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 An advisory committee to the U.S. Food and Drug Administration voted
unanimously to recommend approval of Novartis AG's <NOVN.S>
tisagenlecleucel for treating B-cell acute lymphoblastic leukemia
(ALL) in children and young adults who relapsed or failed
chemotherapy. The FDA is not required to follow the recommendations
of its advisers but typically does so.
Austin Schuetz, who lives in Wisconsin, was treated in 2013 with the
Novartis therapy as part of a clinical trial after leukemia cells
were detected in his brain just two months after a bone marrow
transplant from an anonymous donor.
"We knew it was risky ... but it was the only option for us," said
Kim Schuetz, Austin's mother. She said Austin, then age 6, suffered
fever and severe headaches after the engineered T-cells were
administered, but today shows no signs of cancer.
The new drug class, known as chimeric antigen receptor T-cell or
CAR-T, involves a complicated process of extracting immune system
T-cells from an individual patient, altering the cell DNA to sharpen
their ability to spot and kill cancer cells, and infusing them back
into the patient.
"The majority of calls we are getting are from patients looking for
immunotherapies - particularly CAR-T therapies," said Dr. Gwen
Nichols, chief medical officer at the Leukemia and Lymphoma Society.
Novartis has lagged some other big drugmakers in the first wave of
immunotherapy drugs that are revolutionizing cancer treatment.
Companies including Merck & Co Inc <MRK.N> and Bristol-Myers Squibb
Co <BMY.N> are logging billions of dollars in annual sales of drugs
known as "checkpoint inhibitors" that fight cancer by removing a
brake on the body's immune system.
"The word is out there that this is different from traditional
chemotherapy," Dr. Nichols said.
Between 80 percent and 90 percent of children with ALL are cured
with intense chemotherapy or bone marrow transplant, but there are
few options for remaining patients. "If your child is in that 10 to
20 percent, you are desperate," Dr. Nichols said, while cautioning
that it is too early to tell whether CAR-Ts offer lasting remissions
for patients.
In a clinical trial, 79 percent of patients given the Novartis
therapy were alive a year later. Patients with ALL who fail
chemotherapy typically have only a 16 percent to 30 percent chance
of survival.
CAR-Ts can also pose serious risks, including a potentially
life-threatening inflammatory condition.
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Austin Schuetz, one of a handful of CAR-T patients to achieve
multi-year remission of his cancer, requires biweekly infusions of
immunoglobulin to replace B-cells wiped out by the engineered
cancer-killing T-cells. Without B-cells, his body would not be able
to fight off common infections.
If approved by the FDA, CAR-T therapies could cost up to $500,000
and generate billions of dollars for their developers.
As the cost of cancer drugs increases, health insurers have placed
tighter restrictions on patient access.
"While CAR-T is a promising new type of immunotherapy, it is not
commercially available and we have yet to complete our evaluation,"
T.J. Crawford, a spokesman for health insurer Aetna Inc <AET.N> said
in a statement.
About 6,000 people are diagnosed with ALL in the United States each
year and about 60 percent are children, according to the American
Cancer Society.
The FDA's decision on the Novartis drug, expected by late September,
has significant implications not only for the Switzerland-based
drugmaker but for companies making similar drugs, including Kite
Pharma Inc, Juno Therapeutics Inc and Bluebird bio Inc.
The agency is expected to decide by Nov. 29 whether to approve
Kite's CAR-T, axi-cel, for treatment of adults with advanced and
aggressive lymphoma.
Kite has also reported data showing remission in 73 percent of 11
patients with relapsed ALL treated with axi-cel. It plans to launch
a Phase 2 trial in the fourth quarter.
Juno scrapped its initial CAR-T candidate for ALL after five patient
deaths. The company has since reported early trial results for a
different CAR-T showing that 66 percent of non-Hodgkin lymphoma
patients responded to the drug, and 18 percent suffered severe
neurological side effects.
(Reporting by Deena Beasley in Los Angeles; Editing by Lisa
Shumaker)
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