PHILADELPHIA, Nov 16, 2009 (ASCRIBE NEWS via COMTEX) -- Targeting the normal
cells that surround cancer cells within and around a tumor is a strategy that
could greatly increase the effectiveness of traditional anti-cancer treatments,
say researchers at The Wistar Institute.
In the Journal of Clinical Investigation published online November 16, they
demonstrate the critical role for fibroblast activation protein (FAP), expressed
by one type of these so-called "stromal" cells, in promoting tumor growth in
mice. Genetically deleting or therapeutically targeting FAP significantly
reduced the rate of tumor growth in mice by interrupting or blocking important
signaling pathways and biological processes required for tumor growth, the
Wistar team found.
"It's like taking away the soil from a seed that wants to grow," says senior
author Ellen Pure, Ph.D., a professor in the Molecular and Cellular Oncogenesis
Program at Wistar. "These results provide a proof-of-principle that targeting
and modifying a tumor's microenvironment may be an effective approach to
treating solid tumors."
Tumors are a complex mix of neoplastic cancer cells and normal cells -
inflammatory and immune cells, endothelial cells, fibroblasts, pericytes, and
others, collectively known as stromal cells. In addition, a web-like
extracellular matrix is created by the stromal cells, and its structure is
important for supporting and nurturing tumor growth through molecular signaling
pathways.
The Wistar team focused on fibroblasts and pericytes. In addition to
synthesizing components of the extracellular matrix, fibroblasts associated with
tumors also express FAP, a particular protease that cuts up other proteins while
pericytes are important to the function of the new blood vessels that develop in
tumors. FAP is expressed in 90 percent of all human epithelial (solid) cancers,
and FAP expression is recognized as a marker for and is thought to play a role
in cancer growth, but the mechanisms through which this occurs had been
previously unknown.
"Our data clearly demonstrate that FAP indeed promotes the growth of colon
cancer as well as lung cancer in animal models, and provide insight into how FAP
works," says Pure. To explore how FAP promotes tumor growth, lead author
Angelica Santos, Ph.D., and colleagues took two approaches - genetic deletion
and pharmacologic targeting of FAP to determine the effects of deactivating FAP
in mouse models of lung and colon cancer.
First, they examined the genetic deletion of FAP. In collaboration with Wistar
assistant professor and co-author Joseph Kissil, Ph.D., they mated mice
engineered to spontaneously develop lung cancer when their K-Ras gene is
activated with mice whose FAP gene had been deleted to develop a new strain of
mice with a genetic deletion of FAP and expressing an activated K-Ras gene.
The Wistar team found that lung tumor growth was substantially inhibited in
these mice. In another experiment the investigators transplanted colon cancer
cells into FAP-deficient mice and saw a similarly marked inhibition of tumor
growth.
"We found that FAP inactivation disrupts the organization of the collagen fibers
which are a key component of matrix and that could be critical for many things,
including cell to cell communication, cell-matrix interactions and development
of new blood vessels to feed the tumors," Pure says. "The organization or
architecture of the matrix is important to supporting both stromal and cancer
cells within a tumor. If stromal cells depend on this matrix for structural
support and to communicate with the cancer, they can't do that properly if it is
drastically modified as we observed in the absence of FAP activity. "
To explore the potential for a therapeutic approach, the investigators used a
novel peptide agent, PT630, to shut down FAP activation in the lung and colon
cancer mice. Again, they found a significant reduction in tumor growth by
inhibiting the enzymatic activity of FAP with this candidate drug agent.
"This proof of concept is the first step toward the clinic," Pure says. "We need
more drugs that target the non-cancer cells in tumors, which can then be
combined with specific chemotherapies and biologic drugs to attack both the
tumor and its supporting cells."
One of the benefits of such a strategy, Pure adds, is that a limited number of
agents would likely be required to treat many different cancers, because stromal
cells tend to have common properties and share expression of the FAP protein in
most tumor types. Comparatively, targeted therapies designed for specific tumor
types - such as breast or colon - will likely require a wide variety of
different drugs.
The only agents currently used to treat cancer by targeting the tumor
microenvironment are anti-angiogenesis drugs, like Avastin, which disrupt blood
vessel formation to tumors.
The study was funded by grants from the National Institutes of Health, the
Pennsylvania Department of Health, the Cancer Research Institute, the Ludwig
Institute for Cancer Research and a Wistar Cancer Training Grant. Agents used in
the study were provided by Point Therapeutics. The authors declare no conflict
of interest.
The Wistar Institute is an international leader in biomedical research with
special expertise in cancer research and vaccine development. Founded in 1892 as
the first independent nonprofit biomedical research institute in the country,
Wistar has long held the prestigious Cancer Center designation from the National
Cancer Institute. The Institute works actively to ensure that research advances
move from the laboratory to the clinic as quickly as possible. The Wistar
Institute: Today's Discoveries - Tomorrow's Cures. On the Web at
http://www.wistar.org/ .
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