Kaitlyn Johnson, 7, was diagnosed with leukemia but is in remission after receiving a new genetic and immune therapy Brent Humphreys for TIME
With the usual mix of anticipation and apprehension, Kaitlyn Johnson is getting ready to go to her first summer camp. She's looking forward to meeting new friends and being able to ride horses, swim and host tea parties. She's also a little nervous and a little scared, like any 7-year-old facing her first sleepaway camp.
But
the wonder is that Kaitlyn is leaving the house for anything but a
medical facility. Diagnosed with leukemia when she was 18 months old,
her life has been consumed with cancer treatments, doctors' visits and
hospital stays.
Acute
lymphoblastic leukemia is the most common cancer among young children,
accounting for a quarter of all cancer cases in kids, and it has no
cure. For about 85% to 90% of children, the leukemia can, however, be
effectively treated through chemotherapy.
If
it is not eliminated and comes back, it is, more often than not, fatal.
Rounds of chemotherapy can buy patients time, but as the disease
progresses, the periods of remission get shorter and shorter. "The
options for these patients are not very good at all," says Dr. Theodore
Laetsch, a pediatrician at the University of Texas Southwestern Medical
Center.
When
Kaitlyn's cancer wasn't controlled after three years and round after
round of chemotherapy drugs, her doctors had little else to offer. "They
said, 'This did nothing, it didn't touch it,'" says Kaitlyn's mother
Mandy, a dental assistant from Royce City, Texas. "My stomach just
dropped." Kaitlyn could receive a bone-marrow transplant, but only about
half of those procedures are successful, and there was a good chance
that she would reject the donor cells. If that happened, her chances of
surviving were very small.
In
a calculated gamble, her doctors suggested a radical new option:
becoming a test subject in a trial of an experimental therapy that
would, for the first time, use gene therapy to train a patient's immune
system to recognize and destroy their cancer in the same way it
dispatches bacteria and viruses. The strategy is the latest development
in immunotherapy, a revolutionary approach to cancer treatment that uses
a series of precision strikes to disintegrate cancer from within the
body itself. Joining the trial was risky, since other attempts to
activate the immune system hadn't really worked in the past. Mandy, her
husband James and Kaitlyn traveled from their home in Texas to
Children's Hospital of Philadelphia (CHOP), where they stayed in a hotel
for eight weeks while Kaitlyn received the therapy and recovered. "The
thought crossed my mind that Kaitlyn might not come home again," says
Mandy. "I couldn't tell you how many times I would be in the bathroom at
the hospital, spending an hour in the shower just crying, thinking,
What are we going to do if this doesn't help her?"
Kaitlyn at age 5, after receiving her own genetically modified immune cells Courtesy Johnson Family
But
it did. After receiving the therapy in 2015, the cancer cells in
Kaitlyn's body melted away. Test after test, including one that picks up
one cancer cell in a million, still can't detect any malignant cells
lurking in Kaitlyn's blood. What saved Kaitlyn was an infusion of her
own immune cells that were genetically modified to destroy her leukemia.
"You take someone who essentially has no possibility for a cure--almost
every single one of these patients dies--and with [this] therapy, 90%
go into remission," says Dr. David Porter, director of blood and
bone-marrow transplantation at the University of Pennsylvania. Such
radical immune-based approaches were launched in 2011 with the success
of intravenous drugs that loosen the brakes on the immune system so it
can see cancer cells and destroy them with the same vigor with which
they attack bacteria and viruses. Now, with the genetically engineered
immune cells known as chimeric antigen receptor (CAR) T cells that were
used in Kaitlyn's study, doctors are crippling cancer in more precise
and targeted ways than surgery, chemotherapy and radiation ever could.
While the first cancer immunotherapies were broadly aimed at any cancer,
experts are now repurposing the immune system into a personalized
precision treatment that can not only recognize but also eliminate the
cancer cells unique to each individual patient.
What
makes immune-based therapies like CAR T cell therapy so promising--and
so powerful--is that they are a living drug churned out by the patients
themselves. The treatment isn't a pill or a liquid that has to be taken
regularly, but a one-hit wonder that, when given a single time, trains
the body to keep on treating, ideally for a lifetime.
"This
therapy is utterly transformative for this kind of leukemia and also
lymphoma," says Stephan Grupp, director of the cancer immunotherapy
program at CHOP and one of the lead doctors treating patients in the
study in which Kaitlyn participated.
Eager
to bring this groundbreaking option to more patients, including those
with other types of cancers, an advisory panel for the Food and Drug
Administration voted unanimously in July to move the therapy beyond the
testing phase, during which several hundred people have been able to
take advantage of it, to become a standard therapy for children with
certain leukemias if all other treatments have failed. While the FDA
isn't obligated to follow the panel's advice, it often does, and it is
expected to announce its decision in a matter of weeks.
Across
the country, doctors are racing to enroll people with other
cancers--breast, prostate, pancreatic, ovarian, sarcoma and brain,
including the kind diagnosed in Senator John McCain--in hundreds of
trials to see if they, too, will benefit from this novel approach. They
are even cautiously allowing themselves to entertain the idea that this
living drug may even lead to a cure for some of these patients. Curing
cancers, rather than treating them, would result in a significant drop
in the more than $120 billion currently spent each year on cancer care
in the U.S., as well as untold suffering.
Lon Tweeten for TIME
This revolutionary therapy, however, almost didn't happen. While the
idea of using the body's immune cells against cancer has been around for
a long time, the practical reality had proved daunting. Unlike
infection-causing bacteria and viruses that are distinctly foreign to
the body, cancer cells start out as healthy cells that mutate and grow
out of control, and the immune system is loath to target its own cells.
"Only
a handful of people were doing the research," says Dr. Carl June,
director of the Center for Cellular Immunotherapy at the University of
Pennsylvania's Abramson Cancer Center and the scientist who pioneered
the therapy. A graduate of the U.S. Naval Academy, June is all too
familiar with the devastating effects of cancer, having lost his first
wife to ovarian cancer and battled skin cancer himself. Trial after
trial failed as reinfusions of immune cells turned out to be more of a
hit-or-miss endeavor than a reliable road to remission.
After
spending nearly three decades on the problem, June zeroed in on a
malignant fingerprint that could be exploited to stack the deck of a
cancer patient's immune system with the right destructive cells to
destroy the cancer.
In
the case of leukemias, that marker turned out to be CD19, a protein
that all cancerous blood cells sprout on their surface. June repurposed
immune cells to carry a protein that would stick to CD19, along with
another marker that would activate the immune cells to start attacking
the cancer more aggressively once they found their malignant marks.
Using a design initially developed by researchers at St. Jude Children's
Research Hospital for such a combination, June and his colleague Bruce
Levine perfected a way to genetically modify and grow these
cancer-fighting cells in abundance in the lab and to test them in
animals with leukemia. The resulting immune platoon of CAR T cells is
uniquely equipped to ferret out and destroy cancer cells. But getting
them into patients is a complex process. Doctors first remove a
patient's immune cells from the blood, genetically tweak them in the lab
to carry June's cancer-targeting combination and then infuse the
modified cells back into the patient using an IV.
Because
these repurposed immune cells continue to survive and divide, the
therapy continues to work for months, years and, doctors hope, perhaps a
lifetime. Similar to the way vaccines prompt the body to produce immune
cells that can provide lifelong protection against viruses and
bacteria, CAR T cell therapy could be a way to immunize against cancer.
"The word vaccination would not be inappropriate," says Dr. Otis
Brawley, chief medical officer of the American Cancer Society.
June's
therapy worked surprisingly well in mice, shrinking tumors and, in some
cases, eliminating them altogether. He applied for a grant at the
National Cancer Institute at the National Institutes of Health to study
the therapy in people from 2010 to 2011. But the idea was still so new
that many scientists believed that testing it in people was too risky.
In 1999, a teenager died days after receiving an experimental dose of
genes to correct an inherited disorder, and anything involving gene
therapy was viewed suspiciously. While such deaths aren't entirely
unusual in experimental studies, there were ethical questions about
whether the teenager and his family were adequately informed of the
risks and concerns that the doctor in charge of the study had a
financial conflict of interest in seeing the therapy develop. Officials
in charge of the program acknowledged that important questions were
raised by the trial and said they took the questions and concerns very
seriously. But the entire gene-therapy program was shut down. All of
that occurred at the University of Pennsylvania--where June was. His
grant application was rejected.
It
would take two more years before private funders--the Leukemia and
Lymphoma Society and an alumnus of the university who was eager to
support new cancer treatments--donated $5 million to give June the
chance to bring his therapy to the first human patients.
Bill Ludwig with his prized RV Amy Lombard for TIME
The
date July 31 has always been a milestone for Bill Ludwig, a retired
corrections officer in New Jersey. It's the day that he joined the
Marines as an 18-year-old, and the day, 30 years later, that he married
his wife Darla.
It
was also the day he went to the hospital to become the first person
ever to receive the combination gene and CAR T cell therapy, in 2010.
For Ludwig, the experimental therapy was his only remaining option. Like
many people with leukemia, Ludwig had been living on borrowed time for a
decade, counting the days between the chemotherapy treatments that
would hold the cancer in his blood cells at bay for a time. Inevitably,
like weeds in an untended garden, the leukemia cells would grow and take
over his blood system again.
But
the periods of reprieve were getting dangerously short. "I was running
out of treatments," says Ludwig. So when his doctor mentioned the trial
conducted by June and Porter at the University of Pennsylvania, he
didn't hesitate. "I never thought that the clinical trial was going to
cure me," he says. "I just wanted to live and to continue to fight. If
there was something that would put me into the next month, still
breathing, then that's what I was looking for."
When
Ludwig signed the consent form for the treatment, he wasn't even told
what to expect in terms of side effects or adverse reactions. The
scientists had no way of predicting what would happen. "They explained
that I was the first and that they obviously had no case law, so to
speak," he says. So when he was hit with a severe fever, had difficulty
breathing, showed signs of kidney failure and was admitted to the
intensive care unit, he assumed that the treatment wasn't working.
His
condition deteriorated so quickly and so intensely that doctors told
him to call his family to his bedside, just four days after he received
the modified cells. "I told my family I loved them and that I knew why
they were there," he says. "I had already gone and had a cemetery plot,
and already paid for my funeral."
Rather
than signaling the end, Ludwig's severe illness turned out to be
evidence that the immune cells he received were furiously at work,
eliminating and sweeping away the huge burden of cancer cells choking up
his bloodstream. But his doctors did not realize it at the time.
It
wasn't until the second patient, Doug Olson, who received his CAR T
cells about six weeks after Ludwig, that Porter had a eureka moment.
When he received the call that Olson was also running a high fever,
having trouble breathing and showing abnormal lab results, Porter
realized that these were signs that the treatment was working. "It
happens when you kill huge amounts of cancer cells all at the same
time," Porter says. What threw him off initially is that it's rare for
anything to wipe out that much cancer in people with Ludwig's and
Olson's disease. June and Porter have since calculated that the T cells
obliterated anywhere from 2.5 lb. to 7 lb. of cancer in Ludwig's and
Olson's bodies. "I couldn't fathom that this is why they both were so
sick," says Porter. "But I realized this is the cells: they were
working, and working rapidly. It was not something we see with
chemotherapy or anything else we have to treat this cancer."
Ludwig receiving the revolutionary CAR T cell therapy in 2010 Courtesy Bill Ludwig
Ludwig
has now been in remission for seven years, and his success led to the
larger study of CAR T cell therapy in children like Kaitlyn, who no
longer respond to existing treatments for their cancer. The only side
effect Ludwig has is a weakened immune system; because the treatment
wipes out a category of his immune cells--the ones that turned
cancerous--he returns to the University of Pennsylvania every seven
weeks for an infusion of immunoglobulins to protect him from pneumonia
and colds. Olson, too, is still cancer-free.
While
the number of people who have received CAR T cell therapy is still
small, the majority are in remission. That's especially encouraging for
children, whose lives are permanently disrupted by the repeated cycles
of treatments that currently are their only option. "It's a chance for
these kids to have a normal life and a normal childhood that doesn't
involve constant infusions, transfusions, infections and being away from
their home, family and school," says Dr. Gwen Nichols, chief medical
officer of the Leukemia and Lymphoma Society.
The
hope is that while CAR T cell therapy will at first be reserved for
people who have failed to respond to all standard treatments, eventually
they won't have to wait that long. As doctors learn from pioneers like
Kaitlyn, Ludwig and Olson, they will have more confidence in pushing the
therapy earlier, when patients are stronger and the cancer is less
advanced--perhaps as a replacement for or in combination with other
treatments.
The
severe immune reaction triggered by the therapy remains a big concern.
While it can be monitored in the hospital and managed with steroids or
antibodies that fight inflammation, there have been deaths in other
trials involving CAR T cells. One drug company put one of its studies on
hold due to the toxic side effects. "I am excited by CAR T therapy, but
I'm also worried that some people might get too excited," says the
American Cancer Society's Brawley. "It's important that we proceed
slowly and do this meticulously so that we develop this in the right
way."
For
now, CAR T cells are expensive--some analysts estimate that each
patient's batch of cells would cost hundreds of thousands of
dollars--because they require a bespoke production process. If approved,
Novartis, which licensed the technology from the University of
Pennsylvania, will provide the therapy in about 35 cancer centers in the
U.S. by the end of the year. Other companies are already working toward
universal T cells that could be created for off-the-shelf use in any
patient with cancer. "This is just the beginning," says June.
Since
Ludwig's cancer has been in remission, he and his wife have packed
their RV and taken the vacations they missed while he was a slave to his
cancer and chemotherapy schedule. This year, they're visiting Mount
Rushmore, Grand Teton National Park and Yellowstone National Park before
taking their granddaughter to Disney
World in the fall. "When they told me I was cancer-free, it was just
like someone said, 'You won the lottery,'" he says. "If somebody else
with this disease has the chance to walk in my shoes and live past it,
that would be the greatest gift for me."
Fonte: Time
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