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Establishment of Synergistic Chemoimmunotherapy for Head and Neck Cancer Using Peritumoral Immature Dendritic Cell Injections and Low-Dose Chemotherapies
Authors:Hiroki Ishii  Kazuaki Chikamatsu  Satoshi Igarashi  Hideyuki Takahashi  Kaname Sakamoto  Hiroji Higuchi  Shota Tanaka  Tomokazu Matsuoka  Keisuke Masuyama
Institution:2. Department of Otolaryngology-Head and Neck Surgery, Gunma University Graduate School of Medicine;3. Division of Transfusion Medicine and Cell Therapy, University of Yamanashi Hospital
Abstract:The lack of available tumor antigens with strong immunogenicity, human leukocyte antigen restriction, and immunosuppression via regulatory T-cells (Tregs) and myeloid-derived suppressor cells are limitations for dendritic cell (DC)–based immunotherapy in patients with advanced head and neck cancer (HNC). We sought to overcome these limitations and induce effective antitumor immunity in the host. The effect of low-dose docetaxel (DTX) treatment on DC maturation was examined in an ex vivo study, and a phase I clinical trial of combination therapy with direct peritumoral immature DC (iDC) injection with OK-432 and low-dose cyclophosphamide (CTX) plus DTX was designed. Low-dose DTX did not negatively affect iDC viability and instead promoted maturation and IL-12 production. Five patients with metastatic or recurrent HNC were enrolled for the trial. All patients experienced grade 1 to 3 fevers. Intriguingly, elevated CD8+ effector T-cells and reduced Tregs were observed in four patients who completed two treatment cycles. All patients were judged to have progressive disease, but tumor regressions were observed in a subset of targeted metastatic lesions in two of five patients. Our results show that the combination of direct peritumoral iDC injection with OK-432 and low-dose CTX plus DTX is well tolerated and should give rise to changing the immune profile of T-cell subsets and improvement of immunosuppression in advanced HNC patients. Additionally, our ex vivo data on the effect of low-dose DTX treatment on DC maturation may contribute to developing new combination therapies with low-dose chemotherapy and immunotherapy.
Keywords:Address all correspondence to: Hiroki Ishii or Keisuke Masuyama  Department of Otolaryngology  Head and Neck Surgery  University of Yamanashi  1110 Shimokato  Chuo-City  Yamanashi  409-3898  Japan  
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