hnRNP K: an HDM2 target and transcriptional coactivator of p53 in response to DNA damage
- PMID: 16360036
- DOI: 10.1016/j.cell.2005.09.032
hnRNP K: an HDM2 target and transcriptional coactivator of p53 in response to DNA damage
Retraction in
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Retraction notice to: hnRNP K: An HDM2 Target and Transcriptional Coactivator of p53 in Response to DNA Damage.Cell. 2024 Oct 31;187(22):6413. doi: 10.1016/j.cell.2024.10.008. Epub 2024 Oct 9. Cell. 2024. PMID: 39389056 No abstract available.
Abstract
In response to DNA damage, mammalian cells trigger the p53-dependent transcriptional induction of factors that regulate DNA repair, cell-cycle progression, or cell survival. Through differential proteomics, we identify heterogeneous nuclear ribonucleoprotein K (hnRNP K) as being rapidly induced by DNA damage in a manner that requires the DNA-damage signaling kinases ATM or ATR. Induction of hnRNP K ensues through the inhibition of its ubiquitin-dependent proteasomal degradation mediated by the ubiquitin E3 ligase HDM2/MDM2. Strikingly, hnRNP K depletion abrogates transcriptional induction of p53 target genes and causes defects in DNA-damage-induced cell-cycle-checkpoint arrests. Furthermore, in response to DNA damage, p53 and hnRNP K are recruited to the promoters of p53-responsive genes in a mutually dependent manner. These findings establish hnRNP K as a new HDM2 target and show that, by serving as a cofactor for p53, hnRNP K plays key roles in coordinating transcriptional responses to DNA damage.
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