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FLASH GENE
Symbol DGCR8 contributors: mct/npt/pgu - updated : 19-04-2017
HGNC name microprocessor complex subunit
HGNC id 2847
EXPRESSION
Type ubiquitous
   expressed in (based on citations)
organ(s)
SystemOrgan level 1Organ level 2Organ level 3Organ level 4LevelPubmedSpeciesStageRna symbol
Nervousbrainforebraincerebral cortex highly Homo sapiens
cell lineage
cell lines
fluid/secretion
at STAGE
physiological period fetal
Text
  • eye lens, anterior segment, retina, choroid
  • expressed in the developing cortex
  • PROTEIN
    PHYSICAL PROPERTIES
    STRUCTURE
    motifs/domains
  • two double-stranded RNA binding motifs (DSRM)
  • two WW motifs
  • a heme-binding domain (HBD, AAs 276–498), with a dimerization domain embedded in an independently folded heme-binding domain and directly contributing to association with heme
  • HOMOLOGY
    interspecies homolog to rattus LOC287954
    Homologene
    FAMILY
    CATEGORY RNA associated
    SUBCELLULAR LOCALIZATION     intracellular
    intracellular,cytoplasm,cytosolic
    intracellular,cytoplasm,cytoskeleton,microtubule
    intracellular,nucleus,nucleoplasm,nuclear bodies,nuclear speckles
    intracellular,nucleus,nucleolus
    text
  • locates at the nucleolus and small foci adjacent to splicing speckles in the nucleoplasm (localization of DGCR8 at the nucleolus was changed by the inhibition of RNA transcription)
  • basic FUNCTION
  • essential for biogenesis of miRNAs, functioning in the silencing of embryonic stem cell self-renewal that normally occurs with the induction of differentiation
  • recognizes primary microRNA (pre-miRNA) in two possible orientations
  • stabilizes the RNASEN (Drosha) protein via protein-protein interaction
  • component of the "microprocessor" complex that is essential for microRNA production, resulting in abnormal processing of specific brain miRNAs and working memory deficits
  • novel heme-binding protein with two cysteine side chains as axial ligands
  • native DGCR8 binds heme when expressed in eukaryotic cells
  • RNA-binding protein required for microRNA biogenesis
  • is required for vascular development through the regulation of vascular smooth muscle cells (VSMCs) proliferation, apoptosis, and differentiation
  • DGCR8-dependent miRs are indispensable for osteoclastic control of bone metabolism
  • is likely responsible for modulation of gene expression programs underlying myelin formation and maintenance as well as suppression of an injury-related gene expression program
  • acts likely as an adaptor to recruit the exosome complex to structured RNAs and induce their degradation
  • DGCR8 is an RNA-binding protein that interacts with DROSHA to produce pre-microRNA in the nucleus, while DICER generates not only mature microRNA, but also endogenous small interfering RNAs in the cytoplasm
  • noncanonical function of DGCR8 in the modulation of the alternative splicing of TCF7L1 mRNA in addition to its established function in microRNA biogenesis
  • RNA binding protein that canonically functions with DROSHA to mediate microRNA processing, in the repair of UV-induced DNA lesions
  • CELLULAR PROCESS
    PHYSIOLOGICAL PROCESS
    PATHWAY
    metabolism
    signaling
  • general DROSHA-independent DGCR8/Pasha pathway that promotes proper morphology in multiple neuronal lineages
  • a component
  • RNASEN -DGCR8 complex, also known as Microprocessor, is essential for microRNA (miRNA) maturation, and functioning in mRNA stability control
  • component of the microprocessor complex essential for microRNA production, resulting in abnormal processing of specific brain miRNAs and working memory deficits
  • intricate relationship between DGCR8 and DROSHA in which both proteins are required for binding and processing
  • INTERACTION
    DNA
    RNA binding, binds RNA nonspecifically
    small molecule
    protein
  • crossregulation between RNASEN and DGCR8 may contribute to the homeostatic control of miRNA biogenesis
  • interacting with Nucleolin, ILF3 and others, most of which appeared to be involved in the RNA processing or RNA transportation
  • binds heme through a heme-binding domain (HBD, amino acids 276–498) that can be expressed in a soluble, heme-bound form in the absence of other domains
  • heme may bind and activate DGCR8 while the signal is turned off through protein degradation
  • caspases cleave and inhibit the microRNA processing DGCR8
  • DGCR8 is a direct interactor of TCF7L1 mRNA, a core component of the pluripotency network
  • physically interacted with ERCC6 and RNA polymerase II
  • DROSHA interacts with its cofactor DGCR8 to form the Microprocessor complex, which initiates microRNA (miRNA) maturation by cleaving hairpin structures embedded in primary transcripts
  • cell & other
    REGULATION
    repressed by negatively regulated by the RNASEN-DGCR8 complex through mRNA cleavage
    ASSOCIATED DISORDERS
    corresponding disease(s) DEL22Q11 , DUP22Q11
    Other morbid association(s)
    TypeGene ModificationChromosome rearrangementProtein expressionProtein Function
    constitutional       loss of function
    resulted in smaller dendritic spines and simpler dendritic tree and impaired sensorimotor gating and acquisition of a spatial working memory–dependent task
    constitutional       loss of function
    associated with altered short-term plasticity and is a neural substrate underlying the cognitive dysfunction and the increased risk for schizophrenia associated with the 22q11.2 microdeletions
    tumoral       gain of function
    may be involved in tumorigenesis and aggressiveness of invasive ductal breast carcinoma (IDC)
    constitutional   deletion    
    conditional gene deletion of the essential miRNA-processing enzyme Dgcr8 in the developing renal tubular system results in severe developmental defects and kidney failure
    constitutional       loss of function
    senescence triggered by DGCR8 loss is accompanied by the upregulation of the cell-cycle inhibitor CDKN1A
    Susceptibility
    Variant & Polymorphism
    Candidate gene
    Marker
    Therapy target
    SystemTypeDisorderPubmed
    cancerreproductivebreast
    may serve as future therapeutic target in invasive ductal breast carcinoma (IDC)
    ANIMAL & CELL MODELS
  • Dgcr8+/- mice display reduced expression of a subset of microRNAs in the prefrontal cortex, a deficit that emerges over postnatal development
  • deficiency in Dgcr8-dependent canonical microRNAs causes infertility due to multiple abnormalities during uterine development in mice