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Dive into the research topics where Shinsaku Nakagawa is active.

Publication


Featured researches published by Shinsaku Nakagawa.


Gene Therapy | 2003

Dendritic cells transduced with gp100 gene by RGD fiber-mutant adenovirus vectors are highly efficacious in generating anti-B16bl6 melanoma immunity in mice

Naoki Okada; Yasushige Masunaga; Yuka Okada; Hiroyuki Mizuguchi; Sayaka Iiyama; N Mori; A Sasaki; Shinsaku Nakagawa; Tadanori Mayumi; Takao Hayakawa; Takuya Fujita; Akira Yamamoto

Dendritic cells (DCs) are the most potent professional antigen-presenting cells for the initiation of antigen-specific immune responses, and antigen-loaded DCs have been regarded as promising vaccines in cancer immunotherapy. We previously demonstrated that RGD fiber-mutant adenovirus vector (AdRGD) could attain highly efficient gene transduction into human and murine DCs. The aim of the present study is to demonstrate the predominance of ex vivo genetic DC manipulation using AdRGD in improving the efficacy of DC-based immunotherapy targeting gp100, a melanoma-associated antigen (MAA). Vaccination with murine bone marrow-derived DCs transduced with AdRGD encoding gp100 (AdRGD-gp100/mBM-DCs) dramatically improved resistance to B16BL6 melanoma challenge and pulmonary metastasis as compared with immunization with conventional Ad-gp100-transduced mBM-DCs. The improvement in antimelanoma effects upon immunization with AdRGD-gp100/mBM-DCs correlated with enhanced cytotoxic activities of natural killer (NK) cells and B16BL6-specific cytotoxic T lymphocytes (CTLs). Furthermore, in vivo depletion analysis demonstrated that CD8+ CTLs and NK cells were the predominant effector cells responsible for the anti-B16BL6 immunity induced by vaccination with AdRGD-gp100/mBM-DCs, and that helper function of CD4+ T cells was necessary for sufficiently eliciting effector activity. These findings clearly revealed that highly efficient MAA gene transduction to DCs by AdRGD could greatly improve the efficacy of DC-based immunotherapy against melanoma.


Die Pharmazie | 2010

Cytotoxicity of amorphous silica particles against macrophage-like THP-1 cells depends on particle-size and surface properties.

Tomohiro Morishige; Yasuo Yoshioka; Hiroshi Inakura; Aya Tanabe; Xinglei Yao; Shin-ichi Tsunoda; Yasuo Tsutsumi; Yohei Mukai; Naoki Okada; Shinsaku Nakagawa


Archive | 2000

Method of intracellular sustained-release of drug and preparations

Tadanori Mayumi; Shinsaku Nakagawa; Yasuo Tsutsumi; Mahito Nakanishi


Biological & Pharmaceutical Bulletin | 1997

Therapeutic Effect of Cytomedicine on Mesangio-Proliferative Glomerulonephritis in Human Interleukin-6 Transgenic Mice

Naoki Okada; Hajime Miyamoto; Tatsunobu Yoshioka; Asao Katsume; Hiroyuki Saito; Keigo Yorozu; Otoya Ueda; Shinsaku Nakagawa; Yoshiyuki Ohsugi; Tadanori Mayumi


Archive | 2003

Physiologically active complex with TNF activity

Tadanori Mayumi; Yasuo Tsutsumi; Shinsaku Nakagawa; Hakuo Ikegami


Archive | 2005

Tumor necrosis factor-alpha mutants

Tadanori Mayumi; Yasuo Tsutsumi; Shinsaku Nakagawa; Tsunetaka Ohta


Archive | 2005

Tnf antagonists and tnf inhibitors comprising the same as the active ingredient

Tadanori Mayumi; Yasuo Tsutsumi; Shinsaku Nakagawa; Tsunetaka Ohta


Archive | 2008

Protein expression vector with methionine tag

Takeshi Doi; Tomohito Kiyono; Shinsaku Nakagawa; Takashi Nakagawa; Yoshiaki Okada; Tokuyuki Onishi; Tomoko Takano; Takao Yamamoto; 晋作 中川; 貴 中川; 健 土井; 徳幸 大西; 孝夫 山本; 欣晃 岡田; 智史 清野; 朋子 高野


Archive | 2004

Novel virus vector

Tadanori Mayumi; Shinsaku Nakagawa; Yasuo Tsutsumi; Koichi Kawasaki; Mitsuko Maeda; Takao Hayakawa; Hiroyuki Mizuguchi


Archive | 2003

Physiologically active complex

Tadanori Mayumi; Yasuo Tsutsumi; Shinsaku Nakagawa; Hakuo Ikegami

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Yasuo Tsutsumi

Tokushima Bunri University

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Iwao Ohizumi

Chugai Pharmaceutical Co.

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Naoki Okada

Nara Medical University

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Fumio Kamiyama

Kyoto Pharmaceutical University

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