Tumor-specific delivery of biologics by a novel T-cell line HOZOT

被引:0
作者
Teppei Onishi
Hiroshi Tazawa
Yuuri Hashimoto
Makoto Takeuchi
Takeshi Otani
Shuji Nakamura
Fuminori Sakurai
Hiroyuki Mizuguchi
Hiroyuki Kishimoto
Yuzo Umeda
Yasuhiro Shirakawa
Yasuo Urata
Shunsuke Kagawa
Toshiyoshi Fujiwara
机构
[1] Okayama University Graduate School of Medicine,Department of Gastroenterological Surgery
[2] Dentistry and Pharmaceutical Sciences,undefined
[3] Center for Innovative Clinical Medicine,undefined
[4] Okayama University Hospital,undefined
[5] R&D Center,undefined
[6] Hayashibara Co.,undefined
[7] Ltd.,undefined
[8] Laboratory of Biochemistry and Molecular Biology,undefined
[9] Graduate School of Pharmaceutical Sciences,undefined
[10] Osaka University,undefined
[11] Oncolys BioPharma,undefined
[12] Inc.,undefined
来源
Scientific Reports | / 6卷
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摘要
“Cell-in-cell” denotes an invasive phenotype in which one cell actively internalizes in another. The novel human T-cell line HOZOT, established from human umbilical cord blood, was shown to penetrate a variety of human cancer cells but not normal cells. Oncolytic viruses are emerging as biological therapies for human cancers; however, efficient viral delivery is limited by a lack of tumor-specific homing and presence of pre-existing or therapy-induced neutralizing antibodies. Here, we report a new, intriguing approach using HOZOT cells to transmit biologics such as oncolytic viruses into human cancer cells by cell-in-cell invasion. HOZOT cells were successfully loaded via human CD46 antigen with an attenuated adenovirus containing the fiber protein of adenovirus serotype 35 (OBP-401/F35), in which the telomerase promoter regulates viral replication. OBP-401/F35–loaded HOZOT cells were efficiently internalized into human cancer cells and exhibited tumor-specific killing by release of viruses, even in the presence of anti-viral neutralizing antibodies. Moreover, intraperitoneal administration of HOZOT cells loaded with OBP-401/F35 significantly suppressed peritoneally disseminated tumor growth in mice. This unique cell-in-cell property provides a platform for selective delivery of biologics into human cancer cells, which has important implications for the treatment of human cancers.
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