Trump administration drug officials clash over how to combat fentanyl
copycats
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 [July 10, 2019]
By Sarah N. Lynch
WASHINGTON (Reuters) - Trump administration
officials are divided over part of a proposal to crack down on illicit
versions of fentanyl, the deadly synthetic painkiller that U.S.
President Donald Trump targeted in declaring a national opioid abuse
emergency.
In an inter-agency dispute that highlights the challenges of curbing
opioid abuse, the U.S. Drug Enforcement Administration (DEA) is publicly
backing tighter rules for fentanyl analogues, which are slightly altered
copycat versions of the powerful drug fueling an explosion in overdoses.
But an office of the U.S. Department of Health and Human Services (HHS)
is raising concerns outside of public hearings, sources told Reuters,
about the DEA-backed legislation, offered by Senator Ron Johnson and
Representative Jim Sensenbrenner, both Republicans.
Normally, the DEA and the U.S. Food and Drug Administration review
chemical compounds individually to assign each one a controlled
substance classification, with the FDA determining if such "scheduling"
decisions are scientifically valid.
In this case, the bill would cut the FDA out of the time-consuming
review process by letting the DEA permanently classify illicit fentanyl
analogues as Schedule I drugs, like heroin, which are deemed to be
addictive with no medical use.
The DEA says these legal changes would help prosecutors keep pace with
criminals who constantly churn out chemically tweaked fentanyl analogues
to evade strict Schedule I regulations.
But an expert from HHS's National Institute on Drug Abuse (NIDA) quietly
warned Senate staff at a private June 20 briefing that permanently
placing all fentanyl analogues into Schedule I poses problems, according
to an attendee who spoke to Reuters anonymously because the briefing was
private.
The draft bill would not only put all fentanyl analogues into Schedule I
before anything is known about their potential medical benefits, but
would also make it harder for researchers to win approval to study the
analogues to potentially develop new approaches to tackling the surge in
overdoses, the NIDA expert said.
An HHS spokesperson told Reuters that the department has no position on
the DEA-backed bill, but confirmed that HHS does have some concerns.
"These compounds can be used to develop and test new medications for
preventing opioid addiction and overdose," the spokesperson said, noting
that putting fentanyl analogues into Schedule I without accommodating
scientists with a streamlined approval process "could slow valuable
research aimed at addressing the opioid crisis."
Of 70,200 U.S. drug overdose deaths in 2017, according to the CDC, about
41% involved synthetic opioids, such as fentanyl and illicit analogues
of it. Most of them are made in China.
Fentanyl, some versions of which are approved to treat cancer pain, is
100 times more potent than morphine.
APPROACHING DEADLINE
While the debate over fentanyl analogues dates back to the Obama
administration, the rising death toll has made the issue more urgent.
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Plastic bags of Fentanyl are displayed on a table at the U.S.
Customs and Border Protection area at the International Mail
Facility at O'Hare International Airport in Chicago, Illinois, U.S.
November 29, 2017. REUTERS/Joshua Lott
Adding to that urgency is a February 2020 deadline, when a temporary
2018 DEA emergency order that placed all fentanyl analogues into
Schedule I will expire.
During a July 1 press briefing, DEA Assistant Administrator John
Martin downplayed the bill's impact on research, but acknowledged
HHS's concerns.
"They have some concerns," he said, adding that DEA is "trying to
eliminate the perception out there in the research community that
it's going to be a hindrance."
Because Schedule I drugs have high risk of abuse, the DEA imposes
strict regulations for research applicants. It requires the drugs to
be stored in a safe bolted to the floor and each compound must have
a separate DEA registration.
"Trying to do research on Schedule I compounds is really difficult
for scientists. There are all kinds of regulatory hurdles," said
Sandra Comer, public policy officer for the College on Problems of
Drug Dependence, a scientific group.
Exactly how many fentanyl analogues would be impacted by the bill is
unknown.
While Martin told reporters in the July 1 briefing it could involve
"hundreds to maybe a thousand" fentanyl analogues, another
government official who participated in the June 20 private briefing
told Senate and other government staffers it could affect "millions"
to "an infinite" number, according to people familiar with the
matter.
A DEA spokeswoman said the agency disagreed with that estimate and
that Martin's estimate was accurate.
Meanwhile, an official with the Office of National Drug Control
Policy told lawmakers in public testimony on June 4 it could
potentially impact more than 3,000 fentanyl analogues.
The DEA did not have any immediate comment on that estimate.
Some groups are urging lawmakers to oppose the bill, saying it would
chill research and give the DEA too much power.
"This administration has tried to take a criminal justice approach
to the overdose crisis," Drug Policy Alliance national affairs
director Michael Collins said, "when it is very clear it is a public
health crisis."
(Reporting by Sarah N. Lynch; Editing by Kevin Drawbaugh and Bill
Berkrot)
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