Medicenna Therapeutics Corp. (“Medicenna” or the “Company”) (TSX:
MDNA, OTCQX: MDNAF), a clinical-stage immunotherapy company focused
on the development of Superkines, presented updated clinical
results from the ongoing monotherapy dose expansion and combination
dose escalation portions of the Phase 1/2 ABILITY-1
(
A Beta-only
IL-2
ImmunoTherap
Y) study evaluating
MDNA11, a long-acting ‘beta-enhanced not-alpha’ interleukin-2
(IL-2) super-agonist, as monotherapy or in combination with Merck’s
(known as MSD outside of the US and Canada) anti-PD-1 therapy,
KEYTRUDA® (pembrolizumab), in patients with advanced solid tumors,
at the 39th Annual Meeting of the Society for Immunotherapy of
Cancer (SITC), held in Houston, Texas, on November 9th, 2024.
“We are thrilled to share promising results from
the Phase 1/2 ABILITY-1 study, with MDNA11 continuing to show deep
and durable single-agent activity in patients resistant to
checkpoint therapy including 2 patients with metastatic,
treatment-refractory pancreatic cancer,” said Fahar Merchant,
Ph.D., President and CEO of Medicenna. “We are especially pleased
to see that MDNA11 in combination with KEYTRUDA® is demonstrating a
favorable safety profile, robust pharmacodynamics and early signs
of anti-tumor activity in heavily pre-treated patients allowing us
to bolster the dose of MDNA11 to 120 µg/kg every 2 weeks and begin
to evaluate dosing at a more convenient frequency of once every
three weeks. We look forward to sharing additional clinical updates
from the monotherapy and combination arms at medical conferences in
the first half of 2025.”
Key findings from the on-going monotherapy and
combination dose escalation portions of the ABILITY-1 study at the
time of data cut-off (i.e. October 15th, 2024) include:
Monotherapy Tumor Response in Checkpoint
Resistant Patients
MDNA11 continues to demonstrate encouraging deep
and durable single-agent anti-tumor activity among patients who
progressed on prior ICI therapy:
- An objective response rate (ORR) of
30% in the monotherapy dose expansion arm with 3 PRs among 10
patients who had all previously failed ICI therapy and had advanced
and/or metastatic melanoma, non-melanoma skin cancer or MSI-H/dMMR
tumors irrespective of tumor origin.
- The ORR is 25% (1 CR, 4 PR) from a
total of 20 patients when including 10 phase 2 eligible patients
from the MDNA11 monotherapy dose escalation arm who received at
least 60 µg/kg.
- Objective responses included:
- 2 PRs among 3 MSI-H patients (ORR
of 66.7%) with both responders having pancreatic ductal
adenocarcinoma (PDAC). One patient with MSI-H PDAC was initially
misclassified as MSI-H small bowel cancer with metastases in the
pancreas.
- 1 CR and 2 PRs among 11 patients
with cutaneous melanoma (ORR of 27.3%).
- SD in 6 patients including 3 with
duration > 24 weeks, yielding a clinical benefit rate of 40%
(8/20).
Monotherapy Safety Profile
Key findings from the monotherapy dose
escalation and ongoing monotherapy expansion arms of the ABILITY-1
study demonstrate MDNA11’s favorable safety profile:
As previously reported, DLT or vascular leak
syndrome were not observed during monotherapy dose escalation with
a majority (94%) of treatment-related adverse events (TRAEs) being
either grade 1 or 2 and resolving within 48 hours; grade 3 TRAEs
mainly constituted asymptomatic transient LFT elevations; one
isolated grade 4 TRAE was observed with asymptomatic transient LFT
elevation in the monotherapy dose expansion arm which resolved
within 72 hours without intervention. Repeat administration of
MDNA11 at the target doses continues to improve tolerability.
Monotherapy
Pharmacodynamics
Pharmacodynamic analyses showed potent and
durable systemic immune responses following MDNA11 administration
with clear evidence of immune activation in the tumor
microenvironment:
- MDNA11 showed significant increases
in markers of stemness, central and effector memory and enhanced
effector function in circulating CD8+ T and NK cells.
- Analysis of paired biopsies showed
increased tumor infiltration of CD25+ activated CD8+ T cells and NK
cells post-MDNA11 treatment.
Combination Dose Escalation Safety
Profile
No DLTs, grade 4 or 5 TRAEs were observed in
combination dose escalation cohorts 1 or 2 (60 µg/kg Q2W or 90
µg/kg Q2W MDNA11 with 400 mg Q6W KEYTRUDA®) during the DLT
observation period. The Safety Review Committee approved enrollment
of the next higher-dose cohorts as follows:
Cohort 3: 120 µg/kg Q2W MDNA11 and 400 mg Q6W
KEYTRUDA®Cohort 4: 120 µg/kg Q3W MDNA11 and 400 mg Q6W
KEYTRUDA®
Combination Dose Escalation
Pharmacodynamics
Early pharmacodynamic analyses demonstrated
robust lymphocyte expansion which was sustained with repeat dosing
at both 60 µg/kg and 90 µg/kg Q2W MDNA11 in combination with 400 mg
Q6W KEYTRUDA®.
Combination Dose Escalation Tumor
Response
Encouraging preliminary signs of anti-tumor
activity were observed with MDNA11 in combination with KEYTRUDA®
(400 mg Q6W) in dose escalation cohorts 1 (60 µg/kg Q2W MDNA11) and
2 (90 µg/kg Q2W MDNA11). Among 5 heavily pre-treated
efficacy-evaluable patients, tumor control (PR or SD) was observed
in 4 patients including a PR in a microsatellite-stable (MSS) colon
cancer patient.
A copy of the poster and a related slide deck
have been posted on the “Scientific Presentations” page of
Medicenna’s website.
About MDNA11
MDNA11 is an intravenously administered,
long-acting ‘beta-enhanced not-alpha’ IL-2 Superkine specifically
engineered to overcome the shortcomings of aldesleukin and other
next generation IL-2 variants by preferentially activating immune
effector cells (CD8+ T and NK cells) responsible for killing cancer
cells, with minimal or no stimulation of immunosuppressive Tregs.
These unique proprietary features of the IL-2 Superkine have been
achieved by incorporating seven specific mutations and genetically
fusing it to a recombinant human albumin scaffold to improve the
pharmacokinetic (PK) profile and pharmacological activity of MDNA11
due to albumin’s natural propensity to accumulate in highly
vascularized sites, in particular tumor and tumor draining lymph
nodes. MDNA11 is currently being evaluated in the Phase 1/2
ABILITY-1 study as both monotherapy and in combination with
KEYTRUDA®.
About the ABILITY-1 Study
The ABILITY-1 study (NCT05086692) is a global,
multi-center, open-label study that assesses the safety,
tolerability, pharmacokinetics, pharmacodynamics and anti-tumor
activity of MDNA11 as monotherapy or in combination with KEYTRUDA®.
In the combination dose escalation portion of the Phase 2 study,
approximately 6-12 patients are expected to be enrolled and
administered ascending doses of MDNA11 intravenously in combination
with KEYTRUDA®. This portion of the study includes patients with a
wide range of solid tumors with the potential for susceptibility to
immune modulating therapeutics. Upon identification of an
appropriate dose regimen for combination, the study will proceed to
a combination dose expansion cohort.
About Medicenna Therapeutics
Medicenna is a clinical-stage immunotherapy
company focused on developing novel, highly selective versions of
IL-2, IL-4 and IL-13 Superkines and first-in-class Empowered
Superkines. Medicenna’s long-acting IL-2 Superkine, MDNA11, is a
next-generation IL-2 with superior affinity toward CD122 (IL-2
receptor beta) and no CD25 (IL-2 receptor alpha) binding, thereby
preferentially stimulating cancer-killing effector T cells and NK
cells. MDNA11 is being evaluated in the Phase 1/2 ABILITY-1 Study
(NCT05086692) as a monotherapy and in combination with
pembrolizumab. Medicenna’s IL-4 Empowered Superkine, bizaxofusp
(formerly MDNA55), has been studied in 5 clinical trials enrolling
over 130 patients, including a Phase 2b trial for recurrent GBM,
the most common and uniformly fatal form of brain cancer.
Bizaxofusp has obtained FastTrack and Orphan Drug status from the
FDA and FDA/EMA, respectively. Medicenna’s early-stage
high-affinity IL-2β biased IL-2/IL-15 Super-antagonists, from its
MDNA209 platform, are being evaluated as potential therapies for
autoimmune and graft-versus host diseases. Medicenna’s early-stage
BiSKITs™ (Bifunctional SuperKine ImmunoTherapies) and the T-MASK™
(Targeted Metalloprotease Activated SuperKine) programs are
designed to enhance the ability of Superkines to treat
immunologically “cold” tumors.
For more information, please
visit www.medicenna.com, and follow us on Twitter
and LinkedIn.
KEYTRUDA® is a registered trademark of Merck
Sharp & Dohme LLC, a subsidiary of Merck & Co., Inc.,
Rahway, NJ, USA.
Forward-Looking Statements
This news release contains forward-looking
statements within the meaning of applicable securities laws.
Forward-looking statements include, but are not limited to, express
or implied statements regarding the future operations of the
Company, estimates, plans, strategic ambitions, partnership
activities and opportunities, objectives, expectations, opinions,
forecasts, projections, guidance, outlook or other statements that
are not historical facts, such as statements on the therapeutic
potential and safety profile of MDNA11 (both as monotherapy and in
combination with KEYTRUDA®), and the timing and/or release of any
additional clinical updates. Drug development and commercialization
involve a high degree of risk, and only a small number of research
and development programs result in commercialization of a product.
Results in early-stage pre-clinical or clinical studies may not be
indicative of full results or results from later stage or larger
scale clinical studies and do not ensure regulatory approval. You
should not place undue reliance on these statements, or the
scientific data presented.
Forward-looking statements are often identified
by terms such as “will”, “may”, “should”, “anticipate”, “expect”,
“believe”, “seek”, “potentially” and similar expressions. and are
subject to risks and uncertainties. There can be no assurance that
such statements will prove to be accurate and actual results and
future events could differ materially from those anticipated in
such statements. Important factors that could cause actual results
to differ materially from the Company’s expectations include the
risks detailed in the latest annual information form of the Company
and in other filings made by the Company with the applicable
securities regulators from time to time in Canada.
The reader is cautioned that assumptions used in
the preparation of any forward-looking information may prove to be
incorrect. Events or circumstances may cause actual results to
differ materially from those predicted, as a result of numerous
known and unknown risks, uncertainties, and other factors, many of
which are beyond the control of the Company. The reader is
cautioned not to place undue reliance on any forward-looking
information. Such information, although considered reasonable by
management, may prove to be incorrect and actual results may differ
materially from those anticipated. Forward-looking statements
contained in this news release are expressly qualified by this
cautionary statement. The forward-looking statements contained in
this news release are made as of the date hereof and except as
required by law, we do not intend and do not assume any obligation
to update or revise publicly any of the included forward-looking
statements.
This news release contains hyperlinks to
information that is not deemed to be incorporated by reference in
this new release.
Investor/Media Contact:
Christina CameronInvestor Relations, Medicenna Therapeutics(647)
953-0673ir@medicenna.com
Medicenna Therapeutics (TSX:MDNA)
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