IL1A-Gen

Last updated on: 17.01.2024

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Definition
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The IL1A gene (IL1A stands for: interleukin 1 alpha) is a protein-coding gene located on chromosome 2q14.1.

General information
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The IL1A gene codes for interleukin-1 alpha (IL-1 alpha), a cytokine that is secreted by various cell types of the immune system such as macrophages, monocytes and dendritic cells, but also by fibroblasts and endothelial cells. It owes its name to the fact that it was the first cytokine to be discovered. Interleukin-1alpha is produced in response to bacterial infections (its production is mainly stimulated by LPS, an endotoxin of gram-negative bacteria), the presence of TNF and the interaction of the producing cells with CD4-positive T lymphocytes. Interleuekin-1 alpha has several effects both locally and generally in the body, including the promotion of inflammatory processes in response to bacterial infections such as vasodilation, spasms and fever. It also stimulates the production of prostaglandins by various cell types (muscles, epithelia, etc.), the production of other cytokines such as IL-2 and the activation and recruitment of other cells of the immune system.

After binding to its receptor IL1R1, it forms the high-affinity interleukin-1 receptor complex together with its accessory protein IL1RAP. The signal transmission involves the recruitment of adapter molecules such as MYD88, IRAK1 or IRAK4 (Cohen I et al. 2015). This in turn mediates the activation of NF-kappa-B and the three MAPK signaling pathways p38, p42/p44 and JNK . Within the cell, it acts as an alarmin and is released into the extracellular space after cell death following rupture of the cell membrane to trigger inflammation and alert the host to injury or damage. In addition to its role as a danger signal that occurs when the cytokine is passively released by cell necrosis, it directly recognizes DNA damage and acts as a signal for genotoxic stress without loss of cell integrity.

Note(s)
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Diseases associated with IL1A include cholesteatoma of the middle ear and keratoconjunctivitis sicca. Related signaling pathways include MIF-mediated glucocorticoid regulation and TGF-beta signaling.

Literature
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  1. Cavalli G et al. (2021) Interleukin 1α: a comprehensive review on the role of IL-1α in the pathogenesis and treatment of autoimmune and inflammatory diseases. Autoimmun Rev 20:102763.
  2. Cohen I et al. (2015) IL-1α is a DNA damage sensor linking genotoxic stress signaling to sterile inflammation and innate immunity. Sci Rep 5:14756)
  3. Cominelli F et al. (1994) Rabbit interleukin-1 receptor antagonist. Cloning, expression, functional characterization, and regulation during intestinal inflammation. The Journal of Biological Chemistry 269: 6962-6971. doi:10.1016/S0021-9258(17)37468-9. PMID 7509813.
  4. Kim JS et al. (2021) Immunopathogenesis and treatment of cytokine storm in COVID-19. Theranostics 11:316-329.
  5. Matzinger P (2012) The evolution of the danger theory. Interview by Lauren Constable, Commissioning Editor. Expert Review of Clinical Immunology 8: 311-317.
  6. Nieradko-Iwanicka B et al. (2023) Interleukin 1α and interleukin 18 in patients with vitiligo - Results of a case-control study. Biomed Pharmacother160:114364.
  7. Rider P et al. (2011) IL-1α and IL-1β recruit different myeloid cells and promote different stages of sterile inflammation. Journal of Immunology 187: 4835-4843.
  8. Sahoo M et al. (2011) Role of the inflammasome, IL-1β, and IL-18 in bacterial infections. TheScientificWorldJournal 11: 2037-2050.
  9. Van Damme J et al. (1985) Homogeneous interferon-inducing 22K factor is related to endogenous pyrogen and interleukin-1. Nature 314:266-268.

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Last updated on: 17.01.2024