Possible
new cancer therapy shrinks tumors in melanoma patients, Science
authors report
A treatment that
replaces most of the body's immune system with cancer fighting cells
shrank the melanomas of some seriously ill patients, researchers report.
The findings appear in the journal Science,
published by the American Association for the Advancement of Science.
The therapy takes
advantage of the immune system's ability to deliver a specially targeted
assault on an unwanted invader, and helps boost that assault by
multiplying the number of immune cells involved inside the patient's body.
This approach may also work for treating other cancer types, as well as
infectious diseases, such as AIDS, according to the researchers.
Unlike many other
cancer studies, which are done on mice, this study was done on human
patients, who had not responded to standard therapies.
"To be able to do
something as complex as this in humans, where every human is different and
every tumor is different, has been quite difficult," said study
author Steven Rosenberg of the National Cancer Institute.
The body's immune
system can produce a set of T cells that attack tumors, but often these
alone aren't a match for aggressive cancer. In the past, researchers have
tried to boost these cells' numbers by extracting some from patients,
inducing them to multiply in culture, and then transferring the expanded
population back into the patients. The cells generally failed to
"stick," however and disappeared quickly after the transfer.
By suppressing the
patients' immune systems to "make room" for the new cells, as
physicians do during a tissue transplant, Rosenberg and his colleagues
induced the transferred cells to remain and grow in the body and start
killing the tumor cells. In two cases, the transferred cells repopulated
the patients' blood, becoming the dominant type of active T cell.
"It's very rare
to be able to sustain large numbers of T cells in the body," said
Rosenberg. "When your body fights the flu, maybe three percent of the
T cells are active. In one of our patients, 90 percent of the T cells were
active, and they sustained themselves for over four months. That's a
striking occurrence."
The researchers
studied 13 patients in the advanced stages of melanoma that had resisted
the usual treatments. The researchers removed parts of the patients'
tumors, which contained relatively small amounts of anti-tumor T cells,
and grew the T cells in culture, until they had multiplied by
approximately 1,000 times.
Before transferring
the cells to the patients, Rosenberg's team gave the patients a round of
chemotherapy that suppressed their immune systems' tendency to reject new
cells. A few days after the T cell transfer, the number of tumor-fighting
T cells shot up in more than half of the patients. After the transfer, the
cells proliferated and traveled to the tumor sites, the scientists found.
"We generated and
grew cells in the body to numbers that have never been approached
before," Rosenberg said.
Four of the 13
patients had mixed responses, in which certain tumors shrank while others
did not. Six others had clear regression of tumors at a variety of sites
in the body, lasting from two to 21 months, the authors report.
Of these six,
"patient 9" showed a regression of more than 95 percent of his
melanoma, results that were ongoing 8 months later. Ninety-nine percent of
"patient 10's" tumors had disappeared 7 months after the
treatment, according to the study.
The researchers are
currently working to improve the therapy so that a greater proportion of
patients respond the way patients 9 and 10 did, Rosenberg said.
T cells are usually
made up of a number of subfamilies, each capable of recognizing a slightly
different type of antigen. Antigens are the molecules that trigger an
immune response, whether they are from foreign pathogens or the body's own
cells. In several of the patients, a relatively large portion of T cells
(around 90 percent in patient 10) consisted of a single subfamily, the
researchers found.
For patients 9 and 10,
that subfamily turned out to be primed to attack a particular antigen
called "MART-1." The antigen is involved in producing
pigmentation, and is thus found in normal skin and iris cells, as well as
in melanomas.
Some of the patients
who had positive responses to the therapy developed certain forms of
autoimmunity, in which their T cells reacted to MART-1 antigens in healthy
tissue. Patient 9 and some others developed vitiligo, a skin disorder that
produces white patches of skin. Patient 10 developed uveitis, which is
inflammation in the iris, and was treated successfully with steroid drops,
the authors report.
The researchers didn't
observe any autoimmune disorders more serious than vitiligo and uveitis,
according to Rosenberg. If the therapy works on tumors, "it's a small
price to pay for getting rid of your cancer," he said.
###
The other study
authors are Mark E. Dudley, John R. Wunderlich, Paul F. Robbins, James C.
Yang, Patrick Hwu, Douglas J. Schwartzentruber, Suzanne L. Topalian,
Richard Sherry, Nicholas P. Restifo, Amy M. Hubicki, Mark Raffeld, Paul
Duray, Claudia A. Seipp, Linda Rogers-Freezer, Kathleen E. Morton, Sharon
A. Mavroukakis, and Donald E. White, of the National Cancer Institute, and
Michael R.Robinson, of the National Eye Institute.
Thursday, 19 September 2002
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