期刊
MOLECULAR AND CELLULAR BIOLOGY
卷 26, 期 8, 页码 3071-3084出版社
AMER SOC MICROBIOLOGY
DOI: 10.1128/MCB.26.8.3071-3084.2006
关键词
-
资金
- NIDDK NIH HHS [DK 42394, R37 DK042394, R01 DK042394] Funding Source: Medline
NF-kappa B is critical for determining cellular sensitivity to apoptotic stimuli by regulating both mitochondrial and death receptor apoptotic pathways. The endoplasmic reticulum (ER) emerges as a new apoptotic signaling initiator. However, the mechanism by which ER stress activates NF-kappa B and its role in regulation of ER stress-induced cell death are largely unclear. Here, we report that, in response to ER stress, IKK forms a complex with IRE1 alpha through the adapter protein TRAF2. ER stress-induced NF-kappa B activation is impaired in IRE1 alpha knockdown cells and IRE1 alpha(-/-) MEFs. We found, however, that inhibiting NF-kappa B significantly decreased ER stress-induced cell death in a caspase-8-dependent manner. Gene expression analysis revealed that ER stress-induced expression of tumor necrosis factor alpha (TNF-alpha) was IRE1 alpha and NF-kappa B dependent. Blocking TNF receptor 1 signaling significantly inhibited ER stress-induced cell death. Further studies suggest that ER stress induces down-regulation of TRAF2 expression, which impairs TNF-alpha-induced activation of NF-kappa B and c-Jun N-terminal kinase and turns TNF-alpha from a weak to a powerful apoptosis inducer. Thus, ER stress induces two signals, namely TNF-alpha induction and TRAF2 down-regulation. They work in concert to amplify ER-initiated apoptotic signaling through the membrane death receptor.
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