Skip Header

Contribute Send feedback
Read comments (?) or add your own

A4J6L2 (A4J6L2_DESRM) Unreviewed, UniProtKB/TrEMBL

Last modified December 14, 2011. Version 28. Feed History...

Clusters with 100%, 90%, 50% identity | Third-party data text xml rdf/xml gff fasta
to top of pageNames·Attributes·General annotation·Ontologies·Sequence annotation·Sequences·References·Cross-refs·Entry infoCustomize order
to top of pageNames·Attributes·General annotation·Ontologies·Sequence annotation·Sequences·References·Cross-refs·Entry infoCustomize order

Names and origin

Protein namesRecommended name:
S-adenosylmethionine decarboxylase proenzyme 2 HAMAP MF_00464
Short name=AdoMetDC 2 HAMAP MF_00464
Short name=SAMDC 2 HAMAP MF_00464
EC=4.1.1.50 HAMAP MF_00464
Gene names
Name:speH2 HAMAP MF_00464
Ordered Locus Names:Dred_2200
OrganismDesulfotomaculum reducens (strain MI-1) [Complete proteome] [HAMAP]
Taxonomic identifier349161 [NCBI]
Taxonomic lineageBacteriaFirmicutesClostridiaClostridialesPeptococcaceaeDesulfotomaculum

Protein attributes

Sequence length127 AA.
Sequence statusComplete.
Protein existenceInferred from homology

General annotation (Comments)

Function

Catalyzes the decarboxylation of S-adenosylmethionine to S-adenosylmethioninamine (dcAdoMet), the propylamine donor required for the synthesis of the polyamines spermine and spermidine from the diamine putrescine By similarity. HAMAP MF_00464

Catalytic activity

S-adenosyl-L-methionine = (5-deoxy-5-adenosyl)(3-aminopropyl)-methylsulfonium salt + CO2. HAMAP MF_00464

Cofactor

Pyruvoyl group By similarity. HAMAP MF_00464

Pathway

Amine and polyamine biosynthesis; S-adenosylmethioninamine biosynthesis; S-adenosylmethioninamine from S-adenosyl-L-methionine: step 1/1. HAMAP MF_00464

Subunit structure

Heterotetramer of two alpha and two beta chains arranged as a dimer of alpha/beta heterodimers By similarity. HAMAP MF_00464

Post-translational modification

Is synthesized initially as an inactive proenzyme. Formation of the active enzyme involves a self-maturation process in which the active site pyruvoyl group is generated from an internal serine residue via an autocatalytic post-translational modification. Two non-identical subunits are generated from the proenzyme in this reaction, and the pyruvate is formed at the N-terminus of the alpha chain, which is derived from the carboxyl end of the proenzyme. The post-translation cleavage follows an unusual pathway, termed non-hydrolytic serinolysis, in which the side chain hydroxyl group of the serine supplies its oxygen atom to form the C-terminus of the beta chain, while the remainder of the serine residue undergoes an oxidative deamination to produce ammonia and the pyruvoyl group blocking the N-terminus of the alpha chain By similarity. HAMAP MF_00464

Sequence similarities

Belongs to the prokaryotic AdoMetDC family. Type 1 subfamily. HAMAP MF_00464

Sequence annotation (Features)

Feature keyPosition(s)LengthDescriptionGraphical viewFeature identifier

Sites

Active site631Schiff-base intermediate with substrate; via pyruvic acid By similarity HAMAP MF_00464
Active site681Proton acceptor; for processing activity By similarity HAMAP MF_00464
Active site831Proton donor; for catalytic activity By similarity HAMAP MF_00464
Site62 – 632Cleavage (non-hydrolytic); by autolysis By similarity HAMAP MF_00464

Amino acid modifications

Modified residue631Pyruvic acid (Ser); by autocatalysis By similarity HAMAP MF_00464

Sequences

Sequence LengthMass (Da)Tools
A4J6L2 [UniParc].

Last modified May 1, 2007. Version 1.
Checksum: 1494FF02D031DA3E

FASTA12713,878
        10         20         30         40         50         60 
MKPLGRHVLA EIYGCDFEIL NDVKKVEEIM VNAALESGAE VREYVFHKFS PQGVSGVVVI 

        70         80         90        100        110        120 
SESHLAIHTW PELGYAAVDV FTCGDSVNPW DACNFLTREF GAKDMSAQET KRGILPGMAP 


HLVAANS

« Hide

References

[1]"Complete sequence of Desulfotomaculum reducens MI-1."
Copeland A., Lucas S., Lapidus A., Barry K., Detter J.C., Glavina del Rio T., Hammon N., Israni S., Dalin E., Tice H., Pitluck S., Sims D., Brettin T., Bruce D., Han C., Tapia R., Schmutz J., Larimer F. expand/collapse author list , Land M., Hauser L., Kyrpides N., Kim E., Tebo B.M., Richardson P.
Submitted (MAR-2007) to the EMBL/GenBank/DDBJ databases
Cited for: NUCLEOTIDE SEQUENCE [LARGE SCALE GENOMIC DNA].
Strain: MI-1.

Cross-references

Sequence databases

EMBL
GenBank
DDBJ		CP000612 Genomic DNA. Translation: ABO50715.1.
RefSeqYP_001113540.1. NC_009253.1.

3D structure databases

ProteinModelPortalA4J6L2.
SMRA4J6L2. Positions 2-118.
ModBaseSearch...

Protein-protein interaction databases

STRINGA4J6L2.

Protocols and materials databases

StructuralBiologyKnowledgebaseSearch...

Genome annotation databases

GeneID4955778.
GenomeReviewsGene locus Dred_2200 in contig CP000612_GR.
KEGGdrm:Dred_2200.
PATRIC21730703. VBIDesRed82656_2413.

Organism-specific databases

CMRSearch...

Phylogenomic databases

eggNOGCOG1586.
HOGENOMHBG485559.
OMASYFFKFS.
ProtClustDBPRK03124.

Family and domain databases

HAMAPMF_00464. AdoMetDC_1.
[Tree]
InterProIPR003826. S-AdoMet_decarboxylase-bac/arc.
IPR016067. S-AdoMet_deCO2ase_core.
IPR017716. S-AdoMet_deCOase_pro-enz.
[Graphical view]
Gene3DG3DSA:3.60.90.10. SAM_decarbox. 1 hit.
KOK01611.
PfamPF02675. AdoMet_dc. 1 hit.
[Graphical view]
SUPFAMSSF56276. S-AdenosylMet_decarbase_core. 1 hit.
TIGRFAMsTIGR03330. SAM_DCase_Bsu. 1 hit.
ProtoNetSearch...

Entry information

Entry nameA4J6L2_DESRM
AccessionPrimary (citable) accession number: A4J6L2
Entry history
Integrated into UniProtKB/TrEMBL: May 1, 2007
Last sequence update: May 1, 2007
Last modified: December 14, 2011
This is version 28 of the entry and version 1 of the sequence. [Complete history]
Entry statusUnreviewed (UniProtKB/TrEMBL)
to top of pageNames·Attributes·General annotation·Ontologies·Sequence annotation·Sequences·References·Cross-refs·Entry info