SUNDAY, June 1 (HealthDay News) -- Drugs used widely to treat
anemia in cancer patients may actually speed progression of the
cancer in certain individuals, but researchers report they may
found a way to determine who those individuals are.
"We may have a test to predict whether a patient is susceptible
to having their tumor progress if treated with erythropoietin and,
alternatively, we may be able to predict patients it would be safe
to treat with erythropoietin," study author Dr. Tony Blau, of the
University of Washington in Seattle, said during a Sunday news
conference at the American Society of Clinical Oncology annual
meeting in Chicago.
Recent controversy over erythropoiesis-stimulating agents (ESAs)
such as Procrit, Epogen and Aranesp has centered around whether the
blood-boosting drugs should be withdrawn from the market because of
troubling side effects.
In March, a U.S. Food and Drug Administration advisory panel
voted to recommend continued use of the drugs for patients on
chemotherapy, unless the patient is likely to be cured. They also
voted to recommend against the drugs' use in patients with breast
or head and neck cancer.
Eight clinical trials now suggest these medications actually
speed the growth of tumors and shorten the lives of cancer
victims.
The drugs' manufacturers added a "black box" warning to the
medications last November.
"There has been lots of controversy over these stimulating
agents, and we have an FDA advisory committee to act on this as we
speak," said Dr. Julie Gralow, director of breast oncology at the
University of Washington and Fred Hutchinson Cancer Center in
Seattle and moderator of the Sunday news conference. "The drugs
offer benefits in terms of reducing anemia and reducing
transfusions, but several large trials in a variety of tumor types
suggest that . . . these agents may have some stimulatory effects
on tumor cells, faster progression in some cases, and more death in
others."
Until recently, Blau added, these drugs represented the biggest
U.S. federal expenditures for oncology patients.
The results of the current study were based on analyses of tumor
samples from 101 patients diagnosed with head and neck cancer who
had participated in a previous phase III trial of
erythropoietin.
Scientists measured levels of erythropoietin receptor (EpoR)
messenger RNA (mRNA).
High levels of EpoR mRNA in patients who had undergone radiation
but not surgery tended to signal a worse prognosis. There was a
similar effect with Janus Kinase 2 (Jak2), the main intermediary of
EpoR signaling, Blau added.
"These are preliminary findings, but they're very exciting,"
Gralow said. "If they hold up, they may mean that we may be able to
use ESAs in targeted ways."
"These findings must be considered preliminary until confirmed,"
added Blau. "We believe that the definitive answer to this question
lies locked in the filing cabinets of pathologists' offices that
contain tumors of patients who participated in already completed
phase III studies." That, of course, would be much easier than
initiating entirely new studies.
A second study found the multiple drugs elderly cancer patients
may already be taking could interact significantly with
chemotherapy.
In particular, patients taking drugs that interfered with
protein binding such as Norvasc for high blood pressure, Prilosec
for heartburn, and the pain reliever Celebrex were more likely to
experience hematologic side effects such as low white blood cell
counts.
Patients taking drugs that act on a group of enzymes known as
cytochrome p450 were more likely to experience effects such as
fatigue or diarrhea. Examples of these drugs include the heart
medications such as Pacerone and Cordarone.
"We found that all drugs patients are taking besides
chemotherapy are likely to affect their tolerance to chemotherapy,"
said study author Dr. Mihaela Popa, of the H. Lee Moffitt Cancer
Center in Tampa, Fla.
More information
The
American Cancer Society has more on cancer-related
fatigue and anemia.
