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Role of the C-terminal binding protein PXDLS motif binding cleft in protein interactions and transcriptional repression
- Source :
- Molecular and cellular biology, 26 (2006): 8202–8213., info:cnr-pdr/source/autori:Quinlan, KGR; Verger, A; Kwok, A; Lee, SHY; Perdomo, J; Nardini, M; Bolognesi, M; Crossley, M/titolo:Role of the C-terminal binding protein PXDLS motif binding cleft in protein interactions and transcriptional repression/doi:/rivista:Molecular and cellular biology (Print)/anno:2006/pagina_da:8202/pagina_a:8213/intervallo_pagine:8202–8213/volume:26
- Publication Year :
- 2006
- Publisher :
- American Society for Microbiology, [Washington, D.C.] , Stati Uniti d'America, 2006.
-
Abstract
- C-terminal binding proteins (CtBPs) are multifunctional proteins that can mediate gene repression. CtBPs contain a cleft that binds Pro-X-Asp-Leu-Ser (PXDLS) motifs. PXDLS motifs occur in numerous transcription factors and in effectors of gene repression, such as certain histone deacetylases. CtBPs have been depicted as bridging proteins that self-associate and link PXDLS-containing transcription factors to PXDLS-containing chromatin-modifying enzymes. CtBPs also recruit effectors that do not contain recognizable PXDLS motifs. We have investigated the importance of the PXDLS binding cleft to CtBP's interactions with various partner proteins and to its ability to repress transcription. We used CtBP cleft mutant and cleft-filled fusion derivatives to distinguish between partner proteins that bind in the cleft and elsewhere on the CtBP surface. Functional assays demonstrate that CtBP mutants that carry defective clefts retain repression activity when fused to beterollogous DNA-binding domains. This result suggests that the cleft is not essential for recruiting effectors. In contrast, when tested in the absence of a fused DNA-binding domain, disruption of the cleft abrogates repression activity. These results demonstrate that the PXDLS binding cleft is functionally important but suggest that it is primarily required for localization of the CtBP complex to promoter-bound transcription factors.
- Subjects :
- family
Transcription, Genetic
Protein Conformation
Recombinant Fusion Proteins
Molecular Sequence Data
domain
Plasma protein binding
Biology
DNA-binding protein
Protein–protein interaction
Mice
ADENOVIRUS E1A
Protein structure
Transcription (biology)
Two-Hybrid System Techniques
ikaros
Settore BIO/10 - Biochimica
kruppel
Animals
Amino Acid Sequence
Binding site
Molecular Biology
Psychological repression
Transcription factor
RANGE REPRESSORS
Genetics
ZINC-FINGER PROTEIN
Binding Sites
MOLECULAR-CLONING
Articles
Cell Biology
Phosphoproteins
gene-expression
Cell biology
DNA-Binding Proteins
Alcohol Oxidoreductases
Gene Expression Regulation
COREPRESSOR CTBP
NIH 3T3 Cells
zinc-finger protein
corepressor ctbp
adenovirus e1a
molecular-cloning
range repressors
Co-Repressor Proteins
Protein Binding
Subjects
Details
- Database :
- OpenAIRE
- Journal :
- Molecular and cellular biology, 26 (2006): 8202–8213., info:cnr-pdr/source/autori:Quinlan, KGR; Verger, A; Kwok, A; Lee, SHY; Perdomo, J; Nardini, M; Bolognesi, M; Crossley, M/titolo:Role of the C-terminal binding protein PXDLS motif binding cleft in protein interactions and transcriptional repression/doi:/rivista:Molecular and cellular biology (Print)/anno:2006/pagina_da:8202/pagina_a:8213/intervallo_pagine:8202–8213/volume:26
- Accession number :
- edsair.doi.dedup.....7ddf3b52dfde571d3bff5a0b50358c1e