Nina Rökaeus scite author profile

Reactivation of mutant p53 in human tumor cells should induce cell death by apoptosis and thus eliminate the tumor. Several small molecules that reactivate mutant p53 have been identified. Here we show that STIMA-1, a low molecular weight compound with some structural similarities to the previously identified molecule CP-31398, can stimulate mutant p53 DNA binding in vitro and induce expression of p53 target proteins and trigger apoptosis in mutant p53-expressing human tumor cells. Human diploid fibroblasts are significantly more resistant to STIMA-1 than mutant or wild type p53-carrying tumor cells. STIMA-1 may provide new insights into possible mechanisms of mutant p53 reactivation and thus facilitate the development of novel anticancer drugs that target mutant p53-carrying tumors.

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PRIMA-1MET/APR-246 targets mutant forms of p53 family members p63 and p73

Rökaeus

Shen

Eckhardt

et al. 2010

Oncogene

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PRIMA-1MET induces nucleolar accumulation of mutant p53 and PML nuclear body-associated proteins

et al. 2006

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We have previously identified PRIMA-1, a low molecular weight compound that restores the transcriptional transactivation function to mutant p53 and induction of apoptosis. To explore the molecular mechanism for PRIMA-1-induced mutant p53-dependent apoptosis, we examined the intracellular distribution of mutant p53 upon treatment with PRIMA-1 MET by immunofluorescence staining. We found that PRIMA-1 MET induced nucleolar translocation of mutant p53 and the promyelocytic leukemia (PML) nuclear body-associated proteins PML, CBP and Hsp70. Levels of Hsp70 were significantly enhanced by PRIMA-1 MET treatment. PRIMA-Dead, a compound structurally related to PRIMA-1 but unable to induce mutant p53-dependent apoptosis, failed to induce nucleolar translocation of mutant p53. Our results suggest that redistribution of mutant p53 to nucleoli plays a role in PRIMA-1-induced apoptosis. Oncogene (2007) 26, 982-992.

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Nina Rökaeus

Mutant p53 targeting by the low molecular weight compound STIMA‐1

PRIMA-1MET/APR-246 targets mutant forms of p53 family members p63 and p73

PRIMA-1MET induces nucleolar accumulation of mutant p53 and PML nuclear body-associated proteins

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