MDM2 promoter SNP344T>A (rs1196333) status does not affect cancer risk.

MDM2 promoter SNP344T>A (rs1196333) status does not affect cancer risk.

The MDM2 proto-oncogene plays a key role in central cellular processes like growth control and apoptosis, and the gene locus is frequently amplified in sarcomas. Two polymorphisms located in the MDM2 promoter P2 have been shown to affect cancer risk. One of these polymorphisms (SNP309T>G; rs22797...

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Main Authors: Stian Knappskog, Liv B Gansmo, Pål Romundstad, Merete Bjørnslett, Jone Trovik, Jan Sommerfelt-Pettersen, Erik Løkkevik, Norwegian Breast Cancer Group trial NBCG VI, Rob A E M Tollenaar, Caroline Seynaeve, Peter Devilee, Helga B Salvesen, Anne Dørum, Kristian Hveem, Lars Vatten, Per E Lønning
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2012-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3340411?pdf=render
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spelling doaj-73927cc6763348dd8815069ae625c8b32020-11-24T21:50:45ZengPublic Library of Science (PLoS)PLoS ONE1932-62032012-01-0174e3626310.1371/journal.pone.0036263MDM2 promoter SNP344T>A (rs1196333) status does not affect cancer risk.Stian KnappskogLiv B GansmoPål RomundstadMerete BjørnslettJone TrovikJan Sommerfelt-PettersenErik LøkkevikNorwegian Breast Cancer Group trial NBCG VIRob A E M TollenaarCaroline SeynaevePeter DevileeHelga B SalvesenAnne DørumKristian HveemLars VattenPer E LønningThe MDM2 proto-oncogene plays a key role in central cellular processes like growth control and apoptosis, and the gene locus is frequently amplified in sarcomas. Two polymorphisms located in the MDM2 promoter P2 have been shown to affect cancer risk. One of these polymorphisms (SNP309T>G; rs2279744) facilitates Sp1 transcription factor binding to the promoter and is associated with increased cancer risk. In contrast, SNP285G>C (rs117039649), located 24 bp upstream of rs2279744, and in complete linkage disequilibrium with the SNP309G allele, reduces Sp1 recruitment and lowers cancer risk. Thus, fine tuning of MDM2 expression has proven to be of significant importance with respect to tumorigenesis. We assessed the potential functional effects of a third MDM2 promoter P2 polymorphism (SNP344T>A; rs1196333) located on the SNP309T allele. While in silico analyses indicated SNP344A to modulate TFAP2A, SPIB and AP1 transcription factor binding, we found no effect of SNP344 status on MDM2 expression levels. Assessing the frequency of SNP344A in healthy Caucasians (n = 2,954) and patients suffering from ovarian (n = 1,927), breast (n = 1,271), endometrial (n = 895) or prostatic cancer (n = 641), we detected no significant difference in the distribution of this polymorphism between any of these cancer forms and healthy controls (6.1% in healthy controls, and 4.9%, 5.0%, 5.4% and 7.2% in the cancer groups, respectively). In conclusion, our findings provide no evidence indicating that SNP344A may affect MDM2 transcription or cancer risk.http://europepmc.org/articles/PMC3340411?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Stian Knappskog
Liv B Gansmo
Pål Romundstad
Merete Bjørnslett
Jone Trovik
Jan Sommerfelt-Pettersen
Erik Løkkevik
Norwegian Breast Cancer Group trial NBCG VI
Rob A E M Tollenaar
Caroline Seynaeve
Peter Devilee
Helga B Salvesen
Anne Dørum
Kristian Hveem
Lars Vatten
Per E Lønning
spellingShingle Stian Knappskog
Liv B Gansmo
Pål Romundstad
Merete Bjørnslett
Jone Trovik
Jan Sommerfelt-Pettersen
Erik Løkkevik
Norwegian Breast Cancer Group trial NBCG VI
Rob A E M Tollenaar
Caroline Seynaeve
Peter Devilee
Helga B Salvesen
Anne Dørum
Kristian Hveem
Lars Vatten
Per E Lønning
MDM2 promoter SNP344T>A (rs1196333) status does not affect cancer risk.
PLoS ONE
author_facet Stian Knappskog
Liv B Gansmo
Pål Romundstad
Merete Bjørnslett
Jone Trovik
Jan Sommerfelt-Pettersen
Erik Løkkevik
Norwegian Breast Cancer Group trial NBCG VI
Rob A E M Tollenaar
Caroline Seynaeve
Peter Devilee
Helga B Salvesen
Anne Dørum
Kristian Hveem
Lars Vatten
Per E Lønning
author_sort Stian Knappskog
title MDM2 promoter SNP344T>A (rs1196333) status does not affect cancer risk.
title_short MDM2 promoter SNP344T>A (rs1196333) status does not affect cancer risk.
title_full MDM2 promoter SNP344T>A (rs1196333) status does not affect cancer risk.
title_fullStr MDM2 promoter SNP344T>A (rs1196333) status does not affect cancer risk.
title_full_unstemmed MDM2 promoter SNP344T>A (rs1196333) status does not affect cancer risk.
title_sort mdm2 promoter snp344t>a (rs1196333) status does not affect cancer risk.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2012-01-01
description The MDM2 proto-oncogene plays a key role in central cellular processes like growth control and apoptosis, and the gene locus is frequently amplified in sarcomas. Two polymorphisms located in the MDM2 promoter P2 have been shown to affect cancer risk. One of these polymorphisms (SNP309T>G; rs2279744) facilitates Sp1 transcription factor binding to the promoter and is associated with increased cancer risk. In contrast, SNP285G>C (rs117039649), located 24 bp upstream of rs2279744, and in complete linkage disequilibrium with the SNP309G allele, reduces Sp1 recruitment and lowers cancer risk. Thus, fine tuning of MDM2 expression has proven to be of significant importance with respect to tumorigenesis. We assessed the potential functional effects of a third MDM2 promoter P2 polymorphism (SNP344T>A; rs1196333) located on the SNP309T allele. While in silico analyses indicated SNP344A to modulate TFAP2A, SPIB and AP1 transcription factor binding, we found no effect of SNP344 status on MDM2 expression levels. Assessing the frequency of SNP344A in healthy Caucasians (n = 2,954) and patients suffering from ovarian (n = 1,927), breast (n = 1,271), endometrial (n = 895) or prostatic cancer (n = 641), we detected no significant difference in the distribution of this polymorphism between any of these cancer forms and healthy controls (6.1% in healthy controls, and 4.9%, 5.0%, 5.4% and 7.2% in the cancer groups, respectively). In conclusion, our findings provide no evidence indicating that SNP344A may affect MDM2 transcription or cancer risk.
url http://europepmc.org/articles/PMC3340411?pdf=render
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