The high mobility group A (HMGA) proteins are thought to work as ancillary transcription factors and to regulate the expression of a growing number of genes through direct binding to DNA or via protein-protein interactions. Both HMGA1 and HMGA2 are important regulators of basic biological processes, including cell growth, differentiation and transformation. Their qualitatively or quantitatively altered expression has been described in a number of human tumors. We studied and review here their expression in neuroblastic tumors. HMGA2 is expressed only in a subset of ex vivo neuroblastoma (NB) tumors and in the embryonic adrenal gland, but it is undetectable in the adult adrenal gland, suggesting that its anomalous expression might be associated with NB tumorigenesis and/or tumor progression. In vitro, its expression is easily detectable in retinoic acid (RA)-resistant cell lines. The exogenous expression of HMGA2 is sufficient to convert RA-sensitive SY5Y NB cells into RA-resistant cells, thus suggesting that HMGA2 might be a relevant player in determining NB cell responses to endogenous or therapeutically important growth inhibitory substances. In contrast, HNIGA1 expression is readily detectable in all NB cell lines and tumors, but its expression is consistently higher in less differentiated NBs compared with ganglioneuromas and ganglioneuroblastomas. Interestingly, RA increases HNIGA1 expression in RA-resistant NB cells but inhibits it in cells undergoing RA-induced growth inhibition and neuronal differentiation. Our studies indicate that HMGA molecules might be biologically and pathologically relevant factors in neuroblastic tumor development and progression.

HMGA molecules in neuroblastic tumors / F., Cerignoli; C., Ambrosi; M., Mellone; Massimi, Isabella; DI MARCOTULLIO, Lucia; Gulino, Alberto; Giannini, Giuseppe. - In: ANNALS OF THE NEW YORK ACADEMY OF SCIENCES. - ISSN 0077-8923. - STAMPA. - 1028:1(2004), pp. 122-132. (Intervento presentato al convegno Conference on Signal Transduction and Communication in Cancer Cells tenutosi a Erice, ITALY nel OCT 24-31, 2003) [10.1196/annals.1322.013].

HMGA molecules in neuroblastic tumors

MASSIMI, ISABELLA;DI MARCOTULLIO, LUCIA;GULINO, Alberto;GIANNINI, Giuseppe
2004

Abstract

The high mobility group A (HMGA) proteins are thought to work as ancillary transcription factors and to regulate the expression of a growing number of genes through direct binding to DNA or via protein-protein interactions. Both HMGA1 and HMGA2 are important regulators of basic biological processes, including cell growth, differentiation and transformation. Their qualitatively or quantitatively altered expression has been described in a number of human tumors. We studied and review here their expression in neuroblastic tumors. HMGA2 is expressed only in a subset of ex vivo neuroblastoma (NB) tumors and in the embryonic adrenal gland, but it is undetectable in the adult adrenal gland, suggesting that its anomalous expression might be associated with NB tumorigenesis and/or tumor progression. In vitro, its expression is easily detectable in retinoic acid (RA)-resistant cell lines. The exogenous expression of HMGA2 is sufficient to convert RA-sensitive SY5Y NB cells into RA-resistant cells, thus suggesting that HMGA2 might be a relevant player in determining NB cell responses to endogenous or therapeutically important growth inhibitory substances. In contrast, HNIGA1 expression is readily detectable in all NB cell lines and tumors, but its expression is consistently higher in less differentiated NBs compared with ganglioneuromas and ganglioneuroblastomas. Interestingly, RA increases HNIGA1 expression in RA-resistant NB cells but inhibits it in cells undergoing RA-induced growth inhibition and neuronal differentiation. Our studies indicate that HMGA molecules might be biologically and pathologically relevant factors in neuroblastic tumor development and progression.
2004
hmga; neuroblastic tumors; retinoic acid
01 Pubblicazione su rivista::01a Articolo in rivista
HMGA molecules in neuroblastic tumors / F., Cerignoli; C., Ambrosi; M., Mellone; Massimi, Isabella; DI MARCOTULLIO, Lucia; Gulino, Alberto; Giannini, Giuseppe. - In: ANNALS OF THE NEW YORK ACADEMY OF SCIENCES. - ISSN 0077-8923. - STAMPA. - 1028:1(2004), pp. 122-132. (Intervento presentato al convegno Conference on Signal Transduction and Communication in Cancer Cells tenutosi a Erice, ITALY nel OCT 24-31, 2003) [10.1196/annals.1322.013].
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11573/365265
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