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Publication Date: 10 Feb 2008
Journal: Translational Oncogenomics
Citation: Translational Oncogenomics 2008:3 15-20
1Department of Hematology, Aker University Hospital, University of Oslo, Norway. 2Department of Hematology, Rikshospital and Radium Hospital, University of Oslo, Norway. 3,5The National Norwegian Cancer Registry, Oslo, Norway. 4Department of Biostatistics, Faculty of Mathematics, University of Oslo, Norway.
Abstract
Based on the concept that the tumorogenesis in chronic lymphocytic leukaemia comprises both an initial, inherited mutation and subsequent somatic mutations, the pleiotypic diversity of familial chronic lymphocytic leukaemia and related malignant lymphoproliferative disorders is generally explained by a repertoire of monoallelic polygenes in the initial mutation. Epigenetic genomic imprinting is a likely mechanism behind of the asynchroneous replicating monoallelic polygenes which is discussed in the light of pleiotrophy and birth order effect. Furthermore, it is discussed that one possible mechanism available for the epigenetic transfer of these genes could be the physiological pregnancy-related microchimerism between mother and fetus.
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As an author of a review published in Translational Oncogenomics, I was impressed by the prompt processing and speed of publication. The entire submission, review and publication process was easy, quick and pleasant. The comments from reviewers and associate editor were high quality, scientifically deep and objective. It was a great pleasure to cooperate with such qualified and friendly team. I highly recommend publication in Libertas Academica journals.
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