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FLASH GENE
Symbol CREBBP contributors: mct/npt/pgu - updated : 21-02-2018
HGNC name CREB binding protein
HGNC id 2348
RNA
TRANSCRIPTS type messenger
identificationnb exonstypebpproduct
ProteinkDaAAspecific expressionYearPubmed
30 - 10083 - 2404 - 1995 7606928
31 - 10197 265 2442 - 1995 7606928
EXPRESSION
Type ubiquitous
   expressed in (based on citations)
organ(s)
SystemOrgan level 1Organ level 2Organ level 3Organ level 4LevelPubmedSpeciesStageRna symbol
Digestivemouthtongue  highly
Hearing/Equilibriumearinnercochlea highly
Lymphoid/Immunelymph node   highly
 thymus    
Reproductivemale systemtestis   
Respiratoryrespiratory tractlarynx  highly
tissue
SystemTissueTissue level 1Tissue level 2LevelPubmedSpeciesStageRna symbol
Blood / Hematopoieticbone marrow   
cell lineage
cell lines
fluid/secretion
at STAGE
physiological period fetal
Text cochlea, pancreas
PROTEIN
PHYSICAL PROPERTIES
STRUCTURE
motifs/domains
  • three cysteine-histidine rich (C4-H-C3) PHD type zinc finger motifs
  • a bromodomain (histone acetyltransferase domain, HAT)
  • a nuclear receptor interaction motif (LXXLL), the KIX domain for interaction with MYB
  • a highly conserved cysteine/histidine-rich region (CH2) domain that with the preceding bromodomain interact and mutually stabilize each other, implying a cooperative function
  • a TAZ1 domain, consisting of four alpha-helices (alpha(1)-alpha(4) stabilized by three zinc atoms (for binding to CITED2)
  • C-terminal domain, SID (SRC1 interacting domain) responsible for interaction with SRC1 (NCOA1), and other transcriptional regulators such as E1A, ETS2, IRF3, and p53
    • HOMOLOGY
    interspecies homolog to murine Crebbp
    homolog to EP300
    Homologene
    FAMILY
    CATEGORY transcription factor , signaling
    SUBCELLULAR LOCALIZATION     intracellular
    intracellular,nucleus,nucleoplasm,nuclear bodies
    intracellular,nucleus,chromatin/chromosome,heterochromosome
    text colocalizing with PML in special (PML/SP100) nuclear bodies (NB/POD)
    basic FUNCTION
  • playing an important role as a general co-integrator of multiple signaling pathways
  • potent histone acetyltransferase
  • transcriptional coactivator with EP300 of various nuclear receptors and hypoxia inducible factor 1A (HIF1A)
  • associating to PML which increases its localization in POD (promyelocytic oncoprotein domain)
  • acting as a potent nuclear receptor coactivator
  • playing a pivotal role in embryonic development
  • involved in a variety of transcriptional pathways through chromatin remodeling (acetylation of histone protein H3)
  • participating in basic cellular functions and acting rarely as classical suppressor of tumor
  • regulator with PCAF of involucrin expression in stratified squamous epithelial cells
  • promoting nucleosome acetylation at NOTCH enhancers and activating transcription via its binding to MAML1
  • dosage-dependent regulator of NFKB1 suppression by the estrogen receptor
  • CREBBP and EP300 function as transcriptional coactivators for a large number of DNA-binding transcription factors involved in multiple signalling and developmental pathways, by modifying lysine residues on both histone and non-histone nuclear proteins
  • histone acetyltransferase involved in mental retardation, in the genesis and maintenance of long-lasting systemic and behavioural adaptations to environmental enrichment (EE)(
  • important role for CREBBP in cognitive dysfunction in Huntington disease
  • CREBBP-dependent transcriptional neuroadaptation is an important mediator of EE-induced benefits, a finding with important implications for mental retardation therapeutics
  • CREBBP and KAT5 coordinate histone acetylation at both local and global levels to facilitate RAS-induced transformation
  • KMT2C/KMT2D and H3K27 acetyltransferases CREBBP/EP300 are major enhancer epigenomic writers
    • CELLULAR PROCESS nucleotide, transcription
    PHYSIOLOGICAL PROCESS
    text
  • MADH4 dependent TGFB transcriptional responses in endothelial cells
    • PATHWAY
    metabolism
    signaling signal transduction
    HH signaling transduction pathway
    a component
  • complexing with CITED2 (CBP/p300-interacting transactivator with ED-rich tail), inhibiting the activity of the hypoxia inducible factor (HIF-1alpha)
    • INTERACTION
    DNA binding to cAMP response element
    RNA
    small molecule
    protein
  • MADH4
  • TGFB
  • N4BP2
  • binding to GLI activators
  • SNIP1
  • MAML1
  • interacts with a large number of transcription factors and co-factors, through its numerous protein-binding domains
  • interacting with TRIP10, ZBTB17, SH3GL1, GAK, EIF2B1 in embryonic orofacial tissue
  • interacting with GATA2(CREBPP could increase GATA2 transcriptional activity in the dose-dependent manner)
  • MAP3K4 controls the activity of the histone acetyltransferase CREBBP, and acetylation of histones H2A and H2B by CREBBP is required to maintain the epithelial phenotype
  • displayed histone H3K9-me1/2 demethylase activity and induced leukemogenic oncogene LMO2 expression via a synergistic interaction with CREBBP
  • CREBBP and EP300 play distinct roles in RA-mediated STRA8 gene transcription
  • KIX domains of CREBBP, and especially EP300, are principal mediators of MYB-dependent gene activation and repression that is required for definitive hematopoiesis
  • TDG, as a new coactivator, promotes CTNNB1/TCFs transactivation and functionally cooperates with CREBBP in canonical WNT signaling
  • CREBBP and EP300 cooperate with several key Treg transcription factors that act on the FOXP3 promoter to promote FOXP3 production
  • destabilization of CREBBP by downregulation of PPP1R13L
    • expression levels appears to represent a molecular mechanism that contributes to chemoresistance in melanoma cells
  • AJUBA recruits CREBBP via its LIM domain and facilitates CREBBP binding to PPARG
  • complex regulation of CREBBP activity by HIPK2, which might be relevant for the control of specific sets of target genes involved in cellular proliferation, differentiation and apoptosis
  • TLX3 directly interacts with the epigenetic co-activator cyclic adenosine monophosphate CREBBP and its homeodomain is essential for this interaction
  • CREBBP regulates lung cancer growth by targeting MAPK and CPSF4 signaling pathways 8)
  • interplay between the remodeling activity of SMARCAD1 and histone acetylation by CREBBP sheds light on the function of chromatin and the genome-integrity network
  • CREBBP and EP300, activate transcription of TP53-regulated stress response genes and stabilize TP53 against ubiquitin-mediated degradation
  • DYRK1A functions in enhancer regulation by interacting with EP300/CREBBP and modulating their activity
    • cell & other
    REGULATION
    activated by CREB and CREM after phosphorylation of respectively Ser133 and Ser 117
    ASSOCIATED DISORDERS
    corresponding disease(s) RSTS , AMLT3
    Other morbid association(s)
    TypeGene ModificationChromosome rearrangementProtein expressionProtein Function
    tumoral fusion      
    with MYST3 in acute myeloid leukemia with translocation t(8;16)(p11;p13), see AML3, and with MLL (HRX) in therapy related acute leukemia with translocation t(11;16)(q23;p13), with MYST4 in AML with t(10;16) (q22;p13)
    tumoral fusion      
    fusion genes MYST3-CREBBP in acute myeloid leukemia (AML) by chromosomal translocation
    tumoral somatic mutation     loss of function
    in B-cell non-Hodgkin lymphoma
    tumoral somatic mutation      
    in relapsed acute lymphoblastic leukaemia, mutations impaired histone acetylation and transcriptional regulation of CREBBP targets, including glucocorticoid responsive genes, and may confer resistance to therapy (
    tumoral somatic mutation      
    in hypothalamic hamartoma with gelastic epilepsy
    Susceptibility
    Variant & Polymorphism
    Candidate gene
    Marker
    Therapy target
    SystemTypeDisorderPubmed
    cancerhemopathy 
    use of histone deacetylase inhibitors has a potential therapy in B-cell non-Hodgkin lymphoma
    cancerhemopathy 
    promising therapeutic targets across multiple subtypes in acute myeloid leukemia
    ANIMAL & CELL MODELS
  • mice with a deletion mutation in the CBP CH1 (TAZ1) domain have an Rubinstein-Taybi Syndrome (RTS)-like phenotype that includes ASD-relevant repetitive behaviors, hyperactivity, social interaction deficits, motor dysfunction, impaired recognition memory, and abnormal synaptic plasticity