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Publication : T-ALL leukemia stem cell 'stemness' is epigenetically controlled by the master regulator SPI1.

First Author  Zhu H Year  2018
Journal  Elife Volume  7
PubMed ID  30412053 Mgi Jnum  J:309358
Mgi Id  MGI:6757547 Doi  10.7554/eLife.38314
Citation  Zhu H, et al. (2018) T-ALL leukemia stem cell 'stemness' is epigenetically controlled by the master regulator SPI1. Elife 7:e38314
abstractText  Leukemia stem cells (LSCs) are regarded as the origins and key therapeutic targets of leukemia, but limited knowledge is available on the key determinants of LSC 'stemness'. Using single-cell RNA-seq analysis, we identify a master regulator, SPI1, the LSC-specific expression of which determines the molecular signature and activity of LSCs in the murine Pten-null T-ALL model. Although initiated by PTEN-controlled beta-catenin activation, Spi1 expression and LSC 'stemness' are maintained by a beta-catenin-SPI1-HAVCR2 regulatory circuit independent of the leukemogenic driver mutation. Perturbing any component of this circuit either genetically or pharmacologically can prevent LSC formation or eliminate existing LSCs. LSCs lose their 'stemness' when Spi1 expression is silenced by DNA methylation, but Spi1 expression can be reactivated by 5-AZ treatment. Importantly, similar regulatory mechanisms may be also present in human T-ALL.
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