BAIT

NR3C1

GCCR, GCR, GCRST, GR, GRL

nuclear receptor subfamily 3, group C, member 1 (glucocorticoid receptor)

Alzheimer's Disease Project

GO Process (8)

GO Function (8)

GO Component (4)

Gene Ontology Biological Process

cellular response to steroid hormone stimulus [IDA]

gene expression [TAS]

positive regulation of transcription from RNA polymerase II promoter [IDA]

regulation of transcription, DNA-templated [IDA]

signal transduction [TAS]

transcription from RNA polymerase II promoter [TAS]

transcription initiation from RNA polymerase II promoter [TAS]

transcription, DNA-templated [TAS]

Gene Ontology Molecular Function

RNA polymerase II core promoter proximal region sequence-specific DNA binding [IDA]
RNA polymerase II core promoter proximal region sequence-specific DNA binding transcription factor activity involved in positive regulation of transcription [IDA]
glucocorticoid receptor activity [TAS]
glucocorticoid-activated RNA polymerase II transcription factor binding transcription factor activity [IDA]
protein binding [IPI]
sequence-specific DNA binding transcription factor activity [IDA]
steroid binding [IDA]
steroid hormone binding [IDA]

Gene Ontology Cellular Component

cytoplasm [IDA]

mitochondrial matrix [TAS]

nucleoplasm [IDA, TAS]

CRISPR Database OMIM VEGA HGNC Alliance of Genome Resources Entrez Gene RefSeq UniprotKB Ensembl HPRD

Homo sapiens

PREY

MDM2

ACTFS, HDMX, hdm2

MDM2 proto-oncogene, E3 ubiquitin protein ligase

Glioblastoma Project

GO Process (25)

GO Function (7)

GO Component (9)

Gene Ontology Biological Process

DNA damage response, signal transduction by p53 class mediator resulting in cell cycle arrest [IMP, TAS]

Fc-epsilon receptor signaling pathway [TAS]

cellular response to hypoxia [IEP]

epidermal growth factor receptor signaling pathway [TAS]

establishment of protein localization [IDA]

fibroblast growth factor receptor signaling pathway [TAS]

innate immune response [TAS]

negative regulation of DNA damage response, signal transduction by p53 class mediator [IDA]

negative regulation of cell cycle arrest [IDA]

negative regulation of transcription from RNA polymerase II promoter [IDA]

negative regulation of transcription, DNA-templated [IDA]

neurotrophin TRK receptor signaling pathway [TAS]

peptidyl-lysine modification [IMP]

phosphatidylinositol-mediated signaling [TAS]

positive regulation of cell proliferation [TAS]

positive regulation of mitotic cell cycle [IMP]

positive regulation of proteasomal ubiquitin-dependent protein catabolic process [IDA]

protein complex assembly [IDA]

protein destabilization [IDA]

protein localization to nucleus [IDA]

protein ubiquitination [IDA]

protein ubiquitination involved in ubiquitin-dependent protein catabolic process [IDA]

regulation of protein catabolic process [IDA]

response to antibiotic [IEP]

synaptic transmission [TAS]

Gene Ontology Molecular Function

enzyme binding [IPI]
identical protein binding [IPI]
p53 binding [IPI]
protein binding [IPI]
ubiquitin protein ligase binding [IPI]
ubiquitin-protein transferase activity [IDA, IMP]
zinc ion binding [IDA]

Gene Ontology Cellular Component

cytoplasm [IMP]

endocytic vesicle membrane [TAS]

nuclear body [IDA]

nucleolus [IDA]

nucleoplasm [IDA, TAS]

nucleus [IDA, IMP]

plasma membrane [TAS]

protein complex [IDA]

CRISPR Database HGNC Alliance of Genome Resources OMIM Entrez Gene RefSeq UniprotKB Ensembl HPRD

Homo sapiens

Affinity Capture-Western

An interaction is inferred when a bait protein is affinity captured from cell extracts by either polyclonal antibody or epitope tag and the associated interaction partner identified by Western blot with a specific polyclonal antibody or second epitope tag. This category is also used if an interacting protein is visualized directly by dye stain or radioactivity. Note that this differs from any co-purification experiment involving affinity capture in that the co-purification experiment involves at least one extra purification step to get rid of potential contaminating proteins.

Publication

Ligand-dependent interaction of the glucocorticoid receptor with p53 enhances their degradation by Hdm2.

Sengupta S, Wasylyk B

The glucocorticoid receptor (GR) and the tumor suppressor p53 mediate different stress responses. We have studied the mechanism of their mutual inhibition in normal endothelial cells (HUVEC) in response to hypoxia, a physiological stress, and mitomycin C, which damages DNA. Dexamethasone (Dex) stimulates the degradation of endogenous GR and p53 by the proteasome pathway in HUVEC under hypoxia and mitomycin ... [more]

Genes Dev. Sep. 15, 2001; 15(18);2367-80 [Pubmed: 11562347]

Throughput

Low Throughput

Curated By

BioGRID