Gene/Protein
Disease
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Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
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Drug
Enzyme
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Target Concepts:
Gene/Protein
Disease
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Enzyme
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Query: UNIPROT:P04040 (
Catalase
)
3,577
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
E2F1
and FOXO3 are two transcription factors that have been shown to participate in cellular senescence. Previous report reveals that
E2F1
enhanced cellular senescence in human fibroblast cells, while FOXO transcription factors play against senescence by regulation reactive oxygen species scavenging proteins. However, their functional interplay has been unclear. Here we use
E2F1
knock-out murine Embryonic fibroblasts (MEFs), knockdown RNAi constructs, and ectopic expression of
E2F1
to show that it functions by negatively regulating FOXO3.
E2F1
attenuates FOXO3-mediated expression of MnSOD and
Catalase
without affecting FOXO3 protein stability, subcellular localization, or phosphorylation by Akt. We mapped the interaction between
E2F1
and FOXO3 to a region including the DNA binding domain of
E2F1
and the C-terminal transcription-activation domain of FOXO3. We propose that
E2F1
inhibits FOXO3-dependent transcription by directly binding FOXO3 in the nucleus and preventing activation of its target genes. Moreover, knockdown of the Caenorhabditis elegans
E2F1
ortholog efl-1 significantly extends lifespan in a manner that requires the activity of the C. elegans FOXO gene daf-16. We conclude that there is an evolutionarily conserved signaling connection between
E2F1
and FOXO3, which regulates cellular senescence and aging by regulating the activity of FOXO3. We speculate that drugs and/or therapies that inhibit this physical interaction might be good candidates for reducing cellular senescence and increasing longevity.
...
PMID:E2F transcription factor 1 regulates cellular and organismal senescence by inhibiting Forkhead box O transcription factors. 2534 4
