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Query: UNIPROT:P04637 (
p53
)
77,613
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Single-stranded conformational polymorphism (SSCP) and direct sequencing were performed on uninvolved mucosa, severe
dysplasia
and invasive carcinoma samples from 20 patients with head and neck squamous carcinoma. Seven (35%) of the non-invasive lesions and 15 (75%) of the invasive carcinomas manifested
p53
mutations. Although the majority of mutations were mis-sense, resulting in single amino acid substitution, a silent mutation encoding for the same amino acid and 2 non-sense mutations encoding a stop codon were also observed. Mutations in invasive carcinoma were mostly in exon 8 and involved codons 296, 288 and 298; non-invasive lesions showed more mutations at exons 5 to 7. Five lesions showed simultaneous mutations in 2 different exons; in 3 both non-invasive and invasive carcinomas showed primary mutation at exons 5 to 7, and invasive carcinoma showed a secondary mutation at exon 8. Different codon mutations in the same exon between dysplastic and the corresponding carcinoma samples were found in 2 cases.
p53
alterations were not observed in any of the normal mucosa samples. No apparent association between
p53
mutations and conventional clinicopathologic parameters, including DNA content, was found in this cohort. Our study indicates that (i)
p53
alteration is an early event in the genesis of a subset of head and neck squamous carcinomas, (ii) normal mucosa within the resected specimens lacked
p53
mutation, (iii) sequential mutations of different exons of the
p53
gene suggests accumulation of genetic alterations during the neoplastic transformation of these lesions and (iv) the difference in codon mutation of the same exon between dysplastic and corresponding carcinoma suggests an independent clonal development.
...
PMID:Sequential p53 mutation analysis of pre-invasive and invasive head and neck squamous carcinoma. 762 8
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
Previous studies on
p53 protein
expression in colonic adenomas showed controversial results. The present study evaluates the
p53
expression in colonic adenomas, at different
dysplasia
degrees, by immunohistochemical analysis, using a newly introduced monoclonal anti-
p53
antibody. Paraffin embedded sections of 48 colorectal adenomas, 5 colonic carcinomas and 11 normal colonic biopsies were studied by immunohistochemical analysis using a monoclonal mouse anti-
p53
antibody (clone DO-1). Normal colonic mucosa specimens and 5/48 adenomas were found negative for
p53
staining.
p53
-positive nuclei were less than 10% in 22/48 and between 10 and 40% in 15/48 adenomas. In 6/48 adenomas and in 4/5 carcinomas we found a high percentage of
p53
-positive nuclei (> 40%). Immunohistochemical
p53
-positivity is a common event in colonic adenomas, not dependent on
dysplasia
degree. It might be the result of
p53
wild-type increase, due to the typical genomic instability of colonic adenomas.
...
PMID:High frequency of p53 expression in colo-rectal adenomatous polyps. 765 29
Hyperplastic lesions of the oropharyngeal mucosa such as leukoplakia and oral lichen planus can eventually develop into squamous cell carcinomas (SCC) and provide an excellent model for multistage carcinogenesis. The development of carcinomas is assumed to be the result of the interaction of genetic factors, locally applied carcinogens and immunological unresponsiveness. Recently a novel gene termed mdm2 has been isolated that is found to be involved in transcriptional regulation and can inhibit
p53
function by forming a complex with
p53
. In this study the immunohistochemical detection of the MDM2 protein in 186 paraffin embedded tissue sections of normal mucosa, premalignant, malignant and metastatic lesions of the oropharyngeal mucosa is reported for the first time.
p53 protein
expression was also investigated in the same tissue samples. The increase in the number of
p53
and MDM2 positive biopsies was correlated with the
dysplasia
grade and the loss of differentiation in the premalignant and malignant lesions. In late stages of the disease the number of biopsies that expressed both
p53
and MDM2 increased. Inactivation of
p53
function in head and neck carcinogenesis may also be due to MDM2 binding. Detection of MDM2 protein expression by immunohistochemistry may be an important diagnostic tool in the future.
...
PMID:Detection of p53 and MDM2 protein expression in head and neck carcinogenesis. 765 34
Frequent recurrences and multicentricity of bladder cancer suggest that alterations of the urothelium distant from the tumor may be relevant to prognosis. In this study immunohistochemistry and fluorescence in situ hybridization (FISH) were used to examine expression of
p53
, erbB-2, and epidermal growth factor receptor (EGF-r), genomic aberrations, and tumor cell proliferation (Ki67 LI) in normal and dysplastic urothelium. Biopsy specimens examined included normal urothelium (n = 40), mild
dysplasia
(n = 34), moderate
dysplasia
(n = 18) and carcinoma in situ (CIS; n = 20). Several different oncogene expression patterns were found, only some of which were associated with
dysplasia
. EGF-r expression was equally frequent in normal and dysplastic urothelium and showed a strong association with Ki67 LI (P < .0001). A purely superficial erbB-2 positivity was present in both normal and dysplastic biopsies. However, diffuse erbB-2 positivity and
p53
overexpression were both associated with advanced
dysplasia
(P < .0001 each). FISH analysis showed erbB-2 gene amplification and
p53
deletions in selected CIS, as well as a marked chromosome 17 copy number heterogeneity in all six CIS examined. These findings indicate a considerable genomic instability in bladder CIS. They show that both erbB-2 and
p53
are altered during malignant transformation. Detectable oncogene expression alone, however, is not diagnostic of malignancy in bladder urothelium.
...
PMID:Patterns of p53, erbB-2, and EGF-r expression in premalignant lesions of the urinary bladder. 767 97
Hyperplastic lesions of the oral mucosa such as leukoplakia and oral lichen planus can eventually develop into squamous cell carcinomas (SCC) and provide an excellent model for multistage carcinogenesis. The development of carcinomas is assumed to be the result of interaction of genetic factors, locally applied carcinogens and immunological unresponsiveness. The purpose of this study was, therefore, to determine the role of alterations of the tumour suppressor gene
p53
, and the proliferation status of the lesions determined by PCNA expression. We investigated
p53
and PCNA expression in 265 tissue sections of normal mucosa, premalignant, malignant and metastatic lesions of the oral mucosa by immunohistology. Quantitative analysis showed a gradual increase in PCNA expression from normal mucosa to moderately differentiated SCC.
p53
expression was detectable in benign premalignant lesions. The increase in the number of
p53
-positive biopsies was correlated with the
dysplasia
and loss of differentiation in the premalignant and malignant lesions.
...
PMID:p53 and PCNA expression in carcinogenesis of the oropharyngeal mucosa. 874 74
Immunohistochemically detectable levels of
p53
may be seen early in the malignant transformation of some neoplasms. To determine if
p53
is immunocytochemically detectable, and therefore presumptively abnormal, in oral dysplasias and in situ carcinomas, and to explore the natural history of
p53 protein
expression in these lesions, sequential biopsies from patients with lesions occurring in the same anatomic site were examined. Formalin-fixed, paraffin-embedded sections from 19 patients were evaluated immunohistochemically for
p53 protein
using antibody clones Pab1801 and BP53-12. With two exceptions, comparable results were observed with these antibodies.
p53 protein
was detected immunocytochemically in 6 of 13 patients with dysplasias; 3 of these progressed to
p53
-positive invasive carcinoma, one advanced to a more severe grade of
p53
-positive
dysplasia
, one developed into a
p53
-negative verrucous carcinoma, and one represented a
p53
-positive
dysplasia
developing five years after treatment of a
p53
-positive carcinoma. The
p53
-positive dysplasias, which were found in all subtypes (mild, moderate, severe), preceded histologic malignant change by months to years.
p53
detection was evident in 4 of 6 patients with in situ lesions. Sequential biopsies of three of these lesions showed no change in lesion histology or
p53
staining, and one lesion advanced to a
p53
-positive carcinoma. It is concluded that
p53 protein
may be detected early in the development of a subset of
p53
-positive oral squamous cell carcinomas. This phenomenon may be seen in dysplasias and in situ lesions, and it may have prognostic implications.
...
PMID:p53 protein expression in sequential biopsies of oral dysplasias and in situ carcinomas. 772 17
Accumulation of
p53 protein
was determined by immunohistochemistry in archival material of biopsy specimens from 102 patients with Barrett's oesophagus with different grades of
dysplasia
, in 24 oesophageal adenocarcinomas associated with Barrett's oesophagus, and in 23 cases of metaplastic epithelium adjacent to these carcinomas. Immunostaining for the
p53 protein
was found in 23/102 (23 per cent) cases of the Barrett's oesophagus biopsies and in 12/23 (52 per cent) cases of Barrett's oesophagus adjacent to adenocarcinoma. Significant correlations were found between the grade of
dysplasia
and
p53
immunoreactivity in both Barrett's biopsies without adenocarcinoma (P < 0.001) and Barrett's oesophagus adjacent to adenocarcinoma (P < 0.05). In the adenocarcinomas, intense nuclear immunohistochemical staining for
p53
was diffusely or focally present in 20/24 (83 per cent) of the specimens. In Barrett's oesophagus,
p53
is a progression marker with high expression in high-grade
dysplasia
(89 per cent) and adenocarcinoma (83 per cent).
...
PMID:Accumulation of p53 protein in normal, dysplastic, and neoplastic Barrett's oesophagus. 773 12
The prognosis of gastric carcinoma remains unfavorable despite a greater understanding of its molecular pathology. This retrospective study of primary gastric carcinomas was collected from one of the highest risk regions of China and examined for the oncogenetic expression of
p53
, c-erbB-2, and PCNA using immunohistochemistry and DNA contents by flow cytometry and image analysis. These products are reported to influence the tumor behavior. The
p53
nuclear and c-erbB-2 membrane-bound stainings were seen in 58% and 34% of cases, respectively. A high PCNA index was found in 90% of the tumors. The
p53
expression did not correlate with the histological differentiation, gross morphology, and depth of tumor invasion. Additionally,
p53
and c-erbB-2 reactivity did not correlate with the proliferative index (PI) or S-phase DNA content. However, the mutant p53 expression was detected in the dysplastic cells adjacent to the tumor, suggesting a possible role of the oncogene in tumor pathogenesis. Mutant p53 expression can also be helpful in early detection of cases with
dysplasia
in well-differentiated adenocarcinomas.
...
PMID:Gastric carcinoma: recent issues in prognostic factors. 777 39
Aberrant
p53
immunoreactivity has been found in skin pre-malignancies and dysplasias such as Bowen's disease and actinic keratoses. Vulval lichen sclerosus (LS) has been reported to be pre-malignant, with an association of vulval carcinoma in 3% to 6% of patients. In contrast, non-genital LS appears to have no malignant potential. In this immunocytochemical study, we investigated
p53
expression in 10 cases of histologically proven vulval LS and 9 cases of non-genital LS using the murine monoclonal antibody Do-1 raised against recombinant human
p53
which reacts with both wild-type and mutant p53. None of the vulval specimens had epithelial
dysplasia
or malignancy. Normal vulval (7 cases) and non-genital skin (5 cases) were used as tissue controls, respectively. The cell proliferation index was also studied using the MIB 1 monoclonal antibody which detects the cell-cycle associated Ki-67 antigen. The technique of microwave irradiation for antigen unmasking was employed on formalin-fixed and paraffin-embedded tissues. There was a significant increase in
p53
immunoreactivity in vulval LS (32.13 +/- 15.11 epidermal cells per 100 basal cells) compared to normal vulval skin (7.52 +/- 5.04 epidermal cells per 100 basal cells) (p < 0.001), whereas the MIB 1 labelling index was lower in vulval LS (39.45 +/- 15.88 epidermal cells per 100 basal cells) than in normal controls (86.26 +/- 32.31 epidermal cells per 100 basal cells) (0.001 < p < 0.01). In contrast, there was no significant difference in
p53
immunoreactivity or MIB 1 labelling index between non-genital LS and normal controls.(ABSTRACT TRUNCATED AT 250 WORDS)
...
PMID:Altered p53 expression and epidermal cell proliferation is seen in vulval lichen sclerosus. 779 88
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