6 research outputs found
COL11A1 in FAP polyps and in sporadic colorectal tumors
BACKGROUND: We previously reported that the α-1 chain of type 11 collagen (COL11A1), not normally expressed in the colon, was up-regulated in stromal fibroblasts in most sporadic colorectal carcinomas. Patients with germline mutations in the APC gene show, besides colonic polyposis, symptoms of stromal fibroblast involvement, which could be related to COL11A1 expression. Most colorectal carcinomas are suggested to be a result of an activated Wnt- pathway, most often involving an inactivation of the APC gene or activation of β-catenin. METHODS: We used normal and polyp tissue samples from one FAP patient and a set of 37 sporadic colorectal carcinomas to find out if the up-regulation of COL11A1 was associated with an active APC/β-catenin pathway. RESULTS: In this study we found a statistically significant difference in COL11A1 expression between normal tissue and adenomas from one FAP patient, and all adenomas gave evidence for an active APC/β-catenin pathway. An active Wnt pathway has been suggested to involve stromal expression of WISP-1. We found a strong correlation between WISP-1 and COL11A1 expression in sporadic carcinomas. CONCLUSIONS: Our results suggest that expression of COL11A1 in colorectal tumors could be associated with the APC/β-catenin pathway in FAP and sporadic colorectal cancer
Gene expression in carcinogenesis
It is important to understand the processes of carcinogenesis and to find
out which genes are involved . One way to study the process on a
molecular basis is to identify differences in gene expression. The method
mRNA differential display was used to compare normal tissues to different
cancer tissues and cell lines in three different experiments to study
migration, colon cancer and breast cancer.
The first experiment was designed to isolate genes involved in migration
of cancer cells by studying glioma cells migrating on different matrices
in vitro. In the internal experiment a novel gene, C7, was upregulated in
cells migrating on laminin and was isolated and cloned. C7 is the
homologue of Drosophila L82, a late puff gene and human OXR1, a gene,
which protects cells against oxidation. Additional members of this novel
gene family are found in a number of eukaryotic species. In the adult,
the C7 gene is most highly expressed in brain and testis. It is
upregulated in a cancer cell line, SW480, and a prostate cancer cell
line. C7 has at least 4 transcripts expressed in the mouse embryo and was
localized to the nucleoli of the cell, by immunohistochemistry,
suggesting that it may be involved in the formation or function of this
important organelle.
In the next experiment, colorectal cancer tissue was compared with normal
colon mucosa. The alpha- chain of type 11 collagen (COL11A1) was found to
be upregulated and the water channel protein aquaporin 8 (A QP8) was down
regulated in colorectal cancer.
COL11A is normally not expressed in colon but was here shown to be
expressed in 79% of the colorectal carcinomas. Analyses of other
collagens showed that COL5A2 was not expressed in normal colon but was
co-expressed with COL11A1 in the tumors, suggesting that stromal
expression of COL11A1 and COL5A2 is associated with malignancy in
colorectal cancer. Patients with germline mutations in the APC gene show,
besides colonic polyposis, symptoms of stromal fibroblast involvement,
which could be related to COL11A1 expression. To find out if the COL11A
was an early event in the carcinogenesis, 14 polyps from one FAP patient
were studied. A weak, though statistically significant upregulation in
COL11A1 expression was found in adenomas from one FAP patient. It was
suggested that expression of COL11A1 in colorectal tumors is associated
with the APC pathway in FAP and perhaps also in sporadic colorectal
cancer.
In situ hybridization demonstrated that AQP8 was expressed in the cells
facing the lumen in the normal colonic epithelium. These cells are the
mature cells of the migrating epithelial cells of the colon crypt. The
result suggests that the expression of AQP8 is a marker of normal
proliferating colonic epithelial cells and that tumors arise in cells not
expressing this protein.
In the third experiment, differential display was used to compare breast
cancer tissue, breast cancer cell lines and two normal breast cell lines.
The cyclin D2 gene was downregulated in the tumor tissues and in the
cancer cell lines. Significantly low cyclin D2 expression was seen in
10/39 (25%) sporadic breast cancers, and in 38/70 (54%) of familial
breast cancers. In total, low expression was seen in 48/109 (44%) tumors.
In order to find the explanation for the down-regulation of cyclin D2 we
screened for inactivating mutations in tumors with low expression and
studied methylation of the promoter region in breast cancer cell lines.
Growth factors were used in an attempt to stimulate cell lines to express
cyclin D2, and we transfected the cell lines with a vector expressing
cyclin D2. The results suggest that methylation could be associated with
the low expression of cyclin D2 in breast cancer
<it>COL11A1</it> in FAP polyps and in sporadic colorectal tumors
Abstract Background We previously reported that the α-1 chain of type 11 collagen (COL11A1), not normally expressed in the colon, was up-regulated in stromal fibroblasts in most sporadic colorectal carcinomas. Patients with germline mutations in the APC gene show, besides colonic polyposis, symptoms of stromal fibroblast involvement, which could be related to COL11A1 expression. Most colorectal carcinomas are suggested to be a result of an activated Wnt- pathway, most often involving an inactivation of the APC gene or activation of β-catenin. Methods We used normal and polyp tissue samples from one FAP patient and a set of 37 sporadic colorectal carcinomas to find out if the up-regulation of COL11A1 was associated with an active APC/β-catenin pathway. Results In this study we found a statistically significant difference in COL11A1 expression between normal tissue and adenomas from one FAP patient, and all adenomas gave evidence for an active APC/β-catenin pathway. An active Wnt pathway has been suggested to involve stromal expression of WISP-1. We found a strong correlation between WISP-1 and COL11A1 expression in sporadic carcinomas. Conclusions Our results suggest that expression of COL11A1 in colorectal tumors could be associated with the APC/β-catenin pathway in FAP and sporadic colorectal cancer.</p