Journal
EPIGENOMICS
Volume 1, Issue 2, Pages 261-280Publisher
FUTURE MEDICINE LTD
DOI: 10.2217/EPI.09.19
Keywords
cancer stem cells; chromatin modifications; DNA methylation; epigenetics; histone modifications; microRNAs; pluripotency; stemness
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Funding
- National Institutes of Health/National Cancer Institute (NIHINCI), United States
- Association pour la Recherche sur le Cancer (ARC), France
- la Ligue Nationale (Francaise) Contre le Cancer. France
- European Network of Excellence Environmental Cancer Risk, Nutrition and Individual Susceptibility (ECNIS)
- Agence Nationale de Recherhe Contre le Sida et Hepatites Virales (ANRS, France)
- Swiss Bridge Award
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The physiological properties of pluripotency in stem cells and the processes of cell specialization are governed by epigenetic mechanisms, as they are inheritable but not dependent on the cell genotype. There is cumulating evidence demonstrating the presence of cells with stem cell properties within tumors, suggesting that these cells are responsible for tumor growth and heterogeneity. As epigenetic control of self-renewal and pluripotency is a hallmark of stem cells, there is increased interest in studying similar epigenetic mechanisms governing these sternness properties in cancer stem cells. Here we will review the evidence supporting a role for epigenetic mechanisms in the induction of cancer stem cells, with an emphasis on the epigenetic regulatory networks involved in the establishment of normal self-renewal and pluripotency, and their potential deregulation in cancer. We will also discuss the data supporting the plasticity of these mechanisms and its potential therapeutic implications.
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