IKZF2
IKZF2 | |||||||||||||||||||||||||||||||||||||||||||||||||||
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Aliases | IKZF2, ANF1A2, HELIOS, ZNF1A2, ZNFN1A2, IKAROS family zinc finger 2 | ||||||||||||||||||||||||||||||||||||||||||||||||||
External IDs | OMIM: 606234; MGI: 1342541; HomoloGene: 22659; GeneCards: IKZF2; OMA:IKZF2 - orthologs | ||||||||||||||||||||||||||||||||||||||||||||||||||
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Zinc finger protein Helios is a protein that in humans is encoded by the IKZF2 gene.[5][6][7] This protein is a member of Ikaros family of transcription factors.[8]
This gene encodes a member of the Ikaros family of zinc-finger proteins. This family of transcription factors consists of five members: Ikaros (Ikzf1), Helios (Ikzf2), Aiolos (Ikzf3), Eos (Ikzf4), and Pegasus (Ikzf5). The Ikaros family members are involved in the hematopoietic development, some to a greater extent than others with Ikaros being expressed in all hematopoietic cells.[8] This protein forms homo- or hetero-dimers with other Ikaros family members. Multiple transcript variants encoding different isoforms have been found for this gene, but the biological relevance of some variants has not been determined.[7]
When these factors are missing or altered, lymphocytes suffer from defective development. Since Ikaros family members can interact with each other, it is probable that when one transcription factor is defected, others can substitute it. Because of this, it is rather difficult to assess precise function to each transcription factor.[9]
Structure
Ikaros family members are characterised by having 4 N-terminal zinc finger domains, except for Pegasus, which has only 3. These are the key domains for DNA binding and stabilization of DNA-protein interactions. They also have C-terminal zinc finger domains which serve as a site for interactions with other proteins and hetero- or homodimerization with other family members.[9]
Function
As transcription factor
Helios is said to repress the IL-2 expression in Tregs. This function was also confirmed for Eos, another member of Ikaros family of transcription factors, pointing to their redundant functions. Helios interacts with Foxp3 to lower IL2 expression. They form a complex and bind to the IL2 locus causing repressive epigenetic modifications, namely reduced histone H3 acetylation.[10] Loss of Helios causes decreased binding of Foxp3 to the IL2 promoter and milder IL-2 repression.[9]
Helios is also said to be part of the positive feedback loop of IL-2. It positively affects the IL-2Rα-STAT5 pathway.[11][12] IL-2 maintains Helios expression. IL-2 is probably not the only factor positively affecting Helios expression.[11]
As a tumor suppressor
Helios is said to also function as a tumor suppressor. Such role of Helios was observed when a dominant negative isoform of this protein, that lacked three out of four N-terminal zinc fingers, was found in adult T cell malignancies. Indeed, forced expression of this isoform of Helios did lead to the development of T cell lymphoma in a murine model. However, the ectopic expression of wildtype Helios in B cells results in lymphomas as well. This suggests that Helios might act as a tumor suppressor only in the cells that it is naturally expressed in, when expressed in other cells, it is rather tumorigenic.[8]
Since Helios-deficient Tregs have the ability to produce IFN-γ and TNF-α, they seem to be useful in anti-tumor responses. Such Treg cells can infiltrate the tumor without keeping their suppressive function, subsequently producing IFN-γ and TNF-α, which could help with slowing the tumor growth. Moreover, the loss of suppressive phenotype of Treg cells was observed in tumors, but not in splenic Tregs, which can potentially have great clinical significance. Based on these findings, Helios could be considered a powerful tool in the anti-tumor therapy. However, it is too early for such conclusion and even though the data seem promising, more research needs to be done in this area.[11]
In immune cells
Helios is expressed in many mature T lymphocyte populations, however, it is best known for its expression in T regulatory cell (Treg) population.[9]
Tregs
Treg cells are a population of T cells that can suppress the effector function of other immune cells.[13] We can divide Treg cells into two main subsets: thymus-derived Treg cell (tTreg) and peripherally-induced Treg cell (pTreg). TTregs are the subset of cells that develops in thymus from T lymphocytes that recognise self-antigens. Whereas pTregs are lymphocytes that are induced in the periphery originally from CD4+ Foxp3- cells and which subsequently acquire suppressive function. Both Treg cells subsets are Foxp3+.[8]
Helios is expressed only in 70-80 % of Treg cells in mice and humans. The fact that Helios is not expressed in all Tregs was in the past explained by the observations that Helios could actually be found only in tTregs (Tregs that arise from the thymus), not pTregs. This believe was supported by experimental data, that discovered the expression of Helios only in early Foxp3+ thymocytes or that did not find the expression of Helios in Tregs in the periphery in the first few days. Moreover, experiments generating induced Tregs (iTregs) in vitro, did not find any expression of Helios in the cells. Thus, Helios used to be considered a tTreg marker.[8]
Recently, the idea of Helios as a tTregs specific marker, has become controversial. Current studies indicate that even iTregs can express Helios transcription factor. Thus, it is unclear whether Helios can be used as a marker for tTregs.[8][13]
Current data suggest that Helios is a marker of Treg stability rather than a specific marker for differentiation between tTregs and pTregs.[11]
It was discovered that Helios is not essential for early development of T cells in thymus, but it is important for Treg suppressive function later in their life. This conclusion was drawn when the loss of Helios in T cells did not have any effect on T cell development and homeostasis of the immune system in a mouse model. However, it did result in a defective immune regulation later in the life with the onset of autoimmunity resulting from defective Treg function.[11]
Tregs that lack Helios have lower expression of Foxp3 and lower activation of STAT5. Helios-deficient Tregs also seem to produce effector cytokines that are not usually produced by this cell type – interleukin 17 (IL-17), interferon gamma (IFN-γ) and tumor necrosis factor alpha (TNF-α).[10] Thus, this suggests that Helios is important for the identity of Treg cell and stability of their cytokine profile. It is important to mention, that so far we do not have enough knowledge about the mechanism of Helios keeping Treg stability and even about Helios's own expression in Tregs. Thus, there is a need to uncover the mechanism behind these findings.[11]
In other immune cells
Beside CD4+ Tregs, Helios is also expressed in murine NK cells. In this immune cell subset, Helios is expressed early during their development, and it is later downregulated.[8]
Helios is also expressed in CD8+ regulatory T cells. Helios maintains their suppressive function similarly to the CD4+ Tregs.[12]
References
- ^ a b c GRCh38: Ensembl release 89: ENSG00000030419 – Ensembl, May 2017
- ^ a b c GRCm38: Ensembl release 89: ENSMUSG00000025997 – 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.
- ^ Hahm K, Cobb BS, McCarty AS, Brown KE, Klug CA, Lee R, et al. (March 1998). "Helios, a T cell-restricted Ikaros family member that quantitatively associates with Ikaros at centromeric heterochromatin". Genes & Development. 12 (6): 782–796. doi:10.1101/gad.12.6.782. PMC 316626. PMID 9512513.
- ^ Kelley CM, Ikeda T, Koipally J, Avitahl N, Wu L, Georgopoulos K, Morgan BA (April 1998). "Helios, a novel dimerization partner of Ikaros expressed in the earliest hematopoietic progenitors". Current Biology. 8 (9): 508–515. Bibcode:1998CBio....8..508K. doi:10.1016/S0960-9822(98)70202-7. PMID 9560339.
- ^ a b "Entrez Gene: IKZF2 IKAROS family zinc finger 2 (Helios)".
- ^ a b c d e f g Thornton AM, Shevach EM (November 2019). "Helios: still behind the clouds". Immunology. 158 (3): 161–170. doi:10.1111/imm.13115. PMC 6797934. PMID 31517385.
- ^ a b c d Read KA, Jones DM, Freud AG, Oestreich KJ (March 2021). "Established and emergent roles for Ikaros transcription factors in lymphoid cell development and function". Immunological Reviews. 300 (1): 82–99. doi:10.1111/imr.12936. PMC 8015388. PMID 33331000.
- ^ a b Powell MD, Read KA, Sreekumar BK, Oestreich KJ (2019-06-06). "Ikaros Zinc Finger Transcription Factors: Regulators of Cytokine Signaling Pathways and CD4+ T Helper Cell Differentiation". Frontiers in Immunology. 10: 1299. doi:10.3389/fimmu.2019.01299. PMC 6563078. PMID 31244845.
- ^ a b c d e f Chougnet C, Hildeman D (August 2016). "Helios-controller of Treg stability and function". Translational Cancer Research. 5 (Suppl 2): S338–S341. doi:10.21037/tcr.2016.07.37. PMC 6333417. PMID 30656143.
- ^ a b Nakagawa H, Wang L, Cantor H, Kim HJ (2018-01-01). Alt F (ed.). New Insights into the Biology of CD8 Regulatory T Cells. Advances in Immunology. Vol. 140. Academic Press. pp. 1–20. doi:10.1016/bs.ai.2018.09.001. ISBN 978-0-12-815186-0. PMID 30366517.
- ^ a b Mohr A, Malhotra R, Mayer G, Gorochov G, Miyara M (2018). "Human FOXP3+ T regulatory cell heterogeneity". Clinical & Translational Immunology. 7 (1): e1005. doi:10.1002/cti2.1005. PMC 5822410. PMID 29484183.
Further reading
- Rebollo A, Schmitt C (June 2003). "Ikaros, Aiolos and Helios: transcription regulators and lymphoid malignancies". Immunology and Cell Biology. 81 (3): 171–175. doi:10.1046/j.1440-1711.2003.01159.x. PMID 12752680. S2CID 43733744.
- Sridharan R, Smale ST (October 2007). "Predominant interaction of both Ikaros and Helios with the NuRD complex in immature thymocytes". The Journal of Biological Chemistry. 282 (41): 30227–30238. doi:10.1074/jbc.M702541200. PMID 17681952.
- Tabayashi T, Ishimaru F, Takata M, Kataoka I, Nakase K, Kozuka T, Tanimoto M (February 2007). "Characterization of the short isoform of Helios overexpressed in patients with T-cell malignancies". Cancer Science. 98 (2): 182–188. doi:10.1111/j.1349-7006.2006.00372.x. PMC 11159431. PMID 17297655. S2CID 9787574.
- Sun L, Kerawalla H, Wu X, Lehnert MS, Uckun FM (April 2002). "Expression of a unique helios isoform in human leukemia cells". Leukemia & Lymphoma. 43 (4): 841–849. doi:10.1080/10428190290016980. PMID 12153174. S2CID 8170745.
- Durand C, Kerfourn F, Charlemagne J, Fellah JS (June 2002). "Identification and expression of Helios, a member of the Ikaros family, in the Mexican axolotl: implications for the embryonic origin of lymphocyte progenitors". European Journal of Immunology. 32 (6): 1748–1752. doi:10.1002/1521-4141(200206)32:6<1748::AID-IMMU1748>3.0.CO;2-B. PMID 12115658.
- Nakase K, Ishimaru F, Fujii K, Tabayashi T, Kozuka T, Sezaki N, et al. (April 2002). "Overexpression of novel short isoforms of Helios in a patient with T-cell acute lymphoblastic leukemia". Experimental Hematology. 30 (4): 313–317. doi:10.1016/S0301-472X(01)00796-2. PMID 11937265.
- Perdomo J, Holmes M, Chong B, Crossley M (December 2000). "Eos and pegasus, two members of the Ikaros family of proteins with distinct DNA binding activities". The Journal of Biological Chemistry. 275 (49): 38347–38354. doi:10.1074/jbc.M005457200. PMID 10978333.
- Hosokawa Y, Maeda Y, Seto M (October 1999). "Human Helios, an Ikaros-related zinc finger DNA binding protein: cDNA cloning and tissue expression pattern". Immunogenetics. 50 (1–2): 106–108. doi:10.1007/s002510050696. PMID 10541817. S2CID 39219337.
External links
- IKZF2+protein,+human at the U.S. National Library of Medicine Medical Subject Headings (MeSH)
This article incorporates text from the United States National Library of Medicine, which is in the public domain.