2009
DOI: 10.1182/blood-2008-10-182071
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Identification of a myeloid committed progenitor as the cancer-initiating cell in acute promyelocytic leukemia

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Cited by 125 publications
(122 citation statements)
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“…These results are supported by our recent findings in mCG-PR mice, in which we have demonstrated that PML-RARA is expressed and functional in the KLS compartment (Welch et al, unpublished observations). Both results contradict the current paradigm, which suggests that PML-RARA transforms a committed myeloid precursor (i.e., a promyelocyte) by being expressed at that stage of development (26)(27)(28)(29). This is clearly not the case.…”
Section: Discussioncontrasting
confidence: 58%
“…These results are supported by our recent findings in mCG-PR mice, in which we have demonstrated that PML-RARA is expressed and functional in the KLS compartment (Welch et al, unpublished observations). Both results contradict the current paradigm, which suggests that PML-RARA transforms a committed myeloid precursor (i.e., a promyelocyte) by being expressed at that stage of development (26)(27)(28)(29). This is clearly not the case.…”
Section: Discussioncontrasting
confidence: 58%
“…17,29 Recently, in APL leukemic cells a sub-population enriched in leukemia-initiating cells has been identified, which showed simultaneous expression of more The coiled-coil domain of PML drives leukemogenesis M Occhionorelli et al mature differentiation markers (such as, Gr1), and stem cell markers (such as, c-Kit). 30,31 Indeed, PR, CCR and GCR cells recovered from the third plating showed the co-expression of c-Kit/Gr-1 markers (Figure 4b). 1 Taken together, these results indicate that all chimeric proteins showed a similar biological response in vitro, though GCR was unable to interact with PML and disrupt endogenous NBies.…”
Section: Resultsmentioning
confidence: 96%
“…25,26 Indeed this notion is supported by a recent study showing that PML-RARA conduct partial silencing of CEPBA target genes through DNA methylation of its promoter regions. 42 The promoter analysis also showed that genes upregulated in APL cells versus PMs contained a significant enrichment of binding sites for TFs that propagate proliferation, mobilization and self-renewal of HSCs/LSCs. Among these we identified binding sites for NF-kB suggesting that enhanced activation of NF-kB target genes (Supplementary Table 3) might contribute to malignant transformation in APL.…”
Section: Discussionmentioning
confidence: 96%
“…This hypothesis is supported by recent studies showing that LSCs in murine APL models have a morphology and an immunophenotype similar to that of normal PMs. 42,44 To identify drug candidates that might be used as supplements in current APL treatment protocols, we searched for compounds that generated signatures in the HL-60 leukemia cell line, which reversed our APL and stemness signatures and induced an ATRA signature in APL cells. The rationale for this strategy is to identify compounds that inhibit cellular maintenance and self-renewal by downregulation of APL and stemness genes while at the same time promoting differentiation through upregulation of ATRA-dependent genes.…”
Section: Discussionmentioning
confidence: 99%