Inhibition of Ced-3/ICE-related Proteases Does Not Prevent Cell Death Induced by Oncogenes, DNA Damage, or the Bcl-2 Homologue Bak

Abstract

There is increasing evidence for a central role in mammalian apoptosis of the interleukin-1β– converting enzyme (ICE) family of cysteine proteases, homologues of the product of the nematode “death” gene, ced-3. Ced-3 is thought to act as an executor rather than a regulator of programmed cell death in the nematode. However, it is not known whether mammalian ICE-related proteases (IRPs) are involved in the execution or the regulation of mammalian apoptosis. Moreover, an absolute requirement for one or more IRPs for mammalian apoptosis has yet to be established. We have used two cell-permeable inhibitors of IRPs, Z-Val-Ala-Asp.fluoromethylketone (ZVAD.fmk) and t-butoxy carbonyl-Asp.fluoromethylketone (BD.fmk), to demonstrate a critical role for IRPs in mammalian apoptosis induced by several disparate mechanisms (deregulated oncogene expression, ectopic expression of the Bcl-2 relative Bak, and DNA damage–induced cell death). In all instances, ZVAD.fmk and BD.fmk treatment inhibits characteristic biochemical and morphological events associated with apoptosis, including cleavage of nuclear lamins and poly-(ADP-ribose) polymerase, chromatin condensation and nucleosome laddering, and external display of phosphatidylserine. However, neither ZVAD.fmk nor BD.fmk inhibits the onset of apoptosis, as characterized by the onset of surface blebbing; rather, both act to delay completion of the program once initiated. In complete contrast, IGF-I and Bcl-2 delay the onset of apoptosis but have no effect on the kinetics of the program once initiated. Our data indicate that IRPs constitute part of the execution machinery of mammalian apoptosis induced by deregulated oncogenes, DNA damage, or Bak but that they act after the point at which cells become committed to apoptosis or can be rescued by survival factors. Moreover, all such blocked cells have lost proliferative potential and all eventually die by a process involving cytoplasmic blebbing.

Keywords

ProteasesProgrammed cell deathDNA damageCell biologyApoptosisCellDNAChemistryBiologyBiochemistryEnzyme

MeSH Terms

Amino Acid Chloromethyl KetonesAnimalsApoptosisBloodCaenorhabditis elegans ProteinsCaspase 1CaspasesCell LineCell MembraneCysteine EndopeptidasesCysteine Proteinase InhibitorsDNA DamageFibroblastsGene ExpressionGenesmycHelminth ProteinsInsulin-Like Growth Factor ILaminsMembrane ProteinsMicroscopyVideoNuclear ProteinsPhosphatidylserinesPoly(ADP-ribose) PolymerasesProto-Oncogene Proteins c-bcl-2RatsTamoxifenbcl-2 Homologous Antagonist-Killer Protein

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Publication Info

Year: 1997
Type: article
Volume: 136
Issue: 1
Pages: 215-227
Citations: 547
Access: Closed

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APA Style

                            
                                
                                    Nicola McCarthy, 
                                
                                    Moira K. B. Whyte, 
                                
                                    Christopher S. Gilbert
                                
                                et al.
                            
                            (1997). 
                            Inhibition of Ced-3/ICE-related Proteases Does Not Prevent Cell Death Induced by Oncogenes, DNA Damage, or the Bcl-2 Homologue Bak. 
                            The Journal of Cell Biology
                            , 136
                            (1)
                            , 215-227.
                            https://doi.org/10.1083/jcb.136.1.215
                        

Identifiers

DOI: 10.1083/jcb.136.1.215
PMID: 9008715
PMCID: PMC2132458

Data Quality

Data completeness: 86%