SEATTLE-- Ken Shefveland's body was swollen
with cancer, treatment after treatment failing until doctors gambled on a
radical approach: They removed some of his immune cells, engineered them into
cancer assassins and unleashed them into his bloodstream.
Immune
therapy is the hottest trend in cancer care and this is its next frontier —
creating "living drugs" that grow inside the body into an army that
seeks and destroys tumors.
Looking
in the mirror, Shefveland saw "the cancer was just melting away." A
month later doctors at the Fred Hutchinson Cancer Research Center couldn't find
any signs of lymphoma in the Vancouver, Washington, man's body.
"Today
I find out I'm in full remission — how wonderful is that?"
said Shefveland
with a wide grin, giving his physician a quick embrace.
This
experimental therapy marks an entirely new way to treat cancer — if scientists
can make it work, safely. Early-stage studies are stirring hope as one-time
infusions of supercharged immune cells help a remarkable number of patients
with intractable leukemia or lymphoma.
"It
shows the unbelievable power of your immune system," said Dr. David
Maloney, Fred Hutch's medical director for cellular immunotherapy who treated
Shefveland with a type called CAR-T cells.
"We're
talking, really, patients who have no other options, and we're seeing tumors
and leukemias disappear over weeks," added immunotherapy scientific
director Dr. Stanley Riddell. But, "there's still lots to learn."
T
cells are key immune system soldiers. But cancer can be hard for them to spot,
and can put the brakes on an immune attack. Today's popular immunotherapy drugs
called "checkpoint inhibitors" release one brake so nearby T cells
can strike. The new cellular immunotherapy approach aims to be more potent:
Give patients stronger T cells to begin with.
Currently
available only in studies at major cancer centers, the first CAR-T cell
therapies for a few blood cancers could hit the market later this year. The
Food and Drug Administration is evaluating one version developed by the
University of Pennsylvania and licensed to Novartis, and another created by the
National Cancer Institute and licensed to Kite Pharma.
CAR-T
therapy "feels very much like it's ready for prime time" for advanced
blood cancers, said Dr. Nick Haining of the Dana-Farber Cancer Institute and
Broad Institute of MIT and Harvard, who isn't involved in the development.
Now
scientists are tackling a tougher next step, what Haining calls "the acid
test": Making T cells target far more common cancers — solid tumors like
lung, breast or brain cancer. Cancer kills about 600,000 Americans a year,
including nearly 45,000 from leukemia and lymphoma.
"There's
a desperate need," said NCI immunotherapy pioneer Dr. Steven Rosenberg,
pointing to queries from hundreds of patients for studies that accept only a
few.
For
all the excitement, there are formidable challenges.
Scientists
still are unraveling why these living cancer drugs work for some people and not
others.
Doctors
must learn to manage potentially life-threatening side effects from an
overstimulated immune system. Also concerning is a small number of deaths from
brain swelling, an unexplained complication that forced another company, Juno
Therapeutics, to halt development of one CAR-T in its pipeline; Kite recently
reported a death, too.
And,
made from scratch for every patient using their own blood, this is one of the
most customized therapies ever and could cost hundreds of thousands of dollars.
"It's
a Model A Ford and we need a Lamborghini," said CAR-T researcher Dr.
Renier Brentjens of New York's Memorial Sloan Kettering Cancer Center, which,
like Hutch, has a partnership with Juno.
In
Seattle, Fred Hutch offered a behind-the-scenes peek at research underway to
tackle those challenges. At a recently opened immunotherapy clinic, scientists
are taking newly designed T cells from the lab to the patient and back again to
tease out what works best.
"We
can essentially make a cell do things it wasn't programmed to do
naturally," explained immunology chief Dr. Philip Greenberg. "Your
imagination can run wild with how you can engineer cells to function
better."
TWO LONG WEEKS TO BREW A DOSE
The
first step is much like donating blood. When leukemia patient Claude Bannick
entered a Hutch CAR-T study in 2014, nurses hooked him to a machine that
filtered out his white blood cells, including the T cells.
Technicians
raced his bag of cells to a factory-like facility that's kept so sterile they
must pull on germ-deflecting suits, booties and masks just to enter. Then came
14 days of wait and worry, as his cells were reprogrammed.
Bannick,
67, says he "was almost dead." Chemotherapy, experimental drugs, even
a bone marrow transplant had failed, and "I was willing to try
anything."
GENETICALLY ENGINEERING CELLS
The
goal: Arm T cells with an artificial receptor, a tracking system that can zero
in on identifying markers of cancer cells, known as antigens. For many leukemias
and lymphomas, that's an antigen named CD19.
Every
research group has its own recipe but generally, scientists infect T cells with
an inactive virus carrying genetic instructions to grow the desired
"chimeric antigen receptor." That CAR will bind to its target cancer
cells and rev up for attack.
Millions
of copies of engineered cells are grown in incubators, Hutch technicians
pulling out precious batches to monitor if they're ready for waiting patients.
If they
work, those cells will keep multiplying in the body. If they don't, the doctors
send blood and other samples back to researchers like Riddell to figure out
why.
WHAT'S THE DATA?
Small,
early studies in the U.S. made headlines as 60 percent to 90 percent of
patients trying CAR-Ts as a last resort for leukemia or lymphoma saw their
cancer rapidly decrease or even become undetectable. Last week, Chinese
researchers reported similar early findings as 33 of 35 patients with another
blood cancer, multiple myeloma, reached some degree of remission within two
months.
Too
few people have been studied so far to know how long such responses will last.
A recent review reported up to half of leukemia and lymphoma patients may
relapse.
There
are long-term survivors. Doug Olson in 2010 received the University of
Pennsylvania's CAR-T version for leukemia. The researchers were frank — it had
worked in mice but they didn't know what would happen to him.
"Sitting
here almost seven years later, I can tell you it works," Olson, now 70,
told a recent meeting of the Leukemia and Lymphoma Society.
Bannick,
the Hutch patient treated in 2014, recalls Maloney calling him "the
miracle man." He had some lingering side effects that required
blood-boosting infusions but says CAR-T is "giving me a second life."
SCARY SIDE EFFECTS
"The
more side effects you have, that sort of tells everybody it's working,"
said Shefveland, who was hospitalized soon after his treatment at Hutch when
his blood pressure collapsed. His last clear memory for days: "I was
having a conversation with a nurse and all of a sudden it was gibberish."
As
CAR-T cells swarm the cancer, an immune overreaction called "cytokine
release syndrome" can trigger high fevers and plummeting blood pressure
and in severe cases organ damage. Some patients also experience confusion,
hallucinations or other neurologic symptoms.
Treatment
is a balancing act to control those symptoms without shutting down the cancer
attack.
Experienced
cancer centers have learned to expect and watch for these problems. "And,
most importantly, we've learned how to treat them," said Dr. Len
Lichtenfeld of the American Cancer Society, who is watching CAR-T's
development.
FIGHTING SOLID TUMORS WILL
BE HARDER
CAR-Ts
cause collateral damage, killing some healthy white blood cells, called B
cells, along with cancerous ones because both harbor the same marker. Finding
the right target to kill solid tumors but not healthy organ tissue will be even
more complicated.
"You
can live without some normal B cells. You can't live without your lungs,"
Riddell explained.
Early
studies against solid tumors are beginning, targeting different antigens.
Time-lapse photos taken through a microscope in Riddell's lab show those new
CAR-T cells crawling over aggressive breast cancer, releasing toxic chemicals
until tumor cells shrivel and die.
CARs
aren't the only approach. Researchers also are trying to target markers inside
tumor cells rather than on the surface, or even gene mutations that don't form
in healthy tissue.
"It's
ironic that the very mutations that cause the cancer are very likely to be the
Achilles heel," NCI's Rosenberg said.
And
studies are beginning to test CAR-Ts in combination with older immunotherapy
drugs, in hopes of overcoming tumor defenses.
HOW WILL PATIENTS GET THE
FIRST CAR-T THERAPIES?
If the
FDA approves Novartis' or Kite's versions, eligible leukemia and lymphoma
patients would be treated at cancer centers experienced with this tricky
therapy. Their T cells would be shipped to company factories, engineered, and
shipped back. Gradually, more hospitals could offer it.
Because
only certain patients would qualify for the first drugs, others would have to
search for CAR-T studies to try the treatment. A drug industry report lists 21
CAR-T therapies in development by a dozen companies.
"This
is the hope of any cancer patient, that if you stay in the game long enough,
the next treatment's going to be just around the corner," said Shefveland,
the Hutch patient.
(AP)
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