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Artículo
Molecular basis of FIR-mediated c-myc transcriptional control
Autor/es | Cukier, Cyprian D.
Hollingworth, David Martin, Stephen Kelly, Geoff Díaz Moreno, Irene Ramos, Andrés |
Departamento | Universidad de Sevilla. Departamento de Bioquímica Vegetal y Biología Molecular |
Fecha de publicación | 2010 |
Fecha de depósito | 2019-03-26 |
Publicado en |
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Resumen | The far upstream element (FUSE) regulatory system promotes a peak in the concentration of c-Myc during cell cycle. First, the FBP transcriptional activator binds to the FUSE DNA element upstream of the c-myc promoter. Then, ... The far upstream element (FUSE) regulatory system promotes a peak in the concentration of c-Myc during cell cycle. First, the FBP transcriptional activator binds to the FUSE DNA element upstream of the c-myc promoter. Then, FBP recruits its specific repressor (FIR), which acts as an on/off transcriptional switch. Here we describe the molecular basis of FIR recruitment, showing that the tandem RNA recognition motifs of FIR provide a platform for independent FUSE DNA and FBP protein binding and explaining the structural basis of the reversibility of the FBP-FIR interaction. We also show that the physical coupling between FBP and FIR is modulated by a flexible linker positioned sequentially to the recruiting element. Our data explain how the FUSE system precisely regulates c-myc transcription and suggest that a small change in FBP-FIR affinity leads to a substantial effect on c-Myc concentration. |
Identificador del proyecto | U117574558 |
Cita | Cukier, C.D., Hollingworth, D., Martin, S., Kelly, G., Díaz Moreno, I. y Ramos, A. (2010). Molecular basis of FIR-mediated c-myc transcriptional control. Nature Structural and Molecular Biology, 17 (9), 1058-1064. |
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Molecular basis of FIR.pdf | 1.574Mb | [PDF] | Ver/ | |