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Patient’s own Infection-fighting T Cells put
late-stage Melanoma into long-term remission
Newswise — Researchers
describe the first successful use of a human
patient’s cloned infection-fighting T cells
as the sole therapy to put an advanced
solid-tumor cancer into long-term remission.
A team led by Cassian Yee,
M.D., an associate member of the Clinical
Research Division at Fred Hutchinson Cancer
Research Center, reports these findings in
the June 19 issue of the New England Journal
of Medicine.
Yee and colleagues removed
CD4+ T cells, a type of white blood cell,
from a 52-year-old man whose Stage 4
melanoma had spread to a groin lymph node
and to a lung. T cells specific to targeting
the melanoma were then expanded vastly in
the laboratory using modifications to
existing methods.
The lab-grown cells were then
infused into the patient with no additional
pre- or post-conditioning therapies, such as
growth-factor or cytokine treatment.
Two months later, PET and CT
scans revealed no tumors. The patient
remained disease free two years later, when
he was last checked.
”We were surprised by the
anti-tumor effect of these CD4 T cells and
its duration of response,” Yee said.
“For this patient we were
successful, but we would need to confirm the
effectiveness of therapy in a larger study.”
Yee cautioned that these
results, presented in the journal’s “Brief
Report” section, represent only one patient
with a specific type of immune system whose
tumor cells expressed a specific antigen.
More studies are needed
to confirm the effectiveness of the
experimental T-cell therapy. If proven
successful in more patients, Yee predicted
this therapy could be used for the 25
percent of all late-stage melanoma patients
who have the same immune-system type and
tumor antigen.
Using a patient’s own immune
system to combat cancer, called
immunotherapy, is a growing area of research
that aims to develop less-toxic cancer
treatments than standard chemotherapy and
radiation.
The patient in the journal
report was one of nine patients with
metastatic melanoma who were being treated
in a recently completed clinical trial to
test dose- escalation of autologous CD4+ T
cells.
Earlier studies performed by
Yee used CD8+ T cells, which do not persist
in the body without the support of CD4+ T
cells or growth factors such as interleukin
2.
Yee and colleagues theorized
that infusion of a massive dose of CD4+ T
cells would persist longer in the body
because they make their own growth factor,
interleukin 2, while stimulating the
anti-tumor effect of the patient’s existing
CD8+ T cells.
However, until recently there
was no feasible way to isolate and expand
anti-tumor CD4+ T cells in the lab.
The researchers were
successful in all of these areas. The
patient received a dose of 5 billion cloned
CD4+ T cells with specificity for the
melanoma-associated NY-ESO-1 antigen. The
cells persisted for at least 80 days in the
patient’s body.
And, even though only 50
percent to 75 percent of the patient’s tumor
cells expressed the NY-ESO-1 antigen, the
entire tumor regressed following the
infusion.
The scientists postulated
that the patient’s immune response was
broadened to other antigens expressed by the
tumor cells. Follow-up tests showed T-cell
responses to two additional tumor antigens,
MAGE-3 and MART-1.
Researchers in Yee’s lab, the
University of Washington School of Medicine
and the Ludwig Institute for Cancer Research
in New York collaborated on the research.
The Burroughs-Wellcome
Foundation, Damon Runyon Cancer Research
Foundation, Edson Foundation and National
Cancer Institute funded the study.
At Fred Hutchinson Cancer
Research Center, our interdisciplinary teams
of world-renowned scientists and
humanitarians work together to prevent,
diagnose and treat cancer, HIV/AIDS and
other diseases.
Our researchers, including
three Nobel laureates, bring a relentless
pursuit and passion for health, knowledge
and hope to their work and to the world. For
more information, please visit
www.fhcrc.org
.
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