Your search keyword '"Desideri, Marianna"' showing total 2 results

1. BH4 domain of bcl-2 protein is required for its proangiogenic function under hypoxic condition.

Author

Gabellini, Chiara, De Luca, Teresa, Trisciuoglio, Daniela, Desideri, Marianna, Di Martile, Marta, Passeri, Daniela, Candiloro, Antonio, Biffoni, Mauro, Rizzo, Maria Giulia, Orlandi, Augusto, and Del Bufalo, Donatella

Subjects

NEOVASCULARIZATION, BCL-2 proteins, HYPOXEMIA, APOPTOSIS, VASCULAR endothelial growth factors, HYPOXIA-inducible factor 1, ENDOTHELIAL cells, CANCER cell proliferation

Abstract

Beyond its classical role as apoptosis inhibitor, bcl-2 protein promotes tumor angiogenesis and the removal of N-terminal bcl-2 homology (BH4) domain abrogates bcl-2-induced hypoxia-inducible factor 1 (HIF-1)-mediated vascular endothelial growth factor (VEGF) expression in hypoxic cancer cells. Using M14 human melanoma cell line and its derivative clones stably overexpressing bcl-2 wild-type or deleted of its BH4 domain, we found that conditioned media (CM) from cells expressing BH4-deleted bcl-2 protein showed a reduced capability to increase in vitro human endothelial cells proliferation and differentiation, and in vivo neovascularization compared with CM from cells overexpressing wild-type bcl-2. Moreover, xenografts derived from cells expressing bcl-2 lacking BH4 domain showed a reduction of metastatic potential compared with tumors derived from wild-type bcl-2 transfectants injection. Stably expressing the Flag-tagged N-terminal sequence of bcl-2 protein, encompassing BH4 domain, we found that this domain is sufficient to enhance the proangiogenic HIF-1/VEGF axis under hypoxic condition. Indeed, lacking of BH4 domain abolishes the interaction between bcl-2 and HIF-1α proteins and the capability of exogenous bcl-2 protein to localize in the nucleus. Moreover, when endoplasmic reticulum-targeted bcl-2 protein is overexpressed in cells, this protein lost the capability to synergize with hypoxia to induce the proangiogenic HIF-1/VEGF axis as shown by wild-type bcl-2 protein. These results demonstrate that BH4 domain of bcl-2 is required for the ability of this protein to increase tumor angiogenesis and progression and indicate that bcl-2 nuclear localization may be required for bcl-2-mediated induction of HIF-1/VEGF axis. [ABSTRACT FROM PUBLISHER]

Published

2013

2. Semaphorin 5A drives melanoma progression: role of Bcl-2, miR-204 and c-Myb.

Author

D'Aguanno, Simona, Valentini, Elisabetta, Tupone, Maria Grazia, Desideri, Marianna, Di Martile, Marta, Del Bufalo, Donatella, Trisciuoglio, Daniela, Spagnuolo, Manuela, Rizzo, Maria Giulia, Buglioni, Simonetta, Ercolani, Cristiana, Falcone, Italia, Milella, Michele, De Dominici, Marco, Calabretta, Bruno, Cota, Carlo, and Anichini, Andrea

Subjects

SEMAPHORINS, MELANOMA, DISEASE progression, BCL-2 proteins, MYB gene, MICRORNA

Abstract

Background: Melanoma, the most aggressive form of skin cancer, is characterized by high rates of metastasis, drug resistance and mortality. Here we investigated the role of Semaphorin 5A (Sema5A) on the properties associated with melanoma progression and the factors involved in Sema5A regulation. Methods: Western blotting, qRT-PCR, Chromatin immunoprecipitation (ChIP) assay, immunohistochemistry of melanoma patient specimens and xenograft tissues, in vitro Transwell assay for cell migration and invasion evaluation, in vitro capillary-like structure formation analysis. Results: A significant correlation of Sema5A mRNA expression and melanoma progression was observed by analyzing GEO profile dataset. Endogenous Sema5A protein was detected in 95% of human melanoma cell lines tested, in 70% of metastatic specimens from patients affected by melanoma, and 16% of in situ melanoma specimens showed a focal positivity. We demonstrated that Sema5A regulates in vitro cell migration and invasion and the formation of vasculogenic structures. We also found an increase of Sema5A at both mRNA and protein level after forced expression of Bcl-2. By use of transcriptional and proteasome inhibitors, we showed that Bcl-2 increases the stability of Sema5A mRNA and protein. Moreover, by ChIP we demonstrated that Sema5A expression is under the control of the transcription factor c-Myb and that c-Myb recruitment on Sema5A promoter is increased after Bcl-2 overexpression. Finally, a concomitant decrease in the expression of Sema5A, Bcl-2 and c-Myb proteins was observed in melanoma cells after miR-204 overexpression. Conclusion: Overall our data provide evidences supporting the role of Sema5A in melanoma progression and the involvement of Bcl-2, miR-204 and c-Myb in regulating its expression. [ABSTRACT FROM AUTHOR]

Published

2018