Your search keyword '"Carro, Maria Stella"' showing total 16 results

1. ZBTB18 regulates cytokine expression and affects microglia/macrophage recruitment and commitment in glioblastoma.

Author

Ferrarese, Roberto, Joseph, Kevin, Andrieux, Geoffroy, Haase, Ira Verena, Zanon, Francesca, Kling, Eva, Izzo, Annalisa, Corrales, Eyleen, Schwabenland, Marius, Prinz, Marco, Ravi, Vidhya Madapusi, Boerries, Melanie, Heiland, Dieter Henrik, and Carro, Maria Stella

Abstract

Glioma associated macrophages/microglia (GAMs) play an important role in glioblastoma (GBM) progression, due to their massive recruitment to the tumor site and polarization to a tumor promoting phenotype. GAMs secrete a variety of cytokines, which facilitate tumor cell growth and invasion, and prevent other immune cells from mounting an immune response against the tumor. Here, we demonstrate that zinc finger and BTB containing domain 18 (ZBTB18), a transcriptional repressor with tumor suppressive function in glioblastoma, impairs the production of key cytokines, which function as chemoattractant for GAMs. Consistently, we observe a reduced migration of GAMs when ZBTB18 is expressed by glioblastoma cells, both in cell culture and in vivo experiments. Moreover, RNA sequencing analysis shows that the presence of ZBTB18 in glioblastoma cells alters the commitment of conditioned microglia, suggesting the loss of the immune-suppressive phenotype and the acquisition of pro-inflammatory features. Thus, therapeutic approaches to increase ZBTB18 expression in GBM cells could represent an effective adjuvant to immune therapy in GBM. In vitro, in vivo and in silico studies identify the transcriptional repressor ZBTB18 as a negative regulator of tumor associated macrophage recruitment and of their tumor promoting phenotype in glioblastoma [ABSTRACT FROM AUTHOR]

Published

2024

2. Systematic integration of m6A regulators and autophagy-related genes in combination with long non-coding RNAs predicts survival in glioblastoma multiforme.

Author

Sharma, Amit, Wang, Yulu, Ge, Fangfang, Chen, Peng, Dakal, Tikam Chand, Carro, Maria Stella, Schmidt-Wolf, Ingo G. H., and Maciaczyk, Jarek

Abstract

Glioblastoma multiforme (GBM) is probably the only tumor in which a unique epigenetic alteration, namely methylation of the MGMT gene, possesses direct clinical relevance. Now with the emergence of aberrant N6 methyladenosine (m6A) modifications (the most common epigenetic modification of mRNA, closely linked to the autophagy process) in cancer, the epi-transcriptomic landscape of GBM pathobiology has been expanded. Considering this, herein, we systematically analyzed m6A regulators, assessed their correlation with autophagy-related genes (ATG), and established a long non-coding RNAs (lncRNA)-dependent prognostic signature (m6A-autophagy-lncRNAs) for GBM. Our analysis identified a novel signature of five long non-coding RNAs (lncRNAs: ITGA6-AS1, AC124248.1, NFYC-AS1, AC025171.1, and AC005229.3) associated with survival of GBM patients, and four among them clearly showed cancer-associated potential. We further validated and confirmed the altered expression of two lncRNAs (AC124248.1, AC005229.3) in GBM associated clinical samples using RT-PCR. Concerning the prognostic ability, the obtained signature determined high-/low-risk groups in GBM patients and showed sensitivity to anticancer drugs. Collectively, the m6A-autophagy-lncRNAs signature presented in the study is clinically relevant and is the first attempt to systematically predict the potential interaction between the three key determinants (m6A, autophagy, lncRNA) in cancer, particularly in GBM. [ABSTRACT FROM AUTHOR]

Published

2023

3. ZBTB18 inhibits SREBP-dependent lipid synthesis by halting CTBPs and LSD1 activity in glioblastoma.

Author

Ferrarese, Roberto, Izzo, Annalisa, Andrieux, Geoffroy, Lagies, Simon, Bartmuss, Johanna Paulina, Masilamani, Anie Priscilla, Wasilenko, Alix, Osti, Daniela, Faletti, Stefania, Schulzki, Rana, Yuan, Shuai, Kling, Eva, Ribecco, Valentino, Heiland, Dieter Henrik, Tholen, Stefan, Prinz, Marco, Pelicci, Giuliana, Kammerer, Bernd, Boerries, Melanie, and Carro, Maria Stella

Published

2023

4. T-cell dysfunction in the glioblastoma microenvironment is mediated by myeloid cells releasing interleukin-10.

Author

Ravi, Vidhya M., Neidert, Nicolas, Will, Paulina, Joseph, Kevin, Maier, Julian P., Kückelhaus, Jan, Vollmer, Lea, Goeldner, Jonathan M., Behringer, Simon P., Scherer, Florian, Boerries, Melanie, Follo, Marie, Weiss, Tobias, Delev, Daniel, Kernbach, Julius, Franco, Pamela, Schallner, Nils, Dierks, Christine, Carro, Maria Stella, and Hofmann, Ulrich G.

Subjects

MYELOID cells, INTERLEUKIN-10, GLIOBLASTOMA multiforme, TUMOR microenvironment, IMMUNE response, CYTOTOXIC T cells

Abstract

Despite recent advances in cancer immunotherapy, certain tumor types, such as Glioblastomas, are highly resistant due to their tumor microenvironment disabling the anti-tumor immune response. Here we show, by applying an in-silico multidimensional model integrating spatially resolved and single-cell gene expression data of 45,615 immune cells from 12 tumor samples, that a subset of Interleukin-10-releasing HMOX1+ myeloid cells, spatially localizing to mesenchymal-like tumor regions, drive T-cell exhaustion and thus contribute to the immunosuppressive tumor microenvironment. These findings are validated using a human ex-vivo neocortical glioblastoma model inoculated with patient derived peripheral T-cells to simulate the immune compartment. This model recapitulates the dysfunctional transformation of tumor infiltrating T-cells. Inhibition of the JAK/STAT pathway rescues T-cell functionality both in our model and in-vivo, providing further evidence of IL-10 release being an important driving force of tumor immune escape. Our results thus show that integrative modelling of single cell and spatial transcriptomics data is a valuable tool to interrogate the tumor immune microenvironment and might contribute to the development of successful immunotherapies. The tumour microenvironment counteracts immune therapy in Glioblastomas. Authors show here, using spatially resolved and single cell transcriptomics, that dysfunctional T cells are induced by a myeloid cell subset via Interleukin-10 signalling, and inhibition of the downstream JAK/STAT pathway might restore glioblastoma immune therapy responsiveness. [ABSTRACT FROM AUTHOR]

Published

2022

5. T-cell dysfunction in the glioblastoma microenvironment is mediated by myeloid cells releasing interleukin-10.

Author

Ravi, Vidhya M., Neidert, Nicolas, Will, Paulina, Joseph, Kevin, Maier, Julian P., Kückelhaus, Jan, Vollmer, Lea, Goeldner, Jonathan M., Behringer, Simon P., Scherer, Florian, Boerries, Melanie, Follo, Marie, Weiss, Tobias, Delev, Daniel, Kernbach, Julius, Franco, Pamela, Schallner, Nils, Dierks, Christine, Carro, Maria Stella, and Hofmann, Ulrich G.

Subjects

MYELOID cells, INTERLEUKIN-10, GLIOBLASTOMA multiforme, T cells, TUMOR microenvironment, IMMUNE response, CYTOTOXIC T cells

Abstract

Despite recent advances in cancer immunotherapy, certain tumor types, such as Glioblastomas, are highly resistant due to their tumor microenvironment disabling the anti-tumor immune response. Here we show, by applying an in-silico multidimensional model integrating spatially resolved and single-cell gene expression data of 45,615 immune cells from 12 tumor samples, that a subset of Interleukin-10-releasing HMOX1+ myeloid cells, spatially localizing to mesenchymal-like tumor regions, drive T-cell exhaustion and thus contribute to the immunosuppressive tumor microenvironment. These findings are validated using a human ex-vivo neocortical glioblastoma model inoculated with patient derived peripheral T-cells to simulate the immune compartment. This model recapitulates the dysfunctional transformation of tumor infiltrating T-cells. Inhibition of the JAK/STAT pathway rescues T-cell functionality both in our model and in-vivo, providing further evidence of IL-10 release being an important driving force of tumor immune escape. Our results thus show that integrative modelling of single cell and spatial transcriptomics data is a valuable tool to interrogate the tumor immune microenvironment and might contribute to the development of successful immunotherapies. The tumour microenvironment counteracts immune therapy in Glioblastomas. Authors show here, using spatially resolved and single cell transcriptomics, that dysfunctional T cells are induced by a myeloid cell subset via Interleukin-10 signalling, and inhibition of the downstream JAK/STAT pathway might restore glioblastoma immune therapy responsiveness. [ABSTRACT FROM AUTHOR]

Published

2022

6. NF1 regulates mesenchymal glioblastoma plasticity and aggressiveness through the AP-1 transcription factor FOSL1.

Author

Marques, Carolina, Unterkircher, Thomas, Kroon, Paula, Oldrini, Barbara, Izzo, Annalisa, Dramaretska, Yuliia, Ferrarese, Roberto, Oliver Schnell, Eva Kling2, Nelander, Sven, Wagner, Erwin F., Bakiri, Latifa, Gargiulo, Gaetano, Carro, Maria Stella, and Squatrito, Massimo

Published

2021

7. The aberrant splicing of BAF45d links splicing regulation and transcription in glioblastoma.

Author

Aldave, Guillermo, Gonzalez-Huarriz, Marisol, Rubio, Angel, Romero, Juan Pablo, Ravi, Datta, Miñana, Belén, Cuadrado-Tejedor, Mar, García-Osta, Ana, Verhaak, Roeland, Xipell, Enric, Martinez-Vélez, Naiara, de la Rocha, Arlet Acanda, Puigdelloses, Montserrat, García-Moure, Marc, Marigil, Miguel, Pérez-Larraya, Jaime Gállego, Marín-Bejar, Oskar, Huarte, Maite, Carro, Maria Stella, and Ferrarese, Roberto

Published

2018

8. EGFR feedback-inhibition by Ran-binding protein 6 is disrupted in cancer.

Author

Oldrini, Barbara, Wan-Ying Hsieh, Erdjument-Bromage, Hediye, Codega, Paolo, Carro, Maria Stella, Curiel-García, Alvaro, Campos, Carl, Pourmaleki, Maryam, Grommes, Christian, Vivanco, Igor, Rohle, Daniel, Bielski, Craig M., Taylor, Barry S., Hollmann, Travis J., Rosenblum, Marc, Tempst, Paul, Blenis, John, Squatrito, Massimo, and Mellinghoff, Ingo K.

Subjects

EPIDERMAL growth factor receptors

Abstract

Transport of macromolecules through the nuclear pore by importins and exportins plays a critical role in the spatial regulation of protein activity. How cancer cells co-opt this process to promote tumorigenesis remains unclear. The epidermal growth factor receptor (EGFR) plays a critical role in normal development and in human cancer. Here we describe a mechanism of EGFR regulation through the importin β family member RAN-binding protein 6 (RanBP6), a protein of hitherto unknown functions. We show that RanBP6 silencing impairs nuclear translocation of signal transducer and activator of transcription 3 (STAT3), reduces STAT3 binding to the EGFR promoter, results in transcriptional derepression of EGFR, and increased EGFR pathway output. Focal deletions of the RanBP6 locus on chromosome 9p were found in a subset of glioblastoma (GBM) and silencing of RanBP6 promoted glioma growth in vivo. Our results provide an example of EGFR deregulation in cancer through silencing of components of the nuclear import pathway. [ABSTRACT FROM AUTHOR]

Published

2017

9. Neural networks help zebrafish to step up as a model for efficient drug screening in glioblastoma.

Author

Ferrarese, Roberto and Carro, Maria Stella

Published

2022

10. Functional role of CLIC1 ion channel in glioblastoma-derived stem/progenitor cells.

Author

Setti, Matteo, Savalli, Nicoletta, Osti, Daniela, Richichi, Cristina, Angelini, Marina, Brescia, Paola, Fornasari, Lorenzo, Carro, Maria Stella, Mazzanti, Michele, and Pelicci, Giuliana

Abstract

Background: Chloride channels are physiologically involved in cell division and motility. Chloride intracellular channel 1 (CLIC1) is overexpressed in a variety of human solid tumors compared with normal tissues, suggesting a potential involvement of CLIC1 in the regulation of tumorigenesis. This led us to investigate the role of CLIC1 in gliomagenesis.Methods: We used the neurosphere system to isolate stem/progenitor cells from human glioblastomas (GBMs). CLIC1 targeting in GBM neurospheres was achieved by both lentiviral-mediated short-hairpin RNA transduction and CLIC1 antibody treatment, and its effect on stem-like properties was analyzed in vitro by proliferation and clonogenic assays and in vivo by orthotopic injection in immunocompromised mice. Channel activity was studied by perforated patch clamp technique. Differences in expression were analyzed by analysis of variance with Tamhane's multiple comparison test. Kaplan-Meier analyses and log-rank test were used to assess survival. All statistical tests were two-sided.Results: CLIC1 was statistically significantly overexpressed in GBMs compared with normal brain tissues (P < .001) with a better survival of patients with CLIC1 low-expressing tumors (CLIC1(low) vs CLIC1(high) survival: χ(2) = 74.35; degrees of freedom = 1; log-rank P < .001). CLIC1 was variably expressed in patient-derived GBM neurospheres and was found enriched in the stem/progenitor compartment. CLIC1 silencing reduced proliferative (P < .01), clonogenic (P < .01), and tumorigenic capacity (P < .05) of stem/progenitor cells. The reduction of CLIC1 chloride currents with a specific CLIC1 antibody mirrored the biological effects of CLIC1 silencing in GBM patient-derived neurospheres.Conclusions: Reduced gliomagenesis after CLIC1 targeting in tumoral stem/progenitor cells and the finding that CLIC1 expression is inversely associated with patient survival suggest CLIC1 as a potential target and prognostic biomarker. [ABSTRACT FROM AUTHOR]

Published

2013

11. Functional Role of CLIC1 Ion Channel in Glioblastoma-Derived Stem/Progenitor Cells.

Author

Setti, Matteo, Savalli, Nicoletta, Osti, Daniela, Richichi, Cristina, Angelini, Marina, Brescia, Paola, Fornasari, Lorenzo, Carro, Maria Stella, Mazzanti, Michele, and Pelicci, Giuliana

Subjects

STATISTICAL correlation, ONCOLOGY, REGRESSION analysis, CELL proliferation, EXPERIMENTAL design

Abstract

Background Chloride channels are physiologically involved in cell division and motility. Chloride intracellular channel 1 (CLIC1) is overexpressed in a variety of human solid tumors compared with normal tissues, suggesting a potential involvement of CLIC1 in the regulation of tumorigenesis. This led us to investigate the role of CLIC1 in gliomagenesis. Methods We used the neurosphere system to isolate stem/progenitor cells from human glioblastomas (GBMs). CLIC1 targeting in GBM neurospheres was achieved by both lentiviral-mediated short-hairpin RNA transduction and CLIC1 antibody treatment, and its effect on stem-like properties was analyzed in vitro by proliferation and clonogenic assays and in vivo by orthotopic injection in immunocompromised mice. Channel activity was studied by perforated patch clamp technique. Differences in expression were analyzed by analysis of variance with Tamhane’s multiple comparison test. Kaplan–Meier analyses and log-rank test were used to assess survival. All statistical tests were two-sided. Results CLIC1 was statistically significantly overexpressed in GBMs compared with normal brain tissues (P < .001) with a better survival of patients with CLIC1 low-expressing tumors (CLIC1low vs CLIC1high survival: χ2 = 74.35; degrees of freedom = 1; log-rank P < .001). CLIC1 was variably expressed in patient-derived GBM neurospheres and was found enriched in the stem/progenitor compartment. CLIC1 silencing reduced proliferative (P < .01), clonogenic (P < .01), and tumorigenic capacity (P < .05) of stem/progenitor cells. The reduction of CLIC1 chloride currents with a specific CLIC1 antibody mirrored the biological effects of CLIC1 silencing in GBM patient–derived neurospheres. Conclusions Reduced gliomagenesis after CLIC1 targeting in tumoral stem/progenitor cells and the finding that CLIC1 expression is inversely associated with patient survival suggest CLIC1 as a potential target and prognostic biomarker. [ABSTRACT FROM PUBLISHER]

Published

2013

12. Resistance to Hypoxia-Induced, BNIP3-Mediated Cell Death Contributes to an Increase in a CD133-Positive Cell Population in Human Glioblastomas In Vitro.

Author

Kahlert, Ulf Dietrich, Maciaczyk, Donata, Dai, Fangping, Claus, Rainer, Firat, Elke, Doostkam, Soroush, Bogiel, Tomasz, Carro, Maria Stella, Döbrössy, Mate, Herold-Mende, Christel, Niedermann, Gabriele, Prinz, Marco, Nikkhah, Guido, and Maciaczyk, Jaroslaw

Published

2012

13. The transcriptional network for mesenchymal transformation of brain tumours.

Author

Carro, Maria Stella, Wei Keat Lim, Alvarez, Mariano Javier, Bollo, Robert J., Xudong Zhao, Snyder, Evan Y., Sulman, Erik P., Anne, Sandrine L., Doetsch, Fiona, Colman, Howard, Lasorella, Anna, Aldape, Ken, Califano, Andrea, and Iavarone, Antonio

Subjects

SYSTEMS biology, PHENOTYPES, BRAIN tumors, GLIOBLASTOMA multiforme, CENTRAL nervous system, CANCER cells, GENE expression, TRANSCRIPTION factors, NERVE tissue

Abstract

The inference of transcriptional networks that regulate transitions into physiological or pathological cellular states remains a central challenge in systems biology. A mesenchymal phenotype is the hallmark of tumour aggressiveness in human malignant glioma, but the regulatory programs responsible for implementing the associated molecular signature are largely unknown. Here we show that reverse-engineering and an unbiased interrogation of a glioma-specific regulatory network reveal the transcriptional module that activates expression of mesenchymal genes in malignant glioma. Two transcription factors (C/EBPβ and STAT3) emerge as synergistic initiators and master regulators of mesenchymal transformation. Ectopic co-expression of C/EBPβ and STAT3 reprograms neural stem cells along the aberrant mesenchymal lineage, whereas elimination of the two factors in glioma cells leads to collapse of the mesenchymal signature and reduces tumour aggressiveness. In human glioma, expression of C/EBPβ and STAT3 correlates with mesenchymal differentiation and predicts poor clinical outcome. These results show that the activation of a small regulatory module is necessary and sufficient to initiate and maintain an aberrant phenotypic state in cancer cells. [ABSTRACT FROM AUTHOR]

Published

2010

14. Localizing hotspots of antisense transcription.

Author

Finocchiaro, Giacomo, Carro, Maria Stella, Francois, Stephanie, Parise, Paola, DiNinni, Valentina, and Muller, Heiko

Published

2007

15. DEK Expression is Controlled by E2F and Deregulated in Diverse Tumor Types.

Author

Carro, Maria Stella, Spiga, Fabio Mario, Quarto, Micaela, Di Ninni, Valentina, Volorio, Sara, Alcalay, Myriam, and Müller, Heiko

Published

2006

16. Integrative Network-based Analysis of Magnetic Resonance Spectroscopy and Genome Wide Expression in Glioblastoma multiforme.

Author

Heiland, Dieter Henrik, Mader, Irina, Schlosser, Pascal, Pfeifer, Dietmar, Carro, Maria Stella, Lange, Thomas, Schwarzwald, Ralf, Vasilikos, Ioannis, Urbach, Horst, and Weyerbrock, Astrid

Published

2016