CATH Classification

Domain Context

CATH Clusters

Superfamily 3.40.50.1460
Functional Family Caspase 2

Enzyme Information

3.4.22.55
Caspase-2.
based on mapping to UniProt P42575
Strict requirement for an Asp residue at P1, with 316-asp being essential for proteolytic activity and has a preferred cleavage sequence of Val- Asp-Val-Ala-Asp-|-.
-!- Caspase-2 is an initiator caspase, as are caspases-8 (EC 3.4.22.61), caspase-9 (EC 3.4.22.62) and caspase-10 (EC 3.4.22.63). -!- Contains a caspase-recruitment domain (CARD) in its N-terminal prodomain, which plays a role in procaspase activation. -!- Two forms of caspase-2 exist that have antagonistic effects: caspase- 2L induces programd cell death and caspase-2S suppresses cell death. -!- Caspase-2 is activated by caspase-3 (EC 3.4.22.56), or by a caspase- 3-like protease. -!- Activation involves cleavage of the N-terminal prodomain, followed by self-proteolysis between the large and small subunits of pro-caspase- 2 and further proteolysis into smaller fragments. -!- Proteolysis occurs at Asp residues and the preferred substrate for this enzyme is a pentapeptide rather than a tetrapeptide. -!- Apart from itself, the enzyme can cleave golgin-16, which is present in the Golgi complex and has a cleavage site that is unique for caspase-2. -!- Alpha-II-spectrin, a component of the membrane cytoskeleton, is a substrate of the large isoform of pro-caspase-2 (caspase-2L) but not of the short isoform (caspase-2S). -!- Belongs to peptidase family C14.

UniProtKB Entries (1)

P42575
CASP2_HUMAN
Homo sapiens
Caspase-2

PDB Structure

PDB 3RJM
External Links
Method X-RAY DIFFRACTION
Organism
Primary Citation
Exploiting differences in caspase-2 and -3 S(2) subsites for selectivity: Structure-based design, solid-phase synthesis and in vitro activity of novel substrate-based caspase-2 inhibitors.
Maillard, M.C., Brookfield, F.A., Courtney, S.M., Eustache, F.M., Gemkow, M.J., Handel, R.K., Johnson, L.C., Johnson, P.D., Kerry, M.A., Krieger, F., Meniconi, M., Munoz-Sanjuan, I., Palfrey, J.J., Park, H., Schaertl, S., Taylor, M.G., Weddell, D., Dominguez, C.
Bioorg.Med.Chem.
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