- Enrollment in darovasertib + crizotinib 1L HLA-A2+ MUM
potential Ph2/3 registration-enabling trial is ahead of schedule
and has exceeded 150 patients
- Successful FDA Type C meeting and targeting initiation of Ph3
registration-enabling trial for darovasertib in neoadjuvant UM in
H1 2025; Phase 2 neoadjuvant update with ~49% with >30% ocular
tumor shrinkage & ~61% eyes preserved, and over 75 patients
enrolled
- ENA 2024: Late-breaker oral presentation of IDE397 in
MTAP-deletion UC and NSCLC with confirmed ORR by RECIST 1.1 of 40%,
38%, and 22%, in UC, SqNSCLC, and AdenoNSCLC, respectively;
co-published IDE397 + AMG 193 preclinical combo data in
MTAP-deletion
- IDE397 + AMG 193 combination study ongoing in MTAP-deletion
solid tumors, and targeting expansion in MTAP-deletion NSCLC in
late 2024 to early 2025
- Targeting expansion of Phase 1/2 study of IDE397 in combination
with Trodelvy® in MTAP-deletion UC in Q4 2024, and PR reported at
ENA 2024 has confirmed by RECIST 1.1
- Targeting Phase 1/2 expansion for IDE161 and FPI in combination
with Merck's anti-PD-1 therapy KEYTRUDA® (pembrolizumab) in
MSI-High and MSS EC in Q4 2024
- IDE705 (GSK 101) Pol Theta Helicase Phase 1 dose escalation
ongoing in HRD solid tumors
- Received IND clearance for IDE275 (GSK959) Werner Helicase
development candidate ($7.0 million
milestone) for Phase 1 trial in MSI-High solid tumors
- Targeting Development Candidate nomination for MTAP-deletion,
KAT6 pathway and B7H3/PTK7 Topo-Payload Bispecific-ADC programs in
Q4 2024
- Targeting Investor R&D Day on Monday, December 16, to highlight IDEAYA's
preclinical and clinical pipeline with leading KOL(s) and Pharma
partner(s)
- $1.2 billion of cash, cash
equivalents and marketable securities as of September 30, 2024, anticipated to fund
operations into at least 2028; Completed an oversubscribed
~$302.4 million follow-on financing
in July 2024
SOUTH
SAN FRANCISCO, Calif., Nov. 4, 2024
/PRNewswire/ -- IDEAYA Biosciences, Inc. (Nasdaq: IDYA), a
precision medicine oncology company committed to the discovery and
development of targeted therapeutics, provided a business update,
and announced financial results for the third quarter ended
September 30, 2024.
"This was a transformational quarter for IDEAYA, including
completion of an oversubscribed ~$302.4
million follow-on financing, a late breaker oral
presentation at ENA 2024 for IDE397 in heavily pre-treated
MTAP-deletion urothelial and lung cancer patients, and a successful
Type C meeting with the FDA to enable a potential
registration-enabling trial for darovasertib in neoadjuvant uveal
melanoma. Next, we received IND clearance for Werner Helicase
inhibitor IDE275 with our partner GSK, representing our fifth
potential first-in-class clinical program," said Yujiro S. Hata, Chief Executive Officer and
Founder, IDEAYA Biosciences. "We continue to execute on our
strategic vision to build a leading precision medicine oncology
pipeline, and are on track to nominate our 6th,
7th, and 8th development candidate by year-end,
including from our B7H3/PTK7 bi-specific topo-ADC, MTAP-deletion,
and KAT6 pathway programs. We look forward to highlighting IDEAYA's
potential first-in-class preclinical and clinical programs, and to
continue to establish our scientific leadership in precision
medicine oncology at our upcoming investor R&D day," said
Michael White, Ph.D., Chief
Scientific Officer, IDEAYA Biosciences.
"This past quarter, we made significant progress on the
darovasertib program, including being ahead of our enrollment
targets for the first-line MUM potential registration-enabling
trial, and a successful Type C meeting with the FDA to inform a
potentially registration-enabling trial in the neoadjuvant uveal
melanoma setting. Next, the clinical data update from ENA 2024,
provides further clinical proof-of-concept for IDE397 at the RP2D
in MTAP-deletion urothelial and lung cancer. We are excited
to advance our broader IDE397 rational combination strategy,
including target expansion with AMG 193 in MTAP-deletion NSCLC in
late 2024 to early 2025, and target expansion with Trodelvy®
(sacituzumab govitecan-hziy), Gilead's Trop-2 directed
antibody-drug conjugate, in MTAP-deletion urothelial cancer in the
fourth quarter. Lastly, we are targeting to select a monotherapy
expansion dose for IDE161, and achieve FPI in combination with
Keytruda in MSI-High and MSS endometrial cancer by year-end,"
added Darrin Beaupre, M.D., Ph.D., Chief Medical Officer,
IDEAYA Biosciences.
Summary of Q3 and Recent Key Developments
Research and Clinical Development
- Darovasertib in 1L MUM and Neoadjuvant Uveal Melanoma (UM)
- Enrollment in darovasertib + crizotinib 1L HLA-A2+ MUM
potential Ph2/3 registration-enabling trial is ahead of schedule
and has exceeded 150 patients
- Positive interim Phase 2 results of darovasertib (IDE196) from
the company-sponsored and investigator-sponsored trials (IST) were
highlighted during an Investor Webcast in September 2024, and over 75 patients have been
enrolled in company-sponsored trial.
- Following a successful Type C meeting with the U.S. Food and
Drug Administration (FDA), IDEAYA is finalizing the Phase 3
registrational trial protocol and is targeting to initiate its
potential registration-enabling trial in the first half of
2025.
- IDE397 in MTAP-Deletion Solid Tumors
- Phase 1 expansion results of IDE397 in 27 evaluable
MTAP-deletion urothelial cancer (UC) and non-small cell lung cancer
(NSCLC) patients were presented as a late-breaking oral
presentation at the 36th EORTC-NCI-AACR Symposium (ENA
2024) in Barcelona, Spain.
Additional preclinical data on the anti-tumor activity by
combinatorial inhibition of IDE397 and clinical stage PRMT5
inhibitors AMG 193 and BMS-986504 in MTAP-deleted tumors were
included in a poster presentation.
- Reported positive interim data from 18 evaluable MTAP-deletion
UC and NSCLC patients and selected the move-forward Phase 2
expansion dose (RP2D) in an Investor Webcast in July 2024.
- Enrollment is ongoing in the IDE397 and AMG 193 Phase 1
dose escalation, and targeting expansion in NSCLC in late 2024 to
early 2025.
- Ongoing Phase 1 trial evaluating IDE397 in combination with
Trodelvy in MTAP-deletion UC; targeting combination expansion in
the fourth quarter of 2024. The PR reported at ENA 2024 has
confirmed by RECIST 1.1.
- IDE161 in Tumors with Homologous Recombination Deficiency
- Targeting Phase 1/2 monotherapy expansion for IDE161 PARG
inhibitor in priority solid tumor type(s) in the fourth quarter of
2024.
- Targeting first-patient-in for the Phase 1 trial evaluating
IDE161, IDEAYA's first-in-class potential PARG inhibitor, in
combination with Merck's (known as MSD outside of the US and
Canada) anti-PD-1 therapy,
KEYTRUDA® (pembrolizumab), in MSI-High and MSS endometrial cancer
(EC) in the fourth quarter of 2024.
- Preclinical data on IDE161 and antibody drug conjugate (ADC)
combination rationale presented as a poster at ENA 2024.
- Received FDA IND clearance for IDE275 (GSK959), a potential
first-in-class and best-in-class Werner Helicase inhibitor, for a
Phase 1 trial in high microsatellite instability (MSI-High) tumors
and earned a $7.0 million milestone
from GSK.
- Targeting Development Candidate nomination
for MTAP-deletion, KAT6 pathway and B7H3/PTK7 Topo-Payload
Bispecific-ADC programs in the fourth quarter of 2024.
- IDEAYA is targeting to host a Virtual Investor R&D Day on
Monday, December 16, 2024, to
highlight IDEAYA's potential first-in-class preclinical and
clinical pipeline with management, leading Key Opinion Leader(s)
(KOLs), and Pharma partner(s).
Corporate Development
- Raised gross proceeds of approximately $302.4 million in July
2024 through public offering, generating net proceeds of
approximately $283.8 million.
- Appointed Douglas B. Snyder as Senior Vice President,
General Counsel. Mr. Snyder brings over 25 years of legal
experience with leading healthcare organizations, including GW
Pharmaceuticals, Actelion Pharmaceuticals, Eisai, GSK, and the U.S.
FDA.
Clinical Programs and Upcoming Milestones
Darovasertib (IDE196) Program in Tumors with GNAQ or GNA11
Mutations
Darovasertib is a potent and selective protein kinase C (PKC)
inhibitor being developed to broadly address primary and metastatic
UM. Darovasertib is currently being evaluated in four ongoing
clinical trials. The darovasertib and
crizotinib combination in MUM has FDA Fast Track
designation:
- IDE196-002 (NCT05987332) is a Phase 2/3 potentially
registration-enabling clinical trial of darovasertib + crizotinib
in first-line human leukocyte antigens (HLA)-A2*02:01 negative (-)
MUM. Over 150 patients enrolled as of October 31, 2024.
- IDE196-001 (NCT03947385) is a Phase 1/2 clinical trial of
darovasertib + crizotinib in which we are planning to enroll
additional HLA-A2*02:01 positive (+) patients.
- Phase 2 trials of darovasertib as neoadjuvant / adjuvant
therapy in primary UM:
-
- IDE196-009 (NCT05907954) is a company-sponsored Phase 2 trial
evaluating darovasertib as neoadjuvant treatment of UM prior to
primary interventional treatment of enucleation or radiation
therapy, and as adjuvant therapy following the primary treatment.
Over 75 patients enrolled as of October 31, 2024.
- NADOM (NCT05187884) is a Phase 2 neoadjuvant / adjuvant trial
of darovasertib in ocular melanoma. This is an IST led
by Anthony Joshua, MBBS, PhD, FRACP, Head Department of
Medical Oncology, Kinghorn Cancer Centre, St. Vincent's Hospital
in Sydney with additional participating sites
in Melbourne, Australia.
- Positive interim efficacy data from both the company-sponsored
and the IST trials were highlighted during an Investor webcast in
September 2024:
-
- 31 enucleation and 18 plaque brachytherapy evaluable UM
patients treated with darovasertib neoadjuvant therapy in Phase 2
company-sponsored and IST trials.
- ~59% (29 of 49) of patients with >20% ocular tumor shrinkage
by product of diameters.
- ~49% (24 of 49) of patients with >30% ocular tumor shrinkage
by product of diameters.
- ~61% (19 of 31) eye preservation rate observed.
- Evidence of predicted visual preservation observed by reducing
the amount of radiation associated with plaque brachytherapy.
- Manageable AE profile observed from Phase 2 company-sponsored
trial (n=38), including 11% grade 3 or higher AEs, and 5% serious
AE rate. The discontinuation rate observed was 3%. The most common
AEs observed included diarrhea, nausea, vomiting and fatigue.
- IDEAYA had a successful Type C meeting with the FDA to discuss
the clinical trial design for a registration-enabling Phase 3 trial
in neoadjuvant UM patients. The planned trial aims to enroll
approximately 400 patients in two cohorts: cohort 1 of plaque
brachytherapy eligible UM patients, and cohort 2 of enucleation
eligible UM patients. Cohort 1 will be randomized to darovasertib
followed by plaque brachytherapy versus plaque brachytherapy alone,
and cohort 2 will be randomized with or without darovasertib as
neoadjuvant therapy. The primary endpoint of the trial is planned
to be time to vision loss and eye preservation rate for cohort 1
and 2, respectively. The secondary endpoint for the trial is no
detriment to Event-Free-Survival (EFS). Discussions with the FDA
are ongoing regarding surrogate and composite endpoints to support
earlier approval scenarios. IDEAYA is currently finalizing the
trial protocol and is targeting to initiate the potential Phase 3
registration-enabling study in the first half of 2025.
IDE397 Program in Tumors with MTAP Deletion
IDE397 is a potent and selective small molecule inhibitor targeting
methionine adenosyltransferase 2 alpha (MAT2A) in patients having
solid tumors with methylthioadenosine phosphorylase (MTAP)
deletion. IDEAYA continues to evaluate IDE397 in two trials in
select monotherapy indications and in high conviction clinical
combinations:
- IDE397-001 (NCT04794699) is a Phase 1/2 treatment study with a
monotherapy expansion in MTAP-deletion UC and NSCLC. The estimated
U.S. MTAP-deletion annual incidence in UC and NSCLC is
approximately 48,000 patients.
- Encouraging clinical activity at the 30 mg once-a-day Phase 2
monotherapy expansion dose was observed in the Phase 1 clinical
trial evaluating IDE397 in heavily pre-treated MTAP-deletion UC and
NSCLC patients presented at ENA 2024 in October 2024. The patients evaluated had a median
of two to three prior lines-of-therapy, ranging from one to seven.
The reported Phase 1 clinical expansion data was based on 27
evaluable MTAP-deletion patients, including 10 UC, nine
adenocarcinoma (Adeno) NSCLC, and eight squamous (Sq) NSCLC
patients at the expansion dose of 30 mg once-a-day of IDE397 :
- ~33% Overall Response Rate (ORR). One complete response (CR)
and eight partial responses (PRs) by RECIST 1.1 evaluation out of
27 evaluable patients. Nine of nine responses have been confirmed
by RECIST 1.1, including four UC patients, of which one was a CR,
three squamous NSCLC patients, and two adenocarcinoma NSCLC
patients. Two patients confirmed after the data cutoff date. In the
earlier reported July 8, 2024, IDE397
webcast program update, five confirmed responses were reported out
of 18 evaluable MTAP-deletion UC and NSCLC patients by RECIST 1.1.
There were zero non-evaluable patients reported as of the data
analysis.
- Confirmed ORR% by RECIST 1.1 by Solid Tumor Type: MTAP-deletion
UC = 40% (4 of 10) confirmed ORR%; MTAP-deletion squamous NSCLC =
~38% (3 of 8) confirmed ORR%; MTAP-deletion adenocarcinoma NSCLC =
~22% (2 of 9) confirmed ORR%.
- Multiple confirmed partial responses by RECIST 1.1 harbor
genetic co-alterations, including MTAP-deletion and KRAS G12D
mutation in NSCLC, and MTAP-deletion and FGFR-TACC3 fusion in
UC.
- ~93% Disease Control Rate (DCR). One CR, eight PRs, and 16
stable disease (SD) by RECIST 1.1 evaluation out of 27 evaluable
patients.
- Preliminary durability assessment: 15 of 27 patients still on
treatment. Seven of nine RECIST 1.1 responses remain on
treatment. Median duration of treatment (DOT) has not been reached
and is greater than 6.2 months and median time to response (TTR) is
~2.7 months. The median duration of response and median progression
free survival data is still immature. Three UC patients on
treatment greater than 250 days, four squamous NSCLC patients on
treatment greater than 200 days, and three adenocarcinoma NSCLC
patients on treatment greater than 200 days
- ~81% circulating tumor DNA (ctDNA) Molecular Response Rate
(MRR). 17 of 21 patients with 50% or greater ctDNA reduction, and
~33% (7 of 21) with deep 90% or greater ctDNA reduction. All MRs
(17 of 17) were rapid occurring at the first ctDNA sample analysis.
There were several quality control failures of patient samples that
led to unavailability for MR analysis
- Favorable adverse event (AE) profile. Approximately 18% grade 3
or higher drug-related AEs and no drug-related serious adverse
events (SAEs) observed at the IDE397 30mg once-a-day expansion
dose. No drug-related AEs leading to discontinuations were
observed. We anticipate that the favorable AE profile and dosing
convenience of a 30 mg once-a-day tablet has the potential to
enable long-term dosing and combination development, including with
MTA-cooperative PRMT5 inhibitors and topoisomerase payload antibody
drug conjugates (ADCs)
- Over 35 global clinical trial sites activated in the U.S.,
Canada, Europe and Asia Pasic to enable rapid
enrollment.
- Targeting development of IDE397 registrational plan in
MTAP-deletion solid tumors in 2025.
- Phase 1/2 trial of IDE397 and AMG 193 in MTAP-Deletion
NSCLC (Amgen-sponsored study, NCT05975073)
- Preclinical poster presentation on the antitumor activity
by combinatorial inhibition of MAT2A and PRMT5 in MTAP-deleted
tumors presented at ENA 2024.
- Enrollment is ongoing in the IDE397 and AMG193 Phase 1 dose
escalation. Targeting expansion in NSCLC in late 2024 to early
2025.
- Phase 1 trial of IDE397 and Trodelvy in MTAP-deletion UC
(IDEAYA-sponsored, NCT04794699) evaluating the safety,
tolerability, pharmacokinetics, pharmacodynamics and efficacy is
ongoing.
- Reported the first preliminary clinical case study of the
IDE397 and Trodelvy combination in MTAP-deletion UC at ENA
2024, including a PR by RECIST 1.1 in a patient case report with a
genetic co-alteration of MTAP-deletion and a FGFR3-TACC3 fusion,
and rapid and deep first-evaluation molecular responses with ctDNA
reduction of greater than 95% observed. The PR reported at
ENA 2024 has now confirmed by RECIST 1.1.
- Targeting to initiate the IDE397 and Trodelvy Phase 1/2
combination expansion in MTAP-deletion UC in Q4 2024.
- Pursuant to the clinical study collaboration and supply
agreement, IDEAYA and Gilead retain the commercial rights to their
respective compounds, including with respect to use as a
monotherapy or combination agent. IDEAYA is the study sponsor and
Gilead will provide the supply of Trodelvy to IDEAYA.
- IDE397 monotherapy or in combination with Trodelvy has not been
approved by any regulatory agency and the efficacy and safety of
this combination has not been established.
IDE161 Program in Tumors with Homologous Recombination
Deficiency
IDE161 is a potential first-in-class inhibitor of poly(ADP-ribose)
glycohydrolase (PARG), a novel, mechanistically distinct target in
the same clinically validated biological pathway as
poly(ADP-ribose) polymerase (PARP). IDE161 received two FDA Fast
Track designations in platinum-resistant advanced or metastatic
ovarian cancer patients having tumors with BRCA1/2 mutations, and
in pretreated advanced or metastatic HR+, Her2-, BRACA1/2 mutant
breast cancer.
IDE161 is currently being evaluated in IDE161-001 (NCT05787587),
a Phase 1 trial of IDE161 monotherapy in solid tumors with
homologous recombination deficiency (HRD) and in the planned
combination with Merck's anti-PD-1 therapy, KEYTRUDA®
(pembrolizumab) in microsatellite instability high (MSI-High) and
microsatellite stable (MSS) endometrial cancer. Selection of an
initial Phase 1/2 IDE161 monotherapy expansion dose in priority
solid tumors type(s) is targeted in the fourth quarter of 2024.
Separately, a first-patient-in for IDE161 in combination with
KEYTRUDA is targeted in the fourth quarter of 2024. KEYTRUDA® is a
registered trademark of Merck Sharp & Dohme LLC, a subsidiary
of Merck & Co., Inc., Rahway, NJ, USA.
In addition, preclinical results on IDE161 and ADC combination
rationale were presented as a poster at ENA 2024.
GSK-Partnered Programs
IDE705 (GSK101) Program in Tumors with HRD
IDE705
(GSK101) is a potential first-in-class small molecule inhibitor of
Pol Theta Helicase being developed as a combination treatment with
niraparib for advanced solid tumors with HRD. The dose escalation
portion of the GSK-sponsored Phase 1/2 clinical trial to evaluate
GSK101 in combination with niraparib, the GSK small molecule
inhibitor of PARP, for patients having solid tumors with BRCA or
other HR mutations, or with HRD is currently ongoing.
Upon initiation of the Phase 1 dose expansion, IDEAYA will be
eligible to receive a $10.0 million milestone payment,
with the collaboration having potential further aggregate
later-stage development and regulatory milestones of up
to $465.0 million. GSK is responsible for all research and
development costs for the program. Upon commercialization,
IDEAYA will be eligible to receive up to $475 million of
commercial milestones, and tiered royalties on global net sales of
GSK101 – ranging from high single-digit to sub-teen double-digit
percentages, subject to certain customary reductions.
IDE275 (GSK959) Program in Tumors with MSI-High
IDE275
(GSK959) is a potential first-in-class Werner helicase inhibitor
that received FDA IND clearance for a Phase 1 trial in October 2024. The GSK-sponsored Phase 1
trial will evaluate IDE275 (GSK959) in patients having MSI-High
tumors, as a monotherapy and in combination with a PD-1
inhibitor.
IDEAYA earned a $7 million
milestone payment for the IND clearance and has the potential to
earn up to an additional $10.0 million upon initiation of
Phase 1 clinical dose expansion. In addition, IDEAYA is entitled to
receive up to $465.0 million in further later-stage
development and regulatory milestones. GSK is responsible for 80%
of global research and development costs and IDEAYA is responsible
for 20% of such costs. Upon commercialization, IDEAYA will be
eligible to receive up to $475 million of commercial
milestones, 50% of U.S. net profits and tiered royalties on global
non-U.S. net sales of the Werner Helicase inhibitor development
candidate (DC) – ranging from high single-digit to sub-teen
double-digit percentages, subject to certain customary
reductions.
B7H3/PTK7 Topo-Payload BsADC Program
IDEAYA entered into an option and license agreement for a potential
first-in-class B7H3/PTK7 Topo-Payload BsADC program with Biocytogen
in July 2024. The agreement grants IDEAYA an option for an
exclusive worldwide license from Biocytogen for a potential
first-in-class B7H3/PTK7 Topo-Payload BsADC program. B7H3/PTK7 has
been found to be co-expressed in multiple solid tumor types,
including double-digit percent prevalence in lung, colorectal, and
head and neck cancers, among others. Based on preclinical data, the
potential first-in-class B7H3/PTK7 Topo-Payload BsADC program has
the potential to be developed as a monotherapy agent and used in
combination with multiple programs in IDEAYA's pipeline targeting
DDR-based therapies, including the PARG inhibitor IDE161. A
development candidate nomination for the B7H3/PTK7 Topo-Payload
BsADC program is targeted in the fourth quarter of 2024.
Next-Generation Precision Medicine Pipeline Programs
Early preclinical research programs focused on pharmacological
inhibition of several new targets for patients with solid tumors
characterized by defined biomarkers based on genetic mutations
and/or molecular signatures are ongoing. These programs have the
potential for discovery and development of first-in-class or
best-in-class therapeutics with multiple wholly owned DC
nominations targeted in the fourth quarter of 2024, including in
MTAP-deletion solid tumors indications to enable a potential
wholly-owned clinical combination with IDE397, and separately a DC
nomination in the lysine acetyltransferase 6 (KAT6) pathway.
Financial Results
As of September 30, 2024, IDEAYA had cash, cash
equivalents and marketable securities totaling $1.2 billion. This compared to cash, cash
equivalents and marketable securities of $952.7 million as of June
30, 2024. The increase was primarily attributable to
$283.8 million in net proceeds from
the underwritten public offering of common stock and pre-funded
warrants to purchase common stock in July
2024, partially offset by net cash used in operations.
Research and development (R&D) expenses for the three months
ended September 30, 2024 totaled
$57.2 million compared to
$54.5 million for the three months
ended June 30, 2024. The increase was
primarily due to clinical trial and outside services expenses.
General and administrative (G&A) expenses for the three
months ended September 30, 2024
totaled $9.7 million compared to
$10.4 million for the three months
ended June 30, 2024. The decrease was
primarily due to stock-based compensation expense.
The net loss for the three months ended September 30, 2024 was $51.8 million compared to the net loss of
$52.8 million for the three months
ended June 30, 2024. Total stock
compensation expense for the three months ended September 30, 2024 was $9.2 million compared to $9.7 million for the three months ended
June 30, 2024.
About IDEAYA Biosciences
IDEAYA is a precision
medicine oncology company committed to the discovery and
development of targeted therapeutics for patient populations
selected using molecular diagnostics. IDEAYA's approach integrates
capabilities in identifying and validating translational biomarkers
with drug discovery to select patient populations most likely to
benefit from its targeted therapies. IDEAYA is applying its
research and drug discovery capabilities to synthetic lethality –
which represents an emerging class of precision medicine
targets.
IDEAYA's updated corporate presentation is available on its
website, at its Investor Relations
page: https://ir.ideayabio.com/.
Forward-Looking Statements
This press release contains
forward-looking statements, including, but not limited to,
statements related to (i) the timing, content and venue of
clinical program updates, (ii) the timing of expansion of Phase 1/2
trial of IDE397 in combination with Trodelvy® in MTAP-deletion UC,
(iii) the timing of expansion of Phase 1 trial of IDE397 in
combination with AMG 193 in NSCLC, (iv) the timing of finalization
of Phase 3 registration trial protocol and initiation of trial for
darovasertib, (v) the timing of a first-patient-in in the IDE161
and KEYTRUDA combination study, (vi) the timing of DC nominations
for MTAP-deletion, KAT6 pathway and B7H3/PTK7 Topo-Payload
Bispecific-ADC programs, (vii) the timing of designation of next
generation development candidates, (viii) the extent to
which IDEAYA's existing cash, cash equivalents, and marketable
securities will fund its planned operations, (ix) the estimate of
patient populations, (x) additional clinical combinations, and (xi)
the receipt of development and regulatory milestones. Such
forward-looking statements involve substantial risks and
uncertainties that could cause IDEAYA's preclinical and clinical
development programs, future results, performance or achievements
to differ significantly from those expressed or implied by the
forward-looking statements. Such risks and uncertainties include,
among others, the uncertainties inherent in the drug development
process, including IDEAYA's programs' early stage of development,
the process of designing and conducting preclinical and clinical
trials, the regulatory approval processes, the timing of regulatory
filings, the challenges associated with manufacturing drug
products, IDEAYA's ability to successfully establish, protect and
defend its intellectual property, and other matters that could
affect the sufficiency of existing cash to fund operations. IDEAYA
undertakes no obligation to update or revise any forward-looking
statements. For a further description of the risks and
uncertainties that could cause actual results to differ from those
expressed in these forward-looking statements, as well as risks
relating to the business of IDEAYA in general, see IDEAYA's Annual
Report on Form 10-K dated February 20, 2024 and any
current and periodic reports filed with the U.S. Securities and
Exchange Commission.
Investor and Media Contact
IDEAYA Biosciences
Andres Ruiz Briseno
SVP, Head of Finance and Investor Relations
investor@ideayabio.com
IDEAYA Biosciences, Inc.
|
Condensed Statements
of Operations and Comprehensive Loss
|
(in thousands,
except share and per share amounts)
|
|
|
|
Three Months
Ended
|
|
|
Nine Months
Ended
|
|
|
|
September
30, 2024
|
|
|
June 30,
2024
|
|
|
September
30, 2024
|
|
|
September
30, 2023
|
|
|
|
(Unaudited)
|
|
|
(Unaudited)
|
|
Collaboration
revenue
|
|
$
|
-
|
|
|
$
|
-
|
|
|
$
|
-
|
|
|
$
|
19,463
|
|
Operating
expenses:
|
|
|
|
|
|
|
|
|
|
|
|
|
Research and
development
|
|
|
57,152
|
|
|
|
54,533
|
|
|
|
154,490
|
|
|
|
90,738
|
|
General and
administrative
|
|
|
9,741
|
|
|
|
10,394
|
|
|
|
28,347
|
|
|
|
21,237
|
|
Total operating
expenses
|
|
|
66,893
|
|
|
|
64,927
|
|
|
|
182,837
|
|
|
|
111,975
|
|
Loss from
operations
|
|
|
(66,893)
|
|
|
|
(64,927)
|
|
|
|
(182,837)
|
|
|
|
(92,512)
|
|
Interest income and
other income, net
|
|
|
15,072
|
|
|
|
12,155
|
|
|
|
38,672
|
|
|
|
13,506
|
|
Net loss
|
|
|
(51,821)
|
|
|
|
(52,772)
|
|
|
|
(144,165)
|
|
|
|
(79,006)
|
|
Unrealized (losses)
gains on marketable
securities
|
|
|
5,252
|
|
|
|
(493)
|
|
|
|
3,274
|
|
|
|
2,121
|
|
Comprehensive
loss
|
|
$
|
(46,569)
|
|
|
$
|
(53,265)
|
|
|
$
|
(140,891)
|
|
|
$
|
(76,885)
|
|
Net loss per share
attributable to common
stockholders, basic and diluted
|
|
$
|
(0.60)
|
|
|
$
|
(0.68)
|
|
|
$
|
(1.81)
|
|
|
$
|
(1.44)
|
|
Weighted-average number
of shares
outstanding, basic and diluted
|
|
|
86,188,510
|
|
|
|
77,962,730
|
|
|
|
79,776,728
|
|
|
|
54,916,150
|
|
IDEAYA Biosciences, Inc.
|
Condensed Balance
Sheet Data
|
(in
thousands)
|
|
|
|
September 30,
|
|
|
December 31,
|
|
|
|
2024
|
|
|
2023
|
|
|
|
(Unaudited)
|
|
Cash and cash
equivalents and short-term and
long-term marketable securities
|
|
$
|
1,200,157
|
|
|
$
|
632,606
|
|
Total assets
|
|
|
1,239,873
|
|
|
|
649,316
|
|
Total
liabilities
|
|
|
59,455
|
|
|
|
28,226
|
|
Total liabilities and
stockholders' equity
|
|
|
1,239,873
|
|
|
|
649,316
|
|
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SOURCE IDEAYA Biosciences, Inc.