Participation of the Calcium/Calmodulin-dependent Kinases in Hydrogen Peroxide-induced IκB Phosphorylation in Human T Lymphocytes

NF- Kappa B is an important transcription factor that has a role in a variety of responses such as inflammation, oncogenesis, apoptosis, and viral replication. Oxidative stress is well known to induce the activation of NF- Kappa B. Cells can be exposed to either endogenously produced oxidants or oxi...

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Veröffentlicht in:The Journal of biological chemistry 2002-08, Vol.277 (34), p.30469-30476
Hauptverfasser: Howe, Christopher J., LaHair, Michelle M., Maxwell, Jill A., Lee, John T., Robinson, Penni J., Rodriguez-Mora, Oswaldo, McCubrey, James A., Franklin, Richard A.
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Sprache:eng
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Zusammenfassung:NF- Kappa B is an important transcription factor that has a role in a variety of responses such as inflammation, oncogenesis, apoptosis, and viral replication. Oxidative stress is well known to induce the activation of NF- Kappa B. Cells can be exposed to either endogenously produced oxidants or oxidants produced by surrounding cells. In addition, ischemia reperfusion and certain cancer therapies such as chemotherapy and photodynamic therapy are thought to result in oxygen radical production. Because of the important role that NF- Kappa B has in multiple responses, it is critical to determine the mechanisms by which oxidative stress induces NF- Kappa B activity. We report that the calmodulin antagonist W-7 and the calcium/calmodulin-dependent (CaM) kinase inhibitors KN-93 and K252a, can block oxidative stress-induced I Kappa B phosphorylation in Jurkat T lymphocytes. Furthermore, KN-93 but not KN-92 can block hydrogen peroxide-induced Akt and IKK phosphorylation. In addition, we found that expression of a kinase-dead CaM-KIV construct in two cell lines inhibits I Kappa B phosphorylation or degradation and that expression of CaM-KIV augments hydrogen peroxide-induced I Kappa B phosphorylation and degradation. Although the CaM kinases appear to be required for this response, increases in intracellular calcium do not appear to be required. These results identify the CaM kinases as potential targets that can be used to minimize NF- Kappa B activation in response to oxidative stress.
ISSN:0021-9258
DOI:10.1074/jbc.M205036200