Clinical Trial of the Intratumoral Administration of Labeled DC Combined With Systemic Chemotherapy for Esophageal Cancer

化学免疫疗法 医学 锁孔血蓝蛋白 化疗 食管癌 淋巴 免疫系统 全身给药 抗原 免疫疗法 抗体 癌症 淋巴结 病理 免疫学 体内 内科学 生物 生物技术
作者
Shigehiro Fujiwara,Hisashi Wada,Hiroshi Miyata,Junji Kawada,Ryohei Kawabata,Hiroyoshi Nishikawa,Sacha Gnjatic,Christine Sedrak,Eiichi Sato,Yurika Nakamura,Mitsuru Sakakibara,Tatsuya Kanto,Eku Shimosegawa,Jun Hatazawa,Tsuyoshi Takahashi,Yukinori Kurokawa,Makoto Yamasaki,Kiyokazu Nakajima,Shuji Takiguchi,Eiichi Nakayama,Masaki Mori,Yuichiro� Doki
出处
期刊:Journal of Immunotherapy [Ovid Technologies (Wolters Kluwer)]
卷期号:35 (6): 513-521 被引量:44
标识
DOI:10.1097/cji.0b013e3182619cb4
摘要

Esophageal cancer is a highly aggressive disease, and improved modalities for its treatment are needed. We performed chemoimmunotherapy involving the intratumoral administration of 111In-labeled dendritic cells (DC) in combination with preoperative chemotherapy in 5 esophageal cancer patients. Mature DC were generated and traced by scintigraphy after their administration. No adverse events that were directly related to the intratumoral DC administration were observed. Delayed-type hypersensitivity skin tests against keyhole limpet hemocyanin, which was added to the culture medium, detected a positive response in 3 patients, and keyhole limpet hemocyanin antibody production was observed in 4 patients, suggesting that intratumorally administered DC migrate to the lymph nodes, where they function as antigen-presenting cells. However, scintigraphic images obtained after the DC administration demonstrated that the DC remained at the esophageal tumor injection sites in all cases, and no DC accumulation was observed elsewhere. The accumulation of CD83+ cells in the primary tumor was also observed in 2 out of 4 patients in an immunohistochemical analysis using surgically resected specimens. Although the induction of tumor-specific immune responses during chemoimmunotherapy was also analyzed in enzyme-linked immunosorbent assay against 28 tumor antigens, none of the antibodies against the antigens displayed enhanced titers. No changes of NY-ESO-1-specific cellular immune response was observed in a patient who displayed NY-ESO-1 antibody production before the DC administration. These results suggest that the intratumoral administration of 111In-labeled mature DC during chemotherapy does not lead to detectable DC migration from the primary tumor to the draining lymph nodes, and therefore, might not achieve an optimal clinical response.

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