Role of p53 family members in apoptosis

Sheikh, M. Saeed; Fornace, Albert J.

doi:10.1002/(sici)1097-4652(200002)182:2<171::aid-jcp5>3.0.co;2-3

Cited by 171 publications

(115 citation statements)

References 112 publications

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“…Typically, p53 is activated when DNA damage occurs or the cell is stressed. It translocates to the nucleus, where it can induce proapoptotic gene expression, such as Bax, on the mitochondrial membrane, activate the effector caspase-3 and accelerate cell death (Levine, 1997;Sheikh and Fornace, 2000). Our results showed that the expression level of Bax progressively increased when the fish was treated with PFOS (Fig.…”

Section: Discussionmentioning

confidence: 56%

Developmental toxicity and alteration of gene expression in zebrafish embryos exposed to PFOS

Shi

Lam

et al. 2008

Toxicology and Applied Pharmacology

315

156

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Section: Discussionmentioning

confidence: 56%

Developmental toxicity and alteration of gene expression in zebrafish embryos exposed to PFOS

Shi

Lam

et al. 2008

Toxicology and Applied Pharmacology

315

156

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“…The tumor suppressor p53 is a major regulator of the cellular response to genotoxic stress (47)(48)(49). One way in which p53 modulates the cellular stress response is by functioning as a transcription factor to regulate the expression of genes important to cell growth arrest and apoptosis, such as p21 WAF1 , PUMA, DR5, and BAX.…”

Section: P53 Down-regulates Nsmase3 Mrna Expressionmentioning

confidence: 99%

Neutral Sphingomyelinase-3 Is a DNA Damage and Nongenotoxic Stress-Regulated Gene That Is Deregulated in Human Malignancies

Ponnusamy

et al. 2008

Molecular Cancer Research

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“…[3][4][5] PUMA encodes a BH3 only domain proapoptotic protein that localizes to mitochondria and interacts with antiapoptotic Bcl-2 and Bcl-X L (1)(2)(3). It is now well established that the tumor suppressor p53 predominantly functions as a transcription factor and mediates its effects by inducing growth arrest and/or apoptosis (reviewed in Sheikh and Fornace Jr, 6 Vousden and Lu, 7 and Hofseth et al 8 ). p53 mediates its apoptotic effects by transcriptionally activating the expression of proapoptotic genes, some of which include Bax, NOXA, PUMA and DR5, whose products modulate the intrinsic and extrinsic pathways of apoptosis (reviewed in Hofseth et al 8 ).…”

Section: Introductionmentioning

confidence: 99%

Transcriptional upregulation of PUMA modulates endoplasmic reticulum calcium pool depletion-induced apoptosis via Bax activation

Luo

Huang

et al. 2005

Cell Death Differ

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PUMA, a key mediator of p53-induced apoptosis, is a BH3-only domain proapoptotic protein that localizes to mitochondria and interacts with antiapoptotic Bcl-2 and Bcl-X L . Recent evidence implicates Bax to be an important mediator of PUMA-activated apoptotic signals. We have previously demonstrated that Bax deficiency significantly affects thapsigargin (TG)-mediated endoplasmic reticulum calcium pool depletion-induced apoptosis. We now present evidence that TG upregulates PUMA expression and that although Baxdeficient cells exhibit resistance to TG, Bax deficiency does not attenuate TG upregulation of PUMA expression. Furthermore, TG transcriptionally upregulates PUMA expression in a p53-independent manner and that PUMA-deficient cells are more resistant to undergo TG-induced apoptosis than the PUMA-proficient counterparts. Thus, our results demonstrate that TG engages PUMA and Bax for full transduction of apoptotic signals and both PUMA and Bax appear to exist in the same TG-activated apoptotic pathway in which PUMA may reside upstream of Bax.

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Role of p53 family members in apoptosis

Cited by 171 publications

References 112 publications

Developmental toxicity and alteration of gene expression in zebrafish embryos exposed to PFOS

Developmental toxicity and alteration of gene expression in zebrafish embryos exposed to PFOS

Neutral Sphingomyelinase-3 Is a DNA Damage and Nongenotoxic Stress-Regulated Gene That Is Deregulated in Human Malignancies

Transcriptional upregulation of PUMA modulates endoplasmic reticulum calcium pool depletion-induced apoptosis via Bax activation

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