Metastatic Malignant Neoplasm to Brain Clinical Trial
Official title:
A Phase II Trial: Safety and Tolerance of Intravenous 4-Demethyl-4-cholesteryloxycarbonylpenclomedine (DM-CHOC-PEN) in Patients With Malignancies Involving the Central Nervous System
DM-CHOC-PEN is a polychlorinated pyridine cholesteryl carbonate that has demonstrated
antineoplastic activities in patients with advanced cancers - melanoma, lung, breast and
glioblastoma multiforme (GBM) involving the CNS during a Phase I study. These findings
support the preclinical responses seen in mice bearing intracerebrally implanted human breast
and GBM tumor xenografts. Toxicity was acceptable - hyperbilirubinemia (in patients with
liver disease and/or liver metastasis). No hematological, renal, cardiovascular, behavioral
or cognitive impairment/neurotoxicities were noted during the Phase I human trial or in
previous pre-clinical studies.
The drug is available for use as a soy bean oil/egg yolk lecithin/glycerin water emulsion;
the latter continues to be chemically and biologically stable and safe.
Patients with advanced lung, breast and melanoma cancers spread to the CNS and primary CNS
malignancies will be eligible for enrollment and treatment, providing the required blood and
other eligibility requirements are met. The trial will be 2-tiered - patients with liver
involvement vs. non-liver involvement will be treated with different doses of the drug.
The trial is open and patients are currently being enrolled and treated with the protocol.
DM-CHOC-PEN has been selected for Phase II intravenous studies in the treatment of patients
with advanced malignancies with central nervous system measurable disease based on the
improved PFS and objective responses seen for patients treated during the Phase I DTI-021
trial and the manageable toxicities noted. Melanoma, breast and lung cancers involving the
CNS have responded to DM-CHOC-PEN in the Phase I study, thus the basis for the choice of
tumors to be treated in the Phase II trial. Currently, the opinion is that the drug is
penetrating the blood brain barrier (BBB) attached to rbcs and released intracerebrally in
tumor masses in situ.
The trial will be carefully monitored, and if a cancer type has >3 confirmed responders in
the first 18 evaluable patients (Stage -1 enrollment); accrual will be expanded for that
tumor type with a goal of 7/43 for achieving an 80% power at the 5% level of significance
(Stage-2 enrollment) with unacceptable response rate (P0) 0.1 and desirable response rate
(P1) 0.25. Thus, each arm will have a 2-stage design. This will allow resources to be
directed to the most promising areas - selection of 1 or 2 tumor types to develop via
additional trial studies. A desirable response rate is 25% or better. The above is for each
tumor type - lung, breast, melanoma and GBM.
In summary, for any tumor type or treatment sub-group, a response rate of <15% or a rate of
"possibly treatment-related Gr-3/4 toxicities" of >25% will be considered unacceptable and
enrollment in the respective tumor type category will be discontinued.
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