Cytokine

Not to be confused with Cytokinin.

Cytokines (cyto, from Greek "κύτταρο" kyttaro "cell" + kines, from Greek "κίνηση" kinisi "movement") are a broad and loose category of small proteins (~5–20 kDa) that are important in cell signaling. They are released by cells and affect the behavior of other cells. Cytokines can also be involved in autocrine signaling. Cytokines include chemokines, interferons, interleukins, lymphokines, tumour necrosis factor but generally not hormones or growth factors (despite some overlap in the terminology). Cytokines are produced by a broad range of cells, including immune cells like macrophages, B lymphocytes, T lymphocytes and mast cells, as well as endothelial cells, fibroblasts, and various stromal cells; a given cytokine may be produced by more than one type of cell.[1][2][3]

They act through receptors, and are especially important in the immune system; cytokines modulate the balance between humoral and cell-based immune responses, and they regulate the maturation, growth, and responsiveness of particular cell populations. Some cytokines enhance or inhibit the action of other cytokines in complex ways.[3]

They are different from hormones, which are also important cell signaling molecules, in that hormones circulate in less variable concentrations and hormones tend to be made by specific kinds of cells.

They are important in health and disease, specifically in host responses to infection, immune responses, inflammation, trauma, sepsis, cancer, and reproduction.

Discovery of cytokines

Interferon-alpha, an interferon type I, was identified in 1957 as a protein that interfered with viral replication.[4] The activity of interferon-gamma (the sole member of the interferon type II class) was described in 1965; this was the first identified lymphocyte-derived mediator.[4] Macrophage migration inhibitory factor (MIF) was identified simultaneously in 1966 by John David and Barry Bloom.[4]

In 1969 Dudley Dumonde proposed the term "lymphokine" to describe proteins secreted from lymphocytes and later, proteins derived from macrophages and monocytes in culture were called "monokines". As scientists learned more, it was understood that these proteins and others were part of a broader class of proteins involved in self-defense, and should be called "cytokines".[4]

Difference from hormones

Classic hormones circulate in nanomolar (10-9 M) concentrations that usually vary by less than one order of magnitude. In contrast, some cytokines (such as IL-6) circulate in picomolar (10-12 M) concentrations that can increase up to 1,000-fold during trauma or infection. The widespread distribution of cellular sources for cytokines may be a feature that differentiates them from hormones. Virtually all nucleated cells, but especially endo/epithelial cells and resident macrophages (many near the interface with the external environment) are potent producers of IL-1, IL-6, and TNF-α.[5] In contrast, classic hormones, such as insulin, are secreted from discrete glands (e.g., the pancreas).[6] As of 2008, the current terminology refers to cytokines as immunomodulating agents. However, more research is needed in this area of defining cytokines and hormones.

Part of the difficulty with distinguishing cytokines from hormones is that some of the immunomodulating effects of cytokines are systemic rather than local. For instance, to use hormone terminology, the action of cytokines may be autocrine or paracrine in chemotaxis or chemokinesis and endocrine as a pyrogen. Further, as molecules, cytokines are not limited to their immunomodulatory role.

Nomenclature

Cytokines have been classed as lymphokines, interleukins, and chemokines, based on their presumed function, cell of secretion, or target of action. Because cytokines are characterised by considerable redundancy and pleiotropism, such distinctions, allowing for exceptions, are obsolete.

Classification

Structural

Structural homogeneity has been able to partially distinguish between cytokines that do not demonstrate a considerable degree of redundancy so that they can be classified into four types:

Functional

A classification that proves more useful in clinical and experimental practice outside of structural biology divides immunological cytokines into those that enhance cellular immune responses, type 1 (TNFα, IFN-γ, etc.), and type 2 (TGF-β, IL-4, IL-10, IL-13, etc.), which favor antibody responses.

A key focus of interest has been that cytokines in one of these two sub-sets tend to inhibit the effects of those in the other. Dysregulation of this tendency is under intensive study for its possible role in the pathogenesis of autoimmune disorders.

Several inflammatory cytokines are induced by oxidative stress.[7][8] The fact that cytokines themselves trigger the release of other cytokines[9][10][11] and also lead to increased oxidative stress makes them important in chronic inflammation, as well as other immunoresponses, such as fever and acute phase proteins of the liver (IL-1,6,12, IFN-a).

Cytokines also play a role in anti-inflammatory pathways and are a possible therapeutic treatment for pathological pain from inflammation or peripheral nerve injury.[12] There are both pro-inflammatory and anti-inflammatory cytokines that regulate this pathway.

Receptors

Main article: Cytokine receptor

In recent years, the cytokine receptors have come to demand the attention of more investigators than cytokines themselves, partly because of their remarkable characteristics, and partly because a deficiency of cytokine receptors has now been directly linked to certain debilitating immunodeficiency states. In this regard, and also because the redundancy and pleomorphism of cytokines are, in fact, a consequence of their homologous receptors, many authorities think that a classification of cytokine receptors would be more clinically and experimentally useful.

A classification of cytokine receptors based on their three-dimensional structure has, therefore, been attempted. Such a classification, though seemingly cumbersome, provides several unique perspectives for attractive pharmacotherapeutic targets.

Cellular effects

Each cytokine has a matching cell-surface receptor. Subsequent cascades of intracellular signalling then alter cell functions. This may include the upregulation and/or downregulation of several genes and their transcription factors, resulting in the production of other cytokines, an increase in the number of surface receptors for other molecules, or the suppression of their own effect by feedback inhibition.

The effect of a particular cytokine on a given cell depends on the cytokine, its extracellular abundance, the presence and abundance of the complementary receptor on the cell surface, and downstream signals activated by receptor binding; these last two factors can vary by cell type. Cytokines are characterized by considerable "redundancy", in that many cytokines appear to share similar functions.

It seems to be a paradox that cytokines binding to antibodies have a stronger immune effect than the cytokine alone. This may lead to lower therapeutic doses.

Said et al. showed that inflammatory cytokines cause an IL-10-dependent inhibition of[14] T-cell expansion and function by up-regulating PD-1 levels on monocytes which leads to IL-10 production by monocytes after binding of PD-1 by PD-L.[14]

Adverse reactions to cytokines are characterized by local inflammation and/or ulceration at the injection sites. Occasionally such reactions are seen with more widespread papular eruptions.[15]

Roles of endogenous cytokines in health and disease

Cytokines are often involved in several developmental processes during embryogenesis.[16][nb 1][17][nb 2]

Cytokines are crucial for fighting off infections and in other immune responses.[18] However, they can become dysregulated and pathological in inflammation, trauma, and sepsis.[18]

Adverse effects of cytokines have been linked to many disease states and conditions ranging from schizophrenia, major depression[19] and Alzheimer's disease[20] to cancer.[21] Normal tissue integrity is preserved by feedback interactions between diverse cell types mediated by adhesion molecules and secreted cytokines; disruption of normal feedback mechanisms in cancer, threatens tissue integrity.[22] Over-secretion of cytokines can trigger a dangerous syndrome known as a cytokine storm; this may have been the cause of severe adverse events during a clinical trial of TGN1412. Cytokine storms also were the main cause of death in the 1918 "Spanish Flu" pandemic. Deaths were weighted more heavily towards people with healthy immune systems, due to its ability to produce stronger immune responses, likely increasing cytokine levels. Another important example of cytokine storm is seen in acute pancreatitis. Cytokines are integral and implicated in all angles of the cascade resulting in the systemic inflammatory response syndrome and multi organ failure associated with this intra-abdominal catastrophe.[23]

Medical use as drugs

Some cytokines have been developed into protein therapeutics using recombinant DNA technology.[24] Recombinant cytokines being used as drugs as of 2014 include:[25]

Research into diagnostic use of measured levels

Plasma levels of various cytokines may give information on the presence, or even predictive value of inflammatory processes involved in autoimmune diseases such as rheumatoid arthritis,[28] as well as immunomodulatory effects of foods or drugs.[29] In addition, elevated levels of IL-7, an important cytokine involved in T cell homeostasis, have been detected in the plasma of HIV-infected patients.[30]

See also

Notes

Wikimedia Commons has media related to Cytokines.
  1. Saito explains "much evidence has suggested that cytokines and chemokines play a very important role in the reproduction, i.e. embryo implantation, endometrial development, and trophoblast growth and differentiation by modulating the immune and endocrine systems."(15)
  2. Chen explains the regulatory activity of LIF in human and murine embryos: "In conclusion, human preimplantation embryos express LIF and LIF-R mRNA. The expression of these transcripts indicates that preimplantation embryos may be responsive to LIF originating either from the surrounding environment or from the embryos themselves and exerting its function in a paracrine or autocrine manner."(719)

References

  1. "Cytokine" in John Lackie. A Dictionary of Biomedicine. Oxford University Press. 2010. ISBN 9780199549351
  2. "Cytokine" in Stedman’s Medical Dictionary, 28th ed. Wolters Kluwer Health, Lippincott, Williams & Wilkins (2006)
  3. 1 2 Horst Ibelgaufts. Cytokines in Cytokines & Cells Online Pathfinder Encyclopedia Version 31.4 (Spring/Summer 2013 Edition)
  4. 1 2 3 4 Alexander G. Izaguirre. Molecular Mediators, Cytokines I: Lecture I: Topic I: Cytokines
  5. Boyle JJ (January 2005). "Macrophage activation in atherosclerosis: pathogenesis and pharmacology of plaque rupture". Curr Vasc Pharmacol 3 (1): 63–8. doi:10.2174/1570161052773861. PMID 15638783.
  6. Cannon JG (December 2000). "Inflammatory Cytokines in Nonpathological States". News Physiol. Sci. 15: 298–303. PMID 11390930.
  7. Vlahopoulos S, Boldogh I, Casola A, Brasier AR; Boldogh; Casola; Brasier (September 1999). "Nuclear factor-kappaB-dependent induction of interleukin-8 gene expression by tumor necrosis factor alpha: evidence for an antioxidant sensitive activating pathway distinct from nuclear translocation". Blood 94 (6): 1878–89. PMID 10477716.
  8. David F, Farley J, Huang H, Lavoie JP, Laverty S; Farley; Huang; Lavoie; Laverty (April 2007). "Cytokine and chemokine gene expression of IL-1beta stimulated equine articular chondrocytes". Vet Surg 36 (3): 221–7. doi:10.1111/j.1532-950X.2007.00253.x. PMID 17461946.
  9. Chokkalingam, V.; Tel, J.; Wimmers, F.; Liu, X.; Semenov, S.; Thiele, J.; Figdor, C. G.; Huck, W. T. S. (2013). "Probing cellular heterogeneity in cytokine-secreting immune cells using droplet-based microfluidics". Lab on a Chip 13 (24): 4740–4744. doi:10.1039/C3LC50945A. PMID 24185478.
  10. Carpenter LR, Moy JN, Roebuck KA; Moy; Roebuck (March 2002). "Respiratory syncytial virus and TNF alpha induction of chemokine gene expression involves differential activation of Rel A and NF-kappa B1". BMC Infect. Dis. 2: 5. doi:10.1186/1471-2334-2-5. PMC 102322. PMID 11922866.
  11. Tian B, Nowak DE, Brasier AR; Nowak; Brasier (2005). "A TNF-induced gene expression program under oscillatory NF-kappaB control". BMC Genomics 6: 137. doi:10.1186/1471-2164-6-137. PMC 1262712. PMID 16191192.
  12. Zhang, Jun-Ming; An, Jianxiong (2007-01-01). "Cytokines, Inflammation and Pain". International anesthesiology clinics 45 (2): 27–37. doi:10.1097/AIA.0b013e318034194e. ISSN 0020-5907. PMC 2785020. PMID 17426506.
  13. Gaffen SL (August 2009). "Structure and signalling in the IL-17 receptor family". Nat. Rev. Immunol. 9 (8): 556–67. doi:10.1038/nri2586. PMC 2821718. PMID 19575028.
  14. 1 2 Said EA, Dupuy FP, Trautmann L; et al. (April 2010). "Programmed death-1-induced interleukin-10 production by monocytes impairs CD4+ T cell activation during HIV infection". Nat. Med. 16 (4): 452–9. doi:10.1038/nm.2106. PMC 4229134. PMID 20208540.
  15. James, William; Berger, Timothy; Elston, Dirk (2005). Andrews' Diseases of the Skin: Clinical Dermatology. (10th ed.). Saunders. ISBN 0-7216-2921-0.
  16. Saito S (2001). "Cytokine cross-talk between mother and the embryo/placenta". J. Reprod. Immunol. 52 (1–2): 15–33. doi:10.1016/S0165-0378(01)00112-7. PMID 11600175.
  17. Chen HF, Shew JY, Ho HN, Hsu WL, Yang YS; Shew; Ho; Hsu; Yang (October 1999). "Expression of leukemia inhibitory factor and its receptor in preimplantation embryos". Fertil. Steril. 72 (4): 713–9. doi:10.1016/S0015-0282(99)00306-4. PMID 10521116.
  18. 1 2 Dinarello CA (August 2000). "Proinflammatory cytokines". Chest 118 (2): 503–8. doi:10.1378/chest.118.2.503. PMID 10936147.
  19. Dowlati Y, Herrmann N, Swardfager W; et al. (March 2010). "A meta-analysis of cytokines in major depression". Biol. Psychiatry 67 (5): 446–57. doi:10.1016/j.biopsych.2009.09.033. PMID 20015486.
  20. Swardfager W, Lanctôt K, Rothenburg L, Wong A, Cappell J, Herrmann N; Lanctôt; Rothenburg; Wong; Cappell; Herrmann (November 2010). "A meta-analysis of cytokines in Alzheimer's disease". Biol. Psychiatry 68 (10): 930–41. doi:10.1016/j.biopsych.2010.06.012. PMID 20692646.
  21. Locksley RM, Killeen N, Lenardo MJ; Killeen; Lenardo (February 2001). "The TNF and TNF receptor superfamilies: integrating mammalian biology". Cell 104 (4): 487–501. doi:10.1016/S0092-8674(01)00237-9. PMID 11239407.
  22. Vlahopoulos, SA; Cen, O; Hengen, N; Agan, J; Moschovi, M; Critselis, E; Adamaki, M; Bacopoulou, F; Copland, JA; Boldogh, I; Karin, M; Chrousos, GP (20 June 2015). "Dynamic aberrant NF-κB spurs tumorigenesis: A new model encompassing the microenvironment.". Cytokine & growth factor reviews 26: 389–403. doi:10.1016/j.cytogfr.2015.06.001. PMID 26119834.
  23. Makhija R, Kingsnorth AN; Kingsnorth (2002). "Cytokine storm in acute pancreatitis". J Hepatobiliary Pancreat Surg 9 (4): 401–10. doi:10.1007/s005340200049. PMID 12483260.
  24. Horst Ibelgaufts. Recombinant cytokines in Cytokines & Cells Online Pathfinder Encyclopedia Version 31.4 (Spring/Summer 2013 Edition)
  25. Dimiter S. Dimitrov. Therapeutic Proteins.Chapter 1 in Therapeutic Proteins: Methods and Protocols, Editors: Vladimir Voynov, Justin A. Caravella. Volume 899 of Methods in Molecular Biology. Springer Science+Business Media, LLC 2012. ISBN 978-1-61779-920-4 (Print) 978-1-61779-921-1 (Online)
  26. Woodman, RC; Erickson, RW; Rae, J; Jaffe, HS; Curnutte, JT (Mar 15, 1992). "Prolonged recombinant interferon-gamma therapy in chronic granulomatous disease: evidence against enhanced neutrophil oxidase activity.". Blood 79 (6): 1558–62. PMID 1312372.
  27. Key LL, Jr; Rodriguiz, RM; Willi, SM; Wright, NM; Hatcher, HC; Eyre, DR; Cure, JK; Griffin, PP; Ries, WL (Jun 15, 1995). "Long-term treatment of osteopetrosis with recombinant human interferon gamma". The New England Journal of Medicine 332 (24): 1594–9. doi:10.1056/NEJM199506153322402. PMID 7753137.
  28. Kokkonen, H. Arthritis & Rheumatism, Feb. 2, 2010; vol 62: pp 383–391
  29. Nikolaeva LG, Maystat TV, Masyuk LA, Pylypchuk VS, Volyanskii YL, Kutsyna GA; Maystat; Masyuk; Pylypchuk; Volyanskii; Kutsyna (2009). "Changes in CD4+ T-cells and HIV RNA resulting from combination of anti-TB therapy with Dzherelo in TB/HIV dually infected patients". Drug Des Devel Ther 2: 87–93. PMC 2761183. PMID 19920896.
  30. Napolitano LA, Grant RM, Deeks SG; et al. (January 2001). "Increased production of IL-7 accompanies HIV-1-mediated T-cell depletion: implications for T-cell homeostasis". Nat. Med. 7 (1): 73–9. doi:10.1038/83381. PMID 11135619.

External links

This article is issued from Wikipedia - version of the Tuesday, May 03, 2016. The text is available under the Creative Commons Attribution/Share Alike but additional terms may apply for the media files.