- Company Continuing EC1169 Program in Taxane-Exposed Patients, but Ending Clinical Development of
EC1456 and of EC1169 in Taxane-Naïve Patients -
- Refocusing Efforts on Chimeric Antigen Receptor T-cell (CAR T-cell) and Dual-Targeted DNA
Crosslinker Drug EC2629 Programs -
- Restructuring to Reduce Workforce by Approximately 40%; Will Maintain Core Competencies and
Preserve Capital for Highest Priority Programs -
- Conference Call Today at 8:30 a.m. EDT -
WEST LAFAYETTE, Ind., June 02, 2017 (GLOBE NEWSWIRE) -- Endocyte, Inc. (NASDAQ:ECYT), a leader in developing targeted small
molecule drug conjugates (SMDCs) and companion imaging agents for personalized therapy, today announced updates on clinical
development for EC1456, its folate receptor-targeted tubulysin cancer therapy, and EC1169, its prostate-specific membrane antigen
targeted (PSMA-targeted) tubulysin prostate cancer therapy.
Endocyte will narrow the EC1169 development program to focus only on the cohort of taxane-exposed, metastatic
castration-resistant prostate cancer (mCRPC) patients, for which a top-line efficacy assessment of the expansion phase of this
phase 1 trial is expected before the end of 2017. An interim assessment confirmed clinical activity of the drug in the
taxane-exposed cohort with a partial response in one patient, stable disease in other patients, and other markers of activity.
Endocyte believes EC1169 may have benefit in taxane-exposed patients, with more advanced disease, where upregulation of PSMA
increases with prior treatments. Endocyte will stop enrollment of taxane-naïve mCRPC patients in the EC1169 trial.
In addition, the company plans to stop enrollment in the EC1456 trial, where a careful assessment in folate receptor-positive
(FR-positive) disease across multiple cohorts of patients and multiple dosing schedules did not yield the level of clinical
activity necessary to support continued advancement of this agent. However, enrollment of a small number of patients in the EC1456
ovarian cancer surgical study will continue in order to inform other SMDC programs in development. Preliminary data to-date from
the ovarian surgical study provides evidence that patients with FR-positive disease are being successfully identified with the use
of the etarfolatide imaging agent, but the intratumoral levels of the EC1456 drug payload may be lower than predicted by
pre-clinical models.
“Endocyte is a data-driven company, and we are committed to the disciplined management of clinical programs as the science
guides us,” said Mike Sherman, president and CEO at Endocyte. “Recently gained insight into the safety and efficacy of EC1169 and
EC1456, coupled with our commitment to the productive investment of capital, has led us to refocus efforts on our most promising
programs, which include our CAR T-cell SMDC adaptor platform, our dual-targeted DNA crosslinker drug EC2629, and the cohort of
taxane-exposed patients receiving EC1169.”
Endocyte is advancing its work with Seattle Children’s Research Institute aimed at bringing its CAR T-cell bi-specific adaptor
molecule to the clinic in 2018. In addition, the company plans to file its IND for EC2629 in mid-2017, which includes a potent
DNA-targeted warhead with clinically proven activity. To Endocyte’s knowledge, this is the first drug candidate designed to
simultaneously target both tumor cells and tumor associated macrophages (TAMs), which contribute to disease progression by
interfering with natural anti-tumor immune responses.
Endocyte also announced today plans to reduce its workforce by approximately 40 percent in order to better focus its resources
on the company’s highest value opportunities, while maintaining key capabilities.
“As we refocus our clinical development efforts, we are also aligning our investments and resources to advance our most
compelling pipeline programs to key inflection points," added Sherman. “We are very grateful for all the contributions over the
years from our dedicated, talented team of employees, who have devoted so much of themselves towards helping advance our efforts to
bring our innovative, targeted therapies to patients with cancer and other serious diseases. We’ll be working closely with those
affected by the restructuring to support them through this difficult but necessary transition.”
Endocyte anticipates one-time charges of approximately $2.4 million related to termination benefits and the accelerated closure
of the EC1456 trial. As a result of this restructuring, the company is revising its guidance for 2017 and now expects its cash
balance at the end of 2017 to be approximately $105 million, with a more substantial positive impact from the restructuring
beginning in 2018.
About EC1169 and the Phase 1 Trial
EC1169 is an investigational therapeutic SMDC constructed of a high affinity PSMA-targeting ligand conjugated through a
bioreleasable linker system to a potent microtubule inhibitor, tubulysin B hydrazide (TubBH). Patient PSMA-status is determined
using the investigational companion imaging agent, EC0652. EC1169 and EC0652 are currently being evaluated in a phase 1b study in
up to 50 taxane-exposed mCRPC patients at a maximum clinical EC1169 dose of 6.5 mg/m2. Endocyte is stopping enrollment
of taxane-naïve mCRPC patients (ClinicalTrials.gov Identifier: NCT02202447).
The open-label, multicenter, non-randomized, study is divided into two parts. The first part of the study, now complete, was
designed to determine the maximum clinical dose and recommended Phase 2 dose of EC1169 in patients with mCRPC.
Endocyte is currently enrolling the second part of the study which is designed to evaluate the safety and efficacy of EC1169 in
taxane-exposed patients, with a primary study endpoint of radiographic progression free survival in patients selected as
PSMA-positive. The trial is expected to complete enrollment in Q3 2017 with a more mature endpoint assessment by year-end.
About EC1456 and the Phase 1 Trial
EC1456 is an investigational therapeutic SMDC constructed of a high affinity FR-targeting ligand conjugated through a spacer and
bioreleasable linker system to a potent cytotoxic microtubule inhibitor, TubBH. Patient FR-status is determined using the
investigational companion imaging agent, etarfolatide.
Endocyte completed the dose escalation portion of the study designed to determine the maximum clinical dose for multiple dosing
schedules and is stopping enrollment of the phase 1b study which was evaluating EC1456 at a dose of 6.0mg/m2 twice
weekly (BIW) in up to 40 FR-positive non-small cell lung cancer (NSCLC) patients (as determined by an etarfolatide scan).
Endocyte is currently conducting an ovarian cancer surgical study to characterize etarfolatide imaging and intratumoral EC1456
through a multifaceted analysis of collected tissue samples after administration of the drug.
Conference Call
Endocyte management will host a conference call today at 8:30 a.m. EDT.
U.S. and Canadian participants: |
(877) 845-0711 |
International: |
(760) 298-5081 |
A live, listen-only webcast of the conference call may also be accessed by visiting the Investors & News section of the Endocyte
website, www.endocyte.com.
The webcast will be recorded and available on the company's website for 90 days following the call.
Website Information
Endocyte routinely posts important information for investors on its website, www.endocyte.com, in the “Investors & News” section. Endocyte uses this website as a means of
disclosing material information in compliance with its disclosure obligations under Regulation FD. Accordingly, investors
should monitor the “Investors & News” section of Endocyte’s website, in addition to following its press releases, SEC filings,
public conference calls, presentations and webcasts. The information contained on, or that may be accessed through, Endocyte’s
website is not incorporated by reference into, and is not a part of, this document.
About Endocyte
Endocyte is a biopharmaceutical company and leader in developing targeted therapies for the treatment of cancer and other
serious diseases. Endocyte uses its proprietary drug conjugation technology to create novel SMDCs and companion imaging agents for
personalized targeted therapies. The company’s SMDCs actively target receptors that are over-expressed on diseased cells
relative to healthy cells. This targeted approach is designed to enable the treatment of patients with highly active drugs at
greater doses, delivered more frequently and over longer periods of time than would be possible with the untargeted drug alone. The
companion imaging agents are designed to identify patients whose disease over-expresses the target of the therapy and who are
therefore more likely to benefit from treatment. For additional information, please visit Endocyte’s website at www.endocyte.com.
Forward Looking Statements
Certain of the statements made in this press release are forward looking, such as those, among others, relating to future
spending, future cash balances, reduction in personnel, expected impact from the restructuring, expected charges related to the
restructuring, the successful completion of current and future clinical trials, the enrollment period for, and availability and
reporting, of data from ongoing and future clinical trials, and the company's future development plans including those relating to
the completion of pre-clinical development and regulatory authorizations in preparation for possible future clinical trials. Actual
results or developments may differ materially from those projected or implied in these forward-looking statements. Factors that may
cause such a difference include risks that the company may experience delays in the completion of its clinical trials (whether
caused by competition, adverse events, patient enrollment rates, shortage of clinical trial materials, regulatory issues or other
factors); risks that data from its clinical trials may not be indicative of subsequent clinical trial results; risks related to the
safety and efficacy of the company’s product candidates; risks that early stage pre-clinical data may not be indicative of
subsequent data when expanded to additional pre-clinical models or to subsequent clinical data; risks that evolving competitive
activity and intellectual property landscape may impair the company's ability to capture value for the
technology; risks that expectations and estimates turn out to be incorrect, including estimates of the potential markets for
the company’s product candidates, estimates of the capacity of manufacturing and other facilities required to support its product
candidates, projected cash needs, and expected future revenues, operations, expenditures and cash position. More information about
the risks and uncertainties faced by Endocyte, Inc. is contained in the company’s periodic reports filed with the Securities and
Exchange Commission. Endocyte, Inc. disclaims any intention or obligation to update or revise any forward-looking statements,
whether as a result of new information, future events or otherwise.
Contact: Stephanie Ascher, Stern Investor Relations, Inc., (212) 362-1200, stephanie@sternir.com