Massive expansion of regulatory T-cells following interleukin 2 treatment during a phase I-II dendritic cell-based immunotherapy of metastatic renal cancer

François M. Lemoine, Mustapha Cherai, Camille Giverne, Dalia Dimitri, Michelle Rosenzwajg, Helene Trebeden-Negre, Nathalie Chaput, Benoit Barrou, Nicolas Thioun, Bernard Gattegnio, Frederic Selles, Alain Six, Nabih Azar, Jean Pierre Lotz, Agnes Buzyn, Mathilde Sibony, Annick Delcourt, Olivier Boyer, Serge Herson, David KlatzmannRoger Lacave

Résultats de recherche: Contribution à un journalArticleRevue par des pairs

45 Citations (Scopus)

Résumé

Cytotoxic chemotherapy is ineffective in metastatic renal cancer. However, systemic administration of interleukin 2 (IL-2) or infusion of dendritic cells (DCs) loaded with tumor extracts can lead to some response rates with concomitant survival improvements. We report the results of a phase I-II pilot study combining DCs and IL-2 where six patients were included. DCs were derived from bone marrow CD34+ cells and loaded with autologous tumor extracts. CD34-DC vaccines were infused subcutaneously at day 45, 52, 59, 90 and 120 following surgery in combination with IL-2, that was subsequently administrated after the 3rd and 4th DC vaccinations. Preparation of tumor extracts and CD34-DCs were satisfactory in all patients but one. Due to rapid tumor progression, one patient was excluded before vaccination. In the 4 remaining patients, two received 3 vaccinations, while the 2 others received 5 vaccinations and the full IL-2 treatment. No adverse effect due to the vaccinations was observed. A specific immune response against autologous tumor cells was observed in the 2 patients who completed the treatment. Interestingly, these 2 patients had a more prolonged survival than the patients receiving 3 vaccinations. Importantly, a transient and massive increase of circulating natural regulatory T-cells (nTregs) was evidenced in 3 patients following IL-2 administration. Overall, the use of CD34-DC vaccines is feasible, safe and non-toxic. A specific antitumor immune response can be detected. However, our data highlights that IL-2 is a potent inducer of nTregs in vivo and as such may have a negative impact on cancer immunotherapy.

langue originaleAnglais
Pages (de - à)569-581
Nombre de pages13
journalInternational Journal of Oncology
Volume35
Numéro de publication3
Les DOIs
étatPublié - 21 sept. 2009
Modification externeOui

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