Gene/Protein
Disease
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Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
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Target Concepts:
Gene/Protein
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Query: UMLS:C0677930 (
primary tumor
)
20,210
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
SEMA3F
, isolated from a 3p21.3 deletion, has antitumor activity in transfected cells, and protein expression correlates with tumor stage and histology. In primary tumors,
SEMA3F
and VEGF surface staining is inversely correlated. Coupled with
SEMA3F
at the leading edge of motile cells, we previously suggested that both proteins competitively regulate cell motility and adhesion. We have investigated this using the breast cancer cell line, MCF7.
SEMA3F
inhibited cell attachment and spreading as evidenced by loss of lamellipodia extensions, membrane ruffling, and cell-cell contacts, with cells eventually rounding-up and detaching. In contrast, VEGF had opposite effects. Although
SEMA3F
binds NRP2 with 10-fold greater affinity than NRP1, the effects in MCF7 were mediated by NRP1. This was determined by receptor expression and blocking of anti-NRP1 antibodies. Similar effects, but through NRP2, were observed in the C100 breast cancer cell line. Although we were unable to demonstrate changes in total GTP-bound Rac1 or RhoA, we did observe changes in the localization of Rac1-GFP using time lapse microscopy. Following
SEMA3F
, Rac1 moved to the base of lamellipodia and - with their collapse - to the membrane. These results support the concept that
SEMA3F
and VEGF have antagonistic actions affecting motility in
primary tumor
cell.
...
PMID:Semaphorin SEMA3F and VEGF have opposing effects on cell attachment and spreading. 1265 73
Previously, we demonstrated that loss of
SEMA3F
, a secreted semaphorin encoded in 3p21.3, is associated with higher stages in lung cancer and
primary tumor
cells studied with anti-vascular endothelial growth factor (VEGF) and
SEMA3F
antibodies. In vitro,
SEMA3F
inhibits cell spreading; this activity is opposed by VEGF. These results suggest that VEGF and
SEMA3F
compete for binding to their common neuropilin receptor. In the present report, we investigated the attractive/repulsive effects of
SEMA3F
on cell migration when cells were grown in a three-dimensional system and exposed to a
SEMA3F
gradient. In addition, we adapted the neurobiologic stripe assay to analyze the migration of tumor cells in response to
SEMA3F
. In the motile breast cancer cell line C100, which expresses both neuropilin-1 (NRP1) and neuropilin-2 (NRP2) receptors,
SEMA3F
had a repulsive effect, which was blocked by anti-NRP2 antibody. In less motile MCF7 cells, which express only NRP1,
SEMA3F
inhibited cell contacts with loss of membrane-associated E-cadherin and beta-catenin without motility induction. Cell spreading and proliferation were reduced. These results support the concept that in a first step during tumorigenesis, normal tissues expressing
SEMA3F
would try to prevent tumor cells from spreading and attaching to the stroma for further implantation.
...
PMID:Semaphorin SEMA3F has a repulsing activity on breast cancer cells and inhibits E-cadherin-mediated cell adhesion. 1580 23
