H2A1_HUMAN - dbPTM
H2A1_HUMAN - PTM Information in dbPTM
Basic Information of Protein
UniProt ID H2A1_HUMAN
UniProt AC P0C0S8
Protein Name Histone H2A type 1
Gene Name HIST1H2AG
Organism Homo sapiens (Human).
Sequence Length 130
Subcellular Localization Nucleus. Chromosome.
Protein Description Core component of nucleosome. Nucleosomes wrap and compact DNA into chromatin, limiting DNA accessibility to the cellular machineries which require DNA as a template. Histones thereby play a central role in transcription regulation, DNA repair, DNA replication and chromosomal stability. DNA accessibility is regulated via a complex set of post-translational modifications of histones, also called histone code, and nucleosome remodeling..
Protein Sequence MSGRGKQGGKARAKAKTRSSRAGLQFPVGRVHRLLRKGNYAERVGAGAPVYLAAVLEYLTAEILELAGNAARDNKKTRIIPRHLQLAIRNDEELNKLLGKVTIAQGGVLPNIQAVLLPKKTESHHKAKGK
Overview of Protein Modification Sites with Functional and Structural Information
Experimental Post-Translational Modification Sites

* ASA = Accessible Surface Area

Locations Modification Substrate Peptides
&
Secondary Structure		 ASA (%) Reference Orthologous
Protein Cluster
2Phosphorylation------MSGRGKQGG
------CCCCCCCCC		36.8816319397
2Acetylation------MSGRGKQGG
------CCCCCCCCC		36.8815823041
4Citrullination----MSGRGKQGGKA
----CCCCCCCCCHH		41.66-
4Methylation----MSGRGKQGGKA
----CCCCCCCCCHH		41.66-
4Citrullination----MSGRGKQGGKA
----CCCCCCCCCHH		41.6615823041
6Acetylation--MSGRGKQGGKARA
--CCCCCCCCCHHCH		44.39-
6Other--MSGRGKQGGKARA
--CCCCCCCCCHHCH		44.3924681537
10LactoylationGRGKQGGKARAKAKT
CCCCCCCHHCHHHHH		41.34-
10OtherGRGKQGGKARAKAKT
CCCCCCCHHCHHHHH		41.3427105115
10SuccinylationGRGKQGGKARAKAKT
CCCCCCCHHCHHHHH		41.3422389435
10AcetylationGRGKQGGKARAKAKT
CCCCCCCHHCHHHHH		41.3422389435
14AcetylationQGGKARAKAKTRSSR
CCCHHCHHHHHHHHC		44.88-
14UbiquitinationQGGKARAKAKTRSSR
CCCHHCHHHHHHHHC		44.8822980979
14OtherQGGKARAKAKTRSSR
CCCHHCHHHHHHHHC		44.8827105115
16AcetylationGKARAKAKTRSSRAG
CHHCHHHHHHHHCCC		43.71-
16UbiquitinationGKARAKAKTRSSRAG
CHHCHHHHHHHHCCC		43.7122980979
17PhosphorylationKARAKAKTRSSRAGL
HHCHHHHHHHHCCCC		40.4123882029
19PhosphorylationRAKAKTRSSRAGLQF
CHHHHHHHHCCCCCC		29.4323312004
20PhosphorylationAKAKTRSSRAGLQFP
HHHHHHHHCCCCCCC		23.9027966365
21MethylationKAKTRSSRAGLQFPV
HHHHHHHCCCCCCCH		33.64-
30MethylationGLQFPVGRVHRLLRK
CCCCCHHHHHHHHHC		22.69-
37OtherRVHRLLRKGNYAERV
HHHHHHHCCCHHHHC		52.0227105115
37CrotonylationRVHRLLRKGNYAERV
HHHHHHHCCCHHHHC		52.0221925322
37N6-crotonyl-L-lysineRVHRLLRKGNYAERV
HHHHHHHCCCHHHHC		52.02-
37UbiquitinationRVHRLLRKGNYAERV
HHHHHHHCCCHHHHC		52.02-
40PhosphorylationRLLRKGNYAERVGAG
HHHHCCCHHHHCCCC		20.6428152594
58PhosphorylationYLAAVLEYLTAEILE
HHHHHHHHHHHHHHH		12.75-
75MethylationGNAARDNKKTRIIPR
CHHHHCCCCCCEEHH		60.87-
75OtherGNAARDNKKTRIIPR
CHHHHCCCCCCEEHH		60.8724681537
76OtherNAARDNKKTRIIPRH
HHHHCCCCCCEEHHH		49.6524681537
76MethylationNAARDNKKTRIIPRH
HHHHCCCCCCEEHHH		49.65-
77PhosphorylationAARDNKKTRIIPRHL
HHHCCCCCCEEHHHH		28.8023882029
78MethylationARDNKKTRIIPRHLQ
HHCCCCCCEEHHHHH		33.45-
82MethylationKKTRIIPRHLQLAIR
CCCCEEHHHHHHHHC		32.51-
89MethylationRHLQLAIRNDEELNK
HHHHHHHCCHHHHHH		38.65-
96MalonylationRNDEELNKLLGKVTI
CCHHHHHHHHCCEEE		58.6826320211
96OtherRNDEELNKLLGKVTI
CCHHHHHHHHCCEEE		58.6827105115
96GlutarylationRNDEELNKLLGKVTI
CCHHHHHHHHCCEEE		58.6831542297
96AcetylationRNDEELNKLLGKVTI
CCHHHHHHHHCCEEE		58.6821466224
96UbiquitinationRNDEELNKLLGKVTI
CCHHHHHHHHCCEEE		58.6821890473
96SuccinylationRNDEELNKLLGKVTI
CCHHHHHHHHCCEEE		58.6822389435
100MethylationELNKLLGKVTIAQGG
HHHHHHCCEEECCCC		35.8512937907
100UbiquitinationELNKLLGKVTIAQGG
HHHHHHCCEEECCCC		35.8521906983
100GlutarylationELNKLLGKVTIAQGG
HHHHHHCCEEECCCC		35.8531542297
102O-linked_GlycosylationNKLLGKVTIAQGGVL
HHHHCCEEECCCCCC		17.6823301498
102PhosphorylationNKLLGKVTIAQGGVL
HHHHCCEEECCCCCC		17.6824732914
105MethylationLGKVTIAQGGVLPNI
HCCEEECCCCCCCCE		45.3724352239
119SumoylationIQAVLLPKKTESHHK
EEEEECCCCCHHHHH		72.76-
119AcetylationIQAVLLPKKTESHHK
EEEEECCCCCHHHHH		72.76164037
119GlutarylationIQAVLLPKKTESHHK
EEEEECCCCCHHHHH		72.7631542297
119N6-crotonyl-L-lysineIQAVLLPKKTESHHK
EEEEECCCCCHHHHH		72.76-
119UbiquitinationIQAVLLPKKTESHHK
EEEEECCCCCHHHHH		72.76-
119CrotonylationIQAVLLPKKTESHHK
EEEEECCCCCHHHHH		72.7621925322
119OtherIQAVLLPKKTESHHK
EEEEECCCCCHHHHH		72.7627105115
120UbiquitinationQAVLLPKKTESHHKA
EEEECCCCCHHHHHC		56.4325470042
120N6-crotonyl-L-lysineQAVLLPKKTESHHKA
EEEECCCCCHHHHHC		56.43-
120AcetylationQAVLLPKKTESHHKA
EEEECCCCCHHHHHC		56.43-
120GlutarylationQAVLLPKKTESHHKA
EEEECCCCCHHHHHC		56.4331542297
120CrotonylationQAVLLPKKTESHHKA
EEEECCCCCHHHHHC		56.4321925322
120SumoylationQAVLLPKKTESHHKA
EEEECCCCCHHHHHC		56.43-
121PhosphorylationAVLLPKKTESHHKAK
EEECCCCCHHHHHCC		49.1722071147
123PhosphorylationLLPKKTESHHKAKGK
ECCCCCHHHHHCCCC		35.8025159151
126CrotonylationKKTESHHKAKGK---
CCCHHHHHCCCC---		46.5021925322
126N6-crotonyl-L-lysineKKTESHHKAKGK---
CCCHHHHHCCCC---		46.50-
126UbiquitinationKKTESHHKAKGK---
CCCHHHHHCCCC---		46.50-
126GlutarylationKKTESHHKAKGK---
CCCHHHHHCCCC---		46.5031542297
Upstream regulatory proteins (kinases for phosphorylation sites, E3 ubiquitin ligases of ubiquitination sites, ...)
Modified Location Modified Residue Modification Type of Upstream Proteins Gene Name of Upstream Proteins UniProt AC of Upstream Proteins Sources
1SPhosphorylationKinaseRPS6KA5O75582
GPS
1SPhosphorylationKinaseTRPM6Q9BX84
GPS
2SPhosphorylationKinaseKS6A5O75582
PhosphoELM
120TPhosphorylationKinaseBUB1O43683
PSP
120TPhosphorylationKinaseVRK1Q99986
PSP
121TPhosphorylationKinaseDCAF1Q9Y4B6
Uniprot
-KUbiquitinationE3 ubiquitin ligaseBRCA1P38398
PMID:12431996
-KUbiquitinationE3 ubiquitin ligasePCGF1Q9BSM1
PMID:22199232
-KUbiquitinationE3 ubiquitin ligaseRNF2Q99496
PMID:16702407
-KUbiquitinationE3 ubiquitin ligaseRNF168Q8IYW5
PMID:22199232
-KUbiquitinationE3 ubiquitin ligaseRNF8O76064
PMID:18001824
-KUbiquitinationE3 ubiquitin ligaseUBR2Q8IWV8
PMID:20080676
-KUbiquitinationE3 ubiquitin ligaseBMI1P35226
PMID:17620408
-KUbiquitinationE3 ubiquitin ligaseRING1Q06587
PMID:16359901
-KUbiquitinationE3 ubiquitin ligaseDDB2Q92466
PMID:18593899
-KUbiquitinationE3 ubiquitin ligaseBMI1#RNF2P35226#Q99496
PMID:22199232
Functions of PTM Sites
Modified Location Modified Residue Modification Function Reference
2SAcetylation

11709551
2SPhosphorylation

11709551
2SPhosphorylation

11709551
2SPhosphorylation

11709551
4RMethylation

15823041
14Kubiquitylation

22980979
14Kubiquitylation

22980979
16Kubiquitylation

22980979
16Kubiquitylation

22980979
27KMethylation

15386022
27Kubiquitylation

15386022
63Kubiquitylation

15386022
105QMethylation

24352239
120Kubiquitylation

15386022
120Kubiquitylation

15386022
121TPhosphorylation

15078818
Disease-associated PTM Sites based on SAP

* Distance = the distance between SAP position and PTM sites.

Modified Location Modification Variant Position
(Distance <= 10) 		Residue Change SAP Related Disease Reference

Oops, there are no SNP-PTM records of H2A1_HUMAN !!
Protein-Protein Interaction
Interacting Protein Gene Name Interaction Type PPI Reference Domain-Domain Interactions

Oops, there are no PPI records of H2A1_HUMAN !!
Drug and Disease Associations
Kegg Disease
There are no disease associations of PTM sites.
There are no disease associations of PTM sites.
There are no disease associations of PTM sites.
There are no disease associations of PTM sites.
There are no disease associations of PTM sites.
OMIM Disease
There are no disease associations of PTM sites.
Kegg Drug
There are no disease associations of PTM sites.
There are no disease associations of PTM sites.
There are no disease associations of PTM sites.
There are no disease associations of PTM sites.
There are no disease associations of PTM sites.
DrugBank
There are no disease associations of PTM sites.
Regulatory Network of H2A1_HUMAN

loading...

Related Literatures of Post-Translational Modification
Acetylation
ReferencePubMed
"Precise characterization of human histones in the H2A gene family bytop down mass spectrometry.";
Boyne M.T. II, Pesavento J.J., Mizzen C.A., Kelleher N.L.;
J. Proteome Res. 5:248-253(2006).
Cited for: MASS SPECTROMETRY, AND ACETYLATION AT SER-2.
"Deimination of histone H2A and H4 at arginine 3 in HL-60granulocytes.";
Hagiwara T., Hidaka Y., Yamada M.;
Biochemistry 44:5827-5834(2005).
Cited for: ACETYLATION AT SER-2, CITRULLINATION AT ARG-4, AND MASS SPECTROMETRY.
"Global regulation of post-translational modifications on corehistones.";
Galasinski S.C., Louie D.F., Gloor K.K., Resing K.A., Ahn N.G.;
J. Biol. Chem. 277:2579-2588(2002).
Cited for: IDENTIFICATION BY MASS SPECTROMETRY, PHOSPHORYLATION AT SER-2, ANDACETYLATION AT SER-2.
"Characterization of histones H2A and H2B variants and their post-translational modifications by mass spectrometry.";
Bonenfant D., Coulot M., Towbin H., Schindler P., van Oostrum J.;
Mol. Cell. Proteomics 5:541-552(2006).
Cited for: IDENTIFICATION BY MASS SPECTROMETRY, ACETYLATION AT LYS-6, ANDPHOSPHORYLATION AT SER-2.
Phosphorylation
ReferencePubMed
"Characterization of histones H2A and H2B variants and their post-translational modifications by mass spectrometry.";
Bonenfant D., Coulot M., Towbin H., Schindler P., van Oostrum J.;
Mol. Cell. Proteomics 5:541-552(2006).
Cited for: IDENTIFICATION BY MASS SPECTROMETRY, ACETYLATION AT LYS-6, ANDPHOSPHORYLATION AT SER-2.
"Phosphorylation of histone H2A inhibits transcription on chromatintemplates.";
Zhang Y., Griffin K., Mondal N., Parvin J.D.;
J. Biol. Chem. 279:21866-21872(2004).
Cited for: PHOSPHORYLATION AT SER-2, AND MUTAGENESIS OF SER-2.
"Global regulation of post-translational modifications on corehistones.";
Galasinski S.C., Louie D.F., Gloor K.K., Resing K.A., Ahn N.G.;
J. Biol. Chem. 277:2579-2588(2002).
Cited for: IDENTIFICATION BY MASS SPECTROMETRY, PHOSPHORYLATION AT SER-2, ANDACETYLATION AT SER-2.
Ubiquitylation
ReferencePubMed
"DNA damage triggers nucleotide excision repair-dependentmonoubiquitylation of histone H2A.";
Bergink S., Salomons F.A., Hoogstraten D., Groothuis T.A.M.,de Waard H., Wu J., Yuan L., Citterio E., Houtsmuller A.B.,Neefjes J., Hoeijmakers J.H.J., Vermeulen W., Dantuma N.P.;
Genes Dev. 20:1343-1352(2006).
Cited for: UBIQUITINATION AT LYS-120.
"Role of Bmi-1 and Ring1A in H2A ubiquitylation and Hox genesilencing.";
Cao R., Tsukada Y., Zhang Y.;
Mol. Cell 20:845-854(2005).
Cited for: UBIQUITINATION AT LYS-120.
"Role of histone H2A ubiquitination in Polycomb silencing.";
Wang H., Wang L., Erdjument-Bromage H., Vidal M., Tempst P.,Jones R.S., Zhang Y.;
Nature 431:873-878(2004).
Cited for: UBIQUITINATION AT LYS-120.

TOP
© 2024 Institute of Bioinformatics and Systems Biology, NYCU | Designed by : BiOmics Laboratory