NAA10 | |||||||||||||||||||||||||||||||||||||||||||||||||||
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Identifiers | |||||||||||||||||||||||||||||||||||||||||||||||||||
Aliases | NAA10, ARD1, ARD1A, ARD1P, DXS707, MCOPS1, NATD, TE2, OGDNS, N(alpha)-acetyltransferase 10, NatA catalytic subunit, hARD1, N-alpha-acetyltransferase 10, NatA catalytic subunit | ||||||||||||||||||||||||||||||||||||||||||||||||||
External IDs | OMIM: 300013 MGI: 1915255 HomoloGene: 2608 GeneCards: NAA10 | ||||||||||||||||||||||||||||||||||||||||||||||||||
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N-alpha-acetyltransferase 10 (NAA10) also known as NatA catalytic subunit Naa10 and arrest-defective protein 1 homolog A (ARD1A) is an enzyme subunit that in humans is encoded NAA10 gene.[5][6] Together with its auxiliary subunit Naa15, Naa10 constitutes the NatA (Nα-acetyltransferase A) complex that specifically catalyzes the transfer of an acetyl group from acetyl-CoA to the N-terminal primary amino group of certain proteins. In higher eukaryotes, 5 other N-acetyltransferase (NAT) complexes, NatB-NatF, have been described that differ both in substrate specificity and subunit composition.[7]
Gene and transcripts
The human NAA10 is located on chromosome Xq28 and contains 8 exons, 2 encoding three different isoforms derived from alternate splicing.[8] Additionally, a processed NAA10 gene duplication NAA11 (ARD2) has been identified that is expressed in several human cell lines;[9] however, later studies indicate that Naa11 is not expressed in the human cell lines HeLa and HEK293 or in cancerous tissues, and NAA11 transcripts were only detected in testicular and placental tissues.[10] Naa11 has also been found in mouse, where it is mainly expressed in the testis.[11] NAA11 is located on chromosome 4q21.21 in human and 5 E3 in mouse, and only contains two exons. Mice have another Naa10-like paralog, Naa12. Naa12 has NAT activity and genetically compensates for loss of Naa10, while being Naa10/Naa12 null is embryonic lethal in mic.[12]
In mouse, NAA10 is located on chromosome X A7.3 and contains 9 exons. Two alternative splicing products of mouse Naa10, mNaa10235 and mNaa10225, were reported in NIH-3T3 and JB6 cells that may have different activities and function in different subcellular compartments.[13]
Homologues for Naa10 have been identified in almost all kingdoms of life analyzed, including plants,[14][15][16] fungi,[14][17] amoebozoa,[14] archaeabacteria[14][18][19][20] and protozoa.[21][22] In eubacteria, 3 Nα-acetyltransferases, RimI, RimJ and RimL, have been identified[23][24][25] but according to their low sequence identity with the NATs, it is likely that the RIM proteins do not have a common ancestor and evolved independently.[26][27]
Structure
Size-exclusion chromatography and circular dichroism indicated that human Naa10 consists of a compact globular region comprising two thirds of the protein and a flexible unstructured C-terminus.[28] X-ray crystal structure of the 100 kD holo-NatA (Naa10/Naa15) complex from S. pombe showed that Naa10 adopts a typical GNAT fold containing a N-terminal α1–loop–α2 segment that features one large hydrophobic interface and exhibits interactions with its auxiliary subunit Naa15, a central acetyl CoA-binding region, and C-terminal segments that are similar to the corresponding regions in Naa50, another Nα-acetyltransferase.[29] The X-ray crystal structure of archaeal T. volcanium Naa10 has also been reported, revealing multiple distinct modes of acetyl-Co binding involving the loops between β4 and α3, including the P-loop.[20] Non-complexed (Naa15 unbound) Naa10 adopts a different fold: Leu22 and Tyr26 shift out of the active site of Naa10, and Glu24 (important for substrate binding and catalysis of NatA) is repositioned by ~5 Å, resulting in a conformation that allows for the acetylation of a different subset of substrates.[29] An X-ray crystal structure of human Naa10 in complex with Naa15 and HYPK has been reported.[30]
A functional nuclear localization signal in the C-terminus of hNaa10 between residues 78 and 83 (KRSHRR) has been described.[31][32]
Function
Naa10, as part of the NatA complex, is bound to the ribosome and co-translationally acetylates proteins starting with small side chains such as Ser, Ala, Thr, Gly, Val and Cys, after the initiator methionine (iMet) has been cleaved by methionine aminopeptidases (MetAP).[33] Furthermore, post-translational acetylation by non-ribosome-associated Naa10 might occur. About 40-50 % of all proteins are potential NatA substrates.[7][34] Additionally, in a monomeric state, structural rearrangements of the substrate binding pocket Naa10 allow acetylation of N-termini with acidic side chains.[29][35] Furthermore, Nε-acetyltransferase activity[36][37][38][39][40][41][42] and N-terminal propionyltransferase activity [43] have been reported.
Despite the fact that Nα-terminal acetylation of proteins has been known for many years, the functional consequences of this modification are not well understood. However, accumulating evidence have linked Naa10 to various signaling pathways, including Wnt/β-catenin,[38][39][44][45] MAPK,[44] JAK/STAT,[46] and NF-κB,[47][48][49][50] thereby regulating various cellular processes, including cell migration,[51][52] cell cycle control,[53][54][55] DNA damage control,[49][56] caspase-dependent cell death,[56][57] p53 dependent apoptosis,[54] cell proliferation and autophagy [58] as well as hypoxia,[39][40][42][59][60] although there are some major discrepancies regarding hypoxia[61][62][63][64][65] and even isoform specific effects of Naa10 functions have been reported in mouse.[13][66]
Naa10 is essential in D. melanogaster,[67] C. elegans[68] and T. brucei.[21] In S. cerevisiae, Naa10 function is not essential but yNAA10Δ cells display severe defects including de-repression of the silent mating type locus (HML), failure to enter Go phase, temperature sensitivity, and impaired growth.[17][69] Naa10-knockout mice have very recently been reported to be viable, displaying a defect in bone development.[50]
Disease
In 2001 A c.109T>C (p.Ser37Pro) variant in NAA10 was identified in two unrelated families with Ogden Syndrome, a X-linked disorder involving a distinct combination of an aged appearance, craniofacial anomalies, hypotonia, global developmental delays, cryptorchidism, and cardiac arrhythmias.[70] Patient fibroblasts displayed altered morphology, growth and migration characteristics and molecular studies indicate that this S37P mutation disrupts the NatA complex and decreases Naa10 enzymatic activity in vitro and in vivo.[70][71][72]
Furthermore, two other mutations in Naa10 (R116W mutation in a boy and a V107F mutation in a girl) have been described in two unrelated families with sporadic cases of non-syndromic intellectual disabilities, postnatal growth failure, and skeletal anomalies.[73][74] The girl was reported as having delayed closure of the fontanels, delayed bone age, broad great toes, mild pectus carinatum, pulmonary artery stenosis, atrial septal defect, prolonged QT interval. The boy was reported as having small hands/feet, high arched palate, and wide interdental spaces.
Additionally, a splice mutation in the intron 7 splice donor site (c.471+2T→A) of NAA10 was reported in a single family with Lenz microphthalmia syndrome (LMS), a very rare, genetically heterogeneous X-linked recessive disorder characterized by microphthalmia or anophthalmia, developmental delay, intellectual disability, skeletal abnormalities and malformations of teeth, fingers and toes.[75] Patient fibroblasts displayed cell proliferation defects, dysregulation of genes involved in retinoic acid signaling pathway, such as STRA6, and deficiencies in retinol uptake.[75]
Accumulating evidence suggests Naa10 function might regulate co-translational protein folding through the modulation of chaperone function, thereby affecting pathological formation of toxic amyloid aggregates in Alzheimer's disease or prion [PSI+] propagation in yeast.[76][77][78][79]
Further information on NAA10 related syndromes can be found at www.naa10gene.com
Notes
References
- 1 2 3 GRCh38: Ensembl release 89: ENSG00000102030 - Ensembl, May 2017
- 1 2 3 GRCm38: Ensembl release 89: ENSMUSG00000031388 - 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.
- ↑ Tribioli C, Mancini M, Plassart E, Bione S, Rivella S, Sala C, Torri G, Toniolo D (January 1995). "Isolation of new genes in distal Xq28: transcriptional map and identification of a human homologue of the ARD1 N-acetyl transferase of Saccharomyces cerevisiae". Hum Mol Genet. 3 (7): 1061–7. doi:10.1093/hmg/3.7.1061. PMID 7981673.
- ↑ "Entrez Gene: ARD1A ARD1 homolog A, N-acetyltransferase (S. cerevisiae)".
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- ↑ Pruitt KD, Tatusova T, Maglott DR (January 2007). "NCBI reference sequences (RefSeq): a curated non-redundant sequence database of genomes, transcripts and proteins". Nucleic Acids Research. 35 (Database issue): D61–5. doi:10.1093/nar/gkl842. PMC 1716718. PMID 17130148.
- ↑ Arnesen T, Betts MJ, Pendino F, Liberles DA, Anderson D, Caro J, Kong X, Varhaug JE, Lillehaug JR (25 April 2006). "Characterization of hARD2, a processed hARD1 gene duplicate, encoding a human protein N-alpha-acetyltransferase". BMC Biochemistry. 7: 13. doi:10.1186/1471-2091-7-13. PMC 1475586. PMID 16638120.
- ↑ Pang AL, Clark J, Chan WY, Rennert OM (November 2011). "Expression of human NAA11 (ARD1B) gene is tissue-specific and is regulated by DNA methylation". Epigenetics. 6 (11): 1391–9. doi:10.4161/epi.6.11.18125. PMC 3242813. PMID 22048246.
- ↑ Pang AL, Peacock S, Johnson W, Bear DH, Rennert OM, Chan WY (August 2009). "Cloning, characterization, and expression analysis of the novel acetyltransferase retrogene Ard1b in the mouse". Biology of Reproduction. 81 (2): 302–9. doi:10.1095/biolreprod.108.073221. PMC 2849813. PMID 19246321.
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- ↑ Liu CC, Zhu HY, Dong XM, Ning DL, Wang HX, Li WH, Yang CP, Wang BC (2013). "Identification and analysis of the acetylated status of poplar proteins reveals analogous N-terminal protein processing mechanisms with other eukaryotes". PLOS ONE. 8 (3): e58681. Bibcode:2013PLoSO...858681L. doi:10.1371/journal.pone.0058681. PMC 3594182. PMID 23536812.
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- 1 2 Ma C, Pathak C, Jang S, Lee SJ, Nam M, Kim SJ, Im H, Lee BJ (October 2014). "Structure of Thermoplasma volcanium Ard1 belongs to N-acetyltransferase family member suggesting multiple ligand binding modes with acetyl coenzyme A and coenzyme A". Biochimica et Biophysica Acta (BBA) - Proteins and Proteomics. 1844 (10): 1790–7. doi:10.1016/j.bbapap.2014.07.011. PMID 25062911.
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- ↑ Isono K, Isono S (1980). "Ribosomal protein modification in Escherichia coli. II. Studies of a mutant lacking the N-terminal acetylation of protein S18". Molecular & General Genetics. 177 (4): 645–51. doi:10.1007/bf00272675. PMID 6991870. S2CID 34666905.
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- 1 2 Lim JH, Park JW, Chun YS (15 November 2006). "Human arrest defective 1 acetylates and activates beta-catenin, promoting lung cancer cell proliferation". Cancer Research. 66 (22): 10677–82. doi:10.1158/0008-5472.can-06-3171. PMID 17108104.
- 1 2 3 Lim JH, Chun YS, Park JW (1 July 2008). "Hypoxia-inducible factor-1alpha obstructs a Wnt signaling pathway by inhibiting the hARD1-mediated activation of beta-catenin". Cancer Research. 68 (13): 5177–84. doi:10.1158/0008-5472.can-07-6234. PMID 18593917.
- 1 2 Jeong JW, Bae MK, Ahn MY, Kim SH, Sohn TK, Bae MH, Yoo MA, Song EJ, Lee KJ, Kim KW (27 November 2002). "Regulation and destabilization of HIF-1alpha by ARD1-mediated acetylation". Cell. 111 (5): 709–20. doi:10.1016/S0092-8674(02)01085-1. PMID 12464182. S2CID 18652640.
- ↑ Lee MN, Lee SN, Kim SH, Kim B, Jung BK, Seo JH, Park JH, Choi JH, Yim SH, Lee MR, Park JG, Yoo JY, Kim JH, Lee ST, Kim HM, Ryeom S, Kim KW, Oh GT (17 March 2010). "Roles of arrest-defective protein 1(225) and hypoxia-inducible factor 1alpha in tumor growth and metastasis". Journal of the National Cancer Institute. 102 (6): 426–42. doi:10.1093/jnci/djq026. PMC 2841038. PMID 20194889.
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- ↑ Foyn H, Van Damme P, Støve SI, Glomnes N, Evjenth R, Gevaert K, Arnesen T (January 2013). "Protein N-terminal acetyltransferases act as N-terminal propionyltransferases in vitro and in vivo". Molecular & Cellular Proteomics. 12 (1): 42–54. doi:10.1074/mcp.m112.019299. PMC 3536908. PMID 23043182.
- 1 2 Seo JH, Cha JH, Park JH, Jeong CH, Park ZY, Lee HS, Oh SH, Kang JH, Suh SW, Kim KH, Ha JY, Han SH, Kim SH, Lee JW, Park JA, Jeong JW, Lee KJ, Oh GT, Lee MN, Kwon SW, Lee SK, Chun KH, Lee SJ, Kim KW (1 June 2010). "Arrest defective 1 autoacetylation is a critical step in its ability to stimulate cancer cell proliferation". Cancer Research. 70 (11): 4422–32. doi:10.1158/0008-5472.can-09-3258. PMID 20501853.
- ↑ Lee CF, Ou DS, Lee SB, Chang LH, Lin RK, Li YS, Upadhyay AK, Cheng X, Wang YC, Hsu HS, Hsiao M, Wu CW, Juan LJ (August 2010). "hNaa10p contributes to tumorigenesis by facilitating DNMT1-mediated tumor suppressor gene silencing". The Journal of Clinical Investigation. 120 (8): 2920–30. doi:10.1172/jci42275. PMC 2912195. PMID 20592467.
- ↑ Zeng Y, Min L, Han Y, Meng L, Liu C, Xie Y, Dong B, Wang L, Jiang B, Xu H, Zhuang Q, Zhao C, Qu L, Shou C (October 2014). "Inhibition of STAT5a by Naa10p contributes to decreased breast cancer metastasis". Carcinogenesis. 35 (10): 2244–53. doi:10.1093/carcin/bgu132. PMID 24925029.
- ↑ Kuo HP, Lee DF, Xia W, Lai CC, Li LY, Hung MC (6 November 2009). "Phosphorylation of ARD1 by IKKbeta contributes to its destabilization and degradation". Biochemical and Biophysical Research Communications. 389 (1): 156–61. doi:10.1016/j.bbrc.2009.08.127. PMC 2753275. PMID 19716809.
- ↑ Park J, Kanayama A, Yamamoto K, Miyamoto Y (1 June 2012). "ARD1 binding to RIP1 mediates doxorubicin-induced NF-κB activation". Biochemical and Biophysical Research Communications. 422 (2): 291–7. doi:10.1016/j.bbrc.2012.04.150. PMID 22580278.
- 1 2 Xu H, Jiang B, Meng L, Ren T, Zeng Y, Wu J, Qu L, Shou C (June 2012). "N-α-acetyltransferase 10 protein inhibits apoptosis through RelA/p65-regulated MCL1 expression". Carcinogenesis. 33 (6): 1193–202. doi:10.1093/carcin/bgs144. PMID 22496479.
- 1 2 Yoon H, Kim HL, Chun YS, Shin DH, Lee KH, Shin CS, Lee DY, Kim HH, Lee ZH, Ryoo HM, Lee MN, Oh GT, Park JW (7 November 2014). "NAA10 controls osteoblast differentiation and bone formation as a feedback regulator of Runx2". Nature Communications. 5: 5176. Bibcode:2014NatCo...5.5176Y. doi:10.1038/ncomms6176. PMID 25376646.
- ↑ Hua KT, Tan CT, Johansson G, Lee JM, Yang PW, Lu HY, Chen CK, Su JL, Chen PB, Wu YL, Chi CC, Kao HJ, Shih HJ, Chen MW, Chien MH, Chen PS, Lee WJ, Cheng TY, Rosenberger G, Chai CY, Yang CJ, Huang MS, Lai TC, Chou TY, Hsiao M, Kuo ML (15 February 2011). "N-α-acetyltransferase 10 protein suppresses cancer cell metastasis by binding PIX proteins and inhibiting Cdc42/Rac1 activity". Cancer Cell. 19 (2): 218–31. doi:10.1016/j.ccr.2010.11.010. PMID 21295525.
- ↑ Shin DH, Chun YS, Lee KH, Shin HW, Park JW (14 October 2009). "Arrest defective-1 controls tumor cell behavior by acetylating myosin light chain kinase". PLOS ONE. 4 (10): e7451. Bibcode:2009PLoSO...4.7451S. doi:10.1371/journal.pone.0007451. PMC 2758594. PMID 19826488.
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- ↑ Yi CH, Pan H, Seebacher J, Jang IH, Hyberts SG, Heffron GJ, Vander Heiden MG, Yang R, Li F, Locasale JW, Sharfi H, Zhai B, Rodriguez-Mias R, Luithardt H, Cantley LC, Daley GQ, Asara JM, Gygi SP, Wagner G, Liu CF, Yuan J (19 August 2011). "Metabolic regulation of protein N-alpha-acetylation by Bcl-xL promotes cell survival". Cell. 146 (4): 607–20. doi:10.1016/j.cell.2011.06.050. PMC 3182480. PMID 21854985.
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Further reading
- Brenner V, Nyakatura G, Rosenthal A, Platzer M (1997). "Genomic organization of two novel genes on human Xq28: compact head to head arrangement of IDH gamma and TRAP delta is conserved in rat and mouse". Genomics. 44 (1): 8–14. doi:10.1006/geno.1997.4822. PMID 9286695. S2CID 16453737.
- Hartley JL, Temple GF, Brasch MA (2001). "DNA cloning using in vitro site-specific recombination". Genome Res. 10 (11): 1788–95. doi:10.1101/gr.143000. PMC 310948. PMID 11076863.
- Simpson JC, Wellenreuther R, Poustka A, Pepperkok R, Wiemann S (2001). "Systematic subcellular localization of novel proteins identified by large-scale cDNA sequencing". EMBO Rep. 1 (3): 287–92. doi:10.1093/embo-reports/kvd058. PMC 1083732. PMID 11256614.
- Sugiura N, Adams SM, Corriveau RA (2003). "An evolutionarily conserved N-terminal acetyltransferase complex associated with neuronal development". J. Biol. Chem. 278 (41): 40113–20. doi:10.1074/jbc.M301218200. PMID 12888564.
- Wiemann S, Arlt D, Huber W, Wellenreuther R, Schleeger S, Mehrle A, Bechtel S, Sauermann M, Korf U, Pepperkok R, Sültmann H, Poustka A (2004). "From ORFeome to biology: a functional genomics pipeline". Genome Res. 14 (10B): 2136–44. doi:10.1101/gr.2576704. PMC 528930. PMID 15489336.
- Arnesen T, Gromyko D, Horvli O, Fluge Ø, Lillehaug J, Varhaug JE (2006). "Expression of N-acetyl transferase human and human Arrest defective 1 proteins in thyroid neoplasms". Thyroid. 15 (10): 1131–6. doi:10.1089/thy.2005.15.1131. PMID 16279846.
- Mehrle A, Rosenfelder H, Schupp I, del Val C, Arlt D, Hahne F, Bechtel S, Simpson J, Hofmann O, Hide W, Glatting KH, Huber W, Pepperkok R, Poustka A, Wiemann S (2006). "The LIFEdb database in 2006". Nucleic Acids Res. 34 (Database issue): D415–8. doi:10.1093/nar/gkj139. PMC 1347501. PMID 16381901.
- Arnesen T, Gromyko D, Pendino F, Ryningen A, Varhaug JE, Lillehaug JR (2006). "Induction of apoptosis in human cells by RNAi-mediated knockdown of hARD1 and NATH, components of the protein N-alpha-acetyltransferase complex". Oncogene. 25 (31): 4350–60. doi:10.1038/sj.onc.1209469. PMID 16518407. S2CID 33925881.
- Beausoleil SA, Villén J, Gerber SA, Rush J, Gygi SP (2006). "A probability-based approach for high-throughput protein phosphorylation analysis and site localization". Nat. Biotechnol. 24 (10): 1285–92. doi:10.1038/nbt1240. PMID 16964243. S2CID 14294292.