By Sarah Jane
Tribble and Sydney Lupkin NOVEMBER
30, 2018
The
Food and Drug Administration has failed to ensure that drugs given prized
rare-disease status meet the intent of a 35-year-old law, federal
officials revealed in a report Friday.
The
Government Accountability Office, which spent more than a year investigating
the FDA’s orphan drug program, said “challenges continue” in the program that
was created to spur development of drugs for diseases afflicting fewer than
200,000 patients.
This investigation examines
the booming orphan drug business and how drugmakers have rushed into the
marketplace with hundreds of drugs for rare diseases, helping patients while
landing lucrative federal incentives and monopoly control for every drug that
gets approved.
The
investigation began after a request from three high-profile Republican senators
last year, in the wake of a KHN investigation. KHN
found that the program was being manipulated by drugmakers to maximize profits
and to protect niche markets for medicines being taken by millions.
The GAO
uncovered inconsistent and often incomplete reviews early in the process of
designating medicines as orphan drugs and recommended “executive action” to fix
the system. In some cases, FDA reviewers failed to show they had checked how
many patients could be treated by a drug being considered for orphan drug
status; instead, they appeared to trust what drugmakers told them.
In
response to GAO’s probe, the FDA issued a statement saying it agreed with the
report recommendations regarding documentation and that the agency is
“streamlining our processes.” The agency declined requests for interviews. In a
comment included with the report, Matthew Bassett, assistant secretary for
legislation at the Department of Health and Human Services, said HHS agreed
with GAO’s recommendations.
John
Dicken, director of the GAO’s health care team, said the focus of the report is
“ensuring that the intent of the law is being met.”
The
FDA’s rare-disease program began after Congress overwhelmingly passed the 1983
Orphan Drug Act to motivate pharmaceutical companies to develop drugs for
people who lacked treatments for their conditions. Rare diseases had been
ignored by drugmakers because treatments for them weren’t expected to be profitable.
The law provides fee waivers, tax incentives for research and seven years of
marketing exclusivity for any drug the FDA approves as an “orphan.”
The
incentives, though, have proven to be more powerful and highly coveted than
expected, said Avik Roy, president of the Foundation for Research on Equal
Opportunity, a conservative think tank.
Many
people are “starting to wonder whether or not the Orphan Drug Act
over-corrected for the problem,” Roy said, noting that a third of all pharmaceutical spending
in the U.S. will be on so-called rare-disease medicines in 2020.
GAO
analysts examined FDA records for 148 applications submitted by drugmakers for
orphan drug approval in late 2017. FDA’s reviewers are supposed to apply two
specific criteria — how many patients would be served and whether there is
scientific evidence the drug will treat their disease.
In
nearly 60 percent of the cases, the FDA reviewers did not capture regulatory
history information, including “adverse actions” from other regulatory
agencies. The FDA uses experienced reviewers, Dicken noted, who may already
know the history of certain submitted drugs and not see the need to document
it.
And 15
percent of the time FDA reviewers failed to independently verify patient
estimates provided by the drugmaker.
Of the
148 records the GAO reviewed, 26 applications from manufacturers were granted
orphan status even though the initial FDA staff review was missing information.
“It is
tempting to think that perhaps those approvals were sort of granted routinely
without sufficient scrutiny,” said Bernard Munos, senior fellow at FasterCures
and the Milken Institute.
By
contrast, early Orphan Drug Act advocate Abbey Meyers said she was not
concerned about the lack of population estimates because many rare diseases
lack population studies that show how common a disease is.
Rather,
Meyers said, she’s “disappointed that there is no government-funded agency that
is willing to finance” such research.
The GAO
investigation began after Scott Gottlieb, who took over as FDA commissioner in
May 2017, announced a “modernization” of the rare-disease program.
Critics
have long complained that drugmakers game the FDA’s approval process for orphan
drugs. In January 2017, the KHN investigation, which
was co-published and aired by NPR,
revealed that many orphan drugs aren’t entirely new and don’t always start as
treatments for rare diseases.
The GAO
report, while not analyzing the same years, found that 38.5 percent of orphan
drug approvals from 2008 to 2017 were for drugs that had been previously
approved either for mass-market or rare-disease use. About 71 percent of the
drugs given orphan status were intended to treat diseases affecting fewer than
100,000 people.
KHN’s
investigation found that popular mass-market drugs such as cholesterol
blockbuster Crestor, Abilify for psychiatric conditions, cancer drug Herceptin
and rheumatoid arthritis drug Humira, the best-selling medicine in the world,
all won orphan approval yet were already on the market to treat common
conditions.
In
addition, more than 80 orphan drugs won FDA approval for more than one rare
disease — or several — each one with its own bundle of rich incentives.
Genentech’s
Avastin, a cancer treatment approved for mass-market use in 2004, won three
more orphan-designated approvals this year for the treatment of
three rare forms of cancer. It now has 11 approved orphan uses in all, and
exclusive protections that keep generics at bay won’t run out until 2025.
Sens.
Orrin Hatch (R-Utah), Chuck Grassley (R-Iowa) and Tom Cotton (R-Ark.) sent a
letter in March 2017 asking the GAO to investigate the program and find out
whether Congress’ original intent for it was still being followed.
“Despite
the success of the Orphan Drug Act, 95 percent of rare diseases still have no
treatment options,” Hatch said in a statement Friday. “I hope that my
colleagues will utilize this [GAO] report as they work to strengthen the
accomplishments of the Orphan Drug Act and encourage developers to continue
their investment in this patient population.” The GAO report also mentioned
concerns about prices, noting that “the ability to command high prices” was one
reason the rare-disease market was growing so rapidly.
The
average cost per patient for an orphan drug was $147,308 in 2017 compared with
$30,708 for a mass-market drug, according to a 2018 EvaluatePharma report on the 100
top-selling drugs in the United States. Celgene’s chemotherapy drug Revlimid
was the top-selling orphan with $5.4 billion in sales and $184,011 in revenue
per patient.
“We
have accepted culturally that it’s OK for a company to charge high prices for
[orphan] drugs,” said Roy. “The end result is that a lot of these orphan drugs
are $10 billion drugs, even though they are for rare diseases.”
From
2008 to 2017, more than half of the drugs granted orphan status were for cancer
or blood disorders, according to the GAO report. And nearly two-thirds of drugs
approved in the program were given expedited review processes, such as
accelerated approval or fast-track designation.
Prior
to announcing Gottlieb’s modernization plan, the FDA had a backlog of 138 drug
applications for orphan status that had been waiting more than 120 days. The
backlog was cleared in August 2017 after staff from across the agency stepped
in to help.
KHN’s coverage of prescription drug development, costs and
pricing is supported in part by the Laura and John Arnold Foundation.
Sarah Jane Tribble: sjtribble@kff.org, @SJTribble
Sydney
Lupkin: slupkin@kff.org,
@slupkin
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