Fas Induces Cytoplasmic Apoptotic Responses and Activation of the MKK7-JNK/SAPK and MKK6-p38 Pathways Independent of CPP32-like Proteases

doi:10.1083/jcb.139.4.1005

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© The Rockefeller University Press, 0021-9525/1997//1005 $5.00
The Journal of Cell Biology, Volume 139, Number 4, , 1997 1005-1015

Article

Fas Induces Cytoplasmic Apoptotic Responses and Activation of the MKK7-JNK/SAPK and MKK6-p38 Pathways Independent of CPP32-like Proteases

Fumiko Toyoshima, Tetsuo Moriguchi, and Eisuke Nishida

Department of Biophysics, Graduate School of Science, Kyoto University, Kitashirakawa-Oiwake, Sakyo-ku, Kyoto 606-01, Japan

IL-1β converting enzyme (ICE) family cysteine proteasesare subdivided into three groups; ICE-, CPP32-, and Ich-1–likeproteases. In Fas-induced apoptosis, activation of ICE-likeproteases is followed by activation of CPP32-like proteaseswhich is thought to be essential for execution of the celldeath. It was recently reported that two subfamily members ofthe mitogen-activated protein kinase superfamily, JNK/SAPK and p38, are activated during Fas-induced apoptosis. Here,we have shown that MKK7, but not SEK1/ MKK4, is activated byFas as an activator for JNK/ SAPK and that MKK6 is a major activatorfor p38 in Fas signaling. Then, to dissect various cellularresponses induced by Fas, we used several peptide inhibitorsfor ICE family proteases in Fas-treated Jurkat cells and KBcells. While Z-VAD-FK which inhibited almost all the Fas-inducedcellular responses blocked the activation of JNK/SAPK and p38,Ac-DEVD-CHO and Z-DEVD-FK, specific inhibitors for CPP32-likeproteases, which inhibited the Fas-induced chromatin condensationand DNA fragmentation did not block the activation of JNK/SAPKand p38. Interestingly, these DEVD-type inhibitors did notblock the Fas-induced morphological changes (cell shrinkageand surface blebbing), induction of Apo2.7 antigen, or thecell death (as assessed by the dye exclusion ability). These results suggest that the Fas-induced activation of the JNK/SAPKand p38 signaling pathways does not require CPP32-like proteasesand that CPP32-like proteases, although essential for apoptoticnuclear events (such as chromatin condensation and DNA fragmentation),are not required for other apoptotic events in the cytoplasmor the cell death itself. Thus, the Fas signaling pathway divergesinto multiple, separate processes, each of which may be responsiblefor part of the apoptotic cellular responses.

1. Abbreviation used in this paper: ICE, IL-1β convertingenzyme.

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