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Researchers discover link between Organ
Transplantation and increased Cancer risk
Newswise — Researchers have determined a
novel mechanism through which organ
transplantation often leads to cancer, and
their findings suggest that targeted
therapies may reduce or prevent that risk.
In the July 15, 2008, issue of Cancer
Research, researchers at Harvard Medical
School found in animal and laboratory
experiments that the anti-rejection,
immunosuppressive drug cyclosporine ramps up
expression of vascular endothelial growth
factor (VEGF), which signals the growth of
new blood vessels that can feed tumors.
They also found that simultaneously
administering an anti-VEGF therapy with
cyclosporine in mice repressed this tumor
growth. Several inhibitors of VEGF are
already in use in human cancer therapy
The findings could offer some good news for
the 15 to 20 percent of transplant patients
who develop cancer within a decade of
receiving new organs, according to the
study’s senior investigator, Soumitro Pal,
Ph.D., an assistant professor at Harvard
Medical School’s Transplantation Research
Center at Children’s Hospital in Boston.
“It may be that anti-VEGF agents given
judiciously after transplantation can reduce
future cancer occurrence,” he said.
VEGF expression is markedly increased in
patients post-transplantation, and this can
aid in the development of a blood supply to
a transplanted organ, helping it survive and
thrive.
“But once the organ has stabilized, it may
be possible to lower the level of VEGF
expression to prevent tumor growth,” he
said. “We would need to figure out how to
balance benefit and risk to keep cancer at
bay.”
Tumors that develop after transplantation
may have three potential sources: they may
have pre-existed or could have been a
recurrence of previous cancer – and in both
of these cases, a patient’s pre-transplant
immune system might have kept these cancers
in check – or cancer-causing viruses could
have come from the donor organ.
Physicians have long observed that
immunosuppressive agents, such as the class
of calcineurin inhibitors that includes
cyclosporine, appear to promote cancer
development, often in organs that are not
transplanted, but the cause of this was
unclear.
The Harvard team tested the ability of
cyclosporine to promote growth of
pre-existing tumors in mice implanted with
human renal (kidney) cancer cells. Mice
treated with the agent formed tumors faster
than untreated mice, but anti-VEGF therapy
substantially reduced that excessive growth.
Digging deeper into the biological pathway
of VEGF activation, the scientists found
that cyclosporine activates two of the three
forms of the common protein catalyst,
protein kinase C, which leads to increased
expression of VEGF.
“We think PKC-mediated VEGF transcriptional
activation is a key component in the
progression of cyclosporine-induced
post-transplantation cancer,” Pal said.
“It is likely not the whole story, but this
gives us a clue that we might be able to use
existing or novel therapies to reduce cancer
risk in transplanted patients.”
The mission of the American Association for
Cancer Research is to prevent and cure
cancer. Founded in 1907, AACR is the world’s
oldest and largest professional organization
dedicated to advancing cancer research.
The membership includes more than 28,000
basic, translational and clinical
researchers; health care professionals; and
cancer survivors and advocates in the United
States and 80 other countries.
AACR marshals the full spectrum of expertise
from the cancer community to accelerate
progress in the prevention, diagnosis and
treatment of cancer through high-quality
scientific and educational programs. It
funds innovative, meritorious research
grants.
The AACR Annual Meeting attracts more than
17,000 participants who share the latest
discoveries and developments in the field.
Special conferences throughout the year
present novel data across a wide variety of
topics in cancer research, treatment and
patient care.
AACR publishes five major peer-reviewed
journals: Cancer Research; Clinical Cancer
Research; Molecular Cancer Therapeutics;
Molecular Cancer Research; and Cancer
Epidemiology, Biomarkers & Prevention.
Its most recent publication and its sixth
major journal, Cancer Prevention Research,
is dedicated exclusively to cancer
prevention, from preclinical research to
clinical trials.
The AACR also publishes CR, a magazine for
cancer survivors and their families, patient
advocates, physicians and scientists. CR
provides a forum for sharing essential,
evidence-based information and perspectives
on progress in cancer research, survivorship
and advocacy.
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