Direct Activation of Bax by p53 Mediates Mitochondrial Membrane Permeabilization and Apoptosis

Chipuk, Jerry E.; Kuwana, Tomomi; Bouchier‐Hayes, Lisa; Droin, Nathalie; Newmeyer, Donald D.; Schüler, Martin; Green, Douglas R.

doi:10.1126/science.1092734

Cited by 1,810 publications

(1,523 citation statements)

References 28 publications

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“…Importantly, however, expression of high amounts of p53 without additional DNA-damage did not induce apoptosis in NIH3T3 cells (Figure 4a, b), indicating that damage-induced activation of p53 is required for the pro-apoptotic effect. In accordance with our observation that higher p53 levels do not correlate with higher expression levels of p53 targets (see before), the higher p53 amounts in HA-p53 transfected and Cytosolic p53 accumulates in pre-apoptotic cells and correlates with Bax-activation Recent studies have linked non-transcriptional proapoptotic activities of p53 to a cytosolic or mitochondrial localization of the protein (Chipuk et al, 2003(Chipuk et al, , 2004Dumont et al, 2003;Mihara et al, 2003;Leu et al, 2004). To test whether such a non-transcriptional activity of p53 might account for 100 J/m 2 UV-induced apoptosis in NIH3T3 cells, we monitored differently irradiated NIH3T3 cells for the presence of cytosolic p53.…”

Section: Upregulation Of Bax and Pig3 Is Not Sufficient To Induce Aposupporting

confidence: 91%

“…Further analysis assigned the pro-apoptotic activity of high amounts of activated p53 to cytosolic p53, which was able to trigger Bax-activation. Previous in vitro studies had already shown that cytosolic p53 can activate Bax in a transcription-independent manner analogous to that of BH3-only-proteins, and thereby lead to apoptosis (Chipuk et al, 2003(Chipuk et al, , 2004. Our data demonstrate for the first time the relevance of this mechanism in vivo.…”

Section: Discussionsupporting

confidence: 72%

“…However, cytosolic p53 accumulated to high amounts upon apoptosis-inducing 100 J/m 2 UV-irradiation (Figure 5b, right panel), probably reflecting the high amounts of total p53 in these cells. Cytosolic accumulation of p53, achieved by inhibiting nuclear import, was reported to directly activate Bax, thereby leading to induction of mitochondria-mediated apoptosis (Chipuk et al, 2004). We therefore investigated whether intrinsically generated high cytosolic p53 Dissection of p53 apoptotic activities D Speidel et al levels in 100 J/m 2 UV-irradiated NIH3T3 cells are coupled to activation of Bax.…”

Section: Upregulation Of Bax and Pig3 Is Not Sufficient To Induce Apomentioning

confidence: 97%

“…Elegant in vitro studies demonstrated the ability of p53 to directly activate Bax in a transcription-independent manner (Chipuk et al, 2003(Chipuk et al, , 2004. To prove that p53 and not another factor is responsible for Bax-activation also in our in vivo system, we analysed isogenic mouse fibroblasts based on the p53-deficient cell line 10-1 (Harvey and Levine, 1991;Ziegler, 1998).…”

Section: Stress-induced Bax-activation Is P53-dependent But Transcrimentioning

confidence: 99%

“…Possible mechanisms for non-transcriptional p53 apoptosis, however, were only recently reported. While some studies suggest that translocation of the p53 protein itself to or into the mitochondria is responsible for its pro-apoptotic effect (Marchenko et al, 2000;Dumont et al, 2003;Mihara et al, 2003;Leu et al, 2004), others report a transcription-independent, direct activation of the pro-apoptotic protein Bax by cytosolic p53 (Chipuk et al, 2003(Chipuk et al, , 2004. However, neither the physiological impact of transcription-independent mechanisms for the induction of apoptosis in vivo nor the coordination between transcriptional and non-transcriptional p53 activities has been sufficiently clarified.…”

Section: Introductionmentioning

confidence: 99%

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Dissection of transcriptional and non-transcriptional p53 activities in the response to genotoxic stress

2005

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Following genotoxic stress, p53 either rescues a damaged cell or promotes its elimination. The parameters determining a specific outcome of the p53 response are largely unknown. In mouse fibroblasts treated with different irradiation schemes, we monitored transcriptional and non-transcriptional p53 activities and identified determinants that initiate an anti-or a pro-apoptotic p53 response within the context of p53-independent stress signaling. The primary, transcription-mediated p53 response in these cells is anti-apoptotic, while induction of p53-dependent apoptosis requires an additional, transcription-independent p53 activity, provided by high intracellular levels of activated p53. High intracellular levels of p53 were selectively generated after apoptosis-inducing high-dose UV-irradiation, and correlated with a strongly delayed upregulation of Mdm2. Following high-dose UV-irradiation, p53 accumulated in the cytoplasm and led to activation of the pro-apoptotic protein Bax. As p53-dependent Bax-activation is transcription-independent, we postulated that certain transcription-deficient mutant p53 proteins might also exert this activity. Indeed we found an endogenous, transcription-inactive mutant p53 that upon genotoxic stress induced Bax-activation in vivo. Our results demonstrate the impact and in vivo relevance of non-transcriptional mechanisms for wild-type and mutant p53-mediated apoptosis. Oncogene (2006) 25, 940-953.

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Section: Upregulation Of Bax and Pig3 Is Not Sufficient To Induce Aposupporting

confidence: 91%

Section: Discussionsupporting

confidence: 72%

Section: Upregulation Of Bax and Pig3 Is Not Sufficient To Induce Apomentioning

confidence: 97%

Section: Stress-induced Bax-activation Is P53-dependent But Transcrimentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

Dissection of transcriptional and non-transcriptional p53 activities in the response to genotoxic stress

2005

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The Role of MAGEA2 in Head and Neck Cancer

Glazer

Smith

Bhan³

et al. 2011

Arch Otolaryngol Head Neck Surg

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Objective To examine the role of MAGEA2 in the tumorigenesis of head and neck squamous cell carcinoma (HNSCC). Design Primary tissue microarray data and quantitative reverse transcription–polymerase chain reaction (RT-PCR) showed that MAGEA2 is differentially over-expressed in HNSCC. Functional analyses were then performed using MAGEA2 transfections and small-interfering RNA knockdowns with subsequent anchorage-dependent growth studies and cell cycle analyses. Quantitative RT-PCR was used to evaluate expression changes in p53 downstream targets after transfection of MAGEA2 into normal upper aerodigestive cell lines. Results MAGEA2 is differentially overexpressed in HNSCC. In addition, MAGEA2 promotes growth in normal oral keratinocytes, whereas knockdown of MAGEA2 in HNSCC cells decreases growth. Using the HCT116 p53 wt and null cell line system, transfection of MAGEA2 induced growth in the p53 wt cell line while providing no growth advantage in the p53 mutant cells. Subsequently, transfection of MAGEA2 induced a decrease in messenger RNA expression of the p53 downstream targets CDKN1A and BAX and decreased G1 arrest in cells allowed to remain confluent for longer than 48 hours. Conclusions These data suggest that MAGEA2 is differentially expressed in HNSCC and functions, in part, through the p53 pathway by increasing cellular proliferation and abrogating cell cycle arrest. This improved understanding of MAGEA2 function and expression patterns will potentially allow for the improved ability to use MAGEA2 for detection, surveillance, and targeted therapeutics.

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Voltage‐gated sodium channels β3 subunit promotes tumorigenesis in hepatocellular carcinoma by facilitating p53 degradation

Han

Guo

et al. 2019

FEBS Letters

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The voltage‐gated sodium channels (VGSCs) are aberrantly expressed in a variety of tumors and play an important role in tumor growth and metastasis. Here, we show that VGSCs auxiliary β3 subunit, encoded by the SCN3B gene, promotes proliferation and suppresses apoptosis in HepG2 cells by promoting p53 degradation. β3 significantly increases HepG2 cell proliferation, promotes tumor growth in mouse xenograft models, and suppresses senescence and apoptosis. We found that β3 knockdown stabilizes p53 protein, leading to potentiation of p53‐induced cell cycle arrest, senescence, and apoptosis. Mechanistic studies revealed that β3 could bind to p53, promoting p53 ubiquitination and degradation by stabilizing the p53/MDM2 complex. Our results suggest that β3 is a novel negative regulator of p53 and a potential oncogenic factor.

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Direct Activation of Bax by p53 Mediates Mitochondrial Membrane Permeabilization and Apoptosis

Cited by 1,810 publications

References 28 publications

Dissection of transcriptional and non-transcriptional p53 activities in the response to genotoxic stress

Dissection of transcriptional and non-transcriptional p53 activities in the response to genotoxic stress

The Role of MAGEA2 in Head and Neck Cancer

Voltage‐gated sodium channels β3 subunit promotes tumorigenesis in hepatocellular carcinoma by facilitating p53 degradation

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