Findings
from the AACR Centennial Conference on Translational
Cancer Medicine: From Technology to Treatment Singapore,
Nov. 4-8, 2007
SINGAPORE -- A novel compound that blocks the breakdown
of retinoic acid, derived from vitamin A, is a surprisingly
effective and "promiscuous" agent in treating
animal models of human prostate cancer, say investigators
from the University of Maryland, Baltimore (UMB).
Daily injections of the agent VN/14-1 resulted in
up to a 50 percent decrease in tumor volume in mice
implanted with human prostate cancer cells, reported
Aakanksha Khandelwal, Ph.D., today at the American
Association for Cancer Research Centennial Conference
on Translational Cancer Medicine. No further tumor
growth was seen during the five-week study, Khandelwal
reports.
Importantly, VN/14-1 exerted its effects in multiple
ways, which is the hallmark of a so-called promiscuous
drug, according to the study's senior investigator,
Vincent C.O. Njar, Ph.D., associate professor in
the Department of Pharmacology and Experimental Therapeutics
within UMB's School of Medicine.
"This potent agent causes cancer cells to differentiate,
forcing them to turn back to a non-cancerous state −
which is what we expected it would do −
but it also stops cancer growth by arresting the
cell cycle and pushes cells to die by inducing programmed
cell death," Njar said.
"These functions were unexpected and wonderfully
surprising," he said. "I am not aware that
any other drug currently used to treat prostate cancer
targets so many pathways."
Vitamin A, when converted by the body into retinoic
acid, is known to be involved in maintaining the
normal growth of cells, and other research has shown
that prostate cancer cells contain five to eight
times less retinoic acid than normal prostate cells.
Njar's laboratory developed a number of compounds,
including VN/14-1, with the aim of inhibiting the
normal breakdown of retinoic acid in cancer cells.
The agent is similar in function to the well-known
acne and anti-aging therapy, Retin-A, as well as
to the leukemia drug Vesanoid. These products, known
as retinoids, add all-trans retinoic acid (ATRA)
to skin or cancer cells. VN/14-1, which is a retinoic
acid metabolism blocking agent (RAMBA), works by
inhibiting the breakdown of ATRA, keeping more retinoic
acid available within cancer cells so that the chemical
can redirect these cells back into their normal growth
patterns, which includes programmed cell death.
"Our idea is that rather than give extra ATRA,
we would prevent ATRA already available within cells
from being broken down," Njar said. "We
now call VN/14-1 an atypical RAMBA because in addition
to blocking ATRA metabolism, it has other multiple
desirable anti-cancer effects."
VN/14-1 works by blocking the CYP26 enzyme that
actually transforms ATRA into inactive compounds,
he says. The researchers have successfully tested
VN/14-1 in breast cancer cells and have been funded
to study the compound in preclinical studies that
can lead to a Phase I human clinical trial.
In this study, the researchers found in mouse models
of human prostate cancer that a 5 mg/kg (milligram
per kilogram) dose injected daily resulted in a 33
percent reduction in tumor size; a dose twice as
large reduced tumors by 50 percent.
They also tested a dose of 20 mg/kg through oral
and intravenous administration to study the concentration
of VN/14-1 in the blood over time in rats. They found
that the amount of VN/14-1 in the blood after oral
administration was exceptionally high compared to
intravenous VN/14-1. This indicates that VN/14-1
should be tested orally as this is the preferred
route of drug administration in humans, Njar says. "Giving
an agent orally in small doses is exactly what you
want in an anti-cancer drug," he said.
American Association for Cancer Research |
