ABC-108 is a single-arm Phase IIA clinical study of ABC294640 (Yeliva ®, opaganib) alone
and in combination with hydroxychloroquine sulfate (HCQ) in the treatment of
cholangiocarcinoma (CCA). In Part 1 of this clinical study, all participants will be
receiving ABC294640 and in Part 2 all participants will be receiving ABC294640 and HCQ to
explore the drugs activity signal in CCA. The study drug, ABC294640 is an orally
available inhibitor of the enzyme sphingosine kinase-2 (SK2). SK2 is an innovative target
for anti-cancer therapy because of its critical role in sphingolipid metabolism, which is
known to regulate tumor cell death and proliferation. ABC294640 also inhibits
proliferation and induces apoptosis of cholangiocarcinoma cell lines. Furthermore, in a
recent Phase I trial, ABC294640 demonstrated clinical activity in CCA patients. HCQ, is
an orally available, FDA approved therapy for the treatment of malaria as well as discoid
and systemic lupus erythematosus and rheumatoid arthritis. It is also known as an
inhibitor of autophagy, a pro-survival mechanism utilized by many cancers. Evidence
indicates that inhibition of autophagy can increase the therapeutic activity of ABC294640
in CCA. In Part 1 of this study, ABC294640 will be continuously administrated orally,
twice a day, in 28 day cycles. In Part 2, ABC294640 and HCQ will be continuously
administrated orally (the safe and tolerable will be determined in the study) in 28 day
cycles. Administration of drug/s in both parts of the study will continue until disease
progression, unacceptable toxicity or voluntary withdrawal initiated by the participants
or physician.
Additional locations may be listed on ClinicalTrials.gov for NCT03377179.
See trial information on ClinicalTrials.gov for a list of participating sites.
This is an open-label clinical study to explore the activity signal of ABC294640 and of
ABC294640 and HCQ in adult subjects who have been diagnosed with unresectable
cholangiocarcinoma either intra- perhilar or extra-hepatic. The study will be conducted
at 5 sites in the USA.
For Part 1, a maximum of 39 participants evaluable for efficacy will be enrolled in the
study. Eligible participants will receive ABC294640, 500 mg twice a day, continuously
administered in 28 day cycles.
Part 2 will be a single-arm Phase IIA study identical to Part 1 but treatment will
consist of both ABC294640 together with HCQ. Additionally, Part 2, will consist of two
phases: Phase I: accelerate HCQ dose-escalation run-in starting with a HCQ dose of 200 mg
QD (once a day). Based on safety results, patient cohorts will be expanded, and dosing
will continue to 200 mg BID (twice a day), 400 mg BID and 600 BID. At the end of Part2,
Phase I, it will be determined what is the safe and tolerable HCQ dose for Phase II.
For Part 2, up to 15 patients evaluable for safety and tolerability will be enrolled in
Phase I component of Part 2; and 20 patients evaluable for efficacy in the Phase II
component of Part 2. All eligible participants will receive ABC294640, 500 mg BID in
addition to the determined HCQ dose, continuously administered in 28 day cycles.
In addition to physical, neurological and eye exams (eye exams only for participants
receiving HCQ), blood and urine samples will be routinely collected for safety and to
determine response to the study drugs. Participants will be radiographically assessed for
disease status every 2 cycles of treatment.
Tumor biopsies, when accessible, will be obtained within 21 days prior to the beginning
of treatment and again on the beginning of the second treatment cycle.
All participants will be followed every 2 months for progression and survival for a
maximum of 24 months after the last patient has been entered to the study. Follow up
procedures may include physical examination, laboratory work and radiographic tumor
assessment.
Lead OrganizationRedHill Biopharma Limited
