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Acetylation halts missense mutant p53 aggregation and rescues tumor suppression in non-small cell lung cancers.

iScience | 2023

TP53 mutations are ubiquitous with tumorigenesis in non-small cell lung cancers (NSCLC). By analyzing the TCGA database, we reported that TP53 missense mutations are correlated with chromosomal instability and tumor mutation burden in NSCLC. The inability of wild-type nor mutant p53 expression can't predict survival in lung cancer cohorts, however, an examination of primary NSCLC tissues found that acetylated p53 did yield an association with improved survival outcomes. Molecularly, we demonstrated that acetylation drove the ubiquitination and degradation of mutant p53 but enhanced stability of wild-type p53. Moreover, acetylation of a missense p53 mutation prevented the gain of oncogenic function observed in typical TP53 mutant-expressing cells and enhanced tumor suppressor functions. Consequently, acetylation inducer targeting of missense mutant p53 may be a viable therapeutic goal for NSCLC treatment and may improve the accuracy of current efforts to utilize p53 mutations in a prognostic manner.

Pubmed ID: 37534137 RIS Download

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This is a list of tools and resources that we have found mentioned in this publication.


Peroxidase AffiniPure Goat Anti-Mouse IgG, light chain specific (antibody)

RRID:AB_2338512

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p53 (acetyl K373) antibody [EP356(2)AY] (antibody)

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p53 (acetyl K382) antibody [EPR358(2)] (antibody)

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acetyl Lysine antibody - ChIP Grade (antibody)

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GAPDH antibody (antibody)

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HA-Tag (26D11) Mouse Antibody (antibody)

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ModFit LT (data processing software)

RRID:SCR_016106

Modeling software for flow cytometry histograms. Models for cell-tracking dye studies and synchronized cell lines are built right into the software.

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