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1. 5-Hydroxymethylcytosine Loss in Conjunctival Melanoma

Author

Alexandre Stahl, Nicolo Riggi, Katya Nardou, Michael Nicolas, Gurkan Kaya, and Alexandre Moulin

Subjects
conjunctival melanoma, epigenetics, 5-hydroxymethylcytosine, 5-methylcytosine, TET2, Dermatology, RL1-803
Abstract

Aims: Conjunctival and cutaneous melanoma partially share similar clinical and molecular backgrounds. As 5-hydroxymethylcytosine (5-hmC) loss has been demonstrated in cutaneous melanoma, we decided to assess if similar changes were occurring in conjunctival melanoma. Methods: 5-methylcytosine (5-mC), 5-hmC and TET2 were respectively identified by immunohistochemistry and RNA ISH in 40 conjunctival nevi and 37 conjunctival melanomas. Clinicopathological correlations were established. Results: 5-mC, TET2 and 5-hmC were respectively identified in 67.5%, 95% and 100% of conjunctival nevi and in 81.1%, 35.1% and 54% of conjunctival melanomas. A significant 5-hmC and TET2 loss was identified in conjunctival melanoma comparing to nevus, as well as a significant correlation between TET2 and 5-hmC expression. In the melanomas, 5-hmC expression was only significantly associated with local lymphatic invasion, but not with other clinicopathological parameters. There was a correlation between TET2 expression and the localization of the tumors. 5-mC expression was not associated with any clinicopathological parameters. Conclusions: We identified a significant 5-hmC loss in conjunctival melanoma similar to cutaneous melanoma. This loss may possibly be attributed to TET2 loss or IDH1 mutations. 5-hmC loss in conjunctival melanoma may help in the differential diagnosis between atypical conjunctival nevus and conjunctival melanoma.

Published
2021
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2. β-Catenin Expression and Activation in Conjunctival Melanoma

Author

Emerentienne Larivé, Michael Nicolas, Gürkan Kaya, Nicolo Riggi, and Alexandre P. Moulin

Subjects
Eye, Melanogenesis, Melanoma, Conjunctiva, Dermatology, RL1-803
Abstract

Purpose: To assess the role of the canonical Wnt pathway via activation of β-catenin in tumor progression of conjunctival melanoma. Methods: β-Catenin localization was assessed by immunohistochemistry in 43 conjunctival nevi, 48 primary acquired melanoses (PAM; conjunctival melanocytic intraepithelial neoplasia), and 44 conjunctival melanomas. Activation of the canonical or the noncanonical Wnt pathway was tested in vitro in 4 conjunctival melanoma cell lines with stimulation of either Wnt5a or Wnt3a. Wound healing assays were performed with Wnt5a. Results: Nuclear β-catenin expression was found in 16% of the nevi, in 15% of the melanomas, and in 4% of the PAM. Membranous β-catenin expression was identified in all the nevi and PAM and in 97.7% of the melanomas. In vitro, Wnt5a stimulation in the 4 conjunctival melanomas and in 1 skin melanoma cell line did not induce nuclear translocation of β-catenin, nor did it increase cell motility in the wound healing assays. Wnt3a stimulation did not induce nuclear localization of β-catenin in any of the cell lines tested. Conclusions: In conjunctival melanoma, nuclear localization and activation of β-catenin appear to be limited, suggesting that inhibition of ARF6, responsible for β-catenin activation, in subsets of skin melanoma may not represent a treatment option for this tumor. In vitro, Wnt3a or Wnt5a did not induce nuclear β-catenin localization.

Published
2019
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3. Reciprocal modulation of mesenchymal stem cells and tumor cells promotes lung cancer metastasis

Author

Giulia Fregni, Mathieu Quinodoz, Emely Möller, Joanna Vuille, Sabine Galland, Carlo Fusco, Patricia Martin, Igor Letovanec, Paolo Provero, Carlo Rivolta, Nicolo Riggi, and Ivan Stamenkovic

Subjects
Medicine, Medicine (General), R5-920
Abstract

Metastasis is a multi-step process in which direct crosstalk between cancer cells and their microenvironment plays a key role. Here, we assessed the effect of paired tumor-associated and normal lung tissue mesenchymal stem cells (MSCs) on the growth and dissemination of primary human lung carcinoma cells isolated from the same patients. We show that the tumor microenvironment modulates MSC gene expression and identify a four-gene MSC signature that is functionally implicated in promoting metastasis. We also demonstrate that tumor-associated MSCs induce the expression of genes associated with an aggressive phenotype in primary lung cancer cells and selectively promote their dissemination rather than local growth. Our observations provide insight into mechanisms by which the stroma promotes lung cancer metastasis. Keywords: Tumor-associated MSCs, lung cancer, metastasis, GREM1, LOXL2, ADAMTS12, ITGA11

Published
2018
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4. The RNA Binding Protein IMP2 Preserves Glioblastoma Stem Cells by Preventing let-7 Target Gene Silencing

Author

Nils Degrauwe, Tommy B. Schlumpf, Michalina Janiszewska, Patricia Martin, Alexandra Cauderay, Paolo Provero, Nicolo Riggi, Mario-L. Suvà, Renato Paro, and Ivan Stamenkovic

Subjects
Biology (General), QH301-705.5
Abstract

Cancer stem cells (CSCs) can drive tumor growth, and their maintenance may rely on post-transcriptional regulation of gene expression, including that mediated by microRNAs (miRNAs). The let-7 miRNA family has been shown to induce differentiation by silencing stem cell programs. Let-7-mediated target gene suppression is prevented by LIN28A/B, which reduce let-7 biogenesis in normal embryonic and some cancer stem cells and ensure maintenance of stemness. Here, we find that glioblastoma stem cells (GSCs) lack LIN28 and express both let-7 and their target genes, suggesting LIN28-independent protection from let-7 silencing. Using photoactivatable-ribonucleoside-enhanced crosslinking and immunoprecipitation (PAR-CLIP), we show that insulin-like growth factor 2 mRNA-binding protein 2 (IMP2) binds to let-7 miRNA recognition elements (MREs) and prevents let-7 target gene silencing. Our observations define the RNA-binding repertoire of IMP2 and identify a mechanism whereby it supports GSC and neural stem cell specification.

Published
2016
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5. Synovial sarcoma: when epigenetic changes dictate tumour development

Author

Nicolo Riggi, Luisa Cironi, and Ivan Stamenkovic

Subjects
Chromatin, Epigenetics, pathogenesis, SS18-SSX, synovial sarcoma, Medicine
Abstract

Synovial sarcoma is a highly aggressive soft tissue malignancy that often affects adolescents and young adults. It is associated with a unique chromosomal translocation that results in the formation and expression of the fusion gene SS18-SSX, which underlies its pathogenesis. Although SS18-SSX provides a potentially unique therapeutic target, all attempts to neutralise it have been unsuccessful thus far. When complete surgical removal of the tumour fails, therapy is limited to largely ineffective cytotoxic drug regimens. Nevertheless, recent discoveries about the mechanisms of SS18-SSX protein function have provided insight into potential alternative therapeutic strategies. SS18-SSX displays oncogenic activity through protein-protein interactions and participation in chromatin remodelling complexes. This review summarises our current understanding of the function of SS18-SSX and the mechanisms by which it alters the epigenetic landscape of permissive cells to induce transformation and the subsequent development of synovial sarcoma.

Published
2018
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6. Pan-Cancer Landscape of Aberrant DNA Methylation across Human Tumors

Author

Sadegh Saghafinia, Marco Mina, Nicolo Riggi, Douglas Hanahan, and Giovanni Ciriello

Subjects
Biology (General), QH301-705.5
Abstract

Summary: The discovery of cancer-associated alterations has primarily focused on genetic variants. Nonetheless, altered epigenomes contribute to deregulate transcription and promote oncogenic pathways. Here, we designed an algorithmic approach (RESET) to identify aberrant DNA methylation and associated cis-transcriptional changes across >6,000 human tumors. Tumors exhibiting mutations of chromatin remodeling factors and Wnt signaling displayed DNA methylation instability, characterized by numerous hyper- and hypo-methylated loci. Most silenced and enhanced genes coalesced in specific pathways including apoptosis, DNA repair, and cell metabolism. Cancer-germline antigens (CG) were frequently epigenomically enhanced and their expression correlated with response to anti-PD-1, but not anti-CTLA4, in skin melanoma. Finally, we demonstrated the potential of our approach to explore DNA methylation changes in pediatric tumors, which frequently lack genetic drivers and exhibit epigenomic modifications. Our results provide a pan-cancer map of aberrant DNA methylation to inform functional and therapeutic studies. : Saghafinia et al. present an algorithmic approach to identify cancer-associated DNA methylation changes affecting gene expression. By analyzing >6,000 adult and pediatric tumors, the authors identify numerous DNA methylation changes at gene promoters that coalesce into a few pathways and that were associated with patient prognosis and response to therapy. Keywords: aberrant DNA methylation, cancer epigenetics, DNA methylation instability, TCGA pan-cancer cohort, pediatric cancer

Published
2018
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7. Let-7a is a direct EWS-FLI-1 target implicated in Ewing's sarcoma development.

Author

Claudio De Vito, Nicolo Riggi, Mario-Luca Suvà, Michalina Janiszewska, Janine Horlbeck, Karine Baumer, Paolo Provero, and Ivan Stamenkovic

Subjects
Medicine, Science
Abstract

Ewing's sarcoma family tumors (ESFT) are the second most common bone malignancy in children and young adults, characterized by unique chromosomal translocations that in 85% of cases lead to expression of the EWS-FLI-1 fusion protein. EWS-FLI-1 functions as an aberrant transcription factor that can both induce and suppress members of its target gene repertoire. We have recently demonstrated that EWS-FLI-1 can alter microRNA (miRNA) expression and that miRNA145 is a direct EWS-FLI-1 target whose suppression is implicated in ESFT development. Here, we use miRNA arrays to compare the global miRNA expression profile of human mesenchymal stem cells (MSC) and ESFT cell lines, and show that ESFT display a distinct miRNA signature that includes induction of the oncogenic miRNA 17-92 cluster and repression of the tumor suppressor let-7 family. We demonstrate that direct repression of let-7a by EWS-FLI-1 participates in the tumorigenic potential of ESFT cells in vivo. The mechanism whereby let-7a expression regulates ESFT growth is shown to be mediated by its target gene HMGA2, as let-7a overexpression and HMGA2 repression both block ESFT cell tumorigenicity. Consistent with these observations, systemic delivery of synthetic let-7a into ESFT-bearing mice restored its expression in tumor cells, decreased HMGA2 expression levels and resulted in ESFT growth inhibition in vivo. Our observations provide evidence that deregulation of let-7a target gene expression participates in ESFT development and identify let-7a as promising new therapeutic target for one of the most aggressive pediatric malignancies.

Published
2011
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21. Data from Nongenetic Evolution Drives Lung Adenocarcinoma Spatial Heterogeneity and Progression

Author

Giovanni Ciriello, Igor Letovanec, Elisa Oricchio, Nicolo Riggi, David Gfeller, Thorsten Krueger, Solange Peters, Jessica Sordet-Dessimoz, Marco Mina, Aaron S. Petruzzella, Elie Dheilly, Elena Battistello, and Daniele Tavernari

Abstract

Cancer evolution determines molecular and morphologic intratumor heterogeneity and challenges the design of effective treatments. In lung adenocarcinoma, disease progression and prognosis are associated with the appearance of morphologically diverse tumor regions, termed histologic patterns. However, the link between molecular and histologic features remains elusive. Here, we generated multiomics and spatially resolved molecular profiles of histologic patterns from primary lung adenocarcinoma, which we integrated with molecular data from >2,000 patients. The transition from indolent to aggressive patterns was not driven by genetic alterations but by epigenetic and transcriptional reprogramming reshaping cancer cell identity. A signature quantifying this transition was an independent predictor of patient prognosis in multiple human cohorts. Within individual tumors, highly multiplexed protein spatial profiling revealed coexistence of immune desert, inflamed, and excluded regions, which matched histologic pattern composition. Our results provide a detailed molecular map of lung adenocarcinoma intratumor spatial heterogeneity, tracing nongenetic routes of cancer evolution.Significance:Lung adenocarcinomas are classified based on histologic pattern prevalence. However, individual tumors exhibit multiple patterns with unknown molecular features. We characterized nongenetic mechanisms underlying intratumor patterns and molecular markers predicting patient prognosis. Intratumor patterns determined diverse immune microenvironments, warranting their study in the context of current immunotherapies.This article is highlighted in the In This Issue feature, p. 1307

Published
2023
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22. Video from Inhibition of Haspin Kinase Promotes Cell-Intrinsic and Extrinsic Antitumor Activity

Author

Benjamin Izar, Peter K. Sorger, Kai W. Wucherpfennig, Nicolo Riggi, Dirk Schadendorf, Alexander Spektor, David M. Miller, Titus J. Brinker, Shaolin Mei, Adrienne Luoma, Adam N.R. Cartwright, Meri Rogava, Kartik Subramanian, Steven Rodriguez, Nienke Moret, Derrick Deming, Sushil Kumar, Patricia Waszyk, Eugenio Morelli, Jia-Yun Chen, Clarence Yapp, Caitlin E. Mills, Sreeram Vallabhaneni, and Johannes C. Melms

Abstract

Video Control

Published
2023
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23. Supplementary Figures from Inhibition of Haspin Kinase Promotes Cell-Intrinsic and Extrinsic Antitumor Activity

Author

Benjamin Izar, Peter K. Sorger, Kai W. Wucherpfennig, Nicolo Riggi, Dirk Schadendorf, Alexander Spektor, David M. Miller, Titus J. Brinker, Shaolin Mei, Adrienne Luoma, Adam N.R. Cartwright, Meri Rogava, Kartik Subramanian, Steven Rodriguez, Nienke Moret, Derrick Deming, Sushil Kumar, Patricia Waszyk, Eugenio Morelli, Jia-Yun Chen, Clarence Yapp, Caitlin E. Mills, Sreeram Vallabhaneni, and Johannes C. Melms

Abstract

Suppl. F1: On-target activity and toxicity of CX-6258 Suppl. F2: On-target activity of CX-6258 and siRNA KD of Haspin Suppl. F3: Effects of CX-6258 on cell-cycle and cGAS recruitment Suppl. F4: In vivo effects of CX-6258

Published
2023
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24. Supplementary Table 1 from Inhibition of Haspin Kinase Promotes Cell-Intrinsic and Extrinsic Antitumor Activity

Author

Benjamin Izar, Peter K. Sorger, Kai W. Wucherpfennig, Nicolo Riggi, Dirk Schadendorf, Alexander Spektor, David M. Miller, Titus J. Brinker, Shaolin Mei, Adrienne Luoma, Adam N.R. Cartwright, Meri Rogava, Kartik Subramanian, Steven Rodriguez, Nienke Moret, Derrick Deming, Sushil Kumar, Patricia Waszyk, Eugenio Morelli, Jia-Yun Chen, Clarence Yapp, Caitlin E. Mills, Sreeram Vallabhaneni, and Johannes C. Melms

Abstract

Suppl. Table 1: Compounds used in drug screen

Published
2023
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25. Data from Inhibition of Haspin Kinase Promotes Cell-Intrinsic and Extrinsic Antitumor Activity

Author

Benjamin Izar, Peter K. Sorger, Kai W. Wucherpfennig, Nicolo Riggi, Dirk Schadendorf, Alexander Spektor, David M. Miller, Titus J. Brinker, Shaolin Mei, Adrienne Luoma, Adam N.R. Cartwright, Meri Rogava, Kartik Subramanian, Steven Rodriguez, Nienke Moret, Derrick Deming, Sushil Kumar, Patricia Waszyk, Eugenio Morelli, Jia-Yun Chen, Clarence Yapp, Caitlin E. Mills, Sreeram Vallabhaneni, and Johannes C. Melms

Abstract

Patients with melanoma resistant to RAF/MEK inhibitors (RMi) are frequently resistant to other therapies, such as immune checkpoint inhibitors (ICI), and individuals succumb to their disease. New drugs that control tumor growth and favorably modulate the immune environment are therefore needed. We report that the small-molecule CX-6258 has potent activity against both RMi-sensitive (RMS) and -resistant (RMR) melanoma cell lines. Haspin kinase (HASPIN) was identified as a target of CX-6258. HASPIN inhibition resulted in reduced proliferation, frequent formation of micronuclei, recruitment of cGAS, and activation of the cyclic GMP-AMP synthase (cGAS)–stimulator of interferon genes (STING) pathway. In murine models, CX-6258 induced a potent cGAS-dependent type-I IFN response in tumor cells, increased IFNγ-producing CD8+ T cells, and reduced Treg frequency in vivo. HASPIN was more strongly expressed in malignant compared with healthy tissue and its inhibition by CX-6258 had minimal toxicity in ex vivo–expanded human tumor-infiltrating lymphocytes (TIL), proliferating TILs, and in vitro differentiated neurons, suggesting a potential therapeutic index for anticancer therapy. Furthermore, the activity of CX-6258 was validated in several Ewing sarcoma and multiple myeloma cell lines. Thus, HASPIN inhibition may overcome drug resistance in melanoma, modulate the immune environment, and target a vulnerability in different cancer lineages.Significance:HASPIN inhibition by CX-6258 is a novel and potent strategy for RAF/MEK inhibitor–resistant melanoma and potentially other tumor types. HASPIN inhibition has direct antitumor activity and induces a favorable immune microenvironment.

Published
2023
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26. Supplementary Data from Inhibition of Haspin Kinase Promotes Cell-Intrinsic and Extrinsic Antitumor Activity

Author

Benjamin Izar, Peter K. Sorger, Kai W. Wucherpfennig, Nicolo Riggi, Dirk Schadendorf, Alexander Spektor, David M. Miller, Titus J. Brinker, Shaolin Mei, Adrienne Luoma, Adam N.R. Cartwright, Meri Rogava, Kartik Subramanian, Steven Rodriguez, Nienke Moret, Derrick Deming, Sushil Kumar, Patricia Waszyk, Eugenio Morelli, Jia-Yun Chen, Clarence Yapp, Caitlin E. Mills, Sreeram Vallabhaneni, and Johannes C. Melms

Abstract

Methods and Suppl. Figure Legends

Published
2023
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29. KDM6 demethylases mediate EWSR1-FLI1-driven oncogenic transformation in Ewing Sarcoma

Author

Elisabet Figuerola-Bou, Carla Rios-Astorch, Enrique Blanco, María Sánchez-Jiménez, Pablo Táboas, Guerau Fernández, Soledad Gómez, Oscar Muñoz, Pol Castellano-Escuder, Sara Pérez-Jaume, Estela Prada, Silvia Mateo-Lozano, Nicolo Riggi, Alexandra Avgustinova, Cinzia Lavarino, Luciano Di Croce, Sara Sánchez-Molina, and Jaume Mora

Abstract

SUMMARYEwing Sarcoma (EwS) is an aggressive bone and soft tissue tumor driven by the fusion oncoprotein EWSR1-FLI1. This aberrant transcription factor binds to GGAA microsatellites, causing epigenetic reprogramming through the formation of active neo-enhancers in a permissive cellular context. Inhibition of the oncogene remains challenging and current efforts instead seek to exploit emergent epigenetic treatments targeting EWSR1-FLI1 cofactors. Here, stemming from the genome-wide redistribution of H3K27me3 upon expression of EWSR1-FLI1 in pediatric hMSC, we unravel the contribution of the H3K27me3 demethylases KDM6A and KDM6B in transcriptional activation at EWSR1-FLI1 enhancers. We found that KDM6A has a demethylase-independent role in recruiting the SWI/SNF member BRG1 at EWSR1-FLI1-primed enhancers containing single GGAA motif, which is critical for EwS tumor growth. Conversely, KDM6B demethylates H3K27me3 at EWSR1-FLI1-active enhancers containing multimeric GGAA repeats and its deletion synergizes with EZH2 inhibitors. Our results highlight KDM6 demethylases as EWSR1-FLI1 cofactors with potential for future targeted therapies.

Published
2023
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30. EWS-WT1 fusion isoforms establish oncogenic programs and therapeutic vulnerabilities in desmoplastic small round cell tumors

Author

Gaylor Boulay, Liliane C. Broye, Rui Dong, Sowmya Iyer, Rajendran Sanalkumar, Yu-Hang Xing, Rémi Buisson, Shruthi Rengarajan, Beverly Naigles, Benoît Duc, Angela Volorio, Mary E. Awad, Raffaele Renella, Ivan Chebib, G. Petur Nielsen, Edwin Choy, Gregory M. Cote, Lee Zou, Igor Letovanec, Ivan Stamenkovic, Miguel N. Rivera, and Nicolò Riggi

Subjects
Science
Abstract

Abstract EWS fusion oncoproteins underlie several human malignancies including Desmoplastic Small Round Cell Tumor (DSRCT), an aggressive cancer driven by EWS-WT1 fusion proteins. Here we combine chromatin occupancy and 3D profiles to identify EWS-WT1-dependent gene regulation networks and target genes. We show that EWS-WT1 is a powerful chromatin activator controlling an oncogenic gene expression program that characterizes primary tumors. Similar to wild type WT1, EWS-WT1 has two isoforms that differ in their DNA binding domain and we find that they have distinct DNA binding profiles and are both required to generate viable tumors that resemble primary DSRCT. Finally, we identify candidate EWS-WT1 target genes with potential therapeutic implications, including CCND1, whose inhibition by the clinically-approved drug Palbociclib leads to marked tumor burden decrease in DSRCT PDXs in vivo. Taken together, our studies identify gene regulation programs and therapeutic vulnerabilities in DSRCT and provide a mechanistic understanding of the complex oncogenic activity of EWS-WT1.

Published
2024
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31. Ewing’s Sarcoma

Author

Nicolo Riggi, Ivan Stamenkovic, and Mario L. Suvà

Subjects
Oncology, medicine.medical_specialty, business.industry, Soft tissue, Ewing's sarcoma, Aggressive cancer, General Medicine, 030204 cardiovascular system & hematology, medicine.disease, Sarcoma ewing, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, 030212 general & internal medicine, Sarcoma, business
Abstract

Ewing’s Sarcoma Ewing’s sarcoma, an aggressive cancer of bone and soft tissue, primarily affects children and young adults. A t(11;22) translocation is noted in 85 to 90% of cases. Management inclu...

Published
2021
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32. TLX3 regulates CGN progenitor proliferation during cerebellum development and its dysfunction can lead to autism

Author

Surendran Parvathy, Budhaditya Basu, Suresh Surya, Rahul Jose, Vadakkath Meera, Paul Ann Riya, Nair Pradeep Jyothi, Rajendran Sanalkumar, Viviane Praz, Nicolò Riggi, Biju Surendran Nair, Kamalesh K. Gulia, Mukesh Kumar, Balachandran Krishnamma Binukumar, and Jackson James

Subjects
Neuroscience, Molecular Neuroscience, Cellular Neuroscience, Omics, Transcriptomics, Science
Abstract

Summary: Tlx3, a master regulator of the fate specification of excitatory neurons, is primarily known to function in post-mitotic cells. Although we have previously identified TLX3 expression in the proliferating granule neuron progenitors (GNPs) of cerebellum, its primary role is unknown. Here, we demonstrate that the dysfunction of Tlx3 from the GNPs significantly reduced its proliferation through regulating anti-proliferative genes. Consequently, the altered generation of GNPs resulted in cerebellar hypoplasia, patterning defects, granule neuron-Purkinje ratio imbalance, and aberrant synaptic connections in the cerebellum. This altered cerebellar homeostasis manifested into a typical autism-like behavior in mice with motor, and social function disabilities. We also show the presence of TLX3 variants with uncharacterized mutations in human cases of autism spectrum disorder (ASD). Altogether, our study establishes Tlx3 as a critical gene involved in developing GNPs and that its deletion from the early developmental stage culminates in autism.

Published
2024
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33. β-Catenin Expression and Activation in Conjunctival Melanoma

Author

Michael Nicolas, Emerentienne Larivé, Alexandre Moulin, Gürkan Kaya, and Nicolo Riggi

Subjects
ddc:616, Melanogenesis, Conjunctiva, business.industry, Melanoma, Wnt signaling pathway, lcsh:RL1-803, Eye, medicine.disease, medicine.anatomical_structure, Tumor progression, Catenin, embryonic structures, lcsh:Dermatology, medicine, Cancer research, Immunohistochemistry, Wound healing, business, neoplasms, Conjunctival Melanoma, Research Article
Abstract

To assess the role of the canonical Wnt pathway via activation of β-catenin in tumor progression of conjunctival melanoma. β-Catenin localization was assessed by immunohistochemistry in 43 conjunctival nevi, 48 primary acquired melanoses (PAM, conjunctival melanocytic intraepithelial neoplasia), and 44 conjunctival melanomas. Activation of the canonical or the noncanonical Wnt pathway was tested in vitro in 4 conjunctival melanoma cell lines with stimulation of either Wnt5a or Wnt3a. Wound healing assays were performed with Wnt5a. Nuclear β-catenin expression was found in 16% of the nevi, in 15% of the melanomas, and in 4% of the PAM. Membranous β-catenin expression was identified in all the nevi and PAM and in 97.7% of the melanomas. In vitro, Wnt5a stimulation in the 4 conjunctival melanomas and in 1 skin melanoma cell line did not induce nuclear translocation of β-catenin, nor did it increase cell motility in the wound healing assays. Wnt3a stimulation did not induce nuclear localization of β-catenin in any of the cell lines tested. In conjunctival melanoma, nuclear localization and activation of β-catenin appear to be limited, suggesting that inhibition of ARF6, responsible for β-catenin activation, in subsets of skin melanoma may not represent a treatment option for this tumor. In vitro, Wnt3a or Wnt5a did not induce nuclear β-catenin localization.

Published
2019
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34. 5-Hydroxymethylcytosine Loss in Conjunctival Melanoma

Author

Katya Nardou, Alexandre Moulin, Michael Nicolas, Nicolo Riggi, Gürkan Kaya, and Alexandre Stahl

Subjects
0301 basic medicine, Pathology, medicine.medical_specialty, IDH1, Lymphovascular invasion, 5-hydroxymethylcytosine, 5-methylcytosine, TET2, conjunctival melanoma, epigenetics, Dermatology, ddc:616.07, Article, 03 medical and health sciences, 0302 clinical medicine, medicine, Nevus, neoplasms, ddc:616, business.industry, medicine.disease, 030104 developmental biology, Conjunctival Nevus, 030220 oncology & carcinogenesis, RL1-803, Cutaneous melanoma, Immunohistochemistry, Differential diagnosis, business, Conjunctival Melanoma
Abstract

Aims: Conjunctival and cutaneous melanoma partially share similar clinical and molecular backgrounds. As 5-hydroxymethylcytosine (5-hmC) loss has been demonstrated in cutaneous melanoma, we decided to assess if similar changes were occurring in conjunctival melanoma. Methods: 5-methylcytosine (5-mC), 5-hmC and TET2 were respectively identified by immunohistochemistry and RNA ISH in 40 conjunctival nevi and 37 conjunctival melanomas. Clinicopathological correlations were established. Results: 5-mC, TET2 and 5-hmC were respectively identified in 67.5%, 95% and 100% of conjunctival nevi and in 81.1%, 35.1% and 54% of conjunctival melanomas. A significant 5-hmC and TET2 loss was identified in conjunctival melanoma comparing to nevus, as well as a significant correlation between TET2 and 5-hmC expression. In the melanomas, 5-hmC expression was only significantly associated with local lymphatic invasion, but not with other clinicopathological parameters. There was a correlation between TET2 expression and the localization of the tumors. 5-mC expression was not associated with any clinicopathological parameters. Conclusions: We identified a significant 5-hmC loss in conjunctival melanoma similar to cutaneous melanoma. This loss may possibly be attributed to TET2 loss or IDH1 mutations. 5-hmC loss in conjunctival melanoma may help in the differential diagnosis between atypical conjunctival nevus and conjunctival melanoma.

Published
2021
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35. TWIST1 expression is associated with high-risk Neuroblastoma and promotes Primary and Metastatic Tumor Growth

Author

Katia Balmas Bourloud, Nardou-Auderset K, Nicolas Jauquier, Nicolo Riggi, Annick Mühlethaler-Mottet, Jean-Marc Joseph, Sepporta M, Sartelet H, Praz, Petit A, Raffaele Renella, and Jean-Yves Scoazec

Subjects
Extracellular matrix, Crosstalk (biology), animal structures, Neuroblastoma, Cancer research, medicine, CRISPR, Cancer, Biology, medicine.disease, Embryonic stem cell, Transcription factor, Metastasis
Abstract

The embryonic transcription factors TWIST1/2 are frequently overexpressed in cancer, acting as multifunctional oncogenes. Here we investigate their role in neuroblastoma (NB), a heterogeneous childhood malignancy ranging from spontaneous regression to dismal outcomes despite multimodal therapy. We first reveal the association of TWIST1 expression with poor survival and metastasis in primary NB, while TWIST2 correlates with good prognosis. Secondly, suppression of TWIST1 by CRISPR/Cas9 results in a reduction of tumor growth and metastasis colonization in immunocompromised mice. Moreover, TWIST1 knockout tumors display a less aggressive cellular morphology and a reduced disruption of the extracellular matrix (ECM) reticulin network. Additionally, we identify a TWIST1-mediated transcriptional program associated with dismal outcome in NB and involved in the control of pathways mainly linked to the signaling, migration, adhesion, the organization of the ECM, and the tumor cells versus tumor stroma crosstalk. Taken together, our findings suggest TWIST1 as novel therapeutic target in NB.

Published
2021
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36. Genomic and transcriptomic landscape of conjunctival melanoma

Author

Rosanna Pescini-Gobert, Beryl Royer-Bertrand, Ikram El Zaoui, Leonidas Zografos, Serge Leyvraz, Nicolo Riggi, Carlo Rivolta, Alexandre Moulin, Marc Folcher, Michael Nicolas, Katarina Cisarova, Virginie G. Peter, Donata Rimoldi, and Ann Schalenbourg

Subjects
Male, Cancer Research, Skin Neoplasms, Somatic cell, Gene Expression, QH426-470, medicine.disease_cause, Cell Line, Tumor, Conjunctival Neoplasms/genetics, Conjunctival Neoplasms/metabolism, DNA Copy Number Variations, Female, Humans, Melanoma/genetics, Melanoma/metabolism, Middle Aged, Mutation, Neurofibromin 1/genetics, Proto-Oncogene Proteins B-raf/genetics, Transcriptome, ras Proteins/genetics, 0302 clinical medicine, Basic Cancer Research, Medicine and Health Sciences, Skin Tumors, Melanoma, Genetics (clinical), 0303 health sciences, Neurofibromin 1, Genomics, Oncology, 030220 oncology & carcinogenesis, Cutaneous Melanoma, Transcriptome Analysis, Research Article, Proto-Oncogene Proteins B-raf, Malignant Skin Neoplasms, Conjunctival Neoplasms, Dermatology, Biology, 03 medical and health sciences, Germline mutation, Malignant Tumors, Cancer Genomics, Genomic Medicine, medicine, Genetics, Molecular Biology, Gene, Ecology, Evolution, Behavior and Systematics, 030304 developmental biology, Cancers and Neoplasms, Biology and Life Sciences, Computational Biology, Genome Analysis, Cutaneous melanoma, Cancer research, ras Proteins, Somatic Mutation, Carcinogenesis, Conjunctival Melanoma
Abstract

Conjunctival melanoma (CJM) is a rare but potentially lethal and highly-recurrent cancer of the eye. Similar to cutaneous melanoma (CM), it originates from melanocytes. Unlike CM, however, CJM is relatively poorly characterized from a genomic point of view. To fill this knowledge gap and gain insight into the genomic nature of CJM, we performed whole-exome (WES) or whole-genome sequencing (WGS) of tumor-normal tissue pairs in 14 affected individuals, as well as RNA sequencing in a subset of 11 tumor tissues. Our results show that, similarly to CM, CJM is also characterized by a very high mutation load, composed of approximately 500 somatic mutations in exonic regions. This, as well as the presence of a UV light-induced mutational signature, are clear signs of the role of sunlight in CJM tumorigenesis. In addition, the genomic classification of CM proposed by TCGA seems to be well-applicable to CJM, with the presence of four typical subclasses defined on the basis of the most frequently mutated genes: BRAF, NF1, RAS, and triple wild-type. In line with these results, transcriptomic analyses revealed similarities with CM as well, namely the presence of a transcriptomic subtype enriched for immune genes and a subtype enriched for genes associated with keratins and epithelial functions. Finally, in seven tumors we detected somatic mutations in ACSS3, a possible new candidate oncogene. Transfected conjunctival melanoma cells overexpressing mutant ACSS3 showed higher proliferative activity, supporting the direct involvement of this gene in the tumorigenesis of CJM. Altogether, our results provide the first unbiased and complete genomic and transcriptomic classification of CJM., Author summary Conjunctival melanoma is an extremely rare form of cancer of the eye that arises from melanocytes–the cells producing the protective pigment melanin–in the outmost layer of the eye: the conjunctiva. This tissue, similarly to the skin, can also be exposed to UV light radiation from the sun. We investigated the genetic background of this rare form of cancer in samples from fourteen patients, by global DNA and RNA sequencing. Our results showed that conjunctival melanoma is genetically very similar to cutaneous melanoma. More precisely, in tumor DNA we detected signs of damage caused by UV light, as well as mutations in the genes BRAF, NF1 and NRAS/HRAS, previously described to be involved in cutaneous melanoma. Analysis of tumor gene expression also revealed similarities between these two types of cancer, some of which could be used as prognostic factors or as indicators of a patients’ response to therapy. In addition, we identified frequent somatic mutations in ACSS3, a gene not yet associated with either conjunctival or cutaneous melanoma, which represents a potential key player in oncogenesis of conjunctival melanoma.

Published
2020

37. A live single-cell reporter assay links intratumor heterogeneity to metastatic proclivity in Ewing sarcoma

Author

Raffaele Renella, Tugba Keskin, Mario L. Suvà, Manuel Diezi, Stéphane Cherix, Liliane C. Broye, Igor Letovanec, Stefano La Rosa, Paolo Provero, Ivan Stamenkovic, Elizabeth M. Perez, Beatrice Rucci, Patricia Martin, Carlo Fusco, Sandrine Cornaz-Buros, Nicolo Riggi, and Katarina Cisarova

Subjects
0301 basic medicine, Reporter gene, Multidisciplinary, Cell, Biology, medicine.disease, Phenotype, Metastasis, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, 030220 oncology & carcinogenesis, microRNA, Gene expression, medicine, Cancer research, Sarcoma, Receptor
Abstract

Targeting of the most aggressive tumor cell subpopulations is key for effective management of most solid malignancies. However, the metastable nature of tumor heterogeneity, which allows cells to transition between strong and weak tumorigenic phenotypes, and the lack of reliable markers of tumor-promoting properties hamper identification of the most relevant cells. To overcome these obstacles, we designed a functional microRNA (miR)-based live-cell reporter assay to identify highly tumorigenic cells in xenotransplants of primary Ewing sarcoma (EwS) 3D cultures. Leveraging the inverse relationship between cell pluripotency and miR-145 expression, we successfully separated highly tumorigenic, metastasis-prone (miR-145 low ) cells from poorly tumorigenic, nonmetastatic (miR-145 high ) counterparts. Gene expression and functional studies of the two cell populations identified the EPHB2 receptor as a prognostic biomarker in patients with EwS and a major promoter of metastasis. Our study provides a simple and powerful means to identify and isolate tumor cells that display aggressive behavior.

Published
2020

38. Nongenetic Evolution Drives Lung Adenocarcinoma Spatial Heterogeneity and Progression

Author

Marco Mina, Solange Peters, Elie Dheilly, David Gfeller, Thorsten Krueger, Aaron S. Petruzzella, Giovanni Ciriello, Jessica Sordet-Dessimoz, Igor Letovanec, Nicolo Riggi, Daniele Tavernari, Elisa Oricchio, and Elena Battistello

Subjects
0301 basic medicine, Lung Neoplasms, early-stage, Context (language use), Adenocarcinoma of Lung, Adenocarcinoma of Lung/genetics, Disease Progression, Genetic Heterogeneity, Humans, Lung Neoplasms/genetics, Tumor Microenvironment, Biology, open-label, 03 medical and health sciences, bioconductor package, 0302 clinical medicine, Immune system, tumor-suppressor gene, expression, medicine, cancer, mouse models, Epigenetics, Lung, medicine.disease, never smokers, 3. Good health, Spatial heterogeneity, 030104 developmental biology, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, Adenocarcinoma, somatic mutations, immunotherapy, Reprogramming
Abstract

Cancer evolution determines molecular and morphologic intratumor heterogeneity and challenges the design of effective treatments. In lung adenocarcinoma, disease progression and prognosis are associated with the appearance of morphologically diverse tumor regions, termed histologic patterns. However, the link between molecular and histologic features remains elusive. Here, we generated multiomics and spatially resolved molecular profiles of histologic patterns from primary lung adenocarcinoma, which we integrated with molecular data from >2,000 patients. The transition from indolent to aggressive patterns was not driven by genetic alterations but by epigenetic and transcriptional reprogramming reshaping cancer cell identity. A signature quantifying this transition was an independent predictor of patient prognosis in multiple human cohorts. Within individual tumors, highly multiplexed protein spatial profiling revealed coexistence of immune desert, inflamed, and excluded regions, which matched histologic pattern composition. Our results provide a detailed molecular map of lung adenocarcinoma intratumor spatial heterogeneity, tracing nongenetic routes of cancer evolution., SIGNIFICANCE: Lung adenocarcinomas are classified based on histologic pattern prevalence. However, individual tumors exhibit multiple patterns with unknown molecular features. We characterized nongenetic mechanisms underlying intratumor patterns and molecular markers predicting patient prognosis. Intratumor patterns determined diverse immune microenvironments, warranting their study in the context of current immunotherapies.

Published
2020

39. Preclinical Evaluation and Dosimetry of [111In]CHX-DTPA-scFv78-Fc Targeting Endosialin/Tumor Endothelial Marker 1 (TEM1)

Author

Gopinadh Jakka, Silvano Gnesin, Francesco Cicone, David Viertl, Nicolo Riggi, Niklaus Schaefer, Melita Irving, Thibaut Denoël, George Coukos, and John O. Prior

Subjects
Cancer Research, Biodistribution, Internal dosimetry, medicine.drug_class, Radioimmunoconjugate, TEM1, Radiolabeled scFv78-Fc, Molecular imaging, Monoclonal antibody, Endosialin, CD248, Dose extrapolation, Ewing’s sarcoma, Neuroblastoma, 03 medical and health sciences, 0302 clinical medicine, In vivo, medicine, Dosimetry, Radiology, Nuclear Medicine and imaging, 030304 developmental biology, 0303 health sciences, Chemistry, medicine.disease, Oncology, 030220 oncology & carcinogenesis, Cancer research, Research Article
Abstract

PurposeEndosialin/tumor endothelial marker-1 (TEM1) is an attractive theranostic target expressed by the microenvironment of a wide range of tumors, as well as by sarcoma and neuroblastoma cells. We report on the radiolabeling and preclinical evaluation of the scFv78-Fc, a fully human TEM1-targeting antibody fragment cross-reactive with mouse TEM1.ProceduresThe scFv78-Fc was conjugated with the chelatorp-SCN-Bn-CHX-A”-DTPA, followed by labeling with indium-111. The number of chelators per molecule was estimated by mass spectrometry. A conventional saturation assay, extrapolated to infinite antigen concentration, was used to determine the immunoreactive fraction of the radioimmunoconjugate. The radiopharmaceutical biodistribution was assessed in immunodeficient mice grafted with Ewing’s sarcoma RD-ES and neuroblastoma SK-N-AS human TEM1-positive tumors. The full biodistribution studies were preceded by a dose-escalation experiment based on the simultaneous administration of the radiopharmaceutical with increasing amounts of unlabeled scFv78-Fc. Radiation dosimetry extrapolations to human adults were obtained from mouse biodistribution data according to established methodologies and additional assumptions concerning the impact of the tumor antigenic sink in the cross-species translation.Results[111In]CHX-DTPA-scFv78-Fc was obtained with a radiochemical purity > 98 % after 1 h incubation at 42 °C and ultrafiltration. It showed good stability in human serum and > 70 % immunoreactive fraction. Biodistribution data acquired in tumor-bearing mice confirmed fast blood clearance and specific tumor targeting in both xenograft models. The radiopharmaceutical off-target uptake was predominantly abdominal. After a theoretical injection of [111In]CHX-DTPA-scFv78-Fc to the reference person, the organs receiving the highest absorbed dose would be the spleen (0.876 mGy/MBq), the liver (0.570 mGy/MBq) and the kidneys (0.298 mGy/MBq). The total body dose and the effective dose would be 0.058 mGy/MBq and 0.116 mSv/MBq, respectively.Conclusions[111In]CHX-DTPA-scFv78-Fc binds specifically to endosialin/TEM1in vitroandin vivo. Dosimetry estimates are in the range of other monoclonal antibodies radiolabeled with indium-111. [111In]CHX-DTPA-scFv78-Fc could be potentially translated into clinic.

Published
2020

40. LIN28B Underlies the Pathogenesis of a Subclass of Ewing Sarcoma

Author

Arnaud Bakaric, Nicolo Riggi, Angel M. Carcaboso, Sandrine Cornaz-Buros, Igor Letovanec, Carlo Fusco, Ivan Chebib, Patricia Waszyk, Jaume Mora, Raffaele Renella, Petur Nielsen, Angela Volorio, Edwin Choy, Gaylor Boulay, Gregory M. Cote, Sowmya Iyer, Antonia Digklia, Ivan Stamenkovic, Anupriya S. Kulkarni, Thibaud Geiser, Michael Montemurro, Tugba Keskin, Matteo Torsello, Stéphane Cherix, Paolo Provero, Miguel Rivera, Patricia Martin, Nadja Chevalier, and Mario L. Suvà

Subjects
0301 basic medicine, Messenger RNA, Poor prognosis, Cell, Biology, medicine.disease, Fusion protein, General Biochemistry, Genetics and Molecular Biology, Subclass, Pathogenesis, 03 medical and health sciences, Ews fli1, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, Cancer research, medicine, Sarcoma, 030217 neurology & neurosurgery
Abstract

Ewing sarcoma (EwS) is associated with poor prognosis despite current multimodal therapy. Targeting of EWS-FLI1, the fusion protein responsible for its pathogenesis, and its principal downstream targets has not yet produced satisfactory therapeutic options, fueling the search for alternative approaches. Here, we show that the oncofetal RNA-binding protein LIN28B regulates the stability of EWS-FLI1 mRNA in ~10% of EwSs. LIN28B depletion in these tumors leads to a decrease in the expression of EWS-FLI1 and its direct transcriptional network, abrogating EwS cell self-renewal and tumorigenicity. Moreover, pharmacological inhibition of LIN28B mimics the effect of LIN28B depletion, suggesting that LIN28B sustains the emergence of a subset of EwS in which it also serves as an effective therapeutic target.

Published
2020

41. Preclinical Evaluation and Dosimetry of [

Author

Francesco, Cicone, Thibaut, Denoël, Silvano, Gnesin, Nicolo, Riggi, Melita, Irving, Gopinadh, Jakka, Niklaus, Schaefer, David, Viertl, George, Coukos, and John O, Prior

Subjects
Tomography, Emission-Computed, Single-Photon, Mice, Inbred BALB C, Indium Radioisotopes, Correction, Antibodies, Neoplasm Proteins, Disease Models, Animal, Antigens, CD, Cell Line, Tumor, Animals, Humans, Female, Tissue Distribution, Radiopharmaceuticals, Radiometry, Tomography, X-Ray Computed
Abstract

Endosialin/tumor endothelial marker-1 (TEM1) is an attractive theranostic target expressed by the microenvironment of a wide range of tumors, as well as by sarcoma and neuroblastoma cells. We report on the radiolabeling and preclinical evaluation of the scFv78-Fc, a fully human TEM1-targeting antibody fragment cross-reactive with mouse TEM1.The scFv78-Fc was conjugated with the chelator p-SCN-Bn-CHX-A"-DTPA, followed by labeling with indium-111. The number of chelators per molecule was estimated by mass spectrometry. A conventional saturation assay, extrapolated to infinite antigen concentration, was used to determine the immunoreactive fraction of the radioimmunoconjugate. The radiopharmaceutical biodistribution was assessed in immunodeficient mice grafted with Ewing's sarcoma RD-ES and neuroblastoma SK-N-AS human TEM1-positive tumors. The full biodistribution studies were preceded by a dose-escalation experiment based on the simultaneous administration of the radiopharmaceutical with increasing amounts of unlabeled scFv78-Fc. Radiation dosimetry extrapolations to human adults were obtained from mouse biodistribution data according to established methodologies and additional assumptions concerning the impact of the tumor antigenic sink in the cross-species translation.[[

Published
2020

42. Inhibition of haspin kinase promotes cell-intrinsic and extrinsic antitumor activity

Author

Steven Rodriguez, Alexander Spektor, Caitlin E. Mills, Derrick Deming, Nienke Moret, Johannes C. Melms, Adam N.R. Cartwright, Patricia Waszyk, Kai W. Wucherpfennig, Clarence Yapp, Peter K. Sorger, Eugenio Morelli, Benjamin Izar, Meri Rogava, David Miller, Sreeram Vallabhaneni, Shaolin Mei, Nicolo Riggi, Jia-Yun Chen, Adrienne M. Luoma, Dirk Schadendorf, Kartik Subramanian, Sushil Kumar, and Titus J. Brinker

Subjects
0301 basic medicine, Cancer Research, Indoles, Skin Neoplasms, Cell, Medizin, CD8-Positive T-Lymphocytes, Protein Serine-Threonine Kinases, Biology, Article, Mice, 03 medical and health sciences, Lymphocytes, Tumor-Infiltrating, 0302 clinical medicine, Immune system, In vivo, Interferon, Cell Line, Tumor, Tumor Microenvironment, medicine, Animals, Humans, Melanoma, Protein Kinase Inhibitors, Mitogen-Activated Protein Kinase Kinases, Kinase, Intracellular Signaling Peptides and Proteins, Azepines, medicine.disease, Xenograft Model Antitumor Assays, 030104 developmental biology, medicine.anatomical_structure, Oncology, Drug Resistance, Neoplasm, Cell culture, Gene Knockdown Techniques, 030220 oncology & carcinogenesis, Interferon Type I, Cancer research, Female, raf Kinases, CD8, medicine.drug
Abstract

Patients with melanoma resistant to RAF/MEK inhibitors (RMi) are frequently resistant to other therapies, such as immune checkpoint inhibitors (ICI), and individuals succumb to their disease. New drugs that control tumor growth and favorably modulate the immune environment are therefore needed. We report that the small-molecule CX-6258 has potent activity against both RMi-sensitive (RMS) and -resistant (RMR) melanoma cell lines. Haspin kinase (HASPIN) was identified as a target of CX-6258. HASPIN inhibition resulted in reduced proliferation, frequent formation of micronuclei, recruitment of cGAS, and activation of the cyclic GMP-AMP synthase (cGAS)–stimulator of interferon genes (STING) pathway. In murine models, CX-6258 induced a potent cGAS-dependent type-I IFN response in tumor cells, increased IFNγ-producing CD8+ T cells, and reduced Treg frequency in vivo. HASPIN was more strongly expressed in malignant compared with healthy tissue and its inhibition by CX-6258 had minimal toxicity in ex vivo–expanded human tumor-infiltrating lymphocytes (TIL), proliferating TILs, and in vitro differentiated neurons, suggesting a potential therapeutic index for anticancer therapy. Furthermore, the activity of CX-6258 was validated in several Ewing sarcoma and multiple myeloma cell lines. Thus, HASPIN inhibition may overcome drug resistance in melanoma, modulate the immune environment, and target a vulnerability in different cancer lineages. Significance: HASPIN inhibition by CX-6258 is a novel and potent strategy for RAF/MEK inhibitor–resistant melanoma and potentially other tumor types. HASPIN inhibition has direct antitumor activity and induces a favorable immune microenvironment.

Published
2020

43. Identification of New Vulnerabilities in Conjunctival Melanoma Using Image-Based High Content Drug Screening

Author

Katya Nardou, Michael Nicolas, Fabien Kuttler, Katarina Cisarova, Elifnaz Celik, Mathieu Quinodoz, Nicolo Riggi, Olivier Michielin, Carlo Rivolta, Gerardo Turcatti, and Alexandre Pierre Moulin

Subjects
polo-like kinase, cyclin dependent kinase, Cancer Research, nras mutations, volasertib bi 6727, kinase 1, conjunctival melanoma, drug screening, kinase inhibitors, MAPK pathway, PI3K/mTOR pathway, aurora-kinase, Hsp90, Tirbanibulin, inhibitor dinaciclib mk-7965, dose-escalation, hsp90, mapk pathway, Oncology, antitumor-activity, mek inhibitor, 1st-in-human phase-i, pi3k, mtor pathway, tirbanibulin, braf
Abstract

Simple Summary We determined the sensitivity of several conjunctival melanoma cell lines to kinase inhibitors as well as a few other inhibitors using an image-based high throughput drug screening assay with 542 compounds. All cell lines demonstrated sensitivity to cell cycle inhibition, especially with polo-like inhibitors. The response to MAPK pathway inhibition was better in the presence of BRAF(V600E) mutations, while the response to PI3k/mTOR inhibition was better in the presence of the NRAS(Q61L) mutation. Our study uncovers a large panel of new vulnerabilities in conjunctival melanoma and establishes the background for the expansion of therapeutic options in the management of this tumor. Recent evidence suggests that numerous similarities exist between the genomic landscapes of both conjunctival and cutaneous melanoma. Since alterations of several components of the MAP kinases, PI3K/mTOR, and cell cycle pathways have been reported in conjunctival melanoma, we decided to assess the sensitivity of conjunctival melanoma to targeted inhibition mostly of kinase inhibitors. A high content drug screening assay based on automated fluorescence microscopy was performed in three conjunctival melanoma cell lines with different genomic backgrounds with 489 kinase inhibitors and 53 other inhibitors. IC50 and apoptosis induction were respectively assessed for 53 and 48 compounds. The genomic background influenced the response to MAK and PI3K/mTOR inhibition, more specifically cell lines with BRAF (V600E) mutations were more sensitive to BRAF/MEK inhibition, while CRMM2 bearing the NRAS(Q61L) mutation was more sensitive to PI3k/mTOR inhibition. All cell lines demonstrated sensitivity to cell cycle inhibition, being more pronounced in CRMM2, especially with polo-like inhibitors. Our data also revealed new vulnerabilities to Hsp90 and Src inhibition. This study demonstrates that the genomic background partially influences the response to targeted therapy and uncovers a large panel of potential vulnerabilities in conjunctival melanoma that may expand available options for the management of this tumor.

Published
2022
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44. Necrotic debris and STING exert therapeutically relevant effects on tumor cholesterol homeostasis

Author

Sampath Katakam, Santosh Anand, Patricia Martin, Nicolo Riggi, and Ivan Stamenkovic

Subjects
Health, Toxicology and Mutagenesis, Apoptosis, Plant Science, Biochemistry, Genetics and Molecular Biology (miscellaneous), Necrosis, Cell Line, Tumor, Neoplasms, Spheroids, Cellular, Tumor Cells, Cultured, Alarmins, Homeostasis, Humans, Research Articles, Ecology, Disease Management, Membrane Proteins, Lipid Metabolism, eye diseases, Gene Expression Regulation, Neoplastic, Cholesterol, lipids (amino acids, peptides, and proteins), Disease Susceptibility, Biomarkers, Research Article
Abstract

Necrotic debris and STING affect tumor cell growth by altering cholesterol homeostasis in opposing manner, revealing that modulation of cellular cholesterol load may help control tumor growth., Malignant tumors commonly display necrosis, which invariably triggers an inflammatory response that supports tumor growth. However, the effect on tumor cells of necrotic debris, or damage-associated molecular patterns (DAMPs) released by dying cells is unknown. Here, we addressed the effect of DAMPs on primary Ewing sarcoma (EwS) cells and cell lines grown in 3D (spheroids) and 2D culture. We show that DAMPs promote the growth of EwS spheroids but not 2D cultures and that the underlying mechanism implicates an increase in cholesterol load in spheroids. In contrast, stimulation of the nucleic acid sensor signaling platform STING by its ligand cyclic GMP-AMP decreases the tumor cell cholesterol load and reduces their tumor initiating ability. Overexpression of STING or stimulation with cyclic GMP-AMP opposes the growth stimulatory effect of DAMPs and synergizes with the cholesterol synthesis inhibitor simvastatin to inhibit tumor growth. Our observations show that modulation of cholesterol homeostasis is a major effect of necrotic cell debris and STING and suggest that combining STING agonists with statins may help control tumor growth., Graphical Abstract

Published
2022
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45. Cancer Metastasis: A Reappraisal of Its Underlying Mechanisms and Their Relevance to Treatment

Author

Michel Aguet, Ivan Stamenkovic, and Nicolo Riggi

Subjects
0301 basic medicine, Metastatic cascade, business.industry, Cancer, Cancer metastasis, medicine.disease, Bioinformatics, Primary tumor, Pathology and Forensic Medicine, Metastasis, 03 medical and health sciences, 030104 developmental biology, Neoplasms, Cancer cell, Neoplastic Stem Cells, Humans, Relevance (law), Medicine, Neoplasm Invasiveness, Neoplasm Metastasis, business
Abstract

Metastases are responsible for the vast majority of cancer-related deaths, but, despite intense efforts to understand their underlying mechanisms with the goal of uncovering effective therapeutic targets, treatment of metastatic cancer has progressed minimally. In this review, we examine the biological programs currently proposed to be key drivers of metastasis. On the basis of evidence from a growing body of research, we discuss to what extent the cellular and molecular mechanisms that are suggested to underlie cancer cell dissemination are specific to the metastatic process, as opposed to representing natural primary tumor progression. Our review highlights the contrast between the abundance of insight gained into the events that constitute the metastatic cascade and the paucity of therapeutic options.

Published
2018
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46. Opposing immune and genetic mechanisms shape oncogenic programs in synovial sarcoma

Author

Nikhil Wagle, Peter K. Sorger, Angela Volorio, Christophe H. Georgescu, Nicolo Riggi, Liliane C. Broye, Lan Nguyen, Ivan Chebib, Brian J. Haas, Nathan Mathewson, Johannes C. Melms, Marni E. Shore, Orit Rozenblatt-Rosen, Joseph M. Beechem, Cyril Neftel, Kai W. Wucherpfennig, Ofir Cohen, Jorge E. Buendia-Buendia, Michael Montemurro, Luisa Cironi, Shaolin Mei, Alyssa R. Richman, Igor Letovanec, Miguel Rivera, Mario L. Suvà, Michael S. Cuoco, Hannah R. Weisman, G. Petur Nielsen, Alex B. Haynes, Livnat Jerby-Arnon, Asa Segerstolpe, Cigall Kadoch, Christina C. Luo, John T. Mullen, Gaylor Boulay, Matthew J. McBride, Gregory M. Cote, Aviv Regev, Ravindra Mylvaganam, Benjamin Izar, Stéphane Cherix, Nicole Ortogero, Simon Gritsch, Danny Labes, Ivan Stamenkovic, Malika Sud, Tu Nguyen-Ngoc, Daniel R. Zollinger, Edwin Choy, and Joseph M. Gurski

Subjects
0301 basic medicine, endocrine system, Oncogene Proteins, Fusion, Carcinogenesis, Biology, General Biochemistry, Genetics and Molecular Biology, Article, Histone Deacetylases, Epigenesis, Genetic, 03 medical and health sciences, Sarcoma, Synovial, 0302 clinical medicine, Immune system, Single-cell analysis, Cell Line, Tumor, medicine, Neoplasm, Humans, Molecular Targeted Therapy, RNA-Seq, Immunogenicity, Cyclin-Dependent Kinase 4, General Medicine, Oncogenes, medicine.disease, Synovial sarcoma, Histone Deacetylase Inhibitors, 030104 developmental biology, Cell culture, 030220 oncology & carcinogenesis, Cancer research, biology.protein, Cyclin-dependent kinase 6, Sarcoma, Single-Cell Analysis
Abstract

Synovial sarcoma (SyS) is an aggressive neoplasm driven by the SS18–SSX fusion, and is characterized by low T cell infiltration. Here, we studied the cancer–immune interplay in SyS using an integrative approach that combines single-cell RNA sequencing (scRNA-seq), spatial profiling and genetic and pharmacological perturbations. scRNA-seq of 16,872 cells from 12 human SyS tumors uncovered a malignant subpopulation that marks immune-deprived niches in situ and is predictive of poor clinical outcomes in two independent cohorts. Functional analyses revealed that this malignant cell state is controlled by the SS18–SSX fusion, is repressed by cytokines secreted by macrophages and T cells, and can be synergistically targeted with a combination of HDAC and CDK4/CDK6 inhibitors. This drug combination enhanced malignant-cell immunogenicity in SyS models, leading to induced T cell reactivity and T cell–mediated killing. Our study provides a blueprint for investigating heterogeneity in fusion-driven malignancies and demonstrates an interplay between immune evasion and oncogenic processes that can be co-targeted in SyS and potentially in other malignancies. Single-cell transcriptional profiling of primary human synovial sarcoma tumors suggests that combinatorial treatment with HDAC and CDK4/CDK6 inhibitors could enhance tumor immunogenicity.

Published
2019

47. Opposing immune and genetic forces shape oncogenic programs in synovial sarcoma

Author

Joseph M. Beechem, Zollinger, Ivan Stamenkovic, Alyssa R. Richman, Christophe H. Georgescu, Angela Volorio, Peter K. Sorger, Joseph M. Gurski, Cyril Neftel, HR Weissman, Cuoco, Igor Letovanec, Gaylor Boulay, Nikhil Wagle, Orit Rozenblatt-Rosen, Danny Labes, Mario-Luca Suvà, Edwin Choy, Ivan Chebib, Ben Izar, Miguel Rivera, Christina C. Luo, Matthew J. McBride, Gregory M. Cote, Luisa Cironi, Brian J. Haas, Ofir Cohen, Shaolin Mei, Marni E. Shore, Jorge E. Buendia-Buendia, Aviv Regev, Nicolo Riggi, Livnat Jerby-Arnon, Stéphane Cherix, Cigall Kadoch, Ravindra Mylvaganam, John T. Mullen, Liliane C. Broye, Alex B. Haynes, Jc Melms, Gunnlaugur P. Nielsen, and Lan T. Nguyen

Subjects
0303 health sciences, Tumor microenvironment, Cell, Cell cycle, Biology, medicine.disease, HDAC1, Synovial sarcoma, 3. Good health, 03 medical and health sciences, 0302 clinical medicine, Immune system, medicine.anatomical_structure, Antigen, 030220 oncology & carcinogenesis, medicine, Cancer research, biology.protein, Cyclin-dependent kinase 6, 030304 developmental biology
Abstract

Synovial sarcoma is an aggressive mesenchymal neoplasm, driven by the SS18-SSX fusion, and characterized by immunogenic antigens expression and exceptionally low T cell infiltration levels. To study the cancer-immune interplay in this disease, we profiled 16,872 cells from 12 human synovial sarcoma tumors using single-cell RNA-sequencing (scRNA-Seq). Synovial sarcoma manifests antitumor immunity, high cellular plasticity and a core oncogenic program, which is predictive of low immune levels and poor clinical outcomes. Using genetic and pharmacological perturbations, we demonstrate that the program is controlled by the SS18-SSX driver and repressed by cytokines secreted by macrophages and T cells in the tumor microenvironment. Network modeling predicted that SS18-SSX promotes the program through HDAC1 and CDK6. Indeed, the combination of HDAC and CDK4/6 inhibitors represses the program, induces immunogenic cell states, and selectively targets synovial sarcoma cells. Our study demonstrates that immune evasion, cellular plasticity, and cell cycle are co-regulated and can be co-targeted in synovial sarcoma and potentially in other malignancies.

Published
2019
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48. An integrative model of cellular states, plasticity and genetics for glioblastoma

Author

Daniel P. Cahill, Tracy T. Batchelor, Priscilla K. Brastianos, William T. Curry, Orit Rozenblatt-Rosen, Dennis M. Bonal, John M. DeWitt, Ivan Stamenkovic, Anoop P. Patel, Inder M. Verma, Irene Slavc, Aviv Regev, Ravindra Mylvaganam, René Geyeregger, Mario L. Suvà, Christine M. Hebert, Anat Stemmer-Rachamimov, Julia L. Small, Lisa Mayr, Nicholas Druck, Alexander Kaplan, Simon Gritsch, Sarah Becker, L. Nicolas Gonzalez Castro, David N. Louis, Toshiro Hara, Danielle Dionne, Brian V. Nahed, Rachel L. Servis, Xiaoyang Lan, McKenzie Shaw, Keith L. Ligon, Cyril Neftel, Christopher Rodman, Kristine Pelton, Johannes Gojo, Mariella G. Filbin, Matthew P. Frosch, Esther Rheinbay, Tony Hunter, Michelle Monje, Marni E. Shore, Dana Silverbush, Elizabeth M. Perez, Gilbert J. Rahme, Hiroaki Wakimoto, Jeremy M. Fung, Quang-Dé Nguyen, Itay Tirosh, Maria Martinez-Lage, Julie Laffy, Alyssa R. Richman, Mia Bertalan, Thomas Czech, Christine Haberler, Bradley E. Bernstein, Nicolo Riggi, Bob S. Carter, Massachusetts Institute of Technology. Department of Biology, and Koch Institute for Integrative Cancer Research at MIT

Subjects
Male, Adolescent, Cell Plasticity, Locus (genetics), Computational biology, PDGFRA, Biology, General Biochemistry, Genetics and Molecular Biology, Article, Cohort Studies, 03 medical and health sciences, Genetic Heterogeneity, Mice, 0302 clinical medicine, Single-cell analysis, Mice, Inbred NOD, Cell Line, Tumor, Tumor Microenvironment, Animals, Humans, Cell Lineage, Epigenetics, RNA-Seq, Child, neoplasms, 030304 developmental biology, Aged, 0303 health sciences, Tumor microenvironment, Genetic diversity, Genetic heterogeneity, Brain Neoplasms, Infant, Middle Aged, Mice, Inbred C57BL, Disease Models, Animal, Mutation, Heterografts, Female, Single-Cell Analysis, Glioblastoma, 030217 neurology & neurosurgery
Abstract

Diverse genetic, epigenetic, and developmental programs drive glioblastoma, an incurable and poorly understood tumor, but their precise characterization remains challenging. Here, we use an integrative approach spanning single-cell RNA-sequencing of 28 tumors, bulk genetic and expression analysis of 401 specimens from the The Cancer Genome Atlas (TCGA), functional approaches, and single-cell lineage tracing to derive a unified model of cellular states and genetic diversity in glioblastoma. We find that malignant cells in glioblastoma exist in four main cellular states that recapitulate distinct neural cell types, are influenced by the tumor microenvironment, and exhibit plasticity. The relative frequency of cells in each state varies between glioblastoma samples and is influenced by copy number amplifications of the CDK4, EGFR, and PDGFRA loci and by mutations in the NF1 locus, which each favor a defined state. Our work provides a blueprint for glioblastoma, integrating the malignant cell programs, their plasticity, and their modulation by genetic drivers. Single-cell analyses of glioblastoma samples reveal multiple cellular states, their plasticity and the genetic underpinnings of state proportions in a given tumor., National Cancer Institute (U.S.) (Grants 1U24CA180922, R33CA202820, P30CA14051)

Published
2019

49. Targeting carbonic anhydrase IX improves the anti-cancer efficacy of mTOR inhibitors

Author

Seraina Faes, Tania Santoro, Dipak Datta, Nicolo Riggi, Jean-Christophe Stehle, Catherine Pythoud, Janine Horlbeck, Emilie Uldry, Anne Planche, Nicolas Demartines, Igor Letovanec, and Olivier Dormond

Subjects
0301 basic medicine, Mice, Nude, mTORC1, Small hairpin RNA, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, Animals, Humans, Medicine, Pimonidazole, Carbonic Anhydrase IX, Carbonic Anhydrase Inhibitors, Hypoxia, PI3K/AKT/mTOR pathway, Sirolimus, Antibiotics, Antineoplastic, Tumor hypoxia, rapamycin, business.industry, TOR Serine-Threonine Kinases, CAIX, Drug Synergism, Neoplasms, Experimental, Xenograft Model Antitumor Assays, Acetazolamide, Mice, Inbred C57BL, Treatment Outcome, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Immunology, Cancer cell, mTOR, Cancer research, Female, RNA Interference, Colorectal Neoplasms, business, HT29 Cells, Research Paper, Acetazolamide/pharmacology, Antibiotics, Antineoplastic/pharmacology, Carbonic Anhydrase IX/antagonists & inhibitors, Carbonic Anhydrase IX/genetics, Carbonic Anhydrase IX/metabolism, Carbonic Anhydrase Inhibitors/pharmacology, Colorectal Neoplasms/drug therapy, Colorectal Neoplasms/genetics, Colorectal Neoplasms/metabolism, Neoplasms, Experimental/drug therapy, Neoplasms, Experimental/genetics, Neoplasms, Experimental/metabolism, Sirolimus/pharmacology, TOR Serine-Threonine Kinases/antagonists & inhibitors, TOR Serine-Threonine Kinases/metabolism, acetazolamide, hypoxia, medicine.drug
Abstract

The inhibition of the mechanistic target of rapamycin complex 1 (mTORC1) by chemical inhibitors, such as rapamycin, has demonstrated anti-cancer activity in preclinical and clinical trials. Their efficacy is, however, limited and tumors eventually relapse through resistance formation. In this study, using two different cancer mouse models, we identify tumor hypoxia as a novel mechanism of resistance of cancer cells against mTORC1 inhibitors. Indeed, we show that the activity of mTORC1 is mainly restricted to the non-hypoxic tumor compartment, as evidenced by a mutually exclusive staining pattern of the mTORC1 activity marker pS6 and the hypoxia marker pimonidazole. Consequently, whereas rapamycin reduces cancer cell proliferation in non-hypoxic regions, it has no effect in hypoxic areas, suggesting that cancer cells proliferate independently of mTORC1 under hypoxia. Targeting the hypoxic tumor compartment by knockdown of carbonic anhydrase IX (CAIX) using short hairpin RNA or by chemical inhibition of CAIX with acetazolamide potentiates the anti-cancer activity of rapamycin. Taken together, these data emphasize that hypoxia impairs the anti-cancer efficacy of rapalogs. Therapeutic strategies targeting the hypoxic tumor compartment, such as the inhibition of CAIX, potentiate the efficacy of rapamycin and warrant further clinical evaluation.

Published
2016
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50. Comprehensive Genetic Landscape of Uveal Melanoma by Whole-Genome Sequencing

Author

Serge Leyvraz, Beryl Royer-Bertrand, Laureen Vallat, Leonidas Zografos, Carlo Rivolta, Giovanni Ciriello, Donata Rimoldi, Nicolo Riggi, Rosanna Pescini-Gobert, Ikram El Zaoui, Ann Schalenbourg, Alexandre Moulin, Matteo Torsello, Robert J. Klein, Franck Raynaud, Daniel E. Speiser, Katarina Cisarova, and Michael Nicolas

Subjects
Adult, Male, Uveal Neoplasms, Aged, Aged, 80 and over, Case-Control Studies, DNA Copy Number Variations, Eukaryotic Initiation Factor-1/genetics, Eukaryotic Initiation Factor-1/metabolism, Exons, Female, GTP-Binding Protein alpha Subunits/genetics, GTP-Binding Protein alpha Subunits/metabolism, GTP-Binding Protein alpha Subunits, Gq-G11/genetics, GTP-Binding Protein alpha Subunits, Gq-G11/metabolism, Genome-Wide Association Study, Humans, Melanocytes/pathology, Melanoma/diagnosis, Melanoma/genetics, Membrane Proteins/genetics, Membrane Proteins/metabolism, Middle Aged, Mutation, Phosphoproteins/genetics, Phosphoproteins/metabolism, RNA Splicing Factors/genetics, RNA Splicing Factors/metabolism, Skin Neoplasms, Tumor Suppressor Proteins/genetics, Tumor Suppressor Proteins/metabolism, Tumor Suppressor p53-Binding Protein 1/genetics, Tumor Suppressor p53-Binding Protein 1/metabolism, Ubiquitin Thiolesterase/genetics, Ubiquitin Thiolesterase/metabolism, Ubiquitin-Protein Ligases/genetics, Ubiquitin-Protein Ligases/metabolism, Uveal Neoplasms/diagnosis, Uveal Neoplasms/genetics, 0301 basic medicine, medicine.medical_specialty, Ubiquitin-Protein Ligases, Eukaryotic Initiation Factor-1, Uveal Neoplasm, Biology, medicine.disease_cause, 03 medical and health sciences, Report, Molecular genetics, Genetics, medicine, Melanoma, Genetics (clinical), Whole genome sequencing, GNA11, Tumor Suppressor Proteins, Membrane Proteins, Phosphoproteins, medicine.disease, GTP-Binding Protein alpha Subunits, 3. Good health, 030104 developmental biology, Cutaneous melanoma, GTP-Binding Protein alpha Subunits, Gq-G11, Melanocytes, RNA Splicing Factors, Tumor Suppressor p53-Binding Protein 1, Ubiquitin Thiolesterase, GNAQ
Abstract

Uveal melanoma (UM) is a rare intraocular tumor that, similar to cutaneous melanoma, originates from melanocytes. To gain insights into its genetics, we performed whole-genome sequencing at very deep coverage of tumor-control pairs in 33 samples (24 primary and 9 metastases). Genome-wide, the number of coding mutations was rather low (only 17 variants per tumor on average; range 7–28), thus radically different from cutaneous melanoma, where hundreds of exonic DNA insults are usually detected. Furthermore, no UV light-induced mutational signature was identified. Recurrent coding mutations were found in the known UM drivers GNAQ, GNA11, BAP1, EIF1AX, and SF3B1. Other genes, i.e., TP53BP1, CSMD1, TTC28, DLK2, and KTN1, were also found to harbor somatic mutations in more than one individual, possibly indicating a previously undescribed association with UM pathogenesis. De novo assembly of unmatched reads from non-coding DNA revealed peculiar copy-number variations defining specific UM subtypes, which in turn could be associated with metastatic transformation. Mutational-driven comparison with other tumor types showed that UM is very similar to pediatric tumors, characterized by very few somatic insults and, possibly, important epigenetic changes. Through the analysis of whole-genome sequencing data, our findings shed new light on the molecular genetics of uveal melanoma, delineating it as an atypical tumor of the adult for which somatic events other than mutations in exonic DNA shape its genetic landscape and define its metastatic potential.

Published
2016
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