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Bristol, AbbVie drug
extends multiple myeloma remission: study
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[May 14, 2015]
By Bill Berkrot
(Reuters) - The addition of an experimental
Bristol-Myers Squibb biotech medicine to standard therapy for patients
whose multiple myeloma has relapsed led to longer remissions and cut the
risk of death over standard treatment alone, according to data from a
late stage study.
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 The drug, elotuzumab, which is being developed in collaboration with
AbbVie, extended the duration of remissions by about five months on
average when used with Celgene's Revlimid and the corticosteroid
dexamethasone. It is the first antibody to be used against this type
of blood cancer, researchers said.
In the study of 646 patients with recurrent multiple myeloma, those
who received the three-drug combination on average went 19.4 months
before the cancer began to worsen, compared with 14.9 months for
those who received Revlimid and dexamethasone.
After two years, elotuzumab reduced the risk of cancer progression
and death by 30 percent, according to a brief summary of results
from the Phase III study that will be presented at the American
Society of Clinical Oncology (ASCO) meeting in Chicago beginning
later this month.
"This is probably a practice-changing type of treatment," ASCO
president-elect Dr. Julie Vose said. "I expect they will get
approval."
Survival data was not yet available. However, "there clearly are
very encouraging signs in terms of overall survival," said Dr. Sagar
Lonial, the study's lead investigator from Emory University in
Atlanta.
Elotuzumab received breakthrough designation from the U.S. Food and
Drug Administration, given to medicines it sees as potentially
important advances.
The drug targets a protein found on the surface of myeloma cells and
an immune system component known as natural killer (NK) cells. It is
believed elotuzumab attacks the cancer directly and enhances
activation of NK cells.
"In many ways it's a double whammy in terms of the tumor itself,"
Lonial said.
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After two years, the myeloma had not progressed in 41 percent of
elotuzumab patients versus 27 percent for the control group. At one
year, it had been 68 percent versus 57 percent.
"It was particularly striking that the difference ... seems to get
bigger over time," Lonial said, adding that this "really speaks to
the power of this immune-based approach."
The addition of elotuzumab did not lead to a significant increase in
adverse side effects or toxicity.
"We hope that we will soon have a new treatment option for the
management of these patients," Lonial said.
The companies are also testing elotuzumab in newly diagnosed
multiple myeloma patients.
(Reporting by Bill Berkrot; editing by Andrew Hay)
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