The intrinsic resistance of uveal melanoma to conventional systemic therapies has made the treatment of metastatic uveal melanoma a tough challenge. The development of uveal melanoma at an immune-privileged
site, the eye, made it questionable if immunotherapy would be a suitable treatment method. The lack of proper immune surveillance in the eye can lead to characteristics that make tumor cells more susceptible for recognition by the immune system when cells disseminate systemically, for example, high expression of tumor-specific antigens, as well as less susceptible, for example, resistance to interferon-γ–induced upregulation of major histocompatibility complex selleck class II molecules.36, 37 and 38 At present, accumulating evidence shows that uveal melanoma tumor cells can be lysed by CD8+ T cells in vitro39 and by T cells adoptively transferred in a mouse model,40 indicating the susceptibility of uveal melanoma for immunotherapy. In our study, we vaccinated metastatic uveal melanoma patients with inhibitors autologous, mature dendritic cells to induce or strengthen a tumor-specific immune response. First, we showed that dendritic cell vaccination in metastatic uveal melanoma
is feasible and safe, as shown in more than 200 patients with cutaneous melanoma. Second, the control antigen-specific T-cell proliferation indicated that the vaccine effectively induced de novo immune responses selleck products in all patients. Tumor-specific CD8+ T cells were detected in 29% of patients in peripheral blood or in through antigen-challenged skin sites. Our previous findings in metastatic melanoma patients, of which most had cutaneous melanoma, showed a similar immunologic response rate (32%) and demonstrated that the presence of tumor-specific T cells after dendritic cell vaccination correlates with clinical outcome.28 The cohort is too small to confirm these data in metastatic
uveal melanoma patients. Obviously, our study has several limitations. First, this study consists of a small cohort, mainly because of rarity of the tumor and selection on HLA-A*02:01 phenotype in most protocols (approximately 50% of the white population).41 The latter was necessary because the selected peptides only bind HLA-A*02:01. We do not expect that this has influenced our results, because HLA-A*02:01 phenotype has shown no correlation with survival.42 Other factors were more likely to be of influence on overall survival, for example, excluding patients with World Health Organization performance status of 2 or more. However, patients were not excluded based on anatomic site of metastasis, number of metastases, or metastatic-free interval, all known to be prognostic factors in metastatic uveal melanoma.
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