Beta adrenergic receptor kinase

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Adrenergic, beta, receptor kinase 1
Protein ADRBK1 PDB 1bak.png
PDB rendering based on 1bak.
Available structures
PDB Ortholog search: PDBe, RCSB
Identifiers
Symbols ADRBK1 ; BARK1; BETA-ARK1; GRK2
External IDs OMIM109635 MGI87940 HomoloGene1223 ChEMBL: 4079 GeneCards: ADRBK1 Gene
EC number 2.7.11.15
RNA expression pattern
PBB GE ADRBK1 38447 at tn.png
PBB GE ADRBK1 201401 s at tn.png
PBB GE ADRBK1 201402 at tn.png
More reference expression data
Orthologs
Species Human Mouse
Entrez 156 110355
Ensembl ENSG00000173020 ENSMUSG00000024858
UniProt P25098 Q99MK8
RefSeq (mRNA) NM_001619 NM_001290818
RefSeq (protein) NP_001610 NP_001277747
Location (UCSC) Chr 11:
67.27 – 67.29 Mb
Chr 19:
4.29 – 4.31 Mb
PubMed search [1] [2]

Beta adrenergic receptor kinase (also referred to as βARK or BARK) is a serine/threonine intracellular kinase. It is activated by PKA and its target is the beta adrenergic receptor. It is one method by which the cell will desensitize itself from epinephrine overstimulation.[1][2]

βARK Activation

  • (steps 1) Upon stimulation of the Beta adrenergic receptor by epinephrine, Gs will be activated.
  • (steps 3 through 6) cAMP will then activate cAMP-dependent kinase (PKA), which, among other proteins that it acts on, will phosphorylate serine and threonine residues on βARK.
Beta Adrenergic Receptor Kinase Activation Pathway.
  • (step 7) βARK, itself a serine/threonine kinase, will then phosphorylate serine and threonine residues on the β-adrenergic receptor itself.
  • (step 8) This will facilitate Beta-arrestin's binding to the receptor. Additional stimulation by epinephrine will now be unable to activate Gs due to arrestin.

Therefore, βARK is a negative feedback enzyme that will prevent overstimulation of the β-adrenergic receptor.[1][2]

Other similar systems

In the rhodopsin system, which regulates rod cell function in the retina, rhodopsin kinase will phosphorylate serine and threonine residues on the rhodopsin receptor. Similarly to the βARK system, the phosphorylated rhodopsin residues will then bind to arrestin, resulting in receptor desensitization.

Structure

Protein Structure

The structure of βARK1 consists of a protein of 689 amino acids (79.7 kilodaltons) with a protein kinase catalytic domain that bears greatest sequence similarity to protein kinase C and the cyclic adenosine monophosphate (cyclic AMP)-dependent protein kinase.[3]

Gene structure

The gene spans approximately 23 kilobases and is composed of 21 exons interrupted by 20 introns. Exon sizes range from 52 bases (exon 7) to over 1200 bases (exon 21), intron sizes from 68 bases (intron L) to 10.8 kilobases (intron A). The splice sites for donor and acceptor were in agreement with the canonical GT/AG rule. Functional regions of beta ARK are described with respect to their location within the exon-intron organization of the gene. Primer extension and RNase protection assays suggest a major transcription start site approximately 246 bases upstream of the start ATG. Sequence analysis of the 5'-flanking/promoter region reveals many features characteristic of mammalian housekeeping genes, i.e. the lack of a TATA box, an absent or nonstandard positioned CAAT box, high GC content, and the presence of Sp1-binding sites. The extraordinarily high GC content of the 5'-flanking region (> 80%) helps define this region as a CpG island that may be a principal regulator of beta ARK expression.[4]

Interactions

Beta adrenergic receptor kinase has been shown to interact with:

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See also

References

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External links