Methylation-independent silencing of the p73 gene in neuroblastoma

Open Access

14 September 2000

journal article
research article
Published by Springer Nature in Oncogene

Vol. 19 (39) , 4553-4556
https://doi.org/10.1038/sj.onc.1203807

Abstract

p73 is a p53 homolog that, in vitro, inhibits cell growth and induce apoptosis. In some tumors p73 is monoallelically expressed and this raised the possibility that this gene is subjected to imprinting. Silencing of p73 in acute leukemia and in Burkitt's lymphoma occurs in association with the aberrant methylation of the first exon of the gene. We have analysed the methylation pattern of the p73 promoter and of upstream and downstream sequences in neuroblastoma. Our results demonstrate that p73 expression in this tumor is not regulated by methylation. We concluded that it is unlikely that p73 is imprinted in neuroblastoma and that the methylation-dependent silencing of this gene, thus far, is a characteristic of hematologic malignancies.

Keywords

This publication has 15 references indexed in Scilit:

The p53 gene family
Oncogene, 1999
Stage-independent expression and genetic analysis oftp73 in neuroblastoma
International Journal of Cancer, 1999
Identification of Unique Fragments in Overlapping Large-Insert Clones by Subtraction through Representational Difference Analysis
Analytical Biochemistry, 1999
The Emerging p53 Gene Family
JNCI Journal of the National Cancer Institute, 1999
Cancer-epigenetics comes of age
Nature Genetics, 1999
p73 at chromosome 1p36.3 is lost in advanced stage neuroblastoma but its mutation is infrequent
Oncogene, 1999
Loss of imprinting and allele switching of p73 in renal cell carcinoma
Oncogene, 1998
GENOMIC IMPRINTING IN MAMMALS
Annual Review of Genetics, 1997
Methylation-specific PCR: a novel PCR assay for methylation status of CpG islands.
Proceedings of the National Academy of Sciences, 1996
Epigenetic mechanisms underlying the imprinting of the mouse H19 gene.
Genes & Development, 1993