea Rinaldi, Tommaso Virgilio, Marina Bersudsky, Robert E. Hunger, Joy Bordini, Antonino Bruno, Giulio Sartori, Anna Maria Chiaravalli, Francesco Bertoni, Murodzhon Akhmedov, and Irene Latino

Subjects

business.industry, medicine.medical_treatment, Melanoma, Sentinel lymph node, Immunotherapy, medicine.disease, Metastasis, medicine.anatomical_structure, Lymphatic system, Antigen, Blocking antibody, Cancer research, medicine, business, Lymph node

Abstract

During melanoma metastasization, tumor cells originated in the skin migrate via lymphatic vessels to the sentinel lymph node (sLN) in a process that facilitates their spread across the body. Here, we characterized the innate inflammatory responses to melanoma metastasis in the sLN. For this purpose, we confirmed the migration of fluorescent metastatic melanoma cells to the sLN and we characterized the inflammatory response in the metastatic microenvironment. We found that macrophages located in the subcapsular sinus (SSM), produce pro-tumoral IL-1α after recognition of tumor antigens. Moreover, we confirmed that the administration of an anti-IL-1α depleting antibody reduced metastasis. Conversely, the administration of recombinant IL-1α accelerated the lymphatic spreading of the tumor. Additionally, the elimination of the macrophages significantly reduced the progression of the metastatic spread. To understand the mechanism of action of IL-1α in the context of the lymph node microenvironment, we applied single-cell RNA sequencing to dissected metastases obtained from animals treated with an anti-IL-1α blocking antibody. Amongst the different pathways affected, we identified STAT3 as one of the main targets of IL-1α signaling in metastatic cells. Moreover, we found that the anti-IL-1α anti-tumoral effect was not mediated by lymphocytes, as IL-1R1 KO mice did not show any improvement in metastasis growth. Finally, we found a synergistic anti-metastatic effect of the combination of IL-1α blocking and the STAT3 inhibitor (STAT3i) stattic. In summary, we described a new mechanism by which SSM support melanoma metastasis, highlighting a new target for immunotherapy.

Published

2021

34. GENETIC AND PHENOTYPIC ATTRIBUTES OF SPLENIC MARGINAL ZONE LYMPHOMA

Author

D. Piffaretti, Manuela Mollejo, L. Terzi di Bergamo, M. G. Cittone, Liliana Devizzi, Guido Ghilardi, Estella Matutes, Elena Sabattini, Elisa Lucchini, Sílvia Beà, Lydia Scarfò, Sergio Cogliatti, Stefano Pileri, Davide Rossi, M. Án. Piris, Govind Bhagat, Gilles Salles, Armando López-Guillermo, Maria Joao Baptista, Emanuele Zucca, Alden A. Moccia, Alessandra Tucci, Vincenzo Canzonieri, M. Ladetto, Luca Arcaini, Renzo Boldorini, Gabriela Forestieri, Maria Cristina Pirosa, Elias Campo, Alessandro Broccoli, Thomas Tousseyn, Sascha Dietrich, Roberto Marasca, Gianluca Gaidano, Ricardo Koch, Enrico Derenzini, Fabio Facchetti, Juan F. García, Alexandar Tzankov, Michele Merli, Carlo Visco, Hossein Khiabanian, Francesca Guidetti, Franco Cavalli, Arianna Calcinotto, Francesco Passamonti, Thorsten Zenz, Giuseppe Gritti, Julia T. Geyer, Marco Lucioni, M. Ponzoni, M. Faderl, Francesco Bertoni, Anastasios Stathis, Antonino Maiorana, Urban Novak, L. de Leval, Alexandra Traverse-Glehen, Luca Mazzucchelli, Anna Guidetti, Gabriela Bastidas, Véronique Meignin, P. L. Zinzani, Luciano Cascione, Ferdinando Bonfiglio, Giorgio Inghirami, Felicitas Hitz, Stefano Pizzolitto, Alberto J. Arribas, Angela Rita Elia, Elisa Santambrogio, Georg Stussi, Catherine Thieblemont, David Oscier, Marco Paulli, Bernhard Gerber, Umberto Vitolo, Alessio Bruscaggin, Francesco Piazza, Stefan Dirnhofer, W. Wu, Paolo Ghia, Valeria Spina, L. Bonomini, K. Pini, Gustavo Tapia, M. G. Da Silva, Luca Ceriani, Carlos Montalbán, and Adalgisa Condoluci

Subjects

Cancer Research, Pathology, medicine.medical_specialty, Oncology, medicine, Hematology, General Medicine, Splenic marginal zone lymphoma, Biology, medicine.disease, Phenotype

Published

2021

35. Novel insights into the genetics and epigenetics of MALT lymphoma unveiled by next generation sequencing analyses

Author

Chiara Tarantelli, Alexandar Tzankov, Ivo Kwee, Afua Adjeiwaa Mensah, Roberto N. Miranda, Valeria Spina, Lorenza Pecciarini, Gianluca Gaidano, Alberto J. Arribas, Maurilio Ponzoni, Alexandra Traverse-Glehen, Stephan Dirnhofer, Govind Bhagat, Alessio Bruscaggin, Elaine Y.L. Chung, Randy D. Gascoyne, Lodovico Terzi di Bergamo, Francesco Bertoni, Steven H. Swerdlow, Raul Rabadan, Ken H. Young, Davide Rossi, Andrea Rinaldi, Emanuele Zucca, and Luciano Cascione

Subjects

Regulation of gene expression, Genetics, Extramural, High-Throughput Nucleotide Sequencing, MALT lymphoma, Lymphoma, B-Cell, Marginal Zone, Hematology, Biology, Prognosis, medicine.disease, DNA sequencing, Epigenesis, Genetic, Lymphoma, Gene Expression Regulation, Neoplastic, medicine.anatomical_structure, Biomarkers, Tumor, medicine, Humans, Epigenetics, Online Only Articles, B cell, Epigenesis

Published

2019

36. The novel CD19-targeting antibody-drug conjugate huB4-DGN462 shows improved anti-tumor activity compared to SAR3419 in CD19-positive lymphoma and leukemia models

Author

Filippo Spriano, Francesco Bertoni, Callum M. Sloss, Anastasios Stathis, Stuart W. Hicks, Min Li, Georg Stussi, M. Taborelli, Davide Rossi, Qifeng Qiu, Chiara Tarantelli, Luciano Cascione, Alberto J. Arribas, Katharine C. Lai, Emanuele Zucca, Roberta Pittau Bordone, Alan Wilhem, and Eugenio Gaudio

Subjects

Antibody-drug conjugate, Immunoconjugates, Lymphoma, Non-Hodgkin Lymphoma, Antigens, CD19, Antineoplastic Agents, Antibodies, Monoclonal, Humanized, Article, CD19, Mice, 03 medical and health sciences, 0302 clinical medicine, Antigen, immune system diseases, In vivo, Cell Line, Tumor, hemic and lymphatic diseases, medicine, Animals, Humans, Cytotoxic T cell, Maytansine, Leukemia, Dose-Response Relationship, Drug, biology, business.industry, Hematology, medicine.disease, Xenograft Model Antitumor Assays, Disease Models, Animal, Treatment Outcome, Monoclonal, biology.protein, Cancer research, Female, business, 030215 immunology

Abstract

Antibody-drug conjugates (ADC) are a novel way to deliver potent cytotoxic compounds to cells expressing a specific antigen. Four ADC targeting CD19, including SAR3419 (coltuximab ravtansine), have entered clinical development. Here, we present huB4-DGN462, a novel ADC based on the SAR3419 anti-CD19 antibody linked via sulfo-SPDB to the potent DNA-alkylating agent DGN462. huB4-DGN462 had improved in vitro anti-proliferative and cytotoxic activity compared to SAR3419 across multiple B-cell lymphoma and human acute lymphoblastic leukemia cell lines. In vivo experiments using lymphoma xenografts models confirmed the in vitro data. The response of B-cell lymphoma lines to huB4-DGN462 was not correlated with CD19 expression, the presence of BCL2 or MYC translocations, TP53 inactivation or lymphoma histology. In conclusion, huB4-DGN462 is an attractive candidate for clinical investigation in patients with B-cell malignancies.

Published

2019

37. Genome-wide promoter methylation of hairy cell leukemia

Author

Afua Adjeiwaa Mensah, Giorgia Chiodin, Luciano Cascione, Francesco Bertoni, Davide Rossi, Richard Rosenquist, Andrea Rinaldi, Peter Johnson, Ivo Kwee, Emanuele Zucca, Meena Kanduri, Alberto J. Arribas, Christopher C. Oakes, Gianluca Gaidano, and Francesco Forconi

Subjects

0301 basic medicine, Immunoglobulin gene, Leukemia, Hairy Cell, Lymphoid Neoplasia, Gene Expression Profiling, Chronic lymphocytic leukemia, Hematology, Methylation, DNA Methylation, Biology, medicine.disease, Molecular biology, Gene expression profiling, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, 030220 oncology & carcinogenesis, DNA methylation, medicine, Humans, Hairy Cell, Hairy cell leukemia, Promoter Regions, Genetic, IGHV@, neoplasms

Abstract

Classic hairy cell leukemia (HCL) is a tumor of mature clonal B cells with unique genetic, morphologic, and phenotypic features. DNA methylation profiling has provided a new tier of investigation to gain insight into the origin and behavior of B-cell malignancies; however, the methylation profile of HCL has not been specifically investigated. DNA methylation profiling was analyzed with the Infinium HumanMethylation27 array in 41 mature B-cell tumors, including 11 HCL, 7 splenic marginal zone lymphomas (SMZLs), and chronic lymphocytic leukemia with an unmutated (n = 7) or mutated (n = 6) immunoglobulin gene heavy chain variable (IGHV) region or using IGHV3-21 (n = 10). Methylation profiles of nontumor B-cell subsets and gene expression profiling data were obtained from public databases. HCL had a methylation signature distinct from each B-cell tumor entity, including the closest entity, SMZL. Comparison with normal B-cell subsets revealed the strongest similarity with postgerminal center (GC) B cells and a clear separation from pre-GC and GC cellular programs. Comparison of the integrated analysis with post-GC B cells revealed significant hypomethylation and overexpression of BCR–TLR–NF-κB and BRAF-MAPK signaling pathways and cell adhesion, as well as hypermethylation and underexpression of cell-differentiation markers and methylated genes in cancer, suggesting regulation of the transformed hairy cells through specific components of the B-cell receptor and the BRAF signaling pathways. Our data identify a specific methylation profile of HCL, which may help to distinguish it from other mature B-cell tumors.

Published

2019

38. Abstract 2575: Avanbulin, the active moiety of the tumor checkpoint controller lisavanbulin (BAL101553), has anti-lymphoma activity

Author

Filippo Spriano, Luca Aresu, Luciano Cascione, Alberto J. Arribas, Nicole Forster-Gross, Felix Bachmann, Heidi Lane, and Francesco Bertoni

Subjects

Cancer Research, Oncology

Abstract

Background: Avanbulin (BAL27862) is a microtubule-targeting agent (MTA) that promotes tumor cell death by modulating the spindle assembly checkpoint. Preclinical studies in glioblastoma (GBM) have shown that avanbulin is also active in human cancer cells resistant to other MTAs used in the clinic. Lisavanbulin (BAL101553) is a water-soluble, oral, lysine prodrug of avanbulin, currently in phase 1/2 for patients with recurrent GBM and, in combination with radiotherapy, for newly diagnosed GBM patients. Preclinical studies and clinical signals have also suggested an association between lisavanbulin activity and expression of microtubule plus-end binding protein (EB1). MTAs are active agents for lymphoma patients, as exemplified by the inclusion of vincristine in the R-CHOP regimen, standard treatment for diffuse large B cell lymphoma (DLBCL). Thus, our aim was to evaluate avanbulin, the active moiety of lisavanbulin, for its potential anti-lymphoma activity. Methods: Lymphoma cell lines derived from activated B cell like (ABC) and germinal center B cell type (GCB) DLBCL were exposed to increasing doses of avanbulin; cell proliferation was measured with MTT. Apoptosis induction was performed with annexin V staining on cells incubated in a live cell imaging system (Incucyte) treated with 5, 10, 20 or 40nM avanbulin. Images were taken every 4h for 72h. Cell cycle analysis was performed after 24, 48 and 72h of drug exposure at 20nM. Results: 26 DLBCL cell lines, treated for 72h with increasing avanbulin doses, showed high anti-proliferative activity of the compound, with a median IC50 = 11nM. No differences in terms of IC50 were observed comparing ABC (n=8) to GCB (n=18) DLBCLs, nor based on MYD88, TP53 and BCL2 status. Cell lines with MYC translocation were less sensitive than the ones without translocation. All lymphoma cell lines exhibited high EB1 RNA expression, with no correlation with sensitivity to avanbulin.Live cell imaging demonstrated a strong apoptosis induction in 15 out of 17 cell lines tested at 20 and 40nM. Among the 15 cell lines undergoing apoptosis, 8 cell lines already showed an apoptosis induction within 24h of drug exposure, 6 lines between 24 and 48h and 1 line after 48h exposure. These data confirmed the high activity of avanbulin already seen with the MTT assay.Cell cycle experiments performed at 24, 48 and 72h confirmed the strong cytotoxic effect of avanbulin in 4 DLBCL cell lines, including 2 ABC (OCILY3 and TMD8) and 2 GCB (SUDHL5 and SUDHL16) lines. Sub-G0 accumulation was already present at 24h in all 4 cell lines tested, with an increase over time. Especially at 24h, where we also observed a G2-M arrest in 3 out of 4 cell lines. Conclusions: Our data demonstrate the high cytotoxic anti-lymphoma activity of avanbulin, suggesting a potential activity of its prodrug lisavanbulin in lymphoma patients. Citation Format: Filippo Spriano, Luca Aresu, Luciano Cascione, Alberto J. Arribas, Nicole Forster-Gross, Felix Bachmann, Heidi Lane, Francesco Bertoni. Avanbulin, the active moiety of the tumor checkpoint controller lisavanbulin (BAL101553), has anti-lymphoma activity [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2022; 2022 Apr 8-13. Philadelphia (PA): AACR; Cancer Res 2022;82(12_Suppl):Abstract nr 2575.

Published

2022

39. ASB2 is a direct target of FLI1 that sustains NF-κB pathway activation in germinal center-derived diffuse large B-cell lymphoma

Author

Giulio Sartori, Alberto J. Arribas, Chiara Falzarano, Francesco Bertoni, Laura Barnabei, Margot Thome, Luciano Cascione, Mattia Forcato, Afua Adjeiwaa Mensah, Silvio Bicciato, Sara Napoli, Andrea Rinaldi, Michela Dall'Angelo, Elaine Yee Lin Chung, and Valdemar Priebe

Subjects

Cancer Research, Gene Expression, Suppressor of Cytokine Signaling Proteins, Biology, ETS1, hemic and lymphatic diseases, Cell Line, Tumor, medicine, Diffuse large B-cell lymphoma (DLBCL), Gene silencing, Humans, Lymphoma, Large B-Cell, Diffuse/genetics, NF-kappa B/metabolism, Proto-Oncogene Protein c-fli-1/metabolism, Signal Transduction, Suppressor of Cytokine Signaling Proteins/metabolism, 11q24.3 gain, ASB2, NFKB pathway, Transcription factor FLI1, Transcription factor, RC254-282, Proto-Oncogene Protein c-fli-1, Research, fungi, NF-kappa B, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Germinal center, Cell cycle, medicine.disease, Oncology, Essential gene, FLI1, Cancer research, Lymphoma, Large B-Cell, Diffuse, Diffuse large B-cell lymphoma

Abstract

Background Diffuse large B-cell lymphoma (DLBCL) comprises at least two main biologically distinct entities: germinal center B-cell (GCB) and activated B-cell (ABC) subtype. Albeit sharing common lesions, GCB and ABC DLBCL present subtype-specific oncogenic pathway perturbations. ABC DLBCL is typically characterized by a constitutively active NF-kB. However, the latter is seen in also 30% of GCB DLBCL. Another recurrent lesion in DLBCL is an 11q24.3 gain, associated with the overexpression of two ETS transcription factors, ETS1 and FLI1. Here, we showed that FLI1 is more expressed in GCB than ABC DLBCL and we characterized its transcriptional network. Methods Gene expression data were obtained from public datasets GSE98588, phs001444.v2.p1, GSE95013 and GSE10846. ChIP-Seq for FLI1 paired with transcriptome analysis (RNA-Seq) after FLI1 silencing (siRNAs) was performed. Sequencing was carried out using the NextSeq 500 (Illumina). Detection of peaks was done using HOMER (v2.6); differential expressed genes were identified using moderated t-test (limma R-package) and functionally annotated with g:Profiler. ChIP-Seq and RNA-Seq data from GCB DLBCL cell lines after FLI1 downregulation were integrated to identify putative direct targets of FLI1. Results Analysis of clinical DLBCL specimens showed that FLI1 gene was more frequently expressed at higher levels in GCB than in ABC DLBCL and its protein levels were higher in GCB than in ABC DLBCL cell lines. Genes negatively regulated by FLI1 included tumor suppressor genes involved in negative regulation of cell cycle and hypoxia. Among positively regulated targets of FLI1, we found genes annotated for immune response, MYC targets, NF-κB and BCR signaling and NOTCH pathway genes. Of note, direct targets of FLI1 overlapped with genes regulated by ETS1, the other transcription factor gained at the 11q24.3 locus in DLBCL, suggesting a functional convergence within the ETS family. Positive targets of FLI1 included the NF-κB-associated ASB2 a putative essential gene for DLBCL cell survival. ASB2 gene downregulation was toxic in GCB DLBCL cell lines and induced NF-κB inhibition via downregulation of RelB and increased IκBα. Additionally, downregulation of FLI1, but not ASB2, caused reduction of NF-κB1 and RelA protein levels. Conclusions We conclude that FLI1 directly regulates a network of biologically crucial genes and processes in GCB DLBCL. FLI1 regulates both the classical NF-κB pathway at the transcriptional level, and the alternative NF-κB pathway, via ASB2. FLI1 and ASB2 inhibition represents a potential novel therapeutic approach for GCB DLBCL.

Published

2021

40. Genetic and Phenotypic Attributes of Splenic Marginal Zone Lymphoma

Author

Alessio Bruscaggin, Francesco Passamonti, Thomas Tousseyn, Anna Guidetti, Luca Ceriani, Paolo Corradini, Francesco Piazza, Carlos Montalbán, Adalgisa Condoluci, Marco Bühler, Giorgio A. Vanini, Lodovico Terzi di Bergamo, M. Faderl, Urban Novak, Miguel A. Piris, Luisella Bonomini, Elena Sabattini, Liliana Devizzi, Govind Bhagat, Carlo Visco, Fabio Facchetti, Arianna Calcinotto, Francesca Guidetti, M. Ladetto, Umberto Vitolo, Francesco Bertoni, Armando López-Guillermo, Giuseppe Gritti, Thorsten Zenz, Valeria Spina, Renata Walewska, Marco Paulli, Julia T. Geyer, David Oscier, Catherine Thieblemont, Estella Matutes, Francesco Zaja, Elisa Lucchini, Alexandra Traverse-Glehen, Guido Ghilardi, Emanuele Zucca, Alberto J. Arribas, Renzo Boldorini, Marco Lucioni, Pier Luigi Zinzani, K. Pini, Alden A. Moccia, Stefano Pileri, Alexander Tzankov, Wu Wei, Angela Rita Elia, Maria Joao Baptista, Lydia Scarfò, Stefan Dirnhofer, Laurence de Leval, Sílvia Beà, Gabriela Bastidas, Alessandra Tucci, Giorgio Inghirami, Gianluca Gaidano, Gilles Salles, Felicitas Hitz, Enrico Derenzini, Gustavo Tapia, Ferdinando Bonfiglio, Alessandro Broccoli, Micol Giulia Cittone, Sascha Dietrich, Luca Arcaini, Paolo Ghia, Hossein Khiabanian, Michele Merli, Alessandro Rambaldi, Manuela Mollejo, Maria Cristina Pirosa, Deborah Piffaretti, Anastasios Stathis, Antonino Maiorana, Ricardo Koch, Juan F. García, Sergio Cogliatti, Gabriela Forestieri, Roberto Marasca, Stefano Pizzolitto, Elisa Santambrogio, Georg Stussi, Maurilio Ponzoni, Bernhard Gerber, Maria Gomes da Silva, Corrado Tarella, Luciano Cascione, Elias Campo, Luca Mazzucchelli, Davide Rossi, Véronique Meignin, Vincenzo Canzonieri, Franco Cavalli, Bonfiglio, Ferdinando, Bruscaggin, Alessio, Guidetti, Francesca, Terzi di Bergamo, Lodovico, Faderl, Martin Richard, Spina, Valeria, Condoluci, Adalgisa, Bonomini, Luisella, Forestieri, Gabriela, Koch, Ricardo, Piffaretti, Deborah, Pini, Katia, Pirosa, Maria C, Cittone, Micol Giulia, Arribas, Alberto, Lucioni, Marco, Ghilardi, Guido, Wu, Wei, Arcaini, Luca, Baptista, Maria Joao, Bastidas, Gabriela, Beà, Silvia, Boldorini, Renzo, Broccoli, Alessandro, Bühler, Marco Matteo, Canzonieri, Vincenzo, Cascione, Luciano, Ceriani, Luca, Cogliatti, Sergio B, Corradini, Paolo, Derenzini, Enrico, Devizzi, Liliana, Dietrich, Sascha, Elia, Angela Rita, Facchetti, Fabio, Gaidano, Gianluca, Garcia, Juan F, Gerber, Bernhard, Ghia, Paolo, Gomes da Silva, Maria, Gritti, Giuseppe, Guidetti, Anna, Hitz, Felicita, Inghirami, Giorgio Ga, Ladetto, Marco, López-Guillermo, Armando, Lucchini, Elisa, Maiorana, Antonino, Marasca, Roberto, Matutes, Estella, Meignin, Véronique, Merli, Michele, Moccia, Alden A, Mollejo, Manuela, Montalban, Carlo, Novak, Urban, Oscier, David Graham, Passamonti, Francesco, Piazza, Francesco A, Pizzolitto, Stefano, Rambaldi, Alessandro, Sabattini, Elena, Salles, Gilles Andre, Santambrogio, Elisa, Scarfo, Lydia, Stathis, Anastasio, Stussi, Georg, Geyer, Julia Turbiner, Tapia, Gustavo, Tarella, Corrado, Thieblemont, Catherine, Tousseyn, Thoma, Tucci, Alessandra, Vanini, Giorgio, Visco, Carlo, Vitolo, Umberto, Walewska, Renata, Zaja, Francesco, Zenz, Thorsten, Zinzani, Pier Luigi, Khiabanian, Hossein, Calcinotto, Arianna, Bertoni, Francesco, Bhagat, Govind, Campo, Elia, de Leval, Laurence, Dirnhofer, Stefan, Pileri, Stefano A, Piris, Miguel A, Traverse-Glehen, Alexandra, Tzankov, Alexander, Paulli, Marco, Ponzoni, Maurilio, Mazzucchelli, Luca, Cavalli, Franco, Zucca, Emanuele, and Rossi, Davide

Subjects

Genetically modified mouse, Male, Lymphoma, Immunology, Marginal Zone, 610 Medicine & health, Computational biology, Biology, Biochemistry, Immunophenotyping, Mice, medicine, Tumor Microenvironment, Aged, Animals, Chromosome Aberrations, Female, Humans, Lymphoma, B-Cell, Marginal Zone/diagnosis, Lymphoma, B-Cell, Marginal Zone/genetics, Middle Aged, Multigene Family, Mutation, Spleen/pathology, Splenic Neoplasms/diagnosis, Splenic Neoplasms/genetics, Transcriptome, SMZL. molecular oncology, Splenic marginal zone lymphoma, Gene, Mechanism (biology), Splenic Neoplasms, B-Cell, Cell Biology, Hematology, Lymphoma, B-Cell, Marginal Zone, medicine.disease, Phenotype, Primary tumor, Immune checkpoint, 610 Medizin und Gesundheit, Spleen

Abstract

Splenic marginal zone B-cell lymphoma (SMZL) is a heterogeneous clinico-biological entity. The clinical course is variable, multiple genes are mutated with no unifying mechanism, and essential regulatory pathways and surrounding microenvironments are diverse. We sought to clarify the heterogeneity of SMZL by resolving different subgroups and their underlying genomic abnormalities, pathway signatures, and microenvironment compositions to uncover biomarkers and therapeutic vulnerabilities. We studied 303 SMZL spleen samples collected through the IELSG46 multicenter international study (NCT02945319) by using a multiplatform approach. We carried out genetic and phenotypic analyses, defined self-organized signatures, validated the findings in independent primary tumor metadata and determined correlations with outcome data. We identified 2 prominent genetic clusters in SMZL, termed NNK (58% of cases, harboring NF-κB, NOTCH, and KLF2 modules) and DMT (32% of cases, with DNA-damage response, MAPK, and TLR modules). Genetic aberrations in multiple genes as well as cytogenetic and immunogenetic features distinguished NNK- from DMT-SMZLs. These genetic clusters not only have distinct underpinning biology, as judged by differences in gene-expression signatures, but also different outcomes, with inferior survival in NNK-SMZLs. Digital cytometry and in situ profiling segregated 2 basic types of SMZL immune microenvironments termed immune-suppressive SMZL (50% of cases, associated with inflammatory cells and immune checkpoint activation) and immune-silent SMZL (50% of cases, associated with an immune-excluded phenotype) with distinct mutational and clinical connotations. In summary, we propose a nosology of SMZL that can implement its classification and also aid in the development of rationally targeted treatments.

Published

2021

41. Screening of fractions from marine sponges and other invertebrates to identify new lead compounds with anti-tumor activity in lymphoma models

Author

Filippo Spriano, S. O’Brien, Marilia Barreca, Olivier P. Thomas, Maria Miguel-Gordo, Francesco Bertoni, Alberto J. Arribas, Laurence K. Jennings, Spriano F., Barreca M., Miguel-Gordo M., O'Brien S., Arribas A.J., Jennings L., Thomas O., and Bertoni F.

Subjects

Marine sponges, Antitumor activity, Cancer Research, lymphoma, Biology, medicine.disease, Lymphoma, Lead (geology), Oncology, medicine, Cancer research, anti-tumor activity, Invertebrate, marine sponge

Abstract

Diffuse large B-cell lymphoma (DLBCL) is the commonest type of lymphomas, accounting for 30%-40% of new cases each year. Despite the big improvements achieved in the treatment, still 25–40% of patients still succumb due to refractory or relapsed disease. This highlights the need of new drugs for this cancer. The marine environment has recently been recognized as a source of anti-cancer compounds, as demonstrated by different marine drugs approved by different regulatory agencies (trabectedin, cytarabine, eribulin, plitidepsin) or as components of antibody drug conjugates for lymphoma patients (monomethyl auristatin E in polatuzumab vedotin and brentuximab vedotin). Here, we present a large screening of fractions obtained from different marine invertebrates collected in Ireland and in the Pacific Ocean on DLBCL cell lines

Published

2020

42. High-mobility group box (TOX) antibody a useful tool for the identification of B and T cell subpopulations

Author

Scherezade Jiménez, Miguel A. Piris, Patricia González-García, Alberto J. Arribas, Santiago Montes-Moreno, Lorena Maestre, Eduardo Caleiras, Giovanna Roncador, Alison H. Banham, Álvaro García-González, Juan Fernando García-García, Ana Isabel Reyes-García, European Commission, Comunidad de Madrid (España), Instituto de Salud Carlos III - ISCIII, Comunidad de Madrid, and Instituto de Salud Carlos III

Subjects

0301 basic medicine, Male, B Cells, Physiology, Chronic lymphocytic leukemia, Protein Expression, Follicular lymphoma, Gene Expression, Hematologic Cancers and Related Disorders, White Blood Cells, Antibodies, Monoclonal, Murine-Derived, Mice, fluids and secretions, 0302 clinical medicine, Animal Cells, immune system diseases, Antibody Specificity, T-Lymphocyte Subsets, Immune Physiology, hemic and lymphatic diseases, Medicine and Health Sciences, Lymph node, Staining, Multidisciplinary, T Cells, High Mobility Group Proteins, Cell Staining, Hematology, Marginal zone, Thymocyte, medicine.anatomical_structure, Lymphatic system, Oncology, 030220 oncology & carcinogenesis, Medicine, Lymphomas, Female, Cellular Types, Anatomy, Research Article, Lymphoma, B-Cell, Lymphoid Tissue, Immune Cells, Science, T cell, Immunology, B-Lymphocyte Subsets, Biology, Research and Analysis Methods, Lymphoma, T-Cell, Lymphatic System, 03 medical and health sciences, Cell Line, Tumor, Gene Expression and Vector Techniques, medicine, Animals, Humans, RNA, Messenger, Rats, Wistar, Antibody-Producing Cells, Molecular Biology Techniques, Immunohistochemistry Techniques, Molecular Biology, Molecular Biology Assays and Analysis Techniques, Blood Cells, Biology and Life Sciences, Cancers and Neoplasms, Cell Biology, medicine.disease, Lymphoma, Rats, Histochemistry and Cytochemistry Techniques, Mice, Inbred C57BL, 030104 developmental biology, Specimen Preparation and Treatment, Immunologic Techniques, Cancer research, bacteria, Lymph Nodes, Spleen

Abstract

Thymocyte selection-associated high-mobility group box (TOX) is a DNA-binding factor that is able to regulate transcription by modifying local chromatin structure and modulating the formation of multi-protein complexes. TOX has multiple roles in the development of the adaptive immune system including development of CD4 T cells, NK cells and lymph node organogenesis. However very few antibodies recognizing this molecule have been reported and no extensive study of the expression of TOX in reactive and neoplastic lymphoid tissue has been performed to date. In the present study, we have investigated TOX expression in normal and neoplastic lymphoid tissues using a novel rat monoclonal antibody that recognizes its target molecule in paraffin-embedded tissue sections. A large series of normal tissues and B- and T-cell lymphomas was studied, using whole sections and tissue microarrays. We found that the majority of precursor B/T lymphoblastic, follicular and diffuse large B-cell lymphomas, nodular lymphocyte-predominant Hodgkin lymphomas and angioimmunoblastic T-cell lymphomas strongly expressed the TOX protein. Burkitt and mantle cell lymphomas showed TOX expression in a small percentage of cases. TOX was not found in the majority of chronic lymphocytic leukemia, myelomas, marginal zone lymphomas and classical Hodgkin lymphomas. In conclusion, we describe for the first time the expression of TOX in normal and neoplastic lymphoid tissues. The co-expression of TOX and PD-1 identified in normal and neoplastic T cells is consistent with recent studies identifying TOX as a critical regulator of T-cell exhaustion and a potential immunotherapy target. Its differential expression may be of diagnostic relevance in the differential diagnosis of follicular lymphoma, the identification of the phenotype of diffuse large B-cell lymphoma and the recognition of peripheral T-cell lymphoma with a follicular helper T phenotype. This work was supported by grants from the Plan Nacional de I+D+I, co-financed by the ISCIII-Subdireccion General de Evaluacion and the Fondo Europeo de Desarrollo Regional (FEDER), CIBERONC -CB16/12/00291 (MAP), and Programs of R&D activities among research groups of the Community of Madrid in Biomedicine (B2017/BMD-3778) (MAP, GR, JFGG). All funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript. Sí

Published

2020

43. The Bruton tyrosine kinase inhibitor zanubrutinib (BGB-3111) demonstrated synergies with other anti-lymphoma targeted agents

Author

Luciano Cascione, Emanuele Zucca, Davide Rossi, Chiara Tarantelli, Lu Zhang, Filippo Spriano, Elisabetta Curti, Valdemar Priebe, Alberto J. Arribas, Anastasios Stathis, Francesco Bertoni, and Eugenio Gaudio

Subjects

Niacinamide, Lymphoma, B-Cell, Lymphoma, Mantle-Cell, Piperidines, Antineoplastic Combined Chemotherapy Protocols, Agammaglobulinaemia Tyrosine Kinase, Tumor Cells, Cultured, medicine, Humans, Bruton's tyrosine kinase, Online Only Articles, Cell Proliferation, Sulfonamides, biology, business.industry, Adenine, Drug Synergism, Hematology, Triazoles, Bridged Bicyclo Compounds, Heterocyclic, medicine.disease, Lymphoma, Hydrazines, Pyrimidines, biology.protein, Cancer research, Pyrazoles, business

Published

2019

44. Abstract P073: Pharmacological inhibition of IRAK4 with CA-4948 is beneficial in marginal zone lymphoma models with secondary resistance to PI3K and BTK inhibitors

Author

Francesca Guidetti, Alberto J. Arribas, Filippo Spriano, Laura Barnabei, Reinhard von Roemeling, Elizabeth Martinez, Emanuele Zucca, and Francesco Bertoni

Subjects

Cancer Research, Oncology

Abstract

Background. Marginal zone lymphoma (MZL) is a heterogeneous B-cell malignancy for which no standard treatment exists. B-cell receptor (BCR) signaling dysregulation is a hallmark of MZL and can mimic antigen dependent BCR activation. However, single treatment with BCR signaling inhibitors shows limited complete response rate and relapsing patients. IRAK4 is a protein kinase downstream the Toll-like receptor signaling. CA-4948 is the first-in-class inhibitor of IRAK4 and it is in phase 1/2 studies for patients with relapsed/refractory clinical studies with favorable activity in lymphomas and myeloid neoplasms. Here, we assessed IRAK4 inhibition with CA-4948 against a panel of MZL cell lines in which we have developed secondary resistance to inhibitors of PI3K (idelalisib, copanlisib) or BTK (ibrutinib). Methods. Models with secondary resistance were developed by continuous exposing cell lines derived from splenic MZL (Karpas 1718 and VL51) to high doses of drugs for long period of times. Resistant and parental lines were exposed to increasing doses of CA-4948, alone or in combination with compounds they are resistant to. Cell viability was tested by MTT assay (72h treatment). Synergy of combinations was evaluated according to the Chou-Talalay combination index (CI), as well as potency and efficacy, estimated according to the MuSyC algorithm. Results. The parental Karpas1718, bearing a MYD88 L265P mutation, had an IC50 of 3.29 µM for CA-4948 as single agent, while the parental VL51 and all resistant models presented IC50 values in the range of 19-35 µM. IRAK4 inhibition with CA-4948 had strong benefit when combined to downstream BCR inhibitors. In resistant cells, CA-4948 was strongly synergistic with idelalisib, ibrutinib and, at lesser extent, with copanlisib. CA-4948 in combination with ibrutinib was strongly synergistic especially in the VL51 ibrutinib resistant model compared to the parental one. CA-4948 (from 1 to 5 µM) recovered sensitivity to ibrutinib at IC50 values close to the parental condition. Similarly, CA-4948 in combination with idelalisib was also synergistic and increased sensitivity to idelalisib in idelalisib resistant VL51. Less benefit was seen adding CA-4948 to copanlisib: the combination was synergistic in VL51 parental cell, but with only weak efficacy. In the Karpas1718, CA-4948 was synergistic either in idelalisib resistant or in parental, with improved benefit in the latter, in which synergistic effect was observed when combined with both idelalisib and ibrutinib. The synergistic activity of CA-4948 was mainly due to improved efficacy rather than potency of the combinatorial partners. Conclusions. Our results in MZL cell lines show that the IRAK4 inhibitor CA-4948 is synergistic with small molecules targeting BCR signaling, especially with idelalisib and ibrutinib. Data also suggest that concentrations of CA-4948 comparable to those achieved in patients might overcome or reduce secondary resistance to the tested tyrosine kinase inhibitors. Citation Format: Francesca Guidetti, Alberto J. Arribas, Filippo Spriano, Laura Barnabei, Reinhard von Roemeling, Elizabeth Martinez, Emanuele Zucca, Francesco Bertoni. Pharmacological inhibition of IRAK4 with CA-4948 is beneficial in marginal zone lymphoma models with secondary resistance to PI3K and BTK inhibitors [abstract]. In: Proceedings of the AACR-NCI-EORTC Virtual International Conference on Molecular Targets and Cancer Therapeutics; 2021 Oct 7-10. Philadelphia (PA): AACR; Mol Cancer Ther 2021;20(12 Suppl):Abstract nr P073.

Published

2021

45. Methylation patterns in marginal zone lymphoma

Author

Francesco Bertoni and Alberto J. Arribas

Subjects

0301 basic medicine, Clinical Biochemistry, Biology, 03 medical and health sciences, hemic and lymphatic diseases, medicine, Humans, Splenic marginal zone lymphoma, Gene, Cell Proliferation, Splenic Neoplasms, MALT lymphoma, Promoter, DNA, Neoplasm, Lymphoma, B-Cell, Marginal Zone, Methylation, DNA Methylation, medicine.disease, Marginal zone, Lymphoma, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Oncology, DNA methylation, Immunology, Genome-Wide Association Study

Abstract

Promoter DNA methylation is a major regulator of gene expression and transcription. The identification of methylation changes is important for understanding disease pathogenesis, for identifying prognostic markers and can drive novel therapeutic approaches. In this review we summarize the current knowledge regarding DNA methylation in MALT lymphoma, splenic marginal zone lymphoma, nodal marginal zone lymphoma. Despite important differences in the study design for different publications and the existence of a sole large and genome-wide methylation study for splenic marginal zone lymphoma, it is clear that DNA methylation plays an important role in marginal zone lymphomas, in which it contributes to the inactivation of tumor suppressors but also to the expression of genes sustaining tumor cell survival and proliferation. Existing preclinical data provide the rationale to target the methylation machinery in these disorders.

Published

2017

46. Inhibition of <scp>CHK</scp> 1 and <scp>WEE</scp> 1 as a new therapeutic approach in diffuse large B cell lymphomas with <scp>MYC</scp> deregulation

Author

Laura Carrassa, Alberto J. Arribas, Valentina Restelli, Micaela Vagni, Francesco Bertoni, and Giovanna Damia

Subjects

Male, 0301 basic medicine, Cell Cycle Proteins, Pyrimidinones, Thiophenes, Cell Line, Proto-Oncogene Proteins c-myc, 03 medical and health sciences, Therapeutic approach, 0302 clinical medicine, medicine, Humans, Urea, Protein Kinase Inhibitors, B cell, biology, business.industry, Nuclear Proteins, Hematology, Protein-Tyrosine Kinases, medicine.disease, Wee1, Pyrimidines, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Checkpoint Kinase 1, Cancer research, biology.protein, Pyrazoles, Female, Lymphoma, Large B-Cell, Diffuse, business, Diffuse large B-cell lymphoma

Published

2016

47. Inhibition of Notch pathway arrests PTEN-deficient advanced prostate cancer by triggering p27-driven cellular senescence

Author

Alberto J. Arribas, Abdullah Alajati, Letizia Gnetti, Andrea Alimonti, Hermeto Gerber, Mitko Dimitrov, Ajinkya Revandkar, Maria Luna Perciato, Sandra Pinton, Nicolas Delaleu, Andrea Rinaldi, Marco Losa, Patrick C. Fraering, Emiliano Pasquini, Francesco Bertoni, Alain Nepveu, Alberto Toso, Rocco D'Antuono, and Jingjing Chen

Subjects

0301 basic medicine, Male, General Physics and Astronomy, ADAM17 Protein, Amyloid Precursor Protein Secretases, Animals, Cell Line, Tumor, Cellular Senescence, Cyclin-Dependent Kinase Inhibitor p27, Humans, Mice, PTEN Phosphohydrolase, Prostatic Neoplasms, Receptors, Notch, Signal Transduction, Tetrahydronaphthalenes, Up-Regulation, Valine, Prostate cancer, Prostate, Receptors, Tumor, Multidisciplinary, biology, 3. Good health, medicine.anatomical_structure, Signal transduction, Notch, Science, Notch signaling pathway, General Biochemistry, Genetics and Molecular Biology, Article, Cell Line, 03 medical and health sciences, Downregulation and upregulation, medicine, PTEN, ADAM17 Protein/genetics, ADAM17 Protein/metabolism, Amyloid Precursor Protein Secretases/antagonists & inhibitors, Cellular Senescence/drug effects, Cyclin-Dependent Kinase Inhibitor p27/metabolism, Cyclin-Dependent Kinase Inhibitor p27/physiology, PTEN Phosphohydrolase/genetics, PTEN Phosphohydrolase/metabolism, Prostatic Neoplasms/drug therapy, Prostatic Neoplasms/pathology, Receptors, Notch/antagonists & inhibitors, Receptors, Notch/metabolism, Signal Transduction/drug effects, Tetrahydronaphthalenes/therapeutic use, Valine/analogs & derivatives, Valine/therapeutic use, business.industry, General Chemistry, medicine.disease, 030104 developmental biology, Immunology, biology.protein, Cancer research, business, Amyloid precursor protein secretase

Abstract

Activation of NOTCH signalling is associated with advanced prostate cancer and treatment resistance in prostate cancer patients. However, the mechanism that drives NOTCH activation in prostate cancer remains still elusive. Moreover, preclinical evidence of the therapeutic efficacy of NOTCH inhibitors in prostate cancer is lacking. Here, we provide evidence that PTEN loss in prostate tumours upregulates the expression of ADAM17, thereby activating NOTCH signalling. Using prostate conditional inactivation of both Pten and Notch1 along with preclinical trials carried out in Pten-null prostate conditional mouse models, we demonstrate that Pten-deficient prostate tumours are addicted to the NOTCH signalling. Importantly, we find that pharmacological inhibition of γ-secretase promotes growth arrest in both Pten-null and Pten/Trp53-null prostate tumours by triggering cellular senescence. Altogether, our findings describe a novel pro-tumorigenic network that links PTEN loss to ADAM17 and NOTCH signalling, thus providing the rational for the use of γ-secretase inhibitors in advanced prostate cancer patients., Notch signalling is involved in prostate cancer progression and therapeutic resistance. Here, the authors show that loss of PTEN in prostate cancer models results in increased Notch1 cleavage and activation through CUX1-mediated transactivation of ADAM17.

Published

2016

48. Unraveling transformation of follicular lymphoma to diffuse large B-cell lymphoma

Author

Paloma Martín, Mariano Provencio, Manuela Mollejo, David Pérez-Callejo, Lucia Pedrosa, José Gómez-Codina, Juan F. García, Javier Menárguez, Carmen Bárcena, Luis de la Cruz-Merino, Antonio Rueda, Sagrario Gómez, Margarita Sánchez-Beato, Ana Royuela, Francisca I. Camacho, Cristina Quero, Consuelo Parejo, Alberto J. Arribas, Delvys Rodriguez-Abreu, Julia González-Rincón, Luciano Cascione, Ivo Kwee, Francesco Bertoni, Marta Llanos, Silvia Monsalvo, Carmen Bellas, Santiago Montes-Moreno, Socorro María Rodríguez-Pinilla, Miriam Mendez, and Miguel A. Piris

Subjects

Male, B Cells, Cell Lines, Biopsy, Follicular lymphoma, medicine.disease_cause, Hematologic Cancers and Related Disorders, White Blood Cells, Animal Cells, Medicine and Health Sciences, Copy-number variation, Frameshift Mutation, Lymphoma, Follicular, B-Lymphocytes, Mutation, Multidisciplinary, Massive parallel sequencing, Cell Differentiation, Hematology, Genomics, Diffuse large B-cell lymphoma, Middle Aged, Copy Number Variation, Neoplasm Proteins, Cell Transformation, Neoplastic, Oncology, Medicine, Lymphomas, Female, Biological Cultures, Lymphoma, Large B-Cell, Diffuse, Cellular Types, Raji Cells, Research Article, Adult, Follicular Lymphoma, Immune Cells, Science, Immunology, Surgical and Invasive Medical Procedures, Biology, Research and Analysis Methods, Genome Complexity, Genetics, medicine, Humans, Antibody-Producing Cells, Aged, Blood Cells, Biology and Life Sciences, Cancers and Neoplasms, Computational Biology, Cell Biology, medicine.disease, GNA13, Lymphoma, Transformation (genetics), Cancer research, Follow-Up Studies

Abstract

Follicular lymphoma (FL) is an indolent but largely incurable disease. Some patients suffer histological transformation to a more aggressive subtype with poorer prognosis. This study aimed to improve our understanding of the genetics underlying FL histological transformation, and to identify genetic drivers or promoters of the transformation by elucidating the differences between FL samples from patients who did and did not transform. We conducted targeted massive parallel sequencing of 22 pre-transformed FL/transformed diffuse large B-cell lymphoma pairs and 20 diagnostic samples from non-transformed FL patients. Additionally, 22 matched samples from 11 transformed FL patients (pre-transformed FL and diffuse large B-cell lymphoma) and 9 non-transformed FLs were studied for copy number variation using SNP arrays. We identified recurrently mutated genes that were enriched at transformation, most notably LRP1B, GNA13 and POU2AF1, which have roles in B-cell differentiation, GC architecture and migration. Mutations in POU2AF1 might be associated with lower levels of expression, were more frequent in transformed FLs, and seemed to be specific to transformed- compared with de novo-diffuse large B-cell lymphomas. Pre-transformed FLs carried more mutations per sample and had greater subclonal heterogeneity than non-transformed FLs. Finally, we identified four mutated genes in FL samples that differed between patients who did and did not transform: NOTCH2, DTX1, UBE2A and HIST1H1E. The presence of mutations in these genes was associated with shorter time to transformation when mutated in the FL biopsies. This information might be useful for identifying patients at higher risk of transformation.

Published

2019

49. A Reliable Method to Remove Batch Effects Maintaining Group Differences in Lymphoma Methylation Case Study

Author

Francesco Bertoni, Rosalba Giugno, Luciano Cascione, Alberto J. Arribas, Andrea Rinaldi, and Giulia Pontali

Subjects

Biological data, Mathematical model, Lymphoma, business.industry, Computer science, Machine learning, computer.software_genre, Pipeline (software), Methylation, Batch effects removal, Group differences, Artificial intelligence, Variability, business, computer

Abstract

The amount of biological data is increasing and their analysis is becoming one of the most challenging topics in the information sciences. Before starting the analysis it is important to remove unwanted variability due to some factors such as: year of sequencing, laboratory conditions and use of different protocols. This is a crucial step because if the variability is not evaluated before starting the analysis of interest, the results may be undesirable and the conclusion can not be true. The literature suggests to use some valid mathematical models, but experience shows that applying these to high-throughput data with a non-uniform study design is not straightforward and in many cases it may introduce a false signal. Therefore it is necessary to develop models that allow to remove the effects that can negatively influence the study preserving biological meaning. In this paper we report a new case study related lymphoma methylation data and we propose a suitable pipeline for its analysis.

Published

2019

50. Biology of splenic and nodal marginal zone lymphomas

Author

Afua Adjeiwaa Mensah, Valeria Spina, and Alberto J. Arribas

Subjects

General Medicine, Anatomy, Biology, Marginal zone, NODAL

Published

2021