Atractyloside‐induced release of cathepsin B, a protease with caspase‐processing activity

Vancompernolle, Katia; Herreweghe, Franky Van; Pynaert, Gwenda; Craen, Marc Van de; Vos, Kurt J. De; Totty, Nick; Sterling, Alistar; Fiers, Walter; Vandenabeele, Peter; Grooten, Johan

doi:10.1016/s0014-5793(98)01275-7

Cited by 289 publications

(220 citation statements)

References 38 publications

(50 reference statements)

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“…Our experiments using specific protease inhibitors suggest the involvement of non-caspase proteases in CEACAM1-4L-induced apoptosis including aspartate proteases, metalloproteinases and cathepsin B. In fact, activation of caspase-1 by cathepsin B and inhibition of the corresponding apoptosis pathway by the addition of Z-VAD.fmk have been well documented (Vancompernolle et al, 1998). It is thus likely that procaspase activation may be initiated by these proteases.…”

Section: Activation and Processing Of Ceacam1 During Apoptosis S Nittmentioning

confidence: 60%

The CEACAM1-mediated apoptosis pathway is activated by CEA and triggers dual cleavage of CEACAM1

et al. 2008

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Marked reduction in apoptosis is a hallmark of early colon tumour growth and the vast majority of these tumours exhibit a loss of expression of the glycoprotein carcinoembryonic-antigen-related cell adhesion molecule 1 (CEACAM1). We recently reported that the CEACAM1 functions as a mediator of apoptosis implicating this cell surface protein in early tumour development. However, the mechanistic involvement of CEACAM1 in cell death pathways is unclear. Here, we show that apoptosis triggers cleavage of the long form of CEACAM1 (CEACAM1-4L) at intracellular and extracellular sites in Jurkat cells and HEK293 cells. Signalling through CEACAM1 leads to caspase activation including caspase-1 and -3 and also involves non-caspase proteases. Moreover, we provide evidence that the naturally occurring CEACAM family member CEA is an inducer of CEACAM1-mediated apoptosis in HT29 colon cancer cells, an effect that depends on the abundance of CEACAM1 on the cell surface. Together, our results demonstrate that the CEACAM1-dependent cell death pathway involves dual cleavage of CEACAM1 and caspase activation and can be activated by CEA.

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Section: Activation and Processing Of Ceacam1 During Apoptosis S Nittmentioning

confidence: 60%

The CEACAM1-mediated apoptosis pathway is activated by CEA and triggers dual cleavage of CEACAM1

et al. 2008

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“…In particular, some forms of apoptosis can be inhibited by blocking cathepsin B. It is of interest that many peptide caspase inhibitors are also capable of blocking cathepsin B activity both in vitro and in cells [36,37]. Furthermore, cathepsin B has been shown to process caspase 3 under neutral conditions, albeit weakly [37].…”

Section: Discussionmentioning

confidence: 99%

Perforin‐dependent activation‐induced cell death acts through caspase 3 but not through caspases 8 or 9

et al. 2003

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Activation-induced cell death (AICD) is a phenomenon in which activated T cells undergo apoptosis upon restimulation. We are studying a form of AICD that can occur before cells become competent to die by Fas (hence "early" AICD) and which depends on the presence of perforin. Previous studies indicate that it does not occur through granule exocytosis but via some endogenous pathway. We here investigate a possible role for caspases. Caspase 3 -/-cells were protected, suggesting a role for caspase 3 in early AICD. After recrosslinking, caspase 3 activity could be detected in cell lysates between 3 and 12 h, and CD8 + T cells became annexin V-positive between 15 and 18 h. Blocking anti-Fas ligand antibody failed to inhibit death, and no processing of either caspase 8 or caspase 9 was detected in recrosslinked cells. Furthermore, T cells lacking functional caspase 9 continued to die in early AICD. Thus, perforin-dependent early AICD appears to require activation of caspase 3, but not caspases 8 or 9. As perforin has no intrinsic catalytic abilities, we propose that it releases some endogenous activity that can activate caspase 3.

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“…24 Alternatively, cathepsins could cleave and activate caspases or their downstream death effector substrates, 25 thereby causing apoptosis. In support of the former mechanism, it has been shown that cathepsin B can activate the inflammatory caspases 1 and 11, 17,26 and that cathepsin L may activate caspase-3. 20 The final possible mode of cathepsin action places cathepsins far upstream in the apoptotic cascade, cleaving the proapoptotic Bcl-2 family member Bid to initiate mitochondrial release of cytochrome c. This last hypothesis received in vitro confirmation when it was shown that lysosomal extracts containing cathepsins were able to cleave purified Bid in a physiologically relevant manner that supported apoptosis.…”

Section: Introductionmentioning

confidence: 90%

“…[3][4][5][6][7][8][9][10][11][12][13][14] Although cathepsins normally reside in the lysosome and carry out nonselective degradation of proteins, a strong case was made for the involvement of these proteases in apoptosis when it was shown that agents that disrupted lysosomes and caused cathepsins to redistribute to the cytoplasm inevitably resulted in apoptosis. 13,[15][16][17][18][19] Similarly, cathepsin inhibitor treatment blocked this apoptosis. 11,14,[18][19][20][21][22] Theoretically, the cathepsin proteases could induce apoptosis by a variety of different mechanisms.…”

Section: Introductionmentioning

confidence: 94%

Apoptosis caused by cathepsins does not require Bid signaling in an in vivo model of progressive myoclonus epilepsy (EPM1)

Vilaythong

Yin

et al. 2003

Cell Death Differ

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Apoptosis can be mediated by mechanisms other than the traditional caspase-mediated cleavage cascade. There is growing recognition that alternative proteolytic enzymes such as the lysosomal cathepsin proteases can initiate or propagate proapoptotic signals, but it is currently unclear how cathepsins achieve these actions. Recent in vitro evidence suggests that cathepsins cleave the proapoptotic Bcl-2 family member Bid, thereby activating it and allowing it to induce the mitochondrial release of cytochrome c and subsequent apoptosis. We have tested this hypothesis in vivo by breeding mice that lack cathepsin inhibition (cystatin B-deficient mice) to Bid-deficient mice, to determine whether the apoptosis caused by cathepsins is dependent on Bid signaling. We found that cathepsins are still able to promote apoptosis even in the absence of Bid, indicating that these proteases mediate apoptosis via a different pathway, or that some other molecule can functionally substitute for Bid in this system.

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Atractyloside‐induced release of cathepsin B, a protease with caspase‐processing activity

Cited by 289 publications

References 38 publications

The CEACAM1-mediated apoptosis pathway is activated by CEA and triggers dual cleavage of CEACAM1

The CEACAM1-mediated apoptosis pathway is activated by CEA and triggers dual cleavage of CEACAM1

Perforin‐dependent activation‐induced cell death acts through caspase 3 but not through caspases 8 or 9

Apoptosis caused by cathepsins does not require Bid signaling in an in vivo model of progressive myoclonus epilepsy (EPM1)

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