H Ferritin Gene Silencing in a Human Metastatic Melanoma Cell Line: A Proteomic Analysis

Maddalena Di Sanzo; Marco Gaspari; Roberta Misaggi; Francesco Romeo; Lucia Falbo; Carmela De Marco; Valter Agosti; Barbara Quaresima; Tullio Barni; Giuseppe Viglietto; Martin Røssel Larsen; Giovanni Cuda; Francesco Costanzo; Maria Concetta Faniello

doi:10.1021/pr200705z

H Ferritin Gene Silencing in a Human Metastatic Melanoma Cell Line: A Proteomic Analysis

Authors:

Di Sanzo, Maddalena ;
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Gaspari, Marco ;
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Misaggi, Roberta ;
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Romeo, Francesco ;
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Falbo, Lucia ;
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De Marco, Carmela ;
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Agosti, Valter ;
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Quaresima, Barbara ;
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Barni, Tullio ;
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Viglietto, Giuseppe ;
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Larsen, Martin Røssel ;
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0000-0001-6203-0123
Department of Biochemistry and Molecular Biology, Faculty of Science, University of Southern Denmark
Cuda, Giovanni ;
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Costanzo, Francesco ;
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Faniello, Maria Concetta
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DOI:

10.1021/pr200705z

Abstract:

Ferritin, the major intracellular iron-storage protein, is made of 24 subunits of two types, H and L. Besides regulating intracellular iron homeostasis, it has been found that ferritin, in particular the H subunit (FHC), is involved in different biological events such as cell differentiation and pathologic states (i.e., neurodegeneration and cancer). This study is aimed at investigating the whole-cell proteome of FHC-expressing and sh-RNA-silenced human metastatic melanoma cells (MM07(m)) in the attempt to identify and classify the highest number of proteins directly or indirectly controlled by the FHC. We identified about 200 differentially expressed proteins and classified them in clusters on the basis of their functions, as proteins involved in metabolic processes, cell adhesion, migration, and proliferation processes. Some of them have captured our attention because of their involvement in metabolic pathways related to tumor progression and metastasis. In vitro assays confirmed that the FHC-silenced MM07(m) cells are characterized by a decreased growth activity, a reduced invasiveness, and a reduced cell adhesion capability. Moreover, nude mice (CD1 nu/nu), subcutaneously injected with FHC-silenced MM07(m) cells, showed a remarkable 4-fold reduction of their tumor growth capacity compared to those who received the FHC-unsilenced MM07(m) counterpart. In conclusion, these data indicate that gene silencing technology, coupled to proteomic analysis, is a powerful tool for a better understanding of H ferritin signaling pathways and lend support to the hypothesis that specific targeting of this gene might be an attractive and potentially effective strategy for the management of metastatic melanoma.

Type:

Journal article

Language:

English

Published in:

Journal of Proteome Research, 2011, Vol 10, Issue 12, p. 5444-5453

Main Research Area:

Science/technology

Publication Status:

Published

Review type:

Peer Review

Submission year:

2011

Scientific Level:

Scientific

ID:

187544725

H Ferritin Gene Silencing in a Human Metastatic Melanoma Cell Line: A Proteomic Analysis

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