Kidney Cancer Clinical Trial
Official title:
Immunization of Patients With Renal Cancer Using HLA-A2 and HLA-A3-Binding Peptides From Fibroblast Growth Factors 5 (FGF-5)
This study will evaluate the safety and side effects of two experimental vaccines in
patients with kidney cancer and determine whether the vaccines "turn on" an immune response
to the cancer. Each vaccine contains one of two peptides (pieces of proteins) from the
fibroblast growth factor 5 (FGF-5) antigen, a protein produced by some cancer cells, and an
oil-based liquid called Incomplete Freud's Adjuvant (Montanide ISA-51) that enhances the
immune response to the vaccine.
Patients 16 years of age and older who have kidney cancer that has spread beyond the kidney
or whose primary kidney tumor has been removed within 6 months before entering the study and
are at high risk for disease recurrence may be eligible for this study. Patients must have
tissue type human leukocyte antigen serotype within HLA-A A serotype group (HLA-A2) or human
leukocyte antigen serotype within HLA-A A serotype group (HLA-A3) (determined by a blood
test for human leukocyte antigen (HLA) typing) and their tumors must produce the FGF-5
peptide. Candidates are screened with a physical examination, blood and urine tests,
electrocardiogram (EKG), tumor biopsy (removal of a small sample of tumor for examination)
in patients whose tumor is easily accessible, and scans (computed tomography (CT), bone
scans) and x-rays if current scans are not available.
Participants are divided into two groups according to their HLA type (HLA-A2 or HLA-A3) to
receive the vaccine appropriate for their HLA type. They are then further divided into three
groups: 1) Group 1 includes patients who do not need or are ineligible for treatment with
interleukin-2 (IL-2), a protein made by certain infection-fighting white cells that helps
fight tumors) and patients who have previously had IL-2 therapy; 2) Group 2 includes
patients who require immediate treatment with IL-2; and 3) Group 3 includes patients whose
cancer has been surgically removed but who are at risk for recurrence.
Patients in Groups 1 and 3 receive two peptide injections four times a week every 3 weeks
for up to a year, or until their tumor grows (or returns in patients in Group 3) or the side
effects are too severe to continue. Tumors are evaluated with a physical examination and
scans or x-rays every 12 weeks and blood tests are done every 3 weeks. Patients in Group 2
receive two peptide injections every day for 4 days, along with doses of IL-2 starting the
day after the first peptide injection. The vaccines are given as injections under the skin
of the thigh. IL-2 is infused through a vein over 15 minutes every 8 hours for up to 12
doses, depending on tolerance. The vaccine and IL-2 are repeated every 10 to 14 days, with
tumor evaluations every 2 months. Patients stay in the hospital about 1 week during each
treatment cycle to receive the IL-2.
All patients undergo leukapheresis, a procedure for collecting large numbers of white blood
cells. Blood is collected through a needle in an arm vein and flows through a cell separator
machine, where the white cells are extracted. The rest of the blood is returned to the
patient through the same needle or a needle in the other arm. The white cells are examined
to evaluate how the vaccines change the action of immune cells. Some patients may undergo an
additional biopsy of normal skin and tumor or lymph node to look at the effects of the
vaccine on the immune cells in the tumor.
Patients in Group 1 whose cancer grows and patients in Group C whose cancer returns may be
offered IL-2 treatments as given to Group 2 patients, along with the peptide vaccine. If the
disease responds to IL-2, the treatment may be repeated after 2 months.
Background:
Several preliminary clinical results in the treatment of cancer lend credence to the
hypothesis that augmented T-cell responses will improve IL-2 therapy. A peptide vaccine
derived from the melanoma/melanosomal antigen, GP100, when given with high-dose IL-2
resulted in a response rate over 30% in a small Phase II study. These results have led to
efforts to identify similar T-cells and tumor-associated antigens for IL-2 responsive tumors
such as renal cell cancer. Work in our laboratory generated a renal cancer-reactive T-cell
clone, raised from tumor-infiltrating lymphocytes (TIL) within a renal cell cancer (RCC)
metastasis undergoing spontaneous regression. This clone was HLA-A3 restricted and
recognized autologous tumor as well as a number of allogeneic RCC lines also expressing
HLA-A3. Expression cloning of the antigen recognized by this clone demonstrated that the
RCC-associated antigen being recognized was unmutated fibroblast growth factor 5 (FGF-5). We
concluded from numerous studies that FGF-5 was a tumor associated antigen over-expressed by
a majority of RCC and that it had several favorable characteristics as a target for
immunotherapy. At this point, having demonstrated in the laboratory that tumor-reactive
T-cells generated from patients with renal cancer can recognize naturally presented FGF-5 in
either the context of HLA-A2 or HLA-A3 via the minimal determinants 117-126:FGF-5
(MLSVLEIFAV) or FGF-5:172-176/217-220 (NTYASPRFK), respectively. With this study we plan to
determine if vaccination with these peptides can enhance the number of FGF-5-reactive
cytotoxic T lymphocytes (CTL) precursors in patients with renal cancer or affect the
anticipated response rate from high-dose IL-2.
Objectives:
The primary objective for patients with renal cell carcinoma will be to determine overall
response rates and toxicity of peptide vaccination with HLA-A2 and HLA-A3- binding peptides
from FGF-5 in HLA-appropriate patients, and to explore the effect of such vaccination on the
response rate to high-dose IL-2. The primary objective for patients who are receiving
vaccination in the adjuvant setting will be to evaluate the immunologic responses and
toxicity of FGF-5 peptide vaccination who are likely to receive repeat vaccination prior to
requiring IL-2. The secondary objective is to evaluate the immunologic responses to FGF-5
peptide vaccination.
Eligibility:
Patients who are HLA-A2+ or HLA-A3+, must be age greater than or equal to 16, and have an
expected survival greater than three months. For cohort A and B, patients must have
measurable metastatic renal cancer and FGF-5 tumor expression. For cohort C, patients are
required to have had a Stage III primary tumor (i.e. T3/T4 or N1/N2) excised within the last
6 months.) Patients in cohorts A and B must have tumor sites safely accessible for biopsy or
indications for resection of a site of tumor (e.g. an indicated nephrectomy or symptomatic
metastasis) and be willing to undergo biopsy, and have FGF-5 expression determined by
reverse transcription polymerase chain reaction (RT-PCR) and will only be eligible if it is
detectable. Patients must meet specific safety laboratory criteria. May not have undergone
other systemic therapies for their cancer in the past 3 weeks (6 weeks for nitrosureas), not
have any major medical illnesses, or require systemic steroid therapy.
Design:
Patients will first be divided into cohorts with measurable metastatic disease (Cohorts A
and B) or high-risk loco-regional disease (Cohort C). Patients with measurable metastatic
disease will then be separated into those who require immediate IL-2 therapy (Cohort B) or
those who do not (cohort A).
Cohort A will begin receiving vaccination with HLA-appropriate peptide emulsified in
Montanide ISA-51 or Montanide® (Registered Trademark) ISA 51 VG daily for four days every 3
weeks and will continue this for up to a year, or until tumor progression is documented. At
that point, those ineligible for high-dose IL-2 or who have had previous IL-2 as an
inpatient (considered high dose at doses greater than or equal to 600,000 IU/kg) will be
taken off of study, and those still eligible for IL-2 who have not yet received it, will
have high-dose intravenous bolus IL-2 (720,000 IU/kg/dose every 8 hours up to 12 doses)
added to their peptide vaccination regimen. Two cycles, separated by 10-14 days, will be
given during every two-month period (constitutes a course.). Patients in Cohort A crossing
over to vaccination plus IL-2 therapy, will receive peptide in MONTANIDE ISA-51 or
Montanide® (Registered Trademark) ISA 51 VG vaccination the day prior to starting an IL-2
cycle (instead of every 3 weeks, to accommodate the IL-2 regimen) and repeated daily for
three additional days (for a total of four days) during IL-2 administration.
Patients in Cohort B will begin with high-dose bolus IL-2 therapy in two cycles within every
two month period, with each cycle preceded by a peptide in MONTANIDE ISA-51 or Montanide®
(Registered Trademark) ISA 51 VG vaccine the day prior to starting each IL-2 cycle with
peptide in MONTANIDE ISA-51 or Montanide® (Registered Trademark) ISA 51 VG repeated daily
for three additional days (for a total of four days) during IL-2 administration.
Patients in Cohort C will undergo the same HLA-appropriate vaccination with peptide and
MONTANIDE ISA-51 or Montanide® (Registered Trademark) ISA 51 VG daily for four days every 3
weeks and continue for up to 6 months or until disease relapse is documented. At the time of
relapse, eligible patients in Cohort C will receive treatment with high-dose bolus IL-2 and
continuing peptide vaccination using the same schedule as specified for the Cohort A
crossover arm above.
For patients in cohort A on peptide vaccine alone, evaluation will be performed every 3
months during the first 6 months of therapy and if stable, every 3-6 months thereafter. For
cohorts A and B during peptide vaccine plus high-dose IL-2 therapy, evaluation will be
performed every 2 months while on IL-2, and every 3-6 months for stable patients off
therapy. For cohort C, evaluations will be performed every 3 months for the first year and
every 6-12 months thereafter.
The maximal accrual possible would be 210 patients (Cohort A with 80 patients, Cohort B with
66 patients and Cohort C with 64 patients), and maximal enrollment could take up to 5 years.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Crossover Assignment, Masking: Open Label, Primary Purpose: Treatment
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