Interleukin-20 receptor

interleukin 20 receptor, alpha
Identifiers
SymbolIL20RA
Alt. symbolsZCYTOR7, IL-20R1
NCBI gene53832
HGNC6003
OMIM605620
RefSeqNM_014432
UniProtQ9UHF4
Other data
LocusChr. 6 q23.3
Search for
StructuresSwiss-model
DomainsInterPro
interleukin 20 receptor beta
Identifiers
SymbolIL20RB
Alt. symbolsFNDC6
NCBI gene53833
HGNC6004
OMIM605621
RefSeqNM_144717
UniProtQ6UXL0
Other data
LocusChr. 3 q22.3
Search for
StructuresSwiss-model
DomainsInterPro

Interleukin 20 receptors (IL20R) belong to the IL-10 family. IL20R are involved in both pro-inflammatory and anti-inflammatory immune response.[1][2] There are two types of IL20R: Type I and Type II.

IL20R is found in many organ resident effector cells such as keratinocytes at the skin epidermis, osteoclasts, found in bones, and epithelial cells of the intestine and trachea. IL20R alpha and beta subunits have also been found in some immune cells.[2] IL20R is implicated in diseases such as psoriasis, rheumatoid arthritis, and glaucoma.  

Structure and function

There are two types of IL20R: Type I, made up of the IL-20 receptor alpha subunit and beta subunit, and Type II, made up of the IL-22 receptor and IL-20 receptor beta subunit.[3] Both types of receptor bind the cytokines IL-20, IL-24. Type 1 also binds cytokine IL-19.[4][5]

Signaling

IL20R signalling happens through the JAK-STAT pathway.[4] When an IL-20 subfamily cytokine binds IL20R, JAK's linked to intracellular domains of IL20R activate and phosphorylate tyrosine residues found in the longer alpha chains in the intracellular portion of the receptor. STAT then binds to docking sites created by JAK phosphorylation, and become phosphorylated by JAK's themselves. STATs then dimerize and move to the nucleus to act as transcription factors. The specific genes expressed are dependent on the specific JAK, STAT, as well as by SOCS proteins, which inhibit the JAK-STAT signal to regulate it.[3]

STAT3 is the main transcription factor activated with IL20R signaling.[6]

IL20R subunit gene mutations and differences in gene expression are associated with an increased risk of inflammatory diseases.[2]

IL20R and Psoriasis

IL20R has is involved in skin homeostasis. Research shows that IL-20R may play a role in the immune disease psoriasis, where rapid growth of skin cells leads to dryness and irritation.[3] Mutations in IL20R are associated with an increased risk of psoriasis, and psoriatic skin lesions show elevated levels of IL20R.

Under the current understanding of psoriasis, the over-activation of dendritic cells and macrophages leads to pro-inflammatory cytokine release, including TNFα and IL-23. This cytokine release activates T-helper cells, which produce cytokines IL-17 and IL-22, and subsequently leads to the release of IL-19 IL-20, and IL-24. The binding of IL-20, IL-24, and IL-19 to IL20R, along with other cytokines binding to their respective receptors, leads to high amounts of keratinocytes. The keratinocytes then lead to psoriatic plaque formation.[3]

Rheumatoid arthritis

IL20R is linked with rheumatoid arthritis, an autoimmune condition where the immune system attacks joints and other body areas and leads to pain. Elevated levels of IL20R mRNA and proteins are found in people with rheumatoid arthritis. It is thought that production of IL20 which binds to IL20Rs increases the production of chemoattractants, which are immune signaling molecules that can recruit immune cells. The chemoattractants then attract neutrophils and T-cells, which drive inflammation in the joints and cause pain.[3]

Research also shows that certain gene mutations in IL20R are associated with an increased risk of juvenile idiopathic arthritis.[2]

Glaucoma

Research indicates that IL20Rs, specifically the IL20R beta subunit (IL20RB), may be linked with glaucoma, a disease that can lead to blindness. It’s not believed that IL20RB has a causative effect on the disease, but it may contribute to an increased risk of the disease, along with other factors, such as intraocular pressure.[7]

References

  1. ^ Rutz S, Wang X, Ouyang W (December 2014). "The IL-20 subfamily of cytokines--from host defence to tissue homeostasis". Nature Reviews. Immunology. 14 (12): 783–795. doi:10.1038/nri3766. PMID 25421700. S2CID 29114703.
  2. ^ a b c d Kragstrup TW, Andersen T, Heftdal LD, Hvid M, Gerwien J, Sivakumar P, et al. (2018-09-25). "The IL-20 Cytokine Family in Rheumatoid Arthritis and Spondyloarthritis". Frontiers in Immunology. 9: 2226. doi:10.3389/fimmu.2018.02226. PMC 6167463. PMID 30319661.
  3. ^ a b c d e Wegenka UM (October 2010). "IL-20: biological functions mediated through two types of receptor complexes". Cytokine & Growth Factor Reviews. IL-10 Family of Cytokines. 21 (5): 353–363. doi:10.1016/j.cytogfr.2010.08.001. PMID 20864382.
  4. ^ a b Chen J, Caspi RR, Chong WP (November 2018). "IL-20 receptor cytokines in autoimmune diseases". Journal of Leukocyte Biology. 104 (5): 953–959. doi:10.1002/jlb.mr1117-471r. PMC 6298946. PMID 30260500.
  5. ^ Ouyang W, O'Garra A (April 2019). "IL-10 Family Cytokines IL-10 and IL-22: from Basic Science to Clinical Translation". Immunity. 50 (4): 871–891. doi:10.1016/j.immuni.2019.03.020. PMID 30995504. S2CID 122350808.
  6. ^ Blumberg H, Conklin D, Xu WF, Grossmann A, Brender T, Carollo S, et al. (January 2001). "Interleukin 20: discovery, receptor identification, and role in epidermal function". Cell. 104 (1): 9–19. doi:10.1016/S0092-8674(01)00187-8. PMID 11163236. S2CID 7460710.
  7. ^ Wirtz MK, Keller KE (2016). "The Role of the IL-20 Subfamily in Glaucoma". Mediators of Inflammation. 2016: 4083735. doi:10.1155/2016/4083735. PMC 4745377. PMID 26903709.

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