Histone deacetylase inhibitors upregulate p57Kip2 level by enhancing its expression through Sp1 transcription factor

doi:10.1093/carcin/bgn010

Carcinogenesis Advance Access originally published online on January 19, 2008
Carcinogenesis 2008 29(3):560-567; doi:10.1093/carcin/bgn010

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Histone deacetylase inhibitors upregulate p57^Kip2 level by enhancing its expression through Sp1 transcription factor

Valeria Cucciolla, Adriana Borriello, Maria Criscuolo, Antonio A. Sinisi¹, Debora Bencivenga, Annunziata Tramontano, Anna Chiara Scudieri, Adriana Oliva, Vincenzo Zappia and Fulvio Della Ragione^*

Department of Biochemistry and Biophysics ‘F. Cedrangolo’, Second University of Naples, Via Costantinopoli 16, 80138, Naples, Italy
¹ Dipartimento Medico-Chirurgico di Internistica Clinica e Sperimentale ‘F. Magrassi e A. Lanzara’, Istituto di Endocrinologia, Second University of Naples, 80131, Naples, Italy

^* To whom correspondence should be addressed. Tel: +39 081 5665812; Fax: +39 081 5665812; Email: fulvio.dellaragione{at}unina2.it

Histone deacetylase inhibitors (HDACIs) represent a new classof targeted anticancer agents. Here, we evaluate the effectsof butyrate (BuA) and other HDACIs on p57^Kip2, a cyclin-dependentkinase inhibitor (cki). We observed that inhibitors of classI/II histone deacetylases (HDACs), but not of class III HDACs,induce a remarkable accumulation of p57^Kip2 in several cells.The cki upregulation is associated with an increased gene expressionthat was not prevented by cycloheximide, indicating that HDACIsaffect directly p57^Kip2 transcription. The characterizationof p57^Kip2 promoter indicates that the first 165 bp are mostlyinvolved in the BuA effects. Chromatin immunoprecipitation studiesdemonstrated that the BuA treatment causes the recruitment ofSp1 transcription factor. The Sp1 importance was confirmed bythe reduction of BuA effects by mithramycin A (an Sp1 antagonist)and, most stringently, by Sp1 downregulation due to Sp1 siRNA.Moreover, both the treatments reduce the p57^Kip2 transcriptionin untreated cells, suggesting that Sp1 is required for theconstitutive cki expression. Studies employing plasmids containingparts of the 165 bp of p57^Kip2 promoter indicate that the promoterregion between –87 and –113 bp, which includes twoputative Sp1 consensus sequences, plays a critical role in theresponse to HDACIs. Since this p57^Kip2 promoter region alsoembraces the consensus sequence for the transcriptional repressorchicken ovalbumin upstream promoter transcription factor-interactingprotein 2 (CTIP2), we evaluated whether this factor is involvedinto the BuA effect. When CTIP2 was downregulated by a specificsiRNA, we observed the enhancement of BuA activity on p57^Kip2expression suggesting that CTIP2 might also be involved in HDACIseffects.

Abbreviations: ChIP, chromatin immunoprecipitation; cki, cyclin-dependent kinase inhibitor; CTIP2, chicken ovalbumin upstream promoter transcription factor-interacting protein 2; HDAC, histone deacetylase; HDACI, histone deacetylase inhibitor; PCR, polymerase chain reaction; TSA, trichostatin A

Received July 31, 2007; revised November 26, 2007; accepted January 4, 2008.

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