Recognition of RNA by the p53 tumor suppressor protein in the yeast three-hybrid system

Riley, Kasandra; Cassiday, Laura A.; Kumar, Akash; Maher, L. James

doi:10.1261/rna.2286706

Cited by 22 publications

(35 citation statements)

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“…Perhaps p53 posttranslational modifications prevent p53-RNA interactions in vivo. Together with other recent results [6,7], this work illuminates a historically mysterious aspect of p53 biology. The physiological significance of RNA binding by p53 remains obscure [4].…”

Section: Rna Co-immunoprecipitation After Clipsupporting

confidence: 71%

“…This RNA contamination can easily be misinterpreted as evidence for specific p53-RNA interactions. Whereas unmodified or partially post-translationally modified p53 proteins from E. coli [19], yeast [6], insect cells [7,13,[16][17][18], or reticulocyte lysate [16][17][18] are prone to nonspecific RNA binding, p53 protein is not complexed with RNA when purified from the tested human cells. Perhaps p53 posttranslational modifications prevent p53-RNA interactions in vivo.…”

Section: Rna Co-immunoprecipitation After Clipmentioning

confidence: 99%

“…1A; [4]). Although many RNAbinding proteins are characterized by RNA-recognition motifs (RRMs; [5]), the interaction between p53 and RNA involves the C-terminal 30 amino acids of p53 [6,7], which do not form a RRM but are disordered in solution [7,8] and do not reorganize upon RNA binding [7,9]. p53, like the HIV-1 nucleocapsid protein, has been termed an RNA chaperone [10] that may facilitate RNA folding [11] without ATP hydrolysis [11][12][13].…”

Section: Introductionmentioning

confidence: 99%

“…Similarly, Galy et al reported that recombinant p53 can bind the 5'-UTR of the FGF-2 mRNA [18]. In contrast, reports of p53 RNA-RNA annealing activity [13] and sequence-nonspecific RNA binding [4,6,7,19] suggested that p53 binds RNA promiscuously. Acetylation of four p53 C-terminal lysine residues eliminates detectable RNA binding in vitro [7], as it does for sequence-nonspecific DNA binding [8].…”

Section: Introductionmentioning

confidence: 99%

“…Our previous studies of RNA binding by p53 in yeast and in vitro demonstrated that p53 with incomplete post-translational modifications binds RNA without apparent sequence-or structure-specificity [4,6,7]. It is possible that a partially-modified form of p53 could exist in vivo with one or more specific RNA partners.…”

Section: Introductionmentioning

confidence: 99%

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Analysis of p53–RNA interactions in cultured human cells

Riley

Maher

2007

Biochemical and Biophysical Research Communications

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Tumor suppressor p53 is a well-characterized transcription factor that binds DNA. More enigmatic are the RNA-binding properties of p53 and their physiological relevance. We used three sensitive co-immunoprecipitation methods in an attempt to detect RNAs that tightly associate with p53 in cultured human cells. Although recombinant p53 protein binds RNA in a sequence-nonspecific mode, we do not detect specific in vivo RNA binding by p53. These results suggest that RNA binding is prevented by post-translational p53 modifications. A ribonucleoprotein (not p53) is purified by multiple IgG monoclonal antibodies (including anti-p53 antibodies) from both p53 +/+ and p53 null cells. Caution is therefore required in interpreting RNA co-immunoprecipitation experiments. Though not formally excluded, these results do not support models in which p53 binds specific RNA partners in vivo.

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Section: Rna Co-immunoprecipitation After Clipsupporting

confidence: 71%

Section: Rna Co-immunoprecipitation After Clipmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Analysis of p53–RNA interactions in cultured human cells

Riley

Maher

2007

Biochemical and Biophysical Research Communications

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Two‐ and Three‐Hybrid Systems

Gestwicki

Kumar

2008

Wiley Encyclopedia of Chemical Biology

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One goal of chemical biology is to document and understand the macromolecular interactions that take place in the cell. In this review, we discuss the classic yeast two‐hybrid method (and its derivatives) and how this method continues to provide insight into the number of protein–protein partnerships in a cell. In turn, these platforms have been adapted to explore a variety of interactions, such as those between proteins and small molecules. These systems collectively are called three‐hybrid assays, and they provide new opportunities for the discovery of potential binding pairs. However, two‐ and three‐hybrid assays also have significant disadvantages, such as incomplete coverage and high rates of false positives. With these issues in mind, we discuss emerging ways of minimizing the impact of these limitations using microarrays and mass spectrometry. Finally, chemical probes related to the three‐hybrid concept are going beyond observation and providing active, rational control over individual protein–protein contacts. In these systems, bifunctional compounds are used to homo‐ or heterodimerize target proteins reversibly, thus altering their colocalization. By purposefully controlling protein–protein contacts, these chemical dimerization methods have progressed beyond observation and towards synthetic manipulation of protein function.

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Regulatory roles of tumor‐suppressor proteins and noncoding RNA in cancer and normal cell functions

Garen

2007

Intl Journal of Cancer

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We describe a mechanism for reversible regulation of gene transcription, mediated by a family of tumor-suppressor proteins (TSP) containing a DNA-binding domain (DBD) that binds to a gene and represses transcription, and RNA-binding domains (RBDs) that bind RNA, usually a noncoding RNA (ncRNA), forming a TSP/RNA complex that releases the TSP from a gene and reverses repression. This mechanism appears to be involved in the regulation of embryogenesis, oncogenesis, and steroidogenesis. Embryonic cells express high levels of RNA that bind to a TSP and prevent repression of proto-oncogenes that drive cell proliferation. The level of the RNA subsequently decreases in most differentiating cells, enabling a TSP to repress proto-oncogenes and stop cell proliferation. Oncogenesis can result when the level of the RNA fails to decrease in a proliferating cell or increases in a differentiated cell. This mechanism also regulates transcription of P450scc, the first gene in the steroidogenic pathway. ' 2007 Wiley-Liss, Inc.

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Recognition of RNA by the p53 tumor suppressor protein in the yeast three-hybrid system

Cited by 22 publications

References 65 publications

Analysis of p53–RNA interactions in cultured human cells

Analysis of p53–RNA interactions in cultured human cells

Two‐ and Three‐Hybrid Systems

Regulatory roles of tumor‐suppressor proteins and noncoding RNA in cancer and normal cell functions

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