Melanoma Clinical Trial
— ABCOfficial title:
A Phase II Study of Nivolumab and Nivolumab Combined With Ipilimumab in Patients With Melanoma Brain Metastases
Verified date | March 2024 |
Source | Melanoma Institute Australia |
Contact | n/a |
Is FDA regulated | No |
Health authority | |
Study type | Interventional |
The purpose of this research project is to test the effectiveness of nivolumab versus nivolumab together with ipilimumab for the treatment of melanoma brain metastases. Patients are eligible to join this study if they are aged 18 years or above and have been diagnosed with melanoma with brain metastases.
Status | Active, not recruiting |
Enrollment | 76 |
Est. completion date | December 2028 |
Est. primary completion date | September 4, 2017 |
Accepts healthy volunteers | No |
Gender | All |
Age group | 18 Years and older |
Eligibility | Cohort 1 and 3 Inclusion Criteria: 1. =18 years of age. 2. Written informed consent 3. AJCC Stage IV (any T, any N, M1c) histologically confirmed melanoma or unknown primary melanoma. Patients must have at least 1 radiological definitive brain metastasis that is = 5mm and =40mm measurable per RECIST version 1.1 guidelines. 4. In patients with prior BRAF inhibitor treatment, intracranial disease progression must be demonstrated (RECIST >20% or new measurable brain metastases) compared with nadir of intracranial response during BRAF inhibitor treatment, and confirmed with a second MRI brain scan at any time from the beginning of the drug washout period (dabrafenib=5 days, trametinib=14 days). 5. No prior localised treatment for brain metastases (eg. surgery or radiotherapy). 6. Neurologically asymptomatic from brain metastases. 7. Eastern Cooperative Oncology Group (ECOG) Performance Status of 0-2, and life expectancy > 30 days. 8. Able to undergo MRI with Gadolinium contrast agent. 9. Adequate haematological, hepatic and renal organ function. 10. Women of childbearing potential: negative serum pregnancy test and effective contraception from 14 days prior to study treatment until 23 weeks after the last dose. 11. Men with female partner of childbearing potential to use effective contraception from 14 days prior to study treatment until 31 weeks after the last dose. Exclusion Criteria: 12. Any melanoma brain metastasis >40mm. 13. Ocular melanoma. 14. Prior treatment with an anti-PD-1 or anti-PD-L1 , anti-PD-L2, anti-CD137, or anti-CTLA-4 antibody, or any other antibody or drug specifically targeting T-cell co-stimulation or checkpoint pathways. 15. Patients with active, known or suspected autoimmune disease. Patients with vitiligo, type I diabetes mellitus, residual hypothyroidism due to autoimmune condition only requiring hormone replacement, psoriasis not requiring systemic treatment, or conditions not expected to recur in the absence of an external trigger are permitted to enroll. 16. Current systemic treatment with corticosteroids, except prednisone at nonimmunosuppressive doses of = 10 mg/day (or equivalent). Past treatment for non-neurological symptoms allowed, if ceased 2 weeks prior to starting study treatment. Inhaled or intranasal corticosteroids (with minimal systemic absorption) may be continued if patient on a stable dose. Non-absorbed intraarticular steroid injections will be permitted. 17. Any investigational drug or other systemic drug therapy for melanoma within 28 days or 5 half-lives from baseline. 18. Known to be HIV positive, or a positive test for hepatitis B and C . 19. Another malignancy or concurrent malignancy unless disease-free for 3 years. 20. Serious or unstable pre-existing medical conditions or other conditions that could interfere with the patient's safety, consent, or compliance. 21. Pregnant or breastfeeding females. 22. Administration of any form of live vaccination (such as influenza vaccine) within 30 days of starting trial and anticipated use during the trial. Administration of any other vaccine is cautionary within 30 days of starting the trial and during the trial. Cohort 2 - per Cohorts 1 & 3, except patients must have at least one of the following: 1. Failed prior local therapy for brain metastases (including surgery, stereotactic radiotherapy or whole brain radiotherapy) where disease has progressed per RECIST (>20% increase in SOD or new measurable brain metastases), and/or; 2. Have current neurological symptoms related to brain metastases. IF they have received prior local therapy for brain metastases, the disease must have progressed per RECIST (>20% increase in SOD or new measurable brain metastases), and/or; 3. Have leptomeningeal disease concurrently with measurable brain metastases. IF they have had failed prior local therapy for brain metastases, this must have progressed per RECIST (>20% increase in SOD or new measurable brain metastases). |
Country | Name | City | State |
---|---|---|---|
Australia | Royal Adelaide Hospital | Adelaide | South Australia |
Australia | Peter MacCallum Cancer Centre | East Melbourne | Victoria |
Australia | Melanoma Institute Australia | North Sydney | New South Wales |
Australia | Princess Alexandra Hospital | Woolloongabba | Queensland |
Lead Sponsor | Collaborator |
---|---|
Melanoma Institute Australia | Bristol-Myers Squibb, Melanoma and Skin Cancer Trials Limited |
Australia,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Intracranial response rate | Proportion of patients with a complete or partial response in intracranial metastases as measured using RECIST 1.1 criteria (modified for brain metastases - bm RECIST), from week 12. | Approximately 3 years | |
Secondary | Extracranial response rate | Proportion of patients with an overall complete or partial response in extra cranial metastases as measured using bm RECIST. | Approximately 3 years | |
Secondary | Overall response rate | Proportion of patients with an overall complete or partial response as measured using bm RECIST 1.1 criteria. | Approximately 3 years | |
Secondary | Progression free survival in intracranial disease | Time from the baseline assessment to the date of intracranial progression as measured using bm RECIST 1.1 criteria. | Approximately 3 years | |
Secondary | Progression free survival in extracranial disease | Time from the baseline assessment to the date of extracranial progression as measured using bm RECIST 1.1 criteria. | Approximately 3 years | |
Secondary | Overall progression free survival | Time from the baseline assessment to the date of local or distant progression as measured using bm RECIST 1.1 criteria. Patients dying from causes other than melanoma or treatment related toxicity will be censored at date of death. Patients alive without progression or with second primary cancers will be censored at date of last assessment. | Approximately 3 years | |
Secondary | Overall survival | Time from commencing study treatment to the date of death from any cause. Patient still alive will be censored at the date of last assessment. | Up to approximately 5 years | |
Secondary | Safety and tolerability of nivolumab and nivolumab + ipilimumab (verse events by type, frequency and severity using National Cancer Institute Common Terminology Criteria for Adverse Events (CTCAE) version 4.03.) | Description of adverse events by type, frequency and severity using National Cancer Institute Common Terminology Criteria for Adverse Events (CTCAE) version 4.03.
Number of patients who withdraw from the study due to intolerable adverse reactions. |
Approximately 3 years | |
Secondary | Patient rated quality of life | The mean change from baseline quality of life scores at the time of clinical response, stable disease and progression in each cohort. | Approximately 3 years | |
Secondary | Clinical response using immune related response criteria (irRC) | Proportion of patients with an intracranial, extracranial and overall complete or partial response, stable disease or progression and progression free survival as measured using immune-related response criteria (irRC) and the proportion of concordant or discordant results compared with bm RECIST. | Approximately 3 years | |
Secondary | Tissue and blood biomarkers of response and progression | PD-L1 status, immune markers and genetics of response and resistance in tumour tissue at baseline and at disease progression. Lymphocyte, T cell subsets, myeloid derived suppressor cells and other biomarkers in blood at baseline, after 2 weeks on study treatment and then every 6 weeks, to examine if any specific subsets are predictive or response or progression. | Approximately 3 years | |
Secondary | FET-PET response in the brain at 6 and 12 weeks on therapy (Proportion of patients with a lower standardised uptake value from baseline in intracranial metastases, following at least ONE dose of study treatment) | Comparison of FET-PET to MRI findings. Proportion of patients with a lower standardised uptake value from baseline in intracranial metastases, following at least ONE dose of study treatment(s). | Approximately 1 year |
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