Differential methylation pattern of the X-linked lymphoproliferative (XLP) disease gene SH2D1A correlates with the cell lineage-specific transcription

被引:0
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作者
Ornella Parolini
Andreas Weinhäusel
Birgit Kagerbauer
Joachim Sassmann
Wolfgang Holter
Helmut Gadner
Oskar A. Haas
Walter Knapp
机构
[1] University of Vienna,Institute of Immunology
[2] Ospedale Poliambulanza,Centro Ricerche, Parco Scientifico "E. Menni"
[3] St.Anna Children's Hospital,Children's University Hospital
[4] Friedrich Alexander University Erlangen-Nürnberg,undefined
来源
Immunogenetics | 2003年 / 55卷
关键词
DNA methylation; CpG; SH2D1A; XLP; Tissue-specific expression;
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摘要
SH2D1A, the X-linked lymphoproliferative disease (XLP) gene, encodes a cytoplasmic protein that plays an essential role in controlling Epstein-Barr virus infection. It is expressed in T and NK cells, but not in B cells or in granulocytes. The promoter, the regulatory regions, as well as the mechanisms controlling its tissue-specific expression, are still unknown. We tested the hypothesis that DNA methylation might contribute to tissue-specific SH2D1A gene expression and analyzed the methylation status of 2,300 bp upstream of the ATG starting codon, the coding region and part of intron 1. By bisulfite sequencing and methylation-sensitive restriction enzyme digestion, we show that a differential methylation pattern of CpG-rich regions in the 5′ region and the adjacent exon 1 of the SH2D1A gene indeed correlates with the tissue-specific gene transcription.
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页码:116 / 121
页数:5
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