Phosphorylation of Nrf2 at Ser40 by Protein Kinase C in Response to Antioxidants Leads to the Release of Nrf2 from INrf2, but Is Not Required for Nrf2 Stabilization/Accumulation in the Nucleus and Transcriptional Activation of Antioxidant Response Element-mediated NAD(P)H:Quinone Oxidoreductase-1 Gene Expression

Journal of Biological Chemistry

Volumn 278, Issue 45, 2003, Pages 44675-44682

  Bloom, David A ^b   Jaiswal, Anil K ^a  

^a BAYLOR COLLEGE OF MEDICINE   (United States)

^b NONE

Author keywords

[No Author keywords available]

Indexed keywords

ANTIOXIDANTS; CHEMICAL ACTIVATION; GENES; KETONES; PHOSPHORUS COMPOUNDS;

TRANSCRIPTION FACTORS;

ENZYMES;

2 (2 AMINO 3 METHOXYPHENYL)CHROMONE; ANTIOXIDANT; CALPHOSTIN C; GENISTEIN; LUCIFERASE; MITOGEN ACTIVATED PROTEIN KINASE; MITOGEN ACTIVATED PROTEIN KINASE INHIBITOR; PEPTIDE; PHOSPHATIDYLINOSITOL 3 KINASE; PHOSPHATIDYLINOSITOL 3 KINASE INHIBITOR; PROTEASOME; PROTEIN; PROTEIN INRF2; PROTEIN KINASE C; PROTEIN KINASE C INHIBITOR; PROTEIN NEH2; PROTEIN TYROSINE KINASE; PROTEIN TYROSINE KINASE INHIBITOR; REDUCED NICOTINAMIDE ADENINE DINUCLEOTIDE (PHOSPHATE) DEHYDROGENASE (QUINONE); SB 23580; SERINE; STAUROSPORINE; SYNAPTOPHYSIN; TERT BUTYLHYDROQUINONE; TRANSCRIPTION FACTOR NF E2; TRANSCRIPTION FACTOR NRF2; UNCLASSIFIED DRUG; WORTMANNIN; DNA BINDING PROTEIN; ENZYME INHIBITOR; LEUCINE ZIPPER PROTEIN; NAPHTHALENE DERIVATIVE; NFE2L2 PROTEIN, HUMAN; NQO1 PROTEIN, HUMAN; TRANSACTIVATOR PROTEIN;

ANIMAL CELL; ANTIOXIDANT RESPONSIVE ELEMENT; ARTICLE; CELL NUCLEUS; CELL STRAIN HEPG2; CONTROLLED STUDY; DNA RESPONSIVE ELEMENT; GENE ACTIVATION; GENE EXPRESSION; GENE REPRESSION; HUMAN; HUMAN CELL; INTRACELLULAR TRANSPORT; MOUSE; NONHUMAN; NUCLEOTIDE SEQUENCE; OXIDATIVE STRESS; PRIORITY JOURNAL; PROTEIN BINDING; PROTEIN DEGRADATION; PROTEIN DOMAIN; PROTEIN FUNCTION; PROTEIN INDUCTION; PROTEIN INTERACTION; PROTEIN LOCALIZATION; PROTEIN PHOSPHORYLATION; PROTEIN SECRETION; PROTEIN STABILITY; PROTEIN TARGETING; REGULATORY MECHANISM; REPORTER GENE; SPECIES; TRANSCRIPTION INITIATION; BINDING SITE; CELL LINE; CHEMISTRY; DRUG ANTAGONISM; DRUG EFFECT; ENZYME LINKED IMMUNOSORBENT ASSAY; FLUORESCENT ANTIBODY TECHNIQUE; GENETIC TRANSCRIPTION; GENETIC TRANSFECTION; GENETICS; METABOLISM; PHOSPHORYLATION; PHYSIOLOGY; SITE DIRECTED MUTAGENESIS; STRUCTURE ACTIVITY RELATION; WESTERN BLOTTING;

ANIMALIA;

ANTIOXIDANTS; BINDING SITES; BLOTTING, WESTERN; CELL LINE; CELL NUCLEUS; DNA-BINDING PROTEINS; ENZYME INHIBITORS; FLUORESCENT ANTIBODY TECHNIQUE; GENE EXPRESSION; HUMANS; IMMUNOSORBENT TECHNIQUES; LEUCINE ZIPPERS; MUTAGENESIS, SITE-DIRECTED; NAD(P)H DEHYDROGENASE (QUINONE); NAPHTHALENES; NF-E2-RELATED FACTOR 2; PHOSPHORYLATION; PROTEIN KINASE C; RESPONSE ELEMENTS; SERINE; STAUROSPORINE; STRUCTURE-ACTIVITY RELATIONSHIP; TRANS-ACTIVATORS; TRANSCRIPTION, GENETIC; TRANSFECTION;

EID: 0242666198     PISSN: 00219258     EISSN: None     Source Type: Journal    
DOI: 10.1074/jbc.M307633200     Document Type: Article

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