Glial fibrillary acidic protein

(Redirected from GFAP (gene))

Glial fibrillary acidic protein (GFAP) is a protein that is encoded by the GFAP gene in humans.[5] It is a type III intermediate filament (IF) protein that is expressed by numerous cell types of the central nervous system (CNS), including astrocytes[6] and ependymal cells during development.[7] GFAP has also been found to be expressed in glomeruli and peritubular fibroblasts taken from rat kidneys,[8] Leydig cells of the testis in both hamsters[9] and humans,[10] human keratinocytes,[11] human osteocytes and chondrocytes[12] and stellate cells of the pancreas and liver in rats.[13]

GFAP
Available structures
PDBOrtholog search: PDBe RCSB
Identifiers
AliasesGFAP, ALXDRD, glial fibrillary acidic protein
External IDsOMIM: 137780; MGI: 95697; HomoloGene: 1554; GeneCards: GFAP; OMA:GFAP - orthologs
Orthologs
SpeciesHumanMouse
Entrez
Ensembl
UniProt
RefSeq (mRNA)

NM_002055
NM_001131019
NM_001242376
NM_001363846

NM_001131020
NM_010277

RefSeq (protein)

NP_001124491
NP_001229305
NP_002046
NP_001350775

NP_001124492
NP_034407

Location (UCSC)Chr 17: 44.9 – 44.92 MbChr 11: 102.78 – 102.79 Mb
PubMed search[3][4]
Wikidata
View/Edit HumanView/Edit Mouse

GFAP is closely related to the other three non-epithelial type III IF family members, vimentin, desmin and peripherin, which are all involved in the structure and function of the cell's cytoskeleton. GFAP is thought to help to maintain astrocyte mechanical strength[14] as well as the shape of cells, but its exact function remains poorly understood, despite the number of studies using it as a cell marker. The protein was named and first isolated and characterized by Lawrence F. Eng in 1969.[15] In humans, it is located on the long arm of chromosome 17.[16]

Structure

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Type III intermediate filaments contain three domains, named the head, rod and tail domains. The specific DNA sequence for the rod domain may differ between different type III intermediate filaments, but the structure of the protein is highly conserved. This rod domain coils around that of another filament to form a dimer, with the N-terminal and C-terminal of each filament aligned. Type III filaments such as GFAP are capable of forming both homodimers and heterodimers; GFAP can polymerize with other type III proteins.[17] GFAP and other type III IF proteins cannot assemble with keratins, the type I and II intermediate filaments: in cells that express both proteins, two separate intermediate filament networks form,[18] which can allow for specialization and increased variability.

To form networks, the initial GFAP dimers combine to make staggered tetramers,[19] which are the basic subunits of an intermediate filament. Since rod domains alone in vitro do not form filaments, the non-helical head and tail domains are necessary for filament formation.[17] The head and tail regions have greater variability of sequence and structure. In spite of this increased variability, the head of GFAP contains two conserved arginines and an aromatic residue that have been shown to be required for proper assembly.[20]

Function in the central nervous system

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GFAP is expressed in the central nervous system in astrocyte cells, and the concentration of GFAP differs between different regions in the CNS, where the highest levels are found in medulla oblongata, cervical spinal cord and hippocampus.[6][21][22] It is involved in many important CNS processes, including cell communication and the functioning of the blood brain barrier.

GFAP has been shown to play a role in mitosis by adjusting the filament network present in the cell. During mitosis, there is an increase in the amount of phosphorylated GFAP, and a movement of this modified protein to the cleavage furrow.[23] There are different sets of kinases at work; cdc2 kinase acts only at the G2 phase transition, while other GFAP kinases are active at the cleavage furrow alone. This specificity of location allows for precise regulation of GFAP distribution to the daughter cells. Studies have also shown that GFAP knockout mice undergo multiple degenerative processes including abnormal myelination, white matter structure deterioration, and functional/structural impairment of the blood–brain barrier.[24] These data suggest that GFAP is necessary for many critical roles in the CNS.

GFAP is proposed to play a role in astrocyte-neuron interactions as well as cell-cell communication. In vitro, using antisense RNA, astrocytes lacking GFAP do not form the extensions usually present with neurons.[25] Studies have also shown that Purkinje cells in GFAP knockout mice do not exhibit normal structure, and these mice demonstrate deficits in conditioning experiments such as the eye-blink task.[26] Biochemical studies of GFAP have shown MgCl2 and/or calcium/calmodulin dependent phosphorylation at various serine or threonine residues by PKC and PKA[27] which are two kinases that are important for the cytoplasmic transduction of signals. These data highlight the importance of GFAP for cell-cell communication.

GFAP has also been shown to be important in repair after CNS injury. More specifically for its role in the formation of glial scars in a multitude of locations throughout the CNS including the eye[28] and brain.[29]

Autoimmune GFAP astrocytopathy

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In 2016 a CNS inflammatory disorder associated with anti-GFAP antibodies was described. Patients with autoimmune GFAP astrocytopathy developed meningoencephalomyelitis with inflammation of the meninges, the brain parenchyma, and the spinal cord. About one third of cases were associated with various cancers and many also expressed other CNS autoantibodies.

Meningoencephalitis is the predominant clinical presentation of autoimmune GFAP astrocytopathy in published case series.[30] It also can appear associated with encephalomyelitis and parkinsonism.[31]

Disease states

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GFAP immunostaining in a glial neoplasm (anaplastic astrocytoma)
 
GFAP immunostaining of an astrocyte in cell culture in red and counterstained for vimentin in green. GFAP and vimentin colocalize in cytoplasmic intermediate filaments, so the astrocyte appears yellow. Nuclear DNA is stained blue with DAPI. Antibodies, cell preparation and image generated by EnCor Biotechnology Inc.

There are multiple disorders associated with improper GFAP regulation, and injury can cause glial cells to react in detrimental ways. Glial scarring is a consequence of several neurodegenerative conditions, as well as injury that severs neural material. The scar is formed by astrocytes interacting with fibrous tissue to re-establish the glial margins around the central injury core[32] and is partially caused by up-regulation of GFAP.[33]

Another condition directly related to GFAP is Alexander disease, a rare genetic disorder. Its symptoms include mental and physical retardation, dementia, enlargement of the brain and head, spasticity (stiffness of arms and/or legs), and seizures.[34] The cellular mechanism of the disease is the presence of cytoplasmic accumulations containing GFAP and heat shock proteins, known as Rosenthal fibers.[35] Mutations in the coding region of GFAP have been shown to contribute to the accumulation of Rosenthal fibers.[36] Some of these mutations have been proposed to be detrimental to cytoskeleton formation as well as an increase in caspase 3 activity,[37] which would lead to increased apoptosis of cells with these mutations. GFAP therefore plays an important role in the pathogenesis of Alexander disease.

Notably, the expression of some GFAP isoforms have been reported to decrease in response to acute infection or neurodegeneration.[38] Additionally, reduction in GFAP expression has also been reported in Wernicke's encephalopathy.[39] The HIV-1 viral envelope glycoprotein gp120 can directly inhibit the phosphorylation of GFAP and GFAP levels can be decreased in response to chronic infection with HIV-1,[40] varicella zoster,[41] and pseudorabies.[42] Decreases in GFAP expression have been reported in Down's syndrome, schizophrenia, bipolar disorder and depression.[38]

The generally high abundance of GFAP in the CNS has led to a great interest in GFAP as a blood biomarker of acute injury to the brain and spinal cord in different types of disease mechanisms, such as traumatic brain injury and cerebrovascular disease.[43] Elevated blood levels of GFAP are also found in neuroinflammatory diseases, such as multiple sclerosis and neuromyelitis optica, a disease targeting astrocytes.[43] In a study of 22 child patients undergoing extracorporeal membrane oxygenation (ECMO), children with abnormally high levels of GFAP were 13 times more likely to die and 11 times more likely to suffer brain injury than children with normal GFAP levels.[44]

Interactions

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Glial fibrillary acidic protein has been shown to interact with MEN1[45] and PSEN1.[46]

Isoforms

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Although GFAP alpha is the only isoform which is able to assemble homomerically, GFAP has 8 different isoforms which label distinct subpopulations of astrocytes in the human and rodent brain. These isoforms include GFAP kappa, GFAP +1 and the currently best researched GFAP delta. GFAP delta appears to be linked with neural stem cells (NSCs) and may be involved in migration. GFAP+1 is an antibody which labels two isoforms. Although GFAP+1 positive astrocytes are supposedly not reactive astrocytes, they have a wide variety of morphologies including processes of up to 0.95 mm (seen in the human brain). The expression of GFAP+1 positive astrocytes is linked with old age and the onset of AD pathology.[47]

See also

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References

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  1. ^ a b c GRCh38: Ensembl release 89: ENSG00000131095Ensembl, May 2017
  2. ^ a b c GRCm38: Ensembl release 89: ENSMUSG00000020932Ensembl, May 2017
  3. ^ "Human PubMed Reference:". National Center for Biotechnology Information, U.S. National Library of Medicine.
  4. ^ "Mouse PubMed Reference:". National Center for Biotechnology Information, U.S. National Library of Medicine.
  5. ^ Isaacs A, Baker M, Wavrant-De Vrièze F, Hutton M (July 1998). "Determination of the gene structure of human GFAP and absence of coding region mutations associated with frontotemporal dementia with parkinsonism linked to chromosome 17". Genomics. 51 (1): 152–154. doi:10.1006/geno.1998.5360. PMID 9693047.
  6. ^ a b Jacque CM, Vinner C, Kujas M, Raoul M, Racadot J, Baumann NA (January 1978). "Determination of glial fibrillary acidic protein (GFAP) in human brain tumors". Journal of the Neurological Sciences. 35 (1): 147–155. doi:10.1016/0022-510x(78)90107-7. PMID 624958. S2CID 10224197.
  7. ^ Roessmann U, Velasco ME, Sindely SD, Gambetti P (October 1980). "Glial fibrillary acidic protein (GFAP) in ependymal cells during development. An immunocytochemical study". Brain Research. 200 (1): 13–21. doi:10.1016/0006-8993(80)91090-2. PMID 6998542. S2CID 38131934.
  8. ^ Buniatian G, Traub P, Albinus M, Beckers G, Buchmann A, Gebhardt R, Osswald H (January 1998). "The immunoreactivity of glial fibrillary acidic protein in mesangial cells and podocytes of the glomeruli of rat kidney in vivo and in culture". Biology of the Cell. 90 (1): 53–61. doi:10.1016/s0248-4900(98)80232-3. PMID 9691426. S2CID 31851422.
  9. ^ Maunoury R, Portier MM, Léonard N, McCormick D (December 1991). "Glial fibrillary acidic protein immunoreactivity in adrenocortical and Leydig cells of the Syrian golden hamster (Mesocricetus auratus)". Journal of Neuroimmunology. 35 (1–3): 119–129. doi:10.1016/0165-5728(91)90167-6. PMID 1720132. S2CID 3766335.
  10. ^ Davidoff MS, Middendorff R, Köfüncü E, Müller D, Jezek D, Holstein AF (2002). "Leydig cells of the human testis possess astrocyte and oligodendrocyte marker molecules". Acta Histochemica. 104 (1): 39–49. doi:10.1078/0065-1281-00630. PMID 11993850.
  11. ^ von Koskull H (1984). "Rapid identification of glial cells in human amniotic fluid with indirect immunofluorescence". Acta Cytologica. 28 (4): 393–400. PMID 6205529.
  12. ^ Kasantikul V, Shuangshoti S (May 1989). "Positivity to glial fibrillary acidic protein in bone, cartilage, and chordoma". Journal of Surgical Oncology. 41 (1): 22–26. doi:10.1002/jso.2930410109. PMID 2654484. S2CID 34069861.
  13. ^ Apte MV, Haber PS, Applegate TL, Norton ID, McCaughan GW, Korsten MA, et al. (July 1998). "Periacinar stellate shaped cells in rat pancreas: identification, isolation, and culture". Gut. 43 (1): 128–133. doi:10.1136/gut.43.1.128. PMC 1727174. PMID 9771417.
  14. ^ Cullen DK, Simon CM, LaPlaca MC (July 2007). "Strain rate-dependent induction of reactive astrogliosis and cell death in three-dimensional neuronal-astrocytic co-cultures". Brain Research. 1158: 103–115. doi:10.1016/j.brainres.2007.04.070. PMC 3179863. PMID 17555726.
  15. ^ Eng LF, Ghirnikar RS, Lee YL (October 2000). "Glial fibrillary acidic protein: GFAP-thirty-one years (1969-2000)". Neurochemical Research. 25 (9–10): 1439–1451. doi:10.1023/A:1007677003387. PMID 11059815. S2CID 9221868.
  16. ^ Bongcam-Rudloff E, Nistér M, Betsholtz C, Wang JL, Stenman G, Huebner K, et al. (March 1991). "Human glial fibrillary acidic protein: complementary DNA cloning, chromosome localization, and messenger RNA expression in human glioma cell lines of various phenotypes". Cancer Research. 51 (5): 1553–1560. PMID 1847665.
  17. ^ a b Reeves SA, Helman LJ, Allison A, Israel MA (July 1989). "Molecular cloning and primary structure of human glial fibrillary acidic protein". Proceedings of the National Academy of Sciences of the United States of America. 86 (13): 5178–5182. Bibcode:1989PNAS...86.5178R. doi:10.1073/pnas.86.13.5178. PMC 297581. PMID 2740350.
  18. ^ McCormick MB, Coulombe PA, Fuchs E (June 1991). "Sorting out IF networks: consequences of domain swapping on IF recognition and assembly". The Journal of Cell Biology. 113 (5): 1111–1124. doi:10.1083/jcb.113.5.1111. PMC 2289006. PMID 1710225.
  19. ^ Stewart M, Quinlan RA, Moir RD (July 1989). "Molecular interactions in paracrystals of a fragment corresponding to the alpha-helical coiled-coil rod portion of glial fibrillary acidic protein: evidence for an antiparallel packing of molecules and polymorphism related to intermediate filament structure". The Journal of Cell Biology. 109 (1): 225–234. doi:10.1083/jcb.109.1.225. PMC 2115473. PMID 2745549.
  20. ^ Fuchs E, Weber K (1994). "Intermediate filaments: structure, dynamics, function, and disease". Annual Review of Biochemistry. 63: 345–382. doi:10.1146/annurev.bi.63.070194.002021. PMID 7979242.
  21. ^ Venkatesh K, Srikanth L, Vengamma B, Chandrasekhar C, Sanjeevkumar A, Mouleshwara Prasad BC, Sarma PV (2013). "In vitro differentiation of cultured human CD34+ cells into astrocytes". Neurology India. 61 (4): 383–388. doi:10.4103/0028-3886.117615. PMID 24005729.
  22. ^ Sjölin K, Kultima K, Larsson A, Freyhult E, Zjukovskaja C, Alkass K, Burman J (June 2022). "Distribution of five clinically important neuroglial proteins in the human brain". Molecular Brain. 15 (1): 52. doi:10.1186/s13041-022-00935-6. PMC 9241296. PMID 35765081.
  23. ^ Tardy M, Fages C, Le Prince G, Rolland B, Nunez J (1990). "Regulation of the Glial Fibrillary Acidic Protein (GFAP) and of its Encoding mRNA in the Developing Brain and in Cultured Astrocytes". Molecular Aspects of Development and Aging of the Nervous System. Advances in Experimental Medicine and Biology. Vol. 265. pp. 41–52. doi:10.1007/978-1-4757-5876-4_4. ISBN 978-1-4757-5878-8. PMID 2165732.
  24. ^ Liedtke W, Edelmann W, Bieri PL, Chiu FC, Cowan NJ, Kucherlapati R, Raine CS (October 1996). "GFAP is necessary for the integrity of CNS white matter architecture and long-term maintenance of myelination". Neuron. 17 (4): 607–615. doi:10.1016/S0896-6273(00)80194-4. PMID 8893019. S2CID 14714870.
  25. ^ Weinstein DE, Shelanski ML, Liem RK (March 1991). "Suppression by antisense mRNA demonstrates a requirement for the glial fibrillary acidic protein in the formation of stable astrocytic processes in response to neurons". The Journal of Cell Biology. 112 (6): 1205–1213. doi:10.1083/jcb.112.6.1205. PMC 2288905. PMID 1999469.
  26. ^ Online Mendelian Inheritance in Man (OMIM): Glial Fibrillary Acidic Protein, GFAP - 137780
  27. ^ Harrison BC, Mobley PL (January 1992). "Phosphorylation of glial fibrillary acidic protein and vimentin by cytoskeletal-associated intermediate filament protein kinase activity in astrocytes". Journal of Neurochemistry. 58 (1): 320–327. doi:10.1111/j.1471-4159.1992.tb09313.x. PMID 1727439. S2CID 28248825.
  28. ^ Tuccari G, Trombetta C, Giardinelli MM, Arena F, Barresi G (1986). "Distribution of glial fibrillary acidic protein in normal and gliotic human retina". Basic and Applied Histochemistry. 30 (4): 425–432. PMID 3548695.
  29. ^ Paetau A, Elovaara I, Paasivuo R, Virtanen I, Palo J, Haltia M (1985). "Glial filaments are a major brain fraction in infantile neuronal ceroid-lipofuscinosis". Acta Neuropathologica. 65 (3–4): 190–194. doi:10.1007/bf00686997. PMID 4038838. S2CID 1411700.
  30. ^ Allen A, Gulhar S, Haidari R, Martinez JP, Bekenstein J, DeLorenzo R, et al. (January 2020). "Autoimmune glial fibrillary acidic protein astrocytopathy resulting in treatment-refractory flaccid paralysis". Multiple Sclerosis and Related Disorders. 39: 101924. doi:10.1016/j.msard.2019.101924. PMID 31927153. S2CID 210166834.
  31. ^ Tomczak A, Su E, Tugizova M, Carlson AM, Kipp LB, Feng H, Han MH (December 2019). "A case of GFAP-astroglial autoimmunity presenting with reversible parkinsonism". Multiple Sclerosis and Related Disorders. 39: 101900. doi:10.1016/j.msard.2019.101900. PMID 31881522. S2CID 209498996.
  32. ^ Bunge MB, Bunge RP, Ris H (May 1961). "Ultrastructural study of remyelination in an experimental lesion in adult cat spinal cord". The Journal of Biophysical and Biochemical Cytology. 10 (1): 67–94. doi:10.1083/jcb.10.1.67. PMC 2225064. PMID 13688845.
  33. ^ Smith ME, Eng LF (1987). "Glial fibrillary acidic protein in chronic relapsing experimental allergic encephalomyelitis in SJL/J mice". Journal of Neuroscience Research. 18 (1): 203–208. doi:10.1002/jnr.490180129. PMID 3682026. S2CID 25610288.
  34. ^ HealthLink (2007-11-25). "Alexander Disease". Medical College of Wisconsin. Archived from the original on 2007-02-24. Retrieved 2007-03-05.
  35. ^ Hagemann TL, Connor JX, Messing A (October 2006). "Alexander disease-associated glial fibrillary acidic protein mutations in mice induce Rosenthal fiber formation and a white matter stress response". The Journal of Neuroscience. 26 (43): 11162–11173. doi:10.1523/JNEUROSCI.3260-06.2006. PMC 6674663. PMID 17065456.
  36. ^ Brenner M, Johnson AB, Boespflug-Tanguy O, Rodriguez D, Goldman JE, Messing A (January 2001). "Mutations in GFAP, encoding glial fibrillary acidic protein, are associated with Alexander disease". Nature Genetics. 27 (1): 117–120. doi:10.1038/83679. PMID 11138011. S2CID 10159452.
  37. ^ Chen YS, Lim SC, Chen MH, Quinlan RA, Perng MD (October 2011). "Alexander disease causing mutations in the C-terminal domain of GFAP are deleterious both to assembly and network formation with the potential to both activate caspase 3 and decrease cell viability". Experimental Cell Research. 317 (16): 2252–2266. doi:10.1016/j.yexcr.2011.06.017. PMC 4308095. PMID 21756903.
  38. ^ a b Johnston-Wilson NL, Sims CD, Hofmann JP, Anderson L, Shore AD, Torrey EF, Yolken RH (March 2000). "Disease-specific alterations in frontal cortex brain proteins in schizophrenia, bipolar disorder, and major depressive disorder. The Stanley Neuropathology Consortium". Molecular Psychiatry. 5 (2): 142–149. doi:10.1038/sj.mp.4000696. PMID 10822341.
  39. ^ Cullen KM, Halliday GM (1994). "Chronic alcoholics have substantial glial pathology in the forebrain and diencephalon". Alcohol and Alcoholism. 2: 253–257. PMID 8974344.
  40. ^ Levi G, Patrizio M, Bernardo A, Petrucci TC, Agresti C (February 1993). "Human immunodeficiency virus coat protein gp120 inhibits the beta-adrenergic regulation of astroglial and microglial functions". Proceedings of the National Academy of Sciences of the United States of America. 90 (4): 1541–1545. Bibcode:1993PNAS...90.1541L. doi:10.1073/pnas.90.4.1541. PMC 45910. PMID 8381971.
  41. ^ Kennedy PG, Major EO, Williams RK, Straus SE (December 1994). "Down-regulation of glial fibrillary acidic protein expression during acute lytic varicella-zoster virus infection of cultured human astrocytes". Virology. 205 (2): 558–562. doi:10.1006/viro.1994.1679. PMID 7975257. Archived from the original on 2021-04-27. Retrieved 2019-06-26.
  42. ^ Rinaman L, Card JP, Enquist LW (February 1993). "Spatiotemporal responses of astrocytes, ramified microglia, and brain macrophages to central neuronal infection with pseudorabies virus". The Journal of Neuroscience. 13 (2): 685–702. doi:10.1523/JNEUROSCI.13-02-00685.1993. PMC 6576625. PMID 8381171.
  43. ^ a b Abdelhak A, Foschi M, Abu-Rumeileh S, Yue JK, D'Anna L, Huss A, et al. (March 2022). "Blood GFAP as an emerging biomarker in brain and spinal cord disorders". Nature Reviews. Neurology. 18 (3): 158–172. doi:10.1038/s41582-021-00616-3. PMID 35115728. S2CID 246492708.
  44. ^ "Protein Found to Predict Brain Injury in Children on ECMO Life Support". Johns Hopkins Children's Center. 19 November 2010. Archived from the original on 9 March 2012. Retrieved 11 December 2010.
  45. ^ Lopez-Egido J, Cunningham J, Berg M, Oberg K, Bongcam-Rudloff E, Gobl A (August 2002). "Menin's interaction with glial fibrillary acidic protein and vimentin suggests a role for the intermediate filament network in regulating menin activity". Experimental Cell Research. 278 (2): 175–183. doi:10.1006/excr.2002.5575. PMID 12169273.
  46. ^ Nielsen AL, Holm IE, Johansen M, Bonven B, Jørgensen P, Jørgensen AL (August 2002). "A new splice variant of glial fibrillary acidic protein, GFAP epsilon, interacts with the presenilin proteins". The Journal of Biological Chemistry. 277 (33): 29983–29991. doi:10.1074/jbc.M112121200. PMID 12058025.
  47. ^ Middeldorp J, Hol EM (March 2011). "GFAP in health and disease". Progress in Neurobiology. 93 (3): 421–443. doi:10.1016/j.pneurobio.2011.01.005. PMID 21219963. S2CID 41192525.

Further reading

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