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 A new analysis in the New England Journal of Medicine concludes
that, in many cases, that's not being done.
Dr. Steven Woloshin of the Dartmouth Institute for Health Policy and
Clinical Practice in Lebanon, New Hampshire, and colleagues looked
at federal records and found that among the 614 studies mandated in
2009 and 2010, 20 percent were never started and 9 percent have been
delayed.
"When drugs are approved, the trials are usually small and
short-term, and some side effects may not emerge until the
post-marketing phase," Woloshin told Reuters Health in a telephone
interview. "The problem is, the faster you get them on the market,
the more open questions there are" about their safety or the best
dose.
In a response published in the Journal, the FDA said that by its
tally, 88 percent of all postmarketing requirements - not just those
mandated in 2009 and 2010 - "were progressing according to their
original schedules" as of the 2015 fiscal year.
One of four drug companies contacted by Reuters Health provided
evidence that the information about its post-approval registry
reported by the Woloshin team is inaccurate.
With President Donald Trump vowing to further speed the FDA approval
process, "Drug approval is likely to become increasingly rapid and
rely on looser evidence standards," the Woloshin team writes in its
report. "It will be crucial to ensure that the important questions
that are unanswered at the time of approval are resolved as quickly
as possible, too."
One example of missed deadlines is Indivior's Suboxone, a
combination of buprenorphine and naloxone used to treat opioid
dependence. The FDA wanted to know if it caused a specific problem
with the heart.
"The sponsor was given more than 1 year to submit the trial protocol
and 5 years to complete the trial," the study authors write.
"Nevertheless, as of July 2017, the final protocol had apparently
not been submitted."
And when Novartis' $72,000-a-year multiple sclerosis treatment
Gilenya (fingolimod) was approved, the FDA told the company to test
a lower daily dose.
"Sometimes a lower dose may be as effective, but have fewer side
effects," Woloshin explained.
Yet "more than 6 years after approval, the trial had not been
completed because of recruitment difficulties despite the
manufacturer reporting $2.8 billion in sales," the researchers
write.
The company released a statement to Reuters Health saying
recruitment was slow because multiple sclerosis therapy has evolved.
Results of the study are expected in the second half of next year.
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One example cited by the researchers is being challenged. The case
involves Victoza, Novo Nordisk's widely-prescribed drug for type 2
diabetes. Animal tests showed it might cause thyroid cancer. The FDA
ordered the company to create a 15-year registry to record cases of
thyroid cancer among users. The deadline for submitting rules for
running the registry was July 2010.
The Woloshin team contends that no protocol for the registry has
been submitted and cites an FDA website showing the registry as
"Delayed."
But company spokesman Ken Inchausti supplied a link to the trial on
the website clinicaltrials.gov showing that enrollment began in
January 2012. He told Reuters Health in an email that 996 patients
have been interviewed to date.
Woloshin and colleagues write that their data show 16 percent of the
ongoing studies are on schedule.
"Although being on schedule is reassuring, we would argue that some
FDA-specified schedules are too long," they write. The team believes
the FDA should set shorter deadlines and impose penalties when
companies miss these deadlines.
"For example,” they write, “the schedule for a 1-year pediatric
safety and efficacy study for Welchol (colesevelam), used to assess
treatment effects on type 2 diabetes in children . . . allowed 6
years for completion; an additional 4-year extension was also
granted."
The drug is marketed in the U.S. by Daiichi Sankyo, Japan's second
largest pharmaceutical company.
In some cases, the FDA has simply dropped a requirement for a
postapproval study without giving a reason. "Adding this information
to its public postapproval database would increase transparency,"
Woloshin's team writes.
The FDA statement does not directly respond to the suggestions.
"Over time, advances in science, changes in standards of care, and
new clinical information can affect study feasibility, design
requirements, and even the need for or the appropriateness of a
study," the agency said.
"The FDA tracks these circumstances carefully and works with
manufacturers to ensure that the postmarketing requirement or
commitment study provides the information needed for public health,"
it added.
SOURCE: http://bit.ly/2xuCDqO The New England Journal of Medicine,
online September 20, 2017.
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