- On track to initiate a Phase 3 program for Company’s lead asset
avexitide, a GLP-1 receptor antagonist with FDA Breakthrough
Therapy and Orphan Drug Designations, in post-bariatric
hypoglycemia (PBH) in the first quarter of 2025
- Reported positive topline data from Phase 2 HELIOS clinical
trial of AMX0035 in Wolfram syndrome demonstrating improvement or
stabilization across all disease measures at Week 24 and sustained
improvement at Weeks 36 and 48
- Cash, cash equivalents and marketable securities of $234.4
million as of September 30, 2024; cash runway expected into
2026
- Management to host conference call and webcast today at 8:00
a.m. Eastern Time
Amylyx Pharmaceuticals, Inc. (Nasdaq: AMLX) (“Amylyx” or the
“Company”) today reported financial results for the third quarter
ended September 30, 2024.
“This quarter, we continued to advance our late-stage pipeline
as part of our goal to bring new potential treatments to
communities with high unmet needs. We recently reported positive
topline data from our Phase 2 HELIOS clinical trial in people
living with Wolfram syndrome that show AMX0035 resulted in
meaningful improvements across multiple measures of disease
progression as well as sustained improvement over time. We plan to
engage with the FDA and other stakeholders to inform our Phase 3
program in Wolfram,” said Joshua Cohen and Justin Klee, Co-CEOs of
Amylyx. “Additionally, we are on track to initiate a Phase 3
program for our lead asset avexitide in post-bariatric hypoglycemia
in the first quarter of next year and remain on track to report
interim data from our Phase 2b/3 ORION clinical trial of AMX0035 in
progressive supranuclear palsy in mid-2025. With cash runway into
2026, we believe we are well positioned to deliver on these
milestones as we continue our critical work in neurodegenerative
diseases and endocrine conditions.”
Third Quarter and Recent Updates:
- Announced positive topline data for all 12 participants in
the Phase 2 HELIOS clinical trial, a single-site, single-arm,
open-label trial of AMX0035 (sodium phenylbutyrate [PB] and
taurursodiol [TURSO, also known as ursodoxicoltaurine]) in adults
living with Wolfram syndrome. Wolfram syndrome is a rare,
progressive, monogenic disease impacting approximately 3,000 people
in the U.S. HELIOS showed improvement in pancreatic function, as
measured by C-peptide response after 24 weeks of treatment with
AMX0035, the trial’s primary efficacy endpoint, in contrast to the
expected decrease in pancreatic function with disease progression.
Similar overall improvements or stabilization were observed across
all secondary endpoints, including hemoglobin A1c (HbA1c), time in
target glucose range assessed by continuous glucose monitoring
(CGM), and visual acuity. The safety profile of AMX0035 in HELIOS
was consistent with prior safety data. The Company is engaging with
stakeholders and plans to meet with the U.S. Food and Drug
Administration (FDA) to inform a Phase 3 program and expects to
provide an update in 2025.
- Acquired avexitide, a Phase 3-ready glucagon-like peptide-1
(GLP-1) receptor antagonist with FDA Breakthrough Therapy
Designation and Orphan Drug Designation in hyperinsulinemic
hypoglycemia. Avexitide has been evaluated in five clinical
trials for post-bariatric hypoglycemia (PBH) and has also been
studied in three clinical trials for congenital hyperinsulinism
(HI), two indications characterized by hyperinsulinemic
hypoglycemia. In previous Phase 2 and Phase 2b studies in PBH,
avexitide showed statistically significant reductions in
hypoglycemia events. FDA guidance for industry combined with
initial FDA feedback specific to the planned pivotal Phase 3
program of avexitide for PBH suggest that reduction in hypoglycemia
events could be an endpoint to support approval following positive
results from a pivotal Phase 3 clinical trial.
- Announced publication of data showing encouraging effects of
AMX0035 on cerebrospinal fluid (CSF) biomarkers of core Alzheimer’s
disease (AD) pathology and neurodegeneration in the peer-reviewed
medical journal Alzheimer’s & Dementia: Translational
Research & Clinical Interventions, a journal of the
Alzheimer’s Association. The exploratory analyses on CSF
biomarkers from participants with AD from the Phase 2 PEGASUS
clinical trial suggest that treatment with AMX0035 resulted in
consistent changes in AD and neurodegeneration CSF biomarkers in
participants with a broad range of disease severity. Findings from
the exploratory analysis provide preliminary evidence that AMX0035
engages multiple pathological pathways related to
neurodegeneration, including tau.
- Presented the planned Phase 1 study design of AMX0114 in
people living with amyotrophic lateral sclerosis (ALS) at the 2024
Northeast ALS Consortium Annual Meeting. The Phase 1 LUMINA
clinical trial, a multicenter, randomized, placebo-controlled,
multiple ascending dose trial, will evaluate the safety and
biological activity of AMX0114 in approximately 48 people living
with ALS. Four dose levels of AMX0114 or placebo are planned to be
examined sequentially starting with 12.5 mg.
- Received clearance from Health Canada for the Company’s
Clinical Trial Application for AMX0114 in people living with ALS.
Amylyx plans to begin the LUMINA trial with a starting dose of 12.5
mg in Canada by the end of 2024 or in early 2025. The Company
also submitted an Investigational New Drug application to the FDA
for AMX0114. The FDA restricted dosing to an amount that is lower
than the Company’s proposed starting dose of 12.5 mg and has
requested additional information, which resulted in a clinical
hold. Toxicology data from studies showed a greater than 10X safety
margin at the starting dose of 12.5 mg based on the no observed
adverse effect level (NOAEL) determined by independent toxicology
firms. Amylyx is working to address FDA comments and believes the
trial can be completed outside of the U.S. if needed. The Company
expects early cohort data from LUMINA in 2025.
Upcoming Expected Milestones:
- The Company plans to initiate the Phase 1 LUMINA clinical
trial of AMX0114 in people living with ALS by the end of 2024 or in
the beginning of 2025 in Canada. AMX0114 is an antisense
oligonucleotide targeting inhibition of calpain-2, a
well-established target in a number of neurological diseases and a
protease known to cleave many substrates including neurofilament,
tau, and TDP43 proteins. Amylyx expects early cohort data from
LUMINA in 2025.
- Amylyx continues to expect initiation of its Phase 3 program
for avexitide in PBH in the first quarter of 2025. Topline data
are anticipated in 2026.
- Data from an interim analysis of the Phase 2b/3 ORION
clinical trial of AMX0035 in progressive supranuclear palsy (PSP)
continue to be expected in mid-2025. ORION is an operationally
seamless Phase 2b/3 clinical trial. The Phase 2b portion will
include approximately 100 people living with PSP. Amylyx plans to
conduct an interim analysis in these participants through Week 24
and will use this data to inform a go/no-go decision on the Phase 3
portion of the trial in mid-2025.
Financial Results for the Third Quarter Ended September 30,
2024
Net product revenue: Net product revenue was $0.4 million
for the three months ended September 30, 2024 and was related to
adjustments to the Company’s gross-to-net accrual estimates for
prior period sales of RELYVRIO® and ALBRIOZA™. As previously
disclosed, on April 4, 2024, the Company announced that it had
started a process with the FDA and Health Canada to voluntarily
discontinue the marketing authorizations for RELYVRIO and ALBRIOZA
and remove the product from the market based on topline results
from the global Phase 3 PHOENIX trial, which did not meet its
prespecified primary and secondary endpoints.
Cost of Sales: Cost of sales were $0.8 million in the
three months ended September 30, 2024, and were related to
estimated losses on firm commitments under commercial manufacturing
supply agreements for AMX0035 that were established prior to the
results from the Phase 3 PHOENIX trial.
Acquired in-process research and development: Acquired
in-process research and development expenses were $36.2 million for
the three months ended September 30, 2024, compared to zero for the
same period in 2023. The increase was due to the acquired
in-process research and development assets of avexitide.
R&D Expenses: Research and development expenses were
$21.2 million for the three months ended September 30, 2024,
compared to $30.0 million for the same period in 2023. The decrease
was primarily due to a decrease in clinical expenses and a decrease
in payroll and personnel-related costs. The decrease in clinical
expenses is primarily due to a decrease in spending on AMX0035 for
the treatment of ALS following the topline data from the PHOENIX
trial. The decrease in payroll and personnel-related costs was
primarily related to a decrease in the number of employees
following the restructuring plan announced on April 4, 2024.
SG&A Expenses: Selling, general and administrative
expenses were $17.8 million for the three months ended September
30, 2024, compared to $48.7 million for the same period in 2023.
The decrease was primarily due to a decrease in payroll and
personnel-related costs and a decrease in consulting and
professional services. The decrease in payroll and
personnel-related costs was primarily related to a decrease in the
number of employees as a result of the restructuring plan announced
on April 4, 2024. The decrease in consulting and professional
services was primarily due to a decrease in commercial sales and
marketing activity as a result of removing RELYVRIO/ALBRIOZA from
the markets in the U.S. and Canada based on topline results from
the Phase 3 PHOENIX trial.
Net Loss: Net loss for the three months ended September
30, 2024, was $72.7 million, or $1.07 per share, compared to net
income of $20.9 million, or $0.30 per diluted share for the same
period in 2023.
Cash Position: Cash, cash equivalents, and marketable
securities were $234.4 million as of September 30, 2024, compared
to $309.8 million as of June 30, 2024. The Company expects cash
runway into 2026.
Investor Conference Call Information
Amylyx’ management team will host a conference call today,
November 7, 2024, at 8:00 a.m. ET to discuss financial results and
provide an update on the business. To access the conference call,
please dial +1 (800)-836-8184 (U.S. & Canada) or +1
(646)-357-8785 (international) at least 10 minutes prior to the
start time and ask to be joined into the Amylyx Pharmaceuticals
call. A live audio webcast of the call will be available under
“Events and Presentations” in the Investor section of the Company’s
website, https://investors.amylyx.com/news-events/events. The
webcast will be archived and available for replay for 90 days
following the event.
Available Information
We periodically provide other information for investors on our
corporate website, https://amylyx.com, and our investor relations
website, https://investors.amylyx.com. This includes press releases
and other information about financial performance, information on
corporate governance, and details related to our annual meeting of
stockholders. We intend to use our website as a means of disclosing
material non-public information and for complying with our
disclosure obligations under Regulation FD. Accordingly, investors
should monitor our website, in addition to following the Company’s
press releases, SEC filings, and public conference calls and
webcasts.
About Avexitide
Avexitide is an investigational, first-in-class glucagon-like
peptide-1 (GLP-1) receptor antagonist that has been evaluated in
five Phase 2 clinical studies for post-bariatric hypoglycemia (PBH)
and has also been studied in congenital hyperinsulinism (HI), with
U.S. Food and Drug Administration (FDA) Breakthrough Therapy
Designation for both indications and FDA Rare Pediatric Disease
Designation in congenital HI. Avexitide is designed to bind to the
GLP-1 receptor on pancreatic islet beta cells and block the effect
of excessive GLP-1 to mitigate hypoglycemia by decreasing insulin
secretion and stabilizing glucose levels. In PBH, excessive GLP-1
can lead to the hypersecretion of insulin and subsequent serious
hypoglycemia events. In two Phase 2 PBH trials, avexitide
demonstrated highly statistically significant reductions in
hypoglycemia events. These events can lead to autonomic and
neuroglycopenic symptoms that can have a devastating impact on
daily living.
About AMX0035
AMX0035 is an oral, fixed-dose combination of sodium
phenylbutyrate (PB) and taurursodiol (TURSO; also known as
ursodoxicoltaurine outside of the U.S.). AMX0035 was designed to
slow or mitigate neurodegeneration by targeting endoplasmic
reticulum (ER) stress and mitochondrial dysfunction, two connected
central pathways that lead to cell death and neurodegeneration. We
believe that our proprietary combination of PB and TURSO and their
complementary mechanisms of action will allow us to synergistically
target abnormal cell death to better prevent neurodegeneration than
treatment targeted at either mechanism of action alone. AMX0035 is
being studied as a potential treatment for Wolfram syndrome and
progressive supranuclear palsy, two neurodegenerative diseases.
About AMX0114
AMX0114 is an investigational antisense oligonucleotide designed
to target the gene encoding calpain-2, a key contributor to the
axonal (Wallerian) degeneration pathway. Axonal degeneration has
been recognized as an important early contributor to the clinical
presentation and pathogenesis of ALS and other neurodegenerative
diseases. Calpain-2 has been implicated in the pathogenesis of ALS
based on findings of elevated levels of calpain-2 and its cleavage
products in postmortem ALS tissue, therapeutic benefit of calpain-2
modulation in animal models of ALS, and the role of calpain-2 in
cleaving neurofilament, a broadly researched biomarker in ALS.
Preclinical studies completed to date have shown that AMX0114
achieves potent, dose-dependent, and durable knockdown of CAPN2
mRNA expression and calpain-2 protein levels in human motor
neurons. Moreover, in preclinical efficacy studies, treatment with
AMX0114 reduced extracellular neurofilament light chain levels
following neurotoxic insult in induced pluripotent stem cell
(iPSC)-derived human motor neurons, and improved survival of
iPSC-derived human motor neurons harboring ALS-linked, pathogenic
TDP-43 mutations.
About Post-Bariatric Hypoglycemia (PBH)
Symptomatic post-bariatric hypoglycemia (PBH) is a condition
that affects approximately 8% of people who have undergone
bariatric surgery. It is characterized by an excessive
glucagon-like peptide-1 (GLP-1) response, dysregulated secretion of
insulin, and a rapid drop in blood sugar. PBH can cause serious
hypoglycemia events associated with brain glucose starvation, known
as neuroglycopenia, including impaired cognition, cardiac
arrythmias, loss of consciousness, and seizures. PBH is associated
with a high degree of disability and can result in major
disruptions to life, including falls, motor vehicle accidents, and
job and income loss. It is estimated that ~160,000 people are
currently living with symptomatic PBH in the U.S., classifying it
as an orphan condition.
About Congenital Hyperinsulinism (HI)
Congenital hyperinsulinism (HI) is a rare disease characterized
by hypersecretion of insulin leading to severe, persistent
hypoglycemia in infants and young children with limited therapeutic
options. Common symptoms of congenital HI include lack of energy,
irritability, lethargy, and excessive hunger. Repeated episodes of
low blood glucose increase the risk for serious complications such
as breathing difficulties, seizures, intellectual disability,
vision loss, brain damage, and coma.
About the HELIOS Trial
HELIOS (NCT05676034) is a 12-participant, single-site,
single-arm, open-label, proof of biology, Phase 2 trial designed to
study the effect of AMX0035 on safety and tolerability, and various
measures of endocrinological, neurological, and ophthalmologic
function in adult participants living with Wolfram syndrome.
Participants in HELIOS receive AMX0035 for up to 96 weeks followed
by a four-week safety follow-up. Primary and secondary outcomes are
assessed at Week 24 and at longer-term time points.
In September 2022, researchers from Washington University School
of Medicine in St. Louis, including Dr. Urano, in collaboration
with Amylyx, published preclinical data on AMX0035 in beta cell,
neuronal cell, and mouse models of Wolfram syndrome in the
peer-reviewed Journal of Clinical Investigation Insight. The FDA
and the European Commission granted Orphan Drug Designation to
AMX0035 for the treatment of Wolfram syndrome in November 2020 and
August 2024, respectively.
About Wolfram Syndrome
Wolfram syndrome is a rare, monogenic neurodegenerative disease
characterized by childhood-onset diabetes, optic nerve atrophy, and
neurodegeneration. Common manifestations of Wolfram syndrome
include diabetes mellitus and diabetes insipidus, gradual vision
loss leading to blindness, hearing loss, neurogenic bladder,
difficulties with balance and coordination, and difficulty
breathing. Genetic and experimental evidence suggests that
endoplasmic reticulum (ER) dysfunction is a critical pathogenic
component of Wolfram syndrome. The prognosis of Wolfram syndrome is
poor, and many people with the disease die prematurely with severe
neurological disabilities.
About the ORION Trial
The ORION trial (NCT06122662) is a global, randomized,
double-blind, placebo-controlled Phase 2b/3 clinical trial designed
to assess the efficacy, safety, and tolerability of AMX0035
compared to placebo in people living with progressive supranuclear
palsy (PSP). ORION was designed and planned in collaboration with
key global academic leaders, people living with PSP and their
caregivers, and industry advocacy organizations.
About PSP
Progressive supranuclear palsy (PSP) is a sporadic, rare, and
fatal neurodegenerative disorder that affects movement, gait,
balance, eye movements, swallowing, and speech. People living with
PSP have a life expectancy of six to eight years after initial
diagnosis. PSP typically begins in late-middle age and rapidly
progresses over time. The disease affects approximately seven in
100,000 people worldwide, and there are currently no
disease-modifying therapies approved for the treatment of PSP.
PSP is characterized by abnormal tau inclusions and is
consequently also known as a tauopathy. Similar to other
neurodegenerative diseases, pathophysiologic changes underlying PSP
are multifactorial, with several genetic and environmental factors
likely contributing to tau dysfunction and aggregation.
Multiple pathways, including genetic mutations, endoplasmic
reticulum (ER) stress, and the activation of unfolded protein
response, mitochondrial dysfunction, and neuroinflammation have
been implicated as contributors to tau dysfunction and
aggregation.
About ALS
Amyotrophic lateral sclerosis (ALS, also known as motor neuron
disease) is a relentlessly progressive and fatal neurodegenerative
disorder caused by motor neuron death in the brain and spinal cord.
Motor neuron loss in ALS leads to deteriorating muscle function,
the inability to move and speak, respiratory paralysis, and
eventually, death. More than 90% of people with ALS have sporadic
disease, showing no clear family history. ALS affects around 30,000
people in the U.S., and more than 30,000 people are estimated to be
living with ALS in Europe (European Union and the United Kingdom).
People living with ALS have a median survival of approximately two
years from diagnosis.
About Amylyx Pharmaceuticals
Amylyx is committed to the discovery and development of new
treatment options for communities with high unmet needs, including
people living with serious and fatal neurodegenerative diseases and
endocrine conditions. Since its founding, Amylyx has been guided by
science to address unanswered questions, keeping communities at the
heart and center of all decisions. Amylyx is headquartered in
Cambridge, Massachusetts. For more information, visit amylyx.com
and follow us on LinkedIn and X. For investors, please visit
investors.amylyx.com.
Forward-Looking Statements
Statements contained in this press release and related comments
in our earnings conference call regarding matters that are not
historical facts are “forward-looking statements” within the
meaning of the Private Securities Litigation Reform Act of 1995, as
amended. Because such statements are subject to risks and
uncertainties, actual results may differ materially from those
expressed or implied by such forward-looking statements. Such
statements include, but are not limited to, the potential of
avexitide as a treatment for PBH and HI; expectations regarding the
timing of initiation of a Phase 3 trial of avexitide in PBH; the
potential of AMX0035 (sodium phenylbutyrate and taurursodiol) as a
treatment for Wolfram syndrome and PSP or other neurodegenerative
diseases; expectations regarding the timing of the announcement of
results from the Company’s Phase 3 ORION trial of AMX0035 for the
treatment of PSP; planned discussions with regulatory authorities
related to AMX0035 for the treatment of Wolfram syndrome; the
potential for AMX0114 as a treatment for ALS and the planned
initiation of a trial evaluating AMX0114 in ALS, including
potential expansion into the U.S.; the Company’s expectations
regarding its financial performance; and expectations regarding the
Company’s cash runway and longer-term strategy. Any forward-looking
statements in this press release and related comments in the
Company's earnings conference call are based on management’s
current expectations of future events and are subject to a number
of risks and uncertainties that could cause actual results to
differ materially and adversely from those set forth in or implied
by such forward-looking statements. Risks that contribute to the
uncertain nature of the forward-looking statements include: the
success, cost, and timing of Amylyx’ program development
activities; Amylyx’ ability to execute on its regulatory
development plans and expectations regarding the timing of results
from its planned data announcements and initiation of clinical
studies; the risk that early-stage results may not reflect
later-stage results; Amylyx’ ability to fund operations, and the
impact that global macroeconomic uncertainty, geopolitical
instability, and public health events will have on Amylyx’
operations, as well as the risks and uncertainties set forth in
Amylyx’ United States Securities and Exchange Commission (SEC)
filings, including Amylyx’ Annual Report on Form 10-K for the year
ended December 31, 2023, and subsequent filings with the SEC. All
forward-looking statements contained in this press release and
related comments in our earnings conference call speak only as of
the date on which they were made. Amylyx undertakes no obligation
to update such statements to reflect events that occur or
circumstances that exist after the date on which they were
made.
AMYLYX PHARMACEUTICALS,
INC.
CONDENSED CONSOLIDATED BALANCE
SHEETS
UNAUDITED
(in thousands)
September 30, 2024
December 31, 2023
Assets
Cash, cash equivalents and short-term
investments
$
234,395
$
371,362
Accounts receivable, net
1,731
40,050
Inventories
—
83,280
Prepaid expenses and other current
assets
9,137
14,931
Other assets
5,450
7,831
Total assets
$
250,713
$
517,454
Liabilities and Stockholders’
Equity
Accounts payable and accrued expenses
$
51,943
$
79,785
Other liabilities
2,567
4,237
Total liabilities
54,510
84,022
Stockholders’ equity
196,203
433,432
Total liabilities and stockholders'
equity
$
250,713
$
517,454
AMYLYX PHARMACEUTICALS,
INC.
CONDENSED CONSOLIDATED
STATEMENTS OF OPERATIONS
UNAUDITED
(in thousands, except share
and per share data)
Three Months Ended September
30,
Nine Months Ended September
30,
2024
2023
2024
2023
Product revenue, net
$
416
$
102,693
$
88,036
$
272,337
Operating expenses:
Cost of sales
—
5,218
5,953
16,081
Cost of sales - inventory impairment and
loss on firm purchase commitments
809
—
118,680
—
Acquired in-process research and
development
36,203
—
36,203
—
Research and development
21,237
30,037
81,192
83,273
Selling, general and administrative
17,828
48,718
97,234
136,115
Restructuring expenses
—
—
22,851
—
Total operating expenses
76,077
83,973
362,113
235,469
(Loss) income from operations
(75,661
)
18,720
(274,077
)
36,868
Other income, net
2,957
3,691
10,122
10,953
(Loss) income before income taxes
(72,704
)
22,411
(263,955
)
47,821
Provision for income taxes
—
1,518
242
3,281
Net (loss) income
$
(72,704
)
$
20,893
$
(264,197
)
$
44,540
Net (loss) income per share
Basic
$
(1.07
)
$
0.31
$
(3.89
)
$
0.66
Diluted
$
(1.07
)
$
0.30
$
(3.89
)
$
0.63
Weighted-average shares used in computing
net (loss) income per share
Basic
68,091,446
67,414,669
67,990,613
67,124,407
Diluted
68,091,446
69,748,547
67,990,613
70,143,659
View source
version on businesswire.com: https://www.businesswire.com/news/home/20241107293249/en/
Media Amylyx Media Team +1 (857) 799-7274
amylyxmediateam@amylyx.com
Investors Lindsey Allen Amylyx Pharmaceuticals, Inc. +1
(857) 320-6244 Investors@amylyx.com
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