Abstract
Human p53 protein acts as a transcription factor predominantly in a tetrameric form. Single residue changes, caused by hot-spot mutations of the TP53 gene in human cancer, transform wild-type (wt) p53 tumor suppressor proteins into potent oncoproteins - with gain-of-function, tumor-promoting activity. Oligomerization of p53 allows for a direct interplay between wt and mutant p53 proteins if both are present in the same cells – where a mutant p53's dominant-negative effect known to inactivate wt p53, co-exists with an opposite mechanism – a “dominant-positive” suppression of the mutant p53's gain-of-function activity by wt p53. In this study we determine the oligomerization efficiency of wt and mutant p53 in living cells using FRET-based assays and describe wt p53 to be more efficient than mutant p53 in entering p53 oligomers. The biased p53 oligomerization helps to interpret earlier reports of a low efficiency of the wt p53 inactivation via the dominant-negative effect, while it also implies that the “dominant-positive” effect may be more pronounced. Indeed, we show that at similar wt:mutant p53 concentrations in cells – the mutant p53 gain-of-function stimulation of gene transcription and cell migration is more efficiently inhibited than the wt p53's tumor-suppressive transactivation and suppression of cell migration. These results suggest that the frequent mutant p53 accumulation in human tumor cells does not only directly strengthen its gain-of-function activity, but also protects the oncogenic p53 mutants from the functional dominance of wt p53.
Highlights
Supplementary Figure 5: (A) H1299 cells were transfected with indicated amounts of empty vector and/or vectors encoding p53 protein variants – untagged wt or 344P with/without 273-YFP mutant
The cell migration graph shows average results with SD of area covered by cells post 18h of the wound-healing assay in 3 biological replicates of the wt p53 titration vs p53 273-Y mutant variant
Statistical significance was calculated with one-way ANOVA, Bonferroni post-test, *** p-value
Summary
Supplementary Figure 5: (A) H1299 cells were transfected with indicated amounts of empty vector (vec.) and/or vectors encoding p53 protein variants – untagged wt or 344P with/without 273-YFP mutant. Expression bar graphs show normalized averages with SD of the mRNA levels for wt p53 target genes (strongly induced: CDKN1A and MDM2; moderately induced: BCC3 and BAX) and mutant p53 target genes (PSMA2, PSMC1, RRM1, TK1, CCNA2) in 3 biological replicates of the wt p53 titration vs p53 273-Y mutant variant.
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