Melanoma Clinical Trial
Official title:
A Multi-centre, Two-stage, Open Label Phase II Study to Assess the Efficacy and Safety of APO866 in the Treatment of Patients With Advanced Melanoma.
This phase II study is designed to determine the efficacy and safety of APO866 for the treatment of patients with advanced cutaneous melanoma. APO866 has shown to induce growth inhibition in cultures of human melanoma cells as well as in animal models with subcutaneously implanted melanoma tumors. APO866 was considered to be safe and well tolerated in a phase I study that treated 24 patients with advanced cancer. In that study one of the two patients with advanced melanoma had a stable disease for 5 months with size reduction of some lesions. APO866 is administered by intravenous infusion continuously for 96 hours that is repeated every 4 weeks. Patients will receive 3 cycles of treatment and the primary efficacy endpoint will be assessed at Week 16. Patients will be follow-up for 12 months.
Advanced melanoma is one of the most chemo-resistant types of human cancers. The incidence
increases by about 2.5% on an annual basis, with may partially be related to aging and
growth of the population, as well as other environmental risk factors. Virtually no recent
progress has been made in the treatment of patients with this disease. In the past 30 years,
the FDA has approved only 2 agents, dacarbazine and interleukin-2, on the basis of overall
response and response duration, respectively. However, these outcomes were not accompanied
by a survival benefit. The most recent randomized study of Dacarbazine (DTIC) yielded an
overall response rate of 7%, and to date, no other treatments, including combination
therapies, have shown to improve survival when compared to DTIC alone. Hence, the mainstay
of treatment for patients with advanced melanoma is DTIC-based therapy.
APO866 is a novel drug that induces cell death by specifically inhibiting the biosynthesis
of Niacinamide Adenine Dinucleotide (NAD+) from niacinamide, which is essential for the
cellular metabolism, protein modification and messenger synthesis. APO866 is not subject to
the commonly known mechanisms of multi drug resistance (MDR). Its activity is cell cycle
independent. APO866 exerted high anti-tumor activity on a broad range of different tumor
cells derived from both human solid cancers and leukemias in vitro and on a large number of
human xenografts in nude mice, including melanoma, and rats in vivo. Hematologic cancer
cells were highly sensitive to APO866. Lymphocytes are the most sensitive normal cells to
APO866 resulting in lymphocytopenia and reticulocytopenia in rats, monkeys. Furthermore,
APO866 may have anti-angiogenic properties as shown in vivo.
APO866 was investigated in 24 patients with advanced cancers in a phase I study aiming to
determine the dose-limiting toxicity (DLT) and maximum tolerated dose (MTD). Treatment was
well tolerated and safe. The unique DLT was thrombocytopenia. At dose levels higher than
0.036 mg/m2/hr CTC grade III lymphocytopenia, not thought to be clinically relevant,
preceded all other toxicities. The recommended dose for phase II studies of APO866 is 0.126
mg/m2/hr administered by civ infusion for 4 consecutive days evry 4 weeks. This dose was
selected because of its safety profile, and the translational observation that Css of APO866
at MTD was similar or higher as compared to the concentrations at which efficacy was
established in vitro and in vivo. In addition, a transient decrease of serum vascular
endothelial growth factor (VEGF) levels, a surrogate marker of angiogenesis, was observed
within 96 hrs after the start of treatment in 9 out of 11 patients treated at MTD and the
0.144 mg/m2/hr dose level of APO866.
No objective tumor response was observed. However, 4 patients had stable disease for at
least 3 months: prostate cancer (4 months), melanoma (5 months), sarcomatoid mesothelioma (3
months) and oropharyngeal cancer (5 months). In addition, lesion size reductions were
observed in the melanoma patient (80% size reduction and stable size of other lesions) at an
APO866 dose level of 0.072 mg/m2/hr, and in the mesothelioma patient (moderate size
reductions of pleural lesions) at 0.108 mg/m2/hr.
Treatment with APO866 was safe and well tolerated. The anti-tumor effect of APO866, in
particular on melanoma cells in vitro and in vivo, and its anti-angiogenic propriety support
the rationale to conduct a open phase II study of APO866 in patients with advanced melanoma.
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Endpoint Classification: Safety/Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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