Human ΔNp73 regulates a dominant negative feedback loop for TAp73 and p53

Grob, Tobias; Novak, Urban; Maisse, Carine; Barcaroli, Daniela; Lüthi, Alexander U.; Pirnia, Farzaneh; Hügli, Barbara; Graber, H.U.; Laurenzi, Vincenzo De; Fey, Martin F.; Melino, Gerry; Tobler, Andreas

doi:10.1038/sj.cdd.4400962

Cited by 332 publications

(364 citation statements)

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“…We and other groups have recently demonstrated that tumor cells frequently overexpress N-terminally truncated p73 isoforms that result from abberant splicing or the use of an alternative intronic promoter (Fillippovich et al, 2001;Grob et al, 2001;Kartasheva et al, 2002;Stiewe et al, 2002a, b;Zaika et al, 2002;Pu¨tzer et al, 2003). These DNp73 proteins act as dominant-negative inhibitors of the proapoptotic p53 family members by formation of transactivation-defective heteromeric complexes (Grob et al, 2001;Kartasheva et al, 2002;Stiewe et al, 2002a). Such a dominant-negative function of DNp73 has also been observed in this study with respect to hTERT regulation.…”

Section: Regulation Of Htert By P73 M Beitzinger Et Alsupporting

confidence: 80%

“…In contrast to downregulation of hTERT by differentiation or proapoptotic stress signals, hTERT is typically activated in immortal cells and established tumors . We and other groups have recently demonstrated that tumor cells frequently overexpress N-terminally truncated p73 isoforms that result from abberant splicing or the use of an alternative intronic promoter (Fillippovich et al, 2001;Grob et al, 2001;Kartasheva et al, 2002;Stiewe et al, 2002a, b;Zaika et al, 2002;Pu¨tzer et al, 2003). These DNp73 proteins act as dominant-negative inhibitors of the proapoptotic p53 family members by formation of transactivation-defective heteromeric complexes (Grob et al, 2001;Kartasheva et al, 2002;Stiewe et al, 2002a).…”

Section: Regulation Of Htert By P73 M Beitzinger Et Almentioning

confidence: 99%

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Regulation of telomerase activity by the p53 family member p73

Beitzinger

Oswald

Beinoraviciute-Kellner

et al. 2005

Oncogene

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The terminal ends of eukaryotic chromosomes, termed telomeres, progressively shorten during each round of cell division eventually leading cells into senescence. Tumor cells typically overcome this barrier to unlimited proliferation by activation of the human telomerase reverse transcriptase (hTERT) gene. In contrast, in most human somatic cells hTERT expression is tightly repressed by multiple tumor suppressors. Here, we studied the regulation of hTERT by the p53 family member p73. We show that forced expression of p73 or activation of endogenous p73 by E2F1 results in the downregulation of telomerase activity. Vice versa, siRNA-mediated knockdown of p73 induces hTERT expression. Responsiveness to p73 is conferred by Sp1 binding sites within the hTERT core promoter. In tumor cells, p73 isoforms lacking the transactivation domain (DNp73) are frequently overexpressed and believed to function as oncogenes. We show that DNp73 antagonizes the repressive effect of the proapoptotic p53 family members on hTERT expression and, in addition, induces hTERT expression in telomerase-negative cells by interfering with E2F-RB-mediated repression of the hTERT core promoter. These data provide evidence that the p73 gene functions as an important regulator of telomerase activity with implications for embryonic development, cellular differentiation and tumorigenesis.

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Section: Regulation Of Htert By P73 M Beitzinger Et Alsupporting

confidence: 80%

Section: Regulation Of Htert By P73 M Beitzinger Et Almentioning

confidence: 99%

Regulation of telomerase activity by the p53 family member p73

Beitzinger

Oswald

Beinoraviciute-Kellner

et al. 2005

Oncogene

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“…Each isoform is also subject to extensive alternative splicing at the 3 0 -end of mRNA, resulting in up to 24 transcripts, able to promote or repress apoptosis to different extents (De Laurenzi et al, 1998;Yang et al, 2000). The proteins originating from the second promoter, DNp73, have a dominant negative activity on the tumor suppressor functions of both TAp73 and p53 and this regulatory loop has been implicated in tumorigenesis (Grob et al, 2001).…”

Section: Introductionmentioning

confidence: 99%

p73 and caspase-cleaved p73 fragments localize to mitochondria and augment TRAIL-induced apoptosis

Sayan

Gogvadze

et al. 2008

Oncogene

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The p73 protein, a member of the p53 family, has both developmental and tumorigenic functions. Here we show that p73 is cleaved by caspase-3 and -8 both in vitro and in vivo during apoptosis elicited by DNA-damaging drugs and tumor necrosis factor-related apoptosis-inducing ligand (TRAIL) receptor ligation. TAp73 and some of its cleavage products are localized to mitochondria. siRNA-mediated downregulation of p73 expression induced a small but significant change in the susceptibility of HCT116 cells to TRAIL-induced apoptosis. A transcription-deficient mutant of TAp73 enhanced TRAIL-induced apoptosis suggesting that p73 protein has transcriptionindependent functions during death receptor-mediated apoptosis. Additionally, recombinant p73 protein induced cytochrome c release from isolated mitochondria providing evidence that nonnuclear p73 may have additional functions in the progression of apoptosis.

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“…[9][10][11][12] They act as powerful inhibitors of p53 and TAp73 since they retain their DNA-binding and tetramerization competence. [7][8][9]11,13,14 In cultured cells, DNp73 abrogates the suppressive activity of p53 and TAp73 and inactivates their ability to induce apoptosis and cell cycle arrest. 9 DNp73 overexpression results in malignant transformation of immortalized NIH3T3 fibroblasts 8 and also promotes immortalization in primary cells and cooperates with oncogenic Ras in driving their transformation in vivo.…”

mentioning

confidence: 99%

“…Also, the relative longevity of DNp73 versus TAp73 proteins, when in isolation, supports previous anecdotal observations that DNp73 proteins are more stable than TAp73 in tumors. 13,19 We next tested whether DNp73 proteins can induce stabilization of TAp73 proteins. H1299 cells were transfected with either TAp73a or b alone, or cotransfected with the same amount of TAp73a or b plus increasing amounts of DNp73a or stabilization, possibly because the levels of DNp73a are often higher than DNp73 which might in turn be related to the longer half life of DNp73a compared to b.…”

mentioning

confidence: 99%