Jump to content

Actin, cytoplasmic 2

From Wikipedia, the free encyclopedia
(Redirected from DFNA26)
ACTG1
Available structures
PDBOrtholog search: PDBe RCSB
Identifiers
AliasesACTG1, ACT, ACTG, BRWS2, DFNA20, DFNA26, HEL-176, actin gamma 1
External IDsOMIM: 102560; MGI: 87906; HomoloGene: 74402; GeneCards: ACTG1; OMA:ACTG1 - orthologs
Orthologs
SpeciesHumanMouse
Entrez
Ensembl
UniProt
RefSeq (mRNA)

NM_001199954
NM_001614

NM_009609
NM_001313923

RefSeq (protein)

NP_001186883
NP_001605

NP_001300852
NP_033739

Location (UCSC)Chr 17: 81.51 – 81.52 MbChr 11: 120.24 – 120.24 Mb
PubMed search[3][4]
Wikidata
View/Edit HumanView/Edit Mouse

Actin, cytoplasmic 2, or gamma-actin is a protein that in humans is encoded by the ACTG1 gene.[5] Gamma-actin is widely expressed in cellular cytoskeletons of many tissues; in adult striated muscle cells, gamma-actin is localized to Z-discs and costamere structures, which are responsible for force transduction and transmission in muscle cells. Mutations in ACTG1 have been associated with nonsyndromic hearing loss and Baraitser-Winter syndrome, as well as susceptibility of adolescent patients to vincristine toxicity.

Structure

[edit]

Human gamma-actin is 41.8 kDa in molecular weight and 375 amino acids in length.[6] Actins are highly conserved proteins that are involved in various types of cell motility, and maintenance of the cytoskeleton. In vertebrates, three main groups of actin paralogs, alpha, beta, and gamma, have been identified.[7]

The alpha actins are found in muscle tissues and are a major constituent of the sarcomere contractile apparatus. The beta and gamma actins co-exist in most cell types as components of the cytoskeleton, and as mediators of internal cell motility. Actin, gamma 1, encoded by this gene, is found in non-muscle cells in the cytoplasm, and in muscle cells at costamere structures, or transverse points of cell-cell adhesion that run perpendicular to the long axis of myocytes.[8][9][10]

Function

[edit]

In myocytes, sarcomeres adhere to the sarcolemma via costameres, which align at Z-discs and M-lines.[11] The two primary cytoskeletal components of costameres are desmin intermediate filaments and gamma-actin microfilaments.[12] It has been shown that gamma-actin interacting with another costameric protein dystrophin is critical for costameres forming mechanically strong links between the cytoskeleton and the sarcolemmal membrane.[13][14] Additional studies have shown that gamma-actin colocalizes with alpha-actinin and GFP-labeled gamma actin localized to Z-discs, whereas GFP-alpha-actin localized to pointed ends of thin filaments, indicating that gamma actin specifically localizes to Z-discs in striated muscle cells.[15][16][17]

During development of myocytes, gamma actin is thought to play a role in the organization and assembly of developing sarcomeres, evidenced in part by its early colocalization with alpha-actinin.[18] Gamma-actin is eventually replaced by sarcomeric alpha-actin isoforms,[19][20][21] with low levels of gamma-actin persisting in adult myocytes which associate with Z-disc and costamere domains.[15][22][23]

Insights into the function of gamma-actin in muscle have come from studies employing transgenesis. In a skeletal muscle-specific knockout of gamma-actin in mice, these animals showed no detectable abnormalities in development; however, knockout mice showed muscle weakness and fiber necrosis, along with decreased isometric twitch force, disrupted intrafibrillar and interfibrillar connections among myocytes, and myopathy.[24]

Clinical significance

[edit]

An autosomal dominant mutation in ACTG1 in the DFNA20/26 locus at 17q25-qter was identified in patients with hearing loss. A Thr278Ile mutation was identified in helix 9 of gamma-actin protein, which is predicted to alter protein structure. This study identified the first disease causing mutation in gamma-actin and underlies the importance of gamma-actin as structural elements of the inner ear hair cells.[25] Since then, other ACTG1 mutations have been linked to nonsyndromic hearing loss, including Met305Thr.[26]

A missense mutation in ACTG1 at Ser155Phe has also been identified in patients with Baraitser-Winter syndrome, which is a developmental disorder characterized by congenital ptosis, excessively-arched eyebrows, hypertelorism, ocular colobomata, lissencephaly, short stature, seizures and hearing loss.[27][28]

Differential expression of ACTG1 mRNA was also identified in patients with Sporadic Amyotrophic Lateral Sclerosis, a devastating disease with unknown causality, using a sophisticated bioinformatics approach employing Affymetrix long-oligonucleotide BaFL methods.[29]

Single nucleotide polymorphisms in ACTG1 have been associated with vincristine toxicity, which is part of the standard treatment regimen for childhood acute lymphoblastic leukemia. Neurotoxicity was more frequent in patients that were ACTG1 Gly310Ala mutation carriers, suggesting that this may play a role in patient outcomes from vincristine treatment.[30]

Interactions

[edit]

ACTG1 has been shown to interact with:

See also

[edit]

References

[edit]
  1. ^ a b c GRCh38: Ensembl release 89: ENSG00000184009Ensembl, May 2017
  2. ^ a b c GRCm38: Ensembl release 89: ENSMUSG00000062825Ensembl, 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. ^ "Entrez Gene: ACTG1 actin, gamma 1".
  6. ^ "Protein sequence for human ACTG1 (Uniprot ID: P63261)". Cardiac Organellar Protein Atlas Knowledgebase (COPaKB). Archived from the original on 21 July 2015. Retrieved 18 July 2015.
  7. ^ Rubenstein PA (Jul 1990). "The functional importance of multiple actin isoforms". BioEssays. 12 (7): 309–15. doi:10.1002/bies.950120702. PMID 2203335. S2CID 2163289.
  8. ^ Craig SW, Pardo JV (1983). "Gamma actin, spectrin, and intermediate filament proteins colocalize with vinculin at costameres, myofibril-to-sarcolemma attachment sites". Cell Motility. 3 (5–6): 449–62. doi:10.1002/cm.970030513. PMID 6420066.
  9. ^ Pardo JV, Siliciano JD, Craig SW (Feb 1983). "A vinculin-containing cortical lattice in skeletal muscle: transverse lattice elements ("costameres") mark sites of attachment between myofibrils and sarcolemma". Proceedings of the National Academy of Sciences of the United States of America. 80 (4): 1008–12. Bibcode:1983PNAS...80.1008P. doi:10.1073/pnas.80.4.1008. PMC 393517. PMID 6405378.
  10. ^ Danowski BA, Imanaka-Yoshida K, Sanger JM, Sanger JW (Sep 1992). "Costameres are sites of force transmission to the substratum in adult rat cardiomyocytes". The Journal of Cell Biology. 118 (6): 1411–20. doi:10.1083/jcb.118.6.1411. PMC 2289604. PMID 1522115.
  11. ^ Clark KA, McElhinny AS, Beckerle MC, Gregorio CC (2002). "Striated muscle cytoarchitecture: an intricate web of form and function". Annual Review of Cell and Developmental Biology. 18: 637–706. doi:10.1146/annurev.cellbio.18.012502.105840. PMID 12142273.
  12. ^ Kee AJ, Gunning PW, Hardeman EC (2009). "Diverse roles of the actin cytoskeleton in striated muscle". Journal of Muscle Research and Cell Motility. 30 (5–6): 187–97. doi:10.1007/s10974-009-9193-x. PMID 19997772. S2CID 6632615.
  13. ^ a b Rybakova IN, Patel JR, Ervasti JM (Sep 2000). "The dystrophin complex forms a mechanically strong link between the sarcolemma and costameric actin". The Journal of Cell Biology. 150 (5): 1209–14. doi:10.1083/jcb.150.5.1209. PMC 2175263. PMID 10974007.
  14. ^ Ervasti JM (Apr 2003). "Costameres: the Achilles' heel of Herculean muscle". The Journal of Biological Chemistry. 278 (16): 13591–4. doi:10.1074/jbc.R200021200. PMID 12556452.
  15. ^ a b Nakata T, Nishina Y, Yorifuji H (Aug 2001). "Cytoplasmic gamma actin as a Z-disc protein". Biochemical and Biophysical Research Communications. 286 (1): 156–63. doi:10.1006/bbrc.2001.5353. PMID 11485322.
  16. ^ Papponen H, Kaisto T, Leinonen S, Kaakinen M, Metsikkö K (Jan 2009). "Evidence for gamma-actin as a Z disc component in skeletal myofibers". Experimental Cell Research. 315 (2): 218–25. doi:10.1016/j.yexcr.2008.10.021. PMID 19013151.
  17. ^ Vlahovich N, Kee AJ, Van der Poel C, Kettle E, Hernandez-Deviez D, Lucas C, Lynch GS, Parton RG, Gunning PW, Hardeman EC (Jan 2009). "Cytoskeletal tropomyosin Tm5NM1 is required for normal excitation-contraction coupling in skeletal muscle". Molecular Biology of the Cell. 20 (1): 400–9. doi:10.1091/mbc.E08-06-0616. PMC 2613127. PMID 19005216.
  18. ^ Lloyd CM, Berendse M, Lloyd DG, Schevzov G, Grounds MD (Jul 2004). "A novel role for non-muscle gamma-actin in skeletal muscle sarcomere assembly". Experimental Cell Research. 297 (1): 82–96. doi:10.1016/j.yexcr.2004.02.012. PMID 15194427.
  19. ^ Schwartz RJ, Rothblum KN (Jul 1981). "Gene switching in myogenesis: differential expression of the chicken actin multigene family". Biochemistry. 20 (14): 4122–9. doi:10.1021/bi00517a027. PMID 7284314.
  20. ^ Shani M, Zevin-Sonkin D, Saxel O, Carmon Y, Katcoff D, Nudel U, Yaffe D (Sep 1981). "The correlation between the synthesis of skeletal muscle actin, myosin heavy chain, and myosin light chain and the accumulation of corresponding mRNA sequences during myogenesis". Developmental Biology. 86 (2): 483–92. doi:10.1016/0012-1606(81)90206-2. PMID 7286410.
  21. ^ von Arx P, Bantle S, Soldati T, Perriard JC (Dec 1995). "Dominant negative effect of cytoplasmic actin isoproteins on cardiomyocyte cytoarchitecture and function". The Journal of Cell Biology. 131 (6 Pt 2): 1759–73. doi:10.1083/jcb.131.6.1759. PMC 2120671. PMID 8557743.
  22. ^ Hanft LM, Bogan DJ, Mayer U, Kaufman SJ, Kornegay JN, Ervasti JM (Jul 2007). "Cytoplasmic gamma-actin expression in diverse animal models of muscular dystrophy". Neuromuscular Disorders. 17 (7): 569–74. doi:10.1016/j.nmd.2007.03.004. PMC 1993539. PMID 17475492.
  23. ^ Kee AJ, Schevzov G, Nair-Shalliker V, Robinson CS, Vrhovski B, Ghoddusi M, Qiu MR, Lin JJ, Weinberger R, Gunning PW, Hardeman EC (Aug 2004). "Sorting of a nonmuscle tropomyosin to a novel cytoskeletal compartment in skeletal muscle results in muscular dystrophy". The Journal of Cell Biology. 166 (5): 685–96. doi:10.1083/jcb.200406181. PMC 2172434. PMID 15337777.
  24. ^ Sonnemann KJ, Fitzsimons DP, Patel JR, Liu Y, Schneider MF, Moss RL, Ervasti JM (Sep 2006). "Cytoplasmic gamma-actin is not required for skeletal muscle development but its absence leads to a progressive myopathy". Developmental Cell. 11 (3): 387–97. doi:10.1016/j.devcel.2006.07.001. PMID 16950128.
  25. ^ van Wijk E, Krieger E, Kemperman MH, De Leenheer EM, Huygen PL, Cremers CW, Cremers FP, Kremer H (Dec 2003). "A mutation in the gamma actin 1 (ACTG1) gene causes autosomal dominant hearing loss (DFNA20/26)". Journal of Medical Genetics. 40 (12): 879–84. doi:10.1136/jmg.40.12.879. PMC 1735337. PMID 14684684.
  26. ^ Park G, Gim J, Kim AR, Han KH, Kim HS, Oh SH, Park T, Park WY, Choi BY (18 March 2013). "Multiphasic analysis of whole exome sequencing data identifies a novel mutation of ACTG1 in a nonsyndromic hearing loss family". BMC Genomics. 14: 191. doi:10.1186/1471-2164-14-191. PMC 3608096. PMID 23506231.
  27. ^ Rivière JB, van Bon BW, Hoischen A, Kholmanskikh SS, O'Roak BJ, Gilissen C, Gijsen S, Sullivan CT, Christian SL, Abdul-Rahman OA, Atkin JF, Chassaing N, Drouin-Garraud V, Fry AE, Fryns JP, Gripp KW, Kempers M, Kleefstra T, Mancini GM, Nowaczyk MJ, van Ravenswaaij-Arts CM, Roscioli T, Marble M, Rosenfeld JA, Siu VM, de Vries BB, Shendure J, Verloes A, Veltman JA, Brunner HG, Ross ME, Pilz DT, Dobyns WB (Apr 2012). "De novo mutations in the actin genes ACTB and ACTG1 cause Baraitser-Winter syndrome". Nature Genetics. 44 (4): 440–4, S1–2. doi:10.1038/ng.1091. PMC 3677859. PMID 22366783.
  28. ^ Di Donato N, Rump A, Koenig R, Der Kaloustian VM, Halal F, Sonntag K, Krause C, Hackmann K, Hahn G, Schrock E, Verloes A (Feb 2014). "Severe forms of Baraitser-Winter syndrome are caused by ACTB mutations rather than ACTG1 mutations". European Journal of Human Genetics. 22 (2): 179–83. doi:10.1038/ejhg.2013.130. PMC 3895648. PMID 23756437.
  29. ^ Baciu C, Thompson KJ, Mougeot JL, Brooks BR, Weller JW (24 September 2012). "The LO-BaFL method and ALS microarray expression analysis". BMC Bioinformatics. 13: 244. doi:10.1186/1471-2105-13-244. PMC 3526454. PMID 23006766.
  30. ^ Ceppi F, Langlois-Pelletier C, Gagné V, Rousseau J, Ciolino C, De Lorenzo S, Kevin KM, Cijov D, Sallan SE, Silverman LB, Neuberg D, Kutok JL, Sinnett D, Laverdière C, Krajinovic M (Jun 2014). "Polymorphisms of the vincristine pathway and response to treatment in children with childhood acute lymphoblastic leukemia". Pharmacogenomics. 15 (8): 1105–16. doi:10.2217/pgs.14.68. PMC 4443746. PMID 25084203.
  31. ^ Hubberstey A, Yu G, Loewith R, Lakusta C, Young D (Jun 1996). "Mammalian CAP interacts with CAP, CAP2, and actin". Journal of Cellular Biochemistry. 61 (3): 459–66. doi:10.1002/(SICI)1097-4644(19960601)61:3<459::AID-JCB13>3.0.CO;2-E. PMID 8761950. S2CID 46076387.
  32. ^ Hertzog M, van Heijenoort C, Didry D, Gaudier M, Coutant J, Gigant B, Didelot G, Préat T, Knossow M, Guittet E, Carlier MF (May 2004). "The beta-thymosin/WH2 domain; structural basis for the switch from inhibition to promotion of actin assembly". Cell. 117 (5): 611–23. doi:10.1016/S0092-8674(04)00403-9. PMID 15163409. S2CID 8628287.
  33. ^ Van Troys M, Dewitte D, Goethals M, Carlier MF, Vandekerckhove J, Ampe C (Jan 1996). "The actin binding site of thymosin beta 4 mapped by mutational analysis". The EMBO Journal. 15 (2): 201–10. doi:10.1002/j.1460-2075.1996.tb00350.x. PMC 449934. PMID 8617195.
  34. ^ Hijikata T, Nakamura A, Isokawa K, Imamura M, Yuasa K, Ishikawa R, Kohama K, Takeda S, Yorifuji H (Jun 2008). "Plectin 1 links intermediate filaments to costameric sarcolemma through beta-synemin, alpha-dystrobrevin and actin". Journal of Cell Science. 121 (Pt 12): 2062–74. doi:10.1242/jcs.021634. PMID 18505798. S2CID 207164281.
[edit]

Further reading

[edit]