Developing and testing a
new anti-cancer drug can cost billions of dollars and take many years of research.
Finding an effective anti-cancer medication from the pool of drugs already
approved for the treatment of other medical conditions could cut a considerable
amount of time and money from
the process. Now, using a novel bioinformatics approach, a team led by
investigators at Beth Israel Deaconess Medical Center (BIDMC) has found that
the approved antimicrobial drug pentamidine may help in the treatment of
patients with advanced kidney cancer. Described online in the journal Molecular Cancer Therapeutics,
the discovery reveals how linking cancer gene expression patterns
with drug activity might help advance cancer care.
"The strategy of
repurposing drugs that are currently being used for other indications is of
significant interest to the medical community as well as the pharmaceutical and
biotech industries," says senior author Towia Libermann, PhD, Director of
the Genomics, Proteomics, Bioinformatics and Systems Biology Center at BIDMC
and Associate Professor of Medicine at Harvard Medical School. "Our
results demonstrate that bioinformatics approaches involving the analysis and
matching of cancer and drug gene signatures can indeed help us identify new
candidate cancer therapeutics."
Renal cell cancer
consists of multiple subtypes that are likely caused by different genetic
mutations. Over the years, Libermann has been working to identify new disease
markers and therapeutic targets through gene expression signatures of renal
cell cancer that distinguish these different cancer subtypes from each other,
as well as from healthy individuals. In this paper, he and his colleagues were
looking for drugs that might be effective against clear cell renal cancer, the
most common and highly malignant subtype of kidney cancer. Although patients
with early stage disease can often be successfully treated through surgery, up
to 30 percent of patients with renal cell cancer present with advanced stages
of disease at the time of their diagnosis.
To pursue this search,
they made use of the Connectivity Map (C-MAP) database (http://www.broadinstitute.org/cmap), a collection of gene expression data from human cancer
cells treated with hundreds of small molecule drugs.
"C-MAP uses
pattern-matching algorithms to enable investigators to make connections between
drugs, genes and diseases through common, but inverse, changes in gene
expression," says Libermann. "It provided us with an exciting
opportunity to use our renal cell cancer gene signatures and a new
bioinformatics strategy to match kidney cancer gene expression profiles from
individual patients with gene expression changes inducted by various commonly
used drugs."
After identifying drugs
that may reverse the gene expression changes associated with renal cell cancer,
the investigators used assays to measure the effect of the selected drugs on
cells. This led to the identification of a small number of FDA-approved drugs
that induced cell death in multiple kidney cancer cell lines. The investigators
then tested three of these drugs in an animal model of renal cell cancer and
demonstrated that the antimicrobial agent pentamidine (primarily used for the
treatment of pneumonia) reduced tumor growth and enhanced survival. Gene
expression experiments using microarrays also identified the genes in renal
cell cancer that were counteracted by pentamidine.
Posted By:-
Bioinformatics Department
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