SPY001 was well tolerated with a favorable
safety profile consistent with the anti-α4β7 class
SPY001 pharmacokinetics exceeded expectations
with a ~4-fold increase relative to vedolizumab, supporting
potential Q6M maintenance dosing with a single subcutaneous (SC)
injection
Planned Phase 2 induction regimen targets drug
concentrations in quartile 4 of vedolizumab's exposure-response
relationship, which has the potential to increase or accelerate
efficacy
Single, lowest dose of SPY001 led to complete
saturation of α4β7 receptors through Week 12 (longest follow-up
available for pharmacodynamic data)
Company plans to initiate a platform Phase 2
trial in mid-2025 that will include SPY001, followed by SPY002
(TL1A), SPY003 (IL-23), and combinations thereof, providing three
optimized monotherapy readouts and three potentially
paradigm-changing combination readouts under an efficient single
master protocol
Management will host a webcast and conference
call today at 8:00 a.m. ET
WALTHAM,
Mass., Nov. 12, 2024 /PRNewswire/ -- Spyre
Therapeutics, Inc. (NASDAQ: SYRE) (the "Company" or "Spyre"), a
clinical-stage biotechnology company utilizing best-in-class
antibody engineering, rational therapeutic combinations, and
precision medicine approaches to target improved efficacy and
convenience in the treatment of inflammatory bowel disease ("IBD"),
today announced positive interim Phase 1 data from its
first-in-human trial of SPY001, an investigational novel, extended
half-life monoclonal antibody targeting α4β7. SPY001 was well
tolerated with pharmacokinetic ("PK") data demonstrating a
half-life of >90 days and pharmacodynamic ("PD") data
demonstrating complete target engagement at all time points
available.
Interim results from the trial, with data as of October 30, 2024, exceeded the Company's
expectations and support the potential for SPY001 to become a
next-generation anti-α4β7 therapy and backbone for
paradigm-changing combination therapies in IBD. The PK and PD
results support optimized Phase 2 dosing including (i) increased
induction exposures with the potential to improve or accelerate
efficacy compared to other anti-α4β7 treatments and (ii)
maintenance dosing on a potential Q3M and Q6M frequency via a
single subcutaneous injection. Across single doses of up to 1000 mg
and multiple doses of up to 600 mg, SPY001 was well-tolerated with
no serious adverse events reported and all adverse events being
mild in severity. Based on these data, and subject to regulatory
feedback, the Company plans to initiate a Phase 2 platform trial in
mid-2025 that will ultimately include SPY001, SPY002 (TL1A), SPY003
(IL-23) and combinations thereof, providing three optimized
monotherapy readouts and three potentially paradigm-changing
combination readouts under an efficient single master protocol.
"These interim data exceeded our expectations for SPY001 and
support its potential to become both a differentiated monotherapy
and an ideal backbone for combination therapy in IBD," said
Cameron Turtle, DPhil, Chief
Executive Officer of Spyre. "We look forward to initiating Phase 2
trials next year that explore SPY001's safety and efficacy in IBD
patients. Alongside our half-life-extended antibodies targeting
TL1A and IL-23, we believe the Spyre portfolio is uniquely
positioned to develop products that could substantially improve
upon today's standard of care in IBD."
Key SPY001 Phase 1 Interim Findings
The SPY001 Phase 1 trial is a first-in-human, randomized,
double-blind, placebo-controlled trial designed to evaluate safety
and PK of SPY001 in healthy volunteers. To date, the trial has
enrolled 56 healthy adult participants into five single-ascending
dose (SAD) and two multiple-ascending dose (MAD) cohorts. Doses of
SPY001 evaluated in the trial included single doses of 100 mg SC,
300 mg SC, 600 mg SC, 1,000 mg SC, and 1,000 mg IV and multiple
doses of 300 mg SC and 600 mg IV. Findings from the interim SAD and
MAD portions of the Phase 1 trial are as follows:
- Safety – well-tolerated across all dose groups
- Single doses of SPY001 up to 1,000 mg and multiple doses of 600
mg were well tolerated with a favorable safety profile consistent
with existing third-party data of the anti-α4β7 class
- The most common (i.e., occurring in more than one subject)
treatment-emergent adverse events ("TEAEs") were headache and
nasopharyngitis.
- There were no Grade 2 or above TEAEs or serious adverse events
("SAEs"). No AEs led to trial discontinuation
- PK – meaningfully differentiated profile relative to
vedolizumab
- Half-life estimate is >90 days in the 300mg SC cohort and
>100 days in the 600mg SC cohort, ~4-fold greater
than vedolizumab's 25-day human half-life
- SPY001 half-life supports potential for maintenance dosing via
a single subcutaneous injection on a Q3M and Q6M basis using a
high-concentration, citrate-free formulation
- Dose-proportionality and limited intrasubject variability
observed across key parameters (e.g., Cmax, AUC),
support planned Phase 2 induction dosing to evaluate exposures of
SPY001 in 4th quartile of vedolizumab's exposures to
potentially achieve greater clinical remission rates and/or more
rapid clinical effect
- No apparent impact of anti-drug antibodies observed
on pharmacokinetic exposures
- PD – complete saturation of α4β7 receptor occupancy to
latest time point available
- Single 300 mg dose of SPY001 saturated α4β7 receptor occupancy
up to Day 57 (longest follow-up available with pharmacodynamic
data)
- Exploratory immunophenotyping in progress, expected to be
shared at upcoming academic conferences
Spyre expects to share data from additional cohorts and longer
follow-up from existing cohorts at future medical meetings.
Platform Phase 2 trial in Ulcerative Colitis
Pending regulatory feedback, Spyre plans to advance SPY001 into
a double-blind, randomized, placebo-controlled, Phase 2 platform
trial with a master protocol in patients with
moderately-to-severely active ulcerative colitis. The platform
trial is designed to efficiently evaluate each of Spyre's
monotherapy and combination therapies against a common placebo
control. The trial is also intended to evaluate the contribution of
each monotherapy component to the safety and efficacy of Spyre's
combination therapies.
This Phase 2 ulcerative colitis trial is expected to initiate in
mid-2025 with SPY001 and placebo arms, with SPY002, SPY003, and
combination arms to be added following clinical data, nonclinical
data, and regulatory feedback. The trial is expected to enroll
approximately 500 subjects across treatment arms and consist of a
12-week, placebo-controlled induction period followed by a 38-week
maintenance period.
Updated portfolio guidance for maintenance dosing
Given the PK results of SPY001, the Company is updating its
guidance for maintenance dosing across the portfolio to Q3M-Q6M for
monotherapies and combinations. Updated guidance highlights Spyre's
unique ability to target a product profile with potentially
best-in-indication efficacy and convenience.
Conference Call and Webcast
Spyre will host a conference call and webcast today,
November 12, 2024, at 8:00 a.m. ET to discuss the SPY001 Phase 1
interim results. A live webcast of the call will be available on
the Investor Relations website at
https://ir.spyre.com/events-and-presentations. The webcast will be
made available for replay on the company's website following
completion of the event.
About SPY001
SPY001 is an investigational novel, extended half-life
monoclonal antibody targeting α4β7 for the potential treatment of
IBD. IBD is a chronic condition characterized by inflammation in
the gastrointestinal tract and encompasses two main disorders:
ulcerative colitis and Crohn's disease. In the United States, it is estimated that
approximately 2.4 million individuals currently have IBD. SPY001
targets the same epitope as vedolizumab and demonstrates equivalent
potency and selectivity as vedolizumab in head-to-head preclinical
studies. Interim data from a Phase 1 trial demonstrated that SPY001
was well tolerated and exhibited a human half-life of >90 days,
a ~4-fold increase relative to vedolizumab. This half-life supports
potential for both Q3M and Q6M SC maintenance dosing in a single
autoinjector compared to vedolizumab's Q2W SC profile. Based on
initial Phase 1 clinical data, the company plans to initiate a
Phase 2 platform trial in ulcerative colitis in mid-2025.
About Spyre Therapeutics
Spyre Therapeutics is a clinical-stage biotechnology company
that aims to create next-generation of inflammatory bowel disease
(IBD) products by combining best-in-class antibody engineering,
rational therapeutic combinations, and precision medicine
approaches. Spyre's pipeline includes investigational extended
half-life antibodies targeting α4β7, TL1A, and IL-23.
For more information, please
visit http://spyre.com.
Forward-Looking Statements
This press release contains "forward-looking" statements within
the meaning of the safe harbor provisions of the U.S. Private
Securities Litigation Reform Act of 1995. All statements contained
in this press release, other than statements of historical fact are
forward-looking statements. These forward-looking statements
include statements regarding the Company's business strategy,
including the Company's ability to develop best-in-class
therapeutics for IBD that meaningfully improve both efficacy and
convenience compared to today's standard of care, the SPY001
phase 1 trial final data readout, the efficacy, safety and
tolerability of SPY001 and its other product candidates, the
planned induction and maintenance dosing regimen for SPY001 and its
other product candidates, the potential for increased or
accelerated efficacy, the therapeutic benefits of its product
candidates as monotherapies or in combinations and their extended
half-life, the expected design and timing of the platform Phase 2
trial, and that the human PK data is not based on head-to-head
clinical trials and differences exist between trial design and
patient populations which could confound the results. The words
"believe," "may," "will," "potentially," "estimate," "continue,"
"anticipate," "predict," "target," "intend," "could," "would,"
"should," "project," "plan," "expect," the negatives of these
terms, and similar expressions that convey uncertainty of future
events or outcomes are intended to identify forward-looking
statements, although not all forward-looking statements contain
these identifying words. These forward-looking statements involve a
number of risks, uncertainties (some of which are beyond Spyre's
control) or other assumptions that may cause actual results or
performance, final clinical trial data readouts and clinically
trial designs, including the planned Phase 2 trial to be materially
different from those expressed or implied by these forward-looking
statements. These risks and uncertainties include, but are not
limited to the final SPY001 Phase I trial data readouts not being
consistent with or being different than the interim Phase I SPY001
results reported in this press release, regulatory feedback
including potential disagreement by regulatory authorities with the
Company's interpretation of data and the Company's planned clinical
trials for its product candidates, including the Company's planned
Phase 2 clinical trial design and those uncertainties and factors
described under the heading "Risk Factors" and "Note about
Forward-Looking Statements" in Spyre's most recent Quarterly Report
on Form 10-Q filed with the Securities and Exchange Commission, as
well as discussions of potential risks, uncertainties, and other
important factors included in other filings by Spyre from time to
time. Should one or more of these risks or uncertainties
materialize, or should any of Spyre's assumptions prove incorrect,
actual results may vary in material respects from those projected
in these forward-looking statements. Nothing in this press release
should be regarded as a representation by any person that the
forward-looking statements set forth therein will be achieved or
that any of the contemplated results of such forward-looking
statements will be achieved. You should not place undue reliance on
forward-looking statements in this press release, which speak only
as of the date they are made and are qualified in their entirety by
reference to the cautionary statements herein. Spyre does not
undertake or accept any duty to make any updates or revisions to
any forward-looking statements. This press release does not purport
to summarize all of the conditions, risks and other attributes of
an investment in Spyre.
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