Modifying Immune System Response to Cancer Chemotherapy Could
Lead to New Treatment Approaches
Researchers at the National Cancer Institute (NCI), part of the National Institutes
of Health, have discovered a mechanism by which cancer patients’ immune systems
respond to chemotherapy. The new finding changes the current understanding of
how the immune system responds to chemotherapy and could lead to opportunities
for new treatments based on enhancing the body’s immune response to the disease.
The study findings appear in Nature Medicine*, November
2005
Chemotherapy for cancer is known to severely deplete the number of immune system
T-cells — creating a condition known as lymphopenia. Paradoxically, lymphopenia
leads to increased immune system response It has not been clear how this happens.
Some scientists have believed that chemotherapy-induced lymphopenia results in
selective depletion of "suppressor" T-cells, a type of T-cell that acts to turn
off or inhibit an immune response. Depletion of “suppressor” T-cells increases
immune response in cancer patients. However, this new study indicates that even
though chemotherapy depletes T-cells, it does not selectively destroy suppressor
or regulatory T-cells, as previously assumed. Instead, the study showed that
the lymphopenia condition caused by chemotherapy actually provided a good environment
for proliferation of suppressor T-cells that are believed to contribute to the
ability of tumors to evade the body’s immune system. The mechanism by which this
occurs is not entirely clear, but could involve interleukin-2 (IL-2), a cytokine
which was not previously associated with suppressing immune responses.
Researchers at NCI’s Center for Cancer Research (CCR), Pediatric Oncology Branch,
examined immune recovery in 26 young cancer patients with pediatric sarcomas
(highly malignant tumors) who received cyclophosphamide-based chemotherapy, which
depleted lymphocytes. The patients were then infused with their own frozen lymphocytes,
which had been stored before chemotherapy had begun. Researchers examined the
impact of this treatment on the patients’ immune recovery with or without recombinant
IL-2, an agent that has been considered capable of restoring an immune system
weakened by chemotherapy. The cancer patients in the study were assigned to one
of three groups: the first group received moderate-dose IL-2 therapy; the second
group received low-dose IL-2 treatment, and the third group received no IL-2.
The researchers reported that the patients who received IL-2 — at either
dose — showed a marked increase in suppressor T-cells after chemotherapy.
These findings were confirmed in a parallel study in lymphopenic mice.
“This is a surprising result, since IL-2 has been considered an immune activator — not
a suppressor,” commented Crystal L Mackall, M.D., head of CCR’s Pediatric Oncology
Branch Immunology Section and study co-author. “These results suggest that a
large portion of IL-2’s effects is to suppress immune responses.” If, instead,
a way could be designed to deplete the number of suppressor T-cells, that could
create a chance for a different type of T-cell — that attacks cancer cells — to
increase their numbers to fight the disease, she added.
Such an opportunity may exist, as the researchers also discovered that the suppressor
T-cells that appeared following chemotherapy and IL-2 administration were derived
from existing T-cells, rather than being created anew in the patients’ thymus
glands, where T-cells typically originate. As a result, “if one could deplete
suppressor cells from the patient's system, these cells would not be efficiently
regenerated,” Mackall explained. “If a patient with lymphocyte depletion were
also depleted of suppressor cells, the immune system would be predicted to be
highly reactive — and responsive to antitumor vaccines — and therefore may be
better able to fight cancer.”
The study has important implications for developing future immunotherapies against
cancer, as many researchers are interested in manipulating suppressor cells to
make the immune system more effective in responding to cancer. “This study provides
the first insight into what makes regulatory T-cells tick and therefore provides
ideas for new ways to deplete or manipulate these cells more effectively in humans,” Mackall
added.
CCR’s Pediatric Oncology Branch is planning a follow-up clinical trial that
will attempt to rebuild the immune system in a similar set of patients who are
depleted of suppressor T-cells and also will be administered a tumor vaccine. “We
hope that this setting will lead to very vigorous antitumor immune responses
that can prevent tumor recurrence,” Mackall said.
For more information about cancer, visit the NCI Web site at http://www.cancer.gov or
call NCI's Cancer Information Service at 1-800-4 CANCER (1-800-422-6237).
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agency for conducting and supporting basic, clinical, and translational medical
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