Expression of p53 and p53/47 are controlled by alternative mechanisms of messenger RNA translation initiation

Candeias, Marco M.; Powell, Darren; Roubalová, Eva; Apcher, Sébastien; Bourougaa, Karima; Vojtesek, Borek; Bruzzoni‐Giovanelli, Heriberto; Fåhræus, Robin

doi:10.1038/sj.onc.1209996

Cited by 96 publications

(148 citation statements)

References 42 publications

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“…p53 isoforms gain functions V Olivares-Illana and R Fåhraeus the p53 response (Candeias et al, 2006). Further work showed that suppression of PERK activity, through overexpression of either a dominant-negative PERK or small interfering RNA, resulted in the suppression of p53/47 expression, indicating that PERK is the signal transducer between the ER and p53/47 expression ( Figure 2) (Bourougaa et al, 2010).…”

Section: Introductionmentioning

confidence: 99%

“…In fact, p53/47 was discovered due to the fact Mdm2 can promote the initiation of translation of both p53 and p53/47, but only targets the former for degradation (Yin et al, 2002). Later work showed that translation initiation of p53 and p53/47 can be controlled by separate and, to some extent, competing mechanisms of translation, so that suppression of capdependent translation of p53 results in an increase in the synthesis of p53/47 (Candeias et al, 2006). Insertion of an open-reading frame followed by a hairpin structure in the 5 0 -untranslated region of p53 resulted in an increase in p53/47 synthesis and a decrease in p53, indicating that cap-independent mechanisms of initiation control p53/47 translation via an internal ribosome entry site (IRES) structure located in the region of þ 1 to þ 120 of p53.…”

Section: Introductionmentioning

confidence: 99%

“…Insertion of an open-reading frame followed by a hairpin structure in the 5 0 -untranslated region of p53 resulted in an increase in p53/47 synthesis and a decrease in p53, indicating that cap-independent mechanisms of initiation control p53/47 translation via an internal ribosome entry site (IRES) structure located in the region of þ 1 to þ 120 of p53. Hence, the coding region of p53 serves as IRES for p53/47 (Candeias et al, 2006;Ray et al, 2006;Grover et al, 2009). It has also been shown that p53/47 could be generated by alternative splicing (Ghosh et al, 2004), but it should be a rare event as the full-length p53 mRNA was evident after 20 quantitative PCR cycles, whereas the p53/47 message required 40 quantitative PCR cycles, which represents approximately 2 Â 10 20 times less amount of p53/47 mRNA.…”

Section: Introductionmentioning

confidence: 99%

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p53 isoforms gain functions

Olivares‐Illana

Fåhræus

2010

Oncogene

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Many different cell stress pathways converge on p53 to induce a number of distinct cell biological responses such as G1 or G2 arrest, senescence or apoptosis. One of the outstanding questions with regard to p53 is how the cells can differentiate between different stresses so that p53 activation leads to the correct response. It has been known for some time that the p53 gene expresses isoforms that carry unique domains and properties, and more recent works have started to reveal some of their functions. The alternative mRNA translation product p53/47, which lacks the first 40 codons, including the first of p53's two trans-activation domains, is being linked to endoplasmic reticulum stress and the unfolded protein response to which it causes a specific G2 arrest. On the other hand, p53 itself induces G1 arrest and has no effect on the G2. The two isoforms D133p53, which lacks the first 133 amino acids, and p53b, which carries an alternative C-terminus, are derived from alternative promoter usage or splicing, respectively, and are together implied in controlling cellular senescence. Hence, through different mechanisms of gene expression control, alternative levels of p53 isoforms help the cell to differentiate between p53 activation and the response to diverse stresses. This holds promise to a better understanding of how upstream and downstream p53 pathways have evolved relative to specific p53 domains.

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Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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p53 isoforms gain functions

Olivares‐Illana

Fåhræus

2010

Oncogene

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“…The cDNA of human Mdm2 was kindly provided by N. Varin-Blank (Institut Cochin), and the p53 plasmid was described previously (34). Various tagged forms of ␤-arr2 have been described previously (16).…”

Section: Methodsmentioning

confidence: 99%

β-arrestin 2 oligomerization controls the Mdm2-dependent inhibition of p53

Boularan

Scott

Bourougaa

et al. 2007

Proc. Natl. Acad. Sci. U.S.A.

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␤-arrestins (␤-arrs), two ubiquitous proteins involved in serpentine heptahelical receptor regulation and signaling, form constitutive homo-and heterooligomers stabilized by inositol 1,2,3,4,5,6-hexakisphosphate (IP6). Monomeric ␤-arrs are believed to interact with receptors after agonist activation, and therefore, ␤-arr oligomers have been proposed to represent a resting biologically inactive state. In contrast to this, we report here that the interaction with and subsequent titration out of the nucleus of the protooncogene Mdm2 specifically require ␤-arr2 oligomers together with the previously characterized nucleocytoplasmic shuttling of ␤-arr2. Mutation of the IP6-binding sites impair oligomerization, reduce interaction with Mdm2, and inhibit p53-dependent antiproliferative effects of ␤-arr2, whereas the competence for receptor regulation and signaling is maintained. These observations suggest that the intracellular concentration of ␤-arr2 oligomers might control cell survival and proliferation. bioluminescence resonance energy transfer ͉ FRET ͉ nucleocytoplasmic shuttling ͉ ubiquitination

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“…Several isoforms of p53 have been identified (Courtois et al, 2002;Candeias et al, 2006;Grover et al, 2009;Marcel and Hainaut, 2009), and point mutations influencing the functionality of p53 were elucidated and mimicked in vivo (de Vries et al, 2002;Wijnhoven et al, 2005;Hoogervorst et al, 2005a;Iwakuma and Lozano, 2007;Heinlein et al, 2008). The p53 gene is the most frequently mutated gene in cancer and analysis of many different human tumor types have shown a high prevalence of missense mutations located primarily in the central DNA-binding domain (Levine, 1997).…”

Section: Introductionmentioning

confidence: 99%

Genotoxic exposure: novel cause of selection for a functional ΔN-p53 isoform

Melis¹,

Hoogervorst²,

Oostrom³

et al. 2010

Oncogene

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The p53 gene is frequently mutated in cancers and it is vital for cell cycle control, homeostasis and carcinogenesis. We describe a novel p53 mutational spectrum, different to those generally observed in human and murine tumors. Our study shows a high prevalence of nonsense mutations in the p53 N terminus of 2-acetylaminofluorene (2-AAF)-induced urinary bladder tumors. These nonsense mutations forced downstream translation initiation at codon 41 of Trp53, resulting in the aberrant expression of the p53 isoform DN-p53 (or p44). We propose a novel mechanism for the origination and the selection for this isoform. We show that chemical exposure can act as a novel cause of selection for this truncated protein. In addition, our data suggest that the occurrence of DN-p53 accounts, at least in mice, for a cancer phenotype. We also show that gene expression profiles of embryonic stem (ES) cells carrying the DN-p53 isoform in a p53-null background are divergent from p53 knockout ES cells, and therefore postulate that DN-p53 itself has functional transcriptional properties.

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Expression of p53 and p53/47 are controlled by alternative mechanisms of messenger RNA translation initiation

Cited by 96 publications

References 42 publications

p53 isoforms gain functions

p53 isoforms gain functions

β-arrestin 2 oligomerization controls the Mdm2-dependent inhibition of p53

Genotoxic exposure: novel cause of selection for a functional ΔN-p53 isoform

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