Uroplakin Ib Gene Transcription in Urothelial Tumor Cells Is Regulated by CpG Methylation

Uroplakin Ib is a structural protein on the surface of urothelial cells. Levels of uroplakin Ib mRNA are dramatically reduced or absent in many transitional cell carcinomas, but the molecular mechanisms responsible remain undetermined. Previously, we showed that loss of uroplakin Ib expression corr...

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Main Authors: Prue Cowled, Irene Kanter, Lefta Leonardos, Paul Jackson
Format: Article
Language:English
Published: Elsevier 2005-12-01
Series:Neoplasia: An International Journal for Oncology Research
Subjects:
Sp1
Online Access:http://www.sciencedirect.com/science/article/pii/S1476558605800466
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spelling doaj-c8ef8d755f9448d582e140caca74a4912020-11-24T21:28:25ZengElsevierNeoplasia: An International Journal for Oncology Research1476-55861522-80022005-12-017121091110310.1593/neo.05364Uroplakin Ib Gene Transcription in Urothelial Tumor Cells Is Regulated by CpG MethylationPrue Cowled0Irene Kanter1Lefta Leonardos2Paul Jackson3Department of Surgery, The University of Adelaide, The Queen Elizabeth Hospital, Woodville, South Australia, AustraliaDepartment of Surgery, The University of Adelaide, The Queen Elizabeth Hospital, Woodville, South Australia, AustraliaDepartment of Surgery, The University of Adelaide, The Queen Elizabeth Hospital, Woodville, South Australia, AustraliaOncology Research Centre, Prince of Wales Hospital, Randwick, NSW, Australia Uroplakin Ib is a structural protein on the surface of urothelial cells. Levels of uroplakin Ib mRNA are dramatically reduced or absent in many transitional cell carcinomas, but the molecular mechanisms responsible remain undetermined. Previously, we showed that loss of uroplakin Ib expression correlated with CpG methylation of Sp1/NFκB-binding motifs within the proximal promoter. In this study, we show that reporter activity was completely blocked by the methylation of three CpG pairs in this promoter region. Gel shift analysis using purified proteins or nuclear extracts showed that Sp1 and NFκB bound to motifs encompassing two of the three CpG pairs. Interestingly, the methylation of these two CpG sites did not prevent the binding of proteins to the promoter in gel shift analyses. Additionally, mutation of these two CpGs did not affect reporter activity, but mutation of 6-bp fragment spanning each CpG partially inhibited reporter activity, suggesting that these sites were functional. A requirement for both Spi and NFκB in regulating reporter activity was confirmed in transfection experiments using plasmids expressing individual proteins. Our data suggest that the methylation of specific CpG sites can silence the uroplakin Ib promoter, at least in part, by blocking the binding of Sp1 and NFκB, although other factors may be involved. http://www.sciencedirect.com/science/article/pii/S1476558605800466Methylationtranscriptional regulationuroplakin IbSp1NFκB
collection DOAJ
language English
format Article
sources DOAJ
author Prue Cowled
Irene Kanter
Lefta Leonardos
Paul Jackson
spellingShingle Prue Cowled
Irene Kanter
Lefta Leonardos
Paul Jackson
Uroplakin Ib Gene Transcription in Urothelial Tumor Cells Is Regulated by CpG Methylation
Neoplasia: An International Journal for Oncology Research
Methylation
transcriptional regulation
uroplakin Ib
Sp1
NFκB
author_facet Prue Cowled
Irene Kanter
Lefta Leonardos
Paul Jackson
author_sort Prue Cowled
title Uroplakin Ib Gene Transcription in Urothelial Tumor Cells Is Regulated by CpG Methylation
title_short Uroplakin Ib Gene Transcription in Urothelial Tumor Cells Is Regulated by CpG Methylation
title_full Uroplakin Ib Gene Transcription in Urothelial Tumor Cells Is Regulated by CpG Methylation
title_fullStr Uroplakin Ib Gene Transcription in Urothelial Tumor Cells Is Regulated by CpG Methylation
title_full_unstemmed Uroplakin Ib Gene Transcription in Urothelial Tumor Cells Is Regulated by CpG Methylation
title_sort uroplakin ib gene transcription in urothelial tumor cells is regulated by cpg methylation
publisher Elsevier
series Neoplasia: An International Journal for Oncology Research
issn 1476-5586
1522-8002
publishDate 2005-12-01
description Uroplakin Ib is a structural protein on the surface of urothelial cells. Levels of uroplakin Ib mRNA are dramatically reduced or absent in many transitional cell carcinomas, but the molecular mechanisms responsible remain undetermined. Previously, we showed that loss of uroplakin Ib expression correlated with CpG methylation of Sp1/NFκB-binding motifs within the proximal promoter. In this study, we show that reporter activity was completely blocked by the methylation of three CpG pairs in this promoter region. Gel shift analysis using purified proteins or nuclear extracts showed that Sp1 and NFκB bound to motifs encompassing two of the three CpG pairs. Interestingly, the methylation of these two CpG sites did not prevent the binding of proteins to the promoter in gel shift analyses. Additionally, mutation of these two CpGs did not affect reporter activity, but mutation of 6-bp fragment spanning each CpG partially inhibited reporter activity, suggesting that these sites were functional. A requirement for both Spi and NFκB in regulating reporter activity was confirmed in transfection experiments using plasmids expressing individual proteins. Our data suggest that the methylation of specific CpG sites can silence the uroplakin Ib promoter, at least in part, by blocking the binding of Sp1 and NFκB, although other factors may be involved.
topic Methylation
transcriptional regulation
uroplakin Ib
Sp1
NFκB
url http://www.sciencedirect.com/science/article/pii/S1476558605800466
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