Caspase 2
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Caspase 2, apoptosis-related cysteine peptidase (neural precursor cell expressed, developmentally down-regulated 2)
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| PDB rendering based on 1pyo. | ||||||||||||||
| Available structures: 1pyo, 2p2c | ||||||||||||||
| Identifiers | ||||||||||||||
| Symbol(s) | CASP2; CASP-2; ICH-1L; ICH-1L/1S; ICH1; NEDD2 | |||||||||||||
| External IDs | OMIM: 600639 MGI: 97295 HomoloGene: 7254 | |||||||||||||
| EC number | 3.4.22.55 | |||||||||||||
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| RNA expression pattern | ||||||||||||||
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| Orthologs | ||||||||||||||
| Human | Mouse | |||||||||||||
| Entrez | 835 | 12366 | ||||||||||||
| Ensembl | ENSG00000106144 | ENSMUSG00000029863 | ||||||||||||
| Uniprot | P42575 | P29594 | ||||||||||||
| Refseq | NM_032982 (mRNA) NP_116764 (protein) |
NM_007610 (mRNA) NP_031636 (protein) |
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| Location | Chr 7: 142.7 - 142.71 Mb | Chr 6: 42.19 - 42.21 Mb | ||||||||||||
| Pubmed search | [1] | [2] | ||||||||||||
Caspase 2 is an enzyme that proteolytically cleaves other proteins. It belongs to a family of cysteine proteases called caspases that only cleave proteins at an amino acid following a aspartic acid residue. Within this family, caspase 2 is part of the Ich-1 subfamily. It is one of the most conserved caspases in different species of animal. Caspase 2 has a similar amino acid sequence to initiator caspases, including caspase 1, caspase 4, caspase 5 and caspase 9. It is produced as a zymogen, which contains a long pro-domain that is similar to that of caspase 9 and contains a protein interaction domain known as a CARD domain. Pro-caspase-2 contains two subunits, p19 and p12. It has been shown to associate with several proteins involved in apoptosis using its CARD domain, including RIP-associated Ich-1/Ced-3-homologue protein with a death domain (RAIDD), apoptosis repressor with caspase recruitment domain (ARC) and death effector filament-forming Ced-4 like apoptosis protein (DEFCAP).[1]
[edit] References
- ^ Zhivotovsky B, Orrenius S (2005). "Caspase-2 function in response to DNA damage". Biochem. Biophys. Res. Commun. 331 (3): 859–67. doi:. PMID 15865942.
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