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BOSTON An international
research team, led by investigators from the Massachusetts General
Hospital (MGH) Cancer Center and Dana-Farber Cancer Institute (DFCI),
has found a new way that some lung tumors become resistant to treatment
with targeted therapy drugs like Iressa and Tarceva. Their report,
which will appear in the journal Science and is receiving early online
release, describes a totally new resistance mechanism that may apply
to many types of cancer. It also suggests a treatment strategy for
patients with these resistant tumors.
"
We found that, for about 20 percent of
patients with tumors that become resistant
to Tarceva or Iressa, resistance is caused
by the genetic activation of an oncogene
that is not the normal target of the drug,
which is something that has never been
seen before," says Jeffrey Engelman,
MD, PhD, scientific director of the MGH
Center for Thoracic Cancers, the paper's
lead author.
"
Importantly, we also identified a potential
new way to treat these resistant tumors
with combination therapy directed against
both protein targets," adds Pasi A.
J?nne, MD, PhD, of the Lowe Center for
Thoracic Oncology at DFCI, the study's
senior author.
Drugs like Iressa (gefitinib) and Tarceva
(erlotinib) are used to treat advanced
non-small-cell lung cancer (NSCLC), the
leading cause of cancer deaths in the
U.S. They act by blocking the epidermal
growth factor receptor (EGFR), a molecule
on the surface of cancer cells. In 2004
research teams from MGH and DFCI found
that only tumors in which the EGFR gene
has been mutated in a way that magnifies
the cells' response to the growth factor,
a process that fuels tumor growth, were
sensitive to treatment with these drugs.
Although tumors that respond to EGFR inhibitors
do so rapidly and dramatically, eventually
the tumors become resistant and resume
growing. About half the time, a secondary
mutation that interferes with the drugs'
binding to the receptor develops within
the EGFR gene. A new group of so-called
irreversible EGFR inhibitors that permanently
bind to the protein are currently being
tested in clinical trials. But what leads
to other cases of resistance has been
unknown, and the current study was designed
to discover additional mechanisms.
To do so, the investigators modeled in
a laboratory setting what happens in
lung cancer patients; they used a line
of NSCLC cells with the sensitizing EGFR
mutation and created a cell line resistant
to treatment with Iressa. In a number
of experiments comparing the resistant
line with still-sensitive cells, they
focused on the cell signalling pathway
controlled by EGFR. In earlier research,
Engelman and colleagues had found that
the growth signal that starts with EGFR
works through a related protein called
ERBB3.
The current study showed that, in some
of the resistant cells, ERBB3 is activated
by amplification of a different oncogene
called MET, in essence bypassing the
blockage of EGFR. Analysis of samples
from patients whose tumors became resistant
after initially responding to Iressa
revealed that MET was amplified in resistant
samples from 4 of 18 patients. Although
treating resistant cell lines with either
Iressa or a MET inhibitor did not stop
tumor growth, treatment with both agents
did induce cell death.
"
This method of reactivating the EGFR signalling
pathway with MET may be a common resistance
mechanism in other therapies that target
receptors of the ERBB family, which are
used against breast cancer, colon cancer,
head and neck cancer, and the brain tumor
glioblastoma multiforme," says J?nne,
who is an assistant professor of Medicine
at Harvard Medical School (HMS).
"
Our results suggest that, when patient's
tumors become resistant, repeat biopsies
to identify which resistance mechanism
is involved will be critical and could
help us develop effective therapies for
those resistant tumors," adds co-author
Lewis Cantley, PhD, of the Beth Israel
Deaconess Medical Center.
To that end, the investigators are working
on a research protocol for combined treatment
with FDA-approved EGFR inhibitors and
with MET inhibitors, which are in preapproval
trials against other types of cancer.
They also plan to analyze a larger number
of resistant samples to get a clearer
idea of the frequency of this resistance
mechanism.
Additional co-authors of the Science report
are Kreshnik Zejnullahu, Joon Oh Park,
MD, PhD, Xiaojun Zhao, PhD, Alison Holmes,
Andrew Rogers and Bruce Johnson, MD,
of Dana-Farber; Tetsuya Mitsudomi, MD,
and Takayuki Kosaka, MD, Aichi Cancer
Center Hospital, Nagoya, Japan; Youngchul
Song and Christopher-Michael Gale; Courtney
Hyland, Neal Lindeman, MD, and Charles
Lee, PhD, Brigham and Womens Hospital;
James Christensen, PhD, Pfizer Global
Research and Development; Federico Cappuzzo,
MD, Instituto Clinico Humanitas, Rozzano,
Italy; and Tony Mok, MD, Chinese University
of Hong Kong. The study was supported
by grants from the National Institutes
of Health, including the National Cancer
Institute; the American Cancer Society,
the American Association for Cancer Research;
the International Association for the
Study of Lung Cancer; and the Italian
Association for Cancer Research.
Massachusetts General Hospital (www.massgeneral.org),
established in 1811, is the original
and largest teaching hospital of Harvard
Medical School. The MGH conducts the
largest hospital-based research program
in the United States, with an annual
research budget of nearly $500 million
and major research centers in AIDS, cardiovascular
research, cancer, computational and integrative
biology, cutaneous biology, human genetics,
medical imaging, neurodegenerative disorders,
regenerative medicine, transplantation
biology and photomedicine.
Dana-Farber Cancer Institute (www.dana-farber.org)
is a principal teaching affiliate of
the Harvard Medical School and is among
the leading cancer research and care
centers in the United States. It is a
founding member of the Dana-Farber/Harvard
Cancer Center (DF/HCC), a designated
comprehensive cancer center by the National
Cancer Institute.
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