Human Metabolome Database: Showing Protein Alpha-N-acetylgalactosaminidase (HMDBP13602)

Identification Biological properties Gene properties Protein properties External links References XML Show 1 metabolite

Identification

HMDB Protein ID

HMDBP13602

Secondary Accession Numbers

None

Name

Alpha-N-acetylgalactosaminidase

Synonyms

Alpha-galactosidase B

Gene Name

NAGA

Protein Type

Unknown

Biological Properties

General Function

Not Available

Specific Function

Removes terminal alpha-N-acetylgalactosamine residues from glycolipids and glycopeptides. Required for the breakdown of glycolipids.

Pathways

Glycosphingolipid biosynthesis - globo and isoglobo series
Lysosome

Reactions

Not Available

GO Classification

Biological Process
glycoside catabolic process
glycosylceramide catabolic process
oligosaccharide metabolic process
carbohydrate catabolic process
glycolipid catabolic process
Cellular Component
cytoplasm
lysosome
Molecular Function
alpha-N-acetylgalactosaminidase activity
alpha-galactosidase activity
protein homodimerization activity

Cellular Location

Not Available

Gene Properties

Chromosome Location

Not Available

Locus

Not Available

SNPs

Not Available

Gene Sequence

Not Available

Protein Properties

Number of Residues

415

Molecular Weight

46870.72

Theoretical pI

5.863

Pfam Domain Function

Melibiase_2 (PF16499 )
Melibiase_2_C (PF17450 )

Signals

1-17;

Transmembrane Regions

Not Available

Protein Sequence

Not Available

External Links

GenBank ID Protein

Not Available

UniProtKB/Swiss-Prot ID

Q66H12

UniProtKB/Swiss-Prot Entry Name

NAGAB_RAT

PDB IDs

Not Available

GenBank Gene ID

Not Available

GeneCard ID

Not Available

GenAtlas ID

Not Available

HGNC ID

Not Available

References

General References

Gerhard DS, Wagner L, Feingold EA, Shenmen CM, Grouse LH, Schuler G, Klein SL, Old S, Rasooly R, Good P, Guyer M, Peck AM, Derge JG, Lipman D, Collins FS, Jang W, Sherry S, Feolo M, Misquitta L, Lee E, Rotmistrovsky K, Greenhut SF, Schaefer CF, Buetow K, Bonner TI, Haussler D, Kent J, Kiekhaus M, Furey T, Brent M, Prange C, Schreiber K, Shapiro N, Bhat NK, Hopkins RF, Hsie F, Driscoll T, Soares MB, Casavant TL, Scheetz TE, Brown-stein MJ, Usdin TB, Toshiyuki S, Carninci P, Piao Y, Dudekula DB, Ko MS, Kawakami K, Suzuki Y, Sugano S, Gruber CE, Smith MR, Simmons B, Moore T, Waterman R, Johnson SL, Ruan Y, Wei CL, Mathavan S, Gunaratne PH, Wu J, Garcia AM, Hulyk SW, Fuh E, Yuan Y, Sneed A, Kowis C, Hodgson A, Muzny DM, McPherson J, Gibbs RA, Fahey J, Helton E, Ketteman M, Madan A, Rodrigues S, Sanchez A, Whiting M, Madari A, Young AC, Wetherby KD, Granite SJ, Kwong PN, Brinkley CP, Pearson RL, Bouffard GG, Blakesly RW, Green ED, Dickson MC, Rodriguez AC, Grimwood J, Schmutz J, Myers RM, Butterfield YS, Griffith M, Griffith OL, Krzywinski MI, Liao N, Morin R, Palmquist D, Petrescu AS, Skalska U, Smailus DE, Stott JM, Schnerch A, Schein JE, Jones SJ, Holt RA, Baross A, Marra MA, Clifton S, Makowski KA, Bosak S, Malek J: The status, quality, and expansion of the NIH full-length cDNA project: the Mammalian Gene Collection (MGC). Genome Res. 2004 Oct;14(10B):2121-7. [PubMed:15489334 ]