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Publication : The ploidy conveyor of mature hepatocytes as a source of genetic variation.

First Author  Duncan AW Year  2010
Journal  Nature Volume  467
Issue  7316 Pages  707-10
PubMed ID  20861837 Mgi Jnum  J:232920
Mgi Id  MGI:5780456 Doi  10.1038/nature09414
Citation  Duncan AW, et al. (2010) The ploidy conveyor of mature hepatocytes as a source of genetic variation. Nature 467(7316):707-10
abstractText  Mononucleated and binucleated polyploid hepatocytes (4n, 8n, 16n and higher) are found in all mammalian species, but the functional significance of this conserved phenomenon remains unknown. Polyploidization occurs through failed cytokinesis, begins at weaning in rodents and increases with age. Previously, we demonstrated that the opposite event, ploidy reversal, also occurs in polyploid hepatocytes generated by artificial cell fusion. This raised the possibility that somatic 'reductive mitoses' can also happen in normal hepatocytes. Here we show that multipolar mitotic spindles form frequently in mouse polyploid hepatocytes and can result in one-step ploidy reversal to generate offspring with halved chromosome content. Proliferating hepatocytes produce a highly diverse population of daughter cells with multiple numerical chromosome imbalances as well as uniparental origins. Our findings support a dynamic model of hepatocyte polyploidization, ploidy reversal and aneuploidy, a phenomenon that we term the 'ploidy conveyor'. We propose that this mechanism evolved to generate genetic diversity and permits adaptation of hepatocytes to xenobiotic or nutritional injury.
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