Your search keyword '"De Smaele E"' showing total 6 results

1. Numb isoforms deregulation in medulloblastoma and role of p66 isoform in cancer and neural stem cells

Author

Abballe, L., Mastronuzzi, A., Miele, E., Carai, A., Besharat, Z. M., Moretti, M., De Smaele, E., Giangaspero, F., Locatelli, Franco, Ferretti, E., Po, A., Locatelli F. (ORCID:0000-0002-7976-3654), Abballe, L., Mastronuzzi, A., Miele, E., Carai, A., Besharat, Z. M., Moretti, M., De Smaele, E., Giangaspero, F., Locatelli, Franco, Ferretti, E., Po, A., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Numb is an intracellular protein with multiple functions. The two prevalent isoforms, Numb p66 and Numb p72, are regulators of differentiation and proliferation in neuronal development. Additionally, Numb functions as cell fate determinant of stem cells and cancer stem cells and its abnormal expression has been described in several types of cancer. Involvement of deregulated Numb expression has been described in the malignant childhood brain tumor medulloblastoma, while Numb isoforms in these tumors and in cancer stem-like cells derived from them, have not been studied to date. Here we show that medulloblastoma stem-like cells and cerebellar neuronal stem cells (NSCs) express Numb p66 where its expression tampers stemness features. Furthermore, medulloblastoma samples evaluated in this study express decreased levels of Numb p66 while overexpressed Numb p72 compared with normal tissues. Our results uncover different roles for the two major Numb isoforms examined in medulloblastoma and a critical role for Numb p66 in regulating stem-like cells and NSCs maintenance.

Published

2018

2. Foxm1 controls a pro-stemness microRNA network in neural stem cells

Author

Besharat, Z. M., Abballe, L., Cicconardi, F., Bhutkar, A., Grassi, L., Le Pera, L., Moretti, M., Chinappi, M., D'Andrea, D., Mastronuzzi, A., Ianari, A., Vacca, A., De Smaele, E., Locatelli, Franco, Po, A., Miele, E., Ferretti, E., Locatelli F. (ORCID:0000-0002-7976-3654), Besharat, Z. M., Abballe, L., Cicconardi, F., Bhutkar, A., Grassi, L., Le Pera, L., Moretti, M., Chinappi, M., D'Andrea, D., Mastronuzzi, A., Ianari, A., Vacca, A., De Smaele, E., Locatelli, Franco, Po, A., Miele, E., Ferretti, E., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Cerebellar neural stem cells (NSCs) require Hedgehog-Gli (Hh-Gli) signalling for their maintenance and Nanog expression for their self-renewal. To identify novel molecular features of this regulatory pathway, we used next-generation sequencing technology to profile mRNA and microRNA expression in cerebellar NSCs, before and after induced differentiation (Diff-NSCs). Genes with higher transcript levels in NSCs (vs. Diff-NSCs) included Foxm1, which proved to be directly regulated by Gli and Nanog. Foxm1 in turn regulated several microRNAs that were overexpressed in NSCs: miR-130b, miR-301a, and members of the miR-15∼16 and miR-17∼92 clusters and whose knockdown significantly impaired the neurosphere formation ability. Our results reveal a novel Hh-Gli-Nanog-driven Foxm1-microRNA network that controls the self-renewal capacity of NSCs.

Published

2018

3. Noncanonical GLI1 signaling promotes stemness features and in vivo growth in lung adenocarcinoma

Author

Po, A., Silvano, M., Miele, E., Capalbo, C., Eramo, A., Salvati, Valentina, Todaro, M., Besharat, Z. M., Catanzaro, G., Cucchi, D., Coni, S., Di Marcotullio, L., Canettieri, G., Vacca, A., Stassi, G., De Smaele, E., Tartaglia, Marco, Screpanti, I., De Maria Marchiano, Ruggero, Ferretti, E., Salvati, V., Tartaglia, M., De Maria Marchiano, R. (ORCID:0000-0003-2255-0583), Po, A., Silvano, M., Miele, E., Capalbo, C., Eramo, A., Salvati, Valentina, Todaro, M., Besharat, Z. M., Catanzaro, G., Cucchi, D., Coni, S., Di Marcotullio, L., Canettieri, G., Vacca, A., Stassi, G., De Smaele, E., Tartaglia, Marco, Screpanti, I., De Maria Marchiano, Ruggero, Ferretti, E., Salvati, V., Tartaglia, M., and De Maria Marchiano, R. (ORCID:0000-0003-2255-0583)

Abstract

Aberrant Hedgehog/GLI signaling has been implicated in a diverse spectrum of human cancers, but its role in lung adenocarcinoma (LAC) is still under debate. We show that the downstream effector of the Hedgehog pathway, GLI1, is expressed in 76% of LACs, but in roughly half of these tumors, the canonical pathway activator, Smoothened, is expressed at low levels, possibly owing to epigenetic silencing. In LAC cells including the cancer stem cell compartment, we show that GLI1 is activated noncanonically by MAPK/ERK signaling. Different mechanisms can trigger the MAPK/ERK/GLI1 cascade including KRAS mutation and stimulation of NRP2 by VEGF produced by the cancer cells themselves in an autocrine loop or by stromal cells as paracrine cross talk. Suppression of GLI1, by silencing or drug-mediated, inhibits LAC cells proliferation, attenuates their stemness and increases their susceptibility to apoptosis in vitro and in vivo. These findings provide insight into the growth of LACs and point to GLI1 as a downstream effector for oncogenic pathways. Thus, strategies involving direct inhibition of GLI1 may be useful in the treatment of LACs.

Published

2017

4. Noncanonical GLI1 signaling promotes stemness features and in vivo growth in lung adenocarcinoma

Author

Po, A, Silvano, M, Miele, E, Capalbo, C, Eramo, A, Salvati, Valentina, Todaro, M, Besharat, Zm, Catanzaro, G, Cucchi, D, Coni, S, Di Marcotullio, L, Canettieri, G, Vacca, A, Stassi, G, De Smaele, E, Tartaglia, Marco, Screpanti, I, De Maria Marchiano, Ruggero, Ferretti, E., Salvati V, Tartaglia M, De Maria Marchiano R (ORCID:0000-0003-2255-0583), Po, A, Silvano, M, Miele, E, Capalbo, C, Eramo, A, Salvati, Valentina, Todaro, M, Besharat, Zm, Catanzaro, G, Cucchi, D, Coni, S, Di Marcotullio, L, Canettieri, G, Vacca, A, Stassi, G, De Smaele, E, Tartaglia, Marco, Screpanti, I, De Maria Marchiano, Ruggero, Ferretti, E., Salvati V, Tartaglia M, and De Maria Marchiano R (ORCID:0000-0003-2255-0583)

Abstract

Aberrant Hedgehog/GLI signaling has been implicated in a diverse spectrum of human cancers, but its role in lung adenocarcinoma (LAC) is still under debate. We show that the downstream effector of the Hedgehog pathway, GLI1, is expressed in 76% of LACs, but in roughly half of these tumors, the canonical pathway activator, Smoothened, is expressed at low levels, possibly owing to epigenetic silencing. In LAC cells including the cancer stem cell compartment, we show that GLI1 is activated noncanonically by MAPK/ERK signaling. Different mechanisms can trigger the MAPK/ERK/GLI1 cascade including KRAS mutation and stimulation of NRP2 by VEGF produced by the cancer cells themselves in an autocrine loop or by stromal cells as paracrine cross talk. Suppression of GLI1, by silencing or drug-mediated, inhibits LAC cells proliferation, attenuates their stemness and increases their susceptibility to apoptosis in vitro and in vivo. These findings provide insight into the growth of LACs and point to GLI1 as a downstream effector for oncogenic pathways. Thus, strategies involving direct inhibition of GLI1 may be useful in the treatment of LACs.

Published

2017

5. MicroRNA profiling in human medulloblastoma

Author

Ferretti, E, De Smaele, E, Po, A, Di Marcotullio, L, Tosi, E, Espinola, M, Di Rocco, Concezio, Riccardi, Riccardo, Giangaspero, Felice, Farcomeni, A, Nofroni, I, Laneve, P, Gioia, U, Caffarelli, E, Bozzoni, I, Screpanti, I, Gulino, Alberto, Riccardi, Riccardo (ORCID:0000-0001-7515-6622), Ferretti, E, De Smaele, E, Po, A, Di Marcotullio, L, Tosi, E, Espinola, M, Di Rocco, Concezio, Riccardi, Riccardo, Giangaspero, Felice, Farcomeni, A, Nofroni, I, Laneve, P, Gioia, U, Caffarelli, E, Bozzoni, I, Screpanti, I, Gulino, Alberto, and Riccardi, Riccardo (ORCID:0000-0001-7515-6622)

Abstract

Medulloblastoma is an aggressive brain malignancy with high incidence in childhood. Current treatment approaches have limited efficacy and severe side effects. Therefore, new risk-adapted therapeutic strategies based on molecular classification are required. MicroRNA expression analysis has emerged as a powerful tool to identify candidate molecules playing an important role in a large number of malignancies. However, no data are yet available on human primary medulloblastomas. A high throughput microRNA expression profiles was performed in human primary medulloblastoma specimens to investigate microRNA involvement in medulloblastoma carcinogenesis. We identified specific microRNA expression patterns which distinguish medulloblastoma differing in histotypes (anaplastic, classic and desmoplastic), in molecular features (ErbB2 or c-Myc overexpressing tumors) and in disease-risk stratification. MicroRNAs expression profile clearly differentiates medulloblastoma from either adult or fetal normal cerebellar tissues. Only a few microRNAs displayed upregulated expression, while most of them were downregulated in tumor samples, suggesting a tumor growth-inhibitory function. This property has been addressed for miR-9 and miR-125a, whose rescued expression promoted medulloblastoma cell growth arrest and apoptosis while targeting the proproliferative truncated TrkC isoform. In conclusion, misregulated microRNA expression profiles characterize human medulloblastomas, and may provide potential targets for novel therapeutic strategies.

Published

2008

6. Alternative splicing of theErbB-4 cytoplastic domain and its regulation by hedgehog signaling identif distinct medulloblastoma subsets

Author

Ferretti, E, Marcotullio, L, Gessi, Marco, Greco, A, Mattei, T, Argenti, B, Alimandi, M, De Smaele, E, Giangaspero, Felice, Riccardi, Riccardo, Di Rocco, Concezio, Pazzaglia, S, Maroder, M., Screpanti, I, Gulino, Alberto, Riccardi, Riccardo (ORCID:0000-0001-7515-6622), Ferretti, E, Marcotullio, L, Gessi, Marco, Greco, A, Mattei, T, Argenti, B, Alimandi, M, De Smaele, E, Giangaspero, Felice, Riccardi, Riccardo, Di Rocco, Concezio, Pazzaglia, S, Maroder, M., Screpanti, I, Gulino, Alberto, and Riccardi, Riccardo (ORCID:0000-0001-7515-6622)

Abstract

Medulloblastoma (MB) results from aberrant development of cerebellar neurons in which altered hedgehog (Hh) signalling plays a major role. We investigated the possible influence of Hh signalling on ErbB-receptor expression in MB, in particular that of the ErbB-4 CYT-1 and CYT-2 isoforms generated by alternative splicing of the cytoplasmic domain. ErbB-4 expression was downregulated in Hh-induced MBs from Patched-1(+/-) mice. Hh signalling (reflected by enhanced expression of the Gli1 transcription factor) inhibited ErbB-4 expression in mouse cerebellar granule progenitors and human MB cells. Analysis of 26 human primary MBs revealed a subset of 11 tumors characterized by low Gli1 levels, upregulated ErbB-4 expression and increased CYT-1:CYT-2 ratios. Interestingly, CYT-1 and Gli1 levels were inversely correlated. ErbB-4 CYT-1 and CYT-2 had different phenotypic effects in cultured MB cells: in response to neuregulin treatment, CYT-2 overexpression inhibited proliferation whereas CYT-1, which includes a phosphatidylinositol 3-kinase (PI3K)-binding site that is missing in CYT-2, enhanced resistance to starvation- and etoposide-induced apoptosis by activating PI3K/Akt signalling. CYT-1:CYT-2 ratios displayed correlation with tumor histotype and ErbB-2 levels, which are established prognostic indices for MB. These findings demonstrate that low-level Hh signalling in human MB is associated with the selective maintenance of high ErbB-4 CYT-1 expression, an alteration that exerts tumor-promoting effects

Published

2006