Sustained benefit demonstrated with elevated
expression of alpha-galactosidase A (α-Gal A) activity maintained
for nearly four years for the longest treated patient as of the
data cutoff date
Positive mean estimated glomerular filtration
rate (eGFR) slope observed in the 23 patients who had reached at
least one-year follow-up, indicating notable improvements in renal
function
All 18 patients who began study on enzyme
replacement therapy (ERT) have been withdrawn from, and remain off,
ERT
Data to support Accelerated Approval pathway
expected in first half of 2025, with potential Biologics License
Application (BLA) submission to the U.S. Food and Drug
Administration (FDA) anticipated in second half of 2025
Sangamo continues to advance business
development discussions for a potential ST-920 collaboration
Sangamo Therapeutics, Inc. (Nasdaq: SGMO), a genomic medicine
company, today announced updated data from the Phase 1/2 STAAR
study evaluating isaralgagene civaparvovec, or ST-920, a wholly
owned gene therapy product candidate for the treatment of Fabry
disease. Updated data continue to support the potential of
isaralgagene civaparvovec as a one-time, durable treatment option
for Fabry disease that can improve patient outcomes.
These data will be presented at the 21st Annual WORLDSymposiumTM
in San Diego, CA on February 6, 2025, in an oral presentation in
the Clinical Applications session from 9:30-10:30am P.T. and a
poster presentation from 3:30-5:30pm P.T. (Poster Ref: 146). These
data will also be available on Sangamo’s website on the
Presentations page.
“These updated data from the Phase 1/2 STAAR study are highly
encouraging, particularly the positive mean eGFR slope observed in
patients with at least one year of follow-up, indicating
improvements in renal function, an important predicter of morbidity
and mortality in Fabry disease. Additionally, these data show the
strong safety and sustained benefit profiles of ST-920, as well as
its ability to improve key quality of life measures,” said
Professor Derralynn Hughes, MA Dphil FRCP FRCPath, Royal Free
London NHS Foundation Trust and investigator of the Phase 1/2 STAAR
study. “These data support the potential of ST-920 to be a
single-dose, durable treatment option for people living with Fabry
disease.”
“Following our alignment with the FDA on an Accelerated Approval
Pathway for ST-920, we are thrilled with how the data are
progressing, particularly the positive one-year mean eGFR slope
data that will serve as the primary efficacy endpoint for our
regulatory submission,” said Nathalie Dubois-Stringfellow, Ph. D,
Chief Development Officer at Sangamo. “We look forward to building
upon the STAAR study’s positive results as we advance our
interactions with the FDA ahead of the potential BLA submission in
the second half of 2025 and we also continue to engage with the
European Medicines Agency.”
Updated Phase 1/2 STAAR Study Results (as of the September
12, 2024 cut-off date)
Safety (all dosed patients):
- Isaralgagene civaparvovec continued to be generally
well-tolerated, with the majority of adverse events being grade 1-2
in nature.
- No liver function test (LFT) elevations post-dosing requiring
steroids occurred. No adverse events led to study discontinuation
and there were no deaths.
Efficacy (all dosed patients):
- Elevated expression of α-Gal A activity maintained for up to 47
months for the longest treated patient, and up to 27 months for the
longest treated patient receiving the highest dose (2.63x1013
vg/kg).
- All 18 patients who began the study on ERT have been withdrawn
from ERT and all remain off ERT as of today. Plasma lyso-Gb3 levels
in these patients remained stable following ERT withdrawal for up
to 33 months for the longest treated patient.
- Of the 10 patients who had measurable titers of total
antibodies (Ab) or neutralizing antibodies (Nab) against α-Gal A
associated with ERT at baseline, total Ab or NAb titers decreased
markedly in nine patients and became undetectable in seven
following ST-920 treatment.
Efficacy (23 dosed patients followed for
at least 12 months):
- A positive mean annualized eGFR slope of 3.061
mL/min/1.73m2/year (95% confidence interval: 0.863, 5.258) was
observed, indicating notable improvements in kidney function.
- Improvements in disease severity were reported in the Fabry
Outcome Survey adaptation of the Mainz Severity Score Index
(FOS-MSSI) age-adjusted score, with 15 patients showing
improvements in their total MSSI score and seven patients improving
their FOS-MSSI disease category.
- Significant improvements continued to be observed in the short
form-36 (SF-36) quality of life (QoL) scores reported, with a mean
change in General Health score of 10.6 (p=0.0020). For context, a
three- to five-point change on any SF-36 score is considered a
minimally clinically important difference.
- Significant improvements in physical component, bodily pain,
physical, vitality, social function, and emotional SF-36 scores
were also observed.
- Statistically significant improvements continued to be seen in
the gastrointestinal symptom rating scale (GSRS) compared to
baseline.
- Collectively, Sangamo believes these data continue to support
the potential for isaralgagene civaparvovec as a one-time, durable
treatment for Fabry disease that can improve patient outcomes.
Enrollment and dosing are complete in the Phase 1/2 STAAR study.
In October 2024, Sangamo announced that the FDA had provided a
clear regulatory pathway to Accelerated Approval for isaralgagene
civaparvovec using data from ongoing Phase 1/2 STAAR study,
avoiding the requirement for an additional registrational study and
accelerating estimated time to potential approval by approximately
three years. The FDA agreed in a Type B interaction that data from
the ongoing Phase 1/2 STAAR study can serve as the primary basis
for approval under the Accelerated Approval Program, using eGFR
slope at 52 weeks across all patients as an intermediate clinical
endpoint.
The 52-week eGFR slope data from all enrolled patients in the
Phase 1/2 STAAR study will be available in the first half of 2025.
A potential BLA submission is anticipated in the second half of
2025. Sangamo continues to advance business development discussions
regarding a potential ST-920 collaboration agreement.
A Current Report on Form 8-K summarizing the updated preliminary
results from the Phase 1/2 STAAR study in more detail will be filed
by Sangamo, and this press release is subject to the further detail
provided in that Form 8-K.
About the STAAR Study
The Phase 1/2 STAAR study is a global open-label, single-dose,
dose-ranging, multicenter clinical study designed to evaluate
isaralgagene civaparvovec, or ST-920, a gene therapy product
candidate in patients with Fabry disease. Isaralgagene civaparvovec
requires a one-time infusion without preconditioning. The STAAR
study enrolled patients who are on ERT, are ERT pseudo-naïve
(defined as having been off ERT for six or more months), or who are
ERT-naïve. The FDA has granted Orphan Drug, Fast Track and RMAT
designations to isaralgagene civaparvovec, which has also received
Orphan Medicinal Product designation and PRIME eligibility from the
European Medicines Agency and Innovative Licensing and Access
Pathway from U.K. Medicines and Healthcare products Regulatory
Agency.
About Fabry Disease
Fabry disease is a lysosomal storage disorder caused by
mutations in the galactosidase alpha gene (GLA), which leads to
deficient alpha-galactosidase A (α-Gal A) enzyme activity, which is
necessary for metabolizing globotriaosylceramide (Gb3). The buildup
of Gb3 in the cells can cause serious damage to vital organs,
including the kidney, heart, nerves, eyes, gut and skin. Symptoms
of Fabry disease can include decreased or absent sweat production,
heat intolerance, angiokeratoma (skin blemishes), vision problems,
kidney disease, heart failure, gastrointestinal disturbance, mood
disorders, neuropathic pain and tingling in the extremities.
About Sangamo Therapeutics
Sangamo Therapeutics is a genomic medicine company dedicated to
translating ground-breaking science into medicines that transform
the lives of patients and families afflicted with serious
neurological diseases who do not have adequate or any treatment
options. Sangamo believes that its zinc finger epigenetic
regulators are ideally suited to potentially address devastating
neurological disorders and that its capsid discovery platform can
expand delivery beyond currently available intrathecal delivery
capsids, including the central nervous system. Sangamo’s pipeline
also includes multiple partnered programs and programs with
opportunities for partnership and investment. To learn more, visit
www.sangamo.com and connect with us on LinkedIn and X.
Forward-Looking Statements
This press release contains forward-looking statements regarding
Sangamo’s current expectations. These forward-looking statements
include, without limitation, statements relating to: the safety and
efficacy and therapeutic potential of isaralgagene civaparvovec,
including the potential for it to be a one-time, durable treatment
option for Fabry disease that can improve patient outcomes; the
presentation of clinical data from the Phase 1/2 STAAR study; the
potential for isaralgagene civaparvovec to qualify for the FDA’s
Accelerated Approval program, including the adequacy of data
generated in the Phase 1/2 STAAR study to support any such
approval; expectations concerning the availability of additional
data to support a potential BLA submission for isaralgagene
civaparvovec, and the timing of such submission; the potential to
accelerate the expected timeline to approval of isaralgagene
civaparvovec; Sangamo’s plans to advance discussions with the FDA
and the European Medicines Agency; Sangamo’s plans to seek a
potential collaboration partner for ST-920; and other statements
that are not historical fact. These statements are not guarantees
of future performance and are subject to certain risks and
uncertainties that are difficult to predict. Factors that could
cause actual results to differ include, but are not limited to,
risks and uncertainties related to Sangamo’s lack of capital
resources to obtain regulatory approval for and commercialize its
product candidates in a timely manner or at all, including the
ability to secure a collaboration partner for ST-920; the uncertain
timing and unpredictable nature of clinical trial results,
including the risk that the therapeutic effects observed in the
latest preliminary clinical data from the Phase 1/2 STAAR study
will not be durable in patients and that final clinical trial data
from the study will not validate the safety and efficacy of
isaralgagene civaparvovec, including that the 52-week data from the
Phase 1/2 STAAR study will not support a BLA submission and/or that
the 104-week data from such study will not verify the clinical
benefit of isaralgagene civaparvovec or support FDA approval, and
that the patients withdrawn from ERT will remain off ERT; Sangamo’s
need for substantial additional funding to execute its operating
plan and to continue to operate as a going concern; the effects of
macroeconomic factors or financial challenges on the global
business environment, healthcare systems and Sangamo’s business and
operations; the research and development process; the unpredictable
regulatory approval process for product candidates across multiple
regulatory authorities; the potential for technological
developments that obviate technologies used by Sangamo; Sangamo’s
reliance on collaborators and the potential inability to secure
additional collaborations; and Sangamo’s ability to achieve
expected future financial performance.
There can be no assurance that Sangamo and its current or
potential future partners will be able to develop commercially
viable products. Actual results may differ materially from those
projected in these forward-looking statements due to the risks and
uncertainties described above and other risks and uncertainties
that exist in the operations and business environments of Sangamo
and its collaborators. These risks and uncertainties are described
more fully in Sangamo’s Securities and Exchange Commission, or SEC,
filings and reports, including in Sangamo’s Annual Report on Form
10-K for the year ended December 31, 2023, as supplemented by its
Quarterly Report on Form 10-Q for the quarter ended September 30,
2024, each filed with the SEC, and future filings and reports that
Sangamo makes from time to time with the SEC. Forward-looking
statements contained in this announcement are made as of this date,
and Sangamo undertakes no duty to update such information except as
required under applicable law.
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Investor Relations and Media
Inquiries Louise Wilkie ir@sangamo.com media@sangamo.com
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