2018
DOI: 10.1186/s40170-018-0191-6
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p53-mediated adaptation to serine starvation is retained by a common tumour-derived mutant

Abstract: BackgroundIn response to oncogenic stress, the tumour suppressor protein p53 can induce the elimination of cells through induction of cell death or senescence, helping to restrain malignant progression. Conversely, under nutrient stress, p53 can protect cells by supporting metabolic adaptation. Many cancers express mutant p53 proteins that have lost the cell-elimination properties of wild-type p53. However, a previous report showed that a tumour-derived mutant can retain the ability to support cells under glut… Show more

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Cited by 42 publications
(37 citation statements)
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“…This leads to the interesting possibility that expression of point mutations that selectively retain wild-type p53 survival functions would be selected more strongly during tumour evolution than mutations that abolish p53 entirely. In support of this suggestion, patients carrying tumours with R248 p53 mutants show a particularly poor survival rate (Xu et al, 2014; Humpton et al, 2018), even compared to patients with tumours harbouring other common p53 mutations.…”
mentioning
confidence: 81%
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“…This leads to the interesting possibility that expression of point mutations that selectively retain wild-type p53 survival functions would be selected more strongly during tumour evolution than mutations that abolish p53 entirely. In support of this suggestion, patients carrying tumours with R248 p53 mutants show a particularly poor survival rate (Xu et al, 2014; Humpton et al, 2018), even compared to patients with tumours harbouring other common p53 mutations.…”
mentioning
confidence: 81%
“…Mutant p53 can also promote the mevalonate pathway, so allowing cells to survive under conditions of matrix detachment (Freed-Pastor et al, 2012). Intriguingly, some tumour-associated p53 mutants show selective retention of wild-type functions that contribute to survival under nutrient and oxidative stress (Tran et al, 2017; Humpton et al, 2018). Maintenance of both p21 and MDM2 expression by the hotspot p53 mutant R248, for example, results in an ability to survive glutamine and serine starvation, although this p53 mutant is not able to induce cell death or senescence.…”
mentioning
confidence: 99%
“…For all LC/MS samples, metabolite analysis was performed as described previously (60). Briefly, a Q Exactive Orbitrap mass spectrometer (Thermo Fisher Scientific) was used together with a Thermo Ultimate 3000 HPLC system to analyze prepared samples.…”
Section: Labeled Glucose and Glutamine Metabolomics (Lc/ms)mentioning
confidence: 99%
“…In this context, the loss of p53 function in tumour cells can make these cells more vulnerable to certain types of metabolic stress (Labuschagne et al, 2018;Lacroix et al, 2019). Many cancers express high levels of point-mutated versions of p53 that generally lose the ability to inhibit cell growth, but in some cases retain survival functions and acquire neomorphic oncogenic activity (Freed-Pastor and Prives, 2012;Humpton et al, 2018;Kim and Lozano, 2018;Tran et al, 2017).…”
Section: Introductionmentioning
confidence: 99%