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Query: UNIPROT:P43146 (
tumour suppressor
)
5,935
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
The concept of field cancerisation assumes that in head and neck cancer patients (HNCP) with multiple malignancies the second primary cancers may arise independently from the entire upper aerodigestive tract as a consequence of massive exposure to common carcinogens. Since mutations and/or overexpression of the
p53
tumour suppressor
gene represent a genetic alteration frequently occurring in HNCP, we analysed immunocytochemically
p53
oncoprotein expression in first primary, second primary cancers and in macroscopically uninvolved normal epithelium from different sites of the upper aerodigestive tract from 12 HNCP with multiple malignancies, in comparison with
p53
expression in biopsy specimens of the upper aerodigestive tract from 5 non-neoplastic heavy smokers, as controls. In patients with multiple malignancies 6 cases (50%) showed positive staining of both first and second primaries, whereas 3 (25%) had positive labelling of first primary cancer but not of the subsequent second primary, 2 (17%) patients showed
p53
expression only in the second primary cancer, and finally only 1 patient (8%) showed no
p53
immunoreactivity in both first and second primary tumours. Moreover, 10 out of 12 (83%) HNCP with multiple cancers showed
p53
-positive staining in the normal epithelium from different sites of the upper aerodigestive tract, also at a significant distance from the site of first and second primary malignancies. contrast, sporadic
p53
immunostaining was observed only in three out of 35 (8.5%) specimens from non-neoplastic controls. In addition, in 4 HNCP with multiple tumours the histological examination of apparently normal epithelium from the upper aerodigestive tract revealed signs of moderate or severe dysplasia, and in 1 case an in situ carcinoma.(ABSTRACT TRUNCATED AT 250 WORDS)
...
PMID:p53 expression: a potential biomarker for risk of multiple primary malignancies in the upper aerodigestive tract. 762 89
p53
is a putative
tumour suppressor
gene implicated in a wide range of human malignancies. Mutation of
p53
gene results in a more stable product and increased quantities of
p53 protein
in the cell. Thus, unlike the normal situation, mutated
p53
is detectable by immunohistochemistry. We stained frozen sections of 74 astrocytomas with two antibodies to
p53
, PAb 1801 and PAb 421. Overall 18/74 (24%) of astrocytomas showed
p53
immunoreactivity. Fifteen of 47 (32%) grade IV were
p53
immunopositive, as were 3/16 (19%) grade III, 0/7 (0%) grade II and 0/4 (0%) grade I astrocytomas. These findings are in agreement with previous studies in showing relatively greater numbers of high grade than low grade
p53
immunopositive tumours. Although we found an expected difference in survival according to grade, there was no significant difference in survival (p > 0.1) between
p53
immunopositive and immunonegative tumours. We conclude that, whilst
p53
undoubtedly plays an important role in the molecular 'chain' leading to malignancy in some astrocytomas, within tumours of comparable grade it does not appear to influence survival.
...
PMID:p53 immunoreactivity in astrocytomas and its relationship to survival. 763 59
The mutation of the
p53
tumour suppressor
gene is the most frequently recognised genetic alteration in human cancer. We recently showed that the frequency of
p53
gene mutations in oral squamous cell carcinomas (SCCs) from which cell lines were established (group A) did not significantly differ from that in SCCs from which cell lines could not be established (group B), suggesting that the presence of a
p53
mutation by itself is not sufficient. To assess the relevance of
p53
mutations to cell line establishment, we determined sequences of the mutated genes, constructed the expression plasmids, and compared biological and biochemical activities. Both groups contained typical mutant type mutations at a similar frequency. However, two mutations in group A had strong transforming activity. One of the mutants, codon 306 Stop mutant with C-terminal truncation, was found to have the transactivation and transform suppression activities similar to wild type. The minimum transactivation and transform suppression domains of
p53
were thus determined based on analysis of various C-terminal deletions. Activity disappeared between codons 300 and 282, an interval which contains the C-terminal end of the sequence-specific DNA binding domain, which suggests that the DNA binding domain is essential for the above activities.
...
PMID:Roles of p53 mutation in cell line establishment and identification of the minimum transactivation and transform suppression domains. 763 85
Lymphocytes are particularly susceptible to DNA damage-induced apoptosis, a response which may serve as a form of 'altruistic suicide' to counter their intrinsic high potential for mutation and clonal expansion. The
tumour suppressor
p53
has been shown to regulate this type of apoptosis in thymocytes, but an as yet unknown,
p53
-independent pathway(s) appears to mediate the same event in mitogen-activated mature T lymphocytes. Here we show DNA damage-induced apoptosis in these T lymphocytes is dependent on the antioncogenic transcription factor interferon regulatory factor (IRF)-1. Thus two different anti-onco-genic transcription factors,
p53
and IRF-1, are required for distinct apoptotic pathways in T lymphocytes. We also show that mitogen induction of the interleukin-1 beta converting enzyme (ICE) gene, a mammalian homologue of the Caenorhabditis elegans cell death gene ced-3, is IRF-1-dependent. Ectopic overexpression of IRF-1 results in the activation of the endogenous gene for ICE and enhances the sensitivity of cells to radiation-induced apoptosis.
...
PMID:An IRF-1-dependent pathway of DNA damage-induced apoptosis in mitogen-activated T lymphocytes. 763 9
Partial sequence determinations were performed on exon 8 of
tumour suppressor
gene
p53
of cattle, sheep, goat, horse and pig. High sequence homology between these species and other species including dog, cat, chicken and man is demonstrated. A mutation CGG-->TGG (arginine-->tryptophan) was detected in a feline solid carcinoma of the mammary gland.
...
PMID:Sequence of an exon of tumour suppressor p53 gene--a comparative study in domestic animals: mutation in a feline solid mammary carcinoma. 764 Sep 60
Human papillomavirus (HPVs) adenovirus and simian virus 40 (SV40) are small DNA viruses which can show oncogenic activity. Although not otherwise related, all three have adopted very similar strategies to deregulate cell growth; each virus encoding oncoproteins which interact with the same cellular targets. Of particular interest are the interactions with the cell encoded pRB and
p53
proteins, products of
tumour suppressor
genes. Somatic mutation results in the loss of the pRB and
p53
function in many cancers and the contribution of the viruses to tumour development appears to reflect their ability to inactivate these cellular proteins. Both pRB and
p53
negatively regulate progress through the cell cycle and the action of the viral proteins has highlighted the central importance of these
tumour suppressor
proteins in maintaining normal cell growth.
...
PMID:Regulation of the cell cycle by viral oncoproteins. 764 7
The
p53 protein
is a multifunctional transcription factor which orchestrates cellular responses to DNA damage, so helping to conserve genomic stability. It may also regulate genes involved in intercellular signalling, such as thrombospondin, a negative regulator of angiogenesis and metastatic spread. Activation of p53 target genes requires sequence-specific DNA binding, a function which maps to the central core of the protein. Missense point mutations within this domain inactivate
p53
tumour suppressor
function and involve either (i) DNA contact residues, or (ii) residues important for conformational structure. Using in vitro techniques we have analysed seven DNA contact mutants and 17 structural mutants known to occur in cancer. We show that DNA contact mutants can be carried into specific DNA interaction when co-expressed with wild type protein. For structural mutants, 9/17 retained DNA binding capacity and, with one exception, DNA binding correlated with conformational flexibility of the mutant protein. The exception was Asp281, which appeared essential for DNA interaction, probably due to its ability to form salt bridges with DNA contact residues Arg273 and Arg280. We suggest that different classes of
p53
mutant may prove amenable to different strategies for restoration of wild type
tumour suppressor
function as means of anti-cancer therapy.
...
PMID:Specific DNA binding by different classes of human p53 mutants. 765 40
The present study describes mutations of the
tumour suppressor
gene
p53
in a local collection of colorectal and hepatocellular carcinomas (HCCs). Tumour DNA was extracted from both fresh and paraffin-embedded tissues and exons 5-8 of the
p53
gene were amplified by polymerase chain reaction (PCR). Mutations were detected by single-strand conformation polymorphism (SSCP) analysis followed by direct DNA sequencing. Of the 38 colorectal carcinomas and 42 HCCs examined, 15 (39%) and 13 (31%), respectively, showed
p53
mutations. Two-thirds (10/15) of the mutations in colorectal carcinomas were base transitions with a predominance at CpG dinucleotide sites--a pattern characteristic to an endogenous process in cancer development. Three mutational hotspots at codons 175, 248 and 282 were also identified. Mutations did not correlate with histological grade, Dukes stage, or metastasis. However, tumours at the distal site of the colorectum showed a higher proportion of mutations than the proximal site. In the case of HCCs, majority (9/13) of the mutations were base transitions and no mutations were observed at codon 249. This is in contrast to results from other high-incidence areas such as Africa and China, where aflatoxin is believed to be a major aetiologic factor for liver cancers. The results therefore suggest that other risk factors, rather than dietary exposure to aflatoxin, may contribute to the high HCC incidence in Singapore.
...
PMID:Mutations of the tumour suppressor gene p53 in colorectal and hepatocellular carcinomas. 765 61
p53
tumour suppressor
gene expression was estimated immunohistochemically using DO-1 monoclonal antibody (recognising both wild-type and mutant p53 in 88 human renal tumours. Single strand conformation polymorphism (SSCP) analysis of possible mutations within exons 4-8 of the
p53
gene was performed in 29 of the tumours (mostly immunostaining-positive cases). Obviously elevated
p53
content was detected with DO-1 antibody in chromophobic cell carcinomas and most clear/chromophilic cell tumours (in chromophilic cell populations). In contrast, clear cell carcinomas demonstrated either complete absence of
p53
expression or the presence of single immunopositive nuclei. Oncocytomas were completely negative. Additional immunostaining of the positive samples with mutant p53-specific Pab240 monoclonal antibody failed to detect immunopositive material. No
p53
mutation was found in any of the samples analysed by SSCP. Our results suggest that the elevated
p53
content in human renal cell carcinomas does not result from gene mutation and the
p53
gene alterations are probably not an important mechanism in the development of human renal cell carcinomas. Accumulation of the wild-type
p53 protein
may be a useful prognostic marker indicating neoplastic progression malignancy.
...
PMID:Elevated content of p53 protein in the absence of p53 gene mutations as a possible prognostic marker for human renal cell tumors. 765 36
The frequent involvement of chromosome 17p abnormalities in the progression of chronic myeloid leukaemia (CML) led us to investigate the involvement of the
p53
tumour suppressor
gene located on chromosome 17p. We analysed 31 samples from four patients sequentially, and 16 patients in blast crisis only, using single stranded conformational polymorphism (SSCP) analysis of exons 5-8, followed by cloning and sequencing. The sequential samples ranged from diagnosis through to late disease. We found that 15% of our blast crisis samples had
p53
abnormalities. In our sequential studies we found two of the four patients analysed in more detail had
p53
mutations in the late chronic phase of disease (11 and 5 months prior to blast crisis becoming apparent). These chronic phase mutations differed from the
p53
abnormalities found in the blast crisis samples from these patients. One patient also had the same chronic phase mutation at post bone marrow transplant relapse. Our results suggest that, in some cases, sequential investigations through CML disease progression of
p53
mutations and other oncogenes/proto-oncogenes may provide early indications of the routes of disease progression to blast crisis.
...
PMID:Changing p53 mutations with the evolution of chronic myeloid leukaemia from the chronic phase to blast crisis. 765 97
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