Phase I/II Study of Peptide Vaccination Associated With GM-CT-01, a Galactomannan Oligomer That Inhibits Galectin-3, in Patients With Advanced Metastatic Melanoma

Cliniques universitaires Saint-Luc- Université Catholique de Louvain1 site in 1 country6 target enrollmentApril 2012

ConditionsMetastatic Melanoma

Overview

Phase: Phase 1
Intervention: Not specified
Conditions: Metastatic Melanoma
Sponsor: Cliniques universitaires Saint-Luc- Université Catholique de Louvain
Enrollment: 6
Locations: 1
Primary Endpoint: Response rate in both arms
Status: Terminated
Last Updated: 7 years ago

Overview Investigators Eligibility Criteria Outcomes Sites Similar Trials

Overview

Brief Summary

The purpose of this study is to determine whether the intravenous and/or GM-CT-01 administration can correct Tumor Infiltrating Lymphocytes (TIL) anergy and induce a more efficient and long-lasting anti-tumoral immune response following peptide vaccination.

Detailed Description

Human cancers express tumor antigens that can be targeted by cytolytic T lymphocytes (CTL). These antigens consist of a small peptide, derived from endogenous proteins, that is presented at the cancer cell's surface by an HLA class I molecule. Such antigenic peptides, including MAGE-3.A1 and NA17.A2, have been tested in experimental therapeutic vaccines to elicit CTL responses in cancer patients, mainly with metastatic melanoma. Up to now, only rare tumor responses have been observed. Tumor resistance to CTL killing is the most likely explanation for the poor effectiveness of cancer vaccines. This resistance is probably acquired by the tumor during its development and selected by its repetitive challenge with spontaneous anti-tumoral immune responses. Recently, we have identified a novel mechanism causing anergy of tumor-associated T lymphocytes, and established new approaches to correct this anergy in vitro. Galectin-3, secreted by tumor cells, appears to inhibit CTL function the co-localization of the T cell receptor and the cluster of differentiation 8 coreceptor. Importantly, this functional defect is restored when anergic T cells are incubated with galectin-3 inhibitors such as the disaccharides lactose and N-acetyllactosamine, and the polysaccharide GM-CT-01. GM-CT-01 is a vegetal galactomannan oligomer, currently under clinical investigation in several types of solid malignancies for its capacity to inhibit galectins and to synergize with chemotherapy drugs. Our observations suggest that treatment of cancer patients with GM-CT-01 could correct TIL anergy and induce a more efficient and long-lasting anti-tumoral immune response following peptide vaccination.

Registry

clinicaltrials.gov

Start Date

April 2012

End Date

April 1, 2015

Last Updated

7 years ago

Study Type

Interventional

Study Design

Parallel

Sex

All

Investigators

Sponsor

Cliniques universitaires Saint-Luc- Université Catholique de Louvain

Responsible Party

Sponsor

Eligibility Criteria

Inclusion Criteria

•Patients with histologically proven cutaneous melanoma at one of the following American Joint Committee on Cancer stages : Regional metastatic disease (any T; N2c or N3; M0), no amenable to curative treatment by surgery or isolated limb perfusion.Distant metastatic disease (any T; any N; M1a, M1b or M1c\*).\*except uncontrolled brain metastasis and except Lactate dehydrogenase \>1.5 upper normal value
•HLA-A1 or HLA-A2 (by serology or molecular biology)
•At least one of the two following conditions:
•MAGE-3 gene expression by the tumor if patient is HLA-A1 NA17 gene expression by the tumor if patient is HLA-A2 (determined by reverse transcription and polymerase chain reaction amplification).
•Measurable Disease. Patients must have at least 1 measurable metastasis at study entry for all patients. In addition, patients candidates for enrollment in Group 2 who will receive peri-tumoral injections of GM-CT-01 must have at least 1 superficial metastasis (cutaneous, subcutaneous or superficial lymph node metastasis, with its largest diameter equal to or greater than 5, 5, or 10 mm, respectively) at study entry.
•Age ≥ 18 years.
•Karnofsky Performance status ≥70 or WHO performance status of 0 or 1
•Expected survival of at least 6 months.
•Laboratory values :
•Platelet count ≥100x103/μL Leukocyte count ≥ 3x103/μL Hemoglobin ≥ 9 g/dL Aspartate transaminase and Alanine transaminase ≤ 2 times upper normal value Serum creatinine ≤1.5 times upper normal value Total bilirubin ≤ 1.5 times upper normal value Lactate dehydrogenase ≤ 1.5 times upper normal value

Exclusion Criteria

•Uncontrolled brain or central nervous system metastasis.
•Previous treatment for the melanoma within 6 weeks from inclusion, with any reagent known to modulate the immune system such as a cancer vaccine, interferon-alpha, interleukins or anti-CTLA-4 antibodies.
•Previous chemotherapy, radiotherapy, corticotherapy, or other immune suppressive therapy within 4 weeks from inclusion.
•Clinically significant cardiovascular disease (including cardiac insufficiency New York Heart Association grade III and IV, unstable angina, arrythmia, myocardial infarction, symptomatic congestive heart failure) in the past 12 months before enrollment.
•Other serious acute or chronic illnesses, e.g. active infections requiring antibiotics, bleeding disorders or other conditions requiring concurrent medications not allowed during this study.
•Other malignancy within 3 years prior to entry in the study, except for treated non-melanoma skin cancer and in situ cervical carcinoma.
•Active immunodeficiency disease or autoimmune disease (vitiligo is not an exclusion criterion).
•Lack of availability for immunological and clinical follow-up assessments.
•Participation in any other clinical trial involving another investigational agent within 4 weeks prior to enrollment.
•Subject pregnant or breastfeeding, or planning to become pregnant within 6 months after the end of treatment.

Outcomes

Primary Outcomes

Response rate in both arms

Time Frame: Change from baseline at week 7 and week 20

Efficacy of the combination of a peptide vaccine and GM-CT-01 injections measures performed by CT-scan or MRI

Number of participants with adverse events

Time Frame: 30 days after last administration of Study drugs

Change from baseline in adverse events will be recorded at each patient's visit and up to 30 days after last administration of study drugs. Measurements will use the Common Toxicity Criteria for Adverse Effects 4,0 scale

Secondary Outcomes

Time to Progression(From date of inclusion until the date of first documented progression or date of death from any cause, which ever came first, assessed up to 100 weeks)
Immunogenicity of the treatment(Change from baseline at week 20)
Response rate in group 2 versus group 1(Change from baseline at week 7 and week 20)
Overall Survival(From day of inclusion to date of death)