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Target Concepts:
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Query: UMLS:C0033036 (
APC
)
10,214
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
The molecular genetic alterations in colorectal carcinoma are among the best understood of any common human cancer. Identified abnormalities include both dominant-acting oncogenes (ras, myc, src) and suppressor genes which undergo inactivation or deletion (
deleted in colorectal carcinoma
gene [DCC], p53, adenomatous polyposis coli gene [
APC
], and probably loci on chromosomes 1p and 22q). Accumulation of multiple abnormalities is evident in the adenoma-carcinoma sequence with a preferential order, and alteration of DNA methylation is an especially early event. Identification of molecular genetic markers useful for classification and staging of colorectal carcinoma is in its infancy. Deletion of the p53 gene on chromosome 17p, deletion of the DCC gene on 18q, and high fractional allelic loss (fraction of evaluable nonacrocentric autosomal arms with deletion) have been associated with distant metastases and with poorer prognosis in patients without initial evidence of disseminated disease. Additional studies are needed to determine the possible role of these alterations in clinical management.
...
PMID:Molecular genetic alterations as potential prognostic indicators in colorectal carcinoma. 154 Sep
Accumulating evidences that carcinogenesis requires multiple gene alterations of oncogenes and tumor suppressor genes have recently emerged. In addition, genes related to invasion and metastasis are also important in understanding development of colorectal cancer. In this study, clinical significance and application of tumor suppressor genes and invasion related genes such as
APC
(adenomatous polyposis coli), DCC (
deleted in colorectal carcinoma
) tumor suppressor genes and invasion related gene, matrilysin were studied. In the mouse tumor induced by mutagen contained in cooked food, PhIP (2-amino-1-methyl-6- phenylimidazo [4,5-b] pyridine), nonsense mutations of
APC
gene that is similar to human colorectal cancer have been observed. These results suggested the quite interesting issue of mutagen contained in daily food having etiological role of colorectal cancer. DCC gene alteration, decreased expression of DCC mRNA was detected in 60% of advanced colorectal cancer. In all cases with liver metastasis, DCC expression was absent or markedly decreased, a finding that detection of DCC expression have an clinical importance that predicts metastatic potential of colorectal cancer. Matrilysin, the member of MMPs (matrix metalloproteinases) which degrade matrix components such as type IV collagen, laminin or fibronectin. In most of colorectal cancer, matrilysin was overexpressed in tumor cells. Matrilysin-transfected colorectal cancer cells showed more invasive ability in vitro and gained metastatic potential in SCID mice. Suppression of matrilysin expression by treated with all-trans retinoic acid (ATRA) or introduction of anti-sense matrilysin decreased the invasive ability in vitro. This result suggests that matrilysin plays an important role in invasion and metastasis and have a possibility of new anti-invasion therapy.
...
PMID:[Genetic diagnosis of colorectal cancer]. 872 69
The role of
deleted in colorectal carcinoma
(
DCC
) as a tumour suppressor has been a matter of debate for the past 15 years.
DCC
gene expression is lost or markedly reduced in the majority of advanced colorectal cancers and, by functioning as a dependence receptor,
DCC
has been shown to induce apoptosis unless engaged by its ligand, netrin-1 (ref. 2). However, so far no animal model has supported the view that the
DCC
loss-of-function is causally implicated as predisposing to aggressive cancer development. To investigate the role of
DCC
-induced apoptosis in the control of tumour progression, here we created a mouse model in which the pro-apoptotic activity of
DCC
is genetically silenced. Although the loss of
DCC
-induced apoptosis in this mouse model is not associated with a major disorganization of the intestines, it leads to spontaneous intestinal neoplasia at a relatively low frequency. Loss of
DCC
-induced apoptosis is also associated with an increase in the number and aggressiveness of intestinal tumours in a predisposing
APC
mutant context, resulting in the development of highly invasive adenocarcinomas. These results demonstrate that
DCC
functions as a tumour suppressor via its ability to trigger tumour cell apoptosis.
...
PMID:DCC constrains tumour progression via its dependence receptor activity. 2215 21
