F.D.A. Approves New Treatment for Early Alzheimer’s
·
The
drug, Leqembi, may modestly slow cognitive decline in
early stages of the disease but carries some safety risks. Still, data suggests
it is more promising than the small number of other available treatments.
·
List price for Leqembi (pronounced le-KEM-bee) would be $26,500 per year.
The price is slightly lower than Aduhelm’s
·
To be cost-effective for
patients, the price should be set between $8,500 and $20,600 a year.
·
Very
few patients could afford Aduhelm’s $28,800-a-year
price tag, and the drug has effectively been sidelined
from the marketplace.
·
“Serious adverse events”
occurred in 14 percent of Leqembi patients and 11
percent of those receiving a placebo.
·
It is unclear whether
Medicare will cover Leqembi while it has accelerated
approval.
The newly approved drug, Leqembi,
should be used only for patients in early and mild stages of Alzheimer’s
disease, matching the status of patients in its clinical trials, the F.D.A.
label says.
The Food and Drug Administration on Friday approved
a new Alzheimer’s drug that may modestly slow the pace of cognitive decline
early in the disease, but also carries risks of swelling and bleeding in the
brain.
The approval of the drug, lecanemab,
to be marketed as Leqembi, is likely to generate
considerable interest from patients and physicians. Studies of the drug – an
intravenous infusion administered every two weeks – suggest it is more
promising than the scant number of other treatments available. Still, several
Alzheimer’s experts said it was unclear from the medical evidence whether Leqembi could slow cognitive decline enough to be
noticeable to patients.
Even a recent report of findings from a large
18-month clinical trial, published in the New England Journal of Medicine and
co-written by scientists from the lead company making the drug, concluded that
“longer trials are warranted to determine the efficacy and safety of lecanemab in early Alzheimer’s disease.”
Eisai, a Japanese pharmaceutical company, led the
development and testing of the drug. It is partnering with the American company
Biogen, maker of the controversial Alzheimer’s drug Aduhelm,
for its commercialization and marketing, and the companies will split the
profits equally.
Eisai
said the list price for Leqembi (pronounced
le-KEM-bee) would be $26,500 per year. The price is slightly lower than Aduhelm’s, but higher than that recommended by some
analysts.
“Based on our draft results, that price would
not meet typical cost-effectiveness thresholds,” said Dr.
David Rind, the chief medical officer for the Institute for Clinical and
Economic Review, an independent nonprofit
organization that assesses the value of medicines. In a preliminary report last
month, the institute said that to be cost-effective for patients, the price
should be set between $8,500 and $20,600 a year.
“Given
the large number of patients with Alzheimer’s disease, it is particularly
important that new therapies be priced in line with their value to patients,” Dr. Rind said Friday.
In its
decision, the F.D.A. appeared to be acknowledging the vehement criticism that
erupted when it approved Aduhelm in 2021 after both a
committee of independent advisers and an F.D.A. council of senior officials
said there was not enough evidence that it worked.
Last week, an
18-month investigation by two congressional committees found
that the approval process for Aduhelm was “rife with
irregularities” and involved an unusually close collaboration with Biogen. In
response, the F.D.A. said “the agency has already started implementing changes
consistent with the committees’ recommendations.”
The Leqembi
label says the drug should be used only for patients in early and mild stages
of Alzheimer’s disease, matching the status of patients in the clinical trials
of the drug. It instructs doctors not to treat patients without doing tests to
confirm that they have one of the hallmarks of Alzheimer’s: a buildup of the protein amyloid, which Leqembi
(like Aduhelm) attacks.
“In the case of Leqembi,
more detail and clarity on the most appropriate patient population for use of
the drug, and greater explanation around safety” for brain swelling, brain
bleeding and use of blood thinners with the drug are “now included in the
label,” said the official, who spoke on condition of anonymity to describe
agency deliberations.
The official said the F.D.A. also
requested more data on subgroups of patients characterized by age, gender,
health status and other factors, and that it worked with the companies to
include more diversity in the clinical trials. Participants in the Aduhelm clinical trials were overwhelmingly white, but in
the Leqembi trials about 25 percent of United States
participants were Black or Hispanic.
Ivan Cheung, the chairman and chief
executive of Eisai’s United States operations, said in an interview that in
discussing who should be eligible for the treatment, “we have worked very hard
with the F.D.A. to narrow the population down to a very specific one, the same
as the clinical trials.”
About 1.5 million of the six million
people with Alzheimer’s in the United States are estimated to be in the
beginning phases of the disease, with diagnoses of either mild cognitive
impairment or early-stage Alzheimer’s. How many will be treated with Leqembi will depend significantly on whether Medicare
covers the drug.
Last
year, the federal Centers for Medicare and Medicaid
Services sharply limited Medicare coverage for Aduhelm, citing the treatment’s unclear benefit and safety
risks and allowing payment only for participants in clinical trials. That meant
very few patients could afford Aduhelm’s
$28,800-a-year price tag, and the drug has effectively been sidelined
from the marketplace.
If the agency
determines that Leqembi has clearer evidence of
helping patients, Medicare could cover it for all eligible patients and only
impose a requirement that the patients’ experience be tracked.
Like Aduhelm’s label, Leqembi’s
includes warnings about brain swelling and brain bleeding and notes that
patients with a gene mutation that increases the risk of developing Alzheimer’s
have a greater risk of brain swelling with the treatment.
Leqembi’s label also includes cautionary language
about taking blood thinners while on the treatment, which has been raised as a
concern with anti-amyloid drugs but was not addressed on Aduhelm’s
label. “Additional caution should be exercised” when considering whether to
give blood thinners to a Leqembi patient, the label
says.
Concerns about
safety have been stoked by news reports of the deaths of three patients who
experienced brain swelling and brain bleeding, two of whom were being treated
with blood thinners. Those patients participated in a large Phase 3 trial of
the drug, during which they were not told whether they received it or a
placebo. But their deaths occurred after that phase of the trial, when they
were knowingly being treated with lecanemab in what’s
known as an open-label extension study.
One case, the
subject of a report this week in the New England Journal of
Medicine, involved a 65-year-old woman who had a stroke and, after
receiving a standard treatment for stroke-related blood clots known as t-PA,
experienced serious brain bleeding and died a few days later. In an earlier
article about the case in the journal Science, a
neuropathologist who conducted an autopsy said he believed that Leqembi weakened her blood vessels and made them vulnerable
to bursting when she received the blood clotting treatment.
In
a published letter responding to the New England Journal
of Medicine report, two researchers involved in Eisai’s Leqembi
trial asserted that “t-PA appears to be the proximate cause of death,” not Leqembi, and noted that the woman had two copies of a gene
mutation that increases brain swelling risk with anti-amyloid treatments. But,
they said, “we agree that this case raises important management issues for
patients with Alzheimer’s disease.”
Leqembi —
the brand name, Mr. Cheung said, is based on “qembi”
in Japanese, which “roughly translates into beautiful, healthy, elegant” — was
greenlighted on Friday under a designation called “accelerated approval.” The
F.D.A. can give accelerated approval to drugs with uncertain benefit if they
are for serious diseases with few treatments and attack a biological element of
the disease — in this case, the amyloid protein.
Accelerated approval
was controversial for Aduhelm because the data
involved was contradictory — one clinical trial had failed and another nearly
identical trial showed only slight benefit — and because many Alzheimer’s
experts said years of data had not shown that reducing amyloid slowed cognitive
decline.
With Leqembi, many experts remain unconvinced that attacking
amyloid can provide much noticeable benefit for Alzheimer’s patients. But they
say the data is clearer and more consistent than
with Aduhelm and may be related to the fact that Leqembi targets a different form of amyloid.
Leqembi’s accelerated approval was based on Phase
2 trial data, but in recent months data from a large Phase 3 trial has
supported the earlier results and provided more information. The main positive
outcome of that trial was that patients receiving Leqembi
declined more slowly over 18 months — by less than half a point, 0.45, on an
18-point cognitive scale that assesses functions like memory and
problem-solving — than patients receiving a placebo. (Patients on Leqembi declined by 1.21 points, while patients on placebo
declined by 1.66 points.) That amounts to a 27 percent slower decline.
The Leqembi patients also declined more slowly on three
secondary measures of cognition and daily function, and data on biological
markers was generally stronger for Leqembi than for a
placebo.
“From the
perspective of a scientist, it is exciting that an experimental treatment
targeting brain amyloid in Alzheimer’s disease appears to slow cognitive
decline,” Dr. Madhav Thambisetty,
a neurologist and a senior investigator at the National Institute on Aging,
said about the Phase 3 trial results.
But Dr. Thambisetty added: “From the
perspective of a physician caring for Alzheimer’s patients, the difference
between lecanemab and placebo is well below what is
considered to be a clinically meaningful treatment effect.”
In the Phase 3
trial, nearly 13 percent of patients receiving Leqembi
experienced brain swelling, which was mild or moderate in most cases, while
less than 2 percent of patients receiving the placebo experienced such swelling.
Most brain swelling did not cause any symptoms and generally resolved within a
few months. About 17 percent of Leqembi patients
experienced brain bleeding, compared with 9 percent of patients receiving the
placebo. The most common symptom from brain bleeds was dizziness, the study
said.
The authors reported
that “serious adverse events” occurred in 14 percent of Leqembi
patients and 11 percent of those receiving a placebo. Nearly 7 percent of Leqembi patients dropped out of the trial because of
negative side effects, more than twice the percentage of placebo recipients who
dropped out.
Overall, results
suggest the risk of brain bleeding and swelling was significantly lower than
for patients in trials of Aduhelm.
Accelerated approval
requires companies to conduct another clinical trial of a drug before full
approval can be considered. Mr. Cheung said that, using the Phase 3 trial
results, Eisai intends to quickly apply for full approval.
It is unclear
whether Medicare will cover Leqembi while it has
accelerated approval. Its decision limiting coverage of Aduhelm
technically applies to Leqembi and other medications
in the same class of drugs — monoclonal antibodies that attack amyloid — but
the Medicare agency also said that it would be “nimble” and evaluate each new
medication.
Full approval of Leqembi would make Medicare coverage likely, health
economists say.
In the interview,
citing the Medicare uncertainty, Mr. Cheung sought to lower expectations about
how many patients might be prescribed Leqembi and how
quickly they might start using it. He said that, even if Medicare ends up
covering the drug, in three years “we estimate the number of individuals
potentially on Leqembi is probably about 100,000
people.”
There
are also still many unanswered questions about the drug. For example, Dr. Thambisetty noted, some data
about the drug suggests that it can accelerate brain shrinkage,
which should be investigated because it could be a sign that the pathology of
the disease is worsening. Another question is whether patients with a condition
called cerebral amyloid angiopathy, or C.A.A., should exercise
caution about using Leqembi.
Dr. Michael Irizarry, senior vice president
of clinical research for Eisai, said that, “since C.A.A. is ubiquitous” in
Alzheimer’s, it made sense to allow patients to use Leqembi
with appropriate monitoring because it was the anti-amyloid monoclonal antibody
with the lowest rate of brain swelling and bleeding so far.