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Query: UNIPROT:P04637 (
p53
)
77,613
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Two distinct products are specified by the CDKN2A locus, the p16INK4a cyclin dependent kinase inhibitor and a protein termed
ARF
.
ARF
has been shown to bind to the Mdm2-
p53
complex, resulting in stabilisation of both proteins, and a feedback loop exists through which
ARF
levels are negatively regulated by
p53
. Significantly,
ARF
expression is positively regulated by members of the E2F family of transcription factors. This provides a link between the Rb and
p53
pathways and a mechanism whereby inactivation of Rb and release of E2F will lead to the stabilisation and functional activation of
p53
. The alternative exon encoding the functional amino terminal portion of
ARF
presumably represents an independent gene that has become co-localized with p16INK4a in order to exploit a common regulatory mechanism or purpose.
...
PMID:Alternative product of the p16/CKDN2A locus connects the Rb and p53 tumor suppressors. 1074 Aug 16
Acute hypertonicity causes cell cycle delay and apoptosis in mouse renal inner medullary collecting duct cells (mIMCD3) and increases GADD45 expression. Because the
tumor suppressor protein p53
may be involved in these effects, we have investigated the role of
p53
in mIMCD3 response to hyperosmotic stress. Acute elevation of osmolality with NaCl addition from the control level of 320 mosmol/kg to 500-600 mosmol/kg greatly increased the levels of total and Ser(15)-phosphorylated
p53
within 15 min. However, similar elevation of osmolality with
urea
did not increase
p53
levels. Our studies indicate that induced
p53
is transcriptionally active because NaCl addition to 500-600 mosmol/kg stimulated transcription of a luciferase reporter containing a
p53
consensus element and appropriately altered mRNA levels of known transcriptional targets of
p53
, i.e. increased MDM-2 and decreased BCL-2 levels. Elevating NaCl further to 700-800 mosmol/kg rapidly killed most of the cells by apoptosis. At these higher NaCl concentrations,
p53
levels were further increased although Ser(15) phosphorylation and transcriptional activity were significantly lower than levels at 500-600 mosmol/kg. At NaCl-induced 500 mosmol/kg, apoptosis was rare in the presence of control, nonspecific oligonucleotide but highly prevalent upon addition of
p53
antisense oligonucleotide that substantially reduced
p53
levels. We conclude that induction of active
p53
in mIMCD3 cells by hypertonic stress contributes to cell survival.
...
PMID:Protection of renal inner medullary epithelial cells from apoptosis by hypertonic stress-induced p53 activation. 1074 24
The
p53 tumor suppressor
is activated by many diverse stress signals through mechanisms that result in stabilization and accumulation of the
p53 protein
.
p53
is normally degraded through the proteasome following interaction with MDM2, which both functions as a ubiquitin ligase for
p53
and shuttles to the cytoplasm, where
p53
degradation occurs. Stabilization of
p53
in response to stress is associated with inhibition of MDM2-mediated degradation, which has been associated with phosphorylation of
p53
in response to DNA damage or activation of
ARF
. In this study we show distinct responses, as measured by phosphorylation, transcriptional activity, and subcellular localization, of
p53
stabilized by different activating signals. Although normal cells and wild-type
p53
-expressing tumor cells showed similar responses to actinomycin D and camptothecin treatment, the transcriptional activity of stabilized
p53
induced by deferoxamine mesylate, which mimics hypoxia, in normal cells was lost in all three tumor cell lines tested. Our results show that multiple pathways exist to stabilize
p53
in response to different forms of stress, and they may involve down-regulation of MDM2 expression or regulation of the subcellular localization of
p53
or MDM2. Loss of any one of these pathways may predispose cells to malignant transformation, although reactivation of
p53
might be achieved through alternative pathways that remain functional in these tumor cells.
...
PMID:Stress signals utilize multiple pathways to stabilize p53. 1075 6
The rat hepatocytes were immortalized using a temperature-sensitive mutant of SV40 large T antigen (tsT) to develop as a possible substitute for primary hepatocytes. Four rat hepatocyte lines that have been developed and maintained more than passage 50, were characterized for their cellular morphology, T antigen and
p53
expression, chromosomes, liver-specific differentiation, telomerase activity and anchorage independent growth. All of four cell lines showed a typical epithelial cell morphology, but the population-doubling time became short with passage: 18 to 60%. T antigen expression was increased with passage about 3 to 65 times at permissive temperature but decreased significantly at non-permissive temperature. The expression level of
p53
unchanged during passages was also decreased at non-permissive temperature. The distribution of chromosome number changed somewhat with passage. The production levels of albumin and
urea
in four cell lines were 2.4 to 13.0% and 7.5 to 19.9% of those produced in primary hepatocytes, respectively and were decreased to an undetectable level with passage. Telomerase activity was increased 10 fold following immortalization of cells, but anchorage independent growth of cells did not develop. These results indicate that conditionally immortalized hepatocytes become dedifferentiated with in vitro passage, which may be caused by marked chromosomal damages that occur with compulsive and continuous replications by the increment of T antigen content with passage and its sequential inhibition of
p53
function.
...
PMID:Dedifferentiation of conditionally immortalized hepatocytes with long-term in vitro passage. 1076 59
The INK4a/
ARF
locus is regarded as one of the most important anti-tumoral defenses that mammalian organisms possess. The characterization of its two gene products, p16(INK4a) and p19(
ARF
), has provided a great insight on the functioning of the tumor suppressors Rb and
p53
, respectively. Present evidence indicates that the INK4a/
ARF
locus is transcriptionally activated by oncogenic stresses, resulting in cell-cycle arrest or apoptosis. Here, I review the evidence accumulated on the involvement of the INK4a/
ARF
locus in murine tumorigenesis. Also, I summarize the phenotype of the different transgenic mouse models based on the inactivation of the INK4a/
ARF
locus.
...
PMID:The INK4a/ARF locus in murine tumorigenesis. 1078 5
Little is known about the molecular mechanisms responsible for the development of intracranial germ cell tumors (ICGTs). Recently, we demonstrated that the balance of the
p53
-mdm2 interactions is disrupted in ICGTs. The p14ARF product, a tumor suppresser gene located on the INK4a/
ARF
locus, acts as one of the major factors affecting
p53
-mdm2 interactions via its binding to mdm2 and the stimulation of mdm2 degradation. To evaluate whether genetic alterations of the INK4a/
ARF
locus occur in the genesis of ICGTs, we analyzed the INK4a/
ARF
genes in 21 ICGTs-10 pure germinomas and 11 nongerminomatous germ cell tumors. Fifteen (71%) of the 21 ICGTs displayed genetic alterations, including 14 homozygous deletions and 1 frameshift mutation. Furthermore, the frequency of the alterations was higher in pure germinomas [9 (90%) of the 10] than in nongerminomatous germ cell tumors [6 (55%) of the 11; P = 0.09]. These data suggested that INK4a/
ARF
gene abnormalities could play an important role in the genesis of ICGTs, especially in pure germinoma.
...
PMID:Alterations of the INK4a/ARF locus in human intracranial germ cell tumors. 1078 70
A senescence-like growth arrest is induced in mouse primary embryo fibroblasts by inhibitors of phosphoinositide 3-kinase (PI3K). We observed that senescence-like growth arrest is correlated with an increase in p27(Kip1) but that down-regulation of other cyclin-dependent kinase (CDK) inhibitors, including p15(INK4b), p16(INK4a), p19( INK4d), and p21(Cip1) as well as other negative cell cycle regulators such as
p53
and p19(
ARF
), implies that this senescence-related growth arrest is independent of the activity of
p53
, p19(
ARF
), p16(INK4a), and p21(Cip1), which are associated with replicative senescence. The p27(Kip1) binds to the cyclin/CDK2 complexes and causes a decrease in CDK2 kinase activity. We demonstrated that ectopic expression of p27(Kip1) can induce permanent cell cycle arrest and a senescence-like phenotype in wild-type mouse embryo fibroblasts. We also obtained results suggesting that the kinase inhibitors LY294002 and Wortmannin arrest cell growth and induce a senescence-like phenotype, at least partially, through inhibition of PI3K and protein kinase B/Akt, activation of the forkhead protein AFX, and up-regulation of p27(Kip1)expression. In summary, these observations taken together suggest that p27(Kip1) is an important mediator of the permanent cell cycle arrest induced by PI3K inhibitors. Our data suggest that repression of CDK2 activity by p27(Kip1) is required for the PI3K-induced senescence, yet mouse embryo fibroblasts derived from p27(Kip1-/-) mice entered cell cycle arrest after treatment with LY294002. We show that this is due to a compensatory mechanism by which p130 functionally substitutes for the loss of p27(Kip1). This is the first description that p130 may have a role in inhibiting CDK activity during senescence.
...
PMID:Inhibition of the phosphoinositide 3-kinase pathway induces a senescence-like arrest mediated by p27Kip1. 1079 51
Epidemiological studies suggest that some familial aggregations of glioma may be due to inherited predisposition. Many genes involved in familial cancers are frequently altered in the corresponding sporadic forms. We have investigated several genes known to be altered in sporadic gliomas for their potential contribution to familial glioma. Fifteen glioma patients with a family history of brain tumors were identified through the Mayo Clinic Department of Neurology (nine diffuse astrocytomas, two oligodendrogliomas, two mixed oligoastrocytomas, one pilocytic astrocytoma, and one pineal glioma). Eleven of the propositi had one or more first degree relative with a glioma. Lymphocyte DNA was derived from each of the patients and analyzed by polymerase chain reaction (PCR) and direct sequencing of the PTEN,
p53
, p16(INK4A)/p14(
ARF
), and CDK4 genes. In addition, fluorescence in situ hybridization (FISH) was performed on EBV-transformed lymphocytes from each affected individual to detect germline copy number of the p16(INK4A)/p14(
ARF
) tumor suppressor region. A
p53
germline point mutation was identified in one family with some findings of Li-Fraumeni syndrome, and a hemizygous germline deletion of the p16(INK4A)/p14(
ARF
) tumor suppressor region was demonstrated by FISH in a family with history of both astrocytoma and melanoma. Thus, whereas germ-line mutations of PTEN,
p53
, p16(INK4A)/p14(
ARF
), and CDK4 are not common events in familial glioma, outside of familial cancer syndromes, point mutations of
p53
and hemizygous deletions and other rearrangements of the p16(INK4A)/p14(
ARF
) tumor suppressor region may account for a subset of familial glioma cases. Collectively, these data lend genetic support to the heritable nature of some cases of glioma.
...
PMID:Investigation of germline PTEN, p53, p16(INK4A)/p14(ARF), and CDK4 alterations in familial glioma. 1079 39
We previously reported that two nuclear factor 1-like elements mediated the transcription of the rat
p53
gene. A 40-kDa protein was shown to bind to these elements, which was different from common NF1 family proteins. In this study, the biochemical properties of the 40-kDa binding protein were investigated. The metal ion dependency of the protein was examined with various chelators; the protein was proved to require Mg(2+) for maximum DNA-binding activity. The binding protein was highly resistant to ionic strength and denaturant. The protein-DNA complex was reduced at high NaCl concentration, but residual DNA-binding activity remained. Even 2 M
urea
did not completely eliminate the formation of protein-DNA complex. DNA-binding activity of the protein was also stable at high temperature. Treatment of the protein-DNA complex with increasing concentrations of proteinase K or trypsin demonstrated the existence of a protease-resistant DNA-bound core. These biochemical properties provide new insight into the 40-kDa NF1-like nuclear factor.
...
PMID:Biochemical characterization of a nuclear factor that binds to NF1-like elements in the rat p53 promoter. 1079 61
The
p53
tumour suppressor protein is down-regulated by the action of Mdm2, which targets
p53
for rapid degradation by the ubiquitin-proteasome pathway. The p14ARF protein is also a potent tumour suppressor that acts by binding to Mdm2 and blocking Mdm2-dependent
p53
degradation and transcriptional silencing. We have screened a series of overlapping synthetic peptides derived from the p14ARF protein sequence and found that a peptide corresponding to the first 20 amino acids of
ARF
(Peptide 3) could bind human Mdm2. The binding site for Peptide 3 on Mdm2 was determined by deletion mapping and lies adjacent to the binding site of the anti-Mdm2 antibody 2A10, which on microinjection into cells can activate
p53
-dependent transactivation of a reporter plasmid. To determine whether Peptide 3 could similarly activate
p53
, we expressed a fusion of green fluorescent protein and Peptide 3 in MCF7 and U-2 OS cells and were able to demonstrate induction of
p53 protein
and
p53
-dependent transcription. Peptide 3 was able to block in vitro ubiquitination of
p53
mediated by Mdm2. Small peptides which are sufficient to block degradation of
p53
could provide therapeutic agents able to restore
p53
-dependent cell death pathways in tumours that retain wild-type
p53
expression.
...
PMID:An N-terminal p14ARF peptide blocks Mdm2-dependent ubiquitination in vitro and can activate p53 in vivo. 1082 82
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