Data shows that INO-3107 induced new populations of T cells
in the blood that traveled to airway tissue and were associated
with clinical benefit as measured by reduced need for
surgeries
PLYMOUTH
MEETING, Pa., Feb. 12,
2025 /PRNewswire/ -- INOVIO (NASDAQ: INO), a
biotechnology company focused on developing and commercializing DNA
medicines to help treat and protect people from HPV-related
diseases, cancer, and infectious diseases, today announced that
peer-reviewed data from its Phase 1/2 clinical trial with INO-3107
as a potential treatment for recurrent respiratory papillomatosis
(RRP) were published online in Nature Communications under
the title DNA immunotherapy for recurrent respiratory
papillomatosis (RRP): phase 1/2 study assessing efficacy, safety,
and immunogenicity of INO-3107. In the trial, treatment
with INO-3107 induced new populations of T cells in the blood that
traveled to the airway and papilloma tissue and were correlated
with a reduction in the number of post-treatment surgeries. Of the
32 patients in the trial, 26 patients (81%) required fewer
surgeries post-treatment when compared to the year prior to
treatment. INO-3107 treatment was also well tolerated in the trial.
INOVIO plans to submit its biologics license application (BLA) for
INO-3107 in mid-2025 and request rolling submission and priority
review under the FDA's accelerated approval program. If approved,
INO-3107 would be the first DNA medicine approved for any
indication in the United
States.
The Phase 1/2 study showed the majority of participants
experienced a reduced need for surgery, providing great hope for
RRP patients who face both risk of vocal cord damage and immense
impact on their daily lives with every surgery," said Dr.
Peter Belafsky, Director of the
Center for Voice & Swallowing at UC Davis Health and a
principal investigator on the trial. "INO-3107 was designed with
those patient needs in mind and has the potential to transform the
treatment paradigm for RRP."
Dr. Matthew Morrow, INOVIO's Vice
President of Translational Science stated, "The combination of the
full clinical data set and the immunological evaluation described
in this publication allows for a complete view of the immunological
impact of INO-3107, which is a compelling story of a T cell-based
mechanism of action that drives clinical benefit. The publication
describes in detail how INO-3107 engaged both the innate and
adaptive arms of the immune system of treated patients and directly
points to the emergence of new T cell populations after treatment
that traveled to infected tissue to fight RRP."
"These important data characterizing the cytotoxic T cell-based
mechanism of action of INO-3107, in conjunction with our recently
reported durability data showing that clinical benefit continued to
improve through year two and into year three after initial
treatment, with half of patients not requiring any surgeries
in year two, are part of the growing body of evidence that INO-3107
has the potential to be the preferred product of choice for both
patients and healthcare providers," said Dr. Jacqueline Shea, INOVIO's CEO and President.
"The primary goal for RRP patients is to reduce or eliminate the
need for surgery and INO-3107 has the potential to do just that for
the majority of patients. Every surgery matters and a safe and
effective therapeutic alternative to surgery would be truly
life-changing for RRP patients and their caregivers."
Highlights from the Nature Communications
Paper
- 81.3% (26/32) of patients had a decrease of at least one
surgical intervention from the prior year (defined as the Overall
Clinical Response Rate) after INO-3107 administration, including
28.1% (9/32) that required no surgical intervention (Complete
Response) during or after the dosing window
- The Overall Response Rate, which includes those patients who
had either a Complete Response or a Partial Response (defined as ≥
50% reduction in surgeries) was 72%
- Patients in this trial were required to have ≥2 RRP
surgical interventions in the year prior to initiating
treatment
- INO-3107 was well tolerated in the 32 patients enrolled:
- 41% (13/32) of patients reported a treatment-related Adverse
Event (AE)
- Most frequent treatment-related AEs reported were
injection site pain (31%) and fatigue (9%)
- No treatment-related AEs greater than Grade 2 severity
were reported
- INO-3107 induced T cell responses specific to HPV-6 and HPV-11,
including cytotoxic CD8+ T cells, which were still present at week
52, indicating the establishment of a memory response
- INO-3107 expanded clonal T cell populations in peripheral
blood, including induction of new clonal T cell populations that
traveled to airway and papilloma tissue
- INO-3107 induced inflammatory responses in papilloma and airway
tissue associated with antiviral activity, including:
- Interferon, cytokine and chemokine signaling
- Adaptive and innate immune cell infiltration, with emphasis on
T cells
- TCR sequencing provided direct evidence of increased overall T
cell infiltration compared to pre-treatment
- Cytotoxic T cell signatures were observed in T cell infiltrated
papilloma/airway tissue
- T cell infiltration in airway tissues of clinical responders
were predominantly new T cell clonal populations not detectable
prior to INO-3107 treatment
- Enhanced T cell responses were observed in all patients, but
there were differences in the T cell responses between responders
and non-responders that were associated with clinical benefit among
the responders
About RRP
RRP is a debilitating and rare disease
caused primarily by HPV-6 and/or HPV-11. RRP is characterized by
the development of small, wart-like growths, or papillomas, in the
respiratory tract. While papillomas are generally benign, they
can cause severe, life-threatening airway obstruction and
respiratory complications. RRP can also significantly affect
quality of life for patients by affecting the voice box, limiting
the ability to speak effectively. Surgery to remove papillomas is
the standard of care for RRP; however, the papillomas often grow
back. INOVIO's market research to date with patients and healthcare
professionals indicates that a reduction of even one surgery
matters, because every surgery poses a significant risk of causing
permanent damage to the vocal cords. The most widely cited U.S.
epidemiology data published in 1995 estimated that there were
14,000 active cases and about 1.8 per 100,000 new cases in adults
each year.
About INO-3107
INO-3107 is an investigational DNA
medicine designed to elicit an antigen-specific T cell response
against both HPV-6 and HPV-11 proteins. These targeted T cells seek
out and kill HPV-6 and HPV-11 infected cells, with the aim of
potentially preventing or slowing the growth of new papillomas. In
a Phase 1/2 clinical trial conducted with INO-3107 in patients
requiring ≥2 RRP surgical interventions in the year prior to
initiating treatment, 81.3% (26/32) of patients had a decrease in
surgical interventions in the year after INO-3107 administration
compared to the prior year, including 28.1% (9/32) that required no
surgical intervention (Complete Response) during or after the
dosing window. Patients in the trial had a median range of 4
surgeries (2-8) in the year prior to dosing. After dosing, there
was a median decrease of 3 surgical interventions (95% confidence
interval -3, -2). At the outset of the trial (Day 0), patients had
a clinically warranted procedure to have RRP tissue surgically
removed, but any surgery performed after Day 0 during the dosing
window was counted against the efficacy endpoint. Treatment with
INO-3107 generated a strong immune response in the trial, inducing
activated CD4 T cells and activated CD8 T cells with lytic
potential. T cell responses were also observed at Week 52,
indicating a persistent cellular memory response. INO-3107 was well
tolerated, with trial participants experiencing mostly low-grade
(Grade 1) treatment-emergent adverse effects such as injection site
pain and fatigue. Like other DNA medicines, INO-3107 has shown the
ability to generate antigen-specific T cells that is not affected
by anti-vector immunity impacting immunogenicity, either before
administration or after the first dose unlike other T cell
generating platforms such as viral vectors. This feature of DNA
medicines is anticipated to allow INO-3107 to maintain T cell
response and overall efficacy, which could make it an important
therapeutic option for a majority of RRP patients.
The FDA previously granted INO-3107 Orphan Drug designation and
Breakthrough Therapy designation and has advised INOVIO that it can
submit a biologics license application under the FDA's accelerated
approval program using data from INOVIO's already completed Phase
1/2 trial. The European Commission granted INO-3107 Orphan Drug
designation. In addition, INOVIO has CE-marked its
CELLECTRA® delivery device in the EU, which allows
INOVIO to commercialize the device in the EU and other geographies
that recognize CE-marking. The United
Kingdom awarded INO-3107 the Innovation Passport. This
designation serves as the entry point to the Innovative Licensing
and Access Pathway (ILAP), which aims to accelerate time to market
and facilitate patient access to medicines.
About INOVIO's DNA Medicines Platform
INOVIO's DNA
medicines platform has two innovative components: precisely
designed DNA plasmids, delivered by INOVIO's proprietary
investigational medical device, CELLECTRA®. INOVIO uses
proprietary technology to design its DNA plasmids, which are small
circular DNA molecules that work like software the body's cells can
download to produce specific proteins to target and fight disease.
INOVIO's proprietary CELLECTRA® delivery devices are
designed to optimally deliver its DNA medicines to the body's cells
without requiring chemical adjuvants or lipid nanoparticles and
without the risk of the anti-vector response historically seen with
viral vector platforms.
About INOVIO
INOVIO is a biotechnology company focused
on developing and commercializing DNA medicines to help treat and
protect people from HPV-related diseases, cancer, and infectious
diseases. INOVIO's technology optimizes the design and delivery of
innovative DNA medicines that teach the body to manufacture its own
disease-fighting tools. For more information, visit
www.inovio.com.
Forward-Looking Statements
This press release contains
certain forward-looking statements relating to our business,
including the planned submission of a BLA in mid-2025 and plan to
request rolling submission and priority review under the FDA's
accelerated approval program, and the potential clinical benefit of
INO-3107 if approved. Actual events or results may differ from the
expectations set forth herein as a result of a number of factors,
including uncertainties inherent in pre-clinical studies, clinical
trials, product development programs and commercialization
activities and outcomes, the availability of funding to support
continuing research and studies in an effort to prove safety and
efficacy of electroporation technology as a delivery mechanism or
develop viable DNA medicines, our ability to support our pipeline
of DNA medicine products, the ability of our collaborators to
attain development and commercial milestones for products we
license and product sales that will enable us to receive future
payments and royalties, the adequacy of our capital resources, the
availability or potential availability of alternative therapies or
treatments for the conditions targeted by us or collaborators,
including alternatives that may be more efficacious or cost
effective than any therapy or treatment that we and our
collaborators hope to develop, issues involving product liability,
issues involving patents and whether they or licenses to them will
provide us with meaningful protection from others using the covered
technologies, whether such proprietary rights are enforceable or
defensible or infringe or allegedly infringe on rights
of others or can withstand claims of invalidity and whether we can
finance or devote other significant resources that may be necessary
to prosecute, protect or defend them, the level of corporate
expenditures, assessments of our technology by potential corporate
or other partners or collaborators, capital market conditions, the
impact of government healthcare proposals and other factors set
forth in our Annual Report on Form 10-K for the year ended
December 31, 2023, our Quarterly
Report on Form 10-Q for the quarter ended September 30, 2024, and other filings we make
from time to time with the Securities and Exchange Commission.
There can be no assurance that any product candidate in our
pipeline will be successfully developed, manufactured, or
commercialized, that the results of clinical trials will be
supportive of regulatory approvals required to market products, or
that any of the forward-looking information provided herein will be
proven accurate. Forward-looking statements speak only as of the
date of this release, and we undertake no obligation to update or
revise these statements, except as may be required by law.
Contacts
Media: Jennie
Willson (267) 429-8567 communications@inovio.com
Investors: Peter Vozzo, ICR
Healthcare,
443-213-0505 investor.relations@inovio.com
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