Pancreatic insulin-producing beta-cells have a long lifespan, such that in healthy conditions they replicate little during a lifetime. Nevertheless, they show increased self-duplication after increased metabolic demand or after injury (that is, beta-cell loss). It is not known whether adult mammals can differentiate (regenerate) new beta-cells after extreme, total beta-cell loss, as in diabetes. This would indicate differentiation from precursors or another heterologous (non-beta-cell) source. Here we show beta-cell regeneration in a transgenic model of diphtheria-toxin-induced acute selective near-total beta-cell ablation. If given insulin, the mice survived and showed beta-cell mass augmentation with time. Lineage-tracing to label the glucagon-producing alpha-cells before beta-cell ablation tracked large fractions of regenerated beta-cells as deriving from alpha-cells, revealing a previously disregarded degree of pancreatic cell plasticity. Such inter-endocrine spontaneous adult cell conversion could be harnessed towards methods of producing beta-cells for diabetes therapies, either in differentiation settings in vitro or in induced regeneration.
Conversion of adult pancreatic alpha-cells to beta-cells after extreme beta-cell loss.
成人胰腺α细胞在β细胞严重丢失后转化为β细胞
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作者:Thorel Fabrizio, Népote Virginie, Avril Isabelle, Kohno Kenji, Desgraz Renaud, Chera Simona, Herrera Pedro L
| 期刊: | Nature | 影响因子: | 48.500 |
| 时间: | 2010 | 起止号: | 2010 Apr 22; 464(7292):1149-54 |
| doi: | 10.1038/nature08894 | 研究方向: | 细胞生物学 |
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