Requirement of an ICE/CED-3 protease for Fas/APO-1-mediated apoptosis

Łos, Marek; Craen, Marc Van de; Penning, Louis C.; Schenk, Heike; Westendorp, Michael O.; Baeuerle, Patrick A.; Dröge, Wulf; Krammer, Peter H.; Fiers, Walter; Schulze‐Osthoff, Klaus

doi:10.1038/375081a0

Cited by 588 publications

(372 citation statements)

References 24 publications

(1 reference statement)

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“…Furthermore, caspase-8 was potently inhibited by CrmA, which is inhibitory to Fas-stimulated apoptosis of Jurkat cells though not to that induced by staurosporine . This ®nding, in combination with similarities in sensitivity to CrmA of labeled caspases in Fas-stimulated (F22, F20, F19, and F17) and staurosporine-treated (S22, S20, S19, S17) cells, is consistent with the notion that CrmA inhibition of caspase-8 is responsible for the sensitivity of Fasinduced apoptotic cell death to CrmA (Enari et al, 1995;Los et al, 1995;. Thus, caspase-8, a CrmA-sensitive protease, appears to be critical for the initiation of the protease cascade in Fasstimulated cells.…”

Section: Discussionsupporting

confidence: 86%

“…In particular, we show that the addition of active caspase-8 (MACH/FLICE/Mch5) to extracts from non-apoptotic Jurkat cells can trigger stepwise activation of caspases that is strikingly similar to that induced by Fas stimulation. Finally, we ®nd that caspase-8 is sensitive to CrmA, the inhibitor of Fasinduced apoptotic cell death (Enari et al, 1995;Los et al, 1995;. Taken together, these results support the notion that the activation of multiple caspases is required for the organization of protease cascades as well as for the cleavage of multiple apoptosis-associated substrates.…”

Section: Introductionsupporting

confidence: 80%

“…It has been reported that Fas-induced cell death is prevented by CrmA (Enari et al, 1995;Los et al, 1995;, in contrast to other cell death events such as staurosporine-induced apoptosis . Interestingly, the protease activity of caspase-8 as assessed by the cleavage of DEVD-MCA (Km *7 mM) was *95% inhibited by preincubation with 100 nM CrmA ( Figure 6a).…”

Section: Crma Inhibition Of Caspase-8 Activitymentioning

confidence: 95%

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Affinity labeling displays the stepwise activation of ICE-related proteases by Fas, staurosporine, and CrmA-sensitive caspase-8

et al. 1997

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The activation of multiple interleukin-1b converting enzyme-related proteases (caspases) in apoptotic mammalian cells raises questions as to whether the multiple active caspases have distinct roles in apoptotic execution as well as how these proteases are organized in apoptotic signaling pathways. Here we used an a nity-labeling agent, YV(bio)KD-aomk, to investigate the caspases activated during apoptotic cell death. YV(bio)KD-aomk identi®ed six distinct polypeptides corresponding to active caspases in Fas-stimulated Jurkat T cells. On staurosporine treatment, four polypeptides were detected. Competition experiments showed that the labeled caspases have distinct substrate preferences. Stepwise appearance of the labeled caspases in each cell death event was consistent with the view that the activated caspases are organized into protease cascades. Moreover, we found that stepwise activation of caspases similar to that induced by Fas ligation is triggered by exposing non-apoptotic Jurkat cell extracts to caspase-8 (MACH/FLICE/Mch5). Conversely, CrmA protein, a viral suppressor of Fas-induced apoptosis, inhibited the protease activity of caspase-8. Overall, these ®ndings provide evidence that caspase-8, a CrmA-sensitive protease, is responsible for initiating the stepwise activation of multiple caspases in Fas-stimulated cells.

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Section: Discussionsupporting

confidence: 86%

Section: Introductionsupporting

confidence: 80%

Section: Crma Inhibition Of Caspase-8 Activitymentioning

confidence: 95%

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Affinity labeling displays the stepwise activation of ICE-related proteases by Fas, staurosporine, and CrmA-sensitive caspase-8

et al. 1997

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“…Decreased surface expression of CD95 has been reported to confer resistance to CD95-induced cell death. 34 Engagement of CD95 receptor on the surface leads to the activation of procaspase 8, caspase 3, 35 and ultimately to cleavage of the caspase 3 substrate poly (ADP-ribose) polymerase (PARP). 36 To determine whether higher resistance to anti-CD95-induced cell death in c-Myc-deficient cells correlated with changes in PARP processing, we performed Western blot analysis on these cells.…”

Section: Resultsmentioning

confidence: 99%

c-Myc-deficient B lymphocytes are resistant to spontaneous and induced cell death

2003

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C-myc gene is a member of the myc family of protooncogenes involved in proliferation, differentiation, and apoptosis. Overexpression of c-myc in fibroblasts causes apoptosis under low serum conditions in a process that requires the interaction of CD95 and CD95L on the surface. We have previously reported an in vivo conditional model to inactivate the c-myc gene in B lymphocytes. Here, we show that c-Myc-deficient primary B lymphocytes are resistant to different apoptotic stimuli. Nonactivated c-Myc-deficient B cells are resistant to spontaneous cell death. Upon activation, c-Myc-deficient B lymphocytes express normal surface levels of activation markers, and show resistance to staurosporine and CD95-induced cell death.

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“…It has been reported that Fas-and tumor necrosis factor (TNF) receptor-mediated apoptosis is driven by caspase family, because it is suppressed by their inhibitors, including cowpox virus CrmA Enari et al, 1995;Los et al, 1995), baculovirus p35 and tetrapeptide caspase-1 and caspase-3 inhibitors (Enari et al, 1995;Los et al, 1995;Schlegel et al, 1996;Chinnaiyan et al, 1996;Hasegawa et al, 1996). It has also been reported that thymocytes from caspase-1-de®cient mice are resistant to Fas-mediated apoptosis, indicating the direct involvement of caspase-1 itself in this process of thymocyte death (Kuida et al, 1995).…”

Section: Introductionmentioning

confidence: 99%

Involvement of caspase-4(-like) protease in Fas-mediated apoptotic pathway

et al. 1997

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Proteases of the caspase family, especially caspase-1 (ICE)(-like), caspase-3 (CPP32/Yama/apopain)(-like) and caspase-8 (MACH/FLICE/Mch5) proteases, are implicated in Fas (APO-1/CD95)-mediated apoptosis. Here, we show that the caspase-4 (TX/ICH-2/ICE rel II)(-like) protease, another member of the caspase family, is also involved in Fas-mediated apoptosis, based upon the observations: (i) caspase-4 is processed in response to an agonistic anti-Fas antibody treatment, (ii) overexpression of a mutant caspase-4 with active site mutations in both p20 and p10 subunits delays Fas-mediated apoptosis, (iii) microinjected anti-caspase-4 antibodies inhibit Fasmediated apoptosis. Together with our observations that the mutant caspase-4 inhibits the Fas-mediated activation of caspase-3(-like) proteases and puri®ed caspase-4 cleaves pro-caspase-3 to generate a subunit of active form, these results suggest that Fas-mediated apoptosis is driven by a caspase cascade in which the caspase-4(-like) protease transmits a death signal from caspase-8 to caspase-3(-like) proteases probably through directly cleaving pro-caspase-3(-like) proteases.

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Requirement of an ICE/CED-3 protease for Fas/APO-1-mediated apoptosis

Cited by 588 publications

References 24 publications

Affinity labeling displays the stepwise activation of ICE-related proteases by Fas, staurosporine, and CrmA-sensitive caspase-8

Affinity labeling displays the stepwise activation of ICE-related proteases by Fas, staurosporine, and CrmA-sensitive caspase-8

c-Myc-deficient B lymphocytes are resistant to spontaneous and induced cell death

Involvement of caspase-4(-like) protease in Fas-mediated apoptotic pathway

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