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Amid an unprecedented turnover in leadership at the FDA and mass layoffs of staff, communication has crumbled and uncertainty runs rampant, leaving small and medium biopharma companies without a clear path forward for their therapies.
Change is hard—especially when a new administration comes in gung-ho to overhaul the entire system. For Health Secretary Robert F. Kennedy Jr., this has meant
slashing some 10,000 jobs
at the Department of Health and Human Services and overseeing an extensive turnover of
leadership at the highest levels
. At the FDA, Commissioner Marty Makary has announced plans to speed drug reviews through avenues such as the
Commissioner’s National Priority Voucher
, expedite rare disease therapies through a yet-to-be-defined
conditional approval pathway
and
ban pharmaceutical representatives
from some advisory committees.
With all this upheaval, many biopharma companies have gotten caught up in the confusion. Ironically, many of them are seeking approval for rare disease therapies.
Capricor Therapeutics, Ultragenyx and Replimune have expressed surprise at recent rejections in
Duchenne muscular dystrophy (DMD) cardiomyopathy
,
Sanfilippo syndrome type A
and
melanoma
, respectively. Meanwhile, three deaths stemming from Sarepta’s gene therapy platform—two of which were associated with its DMD therapy Elevidys—prompted the FDA to request the company halt all shipments of the approved therapy.
Amidst these developments, Center for Biologics Evaluation and Research Director Vinay Prasad
suddenly left his role
,
only to return
less than two weeks later. With rumors swirling of his direct involvement in some regulatory decisions, his temporary ouster only adds to the uncertainty some biotechs are facing.
“These companies who don’t have a lot of cash at hand, they’re actually looking to create these treatments for rare diseases,” Rahul Gupta, president of AI/ML company GATC Health, who served as head of the White House Office of National Drug Control Policy under former President Joe Biden, told
BioSpace
. “They need a very clear framework, a blueprint of what’s acceptable, what’s not acceptable, and how things will go so they’re not feeling like they’re gambling with their limited amount of funds every time they go up to the FDA.”
Here,
BioSpace
unpacks the journeys of five biotechs that have tangled with the new FDA over the past six months.
Sarepta’s Summer Saga
Like it or not, the biopharma story of the summer belongs to Sarepta Therapeutics. The Massachusetts-based biotech had a difficult spring, with
two nonambulatory teenage patients
taking Elevidys succumbing to acute liver injury. It appeared that Sarepta was managing the risks, adding a
black box
warning to Elevidys’ label for acute liver injury and acute liver failure.
But after the
death of a third patient
—a 51-year-old nonambultory man who had been participating in a Phase I study of Sarepta’s SRP-9004 for limb-girdle muscular dystrophy (LGMD), which used the same underlying technology as Elevidys—the FDA acted,
requesting
that Sarepta stop all shipments of the gene therapy in the U.S. and pause all LGMD clinical trials. The agency also revoked the platform designation the biotech had previously been granted for its viral vector technology.
Initially, Sarepta stood its ground, refusing the FDA’s request. Notably, in its July 18 statement, the company said, “We first heard of this potential request earlier in the day at the same time the public and our patient communities did, through media reports.” The company noted in the same press release that it had alerted the FDA to the death on July 3. The agency later confirmed this to be true but
told
STAT News
that the report had been lost in the bureaucracy and that it had, in fact, only learned of the death with the rest of the world when
BioCentury
reported it
. The FDA further stated it had always planned to take action if a third death occurred.
Sarepta ultimately
relented
to the FDA’s request to halt Elevidys shipments, setting off a week of action for patient groups eager to regain access to the treatment. That action apparently worked. On July 28, the FDA did a 180 and
recommended
that the voluntary hold on Elevidys be lifted for ambulatory patients. The following day, Prasad was
out as CBER director
—a development
multiple sources
suggested
was connected to the Sarepta saga.
The “unprecedented” FDA leaks were “missteps” on the part of CBER that sowed confusion for both Sarepta and patients, BMO Capital Markets’ Kostas Biliouris
wrote to investors
on July 30.
Capricor Communication Kerfluffle
Capricor has also reportedly been caught on the carousel of FDA change. The
rejection
of the company’s cell therapy deramiocel in July “was unexpected given the trajectory of positive [FDA] interactions,” CEO Linda Marbán
said
during the company’s second-quarter earnings call on Aug. 11.
Drama reportedly predated the rejection, however.
Nicole Verdun, the former director of the FDA’s Office of Therapeutic Products, and her deputy, Rachael Anatol, were allegedly “put on administrative leave because of an argument about our file, and that Prasad wanted to [reject] us and Nicole was fighting it,” Marbán
told
BioSpace
in an earlier interview, attributing the information to a
STAT
reporter who’d contacted her after receiving a tip from an agency insider.
After Prasad stepped aside from his role on July 29, Marbán expressed optimism about the company’s chances of fighting the rejection. Speaking again with
BioSpace
after his
return
less than 10 days later, she said: “My initial reaction was of great surprise. It was pretty clear that he was asked to leave . . . but I think what it showed is that Makary has tremendous faith in him. We all understand the ramifications of that, that there’s not a lot of ladders you can go up besides the Prasad ladder.”
Nevertheless, Capricor is full speed ahead with its resubmission plans for deramiocel. The biotech met with the FDA on Aug. 13 for a type A meeting to discuss a path forward, but Marbán said she would appreciate an audience with Prasad, who did not attend the meeting.
“We’ve never had any direct communication from or with him. We would like that very much, but nothing so far.”
Ultragenyx’s Unread Responses
Also on July 11, the FDA
declined to approve
Ultragenyx’s investigational
in vivo
gene therapy UX111, which the biotech is proposing for Sanfilippo syndrome type A—an ultrarare disease that leads to neurological symptoms including language and developmental delays and progressive intellectual disability.
On the July 17 edition of
STAT News
’ podcast,
The Readout Loud
, Ultragenyx CEO Emil Kakkis said that a number of issues were raised during the CMC inspection process, which the company was in the process of addressing. Ultragenyx had sent the FDA “a number of very large responses,” Kakkis said. However, at the time of the complete response letter (CRL), “they hadn’t actually read or completed review of the last four responses we had given them. They issued the CRL before they had fully reviewed those responses.”
Ultragenyx “believes that these [CMC] observations are readily addressable and many have already been addressed,” Kakkis said in a prepared statement on July 11. Ultragenyx plans to resubmit an approval application and anticipates another six-month review period for UX111.
Replimune’s Surprise Rejection
In contrast to the other three companies on this list, Replimune can apparently thank a legacy FDA leader for the
rejection
of its candidate. According to reporting by multiple news outlets,
Richard Pazdur
, director of the FDA’s Oncology Center of Excellence (OCE) and acting director of the Office of Oncologic Diseases, directly intervened to issue the CRL for Replimune’s advanced melanoma drug, RP1. Pazdur has been the agency’s chief cancer strategist for
more than 25 years
.
An unnamed FDA official
told
STAT News
on Aug. 4 that CBER “mishandled the RP1 review from the beginning,” compelling Pazdur and his team to get involved. The situation was exacerbated, the individual added, by the leadership upheaval within CBER.
In Replimune’s announcement of the CRL, CEO Sushil Patel expressed surprise with the decision.
“The issues highlighted in the CRL were not raised by the agency during the mid- and late-cycle reviews,” he
said
in a prepared statement. “Additionally, we had also aligned on the design of the confirmatory study. We strongly believe that RP1 in combination with nivolumab [Bristol Myers Squibb’s Opdivo] can bring substantial benefit to advanced melanoma patients.”
On Aug. 5, 22 experts who designed and ran RP1’s Phase III trial
issued an open letter
responding to several issues outlined in the CRL and urging the FDA to “re-review” Replimune’s application.
This decision has had further reverberations as well. Late last month,
Krystal Biotech discontinued
a Phase I/II study of its investigational intratumoral therapy KB707, which it is developing for solid tumors.
Speaking with
STAT,
Stéphane Paquette, Krystal’s vice president for corporate development, said “heightened uncertainty regarding potential accelerated approval pathways” for KB707 following the FDA’s rejection of RP1 contributed to the biotech’s decision.
Novavax’s Delay
When the FDA
missed its deadline
to issue a decision regarding the 2024–2025 formulation of Novavax’s COVID-19 vaccine on April 1,
concern circulated
about what it could mean for the broader vaccines space. While the Maryland-based company did ultimately secure a narrow nod for Nuvaxovid, the approval process represented a potential “harbinger” of a threat to the FDA’s integrity, former FDA associate commissioner
Peter Lurie told
BioSpace
in June.
On April 2,
Politico
reported
that deputy FDA commissioner Sara Brenner directly intervened in the review of Novavax’s vaccine application. A few days later, Kennedy
said
the delay reflected HHS’ “shifting [its] priorities to multiple-antigen vaccines,” causing the company’s shares to drop by 24%. The influence of both Brenner and Kennedy is a significant deviation from normal protocols, Lurie and three other former government officials wrote in an op-ed published in the
Journal of the American Medical Association
in June.
On May 16, the FDA
approved Nuvaxovid
for all seniors aged 65 years and older and people 12 through 64 years of age at high risk for severe outcomes from COVID-19.
Similar restrictions
have now also been applied to the three other vaccines marketed in the U.S.—Pfizer and BioNTech’s Comirnaty and Moderna’s Spikevax and mNEXSPIKE—in line with the FDA’s new
risk-based approach
to COVID-19 vaccination introduced in May.