The dynamic DNA methylomes of double-stranded DNA viruses associated with human cancer

  1. Agustin F. Fernandez1,2,
  2. Cecilia Rosales1,
  3. Pilar Lopez-Nieva1,
  4. Osvaldo Graña3,
  5. Esteban Ballestar1,
  6. Santiago Ropero1,
  7. Jesus Espada1,
  8. Sonia A. Melo1,
  9. Amaia Lujambio1,
  10. Mario F. Fraga1,
  11. Irene Pino1,
  12. Biola Javierre1,
  13. Francisco J. Carmona1,2,
  14. Francesco Acquadro4,
  15. Renske D.M. Steenbergen5,
  16. Peter J.F. Snijders5,
  17. Chris J. Meijer5,
  18. Pascal Pineau6,
  19. Anne Dejean6,
  20. Belen Lloveras7,
  21. Gabriel Capella7,
  22. Josep Quer8,
  23. Maria Buti8,
  24. Juan-Ignacio Esteban8,
  25. Helena Allende9,
  26. Francisco Rodriguez-Frias10,
  27. Xavier Castellsague11,
  28. Janos Minarovits12,
  29. Jordi Ponce13,
  30. Daniela Capello14,
  31. Gianluca Gaidano14,
  32. Juan Cruz Cigudosa4,
  33. Gonzalo Gomez-Lopez3,15,
  34. David G. Pisano3,
  35. Alfonso Valencia3,
  36. Miguel Angel Piris16,
  37. Francesc X. Bosch11,
  38. Ellen Cahir-McFarland17,
  39. Elliott Kieff17,18 and
  40. Manel Esteller1,2,19,20
  1. 1Cancer Epigenetics Group, Spanish National Cancer Research Centre (CNIO), Madrid E-28029, Spain;
  2. 2Cancer Epigenetics and Biology Program, Bellvitge Institute for Biomedical Research-Catalan Institute of Oncology (IDIBELL-ICO), Barcelona, Catalonia 08907, Spain;
  3. 3Bioinformatics Unit and Structural Biology and Biocomputing Programme, Spanish National Cancer Research Centre, Madrid E-28029, Spain;
  4. 4Molecular Cytogenetics Group and CIBERER, Human Cancer Genetics Programme, Spanish National Cancer Research Centre, Madrid E-28029, Spain;
  5. 5Department of Pathology, Unit of Molecular Pathology, Vrije Universiteit Medical Center, Amsterdam 1007 MB, The Netherlands;
  6. 6Nuclear Organization and Oncogenesis Unit, INSERM U579, Pasteur Institute, Paris 75724, France;
  7. 7Translational Research Laboratory, Catalan Institute of Oncology (ICO), Barcelona, Catalonia 08907, Spain;
  8. 8Liver Unit, Department of Medicine, Hospital Vall Hebron, and Universitat Autonoma Barcelona and CIBEREHD, Barcelona 08035, Spain;
  9. 9Pathology Department, Hospital Vall Hebron, Barcelona 08035, Spain;
  10. 10Departament Bioquimica, Hospital Vall Hebron and CIBEREHD, Barcelona 08035, Spain;
  11. 11Service of Epidemiology and Cancer Register, Catalan Institute of Oncology (ICO), Barcelona, Catalonia 08907, Spain;
  12. 12Microbiological Reseach Group, National Center for Epidemiology, Budapest 1529, Hungary;
  13. 13Service of Gynecology, Hospital Universitari de Bellvitge, L'Hospitalet, Catalonia 08907, Spain;
  14. 14Division of Hematology, Department of Clinical and Experimental Medicine and Department of Oncology, Amedeo Avogadro University of Eastern Piedmont, Vercelli, Alessandria, Novara 13100, Italy;
  15. 15Biomedical Foundation Complexo Hospitalario, Universitario de Vigo (CHUVI), Vigo 36211, Spain;
  16. 16Lymphoma Group, Molecular Pathology Programme, Spanish National Cancer Research Centre, Madrid E-28029, Spain;
  17. 17Departments of Medicine, Microbiology, and Molecular Genetics, Harvard University, Boston, Massachusetts 02115, USA;
  18. 18Infectious Disease Division, Brigham and Women's Hospital, Boston, Massachusetts 02115, USA;
  19. 19Institucio Catalana de Recerca i Estudis Avançats (ICREA), Barcelona 08010, Spain

    Abstract

    The natural history of cancers associated with virus exposure is intriguing, since only a minority of human tissues infected with these viruses inevitably progress to cancer. However, the molecular reasons why the infection is controlled or instead progresses to subsequent stages of tumorigenesis are largely unknown. In this article, we provide the first complete DNA methylomes of double-stranded DNA viruses associated with human cancer that might provide important clues to help us understand the described process. Using bisulfite genomic sequencing of multiple clones, we have obtained the DNA methylation status of every CpG dinucleotide in the genome of the Human Papilloma Viruses 16 and 18 and Human Hepatitis B Virus, and in all the transcription start sites of the Epstein-Barr Virus. These viruses are associated with infectious diseases (such as hepatitis B and infectious mononucleosis) and the development of human tumors (cervical, hepatic, and nasopharyngeal cancers, and lymphoma), and are responsible for 1 million deaths worldwide every year. The DNA methylomes presented provide evidence of the dynamic nature of the epigenome in contrast to the genome. We observed that the DNA methylome of these viruses evolves from an unmethylated to a highly methylated genome in association with the progression of the disease, from asymptomatic healthy carriers, through chronically infected tissues and pre-malignant lesions, to the full-blown invasive tumor. The observed DNA methylation changes have a major functional impact on the biological behavior of the viruses.

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    1. Published in Advance February 10, 2009, doi: 10.1101/gr.083550.108 Genome Res. 19: 438-451 Copyright © 2009 by Cold Spring Harbor Laboratory Press

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