| Literature DB >> 10085291 |
J F Krebs1, R C Armstrong, A Srinivasan, T Aja, A M Wong, A Aboy, R Sayers, B Pham, T Vu, K Hoang, D S Karanewsky, C Leist, A Schmitz, J C Wu, K J Tomaselli, L C Fritz.
Abstract
The mechanism by which membrane-bound Bcl-2 inhibits the activation of cytoplasmic procaspases is unknown. Here we characterize an intracellular, membrane-associated form of procaspase-3 whose activation is controlled by Bcl-2. Heavy membranes isolated from control cells contained a spontaneously activatable caspase-3 zymogen. In contrast, in Bcl-2 overexpressing cells, although the caspase-3 zymogen was still associated with heavy membranes, its spontaneous activation was blocked. However, Bcl-2 expression had little effect on the levels of cytoplasmic caspase activity in unstimulated cells. Furthermore, the membrane-associated caspase-3 differed from cytosolic caspase-3 in its responsiveness to activation by exogenous cytochrome c. Our results demonstrate that intracellular membranes can generate active caspase-3 by a Bcl-2-inhibitable mechanism, and that control of caspase activation in membranes is distinct from that observed in the cytoplasm. These data suggest that Bcl-2 may control cytoplasmic events in part by blocking the activation of membrane-associated procaspases.Entities:
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Year: 1999 PMID: 10085291 PMCID: PMC2148187 DOI: 10.1083/jcb.144.5.915
Source DB: PubMed Journal: J Cell Biol ISSN: 0021-9525 Impact factor: 10.539