Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Query: UNIPROT:P04637 (
p53
)
77,613
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
To study the oncogenesis of human esophageal
carcinoma
, the presence of DNA sequences homologous to several DNA tumor viruses and the expression of oncogenes and growth factor genes were examined in two esophageal
carcinoma
cell lines of Chinese origin, CE48T/VGH and CE81T/VGH. Southern blot analyses failed to detect sequences homologous to hepatitis B virus (HBV), Epstein-Barr virus (EBV), herpes simplex virus type 2 (HSV-2), cytomegalovirus (CMV) or human papilloma virus (HPV) genomes. Northern blot analyses revealed that c-myc, c-src, c-H-ras, c-abl, c-sis, and
p53
genes were expressed. In addition, transcripts of transforming growth factor alpha (TGF alpha), TGF beta, and platelet derived growth factor A (PDGF A) genes were detected. These studies suggest that DNA tumor viruses may not be involved in the carcinogenesis of esophageal
carcinoma
. However, cooperation among different oncogenes and the production of growth factors may play an important role in that carcinogenesis.
...
PMID:Absence of genomes of DNA tumor viruses and expression of oncogenes and growth factors in two esophageal carcinoma cell lines of Chinese origin. 147 73
Anaplastic carcinoma of the thyroid gland, which is one of the most aggressive, malignant tumors in humans, is considered to originate from preexisting differentiated thyroid cancer. To define the genetic alterations associated with such progression, we examined nine cases of anaplastic thyroid
carcinoma
for mutation in exons 4-9 of the
p53 tumor suppressor
gene. Preliminary screening for mutation by RNase protection analysis demonstrated that two out of nine anaplastic carcinomas contained sequence alterations in the
p53
gene. Subsequent DNA sequencing identified the mutated nucleotides in these two cases; one was a nonsense mutation at codon 165, and the other was a single-base deletion at codon 176 resulting in the creation of a stop codon downstream due to frameshift. The fact that no mutations were detected in coexisting foci of papillary carcinomas from the same patients shows that these mutations of the
p53
gene occurred after development of papillary carcinomas. These results suggest that
p53
gene mutation triggers the progression from differentiated into anaplastic
carcinoma
in the human thyroid gland.
...
PMID:p53 gene mutations associated with anaplastic transformation of human thyroid carcinomas. 148 45
Dominant-negative and/or loss-of-function mutations of the
p53 tumor suppressor
gene are frequently found in squamous cell carcinomas of the skin and of the head-and-neck region. In order to identify the precise mechanisms of inactivation of
p53
in tumors of this class, we examined the status of
p53
RNA, protein and DNA in a panel of eight human squamous
carcinoma
cell lines (head-and-neck, 3; esophagus, 1; lung, 1; uterine cervix, 2; vulva, 1). Three lines (A253, CaLu-1, SqCC/Y1) failed to express any
p53 mRNA
. A253 cells contained a single
p53
allele without mutations in exons 2-9, suggesting that the lack of transcription was the result of mutations in the regulatory region of the gene. Both
p53
alleles were deleted in CaLu-1 cells, whereas the single allele present in SqCC/Y1 cells was rearranged and carried two missense mutations in exon 5. Two cell lines (A431, FaDu) expressed only 50% of the normal level of
p53 mRNA
, either because only one allele was present (A431), or because only one of the two alleles was transcribed (FaDu). The two cervical
carcinoma
lines (CaSki, C4-1) expressed normal levels of
p53 mRNA
, but no wild type protein, presumably as a result of accelerated degradation by the human papillomavirus 16 or -18 E6 oncoprotein present in these cells as previously described (Scheffner et al., Proc. Natl. Acad. Sci. USA 88:5523-5527; 1991). Three of the lines expressed only mutant p53 protein (A431, FaDu, CE-48) resulting from missense mutations in codons 248 and 273.(ABSTRACT TRUNCATED AT 250 WORDS)
...
PMID:Status of the p53 tumor suppressor gene in human squamous carcinoma cell lines. 148 18
Although
carcinoma
of the uterine endometrium is the most frequently diagnosed malignancy of the female reproductive tract, the molecular genetic features of this tumor have yet to be described in significant detail. Since mutations of the
p53 tumor suppressor
gene are the single most common genetic alteration found in human malignancies, we examined the hypothesis that
p53
mutations occur in human endometrial carcinoma. Sequencing analysis of exons 5-8 revealed point mutations in 3 of 21 (14%) tumors; one mutation was an unusual single-base insertion at codons 176-177, resulting in a premature stop codon, whereas the other two were CGG----TGG transitions at codon 248. Two of these tumors showed reduction to homozygosity at the
p53
allele, but one tumor apparently retained heterozygosity. These data indicate that
p53
mutations occur in human endometrial carcinoma, although relatively infrequently, and that loss of the normal
p53
allele does not necessarily occur with point mutation of the
p53
gene in this tumor type.
...
PMID:p53 gene mutations in human endometrial carcinoma. 149
In the search for sensitive and specific tumor markers for bladder
carcinoma
, expression of various oncogenes and gene products (such as c-erb B-2,
p53
) and epidermal growth factor receptor merits particular attention. Although the results are not yet conclusive, important predictive markers are about to emerge from ongoing studies in this field. Bacillus Calmette-Guerrin treatment in superficial bladder cancer is probably the most successful immunotherapy in humans. But there is still a large knowledge deficit in the issues of optimal dose schedule and mechanisms of action. Although promising results of neoadjuvant chemotherapy in patients with invasive bladder cancers are reported, we must be cautious about changing our conventional approach until the results of large scale, controlled, randomized studies evaluating the survival are published.
...
PMID:Bladder cancer. 149 53
Human breast
carcinoma
MCF-7 cells seeded on type I collagen-coated dishes were provided with an anchor via the collagen receptor, integrin, and grew as actively as those in plastic tissue culture dishes. In contrast, cells seeded on a layer of soft agar became anchorage-deficient and their growth was significantly inhibited, although the cell viability and the cell cycle distribution were unaffected. Immunoprecipitation analysis revealed that mutant p53 was phosphorylated at tyrosine in the anchorage-provided cells. In contrast, the
p53
in the anchorage-deficient cells was present in 2-fold greater amount, but was phosphorylated to a lesser extent. Addition of a potent protein-tyrosine kinase inhibitor, herbimycin A, to the anchorage-provided cells caused an elevated level of
p53
, and inhibitions of cell proliferation and
p53
phosphorylation, without interfering with the cell adhesion to the substratum. These results demonstrated that the growth inhibition by anchorage-deficiency or by herbimycin A is associated with an elevated
p53
level and reduced
p53
phosphorylation at tyrosine.
...
PMID:Growth inhibition by anchorage-deficiency is associated with increased level but reduced phosphorylation of mutant p53. 150 70
The molecular genetics of colorectal
carcinoma
are among the best understood of any common human cancer. Reported molecular genetic abnormalities involve tumor-suppressor genes that undergo inactivation (e.g., apc, mcc, dcc,
p53
, and possibly genes on chromosomes 8p, 1p, and 22q) and dominant-acting oncogenes (e.g., ras, src, and myc). Multiple clonal genetic abnormalities accumulate during the development of colorectal
carcinoma
in adenomas. Altered DNA methylation is an early event, and the specific genetic alterations occur in a preferential order. However, the clinical application of molecular genetics in patients who are at risk for or have colorectal
carcinoma
is in its infancy. Patients with a predisposition to colorectal
carcinoma
caused by inheritance of familial adenomatous polyposis can be identified by genetic analysis of the apc gene on chromosome 5q21. In patients who undergo curative resection of colorectal cancer, deletion of the
p53
gene on chromosome 17p, deletion of the dcc gene on 18q, and high fractional allelic loss (fraction of nonacrocentric autosomal arms with deletion) in the primary tumor appear to indicate an increased likelihood of occult disseminated disease and thus a poor prognosis. Additional studies are needed to establish the role of the molecular genetics of colorectal
carcinoma
in the management of patients who are at risk for or already have neoplasia of the large bowel.
...
PMID:Molecular genetics of colorectal carcinoma. 151 69
Alterations in the
p53 tumor suppressor
gene and Epstein-Barr virus status were investigated in 15 nasopharyngeal
carcinoma
(NPC) biopsies, 4 xenografts, and 2 cell lines from the Cantonese region of southern China. One other established NPC cell line obtained from a northern Chinese patient was also studied. Restriction fragment length polymorphism analysis revealed a loss of heterozygosity for chromosome 17p, where the
p53
gene resides, in only one of 15 NPC biopsies. Polymerase chain reaction-single-stranded conformational polymorphism analysis and direct sequencing failed to detect sequence alterations in exons 5 through 8 of the
p53
gene in the 15 tumors and in the 4 NPC xenografts, all of which tested positive for Epstein-Barr virus. In contrast, the 3 NPC cell lines were all negative for Epstein-Barr virus and contained G----C transversions in the
p53
gene, with cell lines CNE-1 and CNE-2 harboring identical AGA (arginine) to ACA (threonine) changes at codon 280. These results suggest that
p53
inactivation is not a necessary component of nasopharyngeal carcinogenesis in Cantonese but may be important in the establishment of cell lines derived from these tumors.
...
PMID:Absence of p53 gene mutations in primary nasopharyngeal carcinomas. 151 42
To elucidate the molecular basis for endocrine tumorigenesis,
p53
mutations in human endocrine tumors were analyzed by using polymerase chain reaction-single strand conformation polymorphism. Exons 5 through 10 of the
p53
gene were studied in genomic DNAs from 134 primary endocrine tumors and 6 human endocrine cancer-derived cell lines. Mutations were detected and identified in 4 endocrine tumors, including one parathyroid adenoma and three thyroid
carcinoma
cell lines. The sites of these mutations were in exons 5 (codon 151 and 152) and 7 (codon 248 and 255). In all of three tumor cell lines, but not in a parathyroid adenoma, the normal allele encoding the
p53
gene was lost. However,
p53
mutations were not found in any other endocrine tumors or cell lines. Based upon these results, we concluded that the
p53
gene may play a role in the tumorigenesis of a limited number of parathyroid adenoma and thyroid cancers, and that the
p53
mutation with an allelic loss of the
p53
gene is an important factor in malignant tumorigenesis of the thyroid gland.
...
PMID:Role of p53 mutations in endocrine tumorigenesis: mutation detection by polymerase chain reaction-single strand conformation polymorphism. 151 62
We have studied expression of
p53
, a tumor suppressor gene, by using both immunohistochemistry and in situ hybridization in 20 cases of squamous cell carcinoma of the esophagus. Immunohistochemical analysis was performed by using monoclonal antibody pAb1801. Immunoreactive
p53
was observed in the nuclei of the tumor cells in 17 cases. We used 35S-labeled anti-sense single-stranded synthetic oligonucleotide probe ON102, which hybridized with DNA sequence near the 5' end of
p53
, for in situ hybridization. In all the cases of invasive squamous cell carcinoma studied, no significant accumulation of
p53
hybridization signals was observed in
carcinoma
cells. This result indicates that overexpression of
p53
observed by immunohistochemical staining is not due to an increase in the steady-state level of
p53 mRNA
in frank
carcinoma
cells. In six cases of morphologically normal esophageal mucosa distant from
carcinoma
, accumulation of hybridization signals was observed in basal and parabasal cells of the mucosa. The mucosa of these cases was negative for
p53
immunoreactivity except for one case showing sporadic positivity. Accumulation of hybridization signals was observed in foci of squamous dysplasia not associated with invasion in three cases.
...
PMID:In situ hybridization and immunohistochemistry of p53 tumor suppressor gene in human esophageal carcinoma. 151 62
<< Previous
1
2
3
4
5
6
7
8
9
10
Next >>
