Pegylated Liposomal Mitomycin C Lipidic Prodrug and Palliative Radiotherapy– a Phase 1B Study
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Abstract
Pegylated Liposomal Mitomycin C Lipidic Prodrug and Palliative Radiotherapy– a Phase 1B Study
Authors: Eli Sapir1, Raphael Pfeffer2, Marc Wygoda3, Adi Levy3, Benjamin Corn4, Patricia Ohana5, Alberto Gabizon6
1Assuta Ashdod University Hospital, Radiation Oncology, Ashdod, Israel; 2Assuta Medical Center, Tel Aviv, Israel, Radiation Oncology, Tel Aviv, Israel; 3Hadassah Hebrew University Medical Center, Radiation Oncology, Jerusalem, Israel; 4Shaare Zedek Medical Center, Radiation Oncology, Jerusalem, Israel; 5Lipomedix Pharmaceuticals, Clinical Trials , Jerusalem, Israel; 6Shaare Zedek Medical Center, Oncology department, Jerusalem, Israel
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Purpose or Objective
Mitomycin C (MMC) is a well-established radiosensitizer.
However, MMC is associated with severe hematological and renal toxicity
limiting its use. Early clinical studies indicate that a novel formulation of
pegylated liposomal MMC lipidic prodrug (Promitil®) is safe and effective with
limited hematotoxicity compared with MMC. Furthermore, in preclinical studies,
it had promising radiosensitizing activity. The primary objectives of this phase
1B study of Promitil® with radiotherapy (RT) were to evaluate safety
and tumor response in the irradiated field in patients requiring palliative RT.
Secondary objectives were to determine plasma prodrug (MLP) levels after each Promitil®
infusion and systemic anti-tumor response
Material and Methods
The protocol was
approved by the respective IRBs. 19 eligible pts with metastatic (18) or inoperable (1) disease, received a combination of Promitil® and standard of care RT. Most pts (16) were diagnosed with
advanced GI tract cancer. The treatment included two Promitil® doses, at 21-day intervals, and RT
initiated 1-3 days after the first Promitil® dose and completed within 2-weeks. Ten fractions
of conventionally fractionated RT or 5 SBRT fractions were allowed. The study consisted
of 3 dose-escalation cohorts of Promitil® of 6 patients each: 1.25 mg/kg, 1.5 mg/kg, and 1.8 mg/kg. Dose escalation
proceeded if no dose-limiting toxicities (DLT) were recorded by study day 43 in
more than 1/6 patients.
Patients were assessed weekly during the Promitil®
cycle (42 days after last dose of Promitil®).
Status of the irradiated and non-irradiated lesions, if present, was
reevaluated by CT between days 43-50, and every 6 weeks thereafter. In
addition, MMC prodrug plasma levels were analyzed 1 h and 1 day after each dose
of Promitil®
Results
18/19 pts completed two Promitil® infusions and the entire RT course.
No DLT was reported. Two SAEs were reported, one considered non-related and one
possibly related Grade 4 neutropenia . Most of the AEs were deemed mild or
moderate. The most common AEs - possibly related to the study drug - were
thrombocytopenia, fatigue and vomiting. No severe RT-related reaction was
reported. 18/19 pts were evaluable for efficacy. 16/18 patients were free of
disease progression in the irradiated target lesion (1 complete response, 9 partial
response, 6 stable, 2 progressive disease). Median survival of patients in the 3
cohorts was 103 weeks. Plasma analysis showed high level of MLP correlating
with the increase in dose level and a similar profile before and after RT. About
50 % of MLP was still in circulation 24h after Promitil® infusion. No
free MMC was detectable in plasma
Conclusion
Promitil® combined
with RT is safe at a dose of 1.8 mg/kg every 3 weeks with a high rate of tumor
control in a variety of tumor types. Drug clearance is not affected by
radiation. Promitil® is a novel and attractive option for
radiosensitization that should be evaluated in future randomized studies in the
palliative (and possibly the curative) setting