RTA 408 Capsules in Patients With Melanoma - REVEAL
Status: | Completed |
---|---|
Conditions: | Skin Cancer |
Therapuetic Areas: | Oncology |
Healthy: | No |
Age Range: | 18 - Any |
Updated: | 9/8/2018 |
Start Date: | October 2014 |
End Date: | July 23, 2018 |
An Open-label, Multicenter, Dose-escalation, Phase 1b/2 Study of the Safety, Efficacy, Pharmacodynamics, and Pharmacokinetics of RTA 408 in Combination With Ipilimumab or Nivolumab in the Treatment of Patients With Unresectable or Metastatic Melanoma
Malignant melanoma is a leading cause of death from cutaneous malignancies, accounting for
approximately three-fourths of all skin cancer deaths. For metastatic or unresectable
melanomas, standard treatment options include immune checkpoint inhibitors (e.g., ipilimumab
and nivolumab) and other therapies, however, approved therapies are rarely curative.
It is now well accepted that tumors are able to evade detection and eradication by the immune
system, even though many tumor types, particularly melanoma, are capable of eliciting a
strong immune response (Swann, 2007). Substantial mechanistic work in recent years has
revealed the key role of myeloid-derived suppressor cells (MDSCs) in masking cancer cells
from the immune system, promoting both tumor progression and resistance to cancer
immunotherapy. The immune-suppressive effect of MDSCs is dependent on the production of
reactive oxygen species (ROS) and reactive nitrogen species (RNS). High levels of these
reactive molecules and their by-products, such as nitrotyrosine, have been correlated with
poor clinical outcomes in melanoma. Currently available melanoma therapies do not target
MDSCs.
In animals, RTA 408 significantly reduces tumor nitrotyrosine burden, inhibits the activity
of MDSCs, and augments T-cell anticancer activity at relevant doses. Thus, through inhibition
of MDSC activity and suppression of tumor ROS/RNS, RTA 408 may work in combination with
T-cell-activating therapeutics such as ipilimumab to enhance the natural immune anticancer
response. RTA 408 also has direct anticancer effects via inhibition of NF-kappa B. Chronic
activation of NF-kappa B is associated with tumor progression, metastasis, and resistance to
therapy.
This proposed study is designed to assess the safety, efficacy, pharmacodynamics, and
pharmacokinetics of omaveloxolone (RTA 408) in combination with ipilimumab or nivolumab in
patients with unresectable or metastatic melanoma.
In this open-label, multicenter, dose-escalation, Phase 1b/2 study, patients who qualify will
receive omaveloxolone (RTA 408) at the assigned dose level in combination with ipilimumab or
nivolumab. Patients will receive omaveloxolone (RTA 408) orally once daily for 1 week prior
to initiation of ipilimumab or nivolumab. For patients treated with ipilimumab , the run-in
period will be followed by omaveloxolone (RTA 408) orally once daily in combination with
ipilimumab administered at Weeks 1, 4, 7, and 10. After Week 10, patients will receive
maintenance treatment with omaveloxolone (RTA 408) alone once daily. For patients treated
with nivolumab, the run-in period will be followed by omaveloxolone (RTA 408) orally once
daily in combination with nivolumab administered approximately every two weeks as clinically
indicated. Each patient will continue at the assigned omaveloxolone (RTA 408) dose level
until disease progression occurs, toxicity requiring discontinuation from study drug (i.e.,
RTA 408) is experienced, the patient has completed approximately 72 weeks of treatment, the
patient is discontinued from the study drug for another reason, or the patient withdraws
consent. Patients will return 4 weeks after omaveloxolone (RTA 408) treatment completion for
a follow-up visit.
The starting omaveloxolone (RTA 408) dose level for the first dose-escalation cohort in this
study has been selected based on available safety and pharmacodynamic data from a Phase 1
study of RTA 408 (NCT02029729). Subsequent cohorts will be enrolled at dose levels based on
available safety and PD data from this study, but they will not be greater than 2-fold above
the prior dose level.
Phase 1b (dose-escalation): In the phase 1b/2 portion of this study, 12 patients will be
enrolled in each dose cohort, with six patients administered omaveloxolone (RTA 408) plus
ipilimumab and the remaining six administered rTA 408 plus nivolumab. Subsequent cohorts will
assess escalating the doses of omaveloxolone (RTA 408) administered in combination with
ipilimumab or nivolumab. Dose escalation decisions will be based on ongoing review of all
available safety information for enrolled patients.
Phase 2: The Phase 2 portion of the study may include separate expansion cohorts consisting
of patients treated with either of the combination therapies. Each expansion cohort will
include an additional 24 patients enrolled at the selected Phase 2 dose level to achieve a
total of 30 patients at that omaveloxolone (RTA 408) dose in combination with ipilimumab or
nivolumab.
approximately three-fourths of all skin cancer deaths. For metastatic or unresectable
melanomas, standard treatment options include immune checkpoint inhibitors (e.g., ipilimumab
and nivolumab) and other therapies, however, approved therapies are rarely curative.
It is now well accepted that tumors are able to evade detection and eradication by the immune
system, even though many tumor types, particularly melanoma, are capable of eliciting a
strong immune response (Swann, 2007). Substantial mechanistic work in recent years has
revealed the key role of myeloid-derived suppressor cells (MDSCs) in masking cancer cells
from the immune system, promoting both tumor progression and resistance to cancer
immunotherapy. The immune-suppressive effect of MDSCs is dependent on the production of
reactive oxygen species (ROS) and reactive nitrogen species (RNS). High levels of these
reactive molecules and their by-products, such as nitrotyrosine, have been correlated with
poor clinical outcomes in melanoma. Currently available melanoma therapies do not target
MDSCs.
In animals, RTA 408 significantly reduces tumor nitrotyrosine burden, inhibits the activity
of MDSCs, and augments T-cell anticancer activity at relevant doses. Thus, through inhibition
of MDSC activity and suppression of tumor ROS/RNS, RTA 408 may work in combination with
T-cell-activating therapeutics such as ipilimumab to enhance the natural immune anticancer
response. RTA 408 also has direct anticancer effects via inhibition of NF-kappa B. Chronic
activation of NF-kappa B is associated with tumor progression, metastasis, and resistance to
therapy.
This proposed study is designed to assess the safety, efficacy, pharmacodynamics, and
pharmacokinetics of omaveloxolone (RTA 408) in combination with ipilimumab or nivolumab in
patients with unresectable or metastatic melanoma.
In this open-label, multicenter, dose-escalation, Phase 1b/2 study, patients who qualify will
receive omaveloxolone (RTA 408) at the assigned dose level in combination with ipilimumab or
nivolumab. Patients will receive omaveloxolone (RTA 408) orally once daily for 1 week prior
to initiation of ipilimumab or nivolumab. For patients treated with ipilimumab , the run-in
period will be followed by omaveloxolone (RTA 408) orally once daily in combination with
ipilimumab administered at Weeks 1, 4, 7, and 10. After Week 10, patients will receive
maintenance treatment with omaveloxolone (RTA 408) alone once daily. For patients treated
with nivolumab, the run-in period will be followed by omaveloxolone (RTA 408) orally once
daily in combination with nivolumab administered approximately every two weeks as clinically
indicated. Each patient will continue at the assigned omaveloxolone (RTA 408) dose level
until disease progression occurs, toxicity requiring discontinuation from study drug (i.e.,
RTA 408) is experienced, the patient has completed approximately 72 weeks of treatment, the
patient is discontinued from the study drug for another reason, or the patient withdraws
consent. Patients will return 4 weeks after omaveloxolone (RTA 408) treatment completion for
a follow-up visit.
The starting omaveloxolone (RTA 408) dose level for the first dose-escalation cohort in this
study has been selected based on available safety and pharmacodynamic data from a Phase 1
study of RTA 408 (NCT02029729). Subsequent cohorts will be enrolled at dose levels based on
available safety and PD data from this study, but they will not be greater than 2-fold above
the prior dose level.
Phase 1b (dose-escalation): In the phase 1b/2 portion of this study, 12 patients will be
enrolled in each dose cohort, with six patients administered omaveloxolone (RTA 408) plus
ipilimumab and the remaining six administered rTA 408 plus nivolumab. Subsequent cohorts will
assess escalating the doses of omaveloxolone (RTA 408) administered in combination with
ipilimumab or nivolumab. Dose escalation decisions will be based on ongoing review of all
available safety information for enrolled patients.
Phase 2: The Phase 2 portion of the study may include separate expansion cohorts consisting
of patients treated with either of the combination therapies. Each expansion cohort will
include an additional 24 patients enrolled at the selected Phase 2 dose level to achieve a
total of 30 patients at that omaveloxolone (RTA 408) dose in combination with ipilimumab or
nivolumab.
Inclusion Criteria:
1. Be ≥18 years of age;
2. Have advanced, unresectable (Stage III) or metastatic (Stage IV) melanoma;
3. Be eligible for commercial receipt of therapy to be used in this study in combination
with RTA 408 (i.e., ipilimumab or nivolumab in the Phase 1b portion and nivolumab only
in the Phase 2 portion);
4. Have discontinued previous treatments for cancer;
5. Have discontinued previous experimental therapies and checkpoint inhibitor antibodies
at least 28 days prior to the Randomization Visit
Exclusion Criteria:
1. Have received prior treatment with therapy to be used in this study in combination
with RTA 408 (i.e., ipilimumab or nivolumab) if enrolling in the Phase 2 portion of
the study. This criterion does not apply to patients enrolling in the Phase 1b portion
of the study.
2. Have prior malignancy active within the previous 2 years;
3. Have any active autoimmune disease or a history of known or suspected autoimmune
disease;
4. History of brain metastases that meet certain conditions;
5. History of specific cardiovascular abnormalities;
6. Have known active fungal, bacterial, and/or viral infection, including human
immunodeficiency virus (HIV) or hepatitis virus (A,B, or C).
We found this trial at
10
sites
Washington, District of Columbia 20007
Principal Investigator: Geoffrey Gibney, MD
Phone: 202-687-2680
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12902 USF Magnolia Dr
Tampa, Florida 33612
Tampa, Florida 33612
(888) 663-3488
Principal Investigator: Joseph Markowitz, MD
Phone: 813-745-4798
H. Lee Moffitt Cancer Center & Research Institute Moffitt Cancer Center in Tampa, Florida, has...
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13001 E. 17th Pl.
Aurora, Colorado 80045
Aurora, Colorado 80045
303-724-5000
Principal Investigator: Rene Gonzalez, MD
Phone: 720-848-7135
University of Colorado Cancer Center - Anschutz Cancer Pavilion The University of Colorado Denver |...
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450 Brookline Ave
Boston, Massachusetts 2215
Boston, Massachusetts 2215
617-632-3000
Principal Investigator: Frank Hodi, MD
Phone: 617-632-5906
Dana-Farber Cancer Institute Since it’s founding in 1947, Dana-Farber has been committed to providing adults...
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20 Duke Clinic Cir
Durham, North Carolina 27710
Durham, North Carolina 27710
(888) 275-3853
Principal Investigator: April Salama, MD
Phone: 919-684-8239
Duke Cancer Institute Leading-edge cancer care and research have been a hallmark of Duke Medicine...
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Fayetteville, Arkansas 72703
Principal Investigator: Thaddeus J Beck, MD
Phone: 479-587-1700
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Houston, Texas 77030
Principal Investigator: Sapna Patel, MD
Phone: 713-792-2921
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Mobile, Alabama 36608
Principal Investigator: Michael Meshad, MD
Phone: 251-607-5283
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Morristown, New Jersey 07960
Principal Investigator: Eric Whitman, MD
Phone: 973-971-5569
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Newark, Delaware 19713
Principal Investigator: Michael Guarino, MD
Phone: 303-623-4639
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