Nov. 14, 2007
VCU Massey Cancer researcher receives $700,000 in research funding to target new cancer treatments
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A Virginia Commonwealth University Massey Cancer Center
researcher has received two grants totaling $700,000 from the V
Foundation for Cancer Research and the Multiple Myeloma Research
Foundation to develop new antileukemic/anti-cancer strategies and to
create novel treatment approaches for multiple myeloma and related
blood cancers.
Through these grants, Steven Grant, M.D.,
Massey’s associate director for translational research and co-leader of
the cancer center’s cancer cell biology program, will focus efforts to
support basic and clinical research.
The VCU Massey Cancer
Center is among just six National Cancer Institute-designated cancer
centers to receive a competitive three-year grant totaling nearly
$600,000 from the V Foundation for Cancer Research. Investigators from
the VCU School of Medicine;
Paul Dent, Ph.D., from the Department of Biochemistry; and John
Roberts, M.D., and Mohamed Rahmani, Ph.D., both from the Department of
Internal Medicine, will collaborate with Grant on this research.
“We
hope to use the information generated with the support of this award to
develop an entirely new antileukemic and anti-cancer strategy in which
novel molecularly targeted agents are rationally combined,” said Grant,
who is also the primary investigator for the project.
In
previously published work, Grant’s team uncovered a new mechanism of
action of the anti-cancer drug sorafenib. Sorafenib inhibits the
oncogene Raf-1, but also induces a process known as ER stress in
leukemia cells that leads to inhibition of protein translation. This
results in the reduced expression of pro-survival factors, such as the
anti-apoptotic protein Mcl-1. In previous research study, Grant’s team
recently reported that the antileukemic activity of a novel Bcl-2
antagonist, which is now entering the clinical arena, depends
critically upon expression levels of Mcl-1 in tumor cells.
“The
purpose of the V Foundation research project is to develop a completely
novel antileukemic strategy in which sorafenib is employed to
down-regulate Mcl-1 and in so doing, to lower the apoptotic threshold
of malignant cells that have been exposed to clinically relevant Bcl-2
antagonists,” said Grant.
According to Grant, the ultimate goal
will be to use these findings as a foundation for initiating clinical
trials combining sorafenib with Bcl-2 antagonists in patients with
refractory leukemia and potentially other hematologic malignancies.
In
other cancer-related research, through a one-year, $100,000 grant from
the Multiple Myeloma Research Foundation, Grant and co-investigator,
Yun Dai, Ph.D., assistant professor of medicine in the School of
Medicine, will work toward developing a new approach to the treatment
of multiple myeloma, an incurable, but treatable form of cancer. They
will combine small molecule inhibitors of anti-apoptotic proteins, such
as Bcl-2, that block the cell death process with the cell cycle
inhibitor flavopiridol. Flavopiridol inhibits cancer-cell progression
through the cell cycle.
“Multiple myeloma is a malignancy that
has proven unusually susceptible to novel targeted agents. Our basic
thesis is that it may be even more vulnerable to rational combinations
of such agents,” said Grant, who is a professor of medicine,
biochemistry and pharmacology.
Grant’s team has previously
reported that, in addition to its cell cycle effects, flavopiridol
blocks the expression of proteins that prevent myeloma cell apoptosis,
or programmed cell death at the transcriptional level. This
dramatically sensitizes these cells to the lethal effects of Bcl-2
antagonists.
In addition, a new schedule of flavopiridol has
recently been developed that has shown encouraging activity in chronic
lymphocytic leukemia, another B-cell malignancy.
Grant said
that the aim of the planned studies supported by the MMRF award will be
to demonstrate that flavopiridol can increase the activity of
clinically relevant Bcl-2 antagonists in patient-derived multiple
myeloma cells, and to test this strategy in an animal model of multiple
myeloma. The ultimate goal of this project will be to translate these
findings into a clinical trial for patients with advanced multiple
myeloma and other related hematologic malignancies.
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