– Positive TNG462 clinical activity across
multiple tumor types in the phase 1/2 clinical trial, program
moving into full development with multiple combination studies
–
– Clinical collaboration established with
Revolution Medicines to evaluate TNG462 in combination with RAS(ON)
multi- and G12D-selective inhibitors –
– Next-generation brain-penetrant
MTA-cooperative PRMT5 inhibitor, TNG456, planned to enter the
clinic in 1H 2025 –
– Strong cash position of $293 million as of
September 30, 2024, with cash runway into 3Q 2026 to prioritize
resourcing of TNG462 and TNG456 clinical trials –
Tango Therapeutics, Inc. (NASDAQ: TNGX), a clinical-stage
biotechnology company committed to discovering and delivering the
next generation of precision cancer medicines, reported its
financial results for the third quarter ended September 30, 2024,
and provided business highlights.
“We have made great progress with our PRMT5 development program,
including positive data from the TNG462 phase 1/2 clinical trial
that showcase the best-in-class potential of TNG462 in multiple
tumor types, including pancreatic and non-small cell lung cancers
(NSCLC). Based on these early data, we are advancing TNG462 into
trials with multiple targeted and standard of care combinations,
including two RAS(ON) tri-complex inhibitors from Revolution
Medicines. Given that nearly all MTAP-deleted pancreatic cancer has
a co-occurring RAS mutation, we believe this could be a powerful
approach to changing the treatment landscape for this challenging
cancer,” said Barbara Weber, M.D., President and Chief Executive
Officer of Tango Therapeutics. “As part of the expanded
capabilities needed to rapidly move TNG462 development forward, Dr.
Maeve Waldron-Lynch, M.D. is joining Tango as Senior Vice
President, Head of Clinical Development. Dr. Waldron-Lynch has
extensive late-stage oncology clinical development and regulatory
experience and will be invaluable as we prepare to advance TNG462
to registration.”
In a separate press release issued earlier today, Tango
Therapeutics provided an update on its ongoing PRMT5 clinical
development program:
- Data from the ongoing phase 1/2 clinical trial of TNG462, a
potentially best-in-class MTA-cooperative PRMT5 inhibitor,
demonstrate clinical activity across multiple tumor types,
including NSCLC and pancreatic cancer. Of note, this includes an
ORR of 43% in cholangiocarcinoma (n=7). Substantive durability and
a good safety and tolerability profile also were observed in this
ongoing trial. The next clinical update is expected in 2025.
- The Company plans to initiate multiple targeted and standard of
care combinations with TNG462 including RAS(ON) multi-selective and
RAS(ON) G12D-selective inhibitors (Revolution Medicines),
osimertinib (AstraZeneca) and pembrolizumab (Merck). These studies
are expected to begin enrolling in 1H 2025.
- TNG908, an MTA-cooperative brain-penetrant PRMT5 inhibitor, is
clinically active and well-tolerated across non-CNS cancers in the
phase 1/2 clinical trial. In particular, there were a total of nine
evaluable pancreatic cancer patients, two with partial responses
(ORR 22%) and five with stable disease as best response to date.
The five ongoing pancreatic cancer patients have been on study for
an average of 24 weeks, the longest for 72 weeks.
- TNG908 did not demonstrate activity in glioblastoma (n=23 at
active doses) likely because CNS exposure did not meet the required
exposure threshold for clinical efficacy.
- TNG908 enrollment is being stopped to allow full resourcing of
TNG462 as a potential best-in-class molecule. In particular, the
notably longer time on treatment observed – 24 weeks and still
increasing for TNG462 versus 16 weeks for TNG908 – the superior
target coverage, and the safety and tolerability profile all
support selection of TNG462 for further development.
- TNG456 is a next-generation brain-penetrant MTA-cooperative
PRMT5 inhibitor that is 55X selective for MTAP deletion with 20 nM
potency. Preclinical studies suggest TNG456 central nervous system
exposure has the potential to be sufficient for meaningful efficacy
in glioblastoma and brain metastases.
- The Company expects to begin enrolling patients in the planned
phase 1/2 trial during 1H 2025.
Business Highlights
Clinical collaboration with Revolution Medicines
- In November 2024, the Company entered into a clinical
collaboration with Revolution Medicines to evaluate the efficacy
and safety of TNG462 in combination with RMC-6236, a RAS(ON)
multi-selective inhibitor, and with RMC-9805, a RAS(ON)
G12D-selective inhibitor.
- The agreement provides that Revolution Medicines will supply
RMC-6236 and RMC-9805 to Tango and that Tango will be the sponsor
of any combination trials. Each company will retain commercial
rights to their respective compounds and the agreement is mutually
non-exclusive.
TNG260, a first-in-class, highly selective CoREST complex
inhibitor
- The TNG260 phase 1/2 clinical trial is ongoing, evaluating
safety, pharmacokinetics, pharmacodynamics and efficacy of TNG260
in combination with pembrolizumab in patients with locally advanced
or metastatic solid tumors with an STK11 loss-of-function mutation.
To date, safety, tolerability and pharmacokinetic profiles are
favorable.
- STK11 mutations occur in approximately 15% of non-small cell
lung, 15% of cervical, 10% of carcinoma of unknown primary, 5% of
breast and 3% of pancreatic cancers.
Upcoming Milestones
- TNG462 clinical data update expected in 2025
- TNG462 combination trial enrollment expected to begin 1H
2025
- TNG456 phase 1/2 trial enrollment expected to begin 1H
2025
- TNG260 clinical data expected in 2025
Additional Business and Pipeline Highlights
Leadership Update
Maeve Waldron-Lynch, M.D. will join Tango as Senior Vice
President, Head of Clinical Development later this month. In this
role, Dr. Waldron-Lynch will lead clinical development functions
under Adam Crystal, M.D., Ph.D., President of Research and
Development at Tango. Dr. Waldron-Lynch most recently served as VP
and Global Clinical Program Head at MorphoSys, where she oversaw
the clinical program for tafasitamab. Prior to MorphoSys, she was a
Clinical Development Medical Director at Novartis. Dr.
Waldron-Lynch also has served as Senior Clinical Director, Oncology
at Roche, and as Associate Director of Medical Science, Oncology at
Mundipharma. Dr. Waldron-Lynch graduated from the University
College Cork School of Medicine and served as a Specialty Registrar
Medical Oncology at the Royal College of Physicians of Ireland, and
a Clinical Fellow in Medical Oncology at the Yale University School
of Medicine.
Financial Results
As of September 30, 2024, the Company held $293.3 million in
cash, cash equivalents and marketable securities, which the Company
expects to be sufficient to fund operations into the third quarter
of 2026, including for additional planned TNG462 and TNG456
clinical trials.
Collaboration revenue was $11.6 million for the three months
ended September 30, 2024, compared to $10.7 million for the same
period in 2023, and $25.9 million for the nine months ended
September 30, 2024 compared to $26.1 million for the same period in
2023. Collaboration revenue increased due to changes to estimated
costs expected to be incurred under the collaboration during the
three months ended September 30, 2024.
License revenue was $0 and $12.1 million for the three and nine
months ended September 30, 2024, respectively, compared to $0 and
$5.0 million for the three and nine months ended September 30,
2023, respectively. The year-to-date increase is primarily due to
licensing a drug discovery program to Gilead for $12.0 million
during the second quarter of 2024 as compared to Gilead licensing a
program for $5.0 million during the second quarter of 2023.
Research and development expenses were $33.3 million for the
three months ended September 30, 2024, compared to $27.1 million
for the same period in 2023, and $110.0 million for the nine months
ended September 30, 2024 compared to $83.9 million for the same
period in 2023. The change is due to increased spend related to the
advancement of TNG462, preclinical programs and personnel-related
costs to support our research and development activities.
General and administrative expenses were $11.2 million for the
three months ended September 30, 2024, compared to $9.2 million for
the same period in 2023, and $32.7 million for the nine months
ended September 30, 2024 compared to $26.4 million for the same
period in 2023. The change was primarily due to increases in
personnel-related costs.
Net loss for the three months ended September 30, 2024 was $29.2
million, or $0.27 per share, compared to a net loss of $22.3
million, or $0.23 per share, in the same period in 2023. Net loss
for the nine months ended September 30, 2024 was $92.6 million, or
$0.85 per share, compared to a net loss of $71.0 million, or $0.78
per share, in the same period in 2023.
About Tango Therapeutics
Tango Therapeutics is a clinical-stage biotechnology company
dedicated to discovering novel drug targets and delivering the next
generation of precision medicine for the treatment of cancer. Using
an approach that starts and ends with patients, Tango leverages the
genetic principle of synthetic lethality to discover and develop
therapies that take aim at critical targets in cancer. For more
information, please visit www.tangotx.com.
Forward-Looking Statements
Certain statements in this press release may be considered
forward-looking statements. Forward-looking statements generally
relate to future events, Tango’s future operating performance and
goals, the anticipated benefits of therapies and combination
therapies (that include a Tango pipeline product), as well as the
expectations, beliefs and development objectives for Tango’s
product pipeline and clinical trials. In some cases, you can
identify forward-looking statements by terminology such as “may”,
“should”, “expect”, “intend”, “will”, “goal”, “estimate”,
“anticipate”, “believe”, “predict”, “designed,” “potential” or
“continue”, or the negatives of these terms or variations of them
or similar terminology. For example, implicit or explicit
statements concerning the following include or constitute
forward-looking statements: the Company is advancing TNG462 into
clinical trials as a monotherapy and with multiple targeted and
standard of care combinations, including two RAS(ON) tri-complex
inhibitors from Revolution Medicines, Inc.; the Company believes
the combination of TNG462 with RAS(ON) inhibitors could be a
powerful approach to changing the treatment landscape for
pancreatic cancer; potential combination strategies for PRMT5
inhibitors; the Company’s view that TNG462 has the potential to be
a best-in-class MTA-cooperative PRMT5 inhibitor in multiple tumor
types, including pancreatic and non-small cell lung cancers; the
Company is moving TNG462 into full development; the Company expects
cash runway into the third quarter of 2026; the Company expects to
share another clinical update on TNG462 in 2025; the Company’s
planned and ongoing clinical trials, including the anticipated
timing for enrollment and the timing to report results and updates
of such trials; the Company’s understanding of the central nervous
system exposure required to provide meaningful efficacy in
glioblastoma and brain metastases; the Company’s plans to enroll
patients in a planned Phase 1/2 clinical trial for TNG456 in the
first half of 2025; the Company continues to advance TNG260 for
cancers with STK11 loss-of-function mutations, with the phase 1/2
clinical trial ongoing; Tango is committed to discovering and
delivering the next generation of precision cancer medicines; Dr.
Weber’s statements in this press release; and the expected timing
of: (i) development candidate declaration for certain targets; (ii)
initiating IND-enabling studies; (iii) filing INDs; (iv) clinical
trial initiation, dose escalation and dose expansion (including for
combination studies) and (v) disclosing initial, interim,
additional and final clinical trial results (including for
combination studies); and the expected benefits of the Company's
development candidates and other product candidates. Such
forward-looking statements are subject to risks, uncertainties, and
other factors which could cause actual results to differ materially
from those expressed or implied by such forward-looking statements.
These forward-looking statements are based upon estimates and
assumptions that, while considered reasonable by Tango and its
management, are inherently uncertain. New risks and uncertainties
may emerge from time to time, and it is not possible to predict all
risks and uncertainties. Factors that may cause actual results to
differ materially from current expectations include, but are not
limited to: the benefits of product candidates seen in preclinical
tests and analyses may not be evident when tested in later
preclinical studies or in clinical trials or when used in broader
patient populations (if approved for commercial sale); Tango has
limited experience conducting clinical trials (and will rely on a
third party to operate its clinical trials) and may not be able to
commence its clinical trials (including opening clinical trial
sites, dosing the first patient, and continued enrollment and
dosing of an adequate number of clinical trial participants) when
expected, may not be able to continue dosing, initiate dose
escalation and/or dose expansion on anticipated timelines, and may
not generate or report clinical trial results (including final,
initial or additional safety, efficacy data and proof-of-mechanism
and proof-of-concept) in the anticipated timeframe (or at all);
future clinical trial data releases may differ materially from
initial or interim data from our current and future clinical
trials; Tango’s pipeline products may not be safe and/or effective
in humans; Tango has a limited operating history and has not
generated any revenue to date from product sales, and may never
become profitable; other companies may be able to identify and
develop product candidates more quickly than the Company and
commercially introduce the product prior to the Company; the
Company’s proprietary discovery platform is novel and may not
identify any synthetic lethal targets for future development; the
Company may not be able to identify development candidates on the
schedule it anticipates due to technical, financial or other
reasons; the Company may not be able to file INDs for development
candidates on time, or at all, due to technical or financial
reasons or otherwise; the Company may utilize cash resources more
quickly than anticipated; Tango will need to raise capital in the
future and if we are unable to raise capital when needed or on
attractive terms, we would be forced to delay, scale back or
discontinue some of our development programs or future
commercialization efforts (which may delay filing of INDs, dosing
patients, initiation of dose expansion, reporting clinical trial
results and filing new drug applications); Tango’s approach to the
discovery and development of product candidates is novel and
unproven, which makes it difficult to predict the time, cost of
development, and likelihood of successfully developing any
products; the Company may be unable to advance our preclinical
development programs into and through the clinic for safety or
efficacy reasons or commercialize our product candidates or we may
experience significant delays in doing so as a result of factors
beyond Tango’s control; the Company may not be able to realize the
benefits of orphan drug or Fast Track designation (and such
designations may not advance any anticipated approval timelines);
the expected benefits of our product candidates in patients as
single agents and/or in combination may not be realized; the
Company may experience delays or difficulties in the initiation,
enrollment, or dosing of patients in clinical trials or the
announcement of clinical trial results, Tango may not identify or
discover additional product candidates or may expend limited
resources to pursue a particular product candidate or indication
and fail to capitalize on product candidates or indications that
may be more profitable or for which there is a greater likelihood
of success; the Company’s product candidates may cause adverse or
other undesirable side effects (or may not show requisite efficacy)
that could, among other things, delay or prevent regulatory
approval; our dependence on one or a limited number third parties
for conducting clinical trials and producing drug substance and
drug product (including drug substance, which is currently sole
sourced); government regulation may negatively impact the Company’s
business, including the potential approval of the BIOSECURE Act;
and our ability to obtain and maintain patent and other
intellectual property protection for our technology and product
candidates or the scope of intellectual property protection
obtained is not sufficiently broad. Additional information
concerning risks, uncertainties and assumptions can be found in
Tango’s filings with the Securities and Exchange Commission (SEC),
including the risk factors referenced in Tango’s Annual Report on
Form 10-K for the fiscal year ended December 31, 2023, as
supplemented and/or modified by its most recent Quarterly Report on
Form 10-Q. 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. Tango specifically disclaims any
duty to update these forward-looking statements.
Consolidated Statements of
Operations
(In thousands, except share
and per share data)
Three Months Ended September
30,
Nine Months Ended September
30,
2024
2023
2024
2023
Collaboration revenue
$
11,607
$
10,732
$
25,852
$
26,096
License revenue
—
—
12,100
5,000
Total revenue
11,607
10,732
37,952
31,096
Operating expenses:
Research and development
33,263
27,149
109,981
83,859
General and administrative
11,222
9,209
32,656
26,397
Total operating expenses
44,485
36,358
142,637
110,256
Loss from operations
(32,878
)
(25,626
)
(104,685
)
(79,160
)
Other income, net
3,765
3,386
12,212
8,266
Loss before income taxes
(29,113
)
(22,240
)
(92,473
)
(70,894
)
Provision for income taxes
(54
)
(23
)
(159
)
(87
)
Net loss
$
(29,167
)
$
(22,263
)
$
(92,632
)
$
(70,981
)
Net loss per common share – basic and
diluted
$
(0.27
)
$
(0.23
)
$
(0.85
)
$
(0.78
)
Weighted average number of common shares
outstanding – basic and diluted
108,507,390
97,033,273
108,990,011
91,268,133
Consolidated Balance
Sheets
(In thousands)
September 30, 2024
December 31, 2023
Assets
Current assets:
Cash and cash equivalents
$
53,148
$
66,385
Marketable securities
240,130
270,500
Restricted cash
—
856
Prepaid expenses and other current
assets
7,537
8,797
Total current assets
300,815
346,538
Property and equipment, net
8,590
9,908
Operating lease right-of-use assets
40,430
43,508
Restricted cash, net of current
portion
2,567
2,567
Other assets
13
46
Total assets
$
352,415
$
402,567
Liabilities and Stockholders'
Equity
Current liabilities:
Accounts payable
$
4,112
$
2,785
Accrued expenses and other current
liabilities
15,006
15,401
Operating lease liabilities
2,863
2,082
Deferred revenue
15,602
25,670
Total current liabilities
37,583
45,938
Operating lease liabilities, net of
current portion
34,763
36,838
Deferred revenue, net of current
portion
50,899
66,683
Total liabilities
123,245
149,459
Total stockholders’ equity
229,170
253,108
Total liabilities and stockholders’
equity
$
352,415
$
402,567
View source
version on businesswire.com: https://www.businesswire.com/news/home/20241106308250/en/
Investor: Sam Martin/Andrew Vulis Argot Partners
tango@argotpartners.com
Media: Amanda Brown Galgay SVP, Corporate Communications,
Tango Therapeutics media@tangotx.com
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