The transcription factor AP-1 plays key roles in tumorigenesis, by regulating a variety of protein-coding genes, implicated in multiple hallmarks of cancer. Among non-coding genes, no AP-1 target has been described yet in tumorigenesis. MicroRNAs (miRNAs) are negative post-transcriptional regulators of protein-coding genes. miRNA expression signatures are highly relevant in cancer and several tumor-associated miRNAs (oncomirs) play critical roles in oncogenesis. Here, we show that the miRNA miR-21, which represents the most frequently upregulated oncomir in solid tumors, is induced by AP-1 in response to RAS. By analyzing validated miR-21 targets, we have found that the tumor suppressors PTEN and PDCD4 are downregulated by RAS in an AP-1- and miR-21-dependent fashion. We further show that, given the role of PDCD4 as negative regulator of AP-1, the miR-21-mediated downregulation of PDCD4 is essential for the maximal induction of AP-1 activity in response to RAS. Our data reveal a novel mechanism of positive autoregulation of the AP-1 complex in RAS transformation and disclose the function of oncomirs as critical targets and regulators of AP-1 in tumorigenesis.

An autoregulatory loop mediated by miR-21 and PDCD4 controls the AP-1 activity in RAS transformation / Talotta, F.; Cimmino, A.; Matarazzo, M. R.; Casalino, L.; DE VITA, Gabriella; D'Esposito, M.; DI LAURO, Roberto; Verde, P.. - In: ONCOGENE. - ISSN 0950-9232. - STAMPA. - 28:1(2009), pp. 73-84. [10.1038/onc.2008.370]

An autoregulatory loop mediated by miR-21 and PDCD4 controls the AP-1 activity in RAS transformation.

DE VITA, GABRIELLA;DI LAURO, ROBERTO;
2009

Abstract

The transcription factor AP-1 plays key roles in tumorigenesis, by regulating a variety of protein-coding genes, implicated in multiple hallmarks of cancer. Among non-coding genes, no AP-1 target has been described yet in tumorigenesis. MicroRNAs (miRNAs) are negative post-transcriptional regulators of protein-coding genes. miRNA expression signatures are highly relevant in cancer and several tumor-associated miRNAs (oncomirs) play critical roles in oncogenesis. Here, we show that the miRNA miR-21, which represents the most frequently upregulated oncomir in solid tumors, is induced by AP-1 in response to RAS. By analyzing validated miR-21 targets, we have found that the tumor suppressors PTEN and PDCD4 are downregulated by RAS in an AP-1- and miR-21-dependent fashion. We further show that, given the role of PDCD4 as negative regulator of AP-1, the miR-21-mediated downregulation of PDCD4 is essential for the maximal induction of AP-1 activity in response to RAS. Our data reveal a novel mechanism of positive autoregulation of the AP-1 complex in RAS transformation and disclose the function of oncomirs as critical targets and regulators of AP-1 in tumorigenesis.
2009
An autoregulatory loop mediated by miR-21 and PDCD4 controls the AP-1 activity in RAS transformation / Talotta, F.; Cimmino, A.; Matarazzo, M. R.; Casalino, L.; DE VITA, Gabriella; D'Esposito, M.; DI LAURO, Roberto; Verde, P.. - In: ONCOGENE. - ISSN 0950-9232. - STAMPA. - 28:1(2009), pp. 73-84. [10.1038/onc.2008.370]
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11588/351649
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