Your search keyword '"Iezzi, Simona"' showing total 4 results

1. Che-1 is targeted by c-Myc to sustain proliferation in pre-B-cell acute lymphoblastic leukemia.

Author

Folgiero, Valentina, Sorino, Cristina, Pallocca, Matteo, De Nicola, Francesca, Goeman, Frauke, Bertaina, Valentina, Strocchio, Luisa, Romania, Paolo, Pitisci, Angela, Iezzi, Simona, Catena, Valeria, Bruno, Tiziana, Strimpakos, Georgios, Passananti, Claudio, Mattei, Elisabetta, Blandino, Giovanni, Locatelli, Franco, and Fanciulli, Maurizio

Abstract

Despite progress in treating B-cell precursor acute lymphoblastic leukemia (BCP-ALL), disease recurrence remains the main cause of treatment failure. New strategies to improve therapeutic outcomes are needed, particularly in high-risk relapsed patients. Che-1/AATF (Che-1) is an RNA polymerase II-binding protein involved in proliferation and tumor survival, but its role in hematological malignancies has not been clarified. Here, we show that Che-1 is overexpressed in pediatric BCP-ALL during disease onset and at relapse, and that its depletion inhibits the proliferation of BCP-ALL cells. Furthermore, we report that c-Myc regulates Che-1 expression by direct binding to its promoter and describe a strict correlation between Che-1 expression and c-Myc expression. RNAseq analyses upon Che-1 or c-Myc depletion reveal a strong overlap of the respective controlled pathways. Genomewide ChIP-seq experiments suggest that Che-1 acts as a downstream effector of c-Myc. These results identify the pivotal role of Che-1 in the control of BCP-ALL proliferation and present the protein as a possible therapeutic target in children with relapsed BCP-ALL. [ABSTRACT FROM AUTHOR]

Published

2018

2. Che-1-induced inhibition of mTOR pathway enables stress-induced autophagy.

Author

Desantis, Agata, Bruno, Tiziana, Catena, Valeria, De Nicola, Francesca, Goeman, Frauke, Iezzi, Simona, Sorino, Cristina, Ponzoni, Maurilio, Bossi, Gianluca, Federico, Vincenzo, La Rosa, Francesca, Ricciardi, Maria Rosaria, Lesma, Elena, De Meo, Paolo D'Onorio, Castrignanò, Tiziana, Petrucci, Maria Teresa, Pisani, Francesco, Chesi, Marta, Bergsagel, P Leif, and Floridi, Aristide

Subjects

MTOR protein, DISEASES, PSYCHOLOGICAL stress, AUTOPHAGY, RAPAMYCIN, CELL growth, CELL metabolism

Abstract

Mammalian target of rapamycin ( mTOR) is a key protein kinase that regulates cell growth, metabolism, and autophagy to maintain cellular homeostasis. Its activity is inhibited by adverse conditions, including nutrient limitation, hypoxia, and DNA damage. In this study, we demonstrate that Che-1, a RNA polymerase II-binding protein activated by the DNA damage response, inhibits mTOR activity in response to stress conditions. We found that, under stress, Che-1 induces the expression of two important mTOR inhibitors, Redd1 and Deptor, and that this activity is required for sustaining stress-induced autophagy. Strikingly, Che-1 expression correlates with the progression of multiple myeloma and is required for cell growth and survival, a malignancy characterized by high autophagy response. [ABSTRACT FROM AUTHOR]

Published

2015

3. Functional interaction of the subunit 3 of RNA polymerase II (RPB3) with transcription factor-4 (ATF4)

Author

De Angelis, Roberta, Iezzi, Simona, Bruno, Tiziana, Corbi, Nicoletta, Di Padova, Monica, Floridi, Aristide, Fanciulli, Maurizio, and Passananti, Claudio

Subjects

*RNA polymerases, *TRANSCRIPTION factors, *PROTEINS

Abstract

RPB3 is a core subunit of RNA polymerase II (pol II) that, together with the RPB11 subunit, forms the heterodimer considered as a functional counterpart of the bacterial α subunit homodimer involved in promoter recognition. We previously employed the yeast two-hybrid system and identified an interaction between RPB3 and the myogenic transcription factor myogenin, demonstrating an involvement of this subunit in muscle differentiation. In this paper we report the interaction between RPB3 and another known transcription factor, ATF4. We found that the intensity of the interaction between RPB3 and ATF4 is similar to the one between RPB3 and myogenin. This interaction involves an RPB3 specific region not homologous to the prokaryotic α subunit. We demonstrated that RBP3 is able to enhance ATF4 transactivation, whereas the region of RPB3 (Sud) that contacts ATF4, when used as a dominant negative, markedly inhibits ATF4 transactivation activity. Interestingly, ATF4 protein level, as reported for its partner RPB3, increases during C2C7 cell line muscle differentiation. [Copyright &y& Elsevier]

Published

2003

4. The α‐like RNA polymerase II core subunit 3 (RPB3) is involved in tissue‐specific transcription and muscle differentiation via interaction with the myogenic factor myogenin.

Author

Corbi, Nicoletta, Di Padova, Monica, De Angelis, Roberta, Bruno, Tiziana, Libri, Valentina, Iezzi, Simona, Floridi, Aristide, Fanciulli, Maurizio, and Passananti, Claudio

Published

2002