Abstract

Tumor suppressor gene inactivation is a crucial event in oncogenesis. Gene inactivation mechanisms include events resulting in loss of heterozygosity (LOH), gene mutation, and transcriptional silencing. The contribution of each of these different pathways varies among tumor suppressor genes and by cancer type. The factors that influence the relative utilization of gene inactivation pathways are poorly understood. In this study, we describe a detailed quantitative analysis of the three major gene inactivation mechanisms for a model gene at two different genomic integration sites in mouse embryonic stem (ES) cells. In addition, we targeted the major DNA methyltransferase gene, Dnmt1, to investigate the relative contribution of DNA methylation to these various competing gene inactivation pathways. Our data show that gene loss is the predominant mode of inactivation of a herpes simplex virus thymidine kinase neomycin phosphotransferase reporter gene (HSV-TKNeo) at the two integration sites tested and that this event is significantly reduced in Dnmt1-deficient cells. Gene silencing by promoter methylation requires Dnmt1, suggesting that the expression of Dnmt3a and Dnmt3b alone in ES cells is insufficient to achieve effective gene silencing. We used a novel assay to show that missense mutation rates are also substantially reduced in Dnmt1-deficient cells. This is the first direct demonstration that DNA methylation affects point mutation rates in mammalian cells. Surprisingly, the fraction of CpG transition mutations was not reduced in Dnmt1-deficient cells. Finally, we show that methyl group-deficient growth conditions do not cause an increase in missense mutation rates in Dnmt1-proficient cells, as predicted by methyltransferase-mediated mutagenesis models. We conclude that Dnmt1 deficiency and the accompanying genomic DNA hypomethylation result in a reduction of three major pathways of gene inactivation in our model system.

Keywords

BiologyDNA methylationGene silencingDNMT1Molecular biologyGene targetingGeneTherapeutic gene modulationTumor suppressor geneGeneticsCarcinogenesisGene expressionGene product

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Year
2001
Type
article
Volume
21
Issue
22
Pages
7587-7600
Citations
66
Access
Closed

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Matilda F. Chan, Renée van Amerongen, Tarlochan Nijjar et al. (2001). Reduced Rates of Gene Loss, Gene Silencing, and Gene Mutation in <i>Dnmt1</i>-Deficient Embryonic Stem Cells. Molecular and Cellular Biology , 21 (22) , 7587-7600. https://doi.org/10.1128/mcb.21.22.7587-7600.2001

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DOI
10.1128/mcb.21.22.7587-7600.2001