HLA-F

HLA class I histocompatibility antigen, alpha chain F is a protein that in humans is encoded by the HLA-F gene.[4][5]

HLA-F
Identifiers
AliasesHLA-F, CDA12, HLA-5.4, HLA-CDA12, major histocompatibility complex, class I, F
External IDsOMIM: 143110 MGI: 3647514 HomoloGene: 133121 GeneCards: HLA-F
Gene location (Human)
Chr.Chromosome 6 (human)[1]
Band6p22.1Start29,722,775 bp[1]
End29,738,528 bp[1]
RNA expression pattern


More reference expression data
Orthologs
SpeciesHumanMouse
Entrez

3134

630294

Ensembl

n/a

UniProt

P30511

Q0WXH6

RefSeq (mRNA)

NM_001098478
NM_001098479
NM_018950

NM_001177467

RefSeq (protein)

NP_001091948
NP_001091949
NP_061823

NP_001170938

Location (UCSC)Chr 6: 29.72 – 29.74 Mbn/a
PubMed search[2][3]
Wikidata
View/Edit HumanView/Edit Mouse

HLA-F

The Major Histocompatibility Complex (MHC) is a group of cell surface proteins that in humans is also called the Human Leukocyte Antigen (HLA) complex. These proteins are encoded by a cluster of genes known as the HLA locus. The HLA locus occupies a ~ 3Mbp stretch that is located on the short arm of chromosome 6, specifically on 6p21.1-21.3.[6] The MHC proteins are classified into three main categories, namely class I, II, and III. There are over 140 genes within the HLA locus and they are often called HLA genes.[7][8] HLA-A, B, and C are the classical class I genes and HLA-E, F and G are the nonclassical class I genes.[9][10] The protein encoded from the gene HLA-F was originally isolated from the human lymphoblastoid cell line 721.[11]

Gene

The HLA-F gene is located on the short arm of chromosome 6, telomeric to the HLA-A locus.[9] HLA-F has little allelic polymorphism[12] and is highly conserved in other primates.[13] HLA-F appears to be a recombinant between two multigene families, one that comprises conserved sequences found in all class I proteins (single transmembrane span) and another distinct family of genes with a conserved 3’ UTR. Many of these genes are highly transcribed and differentially expressed.[4]

Protein

The HLA-F protein is a ~40-41 kDa molecule with conserved domains.[14] Exon 7 is absent from the mRNA of HLA-F.[4][15] The absence of this exon produces a modification in the cytoplasmic tail of the protein making it shorter relative to classical HLA class-I proteins.[4] The cytoplasmic tail helps HLA-F exit the endoplasmic reticulum,[16] and that function is primarily done by the amino acid valine found at the C-terminal end of the tail.[16][17]

Expression

Classic HLA class I molecules interact with HLA-F through their heavy chain.[17] However, HLA class I molecules only interact with HLA-F when they are in the form of an open conformer (free of peptide). Thus, HLA-F is expressed independently of bound peptide.[17][18]

Intracellular expression

HLA-F is expressed intracellularly in peripheral blood lymphocytes (PBL), resting lymphocyte cells (B, T, NK, and monocytes), tonsils, spleen, thymus, bladder, brain, colon, kidney, liver, lymphoblast, T cell leukemia, choriocarcinoma, and carcinoma.[14][19][20]

Extracellular expression

HLA-F is expressed on the cell surface of activated lymphocytes, HeLa cells, EBV-transformed lymphoblastoid cells, and in some activated monocyte cell lines.[16][19] The surface expression of HLA-F coincides with the activated immune response since HLA-F is mostly found on the surface of stimulated T memory cells but not on circulating regulatory T cells.[21]

Expression during pregnancy

HLA-F is expressed on the cells that surround the forming placenta (called extravillous trophoblasts), which are in direct contact with the maternal uterine cells.[22] In these cells, HLA-F is expressed both intracellularly and on the surface.[22]

Function

HLA-F belongs to the non-classical HLA class I heavy chain paralogues. Compared to classical HLA class I molecules, it exhibits very few polymorphisms. This class I molecule mainly exists as a heterodimer associated with the invariant light chain beta-2 microglobulin. The heavy chain is approximately 42 kDa and its gene contains 8 exons. Exon one encodes the leader peptide, exons 2 and 3 encode the alpha1 and alpha2 domains, the putative peptide binding sites, exon 4 encodes the alpha3 domain, exon 5 and 6 encode the transmembrane region and exons 7 and 8 the cytoplasmic tail. However, exons 7 and 8 (the cytoplasmic tail) are not translated due to an in-frame translation termination codon in exon 6.[5]

HLA-F is currently the most enigmatic of the HLA molecules. Hence, its precise functions still remain to be resolved. Though, in contrast to other HLA molecules, it mainly resides intracellularly and rarely reaches the cell surface, e.g. upon activation of NK, B and T cells. Unlike classical HLA class I molecules, which possess ten highly conserved amino acids responsible for antigen recognition, HLA-F only has 5, suggesting a biological function different from peptide presentation. Upon immune cell activation, HLA-F binds free forms of HLA class I molecules and reaches the cell surface as heterodimer. In this way HLA-F stabilizes HLA class I molecules that haven't yet bound peptides, thereby acting as a chaperone and transporting the free HLA class I to, on, and from the cell surface.

Association with specialized ligands

HLA-F has been observed only in a subset of cell membranes, mostly B cells and activated lymphocytes.[22] As a result, it has been suggested that its role involves association with specialized ligands that become available in the cell membrane of activated cells.[14] For example, HLA-F can act as a peptide binding of ILT2 and ILT4.[20][23] HLA-F can associate with TAP (transporter associated with antigen processing) and with the multimeric complex involved in peptide loading.[14][20][19][21]

Maternal immunity tolerance

It has been observed that all three non-classical HLA class I proteins are expressed in placental trophoblasts in contact with maternal immune cells.[12] This suggests that these proteins collaborate in the immune response and that HLA-F plays a fundamental role in both normal and maternal immune response.[12] HLA-F is also expressed in decidual extravillous trophoblasts.[22] During pregnancy, HLA-F interacts with T reg cells and extravillous trophoblasts mediating maternal tolerance to the fetus.[21]

Intermolecular communication

During the interaction between HLA-F and the heavy chain (HC) of HLA class I molecules in activated lymphocytes, HLA-F plays a role as a chaperone, escorting HLA class I HC to the cell surface and stabilizing its expression in the absence of peptide.[17] HLA-F binds most allelic forms of HLA class I open conformers, but it does not bind peptide complexes.[18]

The expression patterns of HLA-F in T cells suggest that HLA-F is involved in the communication pathway between T reg and activated T cells, where HLA-F signals that the immune response has been activated. During this communication, either HLA-F invokes secretion of inhibitory cytokines by the regulatory T cells or it provides a simple inhibitory signal to the regulatory T cells, allowing a normal immune response to proceed.[21]

Exogenous antigen cross-presentation

Viral proteins and other exogenous antigens decrease surface HLA-F expression because the exogenous proteins interact with HLA class I molecules at the same sites where HLA-F interacts, producing crosslinking. The exogenous proteins trigger an internal co-localization of both HLA-F and HLA class I molecules.[18] Exogenous proteins with higher affinity will interact more readily with HLA class I molecules triggering a dissociation of HLA class I/HLA-F, thereby reducing the surface levels of HLA-F.[18] HLA-F interacts with the open conformer (OC) of HLA class I and they function together in cross-presentation of exogenous antigen. Exogenous antigen binds to a structure on the surface of activated cells; this structure is composed of HLA class I open conformer and HLA-F; the peptide-binding point of contact is a specific HLA class I epitope on the exogenous antigen.[18]

Ligand during inflammatory response

The complex HLA-F/HLA class I OC has two distinct roles that are central to the inflammatory response: first, it is a ligand for KIR receptors and can both activate and inhibit KIR; second, it is involved in cross-presentation of exogenous antigen.[24][25][26]

The complex HLA-F/HLA class-I OC is a ligand for a subset of KIR (Killer-cell immunoglobulin-like receptor) receptors.[24] Specifically, it was demonstrated that HLA-F interacts physically and functionally with three KIR receptors: KIR3DL2, KIR2DS4, and KIR3DS1, particularly during the inflammatory response.[24][25][26] KIR directly interacts with both HLA-F and HLA class-I individually (i.e. no dimerization between HLA-F and HLA class-I is necessary).

Disease association

HLA-F has been linked to several diseases (Table). For cancer and tumors, HLA-F expression has been found to be enhanced in gastric adenocarcinoma,[27] breast cancer,[28] esophageal carcinoma,[29] lung cancer,[30] hepatocellular carcinoma,[31] and neuroblastoma.[32] HLA-F has also been associated with susceptibility to several diseases: hepatitis B,[33] Systemic Lupus Erythematosus,[34] and Type 1 diabetes (T1D).[35]

Disease associations
disease reference
gastric adenocarcinoma [27]
breast cancer [28]
esophageal carcinoma [29]
lung cancer [30]
hepatocellular carcinoma [31]
neuroblastoma [32]
hepatitis B [33]
Systemic Lupus Erythematosus [34]
Type 1 Diabetes [35]
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References

  1. ENSG00000237508, ENSG00000234487, ENSG00000206509, ENSG00000137403, ENSG00000235220, ENSG00000204642 GRCh38: Ensembl release 89: ENSG00000229698, ENSG00000237508, ENSG00000234487, ENSG00000206509, ENSG00000137403, ENSG00000235220, ENSG00000204642 - Ensembl, May 2017
  2. "Human PubMed Reference:". National Center for Biotechnology Information, U.S. National Library of Medicine.
  3. "Mouse PubMed Reference:". National Center for Biotechnology Information, U.S. National Library of Medicine.
  4. Geraghty DE, Wei XH, Orr HT, Koller BH (January 1990). "Human leukocyte antigen F (HLA-F). An expressed HLA gene composed of a class I coding sequence linked to a novel transcribed repetitive element". The Journal of Experimental Medicine. 171 (1): 1–18. doi:10.1084/jem.171.1.1. PMC 2187653. PMID 1688605.
  5. "Entrez Gene: HLA-F major histocompatibility complex, class I, F".
  6. Krebs J, Goldstein E, Kilpatrick S (2014). "Chapter 18: Somatic recombination and hypermutation in the immune system". Lewin's GENES XI. USA: Jones & Bartlett Learning. pp. 459–99. ISBN 978-1-4496-5985-1.
  7. Pyo CW, Williams LM, Moore Y, Hyodo H, Li SS, Zhao LP, Sageshima N, Ishitani A, Geraghty DE (May 2006). "HLA-E, HLA-F, and HLA-G polymorphism: genomic sequence defines haplotype structure and variation spanning the nonclassical class I genes". Immunogenetics. 58 (4): 241–51. doi:10.1007/s00251-005-0076-z. PMID 16570139.
  8. Smith WP, Vu Q, Li SS, Hansen JA, Zhao LP, Geraghty DE (May 2006). "Toward understanding MHC disease associations: partial resequencing of 46 distinct HLA haplotypes". Genomics. 87 (5): 561–71. doi:10.1016/j.ygeno.2005.11.020. PMID 16434165.
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  10. Geraghty DE, Wei XH, Orr HT, Koller BH (January 1990). "Human leukocyte antigen F (HLA-F). An expressed HLA gene composed of a class I coding sequence linked to a novel transcribed repetitive element". The Journal of Experimental Medicine. 171 (1): 1–18. doi:10.1084/jem.171.1.1. PMC 2187653. PMID 1688605.
  11. Geraghty DE, Koller BH, Orr HT (December 1987). "A human major histocompatibility complex class I gene that encodes a protein with a shortened cytoplasmic segment". Proceedings of the National Academy of Sciences of the United States of America. 84 (24): 9145–9. doi:10.1073/pnas.84.24.9145. PMC 299709. PMID 3480534.
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  13. Daza-Vamenta R, Glusman G, Rowen L, Guthrie B, Geraghty DE (August 2004). "Genetic divergence of the rhesus macaque major histocompatibility complex". Genome Research. 14 (8): 1501–15. doi:10.1101/gr.2134504. PMC 509259. PMID 15289473.
  14. Wainwright SD, Biro PA, Holmes CH (January 2000). "HLA-F is a predominantly empty, intracellular, TAP-associated MHC class Ib protein with a restricted expression pattern". Journal of Immunology. 164 (1): 319–28. doi:10.4049/jimmunol.164.1.319. PMID 10605026.
  15. O'Callaghan CA, Bell JI (June 1998). "Structure and function of the human MHC class Ib molecules HLA-E, HLA-F and HLA-G". Immunological Reviews. 163: 129–38. doi:10.1111/j.1600-065x.1998.tb01192.x. PMID 9700506.
  16. Boyle LH, Gillingham AK, Munro S, Trowsdale J (June 2006). "Selective export of HLA-F by its cytoplasmic tail". Journal of Immunology. 176 (11): 6464–72. doi:10.4049/jimmunol.176.11.6464. PMID 16709803.
  17. Goodridge JP, Burian A, Lee N, Geraghty DE (June 2010). "HLA-F complex without peptide binds to MHC class I protein in the open conformer form". Journal of Immunology. 184 (11): 6199–208. doi:10.4049/jimmunol.1000078. PMC 3777411. PMID 20483783.
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  22. Ishitani A, Sageshima N, Lee N, Dorofeeva N, Hatake K, Marquardt H, Geraghty DE (August 2003). "Protein expression and peptide binding suggest unique and interacting functional roles for HLA-E, F, and G in maternal-placental immune recognition". Journal of Immunology. 171 (3): 1376–84. doi:10.4049/jimmunol.171.3.1376. PMID 12874228.
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  25. Burian A, Wang KL, Finton KA, Lee N, Ishitani A, Strong RK, Geraghty DE (2016-09-20). "HLA-F and MHC-I Open Conformers Bind Natural Killer Cell Ig-Like Receptor KIR3DS1". PLOS ONE. 11 (9): e0163297. doi:10.1371/journal.pone.0163297. PMC 5029895. PMID 27649529.
  26. Garcia-Beltran WF, Hölzemer A, Martrus G, Chung AW, Pacheco Y, Simoneau CR, Rucevic M, Lamothe-Molina PA, Pertel T, Kim TE, Dugan H, Alter G, Dechanet-Merville J, Jost S, Carrington M, Altfeld M (September 2016). "Open conformers of HLA-F are high-affinity ligands of the activating NK-cell receptor KIR3DS1". Nature Immunology. 17 (9): 1067–74. doi:10.1038/ni.3513. PMC 4992421. PMID 27455421.
  27. Ishigami S, Arigami T, Okumura H, Uchikado Y, Kita Y, Kurahara H, Maemura K, Kijima Y, Ishihara Y, Sasaki K, Uenosono Y, Natsugoe S (April 2015). "Human leukocyte antigen (HLA)-E and HLA-F expression in gastric cancer". Anticancer Research. 35 (4): 2279–85. PMID 25862890.
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  29. Zhang X, Lin A, Zhang JG, Bao WG, Xu DP, Ruan YY, Yan WH (January 2013). "Alteration of HLA-F and HLA I antigen expression in the tumor is associated with survival in patients with esophageal squamous cell carcinoma". International Journal of Cancer. 132 (1): 82–9. doi:10.1002/ijc.27621. PMID 22544725.
  30. Lin A, Zhang X, Ruan YY, Wang Q, Zhou WJ, Yan WH (December 2011). "HLA-F expression is a prognostic factor in patients with non-small-cell lung cancer". Lung Cancer. 74 (3): 504–9. doi:10.1016/j.lungcan.2011.04.006. PMID 21561677.
  31. Xu Y, Han H, Zhang F, Lv S, Li Z, Fang Z (January 2015). "Lesion human leukocyte antigen-F expression is associated with a poor prognosis in patients with hepatocellular carcinoma". Oncology Letters. 9 (1): 300–304. doi:10.3892/ol.2014.2686. PMC 4246689. PMID 25435979.
  32. Morandi F, Cangemi G, Barco S, Amoroso L, Giuliano M, Gigliotti AR, Pistoia V, Corrias MV (2013-11-21). "Plasma levels of soluble HLA-E and HLA-F at diagnosis may predict overall survival of neuroblastoma patients". BioMed Research International. 2013: 956878. doi:10.1155/2013/956878. PMC 3856218. PMID 24350297.
  33. Zhang J, Pan L, Chen L, Feng X, Zhou L, Zheng S (March 2012). "Non-classical MHC-Ι genes in chronic hepatitis B and hepatocellular carcinoma". Immunogenetics. 64 (3): 251–8. doi:10.1007/s00251-011-0580-2. PMID 22015712.
  34. Jucaud V, Ravindranath MH, Terasaki PI, Morales-Buenrostro LE, Hiepe F, Rose T, Biesen R (March 2016). "Serum antibodies to human leucocyte antigen (HLA)-E, HLA-F and HLA-G in patients with systemic lupus erythematosus (SLE) during disease flares: Clinical relevance of HLA-F autoantibodies". Clinical and Experimental Immunology. 183 (3): 326–40. doi:10.1111/cei.12724. PMC 4750595. PMID 26440212.
  35. Richardson SJ, Rodriguez-Calvo T, Gerling IC, Mathews CE, Kaddis JS, Russell MA, Zeissler M, Leete P, Krogvold L, Dahl-Jørgensen K, von Herrath M, Pugliese A, Atkinson MA, Morgan NG (November 2016). "Islet cell hyperexpression of HLA class I antigens: a defining feature in type 1 diabetes". Diabetologia. 59 (11): 2448–58. doi:10.1007/s00125-016-4067-4. PMC 5042874. PMID 27506584.

Further reading

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