Abstract

We have recently discovered relaxation of genomic imprinting in cancer, a novel type of genomic alteration in man. Genomic imprinting is a differential modification of maternal and paternal alleles in the gamete, leading to expression of a single allele in the offspring, depending on its sex of origin. While genomic imprinting has been demonstrated at the molecular level in insects and mice and suspected to play a role in human disease, there previously has been no direct molecular evidence for imprinted genes in man. We have established that two genes, the insulin- like growth factor II gene (IGF2) and a nearby gene, H19, are reciprocally imprinted in man. Thus, only the paternally derived IGF2 allele and the maternally derived Hl9 allele are expressed in human tissues. Surprisingly, we found that in two childhood tumors, Wilms tumor and rhabdoid tumor, these imprints are relaxed and both copies of the genes are expressed. This alteration occurred in the earliest stages of tumorigenesis. In order to understand the role of relaxation or loss of imprinting (LOI) in human carcinogenesis, we will determine its prevalence in two groups of tumors: childhood cancers that express IGF2 and/or Hl9; and a subset of common adult cancers in which IGF2 has been proposed to play an autocrine growth stimulatory role, such as colorectal and breast cancer. As our preliminary data include the first demonstration of normally imprinted genes in man, we will attempt to identify other imprinted genes, using as a guide regions suggested by homology to known imprinted domains in mouse, and we will determine whether these genes also undergo relaxation of imprinting in cancer. We will also determine whether LOI is related to deregulated gene expression in cancer. We earlier discovered widespread alterations of DNA methylation in malignant and premalignant tumors, and DNA methylation has been tentatively linked to genomic imprinting in other organisms. We will investigate the molecular mechanism of LOI by determining whether it is related to specific changes in DNA methylation, and by attempting to modify the pattern of genomic imprinting in vitro with 5-azacytidine, a drug that causes loss of DNA methylation. Finally, in order to determine whether LOI is potentially reversible, which could have important therapeutic implications, we will attempt to restore the pattern of imprinting by genetic complementation. These studies should provide a foundation for understanding the role of normal genomic imprinting in man and the consequences of altered imprinting in cancer.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA065145-02
Application #
2107954
Study Section
Chemical Pathology Study Section (CPA)
Project Start
1994-04-01
Project End
1997-03-31
Budget Start
1995-04-01
Budget End
1996-03-31
Support Year
2
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
Johns Hopkins University
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
045911138
City
Baltimore
State
MD
Country
United States
Zip Code
21218

  Publications

Noren, David P; Chou, Wesley H; Lee, Sung Hoon et al. (2016) Endothelial cells decode VEGF-mediated Ca2+ signaling patterns to produce distinct functional responses. Sci Signal 9:ra20
Brennan, Matthew D; Cheong, Raymond; Levchenko, Andre (2012) Systems biology. How information theory handles cell signaling and uncertainty. Science 338:334-5
Feinberg, Andrew P (2010) Genome-scale approaches to the epigenetics of common human disease. Virchows Arch 456:13-21
Mirsaidov, U; Timp, W; Zou, X et al. (2009) Nanoelectromechanics of methylated DNA in a synthetic nanopore. Biophys J 96:L32-4
Cheong, Raymond; Wang, Chiaochun Joanne; Levchenko, Andre (2009) High content cell screening in a microfluidic device. Mol Cell Proteomics 8:433-42
Timp, Winston; Levchenko, Andre; Feinberg, Andrew P (2009) A new link between epigenetic progenitor lesions in cancer and the dynamics of signal transduction. Cell Cycle 8:383-90
Cheong, Raymond; Wang, Chiaochun Joanne; Levchenko, Andre (2009) Using a microfluidic device for high-content analysis of cell signaling. Sci Signal 2:pl2
Cruz-Correa, Marcia; Zhao, Ronghua; Oviedo, Myriam et al. (2009) Temporal stability and age-related prevalence of loss of imprinting of the insulin-like growth factor-2 gene. Epigenetics 4:114-8
Sun, Lunching; Huang, Lei; Nguyen, Phuongmai et al. (2008) DNA methyltransferase 1 and 3B activate BAG-1 expression via recruitment of CTCFL/BORIS and modulation of promoter histone methylation. Cancer Res 68:2726-35
Nguyen, Phuongmai; Cui, Hengmi; Bisht, Kheem S et al. (2008) CTCFL/BORIS is a methylation-independent DNA-binding protein that preferentially binds to the paternal H19 differentially methylated region. Cancer Res 68:5546-51

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