Metastatic Melanoma Clinical Trial
Official title:
Phase II Evaluation of RFT5-dgA in Patients With Metastatic Melanoma
Background:
- CD4+ cells are white blood cells that regulate the immune system by controlling the
strength and quality of the immune response.
- CD25+ cells are a subset of CD4+ cells that suppress or prevent immune responses.
- RFT-5-dgA is an immunotoxin (substance that kills specific cells in the immune system)
that kills CD25+ cells.
- In mouse studies, RFT-5-dgA showed anti-tumor activity in animals studies.
Objective: To determine whether the immune system of patients with metastatic melanoma
(melanoma that has spread beyond the original site) can cause tumors to shrink if the
patients are given RFT-5-dgA to remove their CD25+ cells.
Eligibility: Patients 18 years of age and older with metastatic melanoma whose disease has
progressed after receiving standard treatment.
Design:
- Patients receive RFT-5-dgA through a vein every other day for a total of 3 doses (one
treatment course). Patients have routine blood tests during the week of treatment.
- Four to 5 weeks after the last dose, patients are evaluated with a physical examination,
blood tests and scans and x-rays to evaluate their tumor.
- Patients whose tumor has shrunk or remained stable may be offered additional treatment
with RFT-5-dgA up to a total of four courses.
- Patients undergo leukapheresis or have several tubes of blood drawn from a vein to
determine the effects of RFT-5-dgA on the immune system. This is done before the first
dose of RFT-5-dgA, after the first three doses, and possibly during subsequent treatment
courses in those patients who receive additional treatment. For leukapheresis, blood is
collected through a needle in an arm vein and flows through a catheter into a machine
that separates it into its components by spinning. The white cells are extracted and the
rest of the blood is returned through another needle in the other arm.
Background:
- RFT5-dgA is an immunotoxin comprised of the IL-2Ra-specific murine IgG1 antibody RFT5
linked to deglycosylated ricin A chain (dgA) via the sterically hindered
heterobifunctional disulfide linker SMPT
(4-succinimidyl-oxycarbonyl-a-methyl-a-(2-pyridyldithio)-toluene).
- RFT5-dgA is a recombinant immunotoxin that selectively targets CD25 expressing cells in
vivo. Further, treatment of human PBMC with RFT5-dgA in vitro results in the
preferential depletion of CD25+ Treg cells.
- Depletion of Treg cells can enhance tumor protection to tumor-associated antigens
expressed as self antigens and the RFT5-dgA immunotoxin had potent antitumor effects in
SCID mice xenografted with L540 cells which express CD25.
- The MTD established in the phase I trial of RFT5-dgA was 15mg/m(2)/course IV.
Objectives:
- The primary objective is to determine whether objective clinical responses can be
obtained in patients with metastatic melanoma following administration of RFT5-dgA.
- Secondary objectives will determine whether changes occur in levels of CD4+CD25+
regulatory T cells (Treg cells) in peripheral blood from before to after treatment and
evaluate the toxicity profile of patients treated on this trial.
Eligibility:
- Patients greater than 18 years of age with measurable metastatic melanoma, an expected
survival greater than three months, who have progressed after receiving standard therapy
will be included.
- Standard clinical laboratory values must be normal for study inclusion and patients may
not be pregnant, breast-feeding or require anticoagulation.
- Patients must be willing to undergo leukapheresis.
- Patients with active infections, other major medical disorders, HAMA levels greater than
1 ug/mL, or who have had prior radiotherapy or who have extensive lung disease will be
excluded.
Design:
- Patients will receive 3 mg/m(2) RFT5-dgA intravenously every other day for a total of 3
doses (one course).
- Four to five weeks after the last dose, patients will undergo tumor evaluation,
evaluation of changes in T-regulatory cells (CD4+CD25+cells and Foxp3 expression), and
toxicity assessment.
- One additional course may be administered to patients with stable disease or partial or
complete response.
- Up to 41 evaluable patients may be accrued to determine whether theRFT5-dgA can produce
a modest response rate targeted to be 20 percent (p1=0.20)
- Enrollment reflects the anticipated enrollment. Actual enrollment is unknown due to no
longer having access to the data as records were destroyed
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