Publication | Open Access
p53 Suppresses c-Myb-induced trans-Activation and Transformation by Recruiting the Corepressor mSin3A
12
Citations
41
References
2004
Year
P53 RecruitmentTranscriptional RegulationSignaling PathwayCell RegulationMolecular RegulationCorepressor Msin3aMedicineM1 CellsGene ExpressionOncogenic AgentC-myb-induced Trans-activationTarget GenesTumor SuppressorSystems BiologyCancer BiologyCell BiologyCell SignalingTumor Biology
p53 is known to repress transcription of a number of genes, but the mechanism of p53 recruitment to these target genes is unknown. The c-myb proto-oncogene product (c-Myb) positively regulates proliferation of immature hematopoietic cells, whereas p53 blocks cell cycle progression. Here, we demonstrate that p53 inhibits c-Myb-induced transcription and transformation by directly binding to c-Myb. The ability of c-Myb to maintain the undifferentiated state of M1 cells was also suppressed by p53. p53 did not affect the ability of c-Myb to bind to DNA but formed a ternary complex with the corepressor mSin3A and c-Myb. Thus, p53 antagonizes c-Myb by recruiting mSin3A to down-regulate specific Myb target genes.
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