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Target Concepts:
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Query: EC:3.4.24.35 (
matrix metalloproteinase 9
)
2,207
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
K-1735 clones 10 and M2 are cell lines cloned from a UV-induced murine melanoma. While both lines are highly tumorigenic, only the M2 cells are highly invasive in vitro and metastatic in vivo. Here we have exposed the
clone 10
cells to the synthetic peptide PA22-2, which contains the IKVAV sequence from the A chain of laminin and which, like laminin, induces
collagenase IV
production and enhances metastasis formation by B16F10 cells. Zymogram analysis of conditioned media from
clone 10
cells cultured on the peptide demonstrated a dose-dependent increase in
collagenase IV
activity. When
clone 10
cells were cultured on a reconstituted basement membrane (Matrigel), this peptide caused an invasive phenotype comparable to the M2 cells. The invasive
clone 10
cells were, however, unable to form lung colonies in vivo in the presence of this peptide. We conclude that this peptide represents an active site on laminin which is able to stimulate the invasiveness of this tumor cell line, but that this activity is not sufficient to confer metastatic potential.
...
PMID:Induction of an invasive phenotype in benign tumor cells with a laminin A-chain synthetic peptide. 129 29
The purpose of this study was to correlate abnormalities in chromosome 14 with the invasive metastatic phenotype of K-1735 murine melanoma cells. Low metastatic K-1735
clone 10
and clone 23 cells were transfected with either basic fibroblast growth factor (bFGF), Kaposi's fibroblast growth factor (kFGF), or c-H-ras gene. A high number of bFGF- and H-ras-transfected cells exhibited chromosome 14 rearrangements. These cells also had increased expression of
collagenase IV
. The kFGF-transfected cells were highly metastatic but did not have increased expression of
collagenase type IV
. The kFGF-transfected cells were highly metastatic but did not have increased expression of
collagenase type IV
, nor abnormalities in chromosome 14. The data imply that karyotypic changes in chromosome 14 are associated with increase expression of
collagenase type IV
.
...
PMID:Chromosome 14 alteration is associated with increased collagenase expression and the metastatic potential of murine melanomas. 895 75
