Noncanonical DNA Motifs as Transactivation Targets by Wild Type and Mutant p53

Jordan, Jennifer; Menéndez, Daniel; Inga, Alberto; Nourredine, Maher; Bell, Douglas A.; Resnick, Michael A.

doi:10.1371/journal.pgen.1000104

Cited by 93 publications

(163 citation statements)

References 109 publications

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“…A second p53-RE decamer is located 4 nt away and contains one mismatch in the CWWG core, making it at most a very weak contributor to p53 transactivation. Most functional p53 target genes have 0 -2-nt spacer (23,27,(43)(44)(45), and we recently demonstrated that a spacer of Ն3 nt greatly impairs p53 transactivation (26). Thus, although RE-5 fits the generally acknowledged consensus, our results demonstrate that the half-decamer is likely responsible for most of the p53-mediated transactivation at p53RE-5.…”

Section: Discussionmentioning

confidence: 43%

“…A 4-kb region surrounding the transcription start site of the human RAP80 promoter was scanned for the presence of p53 response element sequences (p53-REs). Although the commonly accepted consensus p53-RE consists of (RRRCWWGYYY followed by a 0 -13-nt spacer followed by RRRCWWGYYY) with up to approximately five mismatches, we recently established that a fully functional RE has a spacer of Յ3 nt and that a single decamer, a "noncanonical half-site" (23,25,26), could mediate transcriptional activation by p53. The CWWG core is important for p53 responsiveness, where C and G are essential and CATG is the strongest responder.…”

Section: Rap80 Is a Novel Target Of P53-dependent Transcriptionalmentioning

confidence: 99%

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A Regulatory Loop Composed of RAP80-HDM2-p53 Provides RAP80-enhanced p53 Degradation by HDM2 in Response to DNA Damage

Yan¹,

Menéndez

Xiao³

et al. 2009

Journal of Biological Chemistry

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The ubiquitin interaction motif-containing protein RAP80 plays a key role in DNA damage response signaling. Using genomic and functional analysis, we established that the expression of the RAP80 gene is regulated in a DNA damage-responsive manner by the master regulator p53. This regulation occurs at the transcriptional level through a noncanonical p53 response element in the RAP80 promoter. Although it is inducible by p53, RAP80 is also able to regulate p53 through an association with both p53 and the E3 ubiquitin ligase HDM2, providing HDM2-dependent enhancement of p53 polyubiquitination. Depletion of RAP80 by small interfering RNA stabilizes p53, which, following DNA damage, results in an increased transactivation of several p53 target genes as well as greater apoptosis. Consistent with these observations, exogenous expression of RAP80 selectively inhibits p53-dependent transactivation of target genes in an mdm2-dependent manner in MEF cells. Thus, we identify a new DNA damage-associated role for RAP80. It can function in an autoregulatory loop consisting of RAP80, HDM2, and the p53 master regulatory network, implying an important role for this loop in genome stability and oncogenesis.

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Section: Discussionmentioning

confidence: 43%

Section: Rap80 Is a Novel Target Of P53-dependent Transcriptionalmentioning

confidence: 99%

A Regulatory Loop Composed of RAP80-HDM2-p53 Provides RAP80-enhanced p53 Degradation by HDM2 in Response to DNA Damage

Yan¹,

Menéndez

Xiao³

et al. 2009

Journal of Biological Chemistry

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“…Resnick (L9) made the same observation using a diploid yeast system, expressing p53 under the control of a galactose-dependent promoter and a reporter gene driven by p53RE. 3 In this system, increasing the number of spacer nucleotides resulted in a drastic decrease of both p53 transcriptional and DNA binding activities. He also showed that conservation of the p53RE core motif (CWWG) is the main requirement for the definition of a half site, the CATG motif appearing to be the most efficient one.…”

Section: Modulation Of P53 Activitymentioning

confidence: 85%

Understanding wild-type and mutant p53 activities in human cancer: new landmarks on the way to targeted therapies

et al. 2010

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Three decades of p53 research have led to many advances in understanding the basic biology of normal and cancer cells. Nonetheless, the detailed functions of p53 in normal cells, and even more so in cancer cells, remain obscure. A major breakthrough is the realization that mutant p53 has a life of its own: it contributes to cancer not only through loss of activity, but also through gain of specific 'mutant functions'. This new focus on mutant p53 is the rationale behind the meeting series dedicated to advances on mutant p53 biology. This review provides an overview of results presented at the Fourth International Workshop on Mutant p53, held in Akko, Israel in March 2009. New roles and functions of p53 relevant for tumor suppressions were presented, including the regulation of microRNAs networks, the modulation of cell-stroma interactions and the induction of senescence. A main focus of the meeting was the rapidly growing body of knowledge on autonomous properties of mutant p53 and on their oncogenic 'gain of function' impact. Importantly, the meeting highlighted that, 30 years after p53 discovery, research on mutant p53 is entering the clinical and translational era. Two major steps forward in this respect are a better understanding of the active mechanism of small drugs targeting mutant p53 in tumor cells and an improved definition of the prognostic and predictive value of mutant p53 in human cancer.

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“…In fact, recent work has shown that tetrameric p53 is capable of binding to half-and even three quarterconsensus sites, such as those comprising the PIDD and Apaf-1 response elements (Jordan et al 2008). Using a Saccharomyces cerevisiae model system, one study found as much as a 1000-fold difference in transactivation by p53 for its weaker versus its stronger sites, with this difference being largely dependent on the central sequence element in the p53 RE (Inga et al 2002).…”

Section: P53 Response Elementsmentioning

confidence: 99%