2002
DOI: 10.1182/blood.v99.8.2776
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CCAAT/enhancer-binding proteins are required for granulopoiesis independent of their induction of the granulocyte colony-stimulating factor receptor

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Cited by 79 publications
(78 citation statements)
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References 62 publications
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“…Csf3r mRNA expression levels in RP7, RP11, and in five clones expressing RARα-PLZF fused to the tag for tandem affinity purification (RP-TAP15, 19,23,24,33) as well as RP-HA were less than 20% that of parental 32D cells by Northern blotting and/or quantitative RT-PCR analysis ( Fig. 1 D and E).…”
Section: Resultsmentioning
confidence: 99%
“…Csf3r mRNA expression levels in RP7, RP11, and in five clones expressing RARα-PLZF fused to the tag for tandem affinity purification (RP-TAP15, 19,23,24,33) as well as RP-HA were less than 20% that of parental 32D cells by Northern blotting and/or quantitative RT-PCR analysis ( Fig. 1 D and E).…”
Section: Resultsmentioning
confidence: 99%
“…The difference in the role of C/EBPalpha between the adipocyte system and granulocyte system is not clear. Interestingly, C/EBPalpha is required for adipocyte differentiation, whereas in the granulocyte differentiation system C/EBPalpha can be replaced by C/EBPbeta (Popernack et al, 2001;Jones et al, 2002;Wang and Friedman 2002). However, only a low level of C/EBPalpha is sufficient for granulocyte differentiation.…”
Section: -------------------------------------mentioning
confidence: 99%
“…However, in mutated cases with multiple alterations of CEBPA, preventing expression of wt protein, or in single alterations with expression of p30 dominant negative form, the persistence of CEBPA residual cellular functions has been demonstrated. 31,33,34 Therefore, those cases are not identical to KO models since the loss of transactivating properties is dependent of on cis-regulating elements of the CEBPA target genes. Moreover, other members of the CEBPA family, including CEBPB and CEBPE, could partially prevent the effects of the loss of function of mutated CEBPA and allow incomplete myeloid differentiation resulting in M1, M2, M4 and M5 blasts.…”
Section: Pathogenetic Role Of Cebpa Mutationsmentioning
confidence: 99%
“…It has previously been reported that biallelic mutations of another early myeloid differentiation gene (AML1/ RUNX1) could induce M0 AML subtype. 2 Furthermore, mice models of CML blast crisis with CEBPA knockout result in immature erythroid leukemia 30,31 and expression of a dominant negative 30-kDa CEBPA protein inhibits differentiation of myeloid and erythroid progenitors. 32 On the other hand, all CEBPAmutated patients reviewed in this work had M1, M2, M4 or M5 AML subtypes, clearly showing persistence of myeloid differentiation in blast cells.…”
Section: Pathogenetic Role Of Cebpa Mutationsmentioning
confidence: 99%