Nuclear receptor 4A1
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Location (UCSC) | Chr 12: 52.02 – 52.06 Mb | Chr 15: 101.15 – 101.17 Mb | |||||||
PubMed search | [3] | [4] |
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The nuclear receptor 4A1 (NR4A1 for "nuclear receptor subfamily 4 group A member 1") also known as Nur77, TR3, and NGFI-B is a protein that in humans is encoded by the NR4A1 gene.[5][6]
Nuclear receptor 4A1 (NR4A1) is a member of the
Nuclear receptor 4A1 plays a key role in mediating inflammatory responses in macrophages.[9] In addition, subcellular localization of the NR4A1 protein appears to play a key role in the survival and death of cells.[10]
Expression is inducible by
Structure
The NR4A1 gene contains seven exons. An amino terminal transactivation domain is encoded in exon 2, a DNA-binding domain in exons 3 and 4, and dimerisation and a ligand-binding domain is exons 5 to 7.[11]
The protein has an atypical ligand-binding domain that is unlike the classical ligand-binding domain in most nuclear receptors. The classical domain contains a ligand-receiving pocket and co-activator site, both of which are lacking in the NR4A family. Whereas most nuclear receptors have a hydrophobic surface that results in a cleft, NR4A1 has a hydrophilic surface.[7]
Cofactors interact with Nuclear receptor 4A1 at a hydrophobic region between helices 11 and 12 to modulate transcription.[7]
Function
Along with the two other NR4A family members, NR4A1 is expressed in macrophages following inflammatory stimuli. This process is mediated by the NF-κB (nuclear factor-kappa B) complex, a ubiquitous transcription factor involved in cellular response to stress.[9]
Nuclear receptor 4A1 can be induced by many physiological and physical stimuli. These include physiological stimuli such as "fatty acids, stress, prostaglandins, growth factors, calcium, inflammatory cytokines, peptide hormones, phorbol esters, and neurotransmitters" and physical stimuli including "magnetic fields, mechanical agitation (causing fluid shear stress), and membrane depolarization".[7] No endogenous ligands that bind to NR4A1 have yet been identified, so modulation occurs at the level of protein expression and posttranslational modification.Besides these, NR4A1 can mediate T cell function, the transcription factor NR4A1 is stably expressed at high levels in tolerant T cells. Overexpression of Nuclear receptor 4A1 inhibits effector T cell differentiation, whereas deletion of NR4A1 overcomes T cell tolerance and exaggerates effector function, as well as enhancing immunity against tumor and chronic virus. Mechanistically, NR4A1 is preferentially recruited to binding sites of the transcription factor AP-1, where it represses effector gene expression by inhibiting AP-1 function. NR4A1 binding also promotes acetylation of histone 3 at lysine 27 (H3K27ac), leading to activation of tolerance-related genes.[12]
There are several ligands that directly bind NR4A1, including cytosporone B, celastrol, and certain polyunsaturated fatty acids. These NR4A1 ligands bind at various NR4A1 sites and show activities that are dependent on ligand structure and cell context. These NR4A1 ligands may have relevance to treatment of cancer, metabolic disease, inflammation, and endometriosis.[13] NR4A1 may play a role in Drug-induced gingival overgrowth associated with exposure to phenytoin, nifedipine, and cyclosporine A.[14]
Biochemistry
Nuclear receptor 4A1 binds as a
The binding sites on the response elements for NR4A1, which are common to the two other members of the NR4A family, are:[7]
- NBRE - 5’-A/TAAAGGTCA,
- NurRE - a AAAT(G/A)(C/T)CA repeat,
- RXR - DX, a motif.
Evolution and homology
Nuclear receptor 4A1 has the systematic HUGO gene symbol NR4A1. It belongs to a group of three closely related orphan receptors, the NR4A family (NR4A). The other two members are Nuclear receptor 4A2 (NR4A2) and Nuclear receptor 4A3 (NR4A3).
Nuclear receptor 4A1 has a high degree of structural similarity with other family members at the DNA-binding domain with 91-95% sequence conservation. The C-terminal ligand-binding domain is conserved to a lesser extent at 60% and the N-terminal AB region is not conserved, differing in each member.[7]
The three members are similar in biochemistry and function. They are immediate early genes activated in a ligand-independent manner that bind at the homologous sites on response elements.[11]
Nuclear receptor 4A1 and the rest of the NR4A family are structurally similar to other nuclear receptor superfamily members, but contain an extra intron. The DNA-binding domain at exons 3 and 4 of the NR4A1 gene is conserved among all members of the nuclear receptor.[11]
NR4A1 has
Pathology
Along with 16 other genes, NR4A1 is a signature gene in the metastasis of some primary solid tumours. It is downregulated in this process.[19]
Interactions
Nuclear receptor 4A1 has been shown to
- AKT1,[20]
- Bcl-2,[21]
- HIF1A,[22]
- Nuclear receptor co-repressor 2,[23]
- Promyelocytic leukemia protein,[24]
- Retinoid X receptor alpha,[21] and
- Von Hippel-Lindau tumor suppressor.[22]
References
- ^ a b c GRCh38: Ensembl release 89: ENSG00000123358 – Ensembl, May 2017
- ^ a b c GRCm38: Ensembl release 89: ENSMUSG00000023034 – Ensembl, May 2017
- ^ "Human PubMed Reference:". National Center for Biotechnology Information, U.S. National Library of Medicine.
- ^ "Mouse PubMed Reference:". National Center for Biotechnology Information, U.S. National Library of Medicine.
- ^ a b "Entrez Gene: NR4A1 nuclear receptor subfamily 4, group A, member 1".
- ^ PMID 2626032.
- ^ PMID 16604165.
- S2CID 41639878.
- ^ PMID 16339277.
- S2CID 2217539.
- ^ PMID 9073077.
- PMID 30814730.
- S2CID 235360253.
- S2CID 235393903.
- PMID 16835233.
- PMID 9315652.
- PMID 16434970.
- PMID 17407572.
- S2CID 12059602.
- PMID 11274386.
- ^ PMID 14980220.
- ^ PMID 18305400.
- PMID 11559707.
- S2CID 23367035.
Further reading
- Winoto A, Littman DR (April 2002). "Nuclear hormone receptors in T lymphocytes". Cell. 109 Suppl (2): S57–S66. PMID 11983153.
- Engelse MA, Arkenbout EK, Pannekoek H, de Vries CJ (November 2003). "Activin and TR3 orphan receptor: two 'atheroprotective' genes as evidenced in dedicated mouse models". Clinical and Experimental Pharmacology & Physiology. 30 (11): 894–899. S2CID 11046562.
- Bondy GP (April 1991). "Phorbol ester, forskolin, and serum induction of a human colon nuclear hormone receptor gene related to the NUR 77/NGFI-B genes". Cell Growth & Differentiation. 2 (4): 203–208. PMID 1651101.
- Nakai A, Kartha S, Sakurai A, Toback FG, DeGroot LJ (October 1990). "A human early response gene homologous to murine nur77 and rat NGFI-B, and related to the nuclear receptor superfamily". Molecular Endocrinology. 4 (10): 1438–1443. PMID 2283997.
- Ryseck RP, Macdonald-Bravo H, Mattéi MG, Ruppert S, Bravo R (November 1989). "Structure, mapping and expression of a growth factor inducible gene encoding a putative nuclear hormonal binding receptor". The EMBO Journal. 8 (11): 3327–3335. PMID 2555161.
- Uemura H, Mizokami A, Chang C (March 1995). "Identification of a new enhancer in the promoter region of human TR3 orphan receptor gene. A member of steroid receptor superfamily". The Journal of Biological Chemistry. 270 (10): 5427–5433. PMID 7890657.
- Hirata Y, Kiuchi K, Chen HC, Milbrandt J, Guroff G (November 1993). "The phosphorylation and DNA binding of the DNA-binding domain of the orphan nuclear receptor NGFI-B". The Journal of Biological Chemistry. 268 (33): 24808–24812. PMID 8227042.
- Harrison DC, Roberts J, Campbell CA, Crook B, Davis R, Deen K, et al. (2000). "TR3 death receptor expression in the normal and ischaemic brain". Neuroscience. 96 (1): 147–160. S2CID 42030769.
- Li H, Kolluri SK, Gu J, Dawson MI, Cao X, Hobbs PD, et al. (August 2000). "Cytochrome c release and apoptosis induced by mitochondrial targeting of nuclear orphan receptor TR3". Science. 289 (5482): 1159–1164. PMID 10947977.
- Pekarsky Y, Hallas C, Palamarchuk A, Koval A, Bullrich F, Hirata Y, et al. (March 2001). "Akt phosphorylates and regulates the orphan nuclear receptor Nur77". Proceedings of the National Academy of Sciences of the United States of America. 98 (7): 3690–3694. PMID 11274386.
- Sohn YC, Kwak E, Na Y, Lee JW, Lee SK (November 2001). "Silencing mediator of retinoid and thyroid hormone receptors and activating signal cointegrator-2 as transcriptional coregulators of the orphan nuclear receptor Nur77". The Journal of Biological Chemistry. 276 (47): 43734–43739. PMID 11559707.
- Lee MO, Kang HJ, Cho H, Shin EC, Park JH, Kim SJ (November 2001). "Hepatitis B virus X protein induced expression of the Nur77 gene". Biochemical and Biophysical Research Communications. 288 (5): 1162–1168. PMID 11700033.
- Slagsvold HH, Østvold AC, Fallgren AB, Paulsen RE (March 2002). "Nuclear receptor and apoptosis initiator NGFI-B is a substrate for kinase ERK2". Biochemical and Biophysical Research Communications. 291 (5): 1146–1150. PMID 11883936.
- Wu WS, Xu ZX, Ran R, Meng F, Chang KS (May 2002). "Promyelocytic leukemia protein PML inhibits Nur77-mediated transcription through specific functional interactions". Oncogene. 21 (24): 3925–3933. S2CID 23367035.
- Liu S, Wu Q, Ye XF, Cai JH, Huang ZW, Su WJ (June 2002). "Induction of apoptosis by TPA and VP-16 is through translocation of TR3". World Journal of Gastroenterology. 8 (3): 446–450. PMID 12046067.
- Wansa KD, Harris JM, Muscat GE (September 2002). "The activation function-1 domain of Nur77/NR4A1 mediates trans-activation, cell specificity, and coactivator recruitment". The Journal of Biological Chemistry. 277 (36): 33001–33011. PMID 12082103.
- Chtarbova S, Nimmrich I, Erdmann S, Herter P, Renner M, Kitajewski J, Müller O (November 2002). "Murine Nr4a1 and Herpud1 are up-regulated by Wnt-1, but the homologous human genes are independent from beta-catenin activation". The Biochemical Journal. 367 (Pt 3): 723–728. PMID 12153396.
- Wu Q, Liu S, Ye XF, Huang ZW, Su WJ (October 2002). "Dual roles of Nur77 in selective regulation of apoptosis and cell cycle by TPA and ATRA in gastric cancer cells". Carcinogenesis. 23 (10): 1583–1592. PMID 12376465.
External links
- orphan+nuclear+receptor+NGFI-B at the U.S. National Library of Medicine Medical Subject Headings (MeSH)
- orphan+nuclear+receptor+TR3 at the U.S. National Library of Medicine Medical Subject Headings (MeSH)