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Allogeneic partially HLA-matched dendritic cells pulsed with autologous tumor cell lysate as a vaccine in metastatic renal cell cancer: a clinical phase I/II study. | LitMetric

AI Article Synopsis

  • Multi-kinase inhibitors have shown limited long-term success in treating advanced renal cell cancer (RCC), prompting interest in immunotherapeutic methods, especially for patients with low tumor burden.
  • A phase I/II trial involving 7 patients tested the safety and feasibility of a vaccine using allogeneic dendritic cells (DC) pulsed with patients' own tumor lysates, which was administered in 8 doses over 20 weeks, alongside daily interleukin-2 (IL-2) injections.
  • While no significant tumor response was noted, 29% of patients experienced stable disease for an average of 24.6 weeks, with some exhibiting immune responses to RCC-specific antigens, indicating potential for further research in patient

Article Abstract

Multi-kinase inhibitors have been established for the treatment of advanced renal cell cancer, but long-term results are still disappointing and immunotherapeutic approaches remain an interesting experimental option particularly in patients with a low tumor burden. DC are crucial for antigen-specific MHC-restricted T cell immunity. Furthermore, allogeneic HLA-molecules pose a strong immunogenic signal and may help to induce tumor-specific T cell responses. In this phase I/II trial, 7 patients with histologically confirmed progressive metastatic RCC were immunized repetitively with 1 × 10 (7) allogeneic partially HLA-matched DC pulsed with autologous tumor lysate following a schedule of 8 vaccinations over 20 weeks. Patients also received 3 Mio IE IL-2 s.c. once daily starting in week 4. Primary endpoints of the study were feasibility and safety. Secondary endpoints were immunological and clinical responses. Vaccination was feasible and safe with no severe toxicity being observed. No objective response could be documented. However, while all patients had documented progress at study entry, 29% of the patients showed SD throughout the study with a mean TTP of 24.6 weeks (range 5 to 96 weeks). In 3/7 patients, TH1-polarized immune responses against RCC-associated antigens were observed. In one patient showing a minimal clinical response and a TTP of 96 weeks, clonally proliferated T cells against yet undefined antigens were induced by the vaccine. Vaccination with tumor antigen loaded DC remains an interesting experimental approach, but should rather be applied in the situation of minimal residual disease after systemic therapy. Additional depletion of regulatory cells might be a promising strategy.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3901809PMC
http://dx.doi.org/10.4161/hv.24149DOI Listing

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