Hepatocellular Carcinoma Clinical Trial
Official title:
A Phase I/II Dose Escalation Trial of HDAC Inhibitor Tefinostat for Cancer Associated Inflamation in Hepatocellular Carcinoma
This study is being carried out to assess the best dose of a new drug, called tefinostat, in
treating liver cancer.
Tefinostat is a new drug that blocks enzymes called histone deacetylases (pronounced
dee-as-et-isle-azes). Cells need these enzymes to grow and divide. Blocking them may stop
cancer growing. Drugs that block these enzymes are called histone deacetylase inhibitors or
'HDAC inhibitors'.
Tefinostat has never been given to patients with liver cancer before so it isn't known which
dose is best at treating liver cancer. To find this out the study will be testing one dose
and if that is safe, then test a higher dose and so on.
The aim of this study is to find the best dose of tefinostat without causing side effects.
The study will be looking closely at any side effects patients might experience from this
treatment.
This is an open label, dose escalating, phase I/II study of Tefinostat administered orally,
once or twice daily in 28 day cycles of treatment in patients with advanced hepatocellular
carcinoma.
The starting dose of the Phase I dose escalation stage of the study has been based on the
results of a previous Phase I trial of Tefinostat in patients with haematological
malignancies. The starting dose of Tefinostat will be 360mg OD. As Tefinostat has a median
plasma half-life of 0.47h (range 0.19 to 1.18) and CHR-2847 a median half-life of 1.4 h
(range 0.98 to 3.79) twice daily dosing will also be investigated, starting at 240mg BID.
Phase I Up to 5 cohorts of 3-6 patients will be treated for 28 days once or twice daily (360,
480mg once daily, then 240, 360, 480mg twice daily) to determine safety and tolerability of
Tefinostat and to identify the recommended dose for Phase II (RP2D). Patients with stable
disease or with a tumour response will be allowed to continue treatment until PD or
unacceptable toxicity, at the discretion of the Investigator.
Patients with advanced HCC who have not received prior systemic therapy will be eligible for
the study if they are Child-Pugh classification A and are not candidates for surgical
treatment, with adequate bone marrow, hepatic and renal function. Patients should not have a
history of organ allograft or any serious concurrent illness.
Doses will be increased in a stepwise fashion and the decision to do so will be made by the
participating Investigators on the basis of DLT, PK and PD. The starting dose will be 360mg
od. Should this dose not be safe the dose level may be reduced to 240mg od. Dosing will
initially take place once a day, for 28 days, while later cohorts will investigate twice
daily dosing. More than one DLT in a once daily dose cohort will not preclude investigation
of twice daily dosing at a lower dose.
Decisions to escalate to the next dose level, will be made jointly by the participating
Investigators based on review of all the available data from the first cycle of treatment for
each patient of that cohort. The first subject must have completed 7 days of the course of
treatment before the next two subjects are enrolled. All subjects treated in that cohort must
have undergone repeated safety evaluations prior to enrolment of the next dose cohort.
If a subject withdraws or is withdrawn from the study prior to completion of the first
treatment period, in the absence of a DLT, that subject must be replaced and the replacement
patient dosed at the scheduled dose, not completed, before dose escalation can occur.
Upon completion of the first treatment period of 28 days (dose finding, Phase I), suitable
patients may continue with further treatment as described under Duration of Treatment, at the
discretion of the investigator.
The available clinical and safety information from this trial as well as the previous single
agent study of Tefinostat will be reviewed by the participating investigators, who will agree
the RP2D.
The Phase I data will be reviewed by the participating investigators prior to progressing to
Phase II.
Patients will be treated at the recommended phase II dose (RP2D) selected in Phase I, over an
84 day course of treatment. Approximately 39 patients with advanced HCC will be treated.
Patients who have stable disease or with a tumour response after the 84 day treatment period
will be allowed to continue treatment until PD or unacceptable toxicity, at the discretion of
the treating investigator. Patient recruitment will continue until approximately 40 patients
treated at the RP2D, including those already treated at that dose in Phase 1, are evaluable
for response following treatment with at least 84 days of study therapy.
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