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Messenger Ribonucleic Acid (mRNA) Transfected Dendritic Cell Vaccination in High Risk Uveal Melanoma Patients

R

Radboud University Medical Center

Status and phase

Terminated
Phase 2
Phase 1

Conditions

Uveal Melanoma

Treatments

Biological: autologous dendritic cells electroporated with mRNA

Study type

Interventional

Funder types

Other

Identifiers

NCT00929019
NL22553.000.08
KUN2008-035

Details and patient eligibility

About

  1. Rationale

    Immunotherapy applying ex vivo generated and tumor antigen-loaded dendritic cells (DC) has now successfully been introduced in the clinic. A limited, but consistent, number of objective immunological and clinical responses have been observed. Most of the successful results have been observed in patients with minimal residual disease, rather than patients with advanced metastatic disease. Moreover, the investigators' preliminary results show that presence of tumor epitope specific T cells in biopsies taken from delayed type hypersensitivity (DTH) reaction sites highly correlates with prolonged progression free survival (PFS).

    Within uveal melanoma patients, a group with high risk of metastatic disease can be identified on basis of tumor specific genetic changes in loss of chromosome 3.

    At present no standard adjuvant or systemic treatment is available. Applying DC-based immunotherapy in this group of high risk patients might reduce the risk of recurrence without interference in the current treatment guidelines.

  2. Objectives

    In this joint clinical study of Radboud University Nijmegen Medical Centre (RUNMC) and Rotterdam Eye Hospital, the investigators aim to determine the in vivo immunological response induced in high risk uveal melanoma patients vaccinated with mRNA-transfected DC.

  3. Study design

    This study is an open label non-randomized phase II intervention study.

  4. Study population

    The investigators' study population consists of HLA-A2 positive patients with a high risk uveal melanoma with proven expression of melanoma associated antigens tyrosinase and/or gp100.

  5. Main study endpoints

This is an exploratory study aiming to demonstrate proof of principle. The first study endpoints are in vivo immunological response induced in high risk uveal melanoma patients vaccinated with mRNA-transfected DC, administered i.v./i.d. and toxicity. Secondary study endpoints are progression free survival, overall survival, and toxicity.

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Enrollment

23 patients

Sex

All

Ages

18 to 75 years old

Volunteers

No Healthy Volunteers

Inclusion criteria

  • histological documented uveal melanoma
  • HLA-A2.1 phenotype (intervention arm)
  • non-HLA-A2.1 phenotype (control arm)
  • melanoma expressing gp100 and/or tyrosinase
  • high risk genetic profile (loss of chromosome 3) determined by FISH
  • interval since local treatment of uveal melanoma < 12 months
  • no signs of liver metastasis determined by diagnostic CT-abdomen
  • normal serum LDH
  • no signs of cerebral metastases
  • bilirubin < 25 micromol/l
  • WHO performance scale 0-1
  • age 18-75 years
  • written informed consent
  • expected adequacy of followup
  • no pregnant or lactating women

Exclusion criteria

  • history of second malignancy, except adequately treated basal cell carcinoma
  • serious active infections
  • autoimmune disease or organ allografts
  • concomitant use of immunosuppressive drugs
  • known allergy to shell-fish

Trial design

Primary purpose

Treatment

Allocation

Non-Randomized

Interventional model

Single Group Assignment

Masking

None (Open label)

23 participants in 2 patient groups

dendritic cell vaccination
Experimental group
Description:
HLA-A2.1 positive patient will receive 3 biweekly intradermal/intravenous vaccination with autologous mRNA transfected mature dendritic cells, followed by a DTH skin test for monitoring purposes. One such cycle is repeated every 6 months if no signs of progression, up to a total of 3 cycles.
Treatment:
Biological: autologous dendritic cells electroporated with mRNA
control arm
No Intervention group
Description:
For comparison, HLA-A2.1 negative patients will be monitored for clinical response (secondary endpoint).

Trial contacts and locations

2

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Data sourced from clinicaltrials.gov

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