Your search keyword '"Scotlandi Katia"' showing total 29 results

1. Extraskeletal Ewing Sarcoma of the Extremities and Trunk: A Retrospective Analysis of a Mono-Institutional Series.

Author

Bianchi, Giuseppe, Laginestra, Maria Antonella, Simonetti, Elisa, Ibrahim, Toni, Macrì, Fabiana, Ostetto, Federico, Tuzzato, Gianmarco, Paioli, Anna, Gambarotti, Marco, Cocchi, Stefania, Donati, Davide Maria, Scotlandi, Katia, and Laranga, Roberta

Subjects

SOFT tissue tumors, SARCOMA, EWING'S sarcoma, GENETIC profile, TREATMENT effectiveness

Abstract

Introduction: Extraskeletal Ewing sarcoma (EEwS) is a rare malignant tumor, and current international recommendations indicate systemic and local treatment like bone Ewing sarcoma (BEwS); to the best of our knowledge, very few studies tried to explore the clinical and genetic characteristics of this tumor, and the most appropriate treatment strategy remains uncertain. Methods: We reviewed 35 EEwS cases enrolled at Rizzoli Orthopedic Institute in Bologna, Italy, between 1988–2022. We performed RNA sequencing in 18 Ewing sarcoma cases, including 12 BEwSs and 6 EEwSs. We analyzed overall survival (OS), local relapse-free survival (LRFS), and metastasis-free survival (MFS) and the risk factors associated to survival. Results: Unsupervised hierarchical clustering showed no differences in the transcriptional profile between EEwS and BEwS. Five-year OS was 67% (95% confidence interval [CI]: 47–80), 5-year LRFS was 61% (95% CI: 43–75), and 5-year MFS was 55% (95% CI: 38–70). Recurrent tumors, larger than 8 cm, and elevated lactate dehydrogenase (LDH) serum value resulted to be negative prognostic factors. Conclusions: The finding/detection of a genetic profile that is indistinguishable between EEwS and BEwS confirms the view that the two subgroups belong to the same tumor entity and supports the use of a single therapeutic approach for Ewing sarcoma, regardless of the site of origin. Statistical evaluation showed that size bigger than 8 cm, elevated LDH, and recurrent tumors had a worse prognosis, suggesting a risk-stratification method for identifying patients for specific therapy treatment. However, larger, multicenter, prospective trials are called for to validate our findings. [ABSTRACT FROM AUTHOR]

Published

2024

2. IL-1 Family Members in Bone Sarcomas.

Author

Landuzzi, Lorena, Ruzzi, Francesca, Pellegrini, Evelin, Lollini, Pier-Luigi, Scotlandi, Katia, and Manara, Maria Cristina

Subjects

OSTEOSARCOMA, INTERLEUKIN-1, IMMUNOREGULATION, EWING'S sarcoma, IMMUNE checkpoint proteins, PROGRAMMED cell death 1 receptors

Abstract

IL-1 family members have multiple pleiotropic functions affecting various tissues and cells, including the regulation of the immune response, hematopoietic homeostasis, bone remodeling, neuronal physiology, and synaptic plasticity. Many of these activities are involved in various pathological processes and immunological disorders, including tumor initiation and progression. Indeed, IL-1 family members have been described to contribute to shaping the tumor microenvironment (TME), determining immune evasion and drug resistance, and to sustain tumor aggressiveness and metastasis. This review addresses the role of IL-1 family members in bone sarcomas, particularly the highly metastatic osteosarcoma (OS) and Ewing sarcoma (EWS), and discusses the IL-1-family-related mechanisms that play a role in bone metastasis development. We also consider the therapeutic implications of targeting IL-1 family members, which have been proposed as (i) relevant targets for anti-tumor and anti-metastatic drugs; (ii) immune checkpoints for immune suppression; and (iii) potential antigens for immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2024

3. CD99 Modulates the Proteomic Landscape of Ewing Sarcoma Cells and Related Extracellular Vesicles.

Author

De Feo, Alessandra, Manfredi, Marcello, Mancarella, Caterina, Maqueda, Joaquín J., De Giorgis, Veronica, Pignochino, Ymera, Sciandra, Marika, Cristalli, Camilla, Donadelli, Massimo, and Scotlandi, Katia

Subjects

EWING'S sarcoma, EXTRACELLULAR vesicles, CELL migration, PROTEOMICS, MASS spectrometry, FUNCTIONAL analysis

Abstract

Ewing sarcoma (EWS) is an aggressive pediatric bone tumor characterized by unmet clinical needs and an incompletely understood epigenetic heterogeneity. Here, we considered CD99, a major surface molecule hallmark of EWS malignancy. Fluctuations in CD99 expression strongly impair cell dissemination, differentiation, and death. CD99 is also loaded within extracellular vesicles (EVs), and the delivery of CD99-positive or CD99-negative EVs dynamically exerts oncogenic or oncosuppressive functions to recipient cells, respectively. We undertook mass spectrometry and functional annotation analysis to investigate the consequences of CD99 silencing on the proteomic landscape of EWS cells and related EVs. Our data demonstrate that (i) the decrease in CD99 leads to major changes in the proteomic profile of EWS cells and EVs; (ii) intracellular and extracellular compartments display two distinct signatures of differentially expressed proteins; (iii) proteomic changes converge to the modulation of cell migration and immune-modulation biological processes; and (iv) CD99-silenced cells and related EVs are characterized by a migration-suppressive, pro-immunostimulatory proteomic profile. Overall, our data provide a novel source of CD99-associated protein biomarkers to be considered for further validation as mediators of EWS malignancy and as EWS disease liquid biopsy markers. [ABSTRACT FROM AUTHOR]

Published

2024

4. Prognostic Relevance of CCN3 in Bone Sarcomas

Author

Perbal, Bernard, Lazar, Noureddine, Zambelli, Diana, Zuntini, Monia, Serra, Massimo, Lopez-Guerrero, Jose Antonio, Llombart-Bosch, Antonio, Picci, Piero, Scotlandi, Katia, Perbal, Annick, editor, Takigawa, Masaharu, editor, and Perbal, Bernard, editor

Published

2010

5. EHD1-dependent traffic of IGF-1 receptor to the cell surface is essential for Ewing sarcoma tumorigenesis and metastasis.

Author

Chakraborty, Sukanya, Bhat, Aaqib M., Mushtaq, Insha, Luan, Haitao, Kalluchi, Achyuth, Mirza, Sameer, Storck, Matthew D., Chaturvedi, Nagendra, Lopez-Guerrero, Jose Antonio, Llombart-Bosch, Antonio, Machado, Isidro, Scotlandi, Katia, Meza, Jane L., Ghosal, Gargi, Coulter, Donald W., Jordan Rowley, M., Band, Vimla, Mohapatra, Bhopal C., and Band, Hamid

Subjects

CELL receptors, EWING'S sarcoma, NEOPLASTIC cell transformation, GENE expression, CELL membranes

Abstract

Overexpression of the EPS15 Homology Domain containing 1 (EHD1) protein has been linked to tumorigenesis but whether its core function as a regulator of intracellular traffic of cell surface receptors plays a role in oncogenesis remains unknown. We establish that EHD1 is overexpressed in Ewing sarcoma (EWS), with high EHD1 mRNA expression specifying shorter patient survival. ShRNA-knockdown and CRISPR-knockout with mouse Ehd1 rescue established a requirement of EHD1 for tumorigenesis and metastasis. RTK antibody arrays identified IGF-1R as a target of EHD1 regulation in EWS. Mechanistically, we demonstrate a requirement of EHD1 for endocytic recycling and Golgi to plasma membrane traffic of IGF-1R to maintain its surface expression and downstream signaling. Conversely, EHD1 overexpression-dependent exaggerated oncogenic traits require IGF-1R expression and kinase activity. Our findings define the RTK traffic regulation as a proximal mechanism of EHD1 overexpression-dependent oncogenesis that impinges on IGF-1R in EWS, supporting the potential of IGF-1R and EHD1 co-targeting. EHD1 is overexpressed in Ewing sarcoma and required for metastasis and tumorigenesis while regulating cellular trafficking and plasma membrane expression of IGF-1R. [ABSTRACT FROM AUTHOR]

Published

2023

6. Process development of a human recombinant diabody expressed in E. coli: engagement of CD99-induced apoptosis for target therapy in Ewing’s sarcoma

Author

Moricoli, Diego, Carbonella, Damiano Cosimo, Dominici, Sabrina, Fiori, Valentina, Balducci, Maria Cristina, Guerzoni, Clara, Manara, Maria Cristina, Pasello, Michela, Laguardia, Maria Elena, Cianfriglia, Maurizio, Scotlandi, Katia, and Magnani, Mauro

Published

2016

7. ABCA6 affects the malignancy of Ewing sarcoma cells via cholesterol-guided inhibition of the IGF1R/AKT/MDM2 axis.

Author

Pasello, Michela, Giudice, Anna Maria, Cristalli, Camilla, Manara, Maria Cristina, Mancarella, Caterina, Parra, Alessandro, Serra, Massimo, Magagnoli, Giovanna, Cidre-Aranaz, Florencia, Grünewald, Thomas G. P., Bini, Carla, Lollini, Pier-Luigi, Longhi, Alessandra, Donati, Davide Maria, and Scotlandi, Katia

Subjects

EWING'S sarcoma, SUPPRESSOR cells, TREATMENT effectiveness, CELL migration inhibition, CELL migration, CHILDHOOD cancer, ATP-binding cassette transporters

Abstract

Purpose: The relevance of the subfamily A members of ATP-binding cassette (ABCA) transporters as biomarkers of risk and response is emerging in different tumors, but their mechanisms of action have only been partially defined. In this work, we investigated their role in Ewing sarcoma (EWS), a pediatric cancer with unmet clinical issues. Methods: The expression of ABC members was evaluated by RT-qPCR in patients with localized EWS. The correlation with clinical outcome was established in different datasets using univariate and multivariate statistical methods. Functional studies were conducted in cell lines from patient-derived xenografts (PDXs) using gain- or loss-of-function approaches. The impact of intracellular cholesterol levels and cholesterol lowering drugs on malignant parameters was considered. Results: We found that ABCA6, which is usually poorly expressed in EWS, when upregulated became a prognostic factor of a favorable outcome in patients. Mechanistically, high expression of ABCA6 impaired cell migration and increased cell chemosensitivity by diminishing the intracellular levels of cholesterol and by constitutive IGF1R/AKT/mTOR expression/activation. Accordingly, while exposure of cells to exogenous cholesterol increased AKT/mTOR activation, the cholesterol lowering drug simvastatin inhibited IGF1R/AKT/mTOR signaling and prevented Ser166 phosphorylation of MDM2. This, in turn, favored p53 activation and enhanced pro-apoptotic effects of doxorubicin. Conclusions: Our study reveals that ABCA6 acts as tumor suppressor in EWS cells via cholesterol-mediated inhibition of IGF1R/AKT/MDM2 signaling, which promotes the pro-apoptotic effects of doxorubicin and reduces cell migration. Our findings also support a role of ABCA6 as biomarker of EWS progression and sustains its assessment for a more rational use of statins as adjuvant drugs. [ABSTRACT FROM AUTHOR]

Published

2022

8. CIC-Rearranged Sarcomas: An Intriguing Entity That May Lead the Way to the Comprehension of More Common Cancers.

Author

Mancarella, Caterina, Carrabotta, Marianna, Toracchio, Lisa, and Scotlandi, Katia

Subjects

GENETIC mutation, ONCOGENES, NEOPLASTIC cell transformation, SOFT tissue tumors, CELL motility, CELL proliferation, MITOGEN-activated protein kinases, LIPOSARCOMA, EWING'S sarcoma, SYMPTOMS

Abstract

Simple Summary: In this review, we aim to summarize the current clinical and biological knowledge for patients affected by a rare soft-tissue sarcoma, the CIC-rearranged sarcoma, to highlight novel treatment perspectives and to remark the need of innovative clinical trials. CIC-rearranged sarcoma is still entrapped in unspecific therapeutic regimens which result in poor prognosis and high incidence of recurrence. The comprehension of the biology of this tumor and the exact mechanisms of action of its molecular markers are mandatory to identify specific cancer vulnerabilities to exploit for therapy. Clinical research for rare tumors is complicated by the difficulties in patients' recruitment and the lack of interest of Big Pharma in the development of new treatments. An intriguing perspective is given by the identification of CIC and its targets dysregulation as a common determinant of different tumor types, which might fasten the development of effective mechanism-based therapies. Capicua transcriptional repressor (CIC)-rearranged sarcoma, belonging to the undifferentiated round cells sarcoma family, is characterized by high metastatic rate and poor chemo response. CIC sarcoma represents a new entity harboring the recurrent chromosomal translocation between CIC and, in most of the cases, DUX4. CIC-DUX4 imposes a CIC-specific transcriptional signature, which drives cell transformation, proliferation, and migration. While the discovery of the fusion represented the first evidence of a role of CIC in cancer, a complete comprehension of CIC-rearranged activity is still required before providing new potential avenues for therapy. To date, a specific and effective treatment for CIC sarcoma has yet to be defined. In this review, we initially highlight the clinical features and pathogenesis of CIC-rearranged sarcomas along with current therapeutic approaches and then focus on the specific oncogenic mechanisms driven by the CIC-rearrangement. We discuss novel therapeutic options evoked by the aberrant relations of CIC-DUX4 with the IGF system, DUSP6, P300/CBP, and CCNE1. We also discuss how different mutations involving CIC might converge on a common upregulation of CIC-target genes across human cancers. A deeper understanding of the oncogenic mechanisms driven by the chimera CIC-DUX4 might provide novel therapeutic opportunities with a general impact in cancer. [ABSTRACT FROM AUTHOR]

Published

2022

9. Polymorphic variants of IGF2BP3 and SENCR have an impact on predisposition and/or progression of Ewing sarcoma.

Author

Martinelli, Marcella, Mancarella, Caterina, Scapoli, Luca, Palmieri, Annalisa, De Sanctis, Paola, Ferrari, Cristina, Pasello, Michela, Zucchini, Cinzia, and Scotlandi, Katia

Subjects

EWING'S sarcoma, LINCRNA, CARCINOEMBRYONIC antigen, SINGLE nucleotide polymorphisms, GENETIC variation

Abstract

Ewing sarcoma (EWS), the second most common malignant bone tumor in children and adolescents, occurs abruptly without clear evidence of tumor history or progression. Previous association studies have identified some inherited variants associated with the risk of developing EWS but a common picture of the germline susceptibility to this tumor remains largely unclear. Here, we examine the association between thirty single nucleotide polymorphisms (SNPs) of the IGF2BP3, a gene that codes for an oncofetal RNA-binding protein demonstrated to be important for EWS patient's risk stratification, and five SNPs of SENCR, a long non-coding RNA shown to regulate IGF2BP3. An association between polymorphisms and EWS susceptibility was observed for three IGF2BP3 SNPs - rs112316332, rs13242065, rs12700421 - and for four SENCR SNPs - rs10893909, rs11221437, rs12420823, rs4526784 -. In addition, IGF2BP3 rs34033684 and SENCR rs10893909 variants increased the risk for female respect to male subgroup when carried together, while IGF2BP3 rs13242065 or rs76983703 variants reduced the probability of a disease later onset (> 14 years). Moreover, the absence of IGF2BP3 rs10488282 variant and the presence of rs199653 or rs35875486 variant were significantly associated with a worse survival in EWS patients with localized disease at diagnosis. Overall, our data provide the first evidence linking genetic variants of IGF2BP3 and its modulator SENCR to the risk of EWS development and to disease progression, thus supporting the concept that heritable factors can influence susceptibility to EWS and may help to predict patient prognosis. [ABSTRACT FROM AUTHOR]

Published

2022

10. Epithelial cell adhesion molecules and epithelial mesenchymal transition (EMT) markers in Ewing's sarcoma family of tumors (ESFTs). Do they offer any prognostic significance?

Author

Machado, Isidro, López-Guerrero, José A., Navarro, Samuel, Alberghini, Marco, Scotlandi, Katia, Picci, Piero, and Llombart-Bosch, Antonio

Published

2012

11. In Ewing's sarcoma CCN3(NOV) inhibits proliferation while promoting migration and invasion of the same cell type

Author

Benini, Stefania, Perbal, Bernard, Zambelli, Diana, Colombo, Mario Paolo, Manara, Maria Cristina, Serra, Massimo, Parenza, Mariella, Martinez, Vincent, Picci, Piero, and Scotlandi, Katia

Published

2005

12. Molecular mechanisms of CD99-induced caspase-independent cell death and cell–cell adhesion in Ewing's sarcoma cells: actin and zyxin as key intracellular mediators

Author

Cerisano, Vanessa, Aalto, Yan, Perdichizzi, Stefania, Bernard, Ghislaine, Manara, Maria Cristina, Benini, Stefania, Cenacchi, Giovanna, Preda, Paola, Lattanzi, Giovanna, Nagy, Bálint, Knuutila, Sakari, Colombo, Mario Paolo, Bernard, Alain, Picci, Piero, and Scotlandi, Katia

Published

2004

13. Effectiveness of insulin-like growth factor I receptor antisense strategy against Ewing's sarcoma cells

Author

Scotlandi, Katia, Maini, Cecilia, Manara, Maria Cristina, Benini, Stefania, Serra, Massimo, Cerisano, Vanessa, Strammiello, Rosaria, Baldini, Nicola, Lollini, Pier-Luigi, Nanni, Patrizia, Nicoletti, Giordano, and Picci, Piero

Published

2002

14. Novel Targeting of DNA Methyltransferase Activity Inhibits Ewing Sarcoma Cell Proliferation and Enhances Tumor Cell Sensitivity to DNA Damaging Drugs by Activating the DNA Damage Response.

Author

Cristalli, Camilla, Manara, Maria Cristina, Valente, Sergio, Pellegrini, Evelin, Bavelloni, Alberto, De Feo, Alessandra, Blalock, William, Di Bello, Elisabetta, Piñeyro, David, Merkel, Angelika, Esteller, Manel, Tirado, Oscar M., Mai, Antonello, and Scotlandi, Katia

Subjects

DNA damage, EWING'S sarcoma, CELL proliferation, DNA methylation, DNA, DNA methyltransferases, METHYLTRANSFERASES

Abstract

DNA methylation is an important component of the epigenetic machinery that regulates the malignancy of Ewing sarcoma (EWS), the second most common primary bone tumor in children and adolescents. Coordination of DNA methylation and DNA replication is critical for maintaining epigenetic programming and the DNMT1 enzyme has been demonstrated to have an important role in both maintaining the epigenome and controlling cell cycle. Here, we showed that the novel nonnucleoside DNMT inhibitor (DNMTi) MC3343 induces a specific depletion of DNMT1 and affects EWS tumor proliferation through a mechanism that is independent on DNA methylation. Depletion of DNMT1 causes perturbation of the cell cycle, with an accumulation of cells in the G1 phase, and DNA damage, as revealed by the induction of γH2AX foci. These effects elicited activation of p53-dependent signaling and apoptosis in p53wt cells, while in p53 mutated cells, persistent micronuclei and increased DNA instability was observed. Treatment with MC3343 potentiates the efficacy of DNA damaging agents such as doxorubicin and PARP-inhibitors (PARPi). This effect correlates with increased DNA damage and synergistic tumor cytotoxicity, supporting the use of the DNMTi MC3343 as an adjuvant agent in treating EWS. [ABSTRACT FROM AUTHOR]

Published

2022

15. miR-214-3p Is Commonly Downregulated by EWS-FLI1 and by CD99 and Its Restoration Limits Ewing Sarcoma Aggressiveness.

Author

De Feo, Alessandra, Pazzaglia, Laura, Ciuffarin, Lisa, Mangiagli, Fabio, Pasello, Michela, Simonetti, Elisa, Pellegrini, Evelin, Ferrari, Cristina, Bianchi, Giuseppe, Spazzoli, Benedetta, and Scotlandi, Katia

Subjects

CANCER invasiveness, MICRORNA, GENE expression, CELL migration inhibition, CELL lines, EWING'S sarcoma, ANTIGENS, MESENCHYMAL stem cells

Abstract

Simple Summary: Ewing's sarcoma (EWS), the second most frequent primary tumor of bone in the pediatric population, is a very aggressive, undifferentiated mesenchymal malignancy with a high tendency to develop lung and/or bone metastasis. The prognosis of patients with metastasis remains dismal, and new strategies are needed to control the dissemination of EWS cells. EWS is driven by alterations induced by the EWS-FLI1 chimera which acts as an aberrant transcriptional factor that induces the complete reprograming of the gene expression. EWS cells are also characterized by high expression of CD99, a cell surface molecule that interacts with EWS-FLI1 to sustain EWS malignancy. This study shows that miR-214-3p is a common mediator of EWS-FLI1 and CD99, and we report that miR-214-3p acts as on oncosuppressor in EWS. MiR-214-3p is constitutively repressed in cell lines and clinical samples but is re-expressed after the silencing of EWS-FLI1 and/or CD99. The restoration of miR-214-3p limits EWS cell growth and migration and represses the expression of its target HMGA1, supporting the potential role of this miRNA as a marker of tumor aggressiveness. Ewing's sarcoma (EWS), an aggressive pediatric bone and soft-tissue sarcoma, has a very stable genome with very few genetic alterations. Unlike in most cancers, the progression of EWS appears to depend on epigenetic alterations. EWS–FLI1 and CD99, the two hallmarks of EWS, are reported to severely impact the malignancy of EWS cells, at least partly by regulating the expression of several types of non-coding RNAs. Here, we identify miR-214-3p as a common mediator of either EWS-FLI1 or CD99 by in silico analysis. MiR-214-3p expression was lower in EWS cells and in clinical samples than in bone marrow mesenchymal stem cells, and this miRNA was barely expressed in metastatic lesions. Silencing of EWS-FLI1 or CD99 restored the expression of miR-214-3p, leading to a reduced cell growth and migration. Mechanistically, miR-214-3p restoration inhibits the expression of the high-mobility group AT-hook 1 (HMGA1) protein, a validated target of miR-214-3p and a major regulator of the transcriptional machinery. The decrease in HMGA1 expression reduced the growth and the migration of EWS cells. Taken together, our results support that the miR-214-3p is constitutively repressed by both EWS-FLI1 and CD99 because it acts as an oncosuppressor limiting the dissemination of EWS cells. [ABSTRACT FROM AUTHOR]

Published

2022

16. Nuclear shape instability evoked by lamin A deregulation promotes metastases in Ewing sarcoma.

Author

Paganelli, Francesca, Balestra, Tommaso, Capanni, Cristina, Fazio, Antonietta, Romero, Pol Arnau, Manara, Maria Cristina, Landuzzi, Lorena, Petrini, Stefania, Evangelisti, Camilla, Lollini, Pier-Luigi, Martelli, Alberto M., Lattanzi, Giovanna, Scotlandi, Katia, Palumbo, Carla, and Chiarini, Francesca

Subjects

NUCLEAR shapes, EWING'S sarcoma, MEDICAL sciences, METASTASIS, NEUROSCIENCES, NUCLEOCYTOPLASMIC interactions

Abstract

The article presents a study on nuclear shape instability evoked by lamin A deregulation that promotes metastases in ewing sarcoma. Topics include information on Ewing sarcoma (EWS) which is type of bone cancer; presence of metastases at the onset remains the most clinically relevant adverse prognostic factor for EWS; and features of cancer.

Published

2022

17. Correction to: ABCA6 affects the malignancy of Ewing sarcoma cells via cholesterol-guided inhibition of the IGF1R/AKT/MDM2 axis.

Author

Pasello, Michela, Giudice, Anna Maria, Cristalli, Camilla, Manara, Maria Cristina, Mancarella, Caterina, Parra, Alessandro, Serra, Massimo, Magagnoli, Giovanna, Cidre-Aranaz, Florencia, Grünewald, Thomas G. P., Bini, Carla, Lollini, Pier-Luigi, Longhi, Alessandra, Donati, Davide Maria, and Scotlandi, Katia

Subjects

EWING'S sarcoma

Abstract

Publisher's note Springer Nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations. B Correction to: Cellular Oncology b https://doi.org/10.1007/s13402-022-00713-5 In this article an incorrect affiliation had inadvertently been added. [Extracted from the article]

Published

2022

18. Low levels of lamin A and mislocalization of LINC complex proteins are linked to metastatic potential in Ewing sarcoma.

Author

Paganelli, Francesca, Fazio, Antonietta, Balestra, Tommaso, Capanni, Cristina, Manara, Maria Cristina, Petrini, Stefania, Evangelisti, Camilla, Martelli, Alberto M., Lattanzi, Giovanna, Scotlandi, Katia, and Chiarini, Francesca

Subjects

EWING'S sarcoma, NUCLEAR proteins, METASTASIS, PROTEINS, YAP signaling proteins

Abstract

Nuclear morphology abnormalities, loss of nuclear lamina integrity and changes in its constitution are known cancer hallmarks [1]. Alterations in nuclear architecture are mediated by nuclear proteins, such as lamin A/C, the main constituent of nuclear lamina, or LINC complex proteins SUN1, SUN2 and nesprins, which mediate a mechanical link between nucleus and cytoskeleton, determining the overall nuclear structural properties [1]. Lamin alterations may decrease nuclear rigidity, promoting invasiveness or increase protection against mechanical forces, such as interstitial pressure within the tumor [2, 3]. It has been observed that the expression of lamin A can be increased, reduced or absent, depending on the type of cancer. However, changes in lamin A levels are often associated with poor prognosis in multiple human cancers [4]. Here, we reported that low LMNA levels are associated with a worse 5-year OS in Ewing Sarcoma (EWS) patients and correlated with a more metastatic phenotype. To gain mechanistic insights into lamin A-dependent pathways in EWS, a pediatric tumor characterized by a high degree of aggressiveness, we focused on the LINC complex proteins, the major lamin A partners in mechanosignaling transduction [5]. We found that SUN1, SUN2, and nesprin 2 were severely mislocalized, due to a lamin A-dependent mechanism, as forced lamin A expression rescued their nuclear localization and SUN1 expression involved in cytoskeleton remodelling, and directly correlated to EWS invasiveness [6]. While in naïve EWS cells, YAP was recruited to the nucleus, lamin A overexpression reduced its nuclear retention, inhibiting its activity. Lamin A rescue of SUN1 levels/localization was associated with significantly lower ROCK2 levels and reduced motility, in agreement with the critical role played by Rho/ROCK2 pathway in EWS migration [7]. Interestingly, we obtained the same effects treating EWS cells with mevinolin, a statin already employed in clinical practice. Mevinolin treatment caused prelamin A accumulation as expected, but also significantly increased LMNA gene and protein expression, rescuing LINC complex localization and pushing the cells in a more differentiated status. Thus, our findings recognize mevinolin, as a tool capable of reducing invasiveness, while triggering neural differentiation, paving the way to new therapeutic options for this very aggressive cancer. [ABSTRACT FROM AUTHOR]

Published

2021

19. Targeting Glutathione-S transferase enzymes in musculoskeletal sarcomas: a promising therapeutic strategy.

Author

Pasello, Michela, Manara, Maria Cristina, Michelacci, Francesca, Fanelli, Marilù, Hattinger, Claudia Maria, Nicoletti, Giordano, Landuzzi, Lorena, Lollini, Pier Luigi, Caccuri, Annamaria, Picci, Piero, Scotlandi, Katia, and Serra, Massimo

Subjects

GLUTATHIONE transferase, ISOENZYMES, EWING'S sarcoma, RHABDOMYOSARCOMA, DOXORUBICIN, CISPLATIN

Abstract

Recent studies have indicated that targeting glutathione-S-transferase (GST) isoenzymes may be a promising novel strategy to improve the efficacy of conventional chemotherapy in the three most common musculoskeletal tumours: osteosarcoma, Ewing's sarcoma, and rhabdomyosarcoma. By using a panel of 15 drug-sensitive and drug-resistant human osteosarcoma, Ewing's sarcoma, and rhabdomyosarcoma cell lines, the efficay of the GST-targeting agent 6-(7-nitro-2,1,3-benzoxadiazol-4-ylthio)hexanol (NBDHEX) has been assessed and related to GST isoenzymes expression (namely GSTP1, GSTA1, GSTM1, and MGST). NBDHEX showed a relevant in vitro activity on all cell lines, including the drug-resistant ones and those with higher GSTs levels. The in vitro activity of NBDHEX was mostly related to cytostatic effects, with a less evident apoptotic induction. NBDHEX positively interacted with doxorubicin, vincristine, cisplatin but showed antagonistic effects with methotrexate. In vivo studies confirmed the cytostatic efficay of NBDHEX and its positive interaction with vincristine in Ewing's sarcoma cells, and also indicated a positive effect against the metastatisation of osteosarcoma cells. The whole body of evidence found in this study indicated that targeting GSTs in osteosarcoma, Ewing's sarcoma and rhabdomyosarcoma may be an interesting new therapeutic option, which can be considered for patients who are scarcely responsive to conventional regimens. [ABSTRACT FROM AUTHOR]

Published

2011

20. Expression of insulin-like growth factor system components in Ewing’s sarcoma and their association with survival

Author

Scotlandi, Katia, Manara, Maria Cristina, Serra, Massimo, Marino, Maria Teresa, Ventura, Selena, Garofalo, Cecilia, Alberghini, Marco, Magagnoli, Giovanna, Ferrari, Stefano, Lopez-Guerrero, Jose Antonio, Llombard-Bosch, Antonio, and Picci, Piero

Subjects

*ANALYSIS of variance, *CONFIDENCE intervals, *STATISTICAL correlation, *ENZYME-linked immunosorbent assay, *EWING'S sarcoma, *GENE expression, *IMMUNOHISTOCHEMISTRY, *POLYMERASE chain reaction, *PROBABILITY theory, *RNA, *SOMATOMEDIN, *SURVIVAL analysis (Biometry), *T-test (Statistics), *U-statistics, *RELATIVE medical risk, *PROPORTIONAL hazards models, *CHILDREN, *PROGNOSIS

Abstract

Abstract: Aims: The role of IGF system in the pathogenesis of Ewing’s sarcoma (EWS) is well-documented. However, still little information is available about the value of IGF system components as indicators of prognosis. Understanding the clinical role for IGF system in EWS patients may be important because different subtypes of patients have distinct outcome and may require different treatment protocol. We evaluated the expression of insulin-like growth factor (IGF)-receptor (IGF-IR), insulin receptor (IR), IGF-I and some major intracellular mediators (IRS1, p-ERK) in specimens from EWS patients with primary localised untreated tumours. Patients and methods: 290 samples were used for immunohistochemistry studies; 57 samples for Real-Time PCR studies; and serum of 67 patients for ELISA. Results: IGF-IR and IR are expressed in virtually all EWS tumours. Usually both the receptors are present in the same tumour but when one receptor is lacking the other one is always present. Evaluation of IGF-IR, IR and IGF-I with quantitative methods may discriminate differential levels of expression with influences on the patients’ outcome. High expression of IGF-IR, IR and IGF-I mRNAs is significantly associated with more favourable clinical outcomes. Higher circulating levels of IGF-I also correlated with lower risk to disease progression and death. Conclusions: Overall, our clinical data are in contrast with the assumption that higher amounts of IGF/IGF-IR are a surrogate for higher aggressiveness and indicate that in some cancers the transition to frank malignancy and poor treatment responsiveness seem to be associated with a reduction of IGF system activity. [Copyright &y& Elsevier]

Published

2011

21. Prognostic relevance of CCN3 in Ewing sarcoma.

Author

Perbal, Bernard, Lazar, Noureddine, Zambelli, Diana, Lopez-Guerrero, Jose Antonio, Llombart-Bosch, Antonio, Scotlandi, Katia, and Picci, Piero

Subjects

EWING'S sarcoma, MOLECULAR oncology, CANCER prognosis, CHILDHOOD cancer, DISEASES in young adults, CANCER cells, HEALTH outcome assessment, CANCER radiotherapy

Abstract

Summary: Ewing sarcoma is a highly aggressive malignant bone tumor occurring preferentially in children and young adults. At present, only clinical features, such as patient age, presence of clinically evident metastases at diagnosis, and poor response to neoadjuvant chemotherapy, are widely accepted as prognostic indicators in Ewing sarcoma. In this study, we assessed the prognostic value of CCN3 (Nov), a matricellular protein that play crucial roles in bone formation. Polyclonal antibodies directed against each of the different CCN3 modules were used to identify variant CCN3 proteins in tumors and to draw potential relationships between the expression of these variants and the outcome of patients with Ewing sarcoma. Our results confirmed that expression of the full-length CCN3 in Ewing sarcoma is associated to a worse prognostic. Furthermore, we report a possible relationship between the expression of a CCN3 protein lacking an internal module (von Willebrand factor type C) and sensitivity to radiotherapy. We hypothesize that the increased level of variant CCN3 in the tumor cells reduces their tumorigenic potential and results in better outcome. [Copyright &y& Elsevier]

Published

2009

22. Targeting CD99 in association with doxorubicin: An effective combined treatment for Ewing’s sarcoma

Author

Scotlandi, Katia, Perdichizzi, Stefania, Bernard, Ghislaine, Nicoletti, Giordano, Nanni, Patrizia, Lollini, Pier-Luigi, Curti, Antonio, Manara, Maria Cristina, Benini, Stefania, Bernard, Alain, and Picci, Piero

Subjects

*METASTASIS, *IMMUNOGLOBULINS, *CANCER invasiveness, *MONOCLONAL antibodies

Abstract

Abstract: CD99 is a 32kDa surface glycoprotein that is involved in the migration of leukocytes, cell–cell adhesion and apoptosis of T cells and Ewing’s sarcoma (ES) cells, two cell types with a high level of CD99 expression. Engagement of the molecule induces a rapid death signal that appears to be related to the level of expression of this antigen. The rapid apoptosis induced by agonistic anti-CD99 monoclonal antibodies is of clinical interest in ES, a tumour for which no new drugs have been described as clearly effective in the last 10 years. In this study, we show that an anti-CD99 monoclonal antibody can be used to advantage in association with doxorubicin. Striking effectiveness was observed against local tumours and metastases. No remarkably toxic effects of anti-CD99 monoclonal antibody were found in bone marrow against blood precursors. These results provide the necessary rationale and support for a novel modality of therapeutic intervention, which may have application in the care of patients with ES. [Copyright &y& Elsevier]

Published

2006

23. Prognostic and therapeutic relevance of HER2 expression in osteosarcoma and Ewing’s sarcoma

Author

Scotlandi, Katia, Manara, Maria C., Hattinger, Claudia M., Benini, Stefania, Perdichizzi, Stefania, Pasello, Michela, Bacci, Gaetano, Zanella, Licciana, Bertoni, Franco, Picci, Piero, and Serra, Massimo

Subjects

*OSTEOSARCOMA, *ANTINEOPLASTIC agents, *MONOCLONAL antibodies, *P-glycoprotein

Abstract

Abstract: Expression of HER2 was evaluated by immunohistochemical techniques in 84 osteosarcoma (OS) and 113 Ewing’s sarcoma (ES) paraffin-embedded tumour biopsies. HER2 gene status was also assessed in a panel of cell lines as well as in vitro efficacy of trastuzumab (a humanised antibody directed against HER2) as single agent or in combination with the insulin-like growth factor I receptor (IGF-IR) IR3 antibody. Overexpression of HER2 was present in 32% of OS and 16% of ES and was significantly associated with the increased expression of P-glycoprotein, a surface molecule responsible for multidrug resistance. Event-free survival analyses revealed a prognostic value for HER2 and/or P-glycoprotein expression in OS, but not in ES. However, despite its prognostic relevance, no therapeutic effectiveness was observed pre-clinically for trastuzumab-driven therapy, in both OS or ES cell lines, unless the antibody was associated with anti-IGF-IR targeting strategies. Therefore, the therapeutic potential of trastuzumab in these neoplasms may be better exploited in combined treatments with anti-IGF-IR approaches. [Copyright &y& Elsevier]

Published

2005

24. Genomics and Therapeutic Vulnerabilities of Primary Bone Tumors.

Author

Scotlandi, Katia, Hattinger, Claudia Maria, Pellegrini, Evelin, Gambarotti, Marco, and Serra, Massimo

Subjects

*BONE cancer, *EWING'S sarcoma, *GENOMICS, *SARCOMA, *CHONDROSARCOMA, *FOLLICULAR dendritic cells

Abstract

Osteosarcoma, Ewing sarcoma and chondrosarcoma are rare diseases but the most common primary tumors of bone. The genes directly involved in the sarcomagenesis, tumor progression and treatment responsiveness are not completely defined for these tumors, and the powerful discovery of genetic analysis is highly warranted in the view of improving the therapy and cure of patients. The review summarizes recent advances concerning the molecular and genetic background of these three neoplasms and, of their most common variants, highlights the putative therapeutic targets and the clinical trials that are presently active, and notes the fundamental issues that remain unanswered. In the era of personalized medicine, the rarity of sarcomas may not be the major obstacle, provided that each patient is studied extensively according to a road map that combines emerging genomic and functional approaches toward the selection of novel therapeutic strategies. [ABSTRACT FROM AUTHOR]

Published

2020

25. Clinical Significance of Tumor Protein D52 Immunostaining in a Large Series of Ewing's Sarcoma Family of Tumors.

Author

Machado, Isidro, López-Guerrero, José A., Calabuig-Fariñas, Silvia, Hardy, Jayne R., Scotlandi, Katia, Picci, Piero, Byrne, Jennifer A., and Llombart-Bosch, Antonio

Subjects

LETTERS to the editor, TUMOR proteins, EWING'S sarcoma

Abstract

A letter to the editor is presented which discusses the clinicopathologic significance of tumor protein D52 (TPD52) immunostaining in 324 genetically confirmed Ewing's sarcoma family of tumor (ESFTs).

Published

2011

26. Immunoreactivity using anti-ERG monoclonal antibodies in sarcomas is influenced by clone selection.

Author

Machado, Isidro, Mayordomo-Aranda, Empar, Scotlandi, Katia, Picci, Piero, and Llombart-Bosch, Antonio

Subjects

*IMMUNE response, *ELECTRORETINOGRAPHY, *MONOCLONAL antibodies, *IMMUNOHISTOCHEMISTRY, *EWING'S sarcoma, *GENE expression, *THERAPEUTICS

Abstract

The aim of the present study was to explore ERG immunoreactivity in a series of sarcomas, GIST and malignant rhabdoid tumor (MRT), considering the not fully elucidated specificity and sensitivity of this antibody. Paraffin-embedded tissue microarrays from those tumors were stained with anti-ERG against the C-terminus [(EPR3864(2)] and N-terminus (Clone 9FY). EPR3864(2) was positive in almost all angiosarcomas, and MRT.GIST were positive in a large proportion of cases (38.4%), and more than half the synovial sarcomas (52.7%) revealed EPR3864(2) staining. Several chondrosarcomas, osteosarcomas, rhabdomyosarcoma and Ewing's sarcoma family of tumors (ESFT) presented EPR3864(2) expression in a lower number of cases. 9FY was positive in most of the angiosarcomas; however, only sporadic ESFT and synovial sarcoma were positive and the other tumors tested were negative. Fourteen ESFT with EWSR1/Fli-1 gene fusion presented positive nuclear staining for EPR3864(2). Similarly, 5 ESFT with EWSR1/Fli-1 gene fusion presented positive staining for 9FY. We must stress that the difference between the present and previous studies may be due to the source of the anti-ERG employed, anti-ERG against C or N-terminus, protein cross-reactivity and dilution. In conclusion, specificity for ERG staining in sarcomas should be considered with caution and the immunoexpression is undoubtedly influenced by clone and antibody selection. [ABSTRACT FROM AUTHOR]

Published

2014

27. Suppression of Deacetylase SIRT1 Mediates Tumor-Suppressive NOTCH Response and Offers a Novel Treatment Option in Metastatic Ewing Sarcoma.

Author

Ban, Jozef, Aryee, Dave N. T., Fourtouna, Argyro, van der Ent, Wietske, Kauer, Max, Niedan, Stephan, Machado, Isidro, Rodriguez-Galindo, Carlos, Tirado, Oscar M., Schwentner, Raphaela, Picci, Piero, Flanagan, Adrienne M., Berg, Verena, Strauss, Sandra J., Scotlandi, Katia, Lawlor, Elizabeth R., Snaar-Jagalska, Ewa, Llombart-Bosch, Antonio, and Kovar, Heinrich

Subjects

*TUMOR suppressor genes, *CANCER genes, *EWING'S sarcoma, *CANCER treatment, *XENOGRAFTS, *THERAPEUTICS

Abstract

The developmental receptor NOTCH plays an important role in various human cancers as a consequence of oncogenic mutations. Here we describe a novel mechanism of NOTCH-induced tumor suppression involving modulation of the deacetylase SIRT1, providing a rationale for the use of SIRT1 inhibitors to treat cancers where this mechanism is inactivated because of SIRT1 over expression. In Ewing sarcoma cells, NOTCH signaling is abrogated by the driver oncogene EWS-FLI1. Restoration of NOTCH signaling caused growth arrest due to activation of theNOTCHeffector HEY1, directly suppressing SIRT1 and thereby activating p53. This mechanism of tumor suppression was validated in Ewing sarcoma cells, B-cell tumors, and human keratinocytes where NOTCH dysregulation has been implicated pathogenically. Notably, the SIRT1/2 inhibitor Tenovin-6 killed Ewing sarcoma cells in vitro and prohibited tumor growth and spread in an established xenograft model in zebrafish. Using immunohistochemistry to analyze primary tissue specimens, we found that high SIRT1 expression was associated with Ewing sarcoma metastasis and poor prognosis. Our findings suggest a mechanistic rationale for the use of SIRT1 inhibitors being developed to treat metastatic disease in patients with Ewing sarcoma. [ABSTRACT FROM AUTHOR]

Published

2014

28. CD99 inhibits neural differentiation of human Ewing sarcoma cells and thereby contributes to oncogenesis.

Author

Rocchi, Anna, Cristina Manara, Maria, Sciandra, Marika, Zambelli, Diana, Nardi, Filippo, Nicoletti, Giordano, Garofalo, Cecilia, Meschini, Stefania, Astolfi, Annalisa, Colombo, Mario P., Lessnick, Stephen L., Picci, Piero, Scotlandi, Katia, and Manara, Maria Cristina

Subjects

*EWING'S sarcoma, *BONE tumors, *MEMBRANE proteins, *BONE metastasis, *LABORATORY mice, *PHOSPHORYLATION

Abstract

Ewing sarcoma (EWS) is an aggressive bone tumor of uncertain cellular origin. CD99 is a membrane protein that is expressed in most cases of EWS, although its function in the disease is unknown. Here we have shown that endogenous CD99 expression modulates EWS tumor differentiation and malignancy. We determined that knocking down CD99 expression in human EWS cell lines reduced their ability to form tumors and bone metastases when xenografted into immunodeficient mice and diminished their tumorigenic characteristics in vitro. Further, reduction of CD99 expression resulted in neurite outgrowth and increased expression of beta-III tubulin and markers of neural differentiation. Analysis of a panel of human EWS cells revealed an inverse correlation between CD99 and H-neurofilament expression, as well as an inverse correlation between neural differentiation and oncogenic transformation. As knockdown of CD99 also led to an increase in phosphorylation of ERK1/2, we suggest that the CD99-mediated prevention of neural differentiation of EWS occurs through MAPK pathway modulation. Together, these data indicate a new role for CD99 in preventing neural differentiation of EWS cells and suggest that blockade of CD99 or its downstream molecular pathway may be a new therapeutic approach for EWS. [ABSTRACT FROM AUTHOR]

Published

2010

29. Identification of common and distinctive mechanisms of resistance to different anti-IGF-IR agents in Ewing's sarcoma

Author

Alexia Conte, Andrea Grilli, Sara Sigismund, Piero Picci, Cecilia Garofalo, Annalisa Astolfi, Katia Scotlandi, Maria Teresa Marino, Caterina Mancarella, Antonino Belfiore, Maria Cristina Manara, Alessandra Carè, Garofalo, Cecilia, Mancarella, Caterina, Grilli, Andrea, Manara, MARIA CRISTINA, Astolfi, Annalisa, Marino, Maria Teresa, Conte, Alexia, Sigismund, Sara, Carã, Alessandra, Belfiore, Antonino, Picci, Piero, and Scotlandi, Katia

Subjects

MAPK/ERK pathway, Drug Resistance, Pyrrole, Tyrosine-kinase inhibitor, Receptor, IGF Type 1, chemistry.chemical_compound, Endocrinology, Monoclonal, Insulin, Humanized, Original Research, Tumor, Immunoglobulins, Intravenous, Antibodies, Monoclonal, Sarcoma, General Medicine, Antibodies, Monoclonal, Humanized, Cell Line, Tumor, Cell Proliferation, Drug Resistance, Neoplasm, Humans, Insulin-Like Growth Factor II, Pyrimidines, Pyrroles, Receptor, Insulin, Sarcoma, Ewing, Signal Transduction, Molecular Biology, Signal transduction, Intravenous, Receptor, Human, medicine.drug_class, Immunoglobulins, Biology, Antibodies, NO, Cell Line, Ewing, medicine, IGF Type 1, Ewing's sarcoma, Neoplasm, medicine.disease, Gene expression profiling, Figitumumab, Insulin receptor, chemistry, Pyrimidine, Immunoglobulins, Intravenou, Cancer research, biology.protein

Abstract

IGF system contributes significantly to many human malignancies. Targeting IGF-I receptor (IGF-IR) has been reported to be active against several tumors, but particular efficacy was observed only against a minority of Ewing's sarcoma patients. Identification of mechanisms of acquired resistance to anti-IGF-IR agents is mandatory to individualize their use in clinics and optimize cure costs. In this study, we compared gene expression profiles of cells made resistant with three different anti-IGF-IR drugs (human antibodies AVE1642, Figitumumab, or tyrosine kinase inhibitor NVP-AEW541) to highlight common and distinctive mechanisms of resistance. Among common mechanisms, we identified two molecular signatures that distinguish sensitive from resistant cells. Annotation analysis indicated some common altered pathways, such as insulin signaling, MAPK pathway, endocytosis, and modulation of some members of the interferon-induced transmembrane protein family. Among distinctive pathways/processes, resistance to human antibodies involves mainly genes regulating neural differentiation and angiogenesis, whereas resistance to NVP-AEW541 is mainly associated with alterations in genes concerning inflammation and antigen presentation. Evaluation of the common altered pathways indicated that resistant cells seem to maintain intact the IGF-IR internalization/degradation route of sensitive cells but constantly down-regulated its expression. In resistant cells, the loss of proliferative stimulus, normally sustained by IGF-I/IGF-IR autocrine loop in Ewing's sarcoma cells, is compensated by transcriptional up-regulation of IGF-II and insulin receptor-A; this signaling seems to favor the MAPK pathway over the v-akt murine thymoma viral oncogene homolog 1 pathway. Overall, complexity of IGF system requires analytical evaluation of its components to select those patients that may really benefit from this targeted therapy and support the idea of cotargeting IGF-IR and insulin receptor-A to increase the efficacy.

Published

2012