Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
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Drug
Enzyme
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Query: UNIPROT:P04637 (
p53
)
77,613
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
The Fragile Histidine Triad gene, encompassing the FRA3B fragile site at chromosome 3p14.2, is a candidate tumour suppressor gene involved in multiple tumour types including colorectal carcinomas. Recently, it has been reported that the Fragile Histidine Triad gene may be a target of damage in a fraction of mismatch deficient tumours. To explore this hypothesis, we analysed both
Fragile histidine triad
and mismatch repair protein (Msh2 and Mlh1) expression using immumohistochemical methods in 52 advanced colorectal carcinomas (19 well-, 17 moderately-, and 16 poorly-differentiated). In addition, we examined whether the
Fragile histidine triad
and mismatch repair protein expression correlated with
p53
expression and clinicopathological findings. Significant loss or reduction of
Fragile histidine triad
expression was noted in 18 of the 52 (34.6%) advanced colorectal carcinomas: 2 (10.5%) well-differentiated, 3 (17.6%) moderately-differentiated, 13 (81.3%) poorly-differentiated carcinomas, the frequency being significantly higher in the latter than that in the former two (P<0.0001). Loss of mismatch repair protein (mainly, Mlh1) expression was detected in 21 of the 52 (40.4%) colorectal carcinomas. Moreover, reduced
Fragile histidine triad
expression was significantly associated with absence of mismatch repair protein expression in the advanced colorectal carcinomas (P<0.0001). However, the
Fragile histidine triad
and mismatch repair protein expression was not significantly associated with
p53
expression. These results suggested that reduced
Fragile histidine triad
expression might be correlated with mismatch repair expression, but not with
p53
expression.
...
PMID:Reduced Fhit expression is associated with mismatch repair deficiency in human advanced colorectal carcinoma. 1217 81
Frequent loss of heterozygosity in head and neck squamous cell carcinoma (HNSCC) has been found in several chromosomal regions such as 3p, 9p, 11q, 13q and 17p.
Fragile histidine triad
(
FHIT
) gene is located at 3p14.2 encompassing a common fragile site, and is identified as a tumor suppressor gene. We examined 57 patients with HNSCC using immunohistochemistry, western blot, and reverse transcriptase polymerase chain reaction. The association between
FHIT
expression and clinicopathologic characteristics including
p53
and Ki-67 expressions was analyzed. Immunohistochemical analysis revealed 30 patients (53%) of low
FHIT
expression and 27 patients (47%) of high
FHIT
expression. Low
FHIT
expression significantly correlated with high Ki-67 expression, indicating that tumor cells with low
FHIT
expression can proliferate aggressively. No correlation was found between
FHIT
expression and clinical characteristics including age, gender, tumor size, lymph node status, stage grouping, histologic grade,
p53
expression, and prognosis.
FHIT
alteration may play an important role in cancer development of HNSCC, however it did not contribute to the prognosis.
...
PMID:Low expression of fragile histidine triad gene correlates with high proliferation in head and neck squamous cell carcinoma. 1245 22
Fragile histidine triad
(
FHIT
) is a tumour suppressor gene, which is altered in a variety of epithelial tumours, including lung cancer. Biochemical and functional pathways of its tumourigenicity are not yet understood. Its role in tumour proliferation is particularly controversial. The purpose of this study was to correlate the expression of FHIT protein in nonsmall cell lung cancer (NSCLC) with tumour proliferation as estimated by Ki-67 antigen and with
p53
, a suppressor gene.
FHIT
, Ki-67 and
p53
expression were evaluated by immunohistochemistry in 119 resected NSCLC. Altogether, 58 tumours were negative (expression <10%) for
FHIT
. The median expression in tumours was 15% positive cells, in comparison with 100% in normal matched lung tissue. The expression was as strong as in normal tissue in only 19 cases.
FHIT
expression was significantly lower in squamous cell carcinoma (SCC) (5%) than in adenocarcinoma (ADC) (64%). The median expression of Ki-67 was 20% and 69% of tumours were positives (expression >10%). Ki-67 expression was significantly higher in SCC (33.3%) than in ADC (10%). The loss of FHIT protein was not correlated with the expression of
p53
(median: 7.5%, 58% of positive tumours for a cut-off of 10% of positive cells) or Ki-67. But percentage of labelled cells for
p53
and Ki-67 were significantly correlated. The results suggest that for fragile histidine triad, the pathway of tumourigenesis is independent of
p53
and of tumoural proliferation, as reported previously in vitro.
...
PMID:Fragile histidine triad protein expression in nonsmall cell lung cancer and correlation with Ki-67 and with p53. 1276 16
Fragile histidine triad
(
FHIT
), a candidate of tumor suppressor protein, expression was examined on paraffin-embedded specimens in proliferative, secretory, hyperplastic, and neoplastic human endometrium by immunohistochemistry. The results of
FHIT
immunoreactivity in endometrial carcinomas were compared with prognostic indicators as well as with
p53
overexpression. Forty-four cases of endometrial carcinoma, 30 normal functional (15 proliferative, 15 secretory), and 24 hyperplastic endometrium (12 without atypia, 12 with atypia) specimens were studied using polyclonal
FHIT
antibody. The streptavidin-biotin-peroxidase detection system was used, and the intensity and the distribution of immunoreactivity were evaluated semiquantitatively. There were no significant differences in
FHIT
expression in the proliferative, secretory, hyperplastic, either with or without atypia, or carcinomatous endometria. No significant difference in
FHIT
expression of endometrial carcinomas was detected when prognostic parameters or
p53
overexpression were considered. Loss or reduced
FHIT
expression was not found to predict disease-free or cumulative survivals. This study showed that loss or reduction in FHIT protein expression is present in normal functional and hyperplastic endometria as well as in neoplastic endometrium. FHIT protein seems not to be involved directly in endometrial carcinogenesis, but rather, it regulates cell proliferation both in physiologic and in pathologic conditions of endometrium.
...
PMID:FHIT expression in neoplastic, hyperplastic, and normal endometrium. 1634 85
Fragile histidine triad
(
FHIT
) serves a critical function as a tumor suppressor that inhibits
p53
degradation by mouse double minute 2 (MDM2). The functional domains of
FHIT
involved in tumor inhibition was interpreted.
In-silico
screening data were employed to construct truncated forms of
FHIT
to assess their cytotoxic effects on the HT1080 cell line. Full
FHIT
expression was confirmed by western blotting and expression of two
FHIT
truncates were confirmed by RT-PCR. Transfection of these truncated forms into HT1080 cells showed that the N-terminal truncated form (amino acids 17-102) better inhibited proliferation than the full-length
FHIT
. The combined effects of these truncated forms augmented doxorubicin-induced cytotoxicity. Functional analysis demonstrated that these fragments and their combination with doxorubicin can arrest cells in the G2 phase of the cell cycle as specified by flow cytometry. The
FHIT
functional domains can be used as lead compounds for development of drug designs and gene transfer for cancer therapy.
...
PMID:N-Terminal Domain of Fragile Histidine Triad Exerts Potent Cytotoxic Effect in HT1080 Cells and Increases Doxorubicin Cytotoxicity. 3108 60
