The c-IAP-1 and c-IAP-2 proteins are direct inhibitors of specific caspases
Open Access
- 1 December 1997
- journal article
- research article
- Published by Springer Nature in The EMBO Journal
- Vol. 16 (23), 6914-6925
- https://doi.org/10.1093/emboj/16.23.6914
Abstract
The inhibitor of apoptosis (IAP) family of proteins are highly conserved through evolution. However, the mechanisms by which these proteins interfere with apoptotic cell death have been enigmatic. Recently, we showed that one of the human IAP family proteins, XIAP, can bind to and potently inhibit specific cell death proteases (caspases) that function in the distal portions of the proteolytic cascades involved in apoptosis. In this study, we investigated three of the other known members of the human IAP family, c‐IAP‐1, c‐IAP‐2 and NAIP. Similarly to XIAP, in vitro binding experiments indicated that c‐IAP‐1 and c‐IAP‐2 bound specifically to the terminal effector cell death proteases, caspases‐3 and ‐7, but not to the proximal protease caspase‐8, caspases‐1 or ‐6. In contrast, NAIP failed to bind tightly to any of these proteases. Recombinant c‐IAP‐1 and c‐IAP‐2 also inhibited the activity of caspases‐3 and ‐7 in vitro, with estimated Kis of ≤0.1 μM, whereas NAIP did not. The BIR domain‐containing region of c‐IAP‐1 and c‐IAP‐2 was sufficient for inhibition of these caspases, though proteins that retained the RING domain were somewhat more potent. Utilizing a cell‐free system in which caspases were activated in cytosolic extracts by addition of cytochrome c, c‐IAP‐1 and c‐IAP‐2 inhibited both the generation of caspase activities and proteolytic processing of pro‐caspase‐3. Similar results were obtained in intact cells when c‐IAP‐1 and c‐IAP‐2 were overexpressed by gene transfection, and apoptosis was induced by the anticancer drug, etoposide. Cleavage of c‐IAP‐1 or c‐IAP‐2 was not observed when interacting with the caspases, implying a different mechanism from the baculovirus p35 protein, the broad spectrum suicide inactivator of caspases. Taken together, these findings suggest that c‐IAP‐1 and c‐IAP‐2 function similarly to XIAP by inhibiting the distal cell death proteases, caspases‐3 and ‐7, whereas NAIP presumably inhibits apoptosis via other targets.Keywords
This publication has 63 references indexed in Scilit:
- Bik and Bak Induce Apoptosis Downstream of CrmA but Upstream of Inhibitor of ApoptosisJournal of Biological Chemistry, 1997
- Mitochondrial control of apoptosisImmunology Today, 1997
- Induction of Apoptotic Program in Cell-Free Extracts: Requirement for dATP and Cytochrome cCell, 1996
- FLICE, A Novel FADD-Homologous ICE/CED-3–like Protease, Is Recruited to the CD95 (Fas/APO-1) Death-Inducing Signaling ComplexCell, 1996
- Involvement of MACH, a Novel MORT1/FADD-Interacting Protease, in Fas/APO-1- and TNF Receptor–Induced Cell DeathCell, 1996
- Purification and Characterization of an Interleukin-1β-converting Enzyme Family Protease That Activates Cysteine Protease P32 (CPP32)Published by Elsevier ,1996
- Suppression of apoptosis in mammalian cells by NAIP and a related family of IAP genesNature, 1996
- Drosophila homologs of baculovirus inhibitor of apoptosis proteins function to block cell deathCell, 1995
- Inhibition of the Caenorhabditis elegans cell-death protease CED-3 by a CED-3 cleavage site in baculovirus p35 proteinNature, 1995
- The cystatins: Protein inhibitors of cysteine proteinasesFEBS Letters, 1991