Ipilimumab and GMCSF Immunotherapy for Prostate Cancer
| Status: | Withdrawn |
|---|---|
| Conditions: | Prostate Cancer, Cancer |
| Therapuetic Areas: | Oncology |
| Healthy: | No |
| Age Range: | 18 - Any |
| Updated: | 4/21/2016 |
| Start Date: | June 2015 |
| End Date: | December 2018 |
Anti-CTLA4 Blockade Alone or Combined With Systemic GM-CSF for Prostate Cancer Immunotherapy
This is an open-label randomized phase II study. Patients are randomized so as to achieve
uniform patient cohorts treated on each regimen. Twenty-seven patients will be required per
treatment arm, and a total of 54 prostate cancer patients will be required to complete this
study. The study will assess for clinical activity by Prostate Specific Antigen (PSA)
response, of both single agent ipilimumab and the combination of GM-CSF and ipilimumab in
chemotherapy-naïve patients with metastatic castrate resistant prostate cancer.
uniform patient cohorts treated on each regimen. Twenty-seven patients will be required per
treatment arm, and a total of 54 prostate cancer patients will be required to complete this
study. The study will assess for clinical activity by Prostate Specific Antigen (PSA)
response, of both single agent ipilimumab and the combination of GM-CSF and ipilimumab in
chemotherapy-naïve patients with metastatic castrate resistant prostate cancer.
Ipilimumab is an antibody (proteins that can find and destroy foreign molecules such as
those on bacteria and viruses) against CTLA-4 (a molecule that controls a part of the immune
system by shutting it down). It is approved by the U.S. Food and Drug Administration (FDA)
to treat patients with late-stage melanoma, skin cancer. The use of ipilimumab in patients
with CRPC has not been approved by the FDA.
Some patients in this study will receive GM-CSF along with ipilimumab. In clinical trials,
GM-CSF has been safely given to prostate cancer patients in combination with ipilimumab.
GM-CSF is not approved by the FDA for use as treatment for prostate cancer. Studies in
patients with prostate cancer suggest that GM-CSF may activate the immune system. Since
ipilimumab can help keep the immune system from turning off and allow an immune reaction to
occur, and GM-CSF can increase the activity of the immune system, it is possible that they
may work together to increase the immune response to cancer. The use of ipilimumab in
combination with GM-CSF in patients with CRPC has not been approved by the FDA.
It is theorized that if antigen presentation could be improved, the immunostimulatory
effects of CTLA-4 blockade could be augmented with improvements in clinical response. To
that end, UCSF conducted a phase I clinical trial of ipilimumab in combination with GM-CSF,
a cytokine that has been demonstrated to enhance the functional activities of effector
cells, including dendritic cells (DC), neutrophils, and monocytes, in chemotherapy-naïve men
with CRPC (Protocol 6032).32 Exposure to GM-CSF increases class II MHC expression on
dendritic cells and is thought to lead to increased antigen presentation to T cells,
stimulating T cell responses, although this mechanism has not been confirmed. We have
extensively studied the effects of treatment demonstrating a dose-response relationship in
the activation of CD4 and CD8 T cells. Moreover, the expansion of activated (CD25+CD69+) CD4
and CD8 T cells seen with this GM-CSF/ipilimumab combination trial was higher than that seen
with GM-CSF or ipilimumab monotherapy seen in our other trials in prostate cancer patients.
We are proposing to conduct a non-comparative randomized phase II study of repetitive dosing
of ipilimumab either alone or in combination with GM-CSF in patients with metastatic CRPC.
The dosing interval for ipilimumab is based on the prior study which demonstrated drug
levels ≥ 10 mg/mL (a minimum level required for CTLA-4 blockade in pre-clinical models) for
greater than 28 days. Six doses of ipilimumab were chosen because six doses have been given
safely in other trials. Maintenance dosing every three months is empirical, but this dosing
frequency is based on discussions with Medarex, Inc. and Bristol-Meyers Squibb and is based
on reports indicating the safety and potential efficacy of this maintenance regimen.
This study will use ipilimumab given every 28 days for six cycles (induction) followed by
administration once every three months for patients who are not progressing (maintenance). A
dosage of 10 mg/kg has been chosen based on the results to date of the phase I study. GM-CSF
250 mcg/m2 SQ will be administered on days 1-14 in Cycles 1-6 and then every 3 months for 14
days beginning on the day of ipilimumab administration during the maintenance therapy phase.
those on bacteria and viruses) against CTLA-4 (a molecule that controls a part of the immune
system by shutting it down). It is approved by the U.S. Food and Drug Administration (FDA)
to treat patients with late-stage melanoma, skin cancer. The use of ipilimumab in patients
with CRPC has not been approved by the FDA.
Some patients in this study will receive GM-CSF along with ipilimumab. In clinical trials,
GM-CSF has been safely given to prostate cancer patients in combination with ipilimumab.
GM-CSF is not approved by the FDA for use as treatment for prostate cancer. Studies in
patients with prostate cancer suggest that GM-CSF may activate the immune system. Since
ipilimumab can help keep the immune system from turning off and allow an immune reaction to
occur, and GM-CSF can increase the activity of the immune system, it is possible that they
may work together to increase the immune response to cancer. The use of ipilimumab in
combination with GM-CSF in patients with CRPC has not been approved by the FDA.
It is theorized that if antigen presentation could be improved, the immunostimulatory
effects of CTLA-4 blockade could be augmented with improvements in clinical response. To
that end, UCSF conducted a phase I clinical trial of ipilimumab in combination with GM-CSF,
a cytokine that has been demonstrated to enhance the functional activities of effector
cells, including dendritic cells (DC), neutrophils, and monocytes, in chemotherapy-naïve men
with CRPC (Protocol 6032).32 Exposure to GM-CSF increases class II MHC expression on
dendritic cells and is thought to lead to increased antigen presentation to T cells,
stimulating T cell responses, although this mechanism has not been confirmed. We have
extensively studied the effects of treatment demonstrating a dose-response relationship in
the activation of CD4 and CD8 T cells. Moreover, the expansion of activated (CD25+CD69+) CD4
and CD8 T cells seen with this GM-CSF/ipilimumab combination trial was higher than that seen
with GM-CSF or ipilimumab monotherapy seen in our other trials in prostate cancer patients.
We are proposing to conduct a non-comparative randomized phase II study of repetitive dosing
of ipilimumab either alone or in combination with GM-CSF in patients with metastatic CRPC.
The dosing interval for ipilimumab is based on the prior study which demonstrated drug
levels ≥ 10 mg/mL (a minimum level required for CTLA-4 blockade in pre-clinical models) for
greater than 28 days. Six doses of ipilimumab were chosen because six doses have been given
safely in other trials. Maintenance dosing every three months is empirical, but this dosing
frequency is based on discussions with Medarex, Inc. and Bristol-Meyers Squibb and is based
on reports indicating the safety and potential efficacy of this maintenance regimen.
This study will use ipilimumab given every 28 days for six cycles (induction) followed by
administration once every three months for patients who are not progressing (maintenance). A
dosage of 10 mg/kg has been chosen based on the results to date of the phase I study. GM-CSF
250 mcg/m2 SQ will be administered on days 1-14 in Cycles 1-6 and then every 3 months for 14
days beginning on the day of ipilimumab administration during the maintenance therapy phase.
Inclusion Criteria:
1. Histologically confirmed, metastatic prostate cancer (positive bone scan and/or
measurable disease on CT scan and/or MRI of the abdomen and pelvis).
2. Progressive disease after androgen deprivation, as defined by PSA Working Group 237
and/or RECIST criteria.38 Patients must have disease progression by one or both of
the following:
- For patients with measurable disease, progression is defined as at least a 20%
increase in the sum of the longest diameter (LD) of target lesions or the
appearance of one or more new lesions, as per RECIST criteria version 1.1
- For patients with no measurable disease, a positive bone scan and elevated PSA
will be required. PSA evidence for progressive prostate cancer consists of a PSA
level of at least 2 ng/ml, which has risen on at least 2 successive occasions,
at least 1 week apart. If the confirmatory PSA (#3) value is not greater (i.e.,
#3b) than the screening PSA (#2) value, then an additional test for rising PSA
(#4) will be required to document progression
- If no prior orchiectomy has been performed, patients must remain on LHRH agonist
or antagonist therapy. Patients who are receiving an antiandrogen as part of
primary androgen ablation must demonstrate disease progression following
discontinuation of the antiandrogen, defined as two consecutive rising PSA
values, obtained at least two weeks apart, or documented osseous or soft tissue
progression. At least one of the PSA values must be obtained at least four weeks
(flutamide) or six weeks (bicalutamide or nilutamide) after discontinuation
3. Laboratory requirements:
- Absolute neutrophil count (ANC) ≥ 1500/μL
- Bilirubin < 1.5 x ULN
- Hemoglobin ≥ 8 g/dL
- PSA ≥ 2 ng/mL
- Platelets > 100,000/μL
- AST and ALT < 2.5 x ULN
- Creatinine clearance ≥ 60mL/min by the Cockcroft Gault equation Testosterone <
50 ng/dL
4. Eastern Cooperative Oncology Group (ECOG) performance status 0 - 2 and life
expectancy > 12 weeks.
5. At least 18 years of age or older.
6. Patients receiving any other hormonal therapy, including any dose of megestrol
acetate (Megace), Proscar (finasteride), any herbal product known to decrease PSA
levels (e.g. Saw Palmetto, PC-SPES), or any systemic corticosteroid, must discontinue
the agent for at least four weeks prior to study treatment. Progressive disease as
defined above must be documented after discontinuation of any hormonal therapy (with
the exception of a LHRH agonist or antagonist).
7. Prior radiation therapy must be completed > 4 weeks prior to enrollment and the
patient must be recovered from all toxicity. Prior radiopharmaceuticals (strontium,
samarium) must be completed ≥ 8 weeks prior to enrollment.
8. Because of the unknown potential risk to a gamete and/or developing embryo from this
investigational therapy, patients must agree to use adequate contraception (barrier
method for males) for the duration of study participation, and for three months after
discontinuing therapy.
Exclusion Criteria:
1. Prior chemotherapy for prostate cancer, with the exception of neoadjuvant
chemotherapy, because of the potential effect of chemotherapy on the immune system.
2. Prior investigational immunotherapy. Prior sipuleucel-T treatment is allowed but must
be completed at least 4 weeks prior to initiating treatment on this protocol.
3. Current treatment with systemic steroid therapy (inhaled/topical steroids are
acceptable). Systemic corticosteroids must be discontinued for at least 4 weeks prior
to first treatment.
4. History of autoimmune disease including, but not limited to:
- Systemic lupus erythematosis (SLE), scleroderma, CREST syndrome, rheumatoid
arthritis
- Inflammatory bowel disease, celiac disease, primary biliary cirrhosis,
autoimmune hepatitis
- Dermatomyositis, polymyositis, giant cell arteritis
- Autoimmune hemolytic anemia (AIHA), cryoglobulinemia, antiphospholipid antibody
syndrome (APLS)
- Diabetes mellitus type I, myasthenia gravis, Grave's disease
- Wegener's granulomatosis or other vasculitis
- A history of Hashimoto's thyroiditis, psoriasis, or eczema, any of which has
been inactive for at least one year, or isolated Raynaud's phenomenon is
acceptable
5. History or radiologic evidence of central nervous system metastases.
6. Medical or psychiatric illness that would preclude participation in the study or the
ability of patients to provide informed consent for themselves.
7. Cardiovascular disease that meets one of the following: congestive heart failure (New
York Heart Association Class III or IV), active angina pectoris, or recent myocardial
infarction (within the last 6 months).
8. Concurrent or prior malignancy except for the following:
- Adequately treated basal or squamous cell skin cancer
- Adequately treated stage I or II cancer from which the patient is currently in
complete remission
- Any other cancer from which the patient has been disease-free for 5 years
9. HIV or other history of immunodeficiency disorder.
10. Prisoners or subjects who are compulsorily detained (involuntarily incarcerated) for
treatment of either a psychiatric or medical (e.g. infectious) illness.
11. Any underlying medical or psychiatric condition, which in the opinion of the
investigator will make the administration of ipilimumab hazardous or obscure the
interpretation of AEs, such as a condition associated with frequent diarrhea.
12. A history of prior treatment with ipilimumab or prior CD137 agonist or CTLA 4
inhibitor or agonist.
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