2004
DOI: 10.1074/jbc.m403321200
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Serine 18 Phosphorylation of RAX, the PKR Activator, Is Required for PKR Activation and Consequent Translation Inhibition

Abstract: It is now apparent that the double-stranded (ds)RNAdependent protein kinase, PKR, is a regulator of diverse cellular responses to stress. Recently, the murine dsRNA-binding protein RAX and its human ortholog PACT were identified as cellular activators of PKR. Previous reports demonstrate that following stress, RAX/ PACT associates with and activates PKR resulting in eIF2␣ phosphorylation, consequent translation inhibition, and cell death via apoptosis. Although RAX/PACT is phosphorylated during stress, any reg… Show more

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Cited by 56 publications
(65 citation statements)
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“…Analysis of autopsied brain tissues from Alzheimer's disease patients showed accumulation of activated PKR in nuclei. Many of the stimuli that trigger PKR-dependent apoptosis in the absence of viral infection rely on PACT/RAX activation; PACT/RAX mediates PKR activation and subsequent apoptosis in response not only to cytokines and serum withdrawal but also to chemotherapy, ethanol, and viral infection (20). Alterations in levels of any of the array of PKR viral (and cellular) inhibitors (see the next section) also have a profound impact on apoptosis induction (64,351).…”
Section: Pkr Mediates Apoptosis Induced By Different Stimulimentioning
confidence: 99%
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“…Analysis of autopsied brain tissues from Alzheimer's disease patients showed accumulation of activated PKR in nuclei. Many of the stimuli that trigger PKR-dependent apoptosis in the absence of viral infection rely on PACT/RAX activation; PACT/RAX mediates PKR activation and subsequent apoptosis in response not only to cytokines and serum withdrawal but also to chemotherapy, ethanol, and viral infection (20). Alterations in levels of any of the array of PKR viral (and cellular) inhibitors (see the next section) also have a profound impact on apoptosis induction (64,351).…”
Section: Pkr Mediates Apoptosis Induced By Different Stimulimentioning
confidence: 99%
“…Although in vitro analysis shows that domain 3 of PACT is sufficient to activate PKR, all three domains are needed for efficient PKR activation in vivo (282). As mentioned above, different stresses trigger PACT phosphorylation (20), and only then does PACT bind and activate PKR (165,278,282). PACT might thus be involved in PKR activation in uninfected cells.…”
Section: Modulation By Cell Proteinsmentioning
confidence: 99%
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“…[84][85][86][87] PACT/RAX is member of the DRBD family, as described earlier, and has been shown to induce apoptosis following activation of PKR, in response to stress such as serum starvation and arsenite treatment. 31,88 Similar studies aimed at seeking novel PKRinteracting proteins lead to the isolation of nucleophosmin (NPM), a protein often expressed at elevated levels in tumors. 89 NPM was shown to bind to PKR and inhibit its activity, thus preventing apoptotic responses and potentially promoting sporadic malignancies.…”
Section: Pkr and The Control Of Translationmentioning
confidence: 99%
“…We also investigated the role of the pro-survival Akt pathway because of data suggesting that TNF-a -induced PKR activation led to Akt phosphorylation only in PKR +/+ cells. 8 PKR +/+ MEFs exhibited dose-and time-dependent increases in phosphorylation of Akt after radiation, whereas PKR -/-MEFs did not show Akt phosphorylation ( Fig. 5A and B).…”
Section: Irradiation Leads To Nf-kb Activation In Pkrmentioning
confidence: 99%