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: UMLS:C0699790 (
colon cancer
)
28,837
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
The membrane-bound serine proteinase
matriptase
, which is often released from the plasma membrane of epithelial and carcinoma cells, has been implicated to play important roles in both physiological and pathological conditions. However, the regulatory mechanism of its activity is poorly understood. In the present study, we examined expression and activation state of soluble
matriptase
in 24 human cancer cell lines. Soluble
matriptase
was detected in the conditioned media from all of 5 colon and 4 breast carcinoma cell lines and 8 of 10 stomach carcinoma cell lines tested. Only two of five lung cancer cell lines released the
matriptase
protein into the culture media. Out of the five
matriptase
-negative cell lines, two cell lines expressed the
matriptase
mRNA. Among 24 cancer cell lines tested, 13 cell lines secreted trypsin in an active or latent form and all of them released
matriptase
. Most of the 24 cell lines released a latent, single-chain
matriptase
of 75 kDa as a major form, as well as low levels of complex forms of an activated two-chain enzyme with its specific inhibitor HAI-1. Thus, these soluble matriptases appeared to have little proteolytic activity. Treatment of stomach and
colon cancer
cell lines with epidermal growth factor stimulated the release of matripatase/HAI-1 complexes. In cancer cell lines secreting active trypsin, however,
matriptase
was released mostly as an inhibitor-free, two-chain active form. Trypsin seemed to activate the membrane-bound, latent
matriptase
on the cell surface. These results suggest that
matriptase
and trypsin cooperatively function for extracellular proteolysis.
...
PMID:Production of soluble matriptase by human cancer cell lines and cell surface activation of its zymogen by trypsin. 1583 73
Proteases responsible for the increased peritumoral proteolysis associated with cancer represent functional biomarkers for monitoring tumorigenesis. One attractive extracellular biomarker is the transmembrane serine protease
matriptase
. Found on the surface of epithelial cells, the activity of
matriptase
is regulated by its cognate inhibitor hepatocyte growth factor activator inhibitor-1 (HAI-1). Quantitative mass spectrometry allowed us to show that, in selected cancers, HAI-1 expression decreases, leading to active
matriptase
. A preclinical probe specific for the measurement of emergent active
matriptase
was developed. Using an active-site-specific, recombinant human antibody for
matriptase
, we found that the selective targeting of active
matriptase
can be used to visualize the tumorigenic epithelium. Live-cell fluorescence imaging validated the selectivity of the antibody in vitro by showing that the probe localized only to cancer cell lines with active
matriptase
on the surface. Immunofluorescence with the antibody documented significant levels of active
matriptase
in 68% of primary and metastatic colon cancer sections from tissue microarrays. Labeling of the active form of
matriptase
in vivo was measured in human
colon cancer
xenografts and in a patient-derived xenograft model using near-infrared and single-photon emission computed tomography imaging. Tumor uptake of the radiolabeled antibody, (111)In-A11, by active
matriptase
was high in xenografts (28% injected dose per gram) and was blocked in vivo by the addition of a
matriptase
-specific variant of ecotin. These findings suggest, through a HAI-1-dependent mechanism, that emergent active
matriptase
is a functional biomarker of the transformed epithelium and that its proteolytic activity can be exploited to noninvasively evaluate tumorigenesis in vivo.
...
PMID:Imaging a functional tumorigenic biomarker in the transformed epithelium. 2324 18
The binding of hepatocyte growth factor (HGF) to its receptor MET activates a signaling cascade that promotes cell survival, proliferation, cell scattering, migration and invasion of malignant cells. HGF is secreted by cancer cells or by tumor-associated fibroblasts as pro-HGF, an inactive precursor. A key step in the regulation of HGF/MET signaling is proteolytic processing of pro-HGF to its active form by one of the three serine proteases,
matriptase
, hepsin or HGF activator (HGFA).We developed SRI 31215, a small molecule that acts as a triplex inhibitor of
matriptase
, hepsin and HGFA and mimics the activity of HAI-1/2, endogenous inhibitors of HGF activation. We demonstrated that SRI 31215 inhibits fibroblast-induced MET activation, epithelial-mesenchymal transition and migration of cancer cells. SRI 31215 overcomes primary resistance to cetuximab and gefitinib in HGF-producing
colon cancer
cells and prevents fibroblast-mediated resistance to EGFR inhibitors. Thus, SRI 31215 blocks signaling between cancer cells and fibroblasts and inhibits the tumor-promoting activity of cancer-associated fibroblasts.Aberrant HGF/MET signaling supports cell survival, proliferation, angiogenesis, invasion and metastatic spread of cancer cells, establishing HGF and MET as valid therapeutic targets. Our data demonstrate that inhibitors of HGF activation, such as SRI 31215, merit investigation as potential therapeutics in tumors that are addicted to HGF/MET signaling. The findings reported here also indicate that inhibitors of HGF activation overcome primary and acquired resistance to anti-EGFR therapy, providing a rationale for concurrent inhibition of EGFR and HGF to prevent therapeutic resistance and to improve the outcome of cancer patients.
...
PMID:Inhibition of pro-HGF activation by SRI31215, a novel approach to block oncogenic HGF/MET signaling. 2712 Oct 52
