Crinetics Pharmaceuticals, Inc. (Nasdaq: CRNX) today announced two
abstracts from its transformative, in-house discovery and
development programs will be presented at the upcoming North
American Neuroendocrine Tumor Society Multidisciplinary NET Medical
Symposium (NANETS 2024), taking place November 21-23, 2024, in
Chicago.
“We are eager to share our latest pipeline progress at NANETS
2024. Crinetics is committed to the neuroendocrine tumor community,
and we are now utilizing our world class drug discovery and
development capabilities to support people living with both
functional and non-functional NETs,” said Scott Struthers, Ph.D.,
Founder and Chief Executive Officer of Crinetics. “We are excited
to present preclinical data from our groundbreaking nonpeptide drug
conjugate platform for our lead candidate CRN09682, an
investigational anti-tumor therapy targeting SST2-expressing
tumors, including NETs. We will also present data from the Phase 2
clinical study of our investigational drug candidate paltusotine,
highlighting its ability to reduce the frequency and severity of
carcinoid syndrome symptoms in patients with functional NETs.”
CRN09682, is a first-in-class, somatostatin receptor 2 (SST2)
targeted, nonpeptide drug conjugate (NDC). Built upon the
well-validated concept of antibody-drug conjugates, Crinetics’ NDCs
use a highly optimized small molecule G protein coupled receptor
(GPCR) ligand, instead of an antibody, to deliver a potent
anti-cancer agent to tumor cells with high selectivity and
efficiency. CRN09682 was designed to provide enhanced tumor
penetration, selectively bind to SST2 expressing tumor cells,
induce internalization, and intracellularly release a potent
anti-tumor agent, while minimizing systemic exposure and associated
toxicities. In addition, CRN09682 is manufactured by traditional
chemical synthesis methods, avoiding the complex and heterogeneous
manufacturing methods required for antibody drug conjugates.
Preclinical data to be presented at NANETS 2024 demonstrate the
potent and selective anti-tumor activity of CRN09682, potentially
providing a novel alternative for the treatment of NETs and other
SST2-expressing tumors.
Another abstract will be featured as both an oral and poster
presentation, which includes follow-up from an open-label Phase 2
carcinoid syndrome study of investigational candidate paltusotine,
a once-daily, oral, nonpeptide, selective SST2 agonist being
developed for the treatment of acromegaly and carcinoid syndrome.
The NANETS presentation includes findings from all 36 trial
participants, with new analyses that show paltusotine reduced the
frequency and severity of carcinoid syndrome symptoms and was well
tolerated, justifying further clinical development.
Data for paltusotine and CRN09682, along with additional
information on NDCs, will also be featured in a Crinetics-sponsored
symposium titled “Paltusotine and CRN09682: Novel Nonpeptide
Approaches to Treating Carcinoid Syndrome and Neuroendocrine
Tumors” at the conference on Thursday, November 21, from 12:15-1:15
p.m. CT. Featured speakers include Scott Struthers and Dr. Aman
Chauhan, leader of Neuroendocrine Oncology and Co-Leader
Radiopharmaceutical Drug Development at Sylvester Comprehensive
Cancer Center, University of Miami Health System.
Details on the abstracts to be presented
at NANETS are shown below:
Title: |
A Novel
Nonpeptide Drug Conjugate (NDC) for the Treatment of Somatostatin
Receptor 2-Expressing Tumors |
Date/Time: |
Poster: November 21, 5:15 pm CT |
|
|
Title: |
Once-daily Oral Paltusotine in the Treatment of Patients With
Carcinoid Syndrome: Results From a Phase 2, Randomized,
Parallel-Group Study |
Date/Time: |
Oral: November 22 from 3:10 – 3:22 pm CT |
|
Poster: November 21, 5:15 pm CT |
The poster presentations will be made available on the Crinetics
website at the time of presentation in accordance with the NANETS
embargo policy.
ABOUT CRN09682CRN09682 is an investigational,
potentially first-in-class, non-radioactive, nonpeptide drug
conjugate (NDC) linking a somatostatin receptor 2 (SST2) agonist
with the cytotoxic drug monomethyl auristatin E (MMAE) via a spacer
and a cleavable linker for the treatment of neuroendocrine tumors
(NETs) and potentially for use in other solid tumors that express
SST2. The SST2 ligand on the NDC molecule binds to SST2 on the
tumor cell surface and is internalized in the cell whereby enzymes
cleave the MMAE and release it within the cell. MMAE is known to
cause microtubule disruption leading to cell arrest and death. The
NDC approach is intended to enhance tumor penetration, selectively
bind to specific GPCR expressing tumor cells, induce
internalization, and intracellularly release a potent anti-tumor
agent, while minimizing systemic exposure and associated
toxicities. Additionally, NDCs are manufactured by traditional
chemical synthesis methods, avoiding the limitations of
fermentation, bioconjugation, and heterogeneous manufacturing
methods required by most ADCs. NETs are generally incurable when
metastatic, regardless of tumor grade. Overall survival rates vary
significantly by stage, grade, age at diagnosis, primary site, and
time period of diagnosis.
ABOUT PALTUSOTINECrinetics’ lead development
candidate, paltusotine, is the first investigational once-daily,
oral, selective somatostatin receptor type 2 (SST2) nonpeptide
agonist that has completed Phase 3 clinical development for
acromegaly and is in Phase 2 clinical development for carcinoid
syndrome associated with neuroendocrine tumors. It was designed by
Crinetics with the goal of providing a once-daily, oral option for
reliable and consistent control of acromegaly and carcinoid
syndrome. In Phase 3 studies, once-daily, oral paltusotine
maintained IGF-1 levels and symptom control in patients with
acromegaly who were switched from monthly injectable medications
(PATHFNDR-1) and rapidly decreased IGF-1 levels and symptom burden
in medically untreated acromegaly patients (PATHFNDR-2). IGF-1 is
the primary biomarker endocrinologists use to manage acromegaly
patients. Results from the Phase 2 study in carcinoid syndrome
provide supporting data and rationale for paltusotine to initiate a
Phase 3 trial for another important indication related to the
treatment of carcinoid syndrome in patients with neuroendocrine
tumors.
ABOUT CRINETICS PHARMACEUTICALSCrinetics
Pharmaceuticals is a clinical stage pharmaceutical company focused
on the discovery, development, and commercialization of novel
therapeutics for endocrine diseases and endocrine-related tumors.
Crinetics’ lead development candidate, paltusotine, is the
first investigational once-daily, oral, selective somatostatin
receptor type 2 (SST2) nonpeptide agonist that has completed Phase
3 clinical development for acromegaly and is in Phase 2 clinical
development for carcinoid syndrome associated with neuroendocrine
tumors. Crinetics is also developing atumelnant (CRN04894), an
investigational, first-in-class, oral ACTH antagonist, that is
currently completing Phase 2 clinical studies for the treatment of
congenital adrenal hyperplasia and Cushing’s disease. All of the
company’s drug candidates are orally delivered, small molecule new
chemical entities resulting from in-house drug discovery efforts,
including additional discovery programs addressing a variety of
endocrine conditions such as hyperparathyroidism, polycystic kidney
disease, Graves’ disease (including thyroid eye disease), diabetes,
obesity and GPCR -targeted oncology indications.
Forward-Looking Statements This press release
contains forward-looking statements within the meaning of Section
27A of the Securities Act of 1933, as amended, and Section 21E of
the Securities Exchange Act of 1934, as amended. All statements
other than statements of historical facts contained in this press
release are forward-looking statements, including statements
regarding the plans and timelines for the clinical development of
paltusotine and CRN09682, including the therapeutic potential and
clinical benefits or safety profile thereof; and IND-enabling
studies for CRN09682; plans to develop CRN09682; and preclinical
studies may not proceed at the time or in the manner expected, or
at all; the timing and outcome of research, development and
regulatory review is uncertain, and Crinetics’ drug candidates may
not advance in development. In some cases, you can identify
forward-looking statements by terms such as “may,” “will,”
“should,” “expect,” “plan,” “anticipate,” “could,” “intend,”
“target,” “project,” “contemplates,” “believes,” “estimates,”
“predicts,” “potential,” “upcoming,” or “continue” or the negative
of these terms or other similar expressions . These forward-looking
statements speak only as of the date of this press release and are
subject to a number of known and unknown risks, uncertainties and
assumptions, including, without limitation, initial or topline data
that we report may change following a more comprehensive review of
the data related to the clinical studies and such data may not
accurately reflect the complete results of a clinical study, the
possibility of unfavorable new clinical data and further analyses
of existing clinical data, and the U.S. Food and Drug
Administration and other regulatory authorities may not agree with
our interpretation of such results; we may not be able to obtain,
maintain and enforce our patents and other intellectual property
rights, and it may be prohibitively difficult or costly to protect
such rights; geopolitical events may disrupt Crinetics’ business
and that of the third parties on which it depends, including
delaying or otherwise disrupting its clinical studies and
preclinical studies, manufacturing and supply chain, or impairing
employee productivity, unexpected adverse side effects or
inadequate efficacy of the company’s product candidates that may
limit their development, regulatory approval and/or
commercialization; the company’s dependence on third parties in
connection with product manufacturing, research and preclinical and
clinical testing; the success of Crinetics’ clinical and
nonclinical studies; regulatory developments in the United States
and foreign countries; clinical studies and preclinical studies may
not proceed at the time or in the manner expected, or at all; the
timing and outcome of research, development and regulatory review
is uncertain, and Crinetics’ drug candidates may not advance in
development or be approved for marketing; Crinetics may use its
capital resources sooner than expected; any future impacts to our
business resulting from geopolitical developments outside our
control; and the other risks and uncertainties described in the
company’s periodic filings with the Securities and Exchange
Commission (SEC). The events and circumstances reflected in the
company’s forward-looking statements may not be achieved or occur
and actual results could differ materially from those projected in
the forward-looking statements. Additional information on risks
facing Crinetics can be found under the heading “Risk Factors” in
Crinetics’ periodic filings with the SEC, including its annual
report on Form 10-K for the year ended December 31, 2023 and its
Quarterly reports on Form 10-Q for the quarters ended March 31,
2024, June 30, 2024 and September 30, 2024. You are cautioned not
to place undue reliance on these forward-looking statements. Except
as required by applicable law, Crinetics does not plan to publicly
update or revise any forward-looking statements contained herein,
whether as a result of any new information, future events, changed
circumstances or otherwise.
Contact:
Investors:Gayathri DiwakarHead of Investor
Relationsgdiwakar@crinetics.com(858) 345-6340
Media: Natalie BadilloHead of Corporate
Communicationsnbadillo@crinetics.com(858) 345-6075
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