Articles
Register for Fra-1 Governs Cell Migration via Modulation of CD44 Expression in Human Mesotheliomas
Maria E. Ramos-Nino , Steven R Blumen and Brooke T Mossman
Molecular Cancer
2007
A BMC open access
research article
Published: 21 December 2007
Abstract (provisional)
Silencing of Fra-1, a component of the dimeric transcription factor, activator
protein-1 (AP-1), inhibits mRNA expression of c-met and cd44 in rat mesothelioma
cells and is causally linked to maintenance of the transformed phenotype.
However, the mechanisms of Fra-1 regulation and Fra-1 regulated gene expression
in human malignant mesothelioma (MM) are unclear. We first show in a panel of
human MM cells that Fra-1 mRNA expression in MM is complex and regulated by
extracellular signal-regulated kinase (ERK1, ERK2), Src, and
phosphatidyl-inositol-3-kinase (PI3K) pathways in a tumor-specific fashion. Cell
lines with PI3K-dependent Fra-1 expression were SV40 positive and expressed the
lowest basal Fra-1 levels. Levels of Fra-1 expression correlated with amounts of
CD44 expression that were greater in simian virus 40 negative (SV40-) MM cells.
Using dominant negative (dn), short hairpin (sh) and small interference (si) RNA
constructs, we next demonstrate that expression of CD44, the principal
hyaluronic receptor in MMs, correlates with Fra-expression in both simian virus
40 positive (SV40+) and SV40- MMs. Moreover, both Fra-1 and CD44 expression are
linked to cell migration in SV40- MM cells. Lastly, in contrast to normal lung
tissue, tissue microarrays revealed that Fra-1 was expressed in 33 of 34 human
MMs, and that all CD44+ tumors were SV40-. These results suggest that Fra-1 is
associated with cell migration in human MMs and that Fra-1 modulation of CD44
may govern migration of selected MMs.
The complete article is available as a
provisional PDF.
The fully formatted PDF and HTML versions are in production
Molecular Cancer 2007, 6:81doi:10.1186/1476-4598-6-81
Open Access
