Interleukin 6

IL6
Available structures
PDBOrtholog search: PDBe RCSB
Identifiers
Aliases IL6, BSF2, HGF, HSF, IFNB2, IL-6, BSF-2, CDF, IFN-beta-2, interleukin 6
External IDs OMIM: 147620 MGI: 96559 HomoloGene: 502 GeneCards: IL6
RNA expression pattern
More reference expression data
Orthologs
Species Human Mouse
Entrez

3569

16193

Ensembl

ENSG00000136244

ENSMUSG00000025746

UniProt

P05231

P08505

RefSeq (mRNA)

NM_000600
NM_001318095

NM_031168
NM_001314054

RefSeq (protein)

NP_000591.1

NP_112445.1
NP_001300983.1

Location (UCSC) Chr 7: 22.73 – 22.73 Mb Chr 5: 30.01 – 30.02 Mb
PubMed search [1] [2]
Wikidata
View/Edit HumanView/Edit Mouse

Interleukin 6 (IL-6) is an interleukin that acts as both a pro-inflammatory cytokine and an anti-inflammatory myokine. In humans, it is encoded by the IL6 gene.[3]

Interleukin 6 is secreted by T cells and macrophages to stimulate immune response, e.g. during infection and after trauma, especially burns or other tissue damage leading to inflammation. IL-6 also plays a role in fighting infection, as IL-6 has been shown in mice to be required for resistance against bacterium Streptococcus pneumoniae.[4]

In addition, osteoblasts secrete IL-6 to stimulate osteoclast formation. Smooth muscle cells in the tunica media of many blood vessels also produce IL-6 as a pro-inflammatory cytokine. IL-6's role as an anti-inflammatory cytokine is mediated through its inhibitory effects on TNF-alpha and IL-1, and activation of IL-1ra and IL-10.

Function

IL-6 is an important mediator of fever and of the acute phase response. It is capable of crossing the blood-brain barrier[5] and initiating synthesis of PGE2 in the hypothalamus, thereby changing the body's temperature setpoint. In muscle and fatty tissue, IL-6 stimulates energy mobilization that leads to increased body temperature. IL-6 can be secreted by macrophages in response to specific microbial molecules, referred to as pathogen-associated molecular patterns (PAMPs). These PAMPs bind to an important group of detection molecules of the innate immune system, called pattern recognition receptors (PRRs), including Toll-like receptors (TLRs). These are present on the cell surface and intracellular compartments and induce intracellular signaling cascades that give rise to inflammatory cytokine production.

IL-6 is also essential for hybridoma growth and is found in many supplemental cloning media such as briclone. Inhibitors of IL-6 (including estrogen) are used to treat postmenopausal osteoporosis. IL-6 is also produced by adipocytes and is thought to be a reason why obese individuals have higher endogeneous levels of CRP.[6] Intranasally administered IL-6 has been shown to improve sleep-associated consolidation of emotional memories.[7]

IL-6 is responsible for stimulating acute phase protein synthesis, as well as the production of neutrophils in the bone marrow. It supports the growth of B cells and is antagonistic to regulatory T cells.

When psychologically stressed, the human body produces stress hormones like cortisol, which are able to trigger interleukin 6 release into the circulation.[8] Interleukin-6's antagonistic position to T-Cells, seems to be at least partly mediated by the inhibiting effect of PGE2 on the signaling-function of T-Cells. PGE2 gets released in response to an activation by IL-6, leading not only to a greater chance of catching a virus but increasing the chance that a disease developes some sort of severity before the immune-system fully kicks in. It is mainly the T4-helper-cells that have an important signaling function, either communicating B-Cells to produce antibodies or informing killer T-Cells about certain antigens that need to be destroyed. Therefore IL-6 seems to play a major role in the process of acute or chronic stress (f.e. depression, anxiety) suppressing the immune-system. High levels of IL-6 in cancer-patients or in children with encephalitis (as mentioned below) could therefore be explained by the high levels of psychological stress these diseases trigger in the patients minds.

Role as myokine

IL-6 is also considered a myokine, a cytokine produced from muscle, which is elevated in response to muscle contraction.[9] It is significantly elevated with exercise, and precedes the appearance of other cytokines in the circulation. During exercise, it is thought to act in a hormone-like manner to mobilize extracellular substrates and/or augment substrate delivery.[10]

IL-6 has extensive anti-inflammatory functions in its role as a myokine. IL-6 was the first myokine that was found to be secreted into the blood stream in response to muscle contractions.[11] Aerobic exercise provokes a systemic cytokine response, including, for example, IL-6, IL-1 receptor antagonist (IL-1ra), and IL-10. IL-6 was serendipitously discovered as a myokine because of the observation that it increased in an exponential fashion proportional to the length of exercise and the amount of muscle mass engaged in the exercise. It has been consistently demonstrated that the plasma concentration of IL-6 increases during muscular exercise. This increase is followed by the appearance of IL-1ra and the anti-inflammatory cytokine IL-10. In general, the cytokine response to exercise and sepsis differs with regard to TNF-α. Thus, the cytokine response to exercise is not preceded by an increase in plasma-TNF-α. Following exercise, the basal plasma IL-6 concentration may increase up to 100-fold, but less dramatic increases are more frequent. The exercise-induced increase of plasma IL-6 occurs in an exponential manner and the peak IL-6 level is reached at the end of the exercise or shortly thereafter. It is the combination of mode, intensity, and duration of the exercise that determines the magnitude of the exercise-induced increase of plasma IL-6.[12]

IL-6 had previously been classified as a proinflammatory cytokine. Therefore, it was first thought that the exercise-induced IL-6 response was related to muscle damage.[13] However, it has become evident that eccentric exercise is not associated with a larger increase in plasma IL-6 than exercise involving concentric "nondamaging" muscle contractions. This finding clearly demonstrates that muscle damage is not required to provoke an increase in plasma IL-6 during exercise. As a matter of fact, eccentric exercise may result in a delayed peak and a much slower decrease of plasma IL-6 during recovery.[14]

Recent work has shown that both upstream and downstream signalling pathways for IL-6 differ markedly between myocytes and macrophages. It appears that unlike IL-6 signalling in macrophages, which is dependent upon activation of the NFκB signalling pathway, intramuscular IL-6 expression is regulated by a network of signalling cascades, including the Ca2+/NFAT and glycogen/p38 MAPK pathways. Thus, when IL-6 is signalling in monocytes or macrophages, it creates a pro-inflammatory response, whereas IL-6 activation and signalling in muscle is totally independent of a preceding TNF-response or NFκB activation, and is anti-inflammatory.[15]

IL-6, among an increasing number of other recently identified myokines, thus remains an important topic in myokine research. It appears in muscle tissue and in the circulation during exercise at levels up to one hundred times basal rates, as noted, and is seen as having a beneficial impact on health and bodily functioning when elevated in response to physical exercise.[16] IL-6 was the first myokine that was found to be secreted into the blood stream in response to muscle contractions.[17]

Receptor

IL-6 signals through a cell-surface type I cytokine receptor complex consisting of the ligand-binding IL-6Rα chain (CD126), and the signal-transducing component gp130 (also called CD130). CD130 is the common signal transducer for several cytokines including leukemia inhibitory factor (LIF), ciliary neurotropic factor, oncostatin M, IL-11 and cardiotrophin-1, and is almost ubiquitously expressed in most tissues. In contrast, the expression of CD126 is restricted to certain tissues. As IL-6 interacts with its receptor, it triggers the gp130 and IL-6R proteins to form a complex, thus activating the receptor. These complexes bring together the intracellular regions of gp130 to initiate a signal transduction cascade through certain transcription factors, Janus kinases (JAKs) and Signal Transducers and Activators of Transcription (STATs).[18]

IL-6 is probably the best-studied of the cytokines that use gp130, also known as IL-6 signal transducer (IL6ST), in their signalling complexes. Other cytokines that signal through receptors containing gp130 are Interleukin 11 (IL-11), Interleukin 27 (IL-27), ciliary neurotrophic factor (CNTF), cardiotrophin-1 (CT-1), cardiotrophin-like cytokine (CLC), leukemia inhibitory factor (LIF), oncostatin M (OSM), Kaposi's sarcoma-associated herpesvirus interleukin 6-like protein (KSHV-IL6).[19] These cytokines are commonly referred to as the IL-6 like or gp130 utilising cytokines [20]

In addition to the membrane-bound receptor, a soluble form of IL-6R (sIL-6R) has been purified from human serum and urine. Many neuronal cells are unresponsive to stimulation by IL-6 alone, but differentiation and survival of neuronal cells can be mediated through the action of sIL-6R. The sIL-6R/IL-6 complex can stimulate neurites outgrowth and promote survival of neurons and, hence, may be important in nerve regeneration through remyelination.

Interactions

Interleukin-6 has been shown to interact with interleukin-6 receptor.[21][22][23] and glycoprotein 130.[24]

There is considerable functional overlap and interaction between Substance P (SP), the natural ligand for the neurokinin type 1 receptor (NK1R, a mediator of immunomodulatory activity) and IL-6.

Role in disease

IL-6 stimulates the inflammatory and auto-immune processes in many diseases such as diabetes,[25] atherosclerosis,[26] depression,[27] Alzheimer's Disease,[28] systemic lupus erythematosus,[29] multiple myeloma,[30] prostate cancer,[31] Behçet's disease,[32] and rheumatoid arthritis.[33]

Hence, there is an interest in developing anti-IL-6 agents as therapy against many of these diseases.[34][35] The first such is tocilizumab, which has been approved for rheumatoid arthritis,[36] Castleman's disease[37] and systemic juvenile idiopathic arthritis.[38] Others are in clinical trials.[39]

Rheumatoid arthritis

The first FDA approved anti-IL-6 was for RA.

Cancer

Recently, Anestakis et al. outlined the interleukin mechanisms in cancer progression and possibilities in application for cancer immunotherapy in their systematic review.[40] IL-6 was seen to have roles in tumor microenvironment regulation,[41] production of breast cancer stem cell-like cells,[42] metastasis through down-regulation of E-cadherin,[43] and alteration of DNA methylation in oral cancer.[44]

Advanced/metastatic cancer patients have higher levels of IL-6 in their blood.[45] One example of this is pancreatic cancer, with noted elevation of IL-6 present in patients correlating with poor survival rates.[46]

Infectious diseases

Enterovirus 71

High IL-6 levels are associated with the development of encephalitis in children and immunodeficient mouse models infected with Enterovirus 71; this highly contagious virus normally causes a milder illness called Hand, foot, and mouth disease but can cause life-threatening encephalitis in some cases. EV71 patients with a certain gene polymorphism in IL-6 also appear to be more susceptible to developing encephalitis.

Epigenetic modifications

IL-6 has been shown to lead to several neurological diseases through its impact on epigenetic modification within the brain.[47][48] IL-6 activates the Phosphoinositide 3-kinase (PI3K) pathway, and a downstream target of this pathway is the protein kinase B (PKB) (Hodge et al., 2007). IL-6 activated PKB can phosphorylate the nuclear localization signal on DNA methyltransferase-1(DNMT1).[49] This phosphorylation causes movement of DNMT1 to the nucleus, where it can be transcribed.[49] DNMT1 recruits other DNMTs, including DNMT3A and DNMT3B, which, as a complex, recruit HDAC1.[48] This complex adds methyl groups to CpG islands on gene promoters, repressing the chromatin structure surrounding the DNA sequence and inhibiting transcriptional machinery from accessing the gene to induce transcription.[48] Increased IL-6, therefore, can hypermethylate DNA sequences and subsequently decrease gene expression through its effects on DNMT1 expression.[50]

Schizophrenia

The induction of epigenetic modification by IL-6 has been proposed as a mechanism in the pathology of schizophrenia through the hypermethylation and repression of the GAD67 promoter.[48] This hypermethylation may potentially lead to the decreased GAD67 levels seen in the brains of people with schizophrenia.[51] GAD67 may be involved in the pathology of schizophrenia through its effect on GABA levels and on neural oscillations.[52] Neural oscillations occur when inhibitory GABAergic neurons fire synchronously and cause inhibition of a multitude of target excitatory neurons at the same time, leading to a cycle of inhibition and disinhibition.[52] These neural oscillations are impaired in schizophrenia, and these alterations may be responsible for both positive and negative symptoms of schizophrenia.[53]

Depression and major depressive disorder

The epigenetic effects IL-6 have also been implicated in the pathology of depression. The effects of IL-6 on depression are mediated through the repression of brain-derived neurotrophic factor (BDNF) expression in the brain; DNMT1 hypermethylates the BDNF promoter and reduces BDNF levels.[54] Altered BDNF function has been implicated in depression,[55] which is likely due to epigenetic modification following IL-6 upregulation.[54] BDNF is a neutrophic factor implicated in spine formation, density, and morphology on neurons.[56] Downregulation of BDNF, therefore, may cause decreased connectivity in the brain. Depression is marked by altered connectivity, in particular between the anterior cingulate cortex and several other limbic areas, such as the hippocampus.[57] The anterior cingulate cortex is responsible for detecting incongruences between expectation and perceived experience.[58] Altered connectivity of the anterior cingulate cortex in depression, therefore, may cause altered emotions following certain experiences, leading to depressive reactions.[58] This altered connectivity is mediated by IL-6 and its effect on epigenetic regulation of BDNF.[54]

Additional preclinical and clinical data, suggest that Substance P [SP] and IL-6 may act in concert to promote major depression. SP, a hybrid neurotransmitter-cytokine, is co-transmitted with BDNF through paleo-spinothalamic circuitry from the periphery with collaterals into key areas of the limbic system. However, both IL6 and SP mitigate expression of BDNF in brain regions associated with negative affect and memory. SP and IL6 both relax tight junctions of the blood brain barrier, such that effects seen in fMRI experiments with these molecules may be a bidirectional mix of neuronal, glial, capillary, synaptic, paracrine, or endocrine-like effects. At the cellular level, SP is noted to increase expression of interleukin-6 (IL-6) through PI-3K, p42/44 and p38 MAP kinase pathways. Data suggest that nuclear translocation of NF-κB regulates IL-6 overexpression in SP-stimulated cells.[59] This is of key interest as: 1) a meta-analysis indicates an association of major depressive disorder, C-reactive protein and IL6 plasma concentrations,[60] 2) NK1R antagonists [five molecules] studied by 3 independent groups groups in over 2000 patients from 1998-2013 validate the mechanism as dose-related, fully effective antidepressant, with a unique safety profile.[61][62] (see Summary of NK1RAs in Major Depression), 3) the preliminary observation that plasma concentrations of IL6 are elevated in depressed patients with cancer,[63] and 4) selective NK1RAs may eliminate endogenous SP stress-induced augmentation of IL-6 secretion pre-clinically.[64] These and many other reports suggest that a clinical study of a neutralizing IL-6 biological or drug based antagonist is likely warranted in patients with major depressive disorder, with or without co-morbid chronic inflammatory based illnesses; that the combination of NK1RAs and IL6 blockers may represent a new, potentially biomarkable approach to major depression, and possibly bipolar disorder.

The IL-6 antibody sirukumab is now undergoing clinical trials against major depressive disorder.[65]


Asthma

Obesity is a known risk factor in the development of severe asthma. Recent data suggests that the inflammation associated with obesity, potentially mediated by the cytokine IL6, plays a role in causing poor lung function and increased risk for developing asthma exacerbations.[66]

References

  1. "Human PubMed Reference:".
  2. "Mouse PubMed Reference:".
  3. Ferguson-Smith AC, Chen YF, Newman MS, May LT, Sehgal PB, Ruddle FH (Apr 1988). "Regional localization of the interferon-beta 2/B-cell stimulatory factor 2/hepatocyte stimulating factor gene to human chromosome 7p15-p21". Genomics. 2 (3): 203–8. doi:10.1016/0888-7543(88)90003-1. PMID 3294161.
  4. van der Poll T, Keogh CV, Guirao X, Buurman WA, Kopf M, Lowry SF (Aug 1997). "Interleukin-6 gene-deficient mice show impaired defense against pneumococcal pneumonia". The Journal of Infectious Diseases. 176 (2): 439–44. doi:10.1086/514062. PMID 9237710.
  5. Banks WA, Kastin AJ, Gutierrez EG (Sep 1994). "Penetration of interleukin-6 across the murine blood-brain barrier". Neuroscience Letters. 179 (1-2): 53–6. doi:10.1016/0304-3940(94)90933-4. PMID 7845624.
  6. Bastard J, Jardel C, Delattre J, Hainque B, et al. (1999). "Evidence for a Link Between Adipose Tissue Interleukin-6 Content and Serum C-Reactive Protein Concentrations in Obese Subjects". Circulation. 99 (16): 2219–2222. doi:10.1161/01.CIR.99.16.2219.c.
  7. Benedict C, Scheller J, Rose-John S, Born J, Marshall L (Oct 2009). "Enhancing influence of intranasal interleukin-6 on slow-wave activity and memory consolidation during sleep". FASEB Journal. 23 (10): 3629–36. doi:10.1096/fj.08-122853. PMID 19546306.
  8. Cohen S, Doyle WJ, Skoner DP (1999). "Psychological stress, cytokine production, and severity of upper respiratory illness". Psychosomatic Medicine. 61 (2): 175–80. PMID 10204970.
  9. Febbraio MA, Pedersen BK (Jul 2005). "Contraction-induced myokine production and release: is skeletal muscle an endocrine organ?". Exercise and Sport Sciences Reviews. 33 (3): 114–9. doi:10.1097/00003677-200507000-00003. PMID 16006818.
  10. Petersen AM, Pedersen BK (Apr 2005). "The anti-inflammatory effect of exercise". Journal of Applied Physiology. 98 (4): 1154–62. doi:10.1152/japplphysiol.00164.2004. PMID 15772055.
  11. Pedersen BK, Febbraio MA (Oct 2008). "Muscle as an endocrine organ: focus on muscle-derived interleukin-6". Physiological Reviews. 88 (4): 1379–406. doi:10.1152/physrev.90100.2007. PMID 18923185.
  12. Pedersen BK (July 2013). "Muscle as a secretory organ". Compr Physiol 3 (3): 1337–62. doi:10.1002/cphy.c120033. PMID 23897689
  13. Bruunsgaard H, Galbo H, Halkjaer-Kristensen J, Johansen TL, MacLean DA, Pedersen BK (Mar 1997). "Exercise-induced increase in serum interleukin-6 in humans is related to muscle damage". The Journal of Physiology. 499 (3): 833–41. doi:10.1113/jphysiol.1997.sp021972. PMC 1159298Freely accessible. PMID 9130176.
  14. Pedersen BK (Jul 2013). "Muscle as a secretory organ". Comprehensive Physiology. 3 (3): 1337–62. doi:10.1002/cphy.c120033. PMID 23897689.
  15. The Role of Exercise-InducedMyokines in Muscle Homeostasis and the Defense against Chronic Diseases. Claus Brandt and Bente K. Pedersen. Journal of Biomedicine and Biotechnology. Volume 2010, Article ID 520258, 6 pages. doi:10.1155/2010/520258
  16. Muñoz-Cánoves P, Scheele C, Pedersen BK, Serrano AL (Sep 2013). "Interleukin-6 myokine signaling in skeletal muscle: a double-edged sword?". The FEBS Journal. 280 (17): 4131–48. doi:10.1111/febs.12338. PMC 4163639Freely accessible. PMID 23663276.
  17. Pedersen BK, Febbraio MA. Muscle as an endocrine organ: Focus on muscle-derived interleukin-6. Physiol Rev 88: 1379-1406, 2008.
  18. Heinrich PC, Behrmann I, Müller-Newen G, Schaper F, Graeve L (Sep 1998). "Interleukin-6-type cytokine signalling through the gp130/Jak/STAT pathway". The Biochemical Journal. 334 (Pt 2): 297–314. doi:10.1042/bj3340297. PMC 1219691Freely accessible. PMID 9716487.
  19. Kishimoto T, Akira S, Narazaki M, Taga T (Aug 1995). "Interleukin-6 family of cytokines and gp130". Blood. 86 (4): 1243–54. PMID 7632928.
  20. Heinrich PC, Behrmann I, Haan S, Hermanns HM, Müller-Newen G, Schaper F (Aug 2003). "Principles of interleukin (IL)-6-type cytokine signalling and its regulation". The Biochemical Journal. 374 (Pt 1): 1–20. doi:10.1042/BJ20030407. PMC 1223585Freely accessible. PMID 12773095.
  21. Schwantner A, Dingley AJ, Ozbek S, Rose-John S, Grötzinger J (Jan 2004). "Direct determination of the interleukin-6 binding epitope of the interleukin-6 receptor by NMR spectroscopy". The Journal of Biological Chemistry. 279 (1): 571–6. doi:10.1074/jbc.M311019200. PMID 14557255.
  22. Schuster B, Kovaleva M, Sun Y, Regenhard P, Matthews V, Grötzinger J, Rose-John S, Kallen KJ (Mar 2003). "Signaling of human ciliary neurotrophic factor (CNTF) revisited. The interleukin-6 receptor can serve as an alpha-receptor for CTNF". The Journal of Biological Chemistry. 278 (11): 9528–35. doi:10.1074/jbc.M210044200. PMID 12643274.
  23. Taga T, Hibi M, Hirata Y, Yamasaki K, Yasukawa K, Matsuda T, Hirano T, Kishimoto T (Aug 1989). "Interleukin-6 triggers the association of its receptor with a possible signal transducer, gp130". Cell. 58 (3): 573–81. doi:10.1016/0092-8674(89)90438-8. PMID 2788034.
  24. Kallen KJ, zum Büschenfelde KH, Rose-John S (Mar 1997). "The therapeutic potential of interleukin-6 hyperagonists and antagonists". Expert Opinion on Investigational Drugs. 6 (3): 237–66. doi:10.1517/13543784.6.3.237. PMID 15989626.
  25. Kristiansen OP, Mandrup-Poulsen T (Dec 2005). "Interleukin-6 and diabetes: the good, the bad, or the indifferent?". Diabetes. 54 Suppl 2: S114–24. doi:10.2337/diabetes.54.suppl_2.S114. PMID 16306329.
  26. Dubiński A, Zdrojewicz Z (Apr 2007). "[The role of interleukin-6 in development and progression of atherosclerosis]". Polski Merkuriusz Lekarski (in Polish). 22 (130): 291–4. PMID 17684929.
  27. Dowlati Y, Herrmann N, Swardfager W, Liu H, Sham L, Reim EK, Lanctôt KL (Mar 2010). "A meta-analysis of cytokines in major depression". Biological Psychiatry. 67 (5): 446–57. doi:10.1016/j.biopsych.2009.09.033. PMID 20015486.
  28. Swardfager W, Lanctôt K, Rothenburg L, Wong A, Cappell J, Herrmann N (Nov 2010). "A meta-analysis of cytokines in Alzheimer's disease". Biological Psychiatry. 68 (10): 930–41. doi:10.1016/j.biopsych.2010.06.012. PMID 20692646.
  29. Tackey E, Lipsky PE, Illei GG (2004). "Rationale for interleukin-6 blockade in systemic lupus erythematosus". Lupus. 13 (5): 339–43. doi:10.1191/0961203304lu1023oa. PMC 2014821Freely accessible. PMID 15230289.
  30. Gadó K, Domján G, Hegyesi H, Falus A (2000). "Role of INTERLEUKIN-6 in the pathogenesis of multiple myeloma". Cell Biology International. 24 (4): 195–209. doi:10.1006/cbir.2000.0497. PMID 10816321.
  31. Smith PC, Hobisch A, Lin DL, Culig Z, Keller ET (Mar 2001). "Interleukin-6 and prostate cancer progression". Cytokine & Growth Factor Reviews. 12 (1): 33–40. doi:10.1016/S1359-6101(00)00021-6. PMID 11312117.
  32. Hirohata S, Kikuchi H (Dec 2012). "Changes in biomarkers focused on differences in disease course or treatment in patients with neuro-Behçet's disease". Internal Medicine. 51 (24): 3359–65. doi:10.2169/internalmedicine.51.85834. PMID 23257520.
  33. Nishimoto N (May 2006). "Interleukin-6 in rheumatoid arthritis". Current Opinion in Rheumatology. 18 (3): 277–81. doi:10.1097/01.bor.0000218949.19860.d1. PMID 16582692.
  34. Barton BE (Aug 2005). "Interleukin-6 and new strategies for the treatment of cancer, hyperproliferative diseases and paraneoplastic syndromes". Expert Opinion on Therapeutic Targets. 9 (4): 737–52. doi:10.1517/14728222.9.4.737. PMID 16083340.
  35. Smolen JS, Maini RN (2006). "Interleukin-6: a new therapeutic target". Arthritis Research & Therapy. 8 Suppl 2 (Suppl 2): S5. doi:10.1186/ar1969. PMC 3226077Freely accessible. PMID 16899109.
  36. Emery P, Keystone E, Tony HP, Cantagrel A, van Vollenhoven R, Sanchez A, Alecock E, Lee J, Kremer J (Nov 2008). "IL-6 receptor inhibition with tocilizumab improves treatment outcomes in patients with rheumatoid arthritis refractory to anti-tumour necrosis factor biologicals: results from a 24-week multicentre randomised placebo-controlled trial". Annals of the Rheumatic Diseases. 67 (11): 1516–23. doi:10.1136/ard.2008.092932. PMID 18625622.
  37. Nishimoto N, Kanakura Y, Aozasa K, Johkoh T, Nakamura M, Nakano S, Nakano N, Ikeda Y, Sasaki T, Nishioka K, Hara M, Taguchi H, Kimura Y, Kato Y, Asaoku H, Kumagai S, Kodama F, Nakahara H, Hagihara K, Yoshizaki K, Kishimoto T (Oct 2005). "Humanized anti-interleukin-6 receptor antibody treatment of multicentric Castleman disease". Blood. 106 (8): 2627–32. doi:10.1182/blood-2004-12-4602. PMID 15998837.
  38. Yokota S, Imagawa T, Mori M, Miyamae T, Aihara Y, Takei S, Iwata N, Umebayashi H, Murata T, Miyoshi M, Tomiita M, Nishimoto N, Kishimoto T (Mar 2008). "Efficacy and safety of tocilizumab in patients with systemic-onset juvenile idiopathic arthritis: a randomised, double-blind, placebo-controlled, withdrawal phase III trial". Lancet. 371 (9617): 998–1006. doi:10.1016/S0140-6736(08)60454-7. PMID 18358927.
  39. First IL-6–blocking drug nears approval for rare blood disorder, Nature Medicine, October 7, 2013
  40. Anestakis D, Petanidis S, Kalyvas S, Nday CM, Tsave O, Kioseoglou E, Salifoglou A (2015). "Mechanisms and applications of interleukins in cancer immunotherapy". International Journal of Molecular Sciences. 16 (1): 1691–710. doi:10.3390/ijms16011691. PMID 25590298.
  41. Li J, Mo HY, Xiong G, Zhang L, He J, Huang ZF, Liu ZW, Chen QY, Du ZM, Zheng LM, Qian CN, Zeng YX (Oct 2012). "Tumor microenvironment macrophage inhibitory factor directs the accumulation of interleukin-17-producing tumor-infiltrating lymphocytes and predicts favorable survival in nasopharyngeal carcinoma patients". The Journal of Biological Chemistry. 287 (42): 35484–95. doi:10.1074/jbc.M112.367532. PMID 22893706.
  42. Xie G, Yao Q, Liu Y, Du S, Liu A, Guo Z, Sun A, Ruan J, Chen L, Ye C, Yuan Y (Apr 2012). "IL-6-induced epithelial-mesenchymal transition promotes the generation of breast cancer stem-like cells analogous to mammosphere cultures". International Journal of Oncology. 40 (4): 1171–9. doi:10.3892/ijo.2011.1275. PMID 22134360.
  43. Miao JW, Liu LJ, Huang J (Jul 2014). "Interleukin-6-induced epithelial-mesenchymal transition through signal transducer and activator of transcription 3 in human cervical carcinoma". International Journal of Oncology. 45 (1): 165–76. doi:10.3892/ijo.2014.2422. PMID 24806843.
  44. Gasche JA, Hoffmann J, Boland CR, Goel A (Sep 2011). "Interleukin-6 promotes tumorigenesis by altering DNA methylation in oral cancer cells". International Journal of Cancer. Journal International Du Cancer. 129 (5): 1053–63. doi:10.1002/ijc.25764. PMID 21710491.
  45. "Cancer Patients Typically Have Increased Interleukin-6 Levels". American Society of Clinical Oncology 2006 Annual Meeting, Abstracts 8632 and 8633. Medscape.com. 2006-06-26.
  46. Bellone G, Smirne C, Mauri FA, Tonel E, Carbone A, Buffolino A, Dughera L, Robecchi A, Pirisi M, Emanuelli G (Jun 2006). "Cytokine expression profile in human pancreatic carcinoma cells and in surgical specimens: implications for survival". Cancer Immunology, Immunotherapy. 55 (6): 684–98. doi:10.1007/s00262-005-0047-0. PMID 16094523.
  47. Smith SE, Li J, Garbett K, Mirnics K, Patterson PH (Oct 2007). "Maternal immune activation alters fetal brain development through interleukin-6". The Journal of Neuroscience. 27 (40): 10695–702. doi:10.1523/JNEUROSCI.2178-07.2007. PMC 2387067Freely accessible. PMID 17913903.
  48. 1 2 3 4 Kundakovic M, Chen Y, Guidotti A, Grayson DR (Feb 2009). "The reelin and GAD67 promoters are activated by epigenetic drugs that facilitate the disruption of local repressor complexes". Molecular Pharmacology. 75 (2): 342–54. doi:10.1124/mol.108.051763. PMC 2684898Freely accessible. PMID 19029285.
  49. 1 2 Hodge DR, Cho E, Copeland TD, Guszczynski T, Yang E, Seth AK, Farrar WL (2007). "IL-6 enhances the nuclear translocation of DNA cytosine-5-methyltransferase 1 (DNMT1) via phosphorylation of the nuclear localization sequence by the AKT kinase". Cancer Genomics & Proteomics. 4 (6): 387–98. PMID 18204201.
  50. Foran E, Garrity-Park MM, Mureau C, Newell J, Smyrk TC, Limburg PJ, Egan LJ (Apr 2010). "Upregulation of DNA methyltransferase-mediated gene silencing, anchorage-independent growth, and migration of colon cancer cells by interleukin-6". Molecular Cancer Research. 8 (4): 471–81. doi:10.1158/1541-7786.MCR-09-0496. PMID 20354000.
  51. Guidotti A, Auta J, Davis JM, Di-Giorgi-Gerevini V, Dwivedi Y, Grayson DR, Impagnatiello F, Pandey G, Pesold C, Sharma R, Uzunov D, Costa E, DiGiorgi Gerevini V (Nov 2000). "Decrease in reelin and glutamic acid decarboxylase67 (GAD67) expression in schizophrenia and bipolar disorder: a postmortem brain study". Archives of General Psychiatry. 57 (11): 1061–9. doi:10.1001/archpsyc.57.11.1061. PMID 11074872.
  52. 1 2 Gandal MJ, Sisti J, Klook K, Ortinski PI, Leitman V, Liang Y, Thieu T, Anderson R, Pierce RC, Jonak G, Gur RE, Carlson G, Siegel SJ (2012). "GABAB-mediated rescue of altered excitatory-inhibitory balance, gamma synchrony and behavioral deficits following constitutive NMDAR-hypofunction". Translational Psychiatry. 2: e142. doi:10.1038/tp.2012.69. PMC 3410621Freely accessible. PMID 22806213.
  53. Uhlhaas PJ, Singer W (Feb 2010). "Abnormal neural oscillations and synchrony in schizophrenia". Nature Reviews. Neuroscience. 11 (2): 100–13. doi:10.1038/nrn2774. PMID 20087360.
  54. 1 2 3 Sharma RP, Tun N, Grayson DR (2008). "Depolarization induces downregulation of DNMT1 and DNMT3a in primary cortical cultures". Epigenetics. 3 (2): 74–80. doi:10.4161/epi.3.2.6103. PMID 18536530.
  55. Hwang JP, Tsai SJ, Hong CJ, Yang CH, Lirng JF, Yang YM (Dec 2006). "The Val66Met polymorphism of the brain-derived neurotrophic-factor gene is associated with geriatric depression". Neurobiology of Aging. 27 (12): 1834–7. doi:10.1016/j.neurobiolaging.2005.10.013. PMID 16343697.
  56. Ethell IM, Pasquale EB (Feb 2005). "Molecular mechanisms of dendritic spine development and remodeling". Progress in Neurobiology. 75 (3): 161–205. doi:10.1016/j.pneurobio.2005.02.003. PMID 15882774.
  57. Greicius MD, Flores BH, Menon V, Glover GH, Solvason HB, Kenna H, Reiss AL, Schatzberg AF (Sep 2007). "Resting-state functional connectivity in major depression: abnormally increased contributions from subgenual cingulate cortex and thalamus". Biological Psychiatry. 62 (5): 429–37. doi:10.1016/j.biopsych.2006.09.020. PMC 2001244Freely accessible. PMID 17210143.
  58. 1 2 Somerville LH, Heatherton TF, Kelley WM (Aug 2006). "Anterior cingulate cortex responds differentially to expectancy violation and social rejection". Nature Neuroscience. 9 (8): 1007–8. doi:10.1038/nn1728. PMID 16819523.
  59. Azzolina A, Bongiovanni A, Lampiasi N (Dec 2003). "Substance P induces TNF-alpha and IL-6 production through NF kappa B in peritoneal mast cells". Biochimica et Biophysica Acta. 1643 (1-3): 75–83. doi:10.1016/j.bbamcr.2003.09.003. PMID 14654230.
  60. Haapakoski R, Mathieu J, Ebmeier KP, Alenius H, Kivimäki M (Oct 2015). "Cumulative meta-analysis of interleukins 6 and 1β, tumour necrosis factor α and C-reactive protein in patients with major depressive disorder". Brain, Behavior, and Immunity. 49: 206–15. doi:10.1016/j.bbi.2015.06.001. PMC 4566946Freely accessible. PMID 26065825.
  61. Ratti E, Bettica P, Alexander R, Archer G, Carpenter D, Evoniuk G, Gomeni R, Lawson E, Lopez M, Millns H, Rabiner EA, Trist D, Trower M, Zamuner S, Krishnan R, Fava M (May 2013). "Full central neurokinin-1 receptor blockade is required for efficacy in depression: evidence from orvepitant clinical studies". Journal of Psychopharmacology. 27 (5): 424–34. doi:10.1177/0269881113480990. PMID 23539641.
  62. Kramer MS, Cutler N, Feighner J, Shrivastava R, Carman J, Sramek JJ, Reines SA, Liu G, Snavely D, Wyatt-Knowles E, Hale JJ, Mills SG, MacCoss M, Swain CJ, Harrison T, Hill RG, Hefti F, Scolnick EM, Cascieri MA, Chicchi GG, Sadowski S, Williams AR, Hewson L, Smith D, Carlson EJ, Hargreaves RJ, Rupniak NM (Sep 1998). "Distinct mechanism for antidepressant activity by blockade of central substance P receptors". Science. 281 (5383): 1640–5. doi:10.1126/science.281.5383.1640. PMID 9733503.
  63. Musselman DL, Miller AH, Porter MR, Manatunga A, Gao F, Penna S, Pearce BD, Landry J, Glover S, McDaniel JS, Nemeroff CB (Aug 2001). "Higher than normal plasma interleukin-6 concentrations in cancer patients with depression: preliminary findings". The American Journal of Psychiatry. 158 (8): 1252–7. doi:10.1176/appi.ajp.158.8.1252. PMID 11481159.
  64. Zhu GF, Chancellor-Freeland C, Berman AS, Kage R, Leeman SE, Beller DI, Black PH (Jun 1996). "Endogenous substance P mediates cold water stress-induced increase in interleukin-6 secretion from peritoneal macrophages" (PDF). The Journal of Neuroscience. 16 (11): 3745–52. PMID 8642417.
  65. Clinical trial number NCT02473289 for "An Efficacy and Safety Study of Sirukumab in Participants With Major Depressive Disorder." at ClinicalTrials.gov
  66. Peters MC, McGrath KW, Hawkins GA, Hastie AT, Levy BD, Israel E, Phillips BR, Mauger DT, Comhair SA, Erzurum SC, Johansson MW, Jarjour NN, Coverstone AM, Castro M, Holguin F, Wenzel SE, Woodruff PG, Bleecker ER, Fahy JV (July 2016). "Plasma interleukin-6 concentrations, metabolic dysfunction, and asthma severity: a cross-sectional analysis of two cohorts". The Lancet. Respiratory Medicine. 4 (7): 574–84. doi:10.1016/S2213-2600(16)30048-0. PMID 27283230.

Further reading

  • De Kloet ER, Oitzl MS, Schöbitz B (1994). "Cytokines and the brain corticosteroid receptor balance: relevance to pathophysiology of neuroendocrine-immune communication". Psychoneuroendocrinology. 19 (2): 121–34. doi:10.1016/0306-4530(94)90002-7. PMID 8190832. 
  • Morishita R, Aoki M, Yo Y, Ogihara T (Jun 2002). "Hepatocyte growth factor as cardiovascular hormone: role of HGF in the pathogenesis of cardiovascular disease". Endocrine Journal. 49 (3): 273–84. doi:10.1507/endocrj.49.273. PMID 12201209. 
  • Ishihara K, Hirano T (2003). "IL-6 in autoimmune disease and chronic inflammatory proliferative disease". Cytokine & Growth Factor Reviews. 13 (4-5): 357–68. doi:10.1016/S1359-6101(02)00027-8. PMID 12220549. 
  • Culig Z, Bartsch G, Hobisch A (Nov 2002). "Interleukin-6 regulates androgen receptor activity and prostate cancer cell growth". Molecular and Cellular Endocrinology. 197 (1-2): 231–8. doi:10.1016/S0303-7207(02)00263-0. PMID 12431817. 
  • Rattazzi M, Puato M, Faggin E, Bertipaglia B, Zambon A, Pauletto P (Oct 2003). "C-reactive protein and interleukin-6 in vascular disease: culprits or passive bystanders?". Journal of Hypertension. 21 (10): 1787–803. doi:10.1097/01.hjh.0000084735.53355.44. PMID 14508181. 
  • Berger FG (Dec 2004). "The interleukin-6 gene: a susceptibility factor that may contribute to racial and ethnic disparities in breast cancer mortality". Breast Cancer Research and Treatment. 88 (3): 281–5. doi:10.1007/s10549-004-0726-0. PMID 15609131. 
  • Stenvinkel P, Ketteler M, Johnson RJ, Lindholm B, Pecoits-Filho R, Riella M, Heimbürger O, Cederholm T, Girndt M (Apr 2005). "IL-10, IL-6, and TNF-alpha: central factors in the altered cytokine network of uremia--the good, the bad, and the ugly". Kidney International. 67 (4): 1216–33. doi:10.1111/j.1523-1755.2005.00200.x. PMID 15780075. 
  • Vgontzas AN, Bixler EO, Lin HM, Prolo P, Trakada G, Chrousos GP (2005). "IL-6 and its circadian secretion in humans". Neuroimmunomodulation. 12 (3): 131–40. doi:10.1159/000084844. PMID 15905620. 
  • Jones SA (Sep 2005). "Directing transition from innate to acquired immunity: defining a role for IL-6". Journal of Immunology. 175 (6): 3463–8. doi:10.4049/jimmunol.175.6.3463. PMID 16148087. 
  • Copeland KF (Dec 2005). "Modulation of HIV-1 transcription by cytokines and chemokines". Mini Reviews in Medicinal Chemistry. 5 (12): 1093–101. doi:10.2174/138955705774933383. PMID 16375755. 
  • Mastorakos G, Ilias I (Nov 2006). "Interleukin-6: a cytokine and/or a major modulator of the response to somatic stress". Annals of the New York Academy of Sciences. 1088: 373–81. doi:10.1196/annals.1366.021. PMID 17192581. 

External links

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