HOW SELENIUM MODIFIES CROSS-TALK BETWEEN THE PIKK FAMILY AND INSIGHTS ON THE REGULATION OF DNA-PKcs

dc.contributor.advisorCheng, Wen-Hsingen_US
dc.contributor.authorRocourt, Carolineen_US
dc.contributor.departmentNutritionen_US
dc.contributor.publisherDigital Repository at the University of Marylanden_US
dc.contributor.publisherUniversity of Maryland (College Park, Md.)en_US
dc.date.accessioned2010-02-19T07:09:54Z
dc.date.available2010-02-19T07:09:54Z
dc.date.issued2009en_US
dc.description.abstractWe recently found that ATM is required for a selenium-induced senescence response in non-cancerous cells. We hypothesize the selenium-induced DNA damage response modifies ATM and DNA-PKcs cross-talk. Phospho-specific antibodies against ATM and DNA-PKcs were used to follow the phosphorylation events after selenium treatment in normal human cells and two human cancer cell lines. Results from immunofluorescence analysis showed that selenium treatment induces hyperphosphorylation of DNA-PKcs at T2647 and S2056 in non-cancerous MRC-5 cells but not in U-2 OS cancer cells. Further studies in MRC-5 cells treated with an ATM kinase inhibitor, KU 55933, showed attenuation of the selenium-induced DNA-PKcs phosphorylation at both foci, whereas pre-treatment with a DNA-PKcs kinase inhibitor, NU 7026, does not prevent ATM phosphorylation at S1981, an event leading to ATM pathway activation. These results give evidence that DNA-PKcs and ATM have a cooperative role in the DNA damage response pathway.en_US
dc.identifier.urihttp://hdl.handle.net/1903/10009
dc.subject.pqcontrolledHealth Sciences, Nutritionen_US
dc.subject.pqcontrolledBiology, Molecularen_US
dc.subject.pqcontrolledAgriculture, Animal Culture and Nutritionen_US
dc.subject.pquncontrolledDNA damage responseen_US
dc.subject.pquncontrolledPIKK familyen_US
dc.subject.pquncontrolledseleniumen_US
dc.subject.pquncontrolledsupranutritionalen_US
dc.titleHOW SELENIUM MODIFIES CROSS-TALK BETWEEN THE PIKK FAMILY AND INSIGHTS ON THE REGULATION OF DNA-PKcsen_US
dc.typeThesisen_US

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