Epetraborole-treated patients demonstrated
clinical improvements in QOL-B and a post-hoc analysis of MACrO2
with nominal statistical significance when evaluated as continuous
measures
First drug candidate with statistically
favorable patient reported outcome (PRO)-based improvement in
treatment-refractory Mycobacterium avium Complex (TR-MAC)
population
Company plans to meet with FDA to gain
alignment on a development path for epetraborole, including
potentially reinitiating a Phase 3 clinical study, while advancing
its boron chemistry pipeline
Achieved 50% reduction in expenditures through
strategic realignment of operations
Cash, cash equivalents, and investments of
$93.4 million at September 30, 2024 anticipated to fund operations
through 2027 under current operating plan
AN2 Therapeutics, Inc. (Nasdaq: ANTX), a biopharmaceutical
company focused on discovering and developing novel small molecule
therapeutics derived from its boron chemistry platform, today
reported financial results for the quarter ended September 30, 2024
and provided an update from its ongoing analysis of data from the
Phase 2 portion of the EBO-301 trial.
“Treatment options for patients with refractory MAC lung disease
are extremely limited. Many of these patients are significantly
more challenging to convert microbiologically due to the microbial
complexity of their infections as well as their very complex lung
anatomy, and often experience severe clinical symptoms at this
advanced stage of disease. The fact that epetraborole appears to
have demonstrated improvements based on two patient reported
outcome measures is highly encouraging,” said Stephen J. Ruoss,
M.D., Professor of Medicine, Pulmonary and Critical Care Medicine
at Stanford University School of Medicine. “By potentially
improving both their quality of life and clinical outcomes,
epetraborole represents a potentially significant advancement in
treatment possibilities.”
"We are encouraged by this recent data analysis, which indicate
that epetraborole may provide clinical improvement in patients with
treatment-refractory MAC lung disease, as measured by two
patient-reported outcome instruments, including the same instrument
recently selected for the primary endpoint in the Arikayce TN-MAC
pivotal trial," stated Eric Easom, Co-Founder, Chairman, President,
and Chief Executive Officer of AN2 Therapeutics. "We look forward
to engaging with the FDA in the near-term to discuss next steps for
the epetraborole program, including the potential reinitiation of a
pivotal Phase 3 trial for treatment-refractory MAC lung
disease.”
Easom continued, “With a strong cash runway and optimized
operating plan, we continue to advance our diverse pipeline of
boron-based compounds to address unmet patient needs. This includes
the recent strategic expansion into oncology, underscoring our
dedication to innovating and improving patient outcomes across
multiple therapeutic areas."
Third Quarter & Recent Updates:
Ongoing Analysis from Epetraborole Phase 2/3 Clinical Study
in TR-MAC Lung Disease
The Company has provided an update from its ongoing analysis of
the Phase 2 portion of the EBO-301 Phase 2/3 study. Two PROs
evaluated in the trial indicated statistically significant clinical
response, the QOL-B Respiratory Domain (Table 1) and MACrO2
(post-hoc analysis, Table 2), using continuous response measures
instead of the binary responder methodology previously reported.
Patients treated with epetraborole indicated clinical response
using the same PRO instrument (QOL-B respiratory domain) and
analysis method (least squares mean change from Baseline to Month
6) that was recently reported as the primary endpoint in the
Arikayce ENCORE trial, after alignment with FDA. These EBO-301 PRO
findings appear to align with FDA’s current recommendation for
PRO-based primary endpoints in NTM-MAC trials.
Table 1: Quality of Life – Bronchiectasis (QOL-B respiratory
domain) (least squares mean change from Baseline to Month 6)*
EBO-301 prespecified secondary endpoint
Epetraborole + OBR (n=34)
Placebo + OBR (n=35)
LS Mean Difference
p-value
Change from Baseline to Month 6
7.20
0.30
6.90
0.0365
*Measures of patient improvement
for QOL-B are shown by positive changes in the score measured from
baseline.
- Epetraborole treated patients showed nominally statistically
significant improvements in the QOL-B respiratory domain measured
from baseline to month 6.
- The p-value is termed “nominal” because this was not the
prespecified primary endpoint in the Phase 2 part of the
trial.
Table 2: MACrO2 PRO (least squares mean)* Post-hoc
analysis
Epetraborole + OBR (n=34)
Placebo + OBR (n=35)
LS Mean Difference
p-value
Change from Baseline to Month 6
-12.91
-7.10
-5.81
0.0433
*Measures of patient improvement for
MACrO2 are shown by negative changes in the score measured from
baseline. The least squares mean calculation for MACrO2 utilized
the same approach as the prespecified QOL-B LSM in the EBO-301
statistical analysis plan.
- Epetraborole treated patients showed nominally statistically
significant improvements in MACrO2 measured from baseline to month
6 in post-hoc analysis.
There was a high rate of MAC resistance to background
antimycobacterial therapies at baseline, including approximately
one-third of the patients with macrolide resistance and 60% with
amikacin resistance, indicators of the complexity of the patient
population. Notably, there was no evidence of induced epetraborole
resistance in isolates from patients treated with epetraborole.
Further analysis showed no change in the previously reported
safety profile; epetraborole was generally well-tolerated, with 2
(5%) discontinuations due to TEAEs in the epetraborole arm.
Epetraborole: Next Steps
The Company believes these findings are particularly noteworthy
given the severe refractory status of the patients studied, and
that improvements in QOL-B and MACrO2 appear to align with FDA’s
current guidance for the primary efficacy endpoint in NTM-MAC
studies. The Company will seek an End-of-Phase 2 meeting with FDA
in the first half of 2025, with the goal of leveraging insights
from the Phase 2 results to evaluate potential reinitiation of a
pivotal Phase 3 TR-MAC study. In addition, the Company also plans
to seek alignment with the FDA on a statistical analysis plan for
the 97 patients who completed six months of treatment in the Phase
3 portion of EBO-301 at the time the Company halted the trial in
August 2024. The Company anticipates releasing top-line Phase 3
data from these patients in mid-2025, subject to the timing of
discussions with the FDA.
Other AN2 Boron Chemistry Pipeline Programs
Chagas Disease
During the quarter, the Company advanced preclinical activities
aimed to initiate clinical studies in chronic Chagas disease, a
disease that affects an estimated 6-7 million people worldwide,
including approximately 300,000 in the U.S., and causes severe
cardiac disease and death. The Company plans to initiate Phase 1
clinical development with AN2-502998 in mid-2025.
Melioidosis
The Company completed enrollment in a 200-patient observational
trial for epetraborole in acute melioidosis in October 2024 and
these data will inform a Phase 2 proof of concept study that is
planned to initiate enrollment in the second half of 2025.
Melioidosis is a deadly bacterial infection and global bioterrorism
threat with a 90-day mortality rate of approximately 50% using
standard of care (SOC) drugs ceftazidime or meropenem. The aim of
the program is to meaningfully lower the expected mortality rate by
dosing epetraborole on top of SOC.
Boron Chemistry Pipeline
Additional development programs are underway and focused on
targets in infectious diseases and oncology with high unmet needs.
The Company anticipates delivering up to three development
compounds in 2025.
Global Health
In October, the Company announced that it received a second-year
continuation of a research grant from the Bill & Melinda Gates
Foundation to discover novel boron containing small molecules for
the treatment of tuberculosis and malaria. The Company will
continue its efforts to tackle global health disease through
non-dilutive funding.
Selected Third Quarter Financial Results
- Research and Development (R&D) Expenses: R&D
expenses for the third quarter of 2024 were $8.3 million compared
to $14.4 million for the same period during 2023 due to decreased
clinical trial costs, personnel-related expenses, preclinical and
research study expenses, consulting and outside services, and other
costs, partially offset by an increase in chemistry manufacturing
and controls activity.
- General and Administrative (G&A) Expenses: G&A
expenses for the third quarter of 2024 were $3.5 million compared
to $3.8 million for the same period during 2023 due to a decrease
in professional services.
- Restructuring Charges: Restructuring charges for the
third quarter of 2024 were $2.2 million due to severance payments
and other employee termination-related expenses, partially offset
by a reduction in stock-based compensation expense as a result of
applying modification accounting for consulting agreements entered
into with certain terminated employees.
- Other Income, Net: Other income, net for the third
quarter of 2024 was $1.3 million compared to $1.5 million for the
same period during 2023 due to lower cash, cash equivalents and
investment balances.
- Net loss: Net loss for the third quarter of 2024 was
$12.7 million, compared to $16.7 million for the same period during
2023.
- Cash Position: The Company had cash, cash equivalents,
and investments of $93.4 million at September 30, 2024. Company
restructuring initiatives resulted in a 50% reduction in
expenditures, extending AN2’s expected cash runway through
2027.
About AN2 Therapeutics, Inc.
AN2 Therapeutics, Inc. is a biopharmaceutical company focused on
discovering and developing novel small molecule therapeutics
derived from its boron chemistry platform. AN2 has a pipeline of
boron-based compounds in development for Chagas disease, NTM, and
melioidosis, along with early-stage programs focused on targets in
infectious diseases and oncology. For more information, please
visit our website at www.an2therapeutics.com.
Forward-Looking Statements
This press release contains forward-looking statements within
the meaning of the Private Securities Litigation Reform Act of
1995. Forward-looking statements expressed or implied in this press
release include, but are not limited to, statements regarding: the
potential of the Company’s boron chemistry platform and early-stage
pipeline programs; design, initiation and timing of the Company’s
clinical trials and results; anticipated inflection points and
related timing; cash runway and cost savings related to
restructuring; analysis and expectations regarding data analysis
from the Phase 2/3 trial in treatment-refractory MAC lung disease,
including the potential to re-initiate Phase 3 development;
regulatory meetings and pathway and alignment with FDA guidance;
future development of epetraborole for other forms of NTM;
development of AN2-502998 for Chagas disease; development of
epetraborole for melioidosis; development of compounds for
infectious diseases and oncology targets; global health initiatives
and non-dilutive funding; and other statements that are not
historical fact. These statements are based on AN2’s current
estimates, expectations, plans, objectives and intentions, are not
guarantees of future performance and inherently involve significant
risks and uncertainties. Actual results and the timing of events
could differ materially from those anticipated in such
forward-looking statements as a result of these risks and
uncertainties, which include, but are not limited to, risks and
uncertainties related to: future trials of epetraborole in NTM-MAC
and the ability to show clinical efficacy consistent with PRO-based
data observed in prospective and post-hoc analyses to date;
potential disruptions related to AN2’s ability to implement its
plans for its internal boron chemistry platform and early-stage
pipeline programs; timely enrollment of patients in AN2’s existing
and future clinical trials; AN2’s ability to procure sufficient
supply of its product candidates for its existing and future
clinical trials; the potential for results from clinical trials to
differ from preclinical, early clinical, preliminary or expected
results; significant adverse events, toxicities or other
undesirable side effects associated with AN2’s product candidates;
the significant uncertainty associated with AN2’s product
candidates ever receiving any regulatory approvals; continued
funding by the National Institute of Allergy and Infectious Disease
(NIAID) of AN2’s development program for melioidosis; AN2’s ability
to obtain, maintain or protect intellectual property rights related
to its current and future product candidates; implementation of
AN2’s strategic plans for its business and product candidates; the
sufficiency of AN2’s capital resources and need for additional
capital to achieve its goals; global macroeconomic conditions and
global conflicts and other risks, including those described under
the heading “Risk Factors” in AN2’s Annual Reports on Form 10-K and
Quarterly Reports on Form 10-Q, and AN2’s other reports filed with
the U.S. Securities and Exchange Commission (SEC). These filings,
when made, are available on the investor relations section of AN2’s
website at www.an2therapeutics.com and on the SEC’s website at
www.sec.gov. Forward-looking statements contained in this press
release are made as of this date, and AN2 undertakes no duty to
update such information except as required under applicable
law.
AN2 THERAPEUTICS, INC.
CONDENSED STATEMENTS OF
OPERATIONS AND COMPREHENSIVE LOSS
(in thousands, except share
and per share data)
(unaudited)
Three Months Ended September
30,
Nine Months Ended September
30,
2024
2023
2024
2023
Operating expenses:
Research and development
$
8,287
$
14,429
$
35,091
$
39,952
General and administrative
3,484
3,751
10,856
10,868
Restructuring charge
2,243
—
2,243
—
Total operating expenses
14,014
18,180
48,190
50,820
Loss from operations
(14,014
)
(18,180
)
(48,190
)
(50,820
)
Other income, net
1,267
1,473
4,391
2,986
Net loss attributable to common
stockholders
$
(12,747
)
$
(16,707
)
$
(43,799
)
$
(47,834
)
Net loss per share attributable to common
stockholders, basic and diluted
$
(0.43
)
$
(0.65
)
$
(1.47
)
$
(2.22
)
Weighted-average number of shares used in
computing net loss per share, basic and diluted
29,841,169
25,645,421
29,809,839
21,532,537
Other comprehensive loss:
Unrealized (loss) gain on investments
139
(3
)
(163
)
252
Comprehensive loss
$
(12,608
)
$
(16,710
)
$
(43,962
)
$
(47,582
)
AN2 THERAPEUTICS, INC.
CONDENSED BALANCE
SHEETS
(in thousands)
September 30, 2024
(unaudited)
December 31, 2023
Assets
Current assets:
Cash and cash equivalents
$
33,504
$
15,647
Short-term investments
59,922
91,648
Prepaid expenses and other current
assets
4,263
3,212
Long-term investments
—
27,194
Other assets, long-term
—
1,043
Total assets
$
97,689
$
138,744
Liabilities and stockholders’
equity
Current liabilities:
Accounts payable
$
1,711
$
2,676
Other current liabilities
8,306
11,367
Total liabilities
10,017
14,043
Stockholders’ equity
87,672
124,701
Total liabilities and stockholders’
equity
$
97,689
$
138,744
View source
version on businesswire.com: https://www.businesswire.com/news/home/20241113258923/en/
Company Contacts: Lucy O. Day Chief Financial Officer
l.day@an2therapeutics.com
Anne Bowdidge Investor Relations
abowdidge@an2therapeutics.com
AN2 Therapeutics (NASDAQ:ANTX)
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