| Literature DB >> 30602570 |
Luciana P Rangel1,2, Giulia D S Ferretti2,3, Caroline L Costa2,3, Sarah M M V Andrade4, Renato S Carvalho4, Danielly C F Costa2,5, Jerson L Silva6,3.
Abstract
p53 mutants can form amyloid-like structures that accumulate in cells. p53 reactivation with induction of massive apoptosis-1 (PRIMA-1) and its primary active metabolite, 2-methylene-3-quinuclidinone (MQ), can restore unfolded p53 mutants to a native conformation that induces apoptosis and activates several p53 target genes. However, whether PRIMA-1 can clear p53 aggregates is unclear. In this study, we investigated whether PRIMA-1 can restore aggregated mutant p53 to a native form. We observed that the p53 mutant protein is more sensitive to both PRIMA-1 and MQ aggregation inhibition than WT p53. The results of anti-amyloid oligomer antibody assays revealed that PRIMA-1 reverses mutant p53 aggregate accumulation in cancer cells. Size-exclusion chromatography of the lysates from mutant p53-containing breast cancer and ovarian cell lines confirmed that PRIMA-1 substantially decreases p53 aggregates. We also show that MDA-MB-231 cell lysates can "seed" aggregation of the central core domain of recombinant WT p53, corroborating the prion-like behavior of mutant p53. We also noted that this aggregation effect was inhibited by MQ and PRIMA-1. This study provides the first demonstration that PRIMA-1 can rescue amyloid-state p53 mutants, a strategy that could be further explored as a cancer treatment.Entities:
Keywords: amyloid; anticancer drug; p53; protein aggregation; protein misfolding
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Year: 2019 PMID: 30602570 PMCID: PMC6416452 DOI: 10.1074/jbc.RA118.004671
Source DB: PubMed Journal: J Biol Chem ISSN: 0021-9258 Impact factor: 5.157