Abstract

BackgroundNasopharyngeal carcinoma (NPC) is a head and neck malignancy with high occurrence in South-East Asia and Southern China. Recent findings suggest that epigenetic inactivation of multiple tumor suppressor genes plays an important role in the tumourigenesis of NPC. BRD7 is a NPC-associated bromodomain gene that exhibits a much higher-level of mRNA expression in normal than in NPC biopsies and cell lines. In this study, we explored the role of DNA methylation in regulation of BRD7 transcription.MethodsThe presence of CpG islands within BRD7 promoter was predicted by EMBOSS CpGplot and Softberry CpGFinder, respectively. Nested methylation-specific PCR and RT-PCR were employed to detect the methylation status of BRD7 promoter and the mRNA expression of BRD7 gene in tumor cell lines as well as clinical samples. Electrophoretic mobility shift assays (EMSA) and luciferase assay were used to detect the effects of cytosine methylation on the nuclear protein binding to BRD7 promoter.ResultsWe found that DNA methylation suppresses BRD7 expression in NPC cells. In vitro DNA methylation in NPC cells silenced BRD7 promoter activity and inhibited the binding of the nuclear protein (possibly Sp1) to Sp1 binding sites in the BRD7 promoter. In contrast, inhibition of DNA methylation augments induction of endogenous BRD7 mRNA in NPC cells. We also found that methylation frequency of BRD7 promoter is much higher in the tumor and matched blood samples from NPC patients than in the blood samples from normal individuals.ConclusionBRD7 promoter demethylation is a prerequisite for high level induction of BRD7 gene expression. DNA methylation of BRD7 promoter might serve as a diagnostic marker in NPC.

Highlights

  • Nasopharyngeal carcinoma (NPC) is a head and neck malignancy with high occurrence in South-East Asia and Southern China

  • Down-regulation of BRD7 gene expression in NPC cells is due to partly methylation of BRD7 promoter Previous studies have shown that BRD7 was down-regulated in NPC biopsies and NPC cell lines [11]

  • Genomic DNA obtained from various cell lines was treated with sodium bisulfite under conditions where cytosines are converted to uracils, while methylated cytosines remain unmodified

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Summary

Introduction

Nasopharyngeal carcinoma (NPC) is a head and neck malignancy with high occurrence in South-East Asia and Southern China. NPC is a head and neck malignancy with high occurrence in South-East Asia and Southern China [1,2] The development of this EBV-associated cancer may involve cumulative genetic and epigenetic changes in a background of predisposed genetic and environmental factors [3,4]. The methylation frequency of BRD7 promoter is much higher in the tumor and matched blood samples from NPC patients than that in the blood samples from normal individuals. These results will be helpful in further understanding the transcription-repression mechanism of the BRD7 gene in NPC cells and the establishment of noninvasive approach in the early detection and surveillance of NPC

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